PRACTICAL POINTERS
FOR
PRIMARY CARE
ABSTRACTED MONTHLY FROM THE JOURNALS
JANUARY 2005
TREAT THE PATIENT, NOT THE
BLOOD PRESSURE—NOT THE CHOLESTEROL
WHY DO WE UNDERUSE
TREATMENTS THAT ARE BENEFICIAL IN TRIALS?
IS THE EVIDENCE
“GENERALIZABLE” TO MY PATIENT?
FOLIC ACID REPORTED TO
REDUCE RISK OF DEVELOPING HYPERTENSION
AROMATASE INHIBITOR SAFER
AND MORE EFFECTIVE THAN TAMOXIFEN
AN ABCDE MEMORY DEVICE FOR
ACUTE CORONARY SYNDROMES
ADHERENCE TO 4 DIFFERENT
DIETS WAS POOR
FAST FOODS—A
PARTICULARLY OMINOUS PUBLIC HEALTH ISSUE
STOOL ANTIGEN
TEST IS RECOMMENDED TO DETECT H PYLORI
INFECTION
PHYSICIAN’S
POWER CAN BE USED WELL OR ILL, BUT IT CANNOT BE DISOWNED
USPSTF
RECOMMENDS SCREENING FOR AORTIC ANEURYSM IN MEN
ONE OR TWO DRINKS
A DAY MAY DECREASE THE RISK OF COGNITIVE DECLINE
STATINS REDUCE
C-REACTIVE PROTEIN LEVELS
CARDIOVASCULAR
RISK FACTORS MAY INCREASE RISK OF DIABETIC NEUROPATHY
FASTING SERUM GLUCOSE LEVEL
ASSOCIATED WITH CANCER RISK
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 NC
28036 USA www.practicalpointers.org
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been supported financially solely by the publisher as a public service. Now,
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HIGHLIGHTS AND EDITORIAL
COMMENTS JANUARY 2005
Treat the Patient, Not the Blood Pressure—Not the
Cholesterol.
Absolute risk of a cardiovascular disease
is the probability that an individual
patient will have an event over a defined period. It is determined by a
synergistic effect of all CVD risk
factors present in the individual. It may be true that, in a large group of
individuals with a systolic BP of 160, the CVD risk is twice as high as in a large group with a systolic of
110 (relative risk). In an
individual, however, absolute risk depends on much more than a single risk
factor. Indeed, absolute differences in risk can vary more than 20-fold in
patients with the same BP.
“Cardiovascular treatment benefit is
directly proportional to the pre-treatment absolute risk.”
A new approach to preventive therapy is to
modestly reduce all modifiable risk factors rather than concentrating on
reaching “target levels’ of one or two.
This
is a sea change in our approach to lowering risk.
Please
read the full abstract.
Why do we Underuse Treatments That are Beneficial in
Trials?
1-2 EXTERNAL VALIDITY OF RANDOMIZED CONTROLLED
TRIALS: To Whom do the Results of this Trial Apply?
Randomized controlled trials (RCTs) and systematic reviews must be internally validated. (Ie, the design
and conduct of RCTs must keep the possibility of bias to a minimum). To be
clinically useful, however, the results must be relevant to a definable group
of patients in a particular clinical setting.
This is termed external validity.
The most frequent criticism by clinicians
of RCTs, systematic reviews, and guidelines is the lack of external validity.
This explains the widespread underuse in routine practice of treatments that
are beneficial in trials and recommended by guidelines.
Assessment of external validity requires
clinical rather than statistical expertise.
The response to, and compliance with,
treatment can be influenced strongly by the doctor-patient relationship,
placebo effects, and patient preferences. The importance of these factors
outside of trials should not be underestimated. Note the popularity of
“alternative” therapies in which such factors are the only active ingredients.
The
primary care clinician is a final arbiter of external validity. (Would this
application be clinically useful for Mrs. Jones?)
Beware
of surrogate outcomes in RCTs, of composite outcome measures, underreporting of adverse effects, and reports by pharmaceutical companies.
Primary
care difficult, challenging, and so rewarding.
Is the Evidence “Generalizable” to my Patient?
1-3 EVIDENCE-BASED PRACTICE AND THE INDIVIDUAL
Is my patient so different from those in
the trial that its results cannot help me make my treatment decision? The more
family practitioners feel they know their patients, the less likely they are to
apply external evidence to guide management.
Disingenuous surrogate markers and
misleading composite outcomes may create good advertising material, but cannot
obscure data and hinder genuine patient-centered care.
Let us not neglect the central role of
individual patients as decision-makers in their own care. “It is the
responsibility of healthcare workers to communicate objective evidence in a
manner which allows recipients to make an informed choice, and then to respect
that choice.”
“Now and then, clinicians will have to
accept and explain that uncertainty is an inherent facet of the uniqueness of
human nature. Evidence helps to quantify that uncertainty, but cannot remove
it.”
If
Confirmed, This Represents An Enormous Public Health Benefit.
1-4 FOLATE INTAKE AND THE RISK OF HYPERTENSION
AMONG U.S. WOMEN
Oral folic acid supplementation improves endothelial
function. Folate may have beneficial effects on blood pressure by increasing
nitric oxide synthesis in endothelial cells, and by reducing plasma
homocysteine levels. (Homocysteine by itself can cause endothelial cell
injury.)
This study assessed the association of folate intake
with incident hypertension in 2 large groups of women.
Younger women (mean age 36 at baseline):
Identified 7373 incident cases of hypertension (8%)
over 8 years.
Subjects whose daily consumption was at least 1000 ug of total folate (diet + supplement) had a relative risk of developing hypertension of 0.54 compared with women who consumed less than 200 ug daily.
Absolute risk reduction of incident hypertension was
about 8 cases per 1000 person-years.
Older women (mean age 55 at baseline):
Identified 12347 incident cases of hypertension (19%)
over 8 years.
Relative risk of hypertension (1000 ug folate daily vs less than 200 ug) = 0.82.
Absolute risk reduction of incident hypertension was
about 6 per 1000 person-years.
The most significant relationship was associated with
supplemental (not dietary) folate intake.
(Bioavailability of supplemental folate is twice that
of food folate.)
Younger women achieved the most benefit. Younger women
whose intake was at least 1000 ug experienced 1/3 the risk of developing
hypertension over 8 years. (Ie, start
supplementation early. RTJ)
High intake of folate was associated with a decreased
risk of incident hypertension, especially in younger women. Supplemental folate
was independently beneficial.
If confirmed
as true, this has enormous public health benefit.
The benefits
of folate extend to prevention of spina bifida and coronary heart disease. The
benefit/harm-cost ratio is very high.
Aromatase Inhibitor Safer and More Effective Than
Tamoxifen
This study compared the aromatase
inhibitor anastrozole with tamoxifen over 5 years.
Compared with tamoxifen, anastrozole led
to significant improvements for disease-free survival, and time-to-recurrence,
especially in women whose BC was hormone-receptor-positive. Benefits were also demonstrated in hormone-receptor-negative patients.
Benefits were therefore in addition to the risk reduction
previously shown in tamoxifen vs placebo trials. (Ie, anastrozole vs placebo would have shown greater absolute benefits
compared with tamoxifen vs placebo)
The incidence of contralateral BC was
substantially reduced by anastrozole as compared with tamoxifen. (This was also
an improvement over the benefit of tamoxifen alone vs placebo as demonstrated
in previous studies.)
Withdrawals were significantly fewer in
the anastrozole group (11% vs 14%).
Drug-related serious adverse events were
also fewer (5% vs 9%).
Anastrozole was associated with
significant reductions in endometrial cancer, thromboembolic events, ischemic
cerebrovascular events, vaginal bleeding, and hot flushes.
Arthralgias and fractures were more
frequent in the anastrozole group. (The
authors suggest concomitant bisphosphonate therapy because of this finding.)
It is reasonable to switch patients
currently on tamoxifen to an aromatase inhibitor. It is not appropriate to wait
until after a 5-year period of treatment with tamoxifen. The most effective and
well-tolerated therapy should be offered at the earliest opportunity
Anastrozole should be considered the
preferred initial adjuvant endocrine
therapy for post-menopausal women with hormone-receptor positive localized BC.
Aromatase
is the enzyme which catalyses conversion of androgens to estrogens in females.
Aromatase inhibitors block production of estrogen.. There are three 3rd generation
compounds under investigation: exemestane, anastrozole, and letrozole. The
action of exemestane is irreversible.
A
similar study reported in NEJM March 11, 2004 reported similar benefits when
exemestane was substituted for tamoxifen after 2 to 3 years.(See Practical
Pointers March 2004 [3-9] )
I
believe this represents a major improvement in therapy of BC, and likely an
improvement in prevention.
I
wonder—would there be any benefit in treatment of ductal carcinoma in situ?
Proposing
an ABCDE Memory Device to Simplify Adherence to Guidelines
1-6 A SIMPLIFIED APPROACH TO THE MANAGEMENT OF
NON-ST-SEGMENT ELEVATION ACUTE CORONARY SYNDROMES
The study assembled a comprehensive plan through an
“ABCDE” approach. The intention was to provide a memory device to overview
therapies and lifestyle changes that are clinically useful for patients with
NSTE-ACS.
Elements of the plan:
A Antiplatelets;
Anticoagulation; ACE inhibitors; Angiotensin II blockers.
B Beta-blockers;
Blood pressure control
C Cholesterol
management; Cigarette cessation
D Diet; Diabetes management
E Exercise.
This practical approach allows physicians to more
effectively create disease management protocols, define roles and
responsibilities for different medical personnel, and ensure implementation of
evidence-based short-and long-term medical and risk-reducing strategies.
This plan is
almost identical to a check list presented in the Archives Int Med July 2004
for secondary prevention of cardiovascular disease. (See Practical Pointers
July 2004 [7-8])
I believe
check lists can be a valuable addition to primary care. In the hurried pace of
practice, we all omit (simply forget to consider) aspects of treatment and
lifestyle which should be addressed at almost every patient visit. A mneumonic
check list is a practical approach.
Some
clinicians may make their own. I tried to create a mneumonic check list for
diabetes:
D Diet; Depression
I Insulin
A Aspirin; ACE inhibitors
B BMI; BP
E Exercise
T Tests (blood glucose; HbA1c; lipids;
microalbuminuria; liver function; ejection fraction)
E Eye (retinopathy); Extremities (foot health;
foot pulses; peripheral neuropathy)
S Sulfonylureas, Statins, and other oral
drugs; Smoking
Plus (Add
others which might be indicated.)
Adherence
was Poor. Those Who Adhered for One
Year Lost Weight
This study assessed adherence rates and effectiveness
of 4 diets in producing weight loss and reducing cardiac risk factors:
1. Atkins Low carbohydrate—20 g carbohydrate daily
2. Zone High
protein, low glycemic load
3. Weight Watchers Balanced diet—total daily ”points” in a range determined by current weight (Aimed for 24 to 32 points daily.)
4. Ornish Low
fat, vegetarian diet containing 10% of calories as fat.
About half of the subjects in each group failed to
complete the 1-year course. The most common reasons were “too hard to follow”
and “not yielding enough weight loss”. Adherence was particularly low for
Atkins and Ornish.
At 1 year, completers lost more than those who failed
to complete (-3. 9 kg for Atkins and
-6.6 kg for Ornish)
Each diet significantly reduced LDL/HDL-cholesterol ratio
by about 10%. The Atkins diet did not lower LDL-cholesterol significantly. The
Ornish diet did not increase the HDL-cholesterol. No diet significantly altered
triglyceride levels. Reductions of total cholesterol, C-reactive protein, and
insulin levels were significantly associated with the degree of weight loss.
Under realistic conditions a variety of popular diets
can reduce weight and several cardiac risk factors. But only about half of the
subjects in this study sustained a high adherence level.
The problem
is not the diet, it is the patient’s inability to follow it. Recidivism would
be higher still at 5 or 10 years. The
bloom seems to be coming off the Atkins diet.
The authors
suggest that one way to improve dietary adherence in clinical practice may be
to use a broad spectrum of diet options to better match individual patient’s
food preferences, lifestyles, and cardiovascular risk factors. They suspect
adherence would have been better if subjects had been given the option to
choose their diet.
I wonder—would switching from one type of diet to
another every few months increase compliance?
A Particularly Ominous Public Health Issue
1-8 FAST-FOOD HABITS, WEIGHT GAIN, AND INSULIN
RESISTANCE
This study investigated the association
between fast-food habits of young U.S. adults and changes in body weight and
insulin resistance over a 15-year period.
At baseline, weekly visits to fast-food
restaurants = 2.4 for men and 1.7 for women. Younger subjects made more visits.
There was a direct and independent monotonic association between fast-food
frequency and weight and insulin resistance. Subjects who visited three times a
week had a mean weight about 2 kg higher than those who visited less than once
a week.
Over 15 years, frequent visitors gained
more weight compared with those who visited less than once a week. Insulin resistance was directly associated
with visits of 3 times a week. There was a direct and independent monotonic
association between fast-food frequency and weight
and insulin resistance. Compared with subjects whose fast-food visits were less
than once a week, those who visited over 2 times weekly gained an extra 4.5 kg and had a 104% greater increase in insulin
resistance.
Fast-food habits have strong, positive and
independent association with weight gain and insulin resistance in young
adults. This suggests an increased risk of type 2 diabetes and obesity.
I am
sure that this does not surprise anyone.
The
study points out some differences between blacks and whites, and between males
and females. See the text.
“Overload
your truck & it will break down.”
The
fast-food industry is beginning to make some adjustments in their menus. This
is difficult for a highly competitive industry. To stay in business, the
competition must be met. Customers will frequent the establishments offering
the best tasting foods and the largest portion size. The solution lies, not in
forcing the fast-food to change their menus, but by making a sea-change in
public awareness and compliance with a “healthy diet”—an almost impossible task
which will take years to accomplish even partially.
Stool Antigen Test is Recommended
1-9 TEST AND TREAT FOR DYSPEPSIA: But Which Test?
The National Institute for Clinical
Excellence (NICE) of the UK recommends that patients with persistent or recurrent uncomplicated dyspepsia should have a non-invasive test
for Helicobacter pylori. If the test is positive they should receive
eradication (triple antibiotic) therapy
Now the stool antigen test is available.
It detects H pylori antigens passed
in feces. A commercial monoclonal antibody test is available. It is reported to
be as accurate as the urea breath test. It can be introduced with ease into
routine laboratory practice. It is less expensive and less time consuming than
the urea breath test. It is useful also
in confirming eradication of the infection.
“We need to have an easy, accurate
diagnostic test and the stool antigen test is just that.”
There
are some advantages of “test and treat”:
Will treat an
unsuspected peptic ulcer. And reduce risk of subsequent ulcer disease.
Will
reduce or eliminate symptoms in some patients ( ~ 10%). Since about 50% of patients with functional
dyspepsia will be positive, eradication will remove symptoms in only 5% of
patients with dyspepsia.
Remove a risk
factor for gastric cancer.
Physician’s Power Can be Enhanced, Diminished, Used
Well or Ill, but It Cannot be Disowned.
1-10 CONSENT OR
OBEDIENCE? Power and Authority in Medicine
This essay considers the role of inappropriate obedience as a source of abuse in the
teaching hospital and the effect of obedience on patients’ autonomy and
consent.
Patients provide consent not only about
big issues, but, in the course of an illness, sick patients consent innumerable
times to interventions that they would rather not undergo.
Serious illness is marked by losses of
normal function in many dimensions of existence, including the ability to
reason and to act (without which “autonomy” loses meaning). Sick patients do
not reason their way to decisions based on their appraisals of the relevant
information, but because an authority helps them to decide.
A power comes from the hospital setting
and the trappings of medical authority. “Such power can be enhanced,
diminished, used well or ill, but it cannot be disowned.”
Bearing in mind the effect of sickness on
function, we should accept the propensity of sick patients to seek our
approbation, celebrate our expertise, and acknowledge the legitimacy of our
authority by doing as they think we wish. These tendencies present us with
difficult responsibilities.
“The biggest thief of autonomy is
sickness.”
I
enjoyed this thoughtful essay.
We
live in a world in which authority leads multitudes to follow blindly and
commit unspeakable atrocities. The
resistance of one man is a badge of courage.
I
believe physicians apply their power to some extent in every patient encounter.
Physicians, wield your power carefully and always with the aim of benefit to the
patient.
The USPSTF Now Recommends One-Time Screening in Select
Subsets of Men
1-11 SCREENING FOR
ABDOMINAL ANEURYSM
The U.S. Preventive Services Task Force (USPSTF) now recommends one-time
ultrasonographic screening for abdominal aortic aneurysm (AAA) for men ages 65 to 75 who presently smoke or who have smoked
in the past.
The task force makes no recommendation for
or against screening men who have never smoked. It recommends against routine screening for women.
One-time screening is sufficient.
Is
there any medical treatment? Will beta-blockers decrease the rate of expansion
by reducing the stress caused by the steep increase in wall expansion during
systole? Many patients in this age
group with AAAs would be candidates for beta-blocker therapy because of an
increase in risk factors for CVD, including sub-optimal BP control.
As
always, primary care clinicians must judge benefits vs harms of individual
patients. The availability of expert, safe surgery is a major factor influencing
the recommendation.
Advice
for screening carries ethical considerations. Although opportunistic preventive
medicine is considered a part of good medical practice, is it always ethically
justifiable? Consider a male smoker age 70 who consults for arthritis. Should
the primary care clinician at the time of the consultation advise the patient
to undergo screening for AAA? Should the primary care clinician advise a
prostate specific antigen?
Physicians
who offer a screening test carry a considerable responsibility. They must offer
enough information about risks and benefits in order to enable the patient to
give informed consent. Every test carries a chance of a false-positive result
leading to interventions that do not benefit the patient, and may cause harm.
I
believe many primary care clinicians would limit screening for AAA to patients
who consult for a specific indication—assessment of their general health
status.
One or Two Drinks a Day May Decrease the Risk of
Cognitive Decline.
1-12 EFFECTS OF MODERATE
ALCOHOL CONSUMPTION ON COGNITIVE FUNCTION IN WOMEN.
This study asks—What is the effect of moderate consumption of alcohol on
cognition? A benefit is plausible considering the strong link between moderate
alcohol and decreased risk of cardiovascular disease. Cognitive impairment and
cardiovascular disease share common risk factors.
Compared with abstainers, moderate
drinkers (less than 15 g alcohol per day; one drink) had better mean cognitive
scores. (Relative risk of impairment = 0.81 based on a global cognitive
score.) Also, compared with abstainers,
moderate drinkers (15 to 30 g per day) had a reduced relative risk of cognitive
impairment (although slightly less favorable, with wider confidence intervals).
In older women consumption of one
alcoholic drink per day did not impair cognitive function, and may actually
decrease risk of cognitive decline.
Benefits of moderate alcohol consumption have
been reported with remarkable consistency over the past 10 years. Indeed, some
epidemiologists consider abstinence to be a risk factor for cardiovascular
disease.
As
always, we should be cautious about generalizing the conclusions of
observational studies.
Statins Reduce C-Reactive Protein Levels and Improve
Outcomes Independently of LDL-Cholesterol
1-13 STATINS FOR
ATHEROSCLEROSIS—Autoimmunity, Inflammation, and C-reactive Protein.
Statin drugs, in addition to inhibiting
synthesis of cholesterol, now appear to directly inhibit inflammation.
Two articles in this issue of NEJM confirm
that reducing the inflammatory component of cardiovascular disease with statin
therapy improves clinical outcomes independently of the reduction in
cholesterol. Both studies found that the statin-induced decrease in C-reactive
protein (CRP), a marker of
inflammation, is only weakly correlated with changes in lipid levels.
The LDL-c lowering effect of statins and
their effect on lowering CRP are largely independent of each other. Patients
achieving the lowest CRP levels through statin therapy had a higher event-free
survival at all levels of LDL-cholesterol.
Only by assaying both C-reactive protein
and cholesterol can the full effect of statins be identified.
Statins
are the “penicillin” of the last of the 20th century
This
is not a practical point at this time. Although it is still “far out”, I
included the abstract because of its potential. We need a more specific agent
to reduce C-reactive protein levels.
CRP
is formed in the liver in response to acute inflammation. It is a non-specific
marker. C(capsule)-reactive
protein has an interesting history. It was first described in 1930 as an
indicator of pneumococcal infection because it reacts with the polysaccharide
in the capsule of the pneumococcus.
Development May be Delayed by Good Glycemic Control
and Modification of Cardiovascular Risk Factors.
1-14 VASCULAR RISK FACTORS
AND DIABETIC NEUROPATHY
The Diabetes Control and Complications
Trial reported a 60% reduction in DN in the intensively treated group at 5
years. But the incidence still remained substantial. This suggests that DN can
develop despite intensive control of glucose levels. Risk factors other than
glucose are involved.
This study assessed potentially modifiable
risk factors for development of distal, symmetric DN.
Dyslipidemia, elevated BMI, smoking, and
hypertension were associated with development of DN.
Cardiovascular disease at baseline was
associated with double the risk of neuropathy.
What can be done prospectively to try to
prevent DN?
Control glycemia as best it can be controlled
Stop smoking
Control BP
Control weight, obtain lower body mass index
Reduce other cardiovascular risk factors.
(Ie, essentially
standard diabetes management.)
I
enjoyed reviewing the diagnosis of neuropathy.
The mean age at baseline was about 30. Of an
initial cohort, 28% already had DN.
Prospectively, over 7 years 23% developed DN. Thus at age about 40, over
half had DN. I would expect almost all
patients with type 1 diabetes will eventually develop DN.
Fasting
Serum Glucose Level and Diabetes were Associated with Cancer Risk
1-15 FASTING SERUM GLUCOSE LEVEL AND CANCER RISK
IN KOREAN MEN AND WOMEN
Is there any connection between diabetes and cancer?
Some observational studies have suggested there is. This prospective cohort
study investigated this possibility.
A ten-year prospective study enrolled over 829 000 men
and over 468 000 women age 30 to 95 at baseline. (Mean = 46; mean body mass
index = 23)
After adjusting for smoking and alcohol use, the
stratum with the highest fasting glucose (> 140) had higher death rates from
all cancers compared with the stratum with the lowest level (< 90). Hazard ratio = 1.25
Age-adjusted cancer deaths per 100 000 men rose
linearly from about 600 in the groups with fasting glucose < 90 to about
1400 per 100 000 in the group with glucose levels above 140. (Although absolute numbers are low, the
linear relationship depicted on page 196 and 200 is impressive. RTJ).
Similar linear increases were recorded in women, although not as high in
absolute terms. Incidence of cancer was similar to mortality.
The association was strongest for pancreatic cancer.
(Hazard ratio = 2 comparing the highest glucose stratum with the lowest.) Significant associations were also found in
other cancers (esophagus, colo-rectal, liver, cervix).
”We have shown that fasting serum glucose level and
diabetes are associated with cancer risk in a population far leaner than the
Western populations.”
This is my
first encounter with the relation between glucose intolerance and cancer. It is
not a clinically important point now. I
felt it was interesting enough to abstract. I will watch for follow-up studies.
ABSTRACTS JANUARY 2005
Treat the Patient, Not the Blood Pressure—Not the
Cholesterol.
1-1 TREATMENT WITH DRUGS TO LOWER BLOOD
PRESSURE AND BLOOD CHOLESTEROL BASED ON AN INDIVIDUAL’S ABSOLUTE CARDIOVASCULAR
RISK.
Fifty years ago it was thought that people
either had hypertension, or not, in the same way that a woman was pregnant or
not. Now we realize that BP is continuously
related to cardiovascular risk. Hypertension is now being defined as the BP
level above which there would be clinically significant benefits from lowering
BP.
The same applies to dyslipidemia.
Cardiovascular risk factors cannot be
divided into present or absent (yes or no) categories.
This review focuses on the clinical
implications of these definitions. This is relevant because almost every adult
in the USA would be eligible for individualized treatment to lower risk of
cardiovascular disease (CVD) (I
would argue that every adult in the USA could benefit from lowering modifiable
risk factors. RTJ) This has broad public-health implications.
The authors state that treatment decisions
should be based on absolute estimates
on cardiovascular risk. As a result, some patients with average or below
average levels of BP and cholesterol should be treated in preference to other
patients who have higher levels.
Relative
risks of cardiovascular disease:
Meta-analyses show the same general
pattern of the associations between BP and cholesterol and relative risk (RR) of cardiovascular disease. When large groups of patients are
considered, for each change in BP there is a constant relative change in CVD
risk. This applies to the BP range of about 110/70 to 170/105. As systolic BP
is lowered from 170 to 160 to 150 to 140 to 130 to 120 to 110, there is a
relative risk reduction of coronary heart disease and stroke at each step.
Considering 130 as having a RR of 1.00, a large group of patients with a
systolic of 110 has a RR of about 0.75. The RR progressively increases up to
about 2.5 in those with a systolic of 170. (Figure
1 p 435). The same applies for diastolic BP and total cholesterol. This
does not mean, however, that every
man with a systolic of 170 would have his relative risk reduced from 2.5 to
1.00 if his systolic was reduced to 130.
Absolute risk
of cardiovascular disease:
Absolute risk of a cardiovascular disease
is the probability that an individual
patient will have an event over a defined period. It is determined by a
synergistic effect of all CVD risk
factors present in the individual. It may be true that, for a large group of
individuals with a systolic BP of 160, the CVD risk is higher than a large
group with a systolic of 110 (relative risk). In an individual, however,
absolute risk depends on much more than a single risk factor. Indeed, absolute
differences in risk can vary more than 20-fold in patients with the same BP
(eg, systolic 160). The difference is due to the additive effect of other risk
factors present in an individual. Powerful risk predictors such as age,
sedentary lifestyle, obesity, previous symptomatic CVD, left ventricular
hypertrophy, renal impairment, increasing BP, lipid levels, male sex, smoking,
(and others) interact to determine absolute
risk of an individual. Single risk factors (eg, BP, lipids) have a minor effect
on an individual patient’s absolute risk if they exist alone. They can have a
major effect when added to other risk factors.
“Cardiovascular treatment benefit is
directly proportional to the pre-treatment absolute risk.”
The article
presents several figures (pp 436 & 437) to illustrate this point:
Figure 5 (p 437) shows the effect on absolute cardiovascular risk of
successively adding other risk factors in individuals with the same total
cholesterol levels:
Consider a 50-year old women with a total cholesterol
of 150. If she is non-smoking, non-diabetic, has a HDL-cholesterol of 60, and a
systolic BP of 130 she has an absolute 5-year risk of CVD of less than 1%.
Consider another woman with the same total cholesterol
(150). She smokes, has a systolic BP of 170, and a HDL-cholesterol of 38. Her
absolute 5-year risk is 10%
Consider a 50-year old man with the same total
cholesterol (150). He is a smoker, has a systolic BP of 170, and a
HDL-cholesterol of 38. His absolute 5-year risk is 15%.
In all three examples, adding risks associated with
diabetes and increasing age would greatly increase absolute risk even if the
total cholesterol remained at 150.
As a result of the synergistic effect of
risk factors, individuals who have achieved the “target level” BP or
cholesterol might have much higher absolute risk than an individual with higher
BP and cholesterol. This depends on the associated risk factors in each
individual. It is true, when considering a large
group, that reducing cholesterol from 250 to 150 the risk of a CVD event
over 5 years will be lowered on average
by a certain percentage. This does not apply, however, to individual patients
since each has different risk factors and a different absolute risk. Suppose we
push therapy in an individual to achieve a cholesterol of 150 and a systolic BP
of 130. The patient smokes, is obese, and sedentary. His absolute risk will
remain high. In estimating absolute risk, multiple risk factors must be
considered. “These observations emphasize the clinical limitations of terms
such as hypertension and hypercholesterolemia.”
Short-term absolute risk (eg, 5-year risk
of a cardiovascular event) increases exponentially with age. Therefore there is
greater short-term absolute benefit from eliminating risk factors. This would favor treatment of older
patients. It has been argued that younger individuals have the more to gain because
of their greater life expectancy. But, younger persons value time in the
distant future less than in the near future. Case-fatality after a
cardiovascular event is much higher in older than in younger people.
The authors go on to comment on consideration
of the substantial merits of the “Polypill”,
a combination of 6 drugs (aspirin, a statin, folic acid, and 3
antihypertension drugs) given in low dose. A pill given to everyone over age 55
would be consistent with the absolute risk-based treatment strategy that
lessens the importance of lowering individual risk factors to “target level” in
favor of less drastic treatment of multiple risk factors. This would more
effectively lower risk. “Less emphasis should be placed on reaching treatment
targets for specific risk factors, and more on identifying high-risk patients
and targeting multiple risk factors.” Because cardiovascular risk factors act
synergistically, the most effective strategy for lowering cardiovascular risk
might be one that targets moderate
reductions in multiple risk factors
rather than large reductions in single factors. (Beneficial lifestyle changes
are the most productive, and they have no adverse effects.)
Conclusion
Individualized management of
cardiovascular risk should be based on the probable size of absolute treatment
benefits.
Attention should be moved from knowing
one’s blood pressure and cholesterol concentrations to knowing one’s absolute
cardiovascular risk and its determinants.
A quantitative
cardiovascular risk/benefit assessment should be a routine component of quality
clinical practice. “It is time for terms such as hypertension and
hypercholesterolemia to be removed from our clinical vocabulary.” The next
generation of primary care clinicians should treat risk, not risk factors.
Moderate reductions of several risk
factors can be more effective in prevention than major reductions in one.
Treat the patient, not the blood pressure—not the
cholesterol.
Lancet January 29,
2005; 365: 434-41 “Treating
individuals”, commentary, first author Rod Jackson, University of Auckland, New
Zealand.
I believe, with the necessary aid of
computers, primary care is moving closer to judging individual patient’s
absolute risk of disease, and acting on multiple risk factors, not emphasizing
only one or two. (For a beginning effort to assess multiple risks see
www.yourdiseaserisk.harvard.edu.)
We should eventually be able to tell a
patient—“Mr Jones, according to the latest scientific data, your chance of
having a heart attack or stroke in the next 5 years is one in W. You can reduce
this risk to one out of X by lifestyle changes and drug therapy. Over 5 years
you will run the risk of having a serious adverse event due to the drugs of one
in Y. Over 5-years this will cost you
$Z. Is this worth it to you?
We cannot, and should not, tell a patient
on the basis of relative risk studies--“Mr. Jones, your risk of having a heart
attack will be lowered by 30% if you lower your cholesterol to 150”.
There is a corrrelary regarding risks of
adverse drug effects. Consider the recent Cox-2 turmoil. There may be, in large
groups of patients, a small increase in relative risk of stroke and myocardial
infarction in those taking Vioxx.
But, the risk does not apply equally to all. It will be higher in those with
more CVD risk factors. Some will be at very low risk.
In addition to lowering multiple
modifiable risk factors, there are other applications which will lower risk.
Adding external protective factors such as exercising more; drinking a glass of
wine daily; and eating nuts, fish, and fruit and vegetables regularly will
lower risk still farther. (See “The Polymeal” Practical Pointers December 2004 [12-4].
The approach focusing on reduction of
multiple risk factors is not new. This is the most convincing paper on the
subject I have read. I believe this concept points to the future.
Guidelines continue to treat BP and lipid
levels, not individual patients with
varying risk factors.
====================================================================
Why do we Underuse Treatments That are Beneficial in
Trials?
1-2 EXTERNAL
VALIDITY OF RANDOMIZED CONTROLLED TRIALS: To Whom do the Results of this Trial
Apply?
(This is the
first of a series of 5 articles concerning application of trial data to
individual patients.)
Randomized controlled trials (RCTs) and systematic reviews must be internally validated. (Ie, the design
and conduct of RCTs must keep the possibility of bias to a minimum. To be
clinically useful, however, the results must be relevant to a definable group
of patients in a particular clinical setting.
This is termed external validity,
applicability, or generalizability. How should the results best be used in
practice? There are no accepted
guidelines on how external validity of RCTs should be assessed.
The most frequent criticism by clinicians
of RCTs, systematic reviews, and guidelines is the lack of external validity.
This explains the widespread underuse in routine practice of treatments that
are beneficial in trials and recommended by guidelines. The external validity
of an RTC depends on whether the outcomes are clinically relevant. Indeed, RCTs often do lack external validity.
The aim of RCTs is not to measure the benefit that will be derived from
treatment in clinical practice. Assessment of external validity requires
clinical rather than statistical expertise.
RCTs should be designed and reported in a
way that allows clinicians to judge to whom they can reasonably be applied.
The response to, and compliance with,
treatment can be influenced strongly by the doctor-patient relationship,
placebo effects, and patient preferences. The importance of these factors
outside of trials should not be underestimated. Note the popularity of
“alternative” therapies in which such factors are the only active ingredients.
RCTs and systematic reviews cannot be
expected to produce results that are directly relevant to all patients in all
settings. To be externally valid they should at least be designed and reported
in a way that allows patients and clinicians to judge to whom they can
reasonably be applied.
Lancet January 1,
2005; 365: 82-93Commentary by Peter M Rothwell, Radcliffe Infirmary, Oxford, UK
====================================================================
Is the Evidence “Generalizable” to my Patient?
1-3 EVIDENCE-BASED PRACTICE AND THE INDIVIDUAL
(This essay
comments on the 5-part series in the Lancet which concerns applying trial data
to individual patients.)
Focus on the individual is central to the
development of evidence-based practice.
It can be tempting to consider the
application of trial data in rigid terms. “Could my patient have been
randomized in this trial?” If so, the results of the trial may be applicable;
if not they may not be applicable.
A more matter-of-fact approach to clinical
complexity may be to ask—Is my patient so different from those in the trial
that its results cannot help me make my treatment decision? The more family
practitioners feel they know their patient, the less likely they are to apply
external evidence to guide management. How can the clinician be guided through
this dilemma and be assisted in applying personal experience, patient’s
preferences, local resources, and valid evidence to make the best
recommendations for care?
Trialists and journals should embrace
clinically significant outcomes that are meaningful to patients, their
attendants, and care organizations. Disingenuous surrogate markers and
misleading composite outcomes may create good advertising material, but should
not obscure data and hinder genuine patient-centered care.
Let us not neglect the central role of
individual patients as decision-makers in their own care. “It is the
responsibility of healthcare workers to communicate objective evidence in a
manner which allows recipients to make an informed choice, and then to respect
that choice.”
“Now and then, clinicians will have to
accept and explain that uncertainty is an inherent facet of the uniqueness of
human nature. Evidence helps to quantify that uncertainty, but cannot remove
it.”
Lancet January 1,
2005; 365: 13-14 Comment by William
Summerskill, The Lancet, London, UK
=====================================================================
If
Confirmed, This Represents An Enormous Public Health Benefit.
1-4
FOLATE INTAKE AND THE RISK OF HYPERTENSION AMONG U.S. WOMEN
Oral folic acid supplementation improves endothelial
function. Folate may have beneficial effects on blood pressure by increasing
nitric oxide synthesis in endothelial cells, and by reducing plasma
homocysteine levels. (Homocysteine by itself can cause endothelial cell
injury.)
This study assessed the association of folate intake
with incident hypertension in 2 large groups of women.
Conclusion:
Higher total folate intake was associated with decreased risk of incident hypertension.
STUDY
1. The Nurses’ Health Study prospectively
followed 2 cohorts of women: 1) over 93 000 younger women (age 27 to 44 at baseline), and 2) over 62 000 older women
(age 43 to 70 at baseline).
2. None had a history of hypertension.
3. A food frequency questionnaire obtained
information on dietary and supplemental folate intake. This allowed calculation
of total folate intake.
4. Main outcome measure = relative risk of
incident self-reported hypertension during 8 years of follow-up related to
folate intake.
RESULTS
1.
Younger women (mean age 36 at baseline):
Identified 7373 incident cases of hypertension (8%)
over 8 years.
Subjects whose daily consumption was at
least 1000 ug of total folate (diet + supplement) had a relative risk (RR) of developing hypertension of 0.54
compared with women who consumed less than 200 ug daily.
Absolute risk reduction of incident hypertension was about
8 cases per 1000 person-years.
2.
Older women (mean age 55 at baseline):
Identified 12347 incident cases of hypertension (19%)
over 8 years.
Relative risk of hypertension (1000 ug folate daily vs less than 200 ug) = 0.82.
Absolute risk reduction of incident hypertension was
about 6 per 1000 person-years.
3. The recommended folate intake in the
USA is 400 ug per day. When those taking 1000 ug or more per day were compared
with those taking up to 400 ug, subjects taking 1000 ug had a significant
reduction in risk of incident hypertension. (RR = 0.60 for younger women and
0.87 for older). (Ie, there may be
benefit in raising daily intake above the RDA of 400 ug. RTJ)
4. In the group of women whose dietary
folate was low (less than 200 ug), those who took supplements to raise intake
to 800 ug had a RR of hypertension of 0.55 (in younger women) and 0.61 (in
older women).
5. In the women who took no supplements
and whose daily food folate was at least 400 ug, the RR of developing
hypertension was 0.87 compared with those ingesting 200 ug or less.
(Ie, the present
food fortification program may be beneficial. RTJ)
DISCUSSION
1. After controlling for a large number of
covariates, this prospective study found that higher folate intake was
significantly associated with a reduced risk of developing hypertension over an
8-year period.
2. The inverse relationship was robust
even after changing the upper limit of the reference group from 200 ug to 400
ug. (Ie, the present recommended daily
allowance may be too low to obtain maximum benefits. RTJ)
3. The most significant relationship was associated with supplemental (not dietary) folate intake. (Bioavailability of supplemental folate is twice that of food folate.)
4. Younger women achieved the most
benefit. Younger women whose intake was at least 1000 ug experienced 1/3 the
risk of developing hypertension over 8 years. (Ie, start supplementation early. RTJ)
CONCLUSION
1. Higher intake of folate was associated
with a decreased risk of incident hypertension, especially in younger women.
Supplemental folate was independently beneficial.
JAMA January 19, 2005; 293: 320-29 Original investigation, first author John P
Forman, Harvard Medical School, Boston Mass.
==============================================================================
Aromatase Inhibitor Safer and More Effective Than
Tamoxifen
1-5 RESULTS OF THE ATAC (ARMIDEX, TAMOXIFEN,
ALONE OR IN COMBINATION) TRIAL OF 5 YEARS’ ADJUVANT TREATMENT FOR BREAST CANCER
The standard adjuvant endocrine treatment
for post-menopausal women with hormone-receptor-positive localized breast
cancer (BC) is 5 years of tamoxifen.
Recurrence of BC and adverse effects restrict its usefulness.
This study compared the aromatase
inhibitor anastrozole with tamoxifen over 5 years. (This is a preliminary fast-tracked report.)
Conclusion: Compared with tamoxifen, anastrozole was associated with greater
benefits and fewer adverse effects.
STUDY
1. Double-blind, randomized trial compared
tamoxifen alone with anastrozole alone. (It
also presented a subset of tamoxifen + anastrozole vs tamoxifen alone. I omit this data because there was no advantage
over anastrozol alone.)
2. Randomized over 6000 women to either 1)
tamoxifen or 2) anastrozole. All were postmenopausal. All had localized BC.
3. Followed for a median of 68 months.
RESULTS
1. Anastrozole led to significant
improvements compared with tamoxifen for disease-free survival, and time-to
recurrence, especially in women whose BC was hormone-receptor-positive.
Benefits were also demonstrated in hormone-receptor-negative patients.
2. Benefits were therefore in addition to the risk reduction
previously shown in tamoxifen vs
placebo trials. (Ie, anastrozole vs
placebo would have shown greater absolute benefits compared with tamoxifen vs
placebo)
3. Benefits of anastrozole were seen at
all times after the first year.
4. The incidence of contralateral BC was
substantially reduced by anastrozole as compared with tamoxifen. (This was also
an improvement over the benefit of tamoxifen alone vs placebo as demonstrated
in previous studies.)
5. A slight decrease in death from BC was
present in the anastrozole group. (Not
statistically significant possiblydue to the short period of observation.)
6. Since almost all patients had completed
the scheduled course of 5 years, safety and tolerability can be deemed final:
Withdrawals were significantly fewer in
the anastrozole group (11% vs 14%).
Drug-elated serious adverse events were
also fewer (5% vs 9%)
7. Compared with tamoxifen, anastrozole
was associated with significant reductions in endometrial cancer,
thromboembolic events, ischemic cerebrovascular events, vaginal bleeding, and
hot flushes.
8. Arthralgias and fractures were more
frequent in the anastrozole group. (The
authors suggest concomitant bisphosphonate therapy because of this finding.)
DISCUSSION
1. “This analysis…confirms the efficacy and
tolerability of anastrozole as initial
adjuvant treatment for postmenopausal women with localized breast cancer.”
2. Results of other studies evaluating anastrozole or
exemestane (another aromatase inhibitor) after 2 to 3 years of adjuvant
tamoxifen, suggest it is reasonable to switch patients currently on tamoxifen
to an aromatase inhibitor. It is not appropriate to wait until after a 5-year
period of treatment with tamoxifen. The most effective and well-tolerated
therapy should be offered at the earliest opportunity.
CONCLUSION
Anastrozole should be considered the
preferred initial adjuvant endocrine therapy for post-menopausal women with
hormone-receptor positive localized BC.
Lancet January 1,
2005; 365: 60-62 “Research Letter”,
peer-reviewed, fast-tracked for early publication by the ATAC Trialists’ Group,
Anthony Howell, chairman of the steering committee, Christie Hospital,
Manchester UK
=========================================================================
Proposing
an ABCDE Memory Device to Simplify Adherence to Guidelines
1-6 A SIMPLIFIED APPROACH TO THE MANAGEMENT OF
NON-ST-SEGMENT ELEVATION ACUTE CORONARY SYNDROMES
Implementation of guidelines for treatment of
non-ST-elevation acute coronary syndromes (NSTE-ACS)
remains suboptimal. This article attempts to simplify guidelines by proposing a
modification of the “ABC” approach that incorporates risk reduction, lifestyle
changes, and medical therapies that can be easily used by primary care
clinicians.
Many physicians consider guidelines too lengthy and
complex.
Conclusion: An
“ABCDE” approach is presented based on a systematic-review evidence of
efficacy.
STUDY
1. NSTE-ACS is a comprehensive term that
combines two entities: 1) unstable angina and 2) non-ST-elevation myocardial
infarction. It is part of a continuum of disease processes resulting from
reduced coronary blood flow due to plaque disruption and subsequent thrombus
formation.
2. It should be differentiated from
ST-segment-elevation myocardial infarction (STE-MI). The treatment differs. STE-MI is typically characterized
by complete thrombotic occlusion and is generally treated with immediate
reperfusion therapy. NSTE-ACS usually results from a transiently or nearly
occluded vessel and may or may not require revascularization. Anti-ischemic and
anti-thrombotic therapy is recommended for all with NSTE-ACS
3. The study assembled a comprehensive
plan through an “ABCDE” approach. The intention was to provide an overview of
therapies and lifestyle changes that are clinically useful for patients with
NSTE-ACS.
RESULTS
1.
Elements of the plan:
A Antiplatelet;
Anticoagulation; ACE inhibitors; Angiotensin II blockers.
B Beta-blockers; Blood pressure control
C Cholesterol
management; Cigarette cessation
D Diet; Diabetes management
E Exercise.
2.
Antiplatelet:
Aspirin given immediately and continued indefinitely
“Most patients with NSTE-ACS who are at
low bleeding risk should have clopidogrel (Plavix)
added to aspirin at hospitalization with continuation for up to 12 months.”
3.
Anticoagulation:
Patients managed with an early conservative strategy
should receive anticoagulation.
Low-molecular-weight heparin (LMWH; specifically
enoxaparin) should be preferred.
4.
ACE-inhibition:
All with left ventricular systolic
dysfunction, heart failure, hypertension, or other high-risk factors. No preferred agent
5.
Angiotensin II blockers:
All who are intolerant to ACE-inhibitors.
6.
Beta-blockade:
All patients. No preferred agent.
7.
BP control:
ACE-inhibitors and beta-blockers first line drugs.
Goal < 130/85; lower if diabetes or renal disease.
8.
Cholesterol treatment:
All patients.
Start immediately with high-dose statin. Goal LDL-c under 70.
9.
Cigarette cessation:
Long-term behavioral support. Buproprion (Wellbutrin; Zyban; generic) + nicotine replacement
10.
Diet:
Weight reduction. Modification to control lipids. Salt
restriction.
11.
Diabetes management:
HbA1c under 7% at a minimum.
12.
Exercise:
Aerobic and weight bearing 4-5 times
weekly for > 30 minutes, preferably within a cardiac rehabilitation program.
CONCLUSION
This practical approach to NSTE-ACS allows physicians
to more effectively create disease management protocols, define roles and
responsibilities for different medical personnel, and ensure implementation of
evidence-based short- and long-term medical and risk-reducing strategies.
JAMA January 19, 2005; 293: 349-57 “Clinical Review”. First author Ty J
Gluckman, Johns Hopkins Hospital, Baltimore MD
=============================================================================
Adherence
was Poor. Those Who Adhered for One
Year Lost Weight
1-7
COMPARISON OF THE ATKINS, ORNISH, WEIGHT WATCHERS, AND ZONE DIETS FOR
WEIGHT LOSS AND HEART DISEASE RISK REDUCTION
Popular diets are becoming more controversial. More
than 1000 diet books are now available. Many popular diets depart substantially
from mainstream medical advice.
Some (eg, Weight Watchers) are based on long-standing
medical advice which recommends restriction of portion sizes and calories. The
Atkins diet minimizes carbohydrate intake. Ornish recommends fat restriction.
Zone recommends modulation of macronutrients and glycemic load.
This study assessed adherence rates and effectiveness
of the 4 diets in producing weight loss and reducing cardiac risk factors.
Conclusion:
Over 1 year, overall adherence rates were low for all 4 diets. For
adherents, all diets resulted in weight loss and reduction in cardiovascular
risk factors.
STUDY
1. Recruited and followed 160 subjects (mean age 49) to an intention-to-treat analysis. Almost all were obese. (Mean BMI 35)
2.
Randomized equally to each of the 4 diets:
Atkins Low
carbohydrate—20 g carbohydrate daily
Zone High
protein, low glycemic load
Weight Watchers Balanced diet—total daily ”points” in a
range determined by current weight
(Aimed for 24 to 32 points daily.)
Ornish Low
fat, vegetarian diet containing 10% of calories as fat.
3.
Subjects received diet-specific instruction 4 times during the first 2 months.
Thereafter they were on their own.
4.
The study addressed only the dietary component, not any other specific
components of the program.
5.
Followed for 1 year.
RESULTS
1. About half of the subjects in each
group failed to complete the 1-year course. The most common reasons were “too
hard to follow” and “not yielding enough weight loss”. Adherence was
particularly low for Atkins and Ornish.
2. Overall, the mean weight loss at one year varied from 2.1 kg (Atkins) to 4.9 kg
(Weight Watchers) [This assumed no change from baseline among those who
discontinued.]
3. Completers lost more at 1 year. (-3. 9
kg for Atkins and -6.6 kg for Ornish)
4. Each diet significantly reduced
LDL/HDL-cholesterol ratio by about 10%. The Atkins diet did not lower
LDL-cholesterol significantly. The Ornish diet did not increase the
HDL-cholesterol. No diet significantly altered triglyceride levels.
5. No significant effect on glucose levels
or on BP.
6. Reductions of total cholesterol, C-reactive protein, and insulin levels were significantly associated with the degree of weight loss.
DISCUSSION
1. A variety of popular diets can reduce
weight and several cardiac risk factors under realistic conditions. But only about half of the subjects in this
study sustained a high adherence level.
2. The authors suggest that one way to
improve dietary adherence in clinical practice may be to use a broad spectrum
of diet options to better match individual patient’s food preferences,
lifestyles, and cardiovascular risk factors. They suspect adherence would have
been better if subjects had been given the option to choose their diet.
3. Low carbohydrate diet was no better
than other diets.
4. In the long run, sustained adherence rather than the diet type was the key predictor of weight loss and risk reduction.
CONCLUSION
Poor adherence rates were evident for all 4 diets. In
adherent subjects all diets resulted in modest weight loss and reduction in
cardiovascular risk factors.
JAMA January 5, 2005; 293: 43-53 Original investigation, first author Michael
L Dansinger, Tufts New England Medical Center, Boston, Mass.
An editorial in this issue of JAMA by Robert Eckel,
University of Denver, Colo. comments:
There is insufficient knowledge about mechanisms for
recidivism in obesity. One factor may be that, once weight loss of more than
several kilograms occurs, a substantial step-up in the amount of physical
activity is required to maintain the loss and to continue losing. In addition,
continuing and more conscientious attention to the weight-loss program is
required.
What is truly needed now is evidence that weight loss
by diet (and exercise and behavioral modification) along with risk factor
improvement can be achieved and maintained for 10 years, and hard outcomes such
as risks of death, myocardial infarction, cancer, and stroke can be improved.
Meanwhile, the best evidence points toward a modest
persistent restriction in calories with higher intake of fruits, vegetable,
fish, and whole grains along with modest increase in physical activity.
=============================================================================
A Particularly Ominous Public Health Issue
1-8 FAST-FOOD HABITS, WEIGHT GAIN, AND INSULIN
RESISTANCE
About two out of every three US adults
were overweight or obese in the year 2000. Rates were even higher in minority
groups.
The associated rising prevalence of
glucose intolerance and type 2 diabetes is a particularly ominous public health
issue.
One potentially important associated
dietary factor is consumption of fast-foods (defined as convenience food
purchased in self-service or carry out eating places.) (Name
your own. RTJ) Consumption of fast food by children has risen from 2% of
total energy intake in 1970 to 10% in the 1990s. Several factors inherent to
fast food could promote a positive energy balance: excessive portion size (single meals often approach individual
daily energy requirements); palatability; emphasis on primordial taste
preferences for sugar, salt, and fat; high energy density; and high glycemic
load.
Trans fat and glycemic load might also
enhance risk of type 2 diabetes through energy-independent mechanisms.
This study investigated the association
between fast-food habits and changes in body weight and insulin resistance over
a 15-year period.
Conclusion: Fast-food consumption was positively associated with weight gain and
insulin resistance.
STUDY
1. Multicenter prospective study included
over 3000 young adults (age 18-30; mean = 25 at baseline) in 1985-86.
2. Questionnaires assessed the frequency
of fast-food restaurant visits at baseline and follow-up.
3. Correlated fast-food visits with
changes in weight and insulin resistance. Insulin resistance was measured by a
product of glucose concentration (mmol/L) times insulin levels (mU/L).
4. Also assessed total physical activity
and TV watching.
5. Follow-up = 15 years.
RESULTS
1. At baseline:
Weekly visits to fast-food
restaurants = 2.4 for men and 1.7 for
women. Younger subjects made more visits.
There was a direct and independent
monotonic association between fast-food frequency and weight and insulin
resistance. Subjects who visited three times a week had a mean weight about 2
kg higher than those who visited less than once a week.
2. Over 15 years:
Fast-food visits increased over 15 years
in those with high frequency of visits at baseline.
Frequent visitors gained more weight
compared with those who visited less than once a week.
Insulin resistance was directly associated
with visits of 3 times a week.
Compared with subjects whose fast-food
visits were less than once a week, those who visited over 2 times weekly gained
an extra 4.5 kg and had a 104% greater increase in insulin resistance.
3. This association was especially strong among the
least physically active subjects.
DISCUSSION
1. At baseline, there was a direct and
independent monotonic association between fast-food frequency and weight and
insulin resistance.
2. Over 15 years, in young adults living
in the USA, there were strong positive associations between frequency of visits
to fast-food restaurants and increases in bodyweight and insulin resistance,
two major risk factors for type 2 diabetes.
3. The large portion size is the most
obvious aspect of fast food that might lead to weight gain.
4. Fast food also contains large amounts
of partially hydrogenated oils which are associated with insulin resistance.
They also contain large amounts of highly refined starchy food and added sugar,
carbohydrates that have a high glycemic index.
CONCLUSION
Fast-food habits have strong, positive and
independent association with weight gain and insulin resistance in young
adults. This suggests an increased risk of type 2 diabetes and obesity.
Lancet January 1,
2005; 365: 36-42 Original
investigation by the Coronary Artery Risk Development in Young Adults (CARDIA)
study, first author Mark A Pereira, University of Minnesota, Minneapolis.
===========================================================================
Stool Antigen Test is Recommended
1-9 TEST AND TREAT FOR DYSPEPSIA: But Which Test?
The National Institute for Clinical
Excellence (NICE) of the UK
recommends that patients with persistent
or recurrent uncomplicated dyspepsia
should have a non-invasive test for Helicobacter
pylori. If the test is positive
they should receive eradication (triple antibiotic) therapy.
With a policy requiring non-invasive
testing and treatment we need the use of an accurate test so that the patients
receive the correct treatment. The urea breath test and serology were the first
non-invasive tests available. The specificity and sensitivity of the breath
test are high, but the test is time consuming and requires two breath samples
taken 20 minutes apart. Serology is
less accurate.
Now the stool antigen test is available.
It detects H pylori antigens passed
in feces. A commercial monoclonal antibody test is available. It is reported to
be as accurate as the urea breath rest. It can be introduced with ease into
routine laboratory practice. It is less expensive and less time consuming than
the urea breath test. It is useful also
in confirming eradication of the infection.
In developed countries, where typically
25% of dyspeptic patients are H pylori
positive, only 3% will be false positive on the stool antigen test and receive
unnecessary antibiotics. (The serologic test is associated with many more false
positives.)
“We need to have an easy, accurate
diagnostic test and the stool antigen test is just that.”
BMJ January 15, 2005;
330: 105-06 Editorial, first author
Cliodna McNulty, Gloucestershire Royal Hospital, Gloucester, UK
The editorial cites a helpful web site for
guidelines for dyspepsia: www.sign.ac.uk/pdf. This refreshed my memory
regarding some clinical points for dyspepsia:
Definition: Dyspepsia is a symptom, not a disease—pain or discomfort centered
in the upper abdomen. (Ie, in or around the midline.) Pain in the right or left
hypochondrium is not considered. “Discomfort” refers to subjective symptoms the
patient does not consider painful: fullness, early satiety, belching, nausea,
retching, and/or vomiting.
Functional dyspepsia is defined in patients in whom no organic
disease can be demonstrated.
Uncomplicated
dyspepsia refers to dyspepsia not
accompanied by alarm features or NSAID use.
Management for patients under age 55 who
have disturbing, persistent, and recurring functional dyspepsia:
The strategy of “test and treat” is
recommended - ie, treat without endoscopy. If H pylori positive by a non-invasive test, treat with a course of
antibiotics.
Advantages:
Will treat an unsuspected peptic ulcer. And reduce
risk of subsequent ulcer disease.
Will reduce or eliminate symptoms in some
patients (~ 10%). Eradication will remove symptoms in only a small percentage
of patients with dyspepsia.
Remove a risk factor for gastric cancer.
Other therapy:
Diet. No evidence in favor of special diets. Recommend
the usual healthy, balanced diet.
Stop smoking. Take only moderate amounts of caffeine
and alcohol.
Drug therapy. There is a substantial
placebo response. A trial of acid suppression may be considered. Response is
variable. For antacids and prokinetics there is no evidence of efficacy.
Inform patients:
When no disease or abnormality has been found.
Functional dyspepsia is not by itself serious,
although the symptoms are real and may be disturbing.
It is not caused by gastric hypersecretion of acid.
Acid secretion is usually normal.
It is not caused by food allergy or
sensitivity. No specific diet or restriction is required. Nevertheless, avoid
foods you that upset you.
These
applications differ for older patients. Look more carefully for organic
disease.
I
would not dissuade use of antacids, acid-suppressing drugs or changes in food
intake according to individual patients’ judgment.
==============================================================================
Physician’s Power Can be Enhanced, Diminished, Used
Well or Ill, but It Cannot be Disowned.
1-10 CONSENT OR OBEDIENCE? Power and Authority in Medicine
This essay considers the role of inappropriate obedience as a source of abuse in the teaching
hospital and the effect of obedience on patients’ autonomy and consent.
Patients provide consent not only about
big issues, but, in the course of an illness, sick patients consent innumerable
times to interventions that they would rather not undergo.
Serious illness is marked by losses of
normal function in many dimensions of existence, including the ability to
reason and to act (without which “autonomy” loses meaning). Sick patients do
not reason their way to decisions based on their appraisals of the relevant
information, but because an authority helps them to decide.
A power comes from the hospital setting
and the trappings of medical authority. “Such power can be enhanced,
diminished, used well or ill, but it cannot be disowned.”
Bearing in mind the effect of sickness on
function, we should accept the propensity of sick patients to seek our
approbation, celebrate our expertise, and acknowledge the legitimacy of our
authority by doing as they think we wish. These tendencies present us with
difficult responsibilities.
“The biggest thief of autonomy is
sickness.”
I
enjoyed this thoughtful essay.
We
live in a world in which authority leads multitudes to follow blindly and
commit unspeakable atrocities. The
resistance of one man is a badge of courage.
I
believe physicians apply their power to some extent in every patient encounter.
Physicians, wield your power carefully and always with the aim of benefit to
the patients.
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The USPSTF Now Recommends One-Time Screening in Select
Subsets of Men
1-11 SCREENING FOR ABDOMINAL ANEURYSM
The U.S. Preventive Services Task Force (USPSTF) now recommends one-time
ultrasonographic screening for abdominal aortic aneurysm (AAA) for men ages 65 to 75 who presently smoke or who have smoked
in the past.
The task force found good evidence that
screening and surgical repair of large AAAs ( 5.5 cm an over) leads to
decreased AAA-specific mortality.
One-time screening is sufficient.
The task force makes no recommendation for
or against screening men who have never smoked. It recommends against routine screening for women. In
general, women and men under age 65 and adults who have never smoked are at low
risk. The increased presence of co-morbid conditions for people over age 75
decreases the likelihood that they will benefit from screening.
There is only a modest association between
risk factors for atherosclerotic disease and AAA.
In men age 65-75 who have smoked or
continue to smoke, an estimated 500 would need-to-be-screened to prevent one
AAA-related death over the next 5 years.
Clinical judgment guides screening in
other individuals.
For AAAs 4.0 to 5.4 cm, periodic
surveillance offers comparable mortality benefits compared with elective
surgery, with the benefit of fewer operations. Most authorities also recommend
periodic surveillance for those with AAAs 3.0 to 3.9 cm.
Annals Int
Med February 1, 2005; 142: 198-202 “Clinical Guidelines” by the U.S. Preventive Services Task Force.
www.preventiveservices.ahrq.gov
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One or Two Drinks a Day May Decrease the Risk of
Cognitive Decline.
1-12 EFFECTS OF MODERATE ALCOHOL CONSUMPTION ON
COGNITIVE FUNCTION IN WOMEN.
Habitual excess alcohol consumption
impairs the brain.
This study asks—What is the effect of moderate consumption of alcohol on
cognition? A benefit is plausible considering the strong link between moderate
alcohol and decreased risk of cardiovascular disease. Cognitive impairment and
cardiovascular disease share common risk factors.
Moderate alcohol consumption has been
related to a decreased risk of both vascular and non-vascular dementia.
Conclusion: In women, one or two drinks a day may decrease the risk of
cognitive decline.
STUDY
1. The Nurses’ Health Study evaluated
cognitive function in over 12 000 women age 70-81 (mean = 74) at baseline.
Followed over 11 000 for two years. Participants were community dwellers without
a history of stroke.
2. Determined the level of alcohol
consumption at baseline.
3. At baseline, calculated mean global
cognitive scores by a cognitive status score based on the Mini-Mental State
Examination and memory tests of immediate and delayed recall.
4. Correlated degree of cognitive
impairment related to level of alcohol consumption.
5. Also calculated the mean decline in
cognitive function over 2 years related to alcohol consumption.
RESULTS
1. Compared with abstainers, moderate
drinkers (less than 15 g alcohol per day; one drink) had better mean cognitive
scores. (Relative risk of impairment = 0.81 based on a global cognitive score.)
2. Also, compared with abstainers,
moderate drinkers (15 to 30 g per day) had a reduced relative risk of cognitive
impairment (although slightly less favorable, with wider confidence intervals).
3. Over a 2-year period, relative risk of
decline in cognition was 0.85 in moderate drinkers compared with abstainers.
4. No significant differences according to
the type of alcoholic beverage consumed.
DISCUSSION
1. “We found that older women who consumed
up to one drink per day had consistently better cognitive performance than
non-drinkers.”
2. Women who drank up to 15 g alcohol per
day (one drink) had a decrease in risk of cognitive impairment of 20% compared
with abstainers. They were also less likely to experience a decline in
cognitive function over a 2-year period.
3. The relationship was similar for all
types of alcohol.
4. Several mechanisms for the benefit have
been proposed. The most plausible relates to the consistently lower rates of
cardiovascular disease among moderate drinkers. This has been attributed to a
higher HDL-cholesterol and reductions in fibrinogen and other thrombotic
factors. This helps preserve brain vasculature.
5. Another study reported that older
persons without cerebrovascular disease who drank moderately had fewer
white-matter infarcts on MRI.
CONCLUSION
In older women consumption of one
alcoholic drink per day did not impair cognitive function, and may actually
decrease risk of cognitive decline.
NEJM January 20, 2005;
352: 245-53 Original investigation,
first author Meir J Stamfer, Harvard Medical School, Boston, Mass.
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Statins Reduce C-Reactive Protein Levels Independently
of LDL-Cholesterol
1-13 STATINS FOR ATHEROSCLEROSIS—Autoimmunity,
Inflammation, and C-reactive Protein.
Inflammation is a notable component of the
atherosclerotic process.
Statin drugs, in addition to inhibiting
synthesis of cholesterol, now appear to directly inhibit inflammation. The list
of disorders for which statins might prove beneficial is growing and now
extends from multiple sclerosis and neurodegenerative disorders to rheumatoid
arthritis and systemic lupus.
Recent studies have revealed the multiple
immunologic actions of statins. The immune modulator interferon gamma is now
generally accepted as directly promoting atherosclerosis. Statins inhibit its
action.
The immunomodulatory effects of statins
apply to cardiovascular disease, in which immune dysregulation is observed.
“Indeed, the inflammatory component of atherosclerosis, characterized by
increased production of interferon-gamma by T cells has led immunologists to
suggest that atherosclerosis should be added to the list of organ-specific
autoimmune diseases.”
Two articles in this issue of NEJM 1,2 confirm that reducing
the inflammatory component of cardiovascular disease with statin therapy improves
clinical outcomes independently of the reduction in cholesterol. Both studies
found that the statin-induced decrease in C-reactive protein (CRP), a marker of inflammation, is only
weakly correlated with changes in lipid levels.
Only by assaying both C-reactive protein
and cholesterol can the full effect of statins be identified.
NEJM January 6, 2005;
352: 73-74 Editorial, first author
Michael R Ehrenstein, University College, London, UK
1 “C-reactive
Protein Levels and Outcomes after Statin Therapy” NEJM January 6, 2005; 352:
20-28
original investigation, first author Paul M Ridker, Harvard Medical
School, Boston Mass
Statins have a remarkable ability to lower
CRP levels. Patients with acute coronary syndromes who achieve low CRP levels
from statin therapy had better clinical outcomes than those with higher levels.
The LDL-c lowering effect of statins and
their effect on lowering CRP are largely independent of each other. Patients
achieving the lowest CRP levels through statin therapy had a higher event-free
survival at all levels of LDL cholesterol.
The authors suggest that CRP should be
monitored when stain therapy is
employed.
2 “Statin
Therapy, LDL-Cholesterol, C-Reactive Protein, and Coronary Artery Disease” NEJM
January 6, 2005; 352: 29-38 Original investigation, first author Steven
E Nissen, Cleveland Clinic Foundation, Cleveland Ohio
This study reports a reduced rate of
progression of coronary atherosclerosis associated with intensive statin
therapy. This was related to reductions in levels of CRP as well as
LDL-cholesterol.
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Development May be Delayed by Good Glycemic Control
and Modification of Cardiovascular Risk Factors.
1-14 VASCULAR RISK FACTORS AND DIABETIC
NEUROPATHY
Diabetic neuropathy (DN) is a common cause of morbidity and death among patient with
diabetes. Other than glycemic control, there are no treatments for DN. Thus,
identifying potentially modifiable risk factors for neuropathy is critical.
The duration and level of hyperglycemia
are important determinants of micro-vascular complications, including DN.
The Diabetes Control and Complications
Trial reported a 60% reduction in DN in the intensively treated group at 5
years. But the incidence still remained substantial. This suggests that DN can
develop despite intensive control of glucose levels. Risk factors other than
glucose are involved. The relative effects of cardiovascular risk factors
(hypertension, dyslipidemia, overweight and obesity, and smoking) are not fully
understood.
This study assessed potentially modifiable
risk factors for development of distal, symmetric DN.
Conclusion: Dyslipidemia, elevated BMI, smoking, and hypertension were associated
with development of DN.
STUDY
1. Prospectively followed over 1100
patients with type 1 diabetes for 7 years. Mean age of subjects was about 30;
mean duration of DM = 13 years. None had DN at baseline.
2. Used a standard protocol for
diagnosis: clinical evaluation,
quantitative sensory testing, and autonomic function tests.
3. Clinical evaluation included symptoms
of “asleep, numbness or “dead feeling” in the feet, prickling sensation in the
feet, deep aching or burning pains in the legs, unusual difficulty in climbing
stairs, difficulty with bladder control, and nocturnal diarrhea.
4. Vibration perception was tested by a
special “biothesiometer”.
5. Autonomic function assessed by
cardiovascular reflex responses. (Eg,
change in heart rate and BP on standing)
6. Neuropathy was diagnosed in patients
with two or more of these factors:
Two or more symptoms
Absence of two or more reflexes of ankle
and knee tendons
Abnormal vibration-perception
threshold. (A common manifestation)
Abnormal autonomic function.
RESULTS
1. Over 7 years, DN developed in 23% of the subjects
who were without DN at baseline.
2. Cumulative incidence was related to higher
glycosylated hemoglobin values and longer duration of diabetes.
3. After adjustment for the preceding, other factors
were significantly associated with cumulative incidence of DN:
Higher levels of LDL-cholesterol
Higher levels of triglycerides
Higher BMI
Hypertension
Smoking
4. Cardiovascular disease at baseline was associated
with double the risk of neuropathy.
DISCUSSION
1. Over 7 years, about ¼ of patients in
their early 30s with type 1 diabetes developed DN.
2. DN more likely developed in those with
longer duration of diabetes.
3. DN more likely developed in patients
with higher HbA1c levels at baseline and in those whose HbA1c rose during the
observation period.
4. Cardiovascular disease presence at
baseline was related to a much higher risk of DN.
5. Cardiovascular risk factors
(hypertension, smoking, obesity, and dyslipidemia) also related to increased
incidence of DN.
6. Mortality in patients with DN is high.
The cause is often cardiovascular.
7. What can be done prospectively to try to prevent
DN?
Control glycemia as best it can be
controlled
Stop smoking
Control BP
Control weight, obtain lower body mass
index
Reduce other cardiovascular risk factors.
(Ie,
essentially standard diabetes management.)
CONCLUSION
Incidence of DN is associated with
potentially modifiable cardiovascular risk factors
NEJM January 27, 2005;
341-50 Origin investigation from
the EURODIAB Prospective Complications Study Group, first author Solomon
Tesfaye, Royal Hallamshire Hospital, Sheffield, UK.
I
enjoyed reviewing the diagnosis of neuropathy.
The mean age at baseline was about 30. Of an
initial cohort, 28% already had
DN. Prospectively, over 7
23% developed
DN. Thus, at age 40, over 50% had DN. I would expect almost all patients with
type 1 diabetes will eventually develop DN.
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Fasting Serum Glucose Level and Diabetes were
Associated with Cancer Risk
1-15
FASTING SERUM GLUCOSE LEVEL AND CANCER RISK IN KOREAN MEN AND WOMEN
Is there any connection between diabetes and cancer?
Some observational studies have suggested there is. This prospective cohort
study investigated this possibility.
Conclusion: In
Korea, elevated serum glucose levels and a diagnosis of diabetes were
independent risk factors for cancer incidence and cancer deaths.
STUDY
1. A ten-year prospective study enrolled
over 829 000 men and over 468 000 women age 30 to 95 at baseline. (Mean = 46;
mean body mass index = 23) All had
received health care from a national insurance company.
2. Their biannual health examinations
included a fasting serum glucose.
3. Obtained records every 2 years for 10
years regarding cancer incidence and cancer deaths.
RESULTS
1. Over 10 years there were 20 556 cancer
deaths in men (2.5% of cohort) and 5907 cancer deaths in women (1.2% of
cohort). And over 37 000 incident
cancers in men ( 4.5% ) and over 16 000 in women (3.4%).
2. After adjusting for smoking and alcohol
use, the stratum with the highest fasting glucose (> 140) had higher death
rates from all cancers compared with the stratum with the lowest level (<
90). Hazard ratio = 1.25
3 Age-adjusted cancer deaths per 100 000
men rose linearly from about 600 in the groups with fasting glucose < 90 to
about 1400 per 100 000 in the group with glucose levels above 140. (Although absolute numbers are low, the linear
relationship depicted on page 196 and 200 is impressive. RTJ). Similar
linear increases were recorded in women, although not as high in absolute
terms. Incidence of cancer was similar to mortality.
4. The association was strongest for pancreatic cancer. (Hazard ratio = 2 comparing the highest glucose stratum with the lowest.)
5. Significant associations were also
found in other cancers (esophagus, colo-rectal, liver, cervix).
6. For persons with a diagnosis of
diabetes, or a fasting blood glucose over 125, risks for incidence and
mortality from cancer were elevated compared with those without diabetes.
DISCUSSION
1. In Korea, the frequency of obesity is
much lower than in the USA. The average BMI of subjects in this study was 23.
Only ¼ of these subjects had a BMI over 25.
2.”We have shown that fasting serum glucose level and diabetes are associated with cancer risk in a population far leaner than the Western populations.”
3. The authors suggest that the mechanism
of increased cancer risk is a consequences of hyperinsulinism.
CONCLUSION
In Korea, elevated fasting glucose and a diagnosis of
diabetes were independent risk factors for cancer incidence and cancer death.
Risk increased linearly as serum glucose rose.
JAMA January 12, 2005; 293: 194-202 Original investigation, first author Sun Ha
Jee, Yousei University, Seoul, Korea
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