PRACTICAL POINTERS
FOR
PRIMARY CARE
ABSTRACTED MONTHLY FROM THE JOURNALS
JUNE 2004
STATIN THERAPY IMPROVES OUTCOMES OF ACUTE CORONARY SYNDROMES
THE SEARCH FOR THE �HOLY GRAIL� OF CLINICALLY SIGNIFICANT CHD
20-YEAR NATURAL HISTORY OF EARLY, LOCALIZED PROSTATE CANCER
EFFECT OF LIPOSUCTION ON RISK FACTORS FOR CORONARY HEART DISEASE
THERMODYNAMICS, LIPOSUCTION, AND METABOLISM
SURGERY AND COMPRESSION VS COMPRESSION ALONE FOR VENOUS LEG
ULCERATION
FREQUENCY OF SYMPTOMS OF OVARIAN CANCER IN PRIMARY CARE
EFFECT OF LIFESTYLE CHANGES ON ERECTILE DYSFUNCTION IN OBESE MEN
WAITING FOR PLAN B�THE FDA DENIES OTC STATUS FOR EMERGENCY
CONTRACEPTION
FONDAPARINUX (Xa inhibitor) OR ENOXAPARIN FOR THE DEEP VENOUS
THROMBOSIS
LONG TERM DONEPEZIL (ARICEPT)
TREATMENT OF ALZHEIMER�S DISEASE
DONEPEZIL IN ALZHEIMER�S DISEASE�IS IT REALLY EFFECTIVE?
TACKLING THE NEXT INFLUENZA PANDEMIC
DANGERS OF ROSUVASTATIN (CRESTOR)
IDENTIFIED BEFORE AND AFTER FDA APPROVAL
JAMA, NEJM, BMJ, LANCET����������������������������������������������������������� PUBLISHED
BY PRACTICAL POINTERS, INC.
ARCHIVES INTERNAL MEDICINE������������������������� ������� ��������������� EDITED
BY RICHARD T. JAMES JR.�� MD
ANNALS
INTERNAL MEDICINE��������������������������������������������������� � 400 AVINGER LANE, SUITE 203
���������������������������������������������������������������������������������� � DAVIDSON NC 28036� USA��
[email protected]
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HIGHLIGHTS
and EDITORIAL COMMENTS��� JUNE 2004
6-1�� ASSOCIATION
OF STATIN THERAPY WITH OUTCOMES OF ACUTE CORONARY SYNDROMES:� The GRACE Study
Statin drugs may have effects in addition to their
effect on lipids. These include modulation of inflammation, inhibition of
platelet function and thrombosis, and enhancement of endothelial function. The
ability of statins to immediately
affect basic pathophysiologic mechanisms has increased interest in their
potential role in acute coronary syndromes. (ACS)
This study examined the association between previous
and early in-hospital statin therapy and outcomes of ACS.
Patients who presented with an ACS who were already
taking statins were less likely to present with ST-segment elevation MI,
experience a large infarct, and have important clinical complications, or die.
Much of the observed effect was lost if statin therapy
was not continued during hospitalization. Such patients had death rates similar
to patients who had never received statins. Withdrawal of statins reduces the
protective effect of statin pretreatment.�
In statin-na�ve patients, early statin therapy was
associated with an improvement in outcomes.
Should
primary care clinicians act on these conclusions?� Primary care clinicians often act on inconclusive evidence if the
putative benefit/harm-cost ratio of the intervention is high. Although the
outcomes of the study require confirmation and further experience, I believe
the benefit/harm-cost ratio of immediate statin therapy (as of immediate
aspirin therapy) for patients with ACS is potentially high. The benefit is
potentially life-saving.�
The harm and cost of short-term therapy is very low.� I would give a high-dose statin immediately on
presentation of a patient with presumed ACS.�
Those on
statins long-term should be continued on statins when admitted for ACS. Those
not on statins should start them immediately. And,. of course, continue after
discharge.
A study
�Lipid-Lowering Therapy And In-Hospital Mortality Following Major Non-Cardiac
Surgery�� (See Practical Pointers May
2004) also presents evidence of immediate protective effects of statins given
within the first 2 days after major surgery.�
RTJ
6-2 THE SEARCH FOR THE �HOLY GRAIL� OF CLINICALLY
SIGNIFICANT CORONARY ATHEROSCLEROSIS.
In some individuals, coronary atherosclerosis (CA) is stable for years, and in others
it is very unstable, with rapidly progressive lesions that result in sudden
death or an acute coronary syndrome. The diagnostic �Holy Grail� of coronary
atherosclerosis is not to be able to
identify coronary atherosclerosis (which almost all Americans have eventually)
but to identify individuals with unstable
coronary atherosclerotic lesions.
The editorialist describes the evolution of our
understanding the pathophysiology of CA�from the concept of a gradual process
that over decades narrows the arteries, to silent CA diagnosed by treadmill
exercise testing, to coronary angiography, and finally to efforts to detect
unstable plaques.
More myocardial infarctions occur in the larger
sub-population with negative results on a treadmill test than in those with
positive results. More myocardial infarctions are caused by hemodynamically
insignificant lesions than from high grade stenosis.
This
editorial was written in response to a meta-analysis in this issue of Archives
(pp 1285-92) which concluded that the coronary artery calcium score detected by
electron-beam computed tomography is an independent predictor of coronary
events.
The point of
the editorial was to state that the clinical utility of fast computed
tomography is not ready for prime time. While scanning may reveal
calcification, individuals with unstable coronary disease are not always
identified. A patient with potentially unstable coronary atherosclerotic
lesions may have mildly calcified or non-calcified arteries. Patients with
stable and unstable coronary atherosclerosis may have similar calcium scores.�
Prevention of
an essentially universal disease must be universal. Must we wait for screening
tests to detect �higher risk�, and only then encourage patients to change his
or her lifestyles?��
6-3�� NATURAL
HISTORY OF EARLY, LOCALIZED PROSTATE CANCER
Even without any initial treatment, only a small
proportion of patients diagnosed with PC at an early stage die of the disease
within 10 to 15 years following diagnosis.���
This observational study of the long-term natural
history of localized PC (diagnosed at a mean age 72) assessed disease
progression and mortality over years of watchful waiting.
Over 21 years, most patients died, mainly of causes
other than PC.� Only 9% survived.
Poor differentiation (in only 4% of the cohort) was a
strong predictor of cancer-specific death. This became evident within the first
5 years.
Further follow-up after
15 years revealed a substantial worsening of the cancer.� The cause-specific mortality from PC
increased by 3-fold during years 15 to 20 after diagnosis. .
�If our data reflect a real phenomenon, they would
imply that the probability of progression from localized and indolent to
metastatic and mortal disease increases markedly after long-term follow-up.�
This would support radical treatment, notably among
patients with an estimated life expectancy of over 15 years.
This would
argue for greater screening of younger men; less aggressive screening in older
men.� Long-term follow-up may be
necessary to observe the full benefits of early diagnosis and definitive
treatment in younger men. Older men likely die of other causes.
According to
these data, even if your PC is highly differentiated, you still run a risk of
about 2 in 100 of developing metastatic disease each year, and about 1 to 2
chances in 100 of dying of PC each year. If you survive over 15 years, these
chances are increased by 300%.
Prostate
cancer is never cured spontaneously.
If you live
long enough and are not treated, your chance of developing metastatic disease
(requiring orchiectomy or estrogen therapy) and fatal PC is high, even if you
have a highly differentiated PC. If you have a poorly differentiated grade PC
and are not treated, you will likely die of it within 5 years.
No doubt some
lives are saved by radical treatment. Who to treat and when to treat remains a
dilemma.� RTJ
6-4�� ABSENCE
OF AN EFFECT OF LIPOSUCTION ON INSULIN ACTION AND RISK FACTORS FOR CORONARY
HEART DISEASE.
Abdominal obesity (increased abdominal subcutaneous
fat, and increased visceral fat)� is
associated with insulin resistance and other risk factors for coronary
heart� disease (CHD).�
This study asked:�
Which of these fat deposits is associated with insulin resistance and
increased risk of CHD?
Liposuction in 15 grossly obese women reduced volume
of subcutaneous abdominal fat by 44%. Weight loss = 10 kg; total body fat
decreased by 18%. Liposuction did not significantly alter insulin sensitivity
(assessed by stimulation of glucose uptake in muscle); did not suppress glucose
production by the liver; and did not suppress lipolysis of adipose tissue.
Levels of C-reactive protein and other indicators of
inflammation did not change.
Other risk factors for CHD were unchanged (BP, plasma
glucose, insulin, and lipid concentrations).
Large-volume reduction in subcutaneous abdominal fat
mass did not have any beneficial metabolic effects despite a considerable
decrease in body weight, waist circumference, and plasma leptin concentrations
This provides insight into the mechanism by which
conventional weight loss improves insulin sensitivity.
Induction
of a negative energy balance, not simply a decrease in the mass of fat tissue,
is critical for achieving the metabolic benefits of weight loss. Even small
amounts of weight loss induced by a negative energy balance affect many
variables pertaining to body-fat composition and lipid metabolism�variables
that contribute to metabolic abnormalities associated with obesity.
Conventional weight loss decreases visceral fat mass, intrahepatic fat,
fat-cell size, and the rate of release of fatty acids from intra-abdominal
adipose tissue. Liposuction does not.
Adipose tissue is now recognized as an important
endocrine organ that produces several bioactive proteins. Fat loss by
conventional obesity treatment decreases plasma concentrations of C-reactive
protein, interleukin-6, and tumor necrosis factor. It improves insulin
sensitivity and inhibits vascular inflammation.
I abstracted
this article mainly to point out the risks associated with intra-abdominal fat
accumulation. Visceral fat drains directly into the portal circulation and into
the liver; subcutaneous fat drains into the general circulation. There is a
vast metabolic difference. RTJ
6-5�� THERMODYNAMICS,
LIPOSUCTION, AND METABOLISM
Hyperglycemia improves rapidly during caloric restriction. It outpaces the rate of weight
loss. About half of the improvements in glycemic control are achieved during
the first week of a negative energy balance, although the actual fat loss is
typically quite small. Substantial proportions of the early benefits of weight
loss on insulin resistance and hyperglycemia in type 2 diabetes may be
attributed to a negative energy balance.
Similar observations have been made concerning
hypertension. Much of the decrease in BP occurs fairly rapidly in response to a
negative energy balance. There is, however, a return toward hypertensive levels
once weight has reached a plateau.
Visceral adiposity is strongly associated with insulin
resistance. In animals, surgical resection of visceral fat tissue yields marked
and nearly immediate reduction in insulin resistance. The removal of an
equivalent amount of subcutaneous fat has little effect. The relation may be
related, at least in part, to the release of fatty acids into the portal circulation.
Adipose tissue has endocrine functions�synthesizing
leptin, adiponectin, and cytokines such as tumor necrosis factor,
interleukin-6, and C-reactive protein.
During World
War II type 2 diabetes practically disappeared in the Netherlands. This was
related to the near starvation conditions produced by the invasion by Germany.
RTJ
6-6�� COMPARISON
OF SURGERY AND COMPRESSION WITH COMPRESSION ALONE IN CHRONIC VENOUS ULCERATION
(ESCHAR study)
Multilayered elastic compression bandaging, leg
elevation, and exercise achieve healing in up to 80% at 24 weeks. However,
despite continued use of elastic compression stockings, the 12-month recurrence
rate is high. .
Simple superficial venous surgery (saphenous vein
ablation) theoretically removes the underlying venous incompetence in legs in
patients with isolated superficial reflux.
This randomized study reported that healing over 24
weeks was similar between groups. Recurrence of the ulcer within 1 year was
much less likely in the surgery group. [NNT = 6]
The
investigators state that about a quarter of patients with venous ulcers will
refuse surgery. Primary care clinicians then deal with these individuals as
best they can.� RTJ
6-7�� FREQUENCY
OF SYMPTOMS OF OVARIAN CANCER IN WOMEN PRESENTING TO PRIMARY CARE CLINICS.
Ovarian cancer (OC)
has been called the �silent killer� because symptoms are thought not to develop
until advanced stages when chance of cure is poor. Standard textbooks state
that symptoms do not occur until the disease is advanced. However, several
retrospective studies have indicated that the majority of patients with OC do
have early symptoms, although not necessarily gynecologic in nature.
Identification of early symptoms may have important
clinical implications because the 5-year survival for early stage disease is
70% to 90% compared with 20% to 30% for advanced-stage disease.
This study compared the frequency, severity, and
duration of symptoms typically associated with OC vs typical symptoms of women attending primary care clinics.
Women with OC described differences in symptoms
compared with the typical women presenting for care. Symptoms in patients with
OC were more frequent, more severe, and more often had an onset within 6 months.
Patients were much more likely to have a combination of abdominal bloating,
increased abdominal size, and urinary urgency.
These symptoms warrant further diagnostic intervention
because they are more likely to be associated with ovarian tumors.
This requires
the patient to carefully recall and describe her symptoms. And requires the
physician to be especially alert about fully understanding the onset, severity,
and duration of the symptoms. Clarity may be achieved only after several
visits.
Physicians should
ask women presenting with relatively new-onset symptoms specifically about
bloating, abdominal size and urinary symptoms. RTJ
6-8�� EFFECT OF
LIFESTYLE CHANGES ON ERECTILE DYSFUNCTION IN OBESE MEN
Erectile dysfunction (ED) is common, even in young men. Several modifiable lifestyle
factors are associated with maintenance of erectile function. Men with a body
mass index over 28 have a 30% higher risk of ED. The prevalence of overweight
and obesity in men reporting ED may be as high as 79%, although vascular
factors associated with obesity may play an important role.
This study of obese men with ED determined if a
long-term reduction in BMI and an increase in physical activity would
positively affect erectile functions.
At 2 years an intensive dietary-fitness program led to
over 10% loss of body weight and an increase in physical fitness. About 1/3 of
the men regained erectile function.
For many patients, ED is a manifestation of more
generalized pathology. Hypertension, hyperglycemia, and dyslipidemia are common
co-morbidities. Endothelial dysfunction is likely a pathogenic mechanism common
to these co-morbid states, risk of cardiovascular disease, and ED. The study
demonstrated improvements in endothelial function related to weight loss..
This is not,
however, a practical application. Few patients in primary care practice would
be able to complete such a program
The main
message is�maintain a healthy lifestyle, don�t wait to repair damage until
after it is done. RTJ
6-9�� WAITING
FOR PLAN B�THE FDA AND NONPRESCRIPTION ON EMERGENCY CONTRACEPTION
The proposal to switch to levonorgestrel emergency
contraception (EC; Plan B) to
over-the-counter status is in limbo. In May, the FDA rejected the application
for non-prescription sales. The acting director wrote that the company had �not
provided adequate data to support a conclusion that Plan B can be used safely by young adolescent women for emergency
contraception without the professional supervision of a practitioner licensed
by law to administer the drug�. In rejecting the application, the FDA also
rejected the advice of its medical review-staff. (A vote of 23 to 4 in favor of
nonprescription status.)
I would be
willing to wager that this decision will be reversed.� RTJ
6-10�� FONDAPARINUX
OR ENOXAPARIN FOR THE INITIAL TREATMENT OF SYMPTOMATIC DEEP VENOUS THROMBOSIS
Fondaparinux is a selective inhibitor of activated
factor X (Xa). Once-daily injections produce a predictable anticoagulant
effect.
This randomized, double-blind multicenter study
entered over 2200 patients (mean age 61) with established acute symptomatic DVT
of the lower extremity. Randomized to fondaparinux once-daily, or the
low-molecular-weight heparin enoxaparin twice-daily.� Many received injections at home. All were started on oral
anticoagulant therapy within 72 hours.
Double-blind subcutaneous injections were continued
for at least 5 days, or until the warfarin-induced INR reached 2.0 or greater.
Oral therapy was continued for 3 months
Over 3 months, outcomes were very similar between
groups:� recurrent thromboembolic
events, pulmonary embolism, recurrent DVT, major bleeding, and death.
�This study adds to the growing body of evidence that
inhibitors of activated factor X are effective, safe, and easy-to-use
antithrombotics.�
There are
several cautions about at-home treatment with either LMWH or fondaparinux: 1)
concern about undertreatment of DVT and resultant pulmonary embolism, and 2)
the need for careful laboratory monitoring of oral anticoagulation status
during the first days of treatment.
Should
fondaparinux be considered a �me too� drug?�
For a new drug to be adopted into primary care practice to replace an
old effective drug, important attributes must be established�must be
established as just as effective, or more effective; must be established as
just as safe or safer; must be more convenient to administer and require fewer
doses; must be less costly.�
Study
sponsored by Sanofi-Synthelabo and MV Organon.�
I always look for �spin� in drug-company sponsored studies. This study
looks straightforward. We look for confirmation. RTJ
6-11�� LONG
TERM DONEPEZIL (Aricept) TREATMENT IN
565 PATIENTS WITH ALZHEIMER�S DISEASE (AD 2000)
����� All three available cholinesterase
inhibitors produce small improvements in cognitive and global assessments in
selected patients mild-to-moderate AD over 3-12 months. Little is known about
long-term effectiveness, or their usefulness in patients with severe AD.� Nonetheless, the demand from clinicians and
patients remains strong.
This study asked whether the cholinesterase inhibitor
donepezil (Aricept) is cost effective
and produces worthwhile clinical and social improvements����� .
In absolute terms, donepezil group achieved a slightly
higher score on the mini-mental-examination within the first 36 weeks (about 1
point above baseline on a 30-point scale). Thereafter, scores deteriorated back
to baseline at 48 weeks and to minus 4 points at 112 weeks. The placebo group
lost points continuously
during
the 112 weeks.
Comparatively, over 112 weeks, donepezil group
(compared with placebo) maintained a slightly better score (a fraction of one
point) despite declining in absolute terms.
Donepezil was associated with no improvement in activities-of-daily living scale at any time up to 2 years, although,
compared with placebo, decline in ADL score was slightly slower.�
No significant benefits were seen vs placebo in institutionalization, progression of disability,
behavioral and psychological symptoms, psychopathology of carers, formal care
costs, adverse events, or deaths.
No evidence that costs of caring for patients with
Alzheimer�s disease in the community are reduced by
donepezil.
Any effect of donepezil on informal caregiver time is likely to be small.
Benefits of the acetylcholinesterase inhibitor,
donepezil, are �below minimally relevant thresholds�. It is not cost
effective� �The disappointingly little
overall benefit from donepezil cannot be taken lightly.�� Clinicians can validly question whether
other uses of scarce resources allocated for dementia would provide better
value than routine prescription of cholinesterase inhibitors. �
I believe
many patients are continuing to receive CIs far beyond the time of any hope of
benefit.
COST:� about $1600 per year quoted by
drugstore.com. As is often the case, the 10 mg dose costs just a few dollars
more per year than the 5 mg dose. A pill cutter may cut cost in half. There is
no statistically significant difference in effects of 10 mg vs 5 mg. Adverse
effects (eg, gastrointestinal) are greater with the 10 mg dose. RTJ
6-12�� AD 2000:
DONEPEZIL IN ALZHEIMER�S DISEASE
Patients seen in everyday practice differ from those
selected for inclusion in drug-company-sponsored trials. Drug companies use
highly refined selection criteria; often include specialized tests to aid
diagnosis;� restrict allowable
comorbidity and concomitant medications; and the extent of behavioral or
functional impairment. They pay for all protocol-related care, including
medications. �Typical selection criteria for industry sponsored trials would
exclude over 90% of out-patients with mild-to-moderate Alzheimer�s disease in
California who would otherwise be eligible to receive treatment. The
controversy about effectiveness, costs, and the clinical meaning of trial
results has been fueled by the use of participants who do not represent typical
patients.�
In the trial, donepezil and placebo were both
associated with a worsening over time. The mean differences on the MMSE and
activities of daily living scale represent a delay in symptom-worsening of
about 3 months.
This
commentary presents a clinically important point. It emphasizes the gulf which
may separate results of randomized controlled trials from benefits evident in
primary care practice. There may be a large difference between results reported
by a clinical trial for AD and clinical benefits for Mr. Jones, whose family
brings him into your office because of memory loss. A practical office-based,
�real world� trial is more meaningful and convincing. Beware of �spin�.
6-13�� TACKLING
THE NEXT INFLUENZA PANDEMIC
�We must now hasten the preparations for another
inevitable influenza pandemic.�
A recent systemic review concluded that the
prophylactic use of neuraminidase inhibitors (NIs) could lead to a reduction of 70-90% in risk of symptomatic
flu. These drugs have shown efficacy in preventing transmission of influenza in
institutions and community setting. The availability of a highly effective
supplement to vaccination opens to debate the appropriate role of NIs and other
antiviral drugs in the control of pandemic influenza.
What might be an alternative strategy? It is known
that �ring� vaccination, which has been used in the past, will quell smallpox
outbreaks. The strategy entails post-exposure vaccination of close contacts.
For smallpox, this approach has provided a wide safety net of prevention, while
focusing vaccination where it was needed most. Ring prophylaxis may be
applicable to the initial management of an influenza pandemic. NI treatment of
influenza cases with the infection and prophylactic use for their contacts may
decrease attack rates substantially. It limits usage of the drug to where it is
needed most.
Antiviral ring prophylaxis for flu has proved to be
effective in family settings. It requires only short term daily treatment for a
period of 5-10 days, and targets a relatively limited proportion of the
population. Used in this way, NIs may be dispensed more rapidly and require
less of a stockpile.
COST:� Tamiflu, 75 mg cost about $6 each capsule�
$60 for a treatment course; $42 for 7-day prophylaxis. I believe most patients
would consider this a bargain.
Healthcare
workers should be the first in line to receive �ring� prophylaxis, and to
continue it until assured that the current vaccine is effective.
Primary care
clinicians will likely use NIs freely to unvaccinated family members during an
epidemic of flu.� RTJ
6-14�� DANGERS
OF ROSUVASTATIN (Crestor) IDENTIFIED
BEFORE AND AFTER FDA APPROVAL
The lipid-lowering drug rosuvastatin (Crestor; Astra-Zeneca) is currently in
the midst of the most heavily financed launch of a prescription drug ever.
The correspondent presents available pre�marketing and
post-marketing evidence of the adverse effects of the drug. The preapproval
document stated that 80 mg is associated with a high frequency of creatine
kinase elevations (CK 10 times upper normal). Crestor was approved with the belief that lower doses would be much
safer. The 80 mg dose was subsequently discontinued.
Since marketing of rosuvastatin, there have been 18
additional cases of rhabdomyolyis. Two patients were using 40 mg; five using 20
mg; 11 using 10 mg.
The 10, 20, and 40 mg doses have been associated with
a risk of renal toxicity.� There have
been 8 reported cases of acute renal failure and 4 of renal insufficiency since
marketing began. Nine were using 10 mg; two using 40 mg. �By now, the number of
reported cases of rhabdomyolyis and renal insufficiency or renal failure�20 of
which have occurred in people using 10 mg�is certain to have increased
substantially from the number filed by April 13, 2004.�
A statistical review of comparative efficacy found no
significant difference in LDL-cholesterol lowering between 5, 10, and 20 mg of
rosuvastatin and 20, 40 and 80 mg of atorvastatin. (This surrogate laboratory finding does not indicate comparative
clinical effectiveness.)
�� Comment:
These letters
raise an important clinical point. When should primary care clinicians add a
new drug to their practice?
Is Crestor a
unique and important addition to therapeutics?�
Or is it just a �me-too� drug? Should primary care clinicians prescribe
it a the present time?�
1. Is
Crestor more effective in lowering LDL?��
No. Other statins lower LDL just as much, although they might require a
higher dose. Remember, this is a laboratory endpoint, not a clinical endpoint.� Clinical efficacy has not been established.
2.
Is Crestor as safe as other statins?�
This is the dispute. That the 80 mg dose has been withdrawn because of
toxicity raises caution. It will take several years of general use in the USA
for the FDA to determine toxicity. Certainly, Crestor is not safer.
3.
Is Crestor more convenient to administer. Does it require fewer doses? No
4.
Is Crestor less costly?� No. Costs are
comparable.
The first
letter may raise an entirely unwarranted red flag. I do not know.� I abstracted these letters mainly to
reinforce the long-honored and oft-repeated admonishment to primary care
clinicians not to be the first to prescribe a new drug, no matter how highly
touted, unless it is known to be safe and carry unique and important benefits.
Regardless of the question of toxicity, I do not believe the benefits of
Crestor are unique or comparatively important.
I would not
prescribe Crestor at this time. If it proves equally or less toxic, maintains
its reported comparative efficacy in reducing LDL-c, and has a significant cost
benefit, I would consider prescribing it.
I have faced
(as have most older clinicians) the embarrassment of having a drug I had
prescribed suddenly withdrawn from the market. The patient will ask for an
explanation. RTJ
Statin
drugs may have important benefits if given immediately for acute coronary
syndrome
6-1��
ASSOCIATION OF STATIN THERAPY WITH OUTCOMES OF ACUTE CORONARY
SYNDROMES:� The GRACE Study
����� Statin drugs may have effects in addition
to their effect on lipids. These include modulation of inflammation, inhibition
of platelet function and thrombosis, and enhancement of endothelial function.
The ability of statins to immediately
affect basic pathophysiologic mechanisms has increased interest in their
potential role in acute coronary syndromes. (ACS)
This study examined the association between previous
and early in-hospital statin therapy and outcomes of ACS.
Conclusion:�
Statin therapy can modulate early pathophysiologic processes in patients
with ACS.
STUDY
1. Multicountry observational study
enrolled over 19 500 patients with ACS from 1999 to 2002.�
2. All had symptoms of acute ischemia, and
at least one of the following:� ECG
changes consistent with ACS, serial increases in biochemical markers of
myocardial necrosis, documentation of coronary artery disease.
3. Treatments were defined as:� no statin use;� long-term use at home and within 7 days of the presenting event (but not in hospital);�� use in hospital only (not before hospitalization); and use both before and during hospitalization.
4. Determined hospital complications, and
hospital deaths related to statin use. The composite end-point included death,
in-hospital MI, and stroke.
RESULTS
1. 21% (4056) of the patients with ACS
were already taking statins when they presented to the hospitals.� Patients who were already taking statins
when they presented to the hospital were less likely to have ST-segment
elevation.� (Odds ratio = 0.79);
myocardial infarction (OR = 0.78); and other complications.
2.
Incidence of hospital outcomes according to previous statin therapy:
Long-term use (%)������� No long term use (%)
Creatine phosphokinase > 2 times normal���������������������� 28������������������������������������������� 45
MI after 24 hours or recurrent MI������������������������������������ 7��������������������������������������������� 10
Congestive heart failure����������������������������������������������������� 12������������������������������������������� 15
Cardiogenic shock�������������������������������������������������������������� 2��������������������������������������������� 5
Cardiac arrest����������������������������������������������������������������������� 3����� ��������������������������������������� 6
Death������������������������������������������������������������������������������������ 3��������������������������������������������� 7
Final diagnosis:
ST-elevation MI���������������������������������������������������������� 18������������������������������������������� 38
Non-ST-elevation MI������������������������������������������������� 30������������������������������������������� 30
Unstable angina���������������������������������������������������������� 52������������������������������������������� 32
3.
Hospital outcomes according to statin groups (%):
No statin������� Long-term
only���� In hospital only��� Long-term and hospital
Cardiogenic shock�������������������������������������� 6.5������������������ 8.7�������������������������� 2.5������������������������� 1.6
Cardiac arrest����������������������������������������������� 7.5������������������ 8.2�������������������������� 3.4�������������������������� 1.9
Ventricular tachycardia or fibrillation������ 5��������������������� 6.2�������������������������� 4.1�������������������������� 2.8
Death������������������������������������������������������������ 9.9������������������ 11.6������������������������ 2.1�������������������������� 2.1
Death, stroke, or in-hospital MI��������������� 17.9���������������� 17.3 ����������������������� 15.3������������������������ 9.2�
(Note that
the 2 groups receiving statins in hospital had better outcomes than those who
received no statins or received them long-term and discontinued on admission.)
DISCUSSION
1. Results suggest that previous statin
therapy significantly affects severity of hospital presentation and hospital
outcomes. Patients who presented with an ACS who were already taking statins
were less likely to present with ST-segment elevation MI, experience a large
infarct, and have important clinical complications, or die.
2. Much of the observed effect was lost if
statin therapy was not continued during hospitalization. Such patients had
death rates similar to patients who had never received statins. Withdrawal of
statins reduces the protective effect of statin pretreatment
3. Previous studies have reported that
statins (eg, atorvastatin) results in early (within 48 hours) decrease in
C-reactive protein and augmentation of endothelium-dependent blood flow.
Discontinuation in the hospital after admission for an ACS may cause a rebound
phenomenon in which the protective pathophysiologic mechanisms are rapidly
reversed.
4. �These findings are similar to the
results of studies that have examined the effects of previous aspirin therapy
on acute coronary syndrome presentation.� No reason why aspirin, beta-blockers,
and ACE inhibitors cannot be used concomitantly with statins.
5. Some data suggests that initiation of
lipid-lowering therapy during hospitalization in patients with acute MI is
associated with long-term adherence and better post-discharge outcomes.
6. The authors state that their
observational study cannot exclude possible multiple confounding factors.
CONCLUSION�����
This large observational study suggests that patients
who are taking statins when they present with an ACS have less severe
presentations, fewer in-hospital complications, and lower hospital death rates.
The observed beneficial effect on outcomes is less
apparent in those who did not continue statins during hospitalization.
In statin-na�ve patients, early statin therapy was
associated with an improvement in outcomes.
Annals Int Med June 1, 2004;� 140: 857-66 Original investigation by
the GRACE (Global Registry of Acute Coronary Events) investigators, first
author Frederick A Spencer, University of Massachusetts Medical School,
Worcester.
�� Comment:
Should
primary care clinicians act on these conclusions?� Primary care clinicians often act on inconclusive evidence if the
putative benefit/harm-cost ratio of the intervention is high. Although the
outcomes of the study require confirmation and further experience, I believe
the benefit/harm-cost ratio of immediate statin therapy (as of immediate
aspirin therapy) for patients with ACS is potentially high. The benefit is
potentially life-saving.�
The harm and cost of short-term therapy is very low.� I would give a high-dose statin immediately on
presentation of a patient with presumed ACS.�
Those on
statins long-term should be continued on statins when admitted for ACS. Those
not on statins should start them immediately.�
A study
�Lipid-Lowering Therapy And In-Hospital Mortality Following Major Non-Cardiac
Surgery�� (See Practical Pointers May
2004 ) also presents evidence of immediate protective effects of statins given
within the first 2 days after major surgery.�
RTJ
6-2��
THE SEARCH FOR THE �HOLY GRAIL� OF CLINICALLY SIGNIFICANT CORONARY
ATHEROSCLEROSIS.
In some individuals, coronary atherosclerosis is
stable for years, and in others it is very unstable, with rapidly progressive
lesions that result in sudden death or an acute coronary syndrome. The
diagnostic �Holy Grail� of coronary atherosclerosis is not to be able to identify coronary atherosclerosis (which almost
all Americans have eventually) but to identify individuals with unstable coronary atherosclerotic
lesions.
Shortly after World War II, it became apparent that
the greatest threat to the lives of Americans was not from without, but from
within. Our greatest threat was cardiovascular disease, with 50% of Americans
dying from it.
The medical profession�s initial concept was that
coronary atherosclerosis was characterized by a process that gradually, over
decades, narrows the coronary arteries. We systematically looked for silent
coronary disease with �executive physicals� that emphasized the treadmill
exercise test. We were surprised to find that more myocardial infarctions
occurred in the larger sub-population with negative results than in those with
positive results.
These observations led to the era of coronary
angiography, during which we assumed that angiography was the gold standard for
identifying clinically significant coronary artery disease. Again, we found
that, although a high grade coronary lesion was more likely to occlude, more
myocardial infarctions were caused by hemodynamically insignificant lesions
than from high grade stenosis. And there were many more of the hemodynamically
insignificant lesions. When plaques in hemodynamically insignificant lesions
ruptured, coronary artery thrombosis might occur with subsequent sudden death
or an acute coronary syndrome. Most often the rupture is clinically silent. An
estimated one in 100 plaque ruptures actually results in an acute coronary
syndrome. The healing process leads to progressive coronary stenosis.
More recently, coronary intravascular ultrasound
demonstrated that early atherosclerosis often results in �positive remodeling�
of the coronary artery and does not narrow the lumen until the process is far
advanced. As a result, minimal lesions detected by coronary angiography may
reflect advanced disease. These minimal lesions, if unstable, can result in
plaque rupture and major acute coronary events.
How can we identify these unstable plaques? They are
characterized by inflammation. The inflammatory cells produce cytokines that
stimulate the liver to produce C-reactive proteins (CRP) and other acute phase
reactants. High-sensitivity CRP appears to be a marker for more unstable
coronary disease. Increasing levels of high-sensitivity CRP and an increasing
ratio of total cholesterol to high density lipoprotein cholesterol can identify
increased risk.
Scanning the coronary arteries for calcium, and
assuming that one is identifying unstable coronary disease, or the risk for
developing unstable coronary disease, is like scanning an egg and trying to
assess the composition and stability of the yoke by the amount of calcium in
the shell. Unstable coronary atherosclerosis undoubtedly develops before
calcification.
The search for the �Holy Grail�, a fail-safe method
for detecting clinically significant coronary atherosclerotic disease, must
continue.
Archives Int Med June 28, 2004; 164:
1266-67� Editorial by Gordon A Ewy,
University of Arizona, Tucson.
�� Comment:
This
editorial was written in response to a meta-analysis in this issue of Archives
(pp 1285-92) which concluded that the coronary artery calcium score detected by
electron-beam computed tomography is an independent predictor of coronary
events.
The point of
the editorial was to state that the clinical utility of fast computed
tomography is not ready for prime time. While scanning may reveal
calcification, individuals with unstable coronary disease are not always
identified. A patient with potentially unstable coronary atherosclerotic
lesions may have mildly calcified or non-calcified arteries. Patients with
stable and unstable coronary atherosclerosis may have similar calcium scores.
Prevention of
an essentially universal disease must be universal. Must we wait for screening
tests to detect �higher risk�, and only then encourage patients to change
lifestyles?� RTJ
6-3��
NATURAL HISTORY OF EARLY, LOCALIZED PROSTATE CANCER
The challenge of prostate cancer (PC) is to maximize the possibilities of survival without extensive
over- treatment. Even without any initial treatment, only a small proportion of
patients diagnosed at an early stage die from PC within 10 to 15 years
following diagnosis.
No study has hitherto adequately analyzed whether
patients who escaped metastases and death without treatment during 10 to 15
years after diagnosis continue to have an indolent, nonfatal disease course, or
whether in the long-term tumor progression takes a more aggressive turn.
Because it takes several years after operation for any
benefit to emerge, age at diagnosis, comorbidity, and long-term natural history
will determine the potential advantage from radical primary treatment.
This observational study of the long-term natural
history of PC assessed disease progression and mortality after years of
watchful waiting.
Conclusion:�
Although most PCs diagnosed at an early stage have an indolent course,
local recurrence and aggressive metastatic disease may occur in the long term.
STUDY
1. Population-based cohort study followed
223 untreated patients (age range at diagnosis 41-91; mean = 72) with PC over a
mean of 21 years. All had early stage PC: T1, T2;� NX; M0.
[T1-T2 = PC confined within gland; T1 = nodule
surrounded by normal tissue, not palpable; T2 = palpable disease with a large
nodule or multiple nodules; NX (no nodes involved); M0 (no metastases).]
2. The great majority of PCs were highly
differentiated; only 4% were poorly differentiated.
3. None received a PSA determination. The
test was not available when the study began. About half were diagnosed by
histopathologic examinations of specimens obtained at operation for suspected
benign prostatic hyperplasia.
4. All were followed up from diagnosis
until death, or until September 2001, when the study was terminated.� All were followed by clinical examinations,
laboratory tests, and bone scans. If the PC progressed to symptomatic disease,
estrogens or orchiectomy were prescribed. Local progression was defined as
tumor growth through the prostate capsule (T3) as judged by digital rectal examination.
Development to metastases (M1) was classified as generalized disease.
5. Main outcome = progression-free,
cause-specific, and overall survival.
RESULTS
1. Over the 21 years, most patients died
(mainly of causes other than PC)� Only
9% survived.
2. Poor differentiation was a strong
predictor of cancer-specific death. This became evident within the first 5
years.
3. Most cancers had an indolent course
during the first 10 to 15 years. Cancer progression and mortality remained
fairly constant during the first 15 years following diagnosis. Progression to
metastatic disease was 18 per1000 person-years; PC mortality rate = 15 per 1000
person-years. In contrast, after 15 years, an approximately 3-fold higher rate
occurred in both progression and mortality.
4. During the entire 21-year observation,
PC was considered the cause of death in 16%. Among patients under age 70 at diagnosis, 22% died from
PC. At higher ages at diagnosis, the mortality from PC decreased markedly.
5. Further follow-up after 15 years (n =
49 patients) revealed a substantial worsening of the cancer.� Progression-free survival decreased from 45%
to 36%; survival without metastases from 77% to 51%; and prostate cancer
specific survival from 79% to 54%. PC mortality rate increased from 15 per 1000
person-years during the first 15 years to 44 per 1000 beyond 15 years.
DISCUSSION
1. This study revealed an unexpected
change in prognostic outlook after 15 years of observation. The cause-specific
mortality from PC increased by 3-fold after this time as compared with the
first 15 years.
2. The increase occurred consistently
across stage and grade except for poorly differentiated cancers in which excess
mortality became manifest during the first 5 years.
3. Mortality rates were mirrored closely
by rates of disease progression to metastatic disease.
4. �If our data reflect a real phenomenon,
they would imply that the probability of progression from localized and
indolent to metastatic and mortal disease increases markedly after long-term follow-up.�
5. PC mortality was slightly higher among
patients whose cancer was diagnosed at age 70 or younger.
CONCLUSION
Most PCs diagnosed at an early stage have an indolent
course. Local tumor progression and aggressive metastatic disease may develop
long-term (after 15 years). This would support radical treatment, notably among
patients with an estimated life-expectancy of over 15 years.
JAMA June 9, 2002; 291: 2713-19 Original
investigation, first author Jan-Erik Johansson, Orebro University Hospital,
Orebro Sweden.
�� Comment:
The study is
unique. It will never be repeated.
This would
argue for greater screening of younger men; less aggressive screening in older
men. Long term follow-up may be necessary to observe the full benefits of early
diagnosis and treatment in younger men.
According to
these data, even if your PC is highly differentiated, you still run a risk of
about 2 in 100 of developing metastatic disease each year, and about 1 to 2
chances in 100 of dying of PC each year. If you survive over 15 years, these
chances are increased by 300%.
Prostate
cancer is never cured spontaneously.
If you live
long enough and are not treated, your chance of eventually developing
metastatic disease (requiring orchiectomy or estrogen therapy) and fatal PC is
high, even if you have a highly differentiated PC. If you have a poorly
differentiated grade PC and are not treated, you will likely die of it within 5
years.
No doubt some
lives are saved by radical treatment. Which ones?� RTJ
Adipose
tissue is an important endocrine organ that produces several bioactive proteins
Abdominal obesity
(increased abdominal subcutaneous fat, and increased visceral fat) is
associated with insulin resistance and other risk factors for coronary heart
disease (CHD).�
This study asked:�
Which of these fat deposits is associated with insulin resistance and
increased risk of CHD?
Conclusion:�
Removal of subcutaneous abdominal fat does not alleviate insulin
resistance.
STUDY
1. Followed 15 sedentary obese women (mean
age 42) with increased abdominal circumference (mean = 108 cm; mean body mass
index = 38). All had been scheduled for abdominal liposuction for cosmetic
reasons.
2. Evaluated insulin sensitivity of liver,
skeletal muscle and adipose tissue with a euglycemic-hyperinsulinemic clamp
procedure (see text) before and after
liposuction.
3. Also determined levels of inflammatory
mediators and other risk factors for CHD.
RESULTS
1. Liposuction reduced volume of
subcutaneous abdominal fat by 44%. Weight loss = 10 kg; total body fat
decreased by 18%.
2. Liposuction did not significantly alter
insulin sensitivity (assessed by stimulation of glucose uptake in muscle); did
not suppress glucose production by the liver; and did not suppress lipolysis of
adipose tissue.
3. Levels of C-reactive protein and other
indicators of inflammation did not change.
4. Other risk factors for CHD were
unchanged (BP, plasma glucose, insulin, and lipid concentrations).
DISCUSSION
1. Large-volume reduction in subcutaneous
abdominal fat mass did not have any beneficial metabolic effects despite a
considerable decrease in body weight, waist circumference, and plasma leptin
concentrations.
2. The amount of fat removed was
equivalent to weight loss achieved by optimal behavioral and pharmacological
treatments. (about 12% of body weight). This amount of weight loss by these
methods usually results in marked improvements in the metabolic abnormalities
associated with obesity (insulin sensitivity, BP, and lipids), and reduces
levels of circulating markers of inflammation.
3. �It is striking that the amount of fat
loss achieved by liposuction�did not
improve any of these metabolic variables.�
4. This provides insight into the
mechanism by which conventional weight loss improves insulin sensitivity.� Induction of a negative energy balance, not
simply a decrease in the mass of fat tissue, is critical for achieving the
metabolic benefits of weight loss. Even small amounts of weight loss induced by
a negative energy balance affect many variables pertaining to body-fat
composition and lipid metabolism�variables that contribute to metabolic
abnormalities associated with obesity. Weight loss decreases visceral fat mass,
intrahepatic fat, fat-cell size, and the rate of release of fatty acids from
adipose tissue. Liposuction does not.
5. Adipose tissue is an important
endocrine organ that produces several bioactive proteins, including
interleukin-6, tumor necrosis factor, and adiponectin. Interleukin-6 and tumor
necrosis factor can cause insulin resistance and atherosclerosis by impairing
insulin signaling, stimulating lipolysis and fatty acid release, increasing
hepatic synthesis of C-reactive protein, and increasing systemic inflammation,
whereas the production of adiponectin by adipose tissue can improve insulin sensitivity and inhibit
vascular inflammation. Fat loss by conventional obesity treatment decreases
concentrations of C-reactive protein, interleukin-6, and tumor necrosis factor.
Conversely, it increases
concentration of adiponectin. .
6. Liposuction did decrease plasma leptin
concentrations, a marker of adipose-tissue mass.
7. Liposuction may have cosmetic benefits,
but no other.
8. �The effects of a negative energy
balance on specific endogenous triglyceride depots and inflammation, which are
not altered by liposuction, may be necessary to achieve the clinical benefits
of therapy for obesity.�
CONCLUSION
����� Abdominal liposuction does not improve
obesity-associated metabolic abnormalities. It does not achieve the metabolic
benefits of conventional weight loss.
NEJM June 17, 2004; 350:� 2549-57� Original
investigation, first author Samuel Klein, Washington University School of
Medicine, St. Louis, MO.
�� Comment:
I abstracted
this article mainly to point out the risks associated with intra-abdominal fat
accumulation. Visceral fat depots drain directly into the portal circulation
and into the liver; subcutaneous fat depots drain into the general circulation.
There is a vast metabolic difference.
I suspect the
investigators really did not believe subcutaneous abdominal liposuction would
improve metabolic functions. It is important, nevertheless, to have objective
data.
C- reactive
protein is a favored marker of inflammation because a high-sensitivity
determination is available at modest cost.
Liposuction
is the most common aesthetic procedure performed in the USA. New techniques
make it possible to remove considerable amounts of subcutaneous fat tissue. RTJ
Some
adipose tissue has endocrine functions
6-5 THERMODYNAMICS, LIPOSUCTION, AND
METABOLISM
(This editorial comments and expands on the preceding
study.)
The regulation of body weight adheres to the principle
of thermodynamics: a positive energy balance causes weight gain, and a negative
balance weight loss. (Calories still
count.) There is good evidence that a moderate amount of weight loss plus
increased physical activity reduces the likelihood of progression from impaired
glucose tolerance to type 2 diabetes.
The editorialist comments on two important metabolic
benefits that are directly related to effect of a negative energy balance: 1)
rapid improvement in hyperglycemia, and hypertension, and 2) benefits on
metabolic risk factors related to loss of visceral adiposity.
1) Hyperglycemia improves rapidly during caloric restriction. It outpaces the rate of weight
loss. About half of the improvements in glycemic control are achieved during
the first week of a negative energy balance, although the actual fat loss is
typically quite small during short periods of caloric restriction. Substantial
proportions of the early benefits of weight loss on insulin resistance and hyperglycemia
in type 2 diabetes may be attributed to a negative energy balance.
Similar observations have been made concerning
hypertension. Much of the decrease in BP occurs fairly rapidly in response to a
negative energy balance. There is, however, a return toward hypertensive levels
once weight has reached a plateau.
Weight loss by liposuction has no comparable
beneficial effects.�
2) Visceral adiposity is strongly associated with
insulin resistance. In animals, surgical resection of visceral fat tissue
yields marked and nearly immediate improvement in insulin resistance. The
removal of an equivalent amount of subcutaneous fat has little effect.
The relation may be related, at least in part, to the
release of fatty acids into the portal circulation.
Adipose tissue has endocrine functions�synthesizing
leptin, and cytokines such as tumor necrosis factor, interleukin-6, and
C-reactive protein.
It may well be that a negative energy balance permits
a rapid improvement in fat content within liver and muscle, depots of stored
energy that affect the severity of insulin resistance.
NEJM June 17, 2004; 350: 2542-44� Editorial by David E Kelley. University of
Pittsburgh, PA.
�� Comment:
During World
War II type 2 diabetes practically disappeared in the Netherlands. This was
related to the near starvation conditions produced by the invasion by Germany.
RTJ
6-6��
COMPARISON OF SURGERY AND COMPRESSION WITH COMPRESSION ALONE IN CHRONIC
VENOUS ULCERATION (ESCHAR study)
Chronic venous ulceration affects 1-2% of the
population. It usually has a protracted course of healing and can recur many
times.
Multilayered elastic compression bandaging, leg
elevation, and exercise achieve healing in up to 80% at 24 weeks. However,
despite continued use of elastic compression stockings, the 12-month recurrence
rate is 25% or higher.
Conservative measures do little to address the
underlying abnormal venous function. About 50% of patients with ulceration have
reflux in the superficial system of veins alone; about 40% in the superficial
and deep venous systems; and about 10% reflux in the deep system alone.
Simple superficial venous surgery (saphenous vein
ablation) theoretically removes the underlying venous incompetence in legs in
patients with isolated superficial reflux. Surgery to correct venous reflux in
the deep veins is complex and of unproven value.
This study assessed the effect of surgery +
compression vs compression alone on healing and recurrence of ulcers.
Conclusion:�
Surgery reduced 12-month recurrence. It did not hasten healing.
STUDY
1. Performed venous Doppler ultrasound
imaging of ulcerated or recently healed legs in 500 consecutive patients (mean
age 73).�
2.
Randomized those with isolated superficial venous reflux and mixed
superficial-deep reflux to:�
1) Compression alone, or 2) Compression + surgery of
superficial veins.
3.
Compression consisted of multilayer compression bandaging every week until
healing occurred.� Then continued
compression with below-knee support stockings.
4.
Primary endpoints = 24-week healing rates and 12-month recurrence rates.
RESULTS
1.
Healing rates over 24 weeks were similar between groups
Surgery-compression���� Compression
alone�������
Isolated superficial �������������������������������������������� 65%
�������������������������������������� 66%���������������������������������������
Superficial and segmental deep ����������������������� 56% �������������������������������������� 57%
�������������� �����������������
2.
Twelve month ulcer recurrence was significantly reduced in the surgery +
compression group (12% vs 28%).
Surgery-compression���� Compression
alone������� NNT
Isolated superficial��������������������������������������������� 12%��������������������������������������� 28%��������������������������������������� 6
Superficial and segmental deep������������������������ 9%����������������������������������������� 25%��������������������������������������� 6
3. Adverse events: few surgical patients
developed deep vein thrombosis, wound infection, hematoma, and phlebitis.
DISCUSSION
1. Postoperative ultrasound has shown that
segmental reflux in the deep veins is reversed in about 50% of cases by
ablative superficial venous surgery.
2. Healing is not enhanced at 24 weeks by
superficial vein surgery. This is probably because the hemodynamic benefits of
compression are as great as surgery.
3. Superficial vein surgery significantly
reduced recurrence of ulcer at one year.
CONCLUSION
Surgical correction of superficial venous reflux
reduced 12-month recurrence of� leg
ulcers. It did not hasten healing.
Lancet June 5, 2004; 363: 1854-59� Original investigation, first author Jamie R
Barwell, Cheltenham General Hospital, Cheltenham, UK
ESCHAR��� Effect
of Surgery and Compression on Healing And Recurrence
�� Comment:
The
investigators state that about a quarter of patients with venous ulcers will
refuse surgery. Primary care clinicians then deal with these individuals as
best they can.� RTJ
�Ovarian
cancer is not a silent disease.�
6-7��
FREQUENCY OF SYMPTOMS OF OVARIAN CANCER IN WOMEN PRESENTING TO PRIMARY
CARE CLINICS.
Ovarian cancer (OC)
has been called the �silent killer� because symptoms are thought not to develop
until advanced stages when chance of cure is poor. Standard textbooks state
that symptoms do not occur until the disease is advanced. However, several
retrospective studies have indicated that the majority of patients with OC do
have early symptoms, although not necessarily gynecologic in nature.
Identification of early symptoms may have important
clinical implications because the 5-year survival for early stage disease is
70% to 90% compared with 20% to 30% for advanced-stage disease.
Distinguishing symptoms of OC from those that
typically occur in women seeking medical advice remains problematic.
This study compared the frequency, severity, and duration
of symptoms associated with OC with symptoms in a typical population of women
presenting to primary care clinics.
Conclusion:�
Suspicion of OC may be increased if symptoms occur more frequently, are
more severe, and have begun within the past 6 months. Combined abdominal
bloating, increased abdominal size, and urinary symptoms occur much more
frequently in OC patients. .
STUDY
1. Prospective case-control study of women
attending primary care clinics. All voluntarily completed a survey of symptoms experienced
over the past year.� Symptoms severity
was rated on a 5-point scale. Duration was recorded, and frequency indicated as
the number of episodes per month.
A.�
Cases: 128 women with a pelvic mass who were about to undergo surgery
(84 benign; 44 malignant). (Median age of OC patients = 55)
B. Controls:� Over 1700 women (median age 45) actively seeking medical care who
visited a clinic for a total of about 12 000 times.
2. Participants were given a list of 20
symptoms that had been reported to be associated with OC. These included pain,
eating difficulties, abdominal symptoms, bladder symptoms, bowel symptoms,
menstrual and sexual intercourse symptoms, and constitutional symptoms.
3. Main outcome measures:� comparison of self-reported symptoms between
OC patients (the �cases�) and the other clinic visitors.(the �controls�).
RESULTS
1.
Women with OC described differences in symptoms:
A. Frequency:� Women with OC typically experienced more frequent occurrence of
symptoms�20 to 30 times a month (almost daily). Clinic patients typically
reported symptoms which occurred 2 to 3 times per month. In younger women,
symptoms often appeared with menses.
B. Severity:� Symptoms in OC patients were in general more severe. (Controls
typically 2 to 3 on a scale of 1-5: OC patients typically 4 or 5.
C. Onset: New symptoms in OC patients were
of more recent onset:� 60% within 3
months; only 14% started over 1 year ago.�
Women with OC in general had symptoms of significantly shorter
duration�6 months or less. For women with irritable bowel syndrome and controls
the median duration of symptoms was typically 12 to 24 months.
D. Median number of symptoms: OC eight
different symptoms, 4 recurring; controls 4 different symptoms, and 2
recurring.
E. Type of symptom:
OC patients described several symptoms more frequently
than controls:
Odds ratio cases vs controls
Increased abdominal size������������������� 7.4
Bloating ����������������������������������������������� 3.6
Urinary urgency���������������������������������� 2.5
Pelvic pain�������������������������������������������� 2.2
2. The combination of bloating, increased
abdominal size, and urinary symptoms was found in 43% of those with OC, but
only in 8% of controls, and in 13% of women with irritable bowel syndrome (IBS). Women with IBS may present more
difficulty in differential diagnosis. There are differences. Women with IBS
were significantly more likely to have fatigue, gastrointestinal � complaints, and abdominal pain. . Duration of
their symptoms is longer.
3. All symptoms in controls were less
common as age increased except for urinary tract symptoms which increased in
severity with age. (Be especially alert
when an older woman presents a changing symptom pattern as described above.)
4. Any ovarian mass (benign, borderline or
malignant) has a high likelihood of producing symptoms. Most women with benign
ovarian masses had complaints similar to those of OC.
DISCUSSION
1. No screening test or surveillance
strategy has been shown to reduce ovarian cancer mortality. Screening the
general population is not effective.
2. It is important to understand the
symptoms of OC so that the diagnosis can be made as soon as possible.
3. Theoretically, early diagnosis would
lead to greater chance of cure. Optimal cytoreduction of the tumor is
associated with cure in up to 40% and median survival of more than 50 months vs
20% and 36 months for suboptimal cytoreduction.
4. Symptoms typical of OC should not be
attributed to the aging process.
5.
�Ovarian cancer is not a silent disease.�
CONCLUSION
Symptoms that are more severe and frequent than
expected and of more recent onset warrant further diagnostic intervention
because they are more likely to be associated with ovarian tumors, both benign
and malignant.
JAMA June 9, 2004; 291: 2705-12� Original investigation, first author Barbara
A Goff, University of Washington School of Medicine, Seattle.� www.jama.com
An editorial in this issue of JAMA (pp 2755-56, first
author Mary B Daly, Fox Chase Cancer Center, Philadelphia PA comments:
Detected early, cure rates approach 90%. The majority
of OC is unfortunately detected too late. Since an acceptable screening
approach is not available, we must rely on symptom identification for early
diagnosis.
�There is no way to avoid the conclusion that early
diagnosis of ovarian cancer must rely on the elusive practice of clinical
judgment, a skill that involves careful analysis of the characteristics of
the� presenting symptom set within the
context of thoughtful dialogue.� �The importance of this study is not the
validation of a symptom cluster, . . . but rather the reinforcement of the need
for an ongoing process of communication between patients and their physicians.�
� Comment:
This requires
the patient to carefully recall and describe her symptoms. And requires the
physician to be especially alert about eliciting the time of� onset, severity, and� duration, of the symptoms. Clarity may be
achieved only after several visits.
Physicians
should ask specifically about bloating, abdominal size and urinary symptoms.
The authors
did not describe outcomes for the 44 patients with OC who underwent
surgery.� RTJ
About
1/3 of obese men regained erectile function while losing over 10% of their
weight
6-8��
EFFECT OF LIFESTYLE CHANGES ON ERECTILE DYSFUNCTION IN OBESE MEN
Erectile dysfunction (ED) is common, even in younger men. Several modifiable lifestyle
factors are associated with maintenance of erectile function. Men with a body
mass index over 28 have a 30% higher risk of ED. The prevalence of overweight
and obesity in men reporting ED may be as high as 79%, although vascular factors
associated with obesity may play an important role.
ED and endothelial dysfunction may have some shared
pathways through a defect in nitric oxide activity, production of which may be
inhibited through age-, disease-, and behavioral-related pathways.
This study of obese men with ED aimed to determine if a long-term reduction in BMI and an increase in physical activity positively affected erectile functions.
Conclusion: The lifestyle changes were associated with
improvement in erectile function.
STUDY
1. Randomized trial followed 110 obese
sedentary, otherwise healthy, men1� (Mean body mass index = 36; mean age 43) �� who had ED determined by the International Index of Erectile Function.2 �ED was defined by a score
of 21 or less (out of a possible 25) on the index.
2. None had diabetes, hypertension, impaired renal function, or hyperlipidemia.1
3. Randomized to:� 1) intervention group received detailed
advice about how to achieve a loss of 10% or more in body weight by reducing
caloric intake and increasing physical activity, or 2) a control group given
general information about healthy food choices and exercise.
4. Main outcome = erectile function score
and endothelial function assessed by response to L-arginine.3
5. Follow-up = 2 years.
RESULTS
1. In the treated group, over 2 years,
total energy and saturated fat intake decreased considerably. Intake of
mono-and poly-unsaturated fat, and omega-3 fats increased.
2.
Mean changes at 2 years:������������������������������ Treated� (n = 55)���������������������� Control
(n = 55)
Baseline����� 2
years������������������ Baseline����� 2 years
Weight (kg)���������������������������������������������������������� 103����������������� 88����������������������������������� 101����������������� 99
Body mass index������������������������������������������������� 37������������������� 31����������������������������������� 36.4 � ������������� 35.7
Physical activity (min/wk)��������������������������������� 48������������������� 195��������������������������������� 51������������������� 84
IIEF score������������������������������������������������������������� 14������������������� 17����������������������������������� 14������������������� 14
Men with IIEF score of 22 or higher�������������������������������� 17����������������������������������������������������������� 3����� �����������������
(Note that
about 1/3 of men regained function while losing over 10% of their weight,
despite remaining obese. RTJ)
3. There was also evidence in the treated
group of improved endothelial function by responses of platelet aggregation and
BP to L-arginine.
4. C-reactive protein levels decreased in the treated group.
DISCUSSION
1. Healthy lifestyles are associated with
maintenance of good erectile function.
2. Obese men with ED have evidence of
abnormal endothelial function.
3. This study provides evidence that
weight loss achieved by lifestyle changes can improve erectile function in
obese men with ED.
4. Nitric oxide appears to play an
important role in the pathogenesis of ED. Improved NO availability � associated with weight loss may be implicated
in improving erectile function.
5. The investigators state that the
intervention in the treatment group was intensive, and involved frequent
contact with the study team.
CONCLUSION
Lifestyle changes (diet, exercise, and weight loss) in obese men with ED were associated with improvements in erectile function.
JAMA June 23/30 2004; 291: 2978-84� Original investigation , first author
Katherine Esposito, Second University of Naples, Italy.� www.jama.com
1� Grossly obese
sedentary men of this age who are otherwise healthy must be rare indeed. I
would wager that most, if not all, had the metabolic syndrome
2� I had not
encountered this index before.� It
consists of 5 questions about sexual functioning, each divided into a score of
1 to 5 depending on the difficulty experienced. Possible scores range from 5 to
25, the lower number indicating a higher degree of dysfunction. (See
description p 2979) Can be accessed at:�
Google �international index erectile function�
3 �Erectile and
endothelial dysfunction may have some shared pathways through a defect in
nitric acid activity.� Endothelial
function was measured by response of BP and platelet aggregation to an
intravenous bolus of L-arginine, a natural precursor of nitric oxide.� See text and references.
An editorial in this issue of JAMA by Christopher S
Saigal, University of California, Los Angeles, comments and expands on the
study:
The introduction of Viagra in 1998 unleashed a tidal wave of interest in treatment of
ED. The heavy direct-to-consumer marketing campaign contributed to a new, open
discussion in popular culture about this very common condition. ED was suddenly
fair game for late night comics. Within 2 years, a billion dollar industry
developed. Physician office visits for ED increased.
For many patients, ED is a manifestation of more
generalized pathology. Hypertension, hyperglycemia, and dyslipidemia are common
co-morbidities. Endothelial dysfunction is likely a pathogenic mechanism common
to these co-morbid states, risk of cardiovascular disease, and ED. Weight loss
in these obese patients was associated with reduction in serum concentrations
of markers of inflammation such as C-reactive protein. This is further evidence
of improved endothelial function.
Regular physical exercise can have a modifying effect
on risk of developing ED. One study of men age
40 to 70 without ED reported the future risk of
developing ED was much lower in those who started a physical activity program vs those who remained sedentary.
The benefits of this intensive program are not limited
by any means to improvement in ED. Lowering risk of cardiovascular disease is,
for many, more important.
�� Comment:
I
congratulate the investigators, and especially the patients, on maintenance of
a very rigid treatment program. This is not, however, a practical application.
Few patients in primary care practice would be able to complete such a program
The main message is�maintain a healthy lifestyle,
don�t wait to repair damage until after it is done. RTJ
�Unwanted
pregnancy remains a major personal and public health issue�
6-9��
WAITING FOR PLAN B�THE FDA AND NONPRESCRIPTION ON EMERGENCY
CONTRACEPTION
The proposal to switch to levonorgestrel emergency
contraception (EC; Plan B) to
over-the-counter status is in limbo. In May, the FDA rejected the application
of Barr Pharmaceuticals for non-prescription sales. Dr. Steven Galson, the
acting director, wrote that the company had �not provided adequate data to
support a conclusion that Plan B can
be used safely by young adolescent women for emergency contraception without
the professional supervision of a practitioner licensed by law to administer
the drug�. In rejecting the application, the FDA also rejected the advice of
its medical review-staff. (A vote of 23 to 4 in favor of nonprescription
status.)
It is uncertain whether�or when�a revised application
might be approved.
Plan B, approved for prescription use in 1990, consists of
two 0.75 mg pills of the synthetic progestogen, levonorgestrel. (A component of
many birth control pills.)� It should be
taken as soon as possible and within 72 hours of unprotected intercourse.� Taken in the first 24 hours, the rate of
pregnancy is reduced to 0.4%, and to 2.7% when taken within 72 hours.
Rates of pregnancies and induced abortions have
decreased in the US, particularly among adolescents, primarily because
contraceptive use has improved and because girls have been starting to have
intercourse at older ages. Nonetheless, unwanted pregnancy remains a major
personal and public health issue. Commonly cited estimates are that half of all
pregnancies are unintended, that one of every two girls and women between 15
and 44 years has had at least one unintended pregnancy, and that in 2000, as
many as 51 000 abortions were averted by use of EC pills.
Nonprescription use of EC would, according to Dr
Galson. �dramatically increase access to oral contraception and will represent
an important step forward in availability of these products�. Dr Galson stated
that he himself �made the decision� not to approve on the basis of scientific
data. His signing the �Not Approvable� letter was a very unusual action.
There is extensive data about the safety and
effectiveness of Plan B. There have been only isolated findings of increased
rates of intercourse, unprotected intercourse, or intercourse without
appropriate contraceptive methods in association with its availability.
The FDA medical review committee voted unanimously
that �the data demonstrate that Plan B is safe for use in the non-prescription
setting� and that there is no evidence that over-the-counter �availability of
Plan B leads to substitution of emergency contraception for the regular use of
other methods of contraception�. Concerns about young teenagers were discussed,
but these were not the focus of the deliberation. Committee members were not
asked to vote on whether girls younger than 16 years could use nonprescription
Plan B safely. FDA staff members also recommended the approval of the
application.����� As part of the
�questions and answers� document, the agency asked itself, �Did the FDA bow to
political pressure in making this decision?�, and answered �No�.
The president of the American College of Obstetricians
and Gynecologists(ACOG) said the FDA�s action was �morally repugnant�.
Young teenagers account for only a tiny fraction of
the potential users of EC. Side effects and costs of nonprescription pills
would be powerful deterrents to repeated use. Dr. Elizabeth Raymond of Family
Health International, stated that �The FDA�s fixation on young adolescents is
simply unjustified�. Research �shows that they can use the pills correctly and
safely�.
Children may purchase acetaminophen, aspirin, and
NSAIDs without a prescription and without an age check. The FDA has never
required specific data on the safe and correct use of these or other
medications in children and adolescents, although their improper use is harmful
and potentially lethal.
The ACOG urges all obstetrician-gynecologists to
provide prescriptions for EC to all women of reproductive age at every office
visit.
NEJM June 3,2004; 350: 2327-29� �Perspective�, editorial by Robert
Steinbrook, MD, National Correspondent , NEJM
�� Comment:
I would be
willing to wager that this decision will be reversed.� RTJ
�As
effective and as safe as enoxaparin.�
6-10��
FONDAPARINUX OR ENOXAPARIN FOR THE INITIAL TREATMENT OF SYMPTOMATIC DEEP
VENOUS THROMBOSIS
Low-molecular-weight heparin (LMWH) is standard initial for treatment of deep venous thrombosis
(DVT). It consists of once- or twice-daily subcutaneous injections of a dose
adjusted only for bodyweight. Treating suitable patients at home, often with
self-injection, is effective and safe.
Fondaparinux is a selective inhibitor of activated
factor X (Xa). Once-daily injections produce a predictable anticoagulant
effect. It has an advantage of not cross reacting with heparin-induced
antibodies. Platelet monitoring may no longer be needed.
This study asks�is fondaparinux safe and effective
therapy for established DVT? How does it compare with LMWH?
Conclusion: Once-daily fondaparinux was as effective
and as safe as the LMWH enoxaparin.
STUDY
1. Randomized, double-blind multicenter
study entered over 2200 patients (mean age 61) with established acute symptomatic
DVT of the lower extremity.� All were
judged to require antithrombotic therapy. None had symptomatic pulmonary
embolism.
2. Randomized to:� 1) fondaparinux (Axistra) subcutaneously once-daily�5 to 7.5 to 10 mg according to
weight,� or 2) enoxaparin (Lovenox) 1 mg/kg body weight
twice-daily.
3. All were started on oral anticoagulant
therapy within 72 hours. (Choice according to hospital practice to maintain an
INR of 2.0 to 3.0.)
4.�
Double-blind subcutaneous injections were continued for at least 5 days,
or until the warfarin-induced INR reached 2.0 or greater. Oral therapy was
continued for 3 months.
5. Primary efficacy outcome was 3-month
incidence of recurrent symptomatic DVT.
RESULTS
1.
Outcomes at 3 months���������������������������������� Fondaparinux
�������� Enoxaparin
Recurrent thromboembolic events��������������������������� 3.9%������������������������������ 4.1%
Pulmonary embolism
Fatal���������������������������������������������������������������������� 5
patients���������������������� 5 patients
Nonfatal���������������������������������������������������������������� 20
patients�������������������� 12 patients
Recurrent DVT ����������������������������������������������������������� 18
patients�������������������� 26 patients
Major bleeding
During initial treatment�������������������������������������� 1.1%������������������������������ 1.2%
During entire study�������������������������������������������� 2.6%������������������������������ 2.4%
Death during entire study����������������������������������������� 3.8%������������������������������ 3.0%
DISCUSSION
1. The study demonstrated that
fondaparinux is as safe and as effective as enoxaparin (or, in commonly used
parlance, is �non-inferior� 1).
2. Prefilling syringes with 7.5 mg
fondaparinux (the most commonly used dose) makes treatment feasible for
outpatient therapy. About 1/3 of the patients received treatment partially or
entirely at home.
3. Home treatment with self-administered
LMWH is increasingly used, but is subject to dosing errors when bodyweight,
dosage, or dosing intervals are uncertain, and when patients have limited
capability to titrate prefilled syringes, or withdraw dosage from multidose
vials.
4. Fondaparinux does not have a specific
antidote.
5. Primary efficacy outcome = 3-month
incidence of recurrent DVT.
CONCLUSION
Once-daily subcutaneous fondaparinux was at least as
safe and effective (not inferior 1) as twice-daily enoxaparin in the
initial treatment of DVT.�
Annals Int Med�
June 1, 2004; 140: 867-73�
Original investigation, first author Harry R Buller, University of
Amsterdam, the Netherlands.
An editorial in this issue of the Annals (pp 925-26)
by Paolo Prandoni, University of Padua, Italy comments:
There are several cautions about at-home treatment
with either LMWH or fondaparinux:
1) Concern about undertreatment of DVT and
resultant pulmonary embolism, and 2) the need for careful laboratory monitoring
of oral anticoagulation status during the first days of treatment. This is
indispensable to guarantee the correct overlap between subcutaneous drugs and
warfarin.
Fondaparinux has a possible advantage over LMWH in
that it does not bind to platelet factor 4. This makes the development of
immune thrombocytopenia extremely unlikely (although it is rare during
treatment with LMWH).
Fondaparinux has been approved for prophylaxis of VTE
after major orthopedic surgery. Once daily fondaparinux 2.5 mg reduced VTE risk
by more than 50% in comparison with enoxaparin.
Other anticoagulant drugs are in the
offing�ximelagatran, a selective antithrombin, and idraparinux, which can be
administered in fixed doses once weekly.
� Comment:
1� The term �non-inferior� appears frequently
in conclusions of current studies comparing one drug with another. I wonder why
this (negative) terminology is used in favor of the positive �just as effective
and safe�.� Should fondaparinux be
considered a �me too� drug?� For a new
drug to be adopted into primary care practice to replace an old effective drug,
important attributes must be established. Comparing (a) Xa inhibitor to (b)
LMWH:
1.� (a) must be established as just as
effective, or more effective.
2.� (a) must be established as just as safe or
safer.
3. (a) must
be more convenient to administer and require fewer doses.
4. (a) must
be less costly.
�The study presents evidence that 1. and� 2. are likely. Confirmation and more
experience are required.
3. does seem likely.�
4. is to be determined.
Study
sponsored by Sanofi-Synthelabo and MV Organon.�
I hesitate to say it, but I always look for �spin� in drug-company
sponsored studies. This study looks straight forward. We look for confirmation.
RTJ
�Benefits
are below minimally relevant thresholds�
6-11��
LONG TERM DONEPEZIL (Aricept)
TREATMENT IN 565 PATIENTS WITH ALZHEIMER�S DISEASE (AD 2000)
Degeneration in cholinergic forebrain neurons
innervating the cortex is believed to contribute to cognitive defects seen in
Alzheimer�s disease (AD). This
concept triggered development of cholinesterase inhibitors (CIs) which raise acetylcholine levels by blocking the enzymes that
metabolize acetylcholine.
All three available CIs produce small improvements in
cognitive and global assessments in selected patients with mild-to-moderate AD
over 3-12 months. Little is known about long-term effectiveness, or their
usefulness in patients with severe AD.�
Nonetheless, the demand from clinicians and patients remains strong.
CIs (vs
placebo) produce on average a small advantage on simple cognitive tests (eg,
3-points on the 70 point Alzheimer�s Disease Assessment Scale [ADAS-cog] ). Is
this small benefit worthwhile?�
This study asked whether the cholinesterase inhibitor
donepezil (Aricept) is cost effective
and produces worthwhile clinical and social improvements����� .
Conclusion:�
Benefits of donepezil are below minimally relevant thresholds. It is not
cost effective.
STUDY
1. Randomized, double-blind trial entered
565 (and followed 486) community-resident patients (mean age 70-79).� The patients had been referred from � memory clinics. They were diagnosed as having
AD (with or without vascular dementia) by DSM IV criteria. About half were
judged to have mild AD; half to ����� moderate
AD by the Mini-mental-state examination.(MMSE)1�� The doctors
involved were substantially uncertain whether donepezil would produce
worthwhile benefits.2
2. Randomized to:� 1) Donepezil (5 or 10 mg daily), or 2)
Placebo.
3. Followed patients as long as judged
appropriate.
4. Primary endpoints = entry into
institutional care and progression of disability defined by an activity of
daily living scale.
RESULTS
1.
Effects on MMSE:
A. Donepezil group:
In absolute terms, donepezil group
achieved a slightly higher score within the first 36 weeks (about one point
above baseline on a 30-point scale). Thereafter, scores deteriorated back to
baseline at 48 weeks and to minus 4 points at 112 weeks.
B. Placebo group:
In absolute terms, the placebo group continuously lost
points during the 110 weeks.
C. Comparing A. with B.
Comparatively, over 112 weeks, donepezil group maintained a slightly better score (a fraction of one point) despite its continuing decline in absolute terms.
(See figure 6
p 2111)
[Advocates
can point to a slight improvement in MMSE over 36 weeks. The general course over
112 weeks was downward. RTJ ]
2.
Effects on an ADL scale:
A. Donepezil group:� at no
time improved. Scores on the scale gradually deteriorated over 112 weeks to
reach about 9 points lower than baseline.
B. Placebo group:� compared with the donepezil group, ADL
scores deteriorated over each time period at a slightly greater rate. (Scores
about 1 point lower at each time period.)
(See figure 4
p 2110)
[Although the
donepezil group continued to deteriorate by both measures, advocates can state
that the deterioration was slowed by a small margin.. Many clinicians� would consider the difference
inconsequential. RTJ]
2. No significant benefits were seen vs placebo in institutionalization,
progression of disability, behavioral and psychological symptoms, psychopathology
of carers, formal care costs, adverse events, or deaths.
3. No difference between the 5 mg and the
10 mg dose.
DISCUSSION
1. AD 2000 is one of the largest trials in
terms of numbers of patients randomized, and the largest in person-years of placebo-controlled
treatment.
2. Donepezil was associated with no improvement in activities-of-daily
living scale at any time up to 2
years. Compared with placebo, decline in ADL score was slightly slower. (Figure 4 p 2110)
3. Donepezil was associated with a slight
improvement in MMSE (about 1 point out of a possible score of 30) over 6
months. Thereafter, scores deteriorated. Scores in the donepezil group remained
slightly higher than placebo scores at each time period over 2 years. (Figure 6 p 2111)
4. Donepezil produced no measurable
reduction in rate of institutionalization or progress of disability. (These are
the key determinants of overall cost-effectiveness.)
5. No evidence that costs of caring for
patients with Alzheimer�s disease in the community were reduced by donepezil.
6. Any effect of donepezil on informal
caregiver time is likely to be small.
7. Do the (statically) significant but small improvements in cognition (vs placebo) seen over 2 years lead to a
worthwhile clinical �� improvement in heath-related
quality-of-life? The US FDA has suggested that a reversal of the natural
history of cognitive decline by 6 months constitutes a clinically important
difference. This change equates to an annual decline of 1.4 MMSE points in
treated patients vs a mean annual
decline of 2.8 points in untreated patients (difference = 1.4 points).
(Cognition declines both groups�only at a slightly slower rate in the donepezil
group.)� A large survey of clinicians
revealed that 45% judged a 3-point change as the minimum benchmark.
8. A subset of patients could derive
selective benefit from CIs. This assumption underlies government guidance. (And leads family members to hope their
loved-one may be an outlier, and achieve significant benefit. RTJ)� The study did not identify any variables
that might predict treatment response. Apparently good responses are more
likely to be chance fluctuations in the disease.
9. Donepezil is not cost-effective. It
does not delay institutionalization. �The disappointingly little overall
benefit from donepezil cannot be taken lightly.�� Clinicians can validly question whether other uses of scarce
resources allocated to dementia would provide better value than routine
prescription of cholinesterase inhibitors.
9. Future studies need to achieve high
compliance and complete follow-up to avoid bias from differential dropout
rates.
CONCLUSION
Benefits of the acetylcholinesterase inhibitor,
donepezil, are below minimally relevant thresholds. It is not cost effective
Lancet June 16, 2004; 363: 2105-15� Original investigation by the AD 2000
Collaborative Group, correspondence to AD 2000 group, University of Birmingham
UK.
� Comment:
1�
Mild�MMSE score = 18 to 26 points; moderate = 10-18 points (on a 30
point scale).
MMSE
available at��
www.mja.com.au/public/mentalhealth/articles/yellowlees/yelbox4.html
2 Otherwise,
the placebo-controlled trial would have been unethical
This is a
complicated and long report. I believe I have abstracted the main points.
The authors
make the remarkable statement that pharmaceutical companies opposed this trial.
The trial was supported (non-commercially) by�
the UK National Health Service
I believe
many patients are continuing to receive CIs far beyond the time of any hope of
benefit.
COST:� about $1600 per year quoted by
drugstore.com. As is often the case, the 10 mg dose costs just a few dollars
more per year than the 5 mg dose. A pill cutter may cut cost in half. There is
no statistically significant difference in effects of 10 mg vs 5 mg. Adverse
effects (eg, gastrointestinal) are greater with the 10 mg dose RTJ
Trials
use participants who do not represent typical patients.
6-12��
AD 2000: DONEPEZIL IN ALZHEIMER�S DISEASE
(This editorial comments and expands on the preceding
study.)
Many published randomized trials of cholinesterase
inhibitors (CIs) have shown efficacy1 for the treatment of AD.
Approval by regulatory agencies has been world-wide. Nonetheless, effectiveness1 remains controversial.
Many clinicians, while acknowledging measurable and consistent cognitive
effects, question the overall practical effectiveness1 of these drugs. Many others are staunch advocates of
their broad and long-term use.
Patients seen in everyday practice differ from those
selected for inclusion in drug-company-sponsored trials. Drug companies use
highly refined selection criteria; often include specialized tests to aid
diagnosis;� restrict allowable
comorbidity and concomitant medications; and the extent of behavioral or functional
impairment. They pay for all protocol-related care, including medications.
�Typical selection criteria for industry sponsored trials would exclude over
90% of out-patients with mild-to-moderate Alzheimer�s disease in California who
would otherwise be eligible to receive treatment. The controversy about
effectiveness, costs, and the clinical meaning of trial results has been fueled
by the use of participants who do not represent typical patients.�
In the trial, donepezil and placebo were both associated
with a worsening over time. The mean differences on the MMSE and activities of
daily living (ADL) scale represent a
delay in symptom-worsening of about 3 months. The rather broad confidence
intervals around primary endpoints are compatible with both a 30 to 45%
increase and up to a 30% decrease in risks with donepezil.2
AD 2000 undermines the assumption that improvement in
cognition and ADL scores generalize to maintenance of function, cost savings,
or delay in institutionalization. �Results are incompatible with many
drug-company-sponsored studies claiming remarkable effects for cholinesterase
inhibitors.�
Lancet June 26, 2004; 363: 2100-01� �Commentary� an essay by Lon S Schneider,
University of Southern California, Los Angeles.
Comment:
1�
The editorialist uses these two terms carefully. �Efficacy� relates to
conclusions of trials; �Effectiveness� relates to outcomes in the �real world�
of practice.
2�
Families hope that their loved one may be among the outliers who receive
greater benefit. I believe this hope leads to more willingness to begin and to
continue using the CIs.
This commentary presents a clinically important point.
It emphasizes the gulf which may separate results of randomized controlled
trials from benefits evident in primary care practice. There may be a large
difference between results reported by a clinical trial for AD and clinical
benefits for Mr. Jones, whose family brings him into your office because of
memory loss. A practical office-based, �real world� trial is more meaningful
and convincing. Beware of �spin�.
�Ring�
prophylaxis during the next inevitable pandemic of flu.
6-13��
TACKLING THE NEXT INFLUENZA PANDEMIC
�We must now hasten the preparations for another
inevitable influenza pandemic.� Currently. contingency plans are based largely
on rapid vaccination of susceptible populations. Other measures , such as
treatment with antiviral drugs, serve only as adjuncts. Technical constraints
on vaccine production and the time required to initiate mass vaccine production
during a pandemic will limit effectiveness of this measure.
A recent systemic review concluded that the
prophylactic use of neuraminidase inhibitors (NIs) could lead to a reduction of 70-90% in risk of symptomatic
flu. These drugs have shown efficacy in preventing transmission of influenza in
institutions and community setting. The availability of a highly effective
supplement to vaccination opens to debate the appropriate role of NIs and other
antiviral drugs in the control of pandemic influenza.
Challenges to this approach include the need for
long-term, large scale, continuous prophylaxis; inadequate compliance with
prolonged daily use; emergence of resistant viral strains; as well as
insufficient supplies and limited manufacturing ability. �Stockpiling of
antiviral drugs is therefore necessary, but the cost of stockpiling in such
magnitude looks prohibitively expensive.�
What might be an alternative strategy? It is known
that �ring� vaccination, which has been used in the past, will quell smallpox
outbreaks. The strategy entails post-exposure vaccination of close contacts..
For smallpox, this approach has provided a wide safety net of prevention, while
focusing vaccination where it was needed most. Ring prophylaxis may be
applicable to the initial management of an influenza pandemic. NI treatment of
influenza cases with the infection and prophylactic use for their contacts may
decrease attack rates substantially. It limits usage of the drug to where it is
needed most.
Influenza differs considerably for small pox. It has a
shorter incubation period, a higher attack rate, and a lack of specific
symptoms. These characteristics may impose difficulties in accurately
identifying and rapidly treating contacts. Still, this policy, in conjunction
with isolation and quarantine, can be expected to slow down dissemination of
the disease, providing valuable time for production and distribution of a
vaccine.
Antiviral ring prophylaxis for flu has proved to be
effective in family settings. It requires only short term daily treatment for a
period of 5-10 days, and targets a relatively limited proportion of the
population. Used in this way, NIs may be dispensed more rapidly and require
less of a stockpile.
Contacts receiving antiviral prophylaxis may form
protective antibodies due to subclinical infection, rendering them immune for
the duration of the pandemic.
Chemoprophylaxis will not suffice as a sole preventive
measure in case of a pandemic. It must be accompanied by quarantine, isolation,
and prevention of mass congregation as well as vaccination.
BMJ June 12, 2004; 328: 1391-92� Editorial, first author Ran D Balicer,� Israeli Working Group on Influenza Pandemic
Preparedness, Ramat-gan Israel.
� Comment:
COST:� Tamiflu, 75 mg cost about $6 each capsule�
$60 for a treatment course; $42 for prophylaxis. I believe most patients would
consider this a bargain.
Healthcare
workers should be the first in line to receive �ring� prophylaxis, and to continue
it until assured that the current vaccine is effective.
There are two
NIs:� 1) Oseltamivir (Tamiflu) for oral
use, and zanamivir (Relenza) for inhalation. Both are effective for treatment
and prophylaxis of flu.
For
treatment, Tamiflu should be started within 40 hours of onset of symptoms, and
continued for 5 days. The dose for adults is 75 mg twice daily. Children are
given a lower dose�30, 40, or 60 mg twice daily depending on weight (available
as a suspension).
For
prophylaxis, adults are given 75 mg once daily for at least 7 days. Duration of
protection lasts as long as the drug is given. It has been used up to 42 days
in nursing homes. Drug resistance due to mutations of the virus has been
reported.
Primary care
clinicians will likely use NIs freely to unvaccinated family members during an
epidemic of flu.� RTJ
6-14�
DANGERS OF ROSUVASTATIN (Crestor)
IDENTIFIED BEFORE AND AFTER FDA APPROVAL
A letter to the editor from Sidney M Wolfe, Public Citizen�s Health Research Group, Washington
DC. Lancet June 26, 2004; 363: 2189-90
comments:
The lipid-lowering drug rosuvastatin (Crestor; Astra-Zeneca) is currently in
the midst of the most heavily financed launch of a prescription drug ever.
The correspondent presents available pre�marketing and
post-marketing evidence of the adverse effects of the drug.
Pre-marketing:�
Documents included a acknowledgement of a risk of
severe myopathy and rhabdomyolyis which clearly increased at the highest dose
(80 mg). The preapproval document also stated that 80 mg is associated with a
high frequency of creatine kinase elevations (CK 10 times upper normal). Crestor was approved with the belief
that lower doses would be much safer. The 80 mg dose was subsequently
discontinued.�
Post-marketing:
Myopathy:�
Since marketing of rosuvastatin, there have been 18 additional cases of
rhabdomyolyis. Two patients were using 40 mg; five using 20 mg; 11 using 10 mg.
Renal toxicity:�
Rosuvastatin is associated with renal abnormalities.
A small percentage exposed primarily to 80 mg had increased frequency of persistent proteinuria and hematuria, and, in some patients, an increase in serum creatinine. There is a reported dose-associated risk.. The 10, 20, and 40 mg doses have been �� associated with increasing risk up to 1% of patients. In individuals who develop ++ proteinuria or more, the percentage with an increase of creatinine of over 30% rose incrementally with dose�from 14% in the 5 mg daily dose to 33% in the 40 mg dose.
There have been 8 reported cases of acute renal failure and 4 of renal insufficiency since marketing began. Nine were using 10 mg.
Other �currently approved statins do not have similar
renal effects�.
�By now, the number of reported cases of rhabdomyolyis
and renal insufficiency or renal failure�20 of which have occurred in people
using 10 mg�is certain to have increased substantially from the number filed by
April 13, 2004.�
Efficacy:
A statistical review of comparative efficacy found no
significant difference in LDL-cholesterol lowering between 5, 10, and 20 mg of
rosuvastatin and 20, 40 and 80 mg of atorvastatin. (This surrogate laboratory finding does not indicate comparative
clinical effectiveness.)
�The renal toxicity, high rate of cases of
rhabdomyolyis compared with other statins, and lack of unique benefits are
compelling reasons to remove rosuvastatin from the market before additional
patients are injured or killed.�� The
correspondent recalls that cerivastatin (Baychol)
was removed from the market because of increased risk of myopathy.
==========
A
letter to the editor July 10, 2004; 364: 135 from Gunnar O Olsson,
Astra-Zeneca, Molindal, Sweden offers a rebuttal:
Crestor has a safety profile comparable to those of other
marketed statins. (The US FDA has reviewed post-marketing safety data and has
supported this conclusion.)
Crestor was the most extensively studied statin ever
submitted for regulatory review. More than 60 countries have approved it on the
basis of an excellent benefit/risk profile. �More than 80% of patients can
reach their LDL cholesterol goal on the usual start dose of 10 mg.�
The reported rate of rhabdomyolyis has remained very
low (< 1 in 10 000) is consistent with the rates of all currently marketed
statins.
Proteinuria has been associated with Crestor, but is transient, and often
resolves on continued treatment. It is not predictive of acute or progressive
renal disease.
Astra-Zeneca is surprised that The Lancet published a
letter containing inappropriate comparisons that serve to cause undue alarm.
�The letter, which is a rehash of misinformation presented by Public Citizen in
the past includes reference to a non-marketed dose (80 mg) and is �highly
speculative�.
�Rosuvastatin has an excellent benefit-risk profile
compared with other marketed statins, having a better efficacy lowering LDL
cholesterol and raising HDL cholesterol and a safety profile comparable to
those of other marketed statins.�
� Comment:
These letters
raise an important clinical point. When should primary care clinicians add a
new drug to their practice?
Is Crestor a
unique and important addition to therapeutics?�
Or is it just a �me-too� drug? Should primary care clinicians prescribe
it at the present time?
1. Is Crestor more effective in lowering LDL?�� No. Other statins lower LDL just as much, although they might require a higher dose. Remember, this is a laboratory endpoint, not a clinical endpoint.� Clinical efficacy has not been established.
2.
Is Crestor as safe as other statins?�
This is the dispute. That the 80 mg dose has been withdrawn because of
toxicity raises caution. It will take several years of general use in the USA
for the FDA to determine toxicity. Certainly, Crestor is not safer.
3. Is Crestor
more convenient to administer. Does it require fewer doses? No
4. Is Crestor
less costly?� No. Costs are comparable.
The first
letter may raise an entirely unwarranted red flag. I do not know.� I abstracted these letters mainly to
reinforce the long-honored and oft-repeated admonishment to primary care
clinicians not to be the first to prescribe a new drug, no matter how highly
touted, unless it is known to be safe and carry unique and important benefits.
Regardless of the question of toxicity, I do not believe the benefits of
Crestor are unique or comparatively important.
I would not
prescribe Crestor at this time. If it proves equally or less toxic, maintains
its reported comparative efficacy in reducing LDL-c, and has a significant cost
benefit, I would consider prescribing it.
I have faced
(as have most older clinicians) the embarrassment of having a drug I had
prescribed suddenly withdrawn from the market. The patient will ask for an
explanation. RTJ