PRACTICAL POINTERS
ISOLATED SYSTOLIC HYPERTENSION—IMPORTANCE OF CONTROL
OVERCOME CLINICAL INERTIA TO CONTROL SYSTOLIC BP
DOXAZOCIN, FINASTERIDE, AND COMBINATION TO DELAY PROGRESSION
OF BPH
CLINICAL IMPACT OF BLEEDING IN PATIENTS TAKING ORAL
ANTICOAGULANT THERAPY
INTRA-ARTICULAR HYALURONIC ACID FOR KNEE ARTHRITIS—MAINLY
PLACEBO EFFECT?
SCREENING FOR DEPRESSION IN PRIMARY CARE WITH TWO VERBALLY
ASKED QUESTIONS
REVIEW OF SENSITIVITY, SPECIFICITY, PREDICTIVE VALUES AND
LIKELIHOOD RATIOS
ECHINACEA OF NO VALUE IN TREATING UPPER RESPIRATORY TRACT
INFECTIONS IN CHILDREN
SCREENING VIRTUAL COLONOSCOPY—NOT READY FOR PRIME TIME
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
[email protected] DAVIDSON
N2 28036 USA
www.practicalpointers.org
HIGHLIGHTS
AND EDITORIAL COMMENTS
Best evidence indicates that antibiotics
are of minimal or no benefit for sore throat, acute bronchitis, the common
cold, and otitis media. Antibiotics continue to be commonly used for these
conditions. This is potentially
inappropriate prescribing.
This has prompted the use of delayed (or
“as needed”, or “if”) prescriptions. These prescriptions
are
written with the proviso that they are not to be used immediately—only later if
symptoms do not improve in a few days. Use of a delayed prescription should be
restricted to patients who request antibiotics or for whom the doctor thinks
one is not immediately indicated.
A randomized trial in 1997 gave
prescriptions for antibiotics for respiratory infections: 1) to be filled
immediately, or 2) to be filled after 3 days, or 3) no antibiotic prescription.
The immediate group filled 99%.
The delayed group filled 31%.
In the no-prescription group,
13% filled an antibiotic prescription after a return visit to
the physician.
The reduction in use of antibiotics for
upper respiratory infections through using delayed prescriptions is as
effective, and in many cases, more effective than educational projects.
A great many
older adults remain at high risk of heart disease and stroke from untreated
isolated systolic hypertension (ISH; systolic
> 140, diastolic < 90).
Treatment of ISH is associated with clear benefits. The Systolic Hypertension in the Elderly Program ( JAMA 1991) demonstrated a 36% reduction in stroke among participants
assigned to active BP treatment. The Systolic Hypertension in Europe trial (Lancet 1998) reported that active
treatment of ISH significantly reduced the incidence of dementia. And also exerted a strong effect in
preventing heart failure.
This subset of the SHEP study was begun
after closure of the original study. It compared risk of death and
cardiovascular event rates in actively treated patients with ISH, vs placebo
controls, and normotensive controls. Follow up was up to 14 years. Event rates
were decreased by 21% in the actively treated group.
Early treatment, before advanced
atherosclerosis develops, results in the best long-term outcomes. The
prevalence of subclinical atherosclerosis in individuals with ISH is high
compared with normotensive controls. Active treatment of ISH is associated with
slower progression of subclinical atherosclerosis. The development of
atherosclerosis with ISH likely adds to the acceleration of vascular
stiffening, which is the underlying cause of ISH. Thus, early treatment may
slow not only the progression of atherosclerosis, but progression of ISH as
well.
Severe ISH may be difficult to control,
requiring multiple drugs.
It is clear that in individuals younger
than age 50, diastolic BP (DBP) is a
better predictor of future complications of hypertension than in older
individuals. For those older than 50,
systolic BP (SBP) is a better
predictor. Most persons with hypertension are older than 50. For these patients
control of SBP is a high priority, even in the face of a normal DBP.
“Systolic blood pressure alone correctly
classifies hypertensive status in about 98% of adults.”
Most patients with elevated SBP need
aggressive treatment to reach the evidence-based goal of less than 140. We are
beginning to see that 130 and even 120 is some groups such as those with
diabetes, congestive heart failure, and chronic kidney disease is a beneficial
goal. SBP in these mostly older patients is the variable that indicates the
need for more intensive therapy.
This study assessed the long-term
effects of diazoxide (an alpha blocker) alone, finasteride (a reductase
inhibitor) alone, and the combination on clinical progression of BPH. It concluded that long-term therapy with
combined drugs reduced the risk of clinical progression significantly more than
either drug alone.
The number needed to treat by combined
therapy over 5 years was 8, vs 14 to 15
for the drugs used alone.
Risk of acute retention and need for
invasive therapy were reduced by finasteride but not by doxazocin.
The risk of overall clinical progression
increased with increasing baseline PSA levels and prostate volume in the doxazocin
group, but not in the finasteride or
combination group. No alpha blocker
stops the progression of prostate size. Finasteride
reduces circulating dihydro-testosterone levels by about 80%; PSA levels by
50%; and prostate size by 20%. Reductase inhibitors do not act rapidly, and
often require 6 months to reduce prostate size.
Current initial therapy in most cases consists of an
alpha blocker given alone. It acts rapidly to relieve symptoms. In the current
study, clinical progression occurred in only 17% of men in the placebo group.
In men with a low PSA and modest prostate size, progression of BPH may be slow
and use of a reductase inhibitor may be delayed. The study does support dual
use in men whose symptoms progress during monotherapy, or in men at high risk
of progression. (PSA over 4 mg/mL or prostate volume more 40 mL on ultrasound).
In patients with venous thromboembolism (VTE), there is a perception that the clinical impact of
preventing recurrent VTE and possible fatal pulmonary embolism outweighs the
risk of bleeding associated with long-term anticoagulation..
The subgroup of patients with idiopathic
(unprovoked) VTE, and VTE associated with factor V Leiden, prothrombin
mutations, and deficiencies of protein C and protein S make up about half of
the thousands of patients in whom symptomatic VTE is diagnosed each year in the
USA.
The optimal duration of anticoagulation
is still unclear.
This systematic review of randomized,
controlled trials and prospective cohort studies
(10
757 patients; 4373 patient-years) investigated patients with confirmed
idiopathic VTE. All received oral anticoagulant therapy (target INR--2.0 to
3.0) for at least 3 months. Nine of 33 studies reported use for over 3 months
(6 to 24 months).
The chances of a major bleed per year of anticoagulation were 7 in
100 patients with 1 in 1000 chance of fatality, and about 1 chance in 100 of an
intracranial bleed.
The primary care clinician must make
some attempt to balance the risk of bleeding vs the benefits of
12-6
INTRA-ARTICULAR HYALURONIC ACID IN TREATMENT OF KNEE ARTHRITIS
“Based on the findings of this
meta-analysis, intra-articular hyaluronic acid has, at best, modest
efficacy
in the treatment of knee osteoarthritis. This effect . . . “is equivalent to
the effect of NSAIDs over that of acetaminophen, an effect that itself remains
controversial.” .” “Our findings
suggest the controversy surrounding the efficacy of intra-articular hyaluronic
acid is justified and the best evidence does not support its efficacy.”
At least 17 of the 22 trials were
industry sponsored. Others have suggested that findings from
industry-sponsored
trials compared with those that were otherwise funded showed that research
funded by pharmaceutical companies was more likely to have outcomes favoring
the sponsor.
All 22 studies reported improvement of
pain in the intra-articular placebo groups. Placebo injections may have
efficacy for treating knee OA. The investigators calculated that
intra-articular placebo accounted for 79% of the efficacy of intra-articular
hyaluronic acid.
“This supports our hypothesis that the majority of the effect of
intra-articular hyaluronic acid is an
intra-articular
placebo effect.”
Publication
bias may overestimate the effect. Compared with lower-molecular-weight
hyaluronic acid, the higher-molecular weight hyaluronic acid may be more
efficacious, but heterogeneity of studies limits definitive conclusions.
I doubt this study will deter
enthusiasts from using HA. Individual patients who have apparently obtained
relief may insist on continuing.
The only way an individual’s response
can be accurately determined is by an N-of-one trial.
I
doubt this would be feasible considering the ethical issues involved.
The US Preventive Services Task Force endorsed
screening for depression, but did not recommend a specific tool. Many primary
care clinicians find screening questionnaires for depression too cumbersome and
time consuming for routine use.
This study used a simple screening tool of two
questions. If one or two were answered positively, the screen was considered
positive, and further questions were asked to determine if major depression was
present. (A composite interview--the “Gold Standard”)
The screening questions:
1) During the past month have you often been bothered by feeling
down, depressed, or hopeless?
2) During the past month have
you often been bothered by little interest or pleasure in doing things?
In the community setting, the two
verbally asked questions have a good sensitivity (97%)
and
reasonable specificity (67%) for screening for depression. If the screen was
negative (both questions answered negatively) major depression is almost surely
absent.
About 5 false positives would occur for
every true positive when asking the questions alone.
This
is common in screening studies which are in essence a diagnostic test performed
in a low prevalence setting. Further questions will be required to clarify
presence or absence of depression.
Calculate sensitivity from the left column;
specificity from the right column; positive predictive value from the top
row; negative prediction value from the
bottom row; the likelihood ratios from both columns.
See text.
Echinacea is a herbal remedy widely used
for prevention and treatment of upper respiratory infections (URIs). It is one of the most commonly
used herbal remedies in the USA . Three species of echinacea are used.
Beneficial effects are thought to be due to its “immunomodulating” activity,
most notably macrophage activation and enhanced neutrophil phagocytosis.
This study postulated that treatment with E purpurea would result in at least a
1.5- to 2-day reduction in duration of URIs in children, and that symptoms
would be less severe than in patients receiving placebo.
The preparation used in this study was not effective in treating URIs in
children. After the trial was completed, parents could not guess correctly whether their child had taken echinacea or
placebo. “Our results do not support
the use of echinacea for treatment of URIs in children.” Its use was associated with an increased
risk of rash.
This study was supported by a grant from
the National Center for Complementary and Alternative Medicine, Bastyr
University (an alternative medicine institution) and National College of
Naturopathic Medicine, Portland Oregon.
It
continues to amaze me that so many persons take unstandardized and unproven
nostrums and give them to their children. I am sure devotees will fault this
study. They will remain convinced that echinacea is beneficial.
12-10
SCREENING VIRTUAL COLONOSCOPY—READY FOR PRIME TIME?
A new virtual colonoscopy (VC) used a
multidirectional CT scanner providing a primary 3-dimentional endoluminal
display. It permitted faster,
higher-resolution imaging than previously obtainable. Residual fluid and stool
was tagged by contrast material. The imaging software digitally removed all
opacified fluid and stool from the colon by a process called “electronic
cleansing”.
The study subjects received the VC
followed by conventional colonoscopy for comparison:
Sensitivity of VC for detection of
adenomas vs traditional colonoscopy:
10 mm or larger was 92% vs 88%
8 mm or larger was 92% vs 89%
6 mm or larger was 86% vs 90%
The study suggests that VC can detect
polyps of 6 mm or larger as accurately as conventional colonoscopy in a
population with a low prevalence of colorectal neoplasia.
Decisions regarding the use of VC as a
first-line screening test will require more information about cost and
insurance coverage. “The performance of VC in this asymptomatic population is
impressive, with detection rates similar to those achieved by conventional
colonoscopy.” Only if the important questions about the appropriate size
threshold and the surveillance of smaller polyps can be resolved will VC be
ready for prime time.
The bugaboo is the need for follow-up conventional colonoscopy to
remove suspicious polyps.
Patients will be asking about this. Application in the local community
is likely to be far-off.
============
============
Best evidence indicates that antibiotics are of
minimal or no benefit for sore throat, acute bronchitis, the common cold, and
otitis media. Antibiotics continue to be commonly used for these
conditions. This is potentially
inappropriate prescribing.
This has prompted the use of delayed (or
“as needed”, or “if”) prescriptions. These prescriptions
are
written with the proviso that they are not to be used immediately—only later if
symptoms do not improve in a few days.
A randomized trial in 1997 gave prescriptions
for antibiotics for respiratory infections: 1) to be filled immediately, or 2)
to be filled after 3 days, or 3) no antibiotic prescription.
The immediate group filled 99%.
The delayed group filled 31%.
In the no-prescription group, 13%
filled an antibiotic prescription after a return visit to the physician.
Five controlled trials of delayed
prescriptions have been published:
otitis media, sore throat, cough lasting over a week, and the common
cold. In three trials the patients in the delayed prescription arm had more
symptoms during the trial, implying that patients are willing to tolerate some
symptoms to avoid antibiotics.
An additional benefit of delayed
prescriptions may be a reduction in repeat visits, at least for sore throat.
The reduction in use of antibiotics for
upper respiratory infections through using delayed prescriptions is as
effective, and in many cases, more effective than educational projects.
The positive aspects of delayed
prescriptions include avoiding side effects, reducing the drug bill, educating
patients, and involving patients in decision–making. Although reducing
antibiotic resistance is a major concern for physicians, it is not a concern
for patients.
Use of a delayed prescription should be
restricted to patients who request antibiotics or for whom the doctor thinks
one is not immediately indicated.
Comment:
I
have had some experience with delayed prescribing. I believe it is a useful
method to reduce unnecessary antibiotic use. As the article mentioned, patients
are not so concerned about resistance developing in the population. They will
respond to doctor’s advice about adverse effects to themselves as well as costs
of the drug. RTJ
=====================================================
12-2
EXTENT OF CARDIOVASCLUAR RISK REDUCTION ASSOCIATED WITH TREATMENT OF
ISOLATED SYSTOLIC HYPERTENSION
A great many older adults remain at high risk of heart disease and stroke
from untreated isolated systolic hypertension (ISH). Treatment of ISH is associated with clear benefits.
The Systolic Hypertension in the Elderly
Program (SHEP; JAMA 1991) demonstrated a 36% reduction in stroke among
participants assigned to active BP treatment.
Treatment of ISH also reduces risk of dementia and heart failure.
This study of a subset of the SHEP
patients was begun after closure of the original study. It compared risk of death
and cardiovascular event rates in actively treated patients with ISH, vs
placebo controls, and normotensive controls. Follow up was up to 14 years.
Cardiovascular events were reduced by 21% treated patients as compared with
controls.
If treatment is begun before development
of advanced atherosclerosis, the associated risks of
ISH
are reduced to a level close to the baseline risk experienced by a control
group without ISH.
1. Long-term prospective study followed a
cohort (subset) of the original SHEP study. It included
2. At entry, systolic BP (SBP) was between
160 and 219 mm Hg in the SHEP patients; mean = 171.
3. Treated patients received
chlorthalidone 12.5 and then 25 mg. If BP goal not reached, they
4.
After the initial SHEP trial ended, the patients were followed:
A. Those who had received active treatment
were given a 4-month supply of medication
B. The placebo controls (all with systolic
> 160) were asked to visit their physician
C. Control group (no ISH) was followed
annually for development of ISH.
5. All
groups were followed for up to 15 years for development of cardiovascular
events.
1.
Numbers taking antihypertension drugs After
one year After 5 years
Group A (N = 135; SHEP active) 81% 72%
Group B ( N = 133; SHEP placebo) 55% 65%
2.
Of the controls (N = 187) who had normal BP at end of the initial trial, 31%
developed
3.
In group A, a lower event rate (compared with placebo group B) was observed
beginning at year one.
4.
Event rates at 14 years:
Group A 58%
Group B 79% (21%
reduction: NNT = 5)
At 11 years,
Group A 47%
Group B 65%
Group C 35%
5. Among those with no clinical or subclinical
cardiovascular disease at baseline, the ISH group assigned to active treatment (Group
A) had a 10-year event rate similar to those in the control group. (Group C).
1. Long-term treatment of ISH is effective
in reducing cardiovascular events including cardiovascular death.
2. If treatment is begun before
development of advanced atherosclerosis, the associated risks of ISH are
reduced to a level close to the baseline risk experienced by a control group
without ISH.
3. The prevalence of subclinical
atherosclerosis in individuals with ISH is high compared with normotensive controls.
Active treatment of ISH is associated with slower progression of subclinical
atherosclerosis. The development of atherosclerosis with ISH likely adds to the
acceleration of vascular stiffening, which is the underlying cause of ISH.
Thus, early treatment may slow not only the progression of atherosclerosis, but
progression of ISH as well. Severe ISH may be difficult to control, requiring
multiple drugs.
4. There is a common perception that ISH,
particularly in older individuals, does not require
5. ISH is the most frequent subtype of
uncontrolled hypertension. Of the untreated hypertensive
6. Uncontrolled hypertension occurs most
often among adults, most of whom have good access to
7. The Systolic Hypertension in Europe
trial (Lancet 1998; 352: 1347-51)
reported that active treatment of ISH significantly reduced the incidence of
dementia. Active also exerts a strong
protective effect in preventing heart failure.
Long-term treatment of ISH in older adults
is associated with a dramatic reduction of death and cardiovascular events.
Early treatment, before advanced atherosclerosis develops, results in the best
long-term outcomes.
Comment:
Control
of ISH is one of the greatest challenges and opportunities in primary care
medicine. As the article stresses, early treatment is most rewarding.
I believe, low-dose, gradual and careful
titration with generic diuretic + generic beta-blocker + generic angiotensin II
blocker is effective, relatively inexpensive, and well tolerated treatment for
ISH RTJ
“Physicians
Need To Do A Better Job Of Conveying To Patients The Seriousness Of Elevated
BP.”
12-3
OVERCOME CLINICAL INERTIA TO CONTROL SYSTOLIC BP
(This editorial comments and expands on the preceding
study,)
It is clear that in individuals younger
than age 50, diastolic BP (DBP) is a
better predictor of future complications of hypertension than in older
individuals. For those older than 50,
systolic BP (SBP) is a better
predictor. Most persons with hypertension are older than 50. For these patients
control of SBP is a high priority, even in the face of a normal DBP.
“Systolic blood pressure alone correctly
classifies hypertensive status in about 98% of adults.”
The preceding study found that long-term
(14 years) control of SBP in older individuals resulted in a 21% reduction in
cardiovascular events. Thus, only 5 patients need to have SBP controlled to prevent one major complication. Moreover,
early initiation of SBP control increases the benefit.
Concern remains that pursuit of SBP goals
may lead to excessively low DBP. The long-standing debate about potential
disadvantages of DBP less than 55 mm Hg continues. Prudence suggests DBP be
maintained at approximately 55 as a
minimum in most patients. However, the problem of excessively low DBP is
dwarfed by the much more common problem of uncontrolled SBP.
Most patients with elevated SBP need
aggressive treatment to reach the evidence-based goal of less than 140. We are
beginning to see that 130 and even 120 in some groups such as those with
diabetes, congestive heart failure, and chronic kidney disease is a beneficial
goal. SBP in these mostly older patients is the variable that indicates the
need for more intensive therapy.
Diuretics and
angiotensin-enzyme-inhibitors (ACE-I) are excellent choices for initial
therapy. Most patients will eventually require more than one drug to reach
desired levels of SBP. The potential of weight loss, physical activity, and
sodium restriction to improve BP should not substantially delay initiation and
titration of drug therapy.
“Physicians need to do a better job of
conveying to patients the seriousness of elevated BP.” Primary care physicians are experts at
individualizing care, and our knowledge of the particulars of a patient’s case
must also enter into the selection of optimal therapy.
“If the SBP is 140 mm Hg or greater, we
ought to do something. Maybe we need not wait for the next visit. Maybe we
should do something now.”
The bugaboo of white coat hypertension
always enters the consideration to start treatment. Multiple BP readings should
be taken to ensure that the SBP is indeed elevated. Home BP readings and
ambulatory BP readings are preferable. But, in all likelihood, if a clinic SBP
is elevated in an elderly person, it will be a true elevation. RTJ
In
Select Patients The Combination Is Better Than Either Alone
12-4
THE LONG-TERM EFFECT OF DOXAZOCIN, FINASTERIDE, AND
COMBINATION THERAPY ON THE CLINICAL
PROGRESSION OF BENIGN PROSTATIC HYPERPLASIA
Benign prostatic hyperplasia (BPH) is commonly treated with alpha-blockers (eg, doxazocin; Cardura;
Generic) or reductase inhibitors (eg, finasteride; Proscar).
Alpha-adrenergic-receptor
blockers reduce smooth-muscle tone in the prostate and bladder neck. In the
short-to-moderate term they effectively relieve symptoms and improve urinary
flow.
An enzyme (reductase) converts
testosterone (inactive) to the active male hormone dihydro-testosterone.
Finasteride, a reductase inhibitor, prevents conversion of testosterone to
dihydro-testosterone, thereby inducing epithelial atrophy and reducing prostate
volume. Finasteride reduces rate of progression and lessens risk of urinary
retention and need for surgery in men with symptomatic BPH.
This study assessed the long-term effects
of diazoxide alone, finasteride alone, and the combination on clinical
progression of BPH.
Conclusion: Long-term therapy with combined drugs reduced the risk of
clinical progression significantly more than either drug alone.
1. Double blind, placebo-controlled trial
involved over 3000 men over age 50 with symptomatic BPH. All had American Urological Association (AUA)
symptom scores of 8 to 35. (Scores can range from 0 to 35.)
2. Randomized to: 1) doxazocin alone, 2) finasteride alone, 3) both together, or
4) placebo.
3. Primary outcome = risk of clinical
progression defined as: an increase of
4 points over baseline in the AUA symptom score, acute urinary retention, renal
insufficiency, recurrent urinary tract infection, or urinary incontinence.
4.
Mean follow-up = 4.5 years.
1. Compared with placebo, the rate of
clinical progression, was significantly reduced
by doxazocin
Event Placebo
( N=737) Doxazocin (N=756) Finasteride (N=768) Both (N=786)
Overall
progression 4.5 2.7 2.9 1.5
>
4 point AUA increase 3.6 1.9 2.5 1.3
Retention 0.6 0.4 0.2 0.1
Incontinence 0.3 0.3 0.3 0.1
Invasive
therapy 1.3 1.3 0.5 0.4
3.
The number needed to treat by combined therapy over 5 years was 8, vs14 to 15
for the drugs
4. Doxazocin alone did not reduce risk of
acute retention and need for invasive therapy. Finasteride
5. The risk of overall clinical
progression increased with increasing baseline PSA levels and prostate
6. Adverse
events:
Doxazocin—dizziness, postural hypotension,
and asthenia.
Finasteride—erectile dysfunction,
decreased libido, abnormal ejaculation.
Up to 27% discontinued mainly because of
adverse effects.
1. Treatment with finasteride alone, or
doxazocin alone, ameliorated symptoms and improved urinary
2. Combination therapy was more effective
than either drug alone in decreasing risk of clinical progression.
3. Continued growth of the prostate in the
doxazocin alone group eventually overcame the reduction in
4. Progression in men with a low PSA tended
to be low even in the placebo group. Benefit of
Long-term combined finasteride plus doxazocin
was safe and reduced risk of overall clinical progression of BPH significantly
more than either drug alone. Risk of urinary retention and need for surgery
were also reduced.
An
editorial in this issue of NEJM by E Darracott Vaughn Jr comments and expands on the study:
A
number of alpha blockers are available for prescription. At present,
tamsulosin (Flomax; a specific alpha blocker) is favored over doxazocin. The
daily dose (5 mg) does not have to be titrated. The incidence of side effects
is lower than for non-specific alpha blockers. However, no alpha blocker stops
the progression of prostate size. Finasteride
reduces circulating dihydro-testosterone levels by about 80%; PSA levels by
50%; and prostate size by 20%. Reductase inhibitors do not act rapidly, and
often require 6 months to reduce prostate size.
Current initial therapy in most cases
consists of an alpha blocker given alone. It acts rapidly to relieve symptoms.
In men with a low PSA, progression of BPH may be slow and use of a reductase
inhibitor may be delayed. In the
current study, clinical progression occurred in only 17% of men in the placebo
group. The study does support dual use in men whose symptoms progress during
monotherapy, or men at high risk of progression. (ie, PSA over 4 mg/mL or
prostate volume more 40 mL on ultrasound).
The Prostate Cancer Prevention Trial
(See Practical Pointers July 2003)
reported that finasteride reduced prevalence of prostate cancer by 25%, but
increased the likelihood of development of high grade cancers (Gleason grade 7
to 10). Caution is warranted for long-term use until this point is clarified.
Men should be advised of this possible complication.
Note that about ¼ of men withdrew from the
study. I believe Flomax would be better tolerated and reduce numbers of withdrawals.
Cost of long-term medication is critical in determining compliance. Flomax
+ Proscar would cost over $7500.00
for 5 years. RTJ
Risk
Is Considerable And Dangerous
12-5
CLINICAL IMPACT OF BLEEDING IN PATIENTS TAKING ORAL ANTICOAGULANT
THERAPY FOR VENOUS THROMBOEMBOLISM
In patients with venous thromboembolism (VTE), there is a perception that the clinical impact of
preventing recurrent VTE and possible fatal pulmonary embolism outweighs the
risk of bleeding associated with long-term anticoagulation.
The subgroup of patient with idiopathic
(unprovoked) VTE, and VTE associated with factor V Leiden, prothrombin
mutations, and deficiencies of protein C and protein S make up about half of
the thousands of patients in whom symptomatic VTE is diagnosed each year in the
USA.
The optimal duration of anticoagulation is
still unclear.
The objective of this meta-analysis was to
obtain reliable estimates of the clinical impact of anticoagulant-related
bleeding in patients with unprovoked VTE.
Conclusion: The clinical impact of major bleeding in patients given
anticoagulant therapy in patients with unprovoked VTE is considerable.
1. Conducted a systematic review of
randomized, controlled trials and prospective cohort studies
2. All studies reported major bleeding and
death as primary outcomes. Defined a major bleeding episode as one which
involved a major organ or body cavity, or required transfusion, or hospitalization,
or was fatal.
1.
10 757 patients received anticoagulation; 8335 for 3 months only; 2433 over 3 months for up to 24 months.
2.
Overall incidence of major bleeding and death (N = 10 757):
Major bleeding episodes 2.6% (276 patients)
Died from the bleeding 13% of the 276 (36 patients)
(The risk of major bleeding overall was 2
to 3 per 100 patients treated for up to 24 months.
Risk of death from bleeding was
about 3 to 4 per 1000 patients treated.
3. Incidence of intracranial bleeding = about 2 per
1000 (24 patients) Died of intracranial
bleeding 11 of 24 (about 1 in 1000 patients treated) Intracranial bleeding was associated with greater risk of death.
Almost half died of the bleeding.
4. Nine studies involved 2422 patients (606
patient-years) who received anticoagulation for
First
3 months (N = 2422) 3 to 24 months (N = 2422)
Major bleeding 54 patients 44 patients
Rate per 100 treated 2.2% 1.8%
5.
Calculated on a patient-year basis:
(Per 100 patient-years):
Major bleeding 7
Fatal bleeding 0.3
Intracranial bleeding 1.2
(The
chances of a major bleed per year of
anticoagulation for at least 2 years were 7 in 100 patients with 1 in 1000
chance of fatality, and about 1 chance in 100 of an intracranial bleed.)
1. Calculated on a patient-year basis, over a 2-year period, major bleeding occurred in 7 of 100 patients;
2. About 1 in 7 major bleeding episodes
was fatal or intracranial.
3. There appears to be a front-loading of
major bleeding episode shortly after initiation of therapy.
As
many major bleeding episodes occurred during the initial 3 months of
anticoagulation as during the entire year thereafter. (I believe, as time of anticoagulation is extended and patients age, the incidence of major
bleeding will increase, and far exceed the incidence in the first 3 months. RTJ
)
Other studies have noted that patients are more likely
to bleed soon after start of therapy. Many major bleeds occur in the initial 3
weeks of treatment, consistent with an underlying predisposition to bleeding. (I believe also in part due to
the initial difficulty of regulating INR.)
The clinical impact of
anticoagulant-related major bleeding in patients treated for VTE is
considerable. Calculated on a patient-year basis, over a 2-year period, major
bleeding occurred in 7 of 100 patients; fatal bleeding in 3 of 1000; and
intracranial bleeding in 1 to 2 per 100
Comment:
The investigators comment that their
estimates of bleeding in this study are consistent with the bleeding rates of
patients in the “real world”. I disagree.
I believe the risk of major bleeding occurring in primary care will be
higher than the risk in these well-conducted trials in which control of INR was
likely be more stringent. Most randomized, controlled trials appearing in the
journals tend to report relatively low rates of major bleeding in part because
of more careful and expert monitoring, and usually a shorter period of
observation. Control is inevitably less strict in primary care. And duration of
therapy may be much longer.
The difficulty of maintaining an INR of
2.0 to 3.0 is well known. Risk continues and adds up the longer the
anticoagulation is continued. A host of variables may interfere with control.
Indeed, I believe some degree of bleeding is inevitable in patients receiving
long-term anticoagulation.
Note that this study did not consider patients with atrial
fibrillation who were receiving anticoagulation. These individuals require
long-term therapy. Their risk of major bleeding increases continuously with
time and as the patients age. The risk of bleeding from anticoagulation must be
balanced against the increased severity and fatality of stroke from emboli
arising in the heart in patients with AF.
Not all patients with a history of VTE
need long-term anticoagulation. Some who are judged at lower risk for
recurrence may be treated with aspirin or with warfarin aimed an INR of 1.5 TO
2.0. The advent of the direct thrombin
inhibitor, ximelagatran may lead to a lower risk of bleeding. RTJ
At Best, A Small Benefit. The Placebo
Effect Predominated
12-6
INTRA-ARTICULAR HYALURONIC ACID IN TREATMENT OF KNEE ARTHRITIS
Hyaluronic acid (HA) is a large molecule composed of repeating disaccharides of
glucuronic acid and acetylglucosamine. It is naturally present in synovial
fluid. The FDA has approved it for treatment of osteoarthritis (OA). Despite FDA approval, the
efficacy of HA remains controversial. There is insufficient evidence to allow a
statement more definitive than that it is “probably effective in knee OA”. The
American College of Rheumatology has recommended intra-articular HA as an
alternative for use in patients at increased risk of gastrointestinal tract
adverse events from oral agents.
There has been an absence of data
supporting treatment efficacy. Many of the clinical trials had design flaws
including problems with patient selection, inadequate blinding, and an
inappropriate focus on analyses of subjects that completed the trials in
preference to intention-to-treat analyses.
This study evaluated whether
intra-articular HA, compared with placebo injections is efficacious.
Conclusion: HA has a small effect when compared with an intra-articular
placebo. The placebo effect may be the main reason for pain relief.
1. Meta-analysis of 22 single- or double-blind
randomized controlled trials compared
2. For each trial these investigators
calculated an effect size: small-effect sizes--0.2 to 0.5; and
1.
The overall dropout rate was 12%.
2.
At least 17 of the 22 trials were industry sponsored .
3.
There was significant heterogeneity among studies.
4. Including all studies, the pooled effect size
was 0.32, consistent with a small effect. No trials had
5.
Two outlier trials evaluating the highest-molecular-weight HA had effect in
excess of 1.5.
(The investigators suggest that effect sizes
comparable to knee replacement do not seem realistic.)
6.
There was evidence of publication bias. The pooled effect size of the
unpublished studies
1. “Based on the findings of this
meta-analysis, intra-articular hyaluronic acid has, at best, modest
2. This effect . . . “is equivalent to the
effect of NSAIDs over that of acetaminophen, an effect that
3. The effect size of most trials had 95%
confidence intervals that included an effect size of zero,
4. Multiple trials used analysis of only
those who completed the trials and not intention-to-treat. They
5. At least 17 of the 22 trials were
industry sponsored. Others have suggested that findings from
6. All 22 studies reported improvement of pain
in the intra-articular placebo groups. Placebo
7. “This supports our hypothesis that the
majority of the effect of intra-articular hyaluronic acid is an
Intra-articular hyaluronic acid has a
small effect when compared with intra-articular placebo.
Publication bias may overestimate the effect.
Compared with lower-molecular-weight hyaluronic acid, the higher-molecular
weight hyaluronic acid may be more efficacious, but heterogeneity of studies
limits definitive conclusions.
Comment:
This
article presents some interesting points:
1.
Enthusiasm of early trials usually is blunted by later on-going trials. (Partly
due to reduction toward the mean?)
2.
Industry-sponsored trials unfortunately are suspect. This is a shame, I believe
that many trials so sponsored do not
include bias promoted by manufacturers. However, enthusiastic independent
investigators may subconsciously be biased toward the sponsored drug.
3.
Industry-sponsored trial drugs showing little or no benefit over placebo or
over a previously effective similar drug
are less likely to be published.
I doubt this study will deter
enthusiasts for using HA. Individual patients who have apparently obtained
relief may insist on continuing.
The only way an individual’s response
can be accurately determined is by an N-of-one trial.
I
doubt this would be feasible considering the ethical issues involved. RTJ
12-7
SCREENING FOR DEPRESSION IN PRIMARY CARE WITH TWO
VERBALLY ASKED QUESTIONS
The US Preventive Services Task Force endorsed
screening for depression, but did not recommend a specific screening tool. Many primary care clinicians find screening
questionnaires for depression too cumbersome and time consuming for routine
use. This study used a simple screening tool of two questions. If one or two
were answered positively, further questions were asked to determine if major
depression was present. (A composite interview--the “Gold Standard”)
The screening questions:
1)
During the past month have you often been bothered by feeling down,
depressed,
2) During the past month have you
often been bothered by little interest or pleasure
The objective of this study was to
determine the diagnostic accuracy of these questions when asked verbally.
Conclusion: The questions would detect almost all cases of depression in
primary care. Many false positives occurred and would require further
investigation. If the questions were answered negatively, depression was ruled
out.
1. Cross sectional study of 15 general
practices asked the questions of 421 consecutive patients.
2. Practitioners asked the questions at
any time during the consultation. If either was answered positively, the test
was considered positive.
3.
The gold standard for depression was a composite interview.
1.
The sensitivity of the two screening questions was 97% (few false positives).
2.
The specificity of the two questions was 67%. (many false positives)
3. True
and false positives: true and false negatives:
Positive screen Negative
screen
True positive False positive True negative False
negative
28 129 263 1
4. The high sensitivity was accompanied by a high
number of false positive results. This
would require
DISCUSSION
1. In the community setting, the two verbally asked
questions have a good sensitivity (97%)
2. About 5 false positives would occur for
every true positive when asking the questions alone.
3. The two questions are considerably
shorter than the shortest (7 questions) screening
Two verbally asked questions for screening
for depression would detect most cases of depression in primary care. Many
false positive tests occur, necessitating further questioning in subjects with
a positive 2-question screen.
Comment:
The
investigators stress that the questions should be asked verbally. They did not
go into detail about their reasons. I assume the verbal response would be more
revealing (body language) than responses to written questions. The gist to the
screen is that if it is negative, depression is very unlikely. If the screen is
positive, doubt remains, and further investigation is warranted.
12-8 REVIEW OF SENSITIVITY, SPECIFICITY,
PREDICTIVE VALUES AND LIKELIHOOD RATIOS
I
abstracted the preceding article in part because it gave me the opportunity to
review various applications of “evidence-based medicine” which are so often
included in studies I abstract. If I do not review them periodically, I will
forget how to calculate them. RTJ
Truly
depressed* Not depressed* Total
Test
positive 27 (a; true positive) 129 (b; false positive) 156 (g)
Test
negative 1 (c; false negative) 263 (d; true negative) 264 (h)
Total 28 (e) 392 (f)
(*By
composite interview—the “gold standard”)
A. Sensitivity of test = % of subjects with depression who had a positive test = a/e = 27/28 = 97%
(When
a test has a high sensitivity (few false negatives), a negative result makes
the diagnosis
(Note—this
calculation is made from the first column.)
B. Specificity of test = % of subjects without depression who had a negative test = d/f = 263/392
= 67%
(When a test has a high
sensitivity (few false positives) most subjects with a positive test will be
2. Predictive values:
A. Positive predictive value (+PV)
= the proportion of subjects with positive tests who have depression =
True + / total + = 27/156 = a/g = 0.17
= 17%
In
the study the test does not have a very high +PV (only 17%). Thus a positive
test does not indicate a high probability that the subject has depression. (too
many false + tests.)
(Note—the
+PV is calculated from the top row.)
B.
Negative predictive value (-PV) = the proportion of subjects with a negative
who do not have
In this study a negative test has a high probability (99%) or ruling out depression. (Very few false negatives.) At a population prevalence of 6% of major depression, a negative test would almost always rule out depression. (Note that the-PV calculated from the bottom row.)
3. Likelihood ratios
A. Positive likelihood ratio (+LR)
Ratio
between positive tests:
1)
The % of subjects with depression who
have a positive test (true + percent)
and
2)
The % of subjects without depression
who have a positive test.(false +
percent)
In
this study 1) = a/e = 27/28 = 97%
2)
= d/f = 129/392 = 33%
The
positive likelihood ratio = 97/33 = 2.9
(Note
that the + LR = sensitivity of the test/100 – specificity of the test. The
calculation
Likelihood
ratios of greater than one produce a post-test probability that is higher than
the pre-test probability. 2.9 is a
modest +LR and indicates the probability that depression is present by a small degree. A +LR of 10 or 20
would indicate a strong possibility that depression is present.
B. Negative
likelihood ratio (-LR):
The
ratio between negative tests:
1)
The % of subjects with depression who
had a negative test and
2)
The % of subjects without depression
who had a negative test.
In
this study: 1) = a/e = 1/28 = 3.5%
(false positive percent)
2)
= d/f = 263/392 = 75% (false negative %)
1)
/ 2) = 3.5/75 = 0.05
Likelihood
ratios of less than one produce a post-test probability that is lower than the
pre-test probability. 0.05 virtually
rules out the probability that the patients have depression.
I still
struggle with these calculations. And when I complete them I am not certain
they are correct. The more often I calculate them, the more certain I become.
Readers, have I calculated them correctly?
RTJ
This
Preparation Was Not Effective
12-9 EFFICACY AND SAFETY OF ECHINACEA IN
TREATING UPPER RESPIRATORY TRACT INFECTIONS IN CHILDREN
Echinacea is a herbal remedy widely used for
prevention and treatment of upper respiratory infections (URIs). It is one of the most commonly used herbal remedies in the
USA . Three species of echinacea are used for medical purposes. Beneficial
effects are thought to be due to its “immunomodulating” activity, most notably
macrophage activation and enhanced neutrophil phagocytosis.
A number of clinical trials of echinacea
have concerned adults. Results have been mixed. Most investigations have
concluded that the evidence suggests that it may be an efficacious treatment
for URIs. This conclusion is limited by
methodological flaws in many of the studies. There are limited data in
pediatric patients.
This study postulated that treatment with E purpurea would result in at least a
1.5- to 2-day reduction in duration of URIs in children, and that symptoms
would be less severe than in patients receiving placebo.
Conclusion: The preparation used in this study was not effective in treating URIs in children.
1.
Randomized, double-blind, placebo-controlled trial entered over 400 healthy
children age 2 to 11. (Mean age 5)
2.
Randomized to: 1) echinacea, or 2)
placebo. Study medication was begun at the onset of URI symptoms and continued
throughout the URI, for a maximum of 10 days.
3. The preparation used was made from
juice pressed from flowering E purpurea
which was then dried and combined with syrup. Plain syrup was used as the
placebo. This extract has been used extensively. The dosing instructions were based on the recommendations of the
manufacturer. The study medication was begun at the start of the URI and
continued until all symptoms had resolved.
4. Parents were asked to monitor their child’s
symptoms daily and record severity of symptoms (sneezing, coughing, nasal
congestion, and runny nose) on a 4-point scale. The overall severity was
computed by summing daily scores.
5.
Main outcome measures: duration and
severity of symptoms, and adverse events
6.
“Other symptoms” were classified as an adverse event.
1.
Data on 707 URIs in 407 children:
Outcomes Echinacea (n =200) Placebo
(N = 207)
Duration of symptoms (days) 9 9
Severity of symptoms (median) 33 33 (sum of daily scores)
Days of fever 0.81 0.64
Peak severity of symptoms 6.0 6.1
No. of days of peak severity 1.6 1.6
Parental assessment of severity (%)
Mild 46 46
Moderate 40 43
Severe 4 11
2.
Adverse events:
Rash 24 (7.1%) 10 (2.7%)
(P value .008)
(At least one adverse event was reported
during 43% of URIs, with no significant difference between groups except for
rash.)
Two children (both in the echinacea group)
had an adverse event (sudden onset of stridor) severe enough to necessitate a
visit to the emergency department.
3.
Parents were asked to guess which medication their child had taken.
Echinacea
group Placebo group
Correct guess 35% 34%
Thought taken placebo 23%
Thought taken echinacea 34%
Didn’t know 42% 41%
1.
Echinacea as given in this study was not effective in shortening duration or
decreasing severity of URIs in children. In no group of children studied did
echinacea appear to have a positive effect.
2.
Rash was more common in those taking echinacea. Severe reactions to echinacea,
including anaphylaxis have been reported.
3.
Because the active ingredients in echinacea have not been standardized, it is
difficult to determine the optimal dosing regimen in children.
4.
The effect of echinacea in prevention
of URIs deserves additional study.
“Our results do not support the use of
echinacea for treatment of URIs in children.”
Its use was associated with an increased risk of rash.
Comment:
This
study was supported by a grant from the National Center for Complementary and Alternative
Medicine. Bastyr University is an alternative medicine institution.
It continues to amaze me that so many
persons take unstandardized and unproven nostrums and give them to their
children. I am sure devotees will fault this study. They will remain convinced
that echinacea is beneficial.
Several “alternative and complementary”
interventions have recently fared poorly when examined scientifically:
St
John’s wort: Significantly induces
cytochrome P450 in the liver. This hastens the metabolism of at least half of
all marketed medications thus diminishing their clinical effectiveness. Recent
randomized, placebo controlled studies do not support its effectiveness for
moderate or severe depression. (JAMA September
17, 2003; 290: 1500-04)
Evening primrose: Gamma linolenic acid, the presumed active
ingredient in Evening Primrose oil (“Borage oil”) has been used extensively for
treatment of atopic dermatitis. A randomized,
double-blind, placebo-controlled trial GLA failed to find any benefit. (BMJ December 13, 2003; 327: 1385-87 and Editorial in
the same issue pp 1358-59) The
UK’s Medicines Control Agency has withdrawn the product license.
Magnets for plantar heel pain: A randomized, double-blind, placebo
controlled trial reported no benefit. (JAMA September 17, 2003; 290: 1474-78)
Ephedra: The FDA recently ordered its
removal from over-the-counter distribution due to reports of a number of
deaths. RTJ
Interesting,
But Far-Off
12-10
SCREENING VIRTUAL COLONOSCOPY—READY FOR PRIME TIME?
Screening for colo-rectal cancer (CRC) is recommended for asymptomatic,
average-risk adults, beginning at age 50. Screening detects early-stage
non-metastatic cancers that are surgically curable, and permits removal of
benign adenomas, the precursor lesions of nearly all adenocarcinomas.
Several approaches to screening are available. Each
test has inherent strengths and weaknesses.
Fiberoptic colonoscopy is the current gold
standard for screening against which all other tests are compared. It provides
high sensitivity with a false-negative rate of about 6% for adenomas 10 cm or
more in diameter. Its drawbacks include need for insertion of an intravenous
catheter for administration of sedatives, a recovery time of 30- to 60-minutes,
and the requirement for a driver to accompany the patient home. Total time is
about 2 hours. It carries some risk of perforation and bleeding, effects of
sedatives, and other complications. Most consider the risks to be acceptable.
Virtual colonoscopy (computed tomographic
colonography) was first described in 1994. It requires the same bowel-cleansing
preparation as conventional colonoscopy. And insertion of a rectal tube, and
insufflation of air or carbon dioxide to distend the colon. Time required is
about 10 to 15 minutes, with an additional 30 minutes for interpretation.
A study reported in this issue of NEJM describes
a new technique for virtual colonoscopy.
The
new VC used a multidirectional CT scanner providing a primary 3-dimentional
endoluminal display which permitted faster, higher-resolution imaging than
previously obtainable. Residual fluid and stool was tagged by contrast
material. The imaging software digitally removed all opacified fluid and stool
from the colon by a process called “electronic cleansing”.
Subjects received the new virtual
colonoscopy (VC) followed by conventional colonoscopy for comparison:
Sensitivity of VC for detection of adenomas vs traditional
colonoscopy:
10 mm or larger was 92% vs 88%
8 mm or larger was 92% vs 89%
6 mm or larger was 86% vs 90%
The study suggests that VC can detect
polyps of 6 mm or larger as accurately as conventional colonoscopy in a
population with a low prevalence of colorectal neoplasia.
A critical issue remains—what is the
choice of polyp size for VC that should trigger referral for conventional
colonoscopy? “The referral of all
patients who were found on VC to have a polyp 10 mm or larger would probably
result in the detection of nearly all cancers and eliminate the need for a
large number of colonoscopies. “
At the close of the study patients were
asked to state their preference, VC or traditional. Only 50% chose VC; 41%
chose conventional. A substantial
proportion may still opt for conventional because it allows suspicious lesions
to be removed
Decisions regarding the use of VC as a
first-line screening test will require more information about cost and
insurance coverage. “The performance of VC in this asymptomatic population is
impressive, with detection rates similar to those achieved by conventional
colonoscopy.” Only if the important questions about the appropriate size
threshold and the surveillance of smaller polyps can be resolved will VC be
ready for prime time.
1 “Computed Tomographic Virtual Colonoscopy to
Screen for Colorectal Neoplasia in Asymptomatic Adults” NEJM December 4, 2003;
349: 2191-200, original investigation, first author Perry J Pichhardt, Uniformed Services University of
the Health Sciences, Bethesda, MD
The investigators commented that VC also
detected 5 asymptomatic cancers outside the colon as well as aortic aneurysms,
and renal and gall bladder calculi.
I abstracted this editorial as a look into
the future. Patients may be asking about it. Much more training, experience and
local availability will be needed for this new VC to reach primary screening
status. One large bugaboo is the need for a follow-up conventional colonoscopy
for removal of polyps of a certain size. And repeated follow up scans in those
with polyps under a stated size. This size is not yet determined. RTJ