PRACTICAL POINTERS
FOR
PRIMARY CARE
ABSTRACTED MONTHLY FROM THE JOURNALS
JULY 2005
POST-MENOPAUSAL WOMEN EXPERIENCE
DISTURBING SYMPTOMS AFTER DISCONTINUING USE OF HRT
WHITE-COAT HYPERTENSION PREDICTS
DEVELOPMENT OF SUSTAINED HYPERTENSION
INDIVIDUAL HIGH-DOSE
VITAMINS—USEFUL OR TOXIC?
A CRITIQUE OF PROSTATE-SPECIFIC
ANTIGEN HOW USEFUL IS
IT?
TREATMENT OF MENOPAUSAL SYMPTOMS: AN
OVERVIEW
WHY IS RIGHT-BRAIN STROKE
UNDERDIAGNOSED?
CONGESTIVE HEART FAILURE MAY BE RELATED
TO INSULIN RESISTANCE.
ECHINACEA ANGUSTIFOLIA NOT
EFFECTIVE FOR EXPERIMENTAL RHINOVIRUS INFECTIONS
COFFEE CONSUMPTION MAY DECREASE RISK
OF TYPE 2 DIABETES
JAMA, NEJM, BMJ, LANCET PUBLISHED
BY PRACTICAL POINTERS, INC.
ARCHIVES INTERNAL MEDICINE EDITED BY RICHARD T. JAMES JR. MD
ANNALS INTERNAL MEDICINE
[email protected]
DAVIDSON
NC 28036 USA
www.practicalpointers.org
This document is divided into two parts:
1) The Highlights
section contains brief comments patterned after the “abstract”
placed on the first page of many studies reported in journals. Highlights
condenses the content of studies, and allows a quick review of pertinent points
of each article.
The Editorial Comments are the editor’s assessments of the
clinical practicality of articles based on his long-term review of the current
literature and his 20-year publication of Practical
Pointers.
2) The main Abstracts section is designed as a reference. It presents
structured summaries of the content of articles in much more detail.
An Index containing all the Highlights is published twice a year. In
an evening or two, the reader can refresh memory of the entire content of practical
points abstracted from 6 major journals over the 6-month period.
I hope you will find Practical Pointers interesting and
helpful. The complete content of all issues for the past 5 years can be
accessed at www.practicalpointers.org
Richard T. James Jr, M.D.
Editor/Publisher.
HIGHLIGHTS AND EDITORIAL COMMENTS
JULY 2005
Antibiotic Therapy Shortened The Time
To Resolution Of Symptoms.
A sizable group of women with urinary
symptoms who subsequently have UTI established by culture are dipstick
negative.
This pragmatic trial (as in primary
care practice) compared the effectiveness of antibiotic treatment vs placebo in
women with symptoms of UTI who had a negative dipstick.
Double-blind placebo-controlled study
followed 59 women presenting to
primary care with a history of
dysuria and frequency. All had a negative dipstick for both leukocytes and
nitrites.
All were treated with: 1)
Trimethoprim 300 mg daily for 3 days, or 2) placebo.
The median time to resolution of dysuria: Trimethoprim—3 days;
placebo—5 days.
Ongoing symptoms At 3
days At
7 days
Trimethoprim 24% 10%
Placebo 74% 41%
(Number needed to treat with
trimethoprim to benefit one patient = 4.)
Only 5 women (of 59) had
microbiological evidence of bacterial infection when standard criteria were
used—a pure growth of 100 000 organisms per mL. Three were in the
treatment group; 2 in the placebo group.
“These results indicate a
bacterial or other infectious cause for the symptoms that was missed by
dipstick testing and standard testing [by
culture] in a diagnostic laboratory.”
The resolution of symptoms that
generally accompany infection would provide some support for an atypical or
occult cause, implying that these women do not have “urethral
syndrome”, a diagnosis of exclusion.
A past history of UTI increases the
risk of subsequent infection. Ninety % of the women in the study reported a
history of similar symptoms.
Admittedly, this is a small trial. Confirmation with a larger number of
subjects would be more convincing. Nevertheless, I believe it has clinical
validity.
Many primary care clinicians treat symptoms of UTI empirically with
antibiotics, rather than wait for bacterial confirmation. This would apply
particularly to patients who have had a history of repeated UTI. Indeed, I
believe some clinicians will prescribe an antibiotic to be reserved at home for
patients to take at the onset of symptoms.
Many Elderly Women Experience
Recurrence Of Symptoms
7-2 SYMPTOM EXPERIENCE AFTER
DISCONTINUING USE OF ESTROGEN PLUS PROGESTIN
The publication of the Women Health
Initiative (WHI) Trial led to a change
in the clinical use of combined estrogen + progestin (E + P) in symptomatic post-menopausal women. Previous
observational studies suggested a significant protective effect against
cardiovascular disease. The WHI, a randomized, placebo-controlled trial, not
only disproved any protective effect, but reported a slight increase in risks.
The present study, an extension of
the WHI, determined the frequency of recurrence of symptoms after discontinuing
E + P.
Over half of the women (now mean age
69) who had been taking CEE + MPA for 5 years reported recurrence of at least
one moderate or severe symptom 8 to 12 months after discontinuing use.
Symptoms also recurred in women who
had been taking placebo although to a lesser extent than women who had taken active
hormones.
This study pointed out the high rate of recurrence of menopausal symptoms
after discontinuation of both E + P and placebo—years after the
menopause. Clinicians then must
decide how to help patients with more severe symptoms. Women with severe
recurring vasomotor symptoms after discontinuing active hormone therapy may be
informed about the risk/benefit ratio and asked to express their personal
preference. Judicious use of HRT at
low doses for a limited time is reasonable. I would avoid use in patients with risk
factors such as smoking, history of CVD, dyslipidemia, hypertension, and
diabetes. Life-style changes may help these patients.
Note that the mean baseline age of subjects was 63 at the beginning of
the WHI study. Many had a history
of smoking, diabetes, hypertension, dyslipidemia, and cardiovascular disease.
(Ie, they represented a cross section of women in this age group.) Risks of HRT
would be much lower in women who start at a younger age, and in women who had
none of the other risk factors. Risks are also much less in patients who take
only estrogen.
Following publication of the WHI trial, the media proclaimed that
hormones were dangerous. The study led many clinicians to advise women to
discontinue HRT. The risks of E + P were exaggerated by patients and physicians
alike. I believe that the risk of serious adverse events from aspirin and
NSAIDs in a comparable group of 10 000 women is greater.
“Not A Totally Benign
Condition.”
7-3 WHITE-COAT HYPERTENSION AS A RISK
FACTOR OF THE DEVELOPMENT OF HOME HYPERTENSION
White-coat hypertension (WCHT) is characterized by an elevated
BP in medical settings, and a normal BP when self-recorded at home, or
determined by ambulatory recorders.
Sustained hypertension is the
presence of an elevated BP regardless of the setting.
In this study, WCHT was defined as
home BP < 135/85; and office BP > 140/90). Sustained normotension was
defined as home BP < 135/85 and office BP < 140/90.
During the 8-year follow-up, 47% of
the WCHT group progressed to home hypertension, vs 22% of the sustained
normotension group. (Odds ratio= 2.9)
WCHT was a significant predictor of
the development of sustained home hypertension, independent of other
confounding factors and baseline home BP levels. “WCHT is not a totally
benign condition.”
This begs the questions: What
should clinicians do about patients with WCHT? What can be done?
Patients with WCHT should be followed more closely. They should be
treated judiciously, especially with lifestyle interventions, to lower all
cardiovascular risk factors.
I believe home BP determinations are essential in primary care practice.
This will lead to both an increase and a decrease in prescription of
anti-hypertension drugs. The Japanese are well ahead of us in this respect.
Use Of High Doses Of Single Nutrients
To Prevent Disease Has Been Disappointing
7-4 ESSENTIAL NUTRIENTS: FOOD OR SUPPLEMENTS. Where Should The Emphasis Be?
In the
However, instead of focusing on
dietary patterns, most intervention trials have used high doses of single
nutrients in an attempt to prevent disease. These results for the most part
have been disappointing.
The American Heart Association now
concludes that…“There is currently no basis for recommending that
patients take vitamin C or E supplements or other antioxidants for the express
purpose of preventing or treating coronary artery disese”.
High dose beta-carotene does not
reduce risk of lung cancer in smokers.
A recent meta-analysis of vitamin E supplements
suggested that doses greater than 400 IU daily (10 times RDA) increased all-cause mortality.
Recent studies have reported that
folic acid, B12, and B6 given to patients who had experienced a non-disabling
stroke had no significant benefit on vascular outcomes.
Conclusion: “There are insufficient data to
justify an alteration in public health policy from one that emphasizes food and
diet to one that emphasizes nutrient supplements.”
The vitamin E bubble has burst with a loud bang. High doses do not reduce
risk of CHD or cancer. Indeed, they may slightly increase risk of congestive
heart failure. Vitamin E does not reduce risk of progression of mild cognitive
impairment to Alzheimer’s
disease (See Practical Pointers June 2005 [6-10])
It is estimated that an astounding 10% of Americans use high dose vitamin
E (400 IU and higher).
I do not believe the authors of the article were talking about the daily
use of supplements containing the RDAs of vitamins and minerals. I do not
believe the authors infer that supplements which mimic daily requirements are
harmful. Many of the individual components will be unnecessary, but I do not
believe they are harmful.
There Is No Cutpoint Of PSA With
Simultaneous High Sensitivity And High Specificity
7-5 OPERATING CHARACTERISTICS OF
PROSTATE-SPECIFIC ANTIGEN
PSA screening has become
controversial. No studies have proven that it leads to a reduction in mortality
from prostate cancer (PC). After 2
decades of screening, mortality from PC has decreased, but it is not known if
this is due to screening or other factors such as treatment efficacy. PC
mortality rates have also declined in countries where PSA screening is
uncommon. In the
A potential explanation for these
observations may be due to the characteristics of PSA measurement as a
screening test. In general, biopsy has not been recommended unless PSA levels
exceed a threshold of 4.0 ng/mL. Other studies have reported that as many as
15% of men with a PSA less than 4.0 have PC, and that 15% of these are high
grade.
This study estimated the relation
between true positive PSA tests and true negative PSA tests over a range of PSA
cutpoints. (Sensitivity vs specificity)
Conclusion: For monitoring healthy men, there is no cutpoint of PSA with simultaneous
high sensitivity and high specificity:
A. Setting the cutpoint high will
result in:
More men with
cancer being missed. (Many men with PC will have a PSA below the high cutpoint
- many false negative tests for PC.)
Fewer men without
cancer being falsely considered positive for cancer and subject to biopsy. (Few
men without PC will have a PSA above the high cutpoint—few false positive
tests for PC.)
B. Setting the cutpoint low will
result in:
More men with
cancer being diagnosed. (Many more men with PC will have a PSA above the low
cutpoint—more true positive tests for PC.)
More men without
cancer being falsely considered positive for cancer and subject to biopsy. (More men without PC will have a PSA
above the low cutpoint—more false positive tests for PC.)
I struggled to present this article in a clear, simple, meaningful
manner. Teasing out sensitivities and specificities is always challenging and
remains confusing at times even to individuals who frequently try to decipher
them
Even now, I remain uncertain at times as to whether I have presented the
data correctly. The best approach is to begin with the classical 2 X 2 chart:
Disease
present Disease
absent
Test positive True
positive (sensitivity) False
positive
Test negative False
negative True
negative (specificity)
I am sure other similar studies would come up with different figures for
cutpoints of sensitivity and specificity
I believe, however, the principle is sound:
1) At low
cutpoints, more men who actually have cancer will be diagnosed. And more men
who do not have cancer will be considered positive for PC.
2) At high cutpoints, fewer men who actually have cancer will
be diagnosed. And fewer men who do not have cancer will be considered positive
for PC.
There is an important corrrelary to these observations. Since more men
screened with PSA do not have PC than men who have PC, PSA screening
will necessarily lead to more false positives and unnecessary investigation as
compared with those who are diagnosed as truly having cancer.
Consider screening a group of 100 000 men. Assume that:
20 % ( n = 20 000) actually have PC, and
80% (n = 80 000) do not have PC.
According to this study:
1) Of the 20 000 with cancer, 20% will have a PSA level 4.1 and above. Thus using 4.1 as a
cutpoint, 4000 will be diagnosed. The great majority will be missed.
2) Of the 80 000 without cancer, 6% will have a PSA level of
4.1 and above. Thus 4800 will be considered falsely to have PC, and be subject
to unneeded biopsy,.
3) If the PSA cutpoint is
set at 2.1, the numbers will be 1) 8000 vs 2) 15 200.
In addition, of the 4000 men with PC, many will have indolent cancers and
many more will have co-morbidity which will cause their deaths before PC might
cause death. Thus, prostatectomy will cause many adverse effects, and
relatively few years of quality-life will be gained. One recent study reported
that men over age 65 with PC did not benefit from prostatectomy as compared
with watchful waiting.
(NEJM May 12,2005; 352: 1977-84 See Practical Pointers May 2005 [5-9] )
7-6 TREATMENT OF MENOPAUSAL SYMPTOMS:
What Shall We Do Now?
Almost all women who reach the
menopause will have symptoms at some point. Almost 80% have hot flashes and
night sweats. About 20% of these find them intolerable. Many will request
treatment. Hot flashes may continue for up to 5 years and, in some individuals,
even longer.
During the past few years, a
substantial number of women have discontinued hormone replacement therapy (HRT)—the most effective therapy,
because of concerns about adverse effects.
This review article (based on a
PubMed search of randomized controlled trials and observational studies)
summarizes data from studies addressing the efficacy, risks, and benefits of
frequently prescribed treatments.
I believe the risks of HRT have been grossly overemphasized. And that
many women who would benefit greatly have been denied treatment because of fear
of adverse effects.
Adverse effects would be essentially absent in women closer to the
menopausal age, in those with no risk factors for cardiovascular disease, in
those who use estrogen alone, and in those using low-dose for a shorter time.
Right-Sided Stroke Or TIA May Be
“Silent”, At Least As Far As Recognition Goes.
7-7 UNDERDIAGNOSIS OF RIGHT-BRAIN
STROKE
A study in the July 30, 2005 issue of
Lancet included over 20 000 patients with stroke or TIA. It reported a striking
difference in the rate of diagnosis of left-sided and right-sided ischemic
events. Symptoms of cerebrovascular events due to anterior (carotid)
circulation deficits differ depending on the hemisphere involved.
The major difference between
hemispheres is the lateralization of cognitive functions, particularly the
left-hemisphere dominance of language. Patients, families, and physicians might
be more likely to recognize a disturbance of speech or language, and apraxia of
the right hand due to left-hemisphere ischemia than more difficult-to-define
cognitive deficits (sudden confusion) or apraxia of the non-dominate left hand
from a corresponding lesion in the right hemisphere. Neglect (defined as a
reduction in awareness of neurological deficits) is associated with
right-hemisphere lesions.
Assuming that right- and left-sided
strokes have equal frequency, the German study suggested that, for every eight patients currently
hospitalized for
anterior-circulation stroke or TIA, one patient with right-sided ischemia will be overlooked.
These patients are unlikely to receive the same standard of management for
secondary prevention.
The authors stress that the
difficulty in recognizing right hemisphere lesions pertains only to minor
stroke or TIA. Major stroke, especially hemorrhagic, is more easily recognized.
I believe this difficulty in recognizing right hemisphere lesions is clinically
important.
The major differences in presentation:
Right hemisphere lesion Left
hemisphere lesion
No aphasia Aphasia
Less awareness of neurological deficits More
awareness of neurological deficits
(Symptoms less readily recognized (Symptoms
more readily recognized.
Neglect in recognizing confusion Less
neglect. Aphasia and apraxia of,
and apraxia of the left hand) the
right hand more readily recognized).
“All Women Should Have A
Measurement Of Bone Mineral Density At The Age Of 65.”
7-8 SCREENING FOR OSTEOPOROSIS
Clinicians should routinely recommend
that patients have an adequate total intake of calcium (1200 mg per day), and
of vitamin D (400 to 800 IU per day), and participate in weight bearing
exercises. Many patients will not lose bone if they have an adequate intake of
calcium and vitamin D and exercise regularly. Nevertheless, the rates of
fractures remain high in individuals who receive these interventions.
It is important to identify high-risk
persons by appropriate screening.
Dual x-ray absorptiometry at the lumbar spine and hip is a
reliable and safe way of assessing fracture risk in postmenopausal women.
Peripheral measurements (eg, ultrasonography) should not be used for decision making.
The 10-year risk of a fragility
fracture in a postmenopausal woman with a T-score at -2.5 standard deviations
or less (compared with a normal young woman), and no other risk factors is more
than 20% at age 65.
“Low bone mass”
(osteopenia) is defined by a T-score between -1.0 and -2.5. About half of
fragility fractures occur in the osteopenic group.
Despite the recommendations for
screening, there is little evidence of its effectiveness in enhancing
prevention and treatment programs.
These screening efforts detect the disease after it has been present for
several years. Treatment is then “catch up”.
If a woman lives long enough, osteoporosis seems inevitable. I await a
study which begins low-dose prophylactic drug therapy (in addition to calcium
and vitamin D) at the time of menopause to prevent the disease or at least to
delay it for decades.
2-Hour PC Blood Glucose—A Risk
Marker For CHF
7-9 INSULIN RESISTANCE AND RISK OF
CONGESTIVE HEART FAILURE
Diabetes and obesity are established
risk factors for congestive heart failure (CHF).
Both are related to insulin resistance. In patients with established CHF,
insulin resistance is associated with more severe disease and a worse
prognosis.
This study explored if insulin
resistance, determined by 2-hour blood glucose on the oral glucose tolerance
test, as well as several other more sophisticated methods, might predict CHF
and provide the link between obesity and CHF.
After adjusting for multiple
established risk factors, an increase of 1 standard deviation in the 2-hour glucose value was associated with
an increased hazard ratio of 1.44 in incidence of CHF. After adjusting for
diabetes, fasting glucose levels were not predictive.
Insulin resistance predicted incidence
of CHF independently of diabetes, truncal and overall obesity, and other risk
factors. The previously described association between obesity and CHF may be
mediated, in part, by insulin resistance.
This sophisticated study presented more detailed methods of measuring
insulin resistance than I have included.
My purpose was to describe a simple risk marker (2-hour p.c. glucose)
which is readily applicable to primary care practice.
I believe the 2-hour glucose should be a standard and important measure
of risk. It is often neglected. The lower, the better. A level of 140 is much too high. A
fasting glucose is less predictive.
7-10 AN EVALUATION OF ECHINACEA ANGUSTIFOLIA IN EXPERIMENTAL
RHINOVIRUS INFECTIONS
This study extracted 3 different
preparations of echinacea.
About 400 volunteers were randomized
to either: 1) prophylaxis with echinacea beginning 7 days before viral
challenge with rhinovirus), or 2) treatment of the experimental infection
(beginning on the day of
challenge), or 3) placebo.
There were no significant effects of
echinacea extracts on severity of symptoms, volume of nasal secretions,
polymorphonuclear leukocytes, interleukin-8 concentrations in nasal-lavage
specimens, or on quantitative virus titers.
These extracts, either alone or in
combination, do not have clinically significant effects on rhinovirus
infection, or on the resultant clinical illness.
This brief abstract does not do justice to the meticulous methods in
which this remarkable study was conducted. To gain the full flavor, read the
article.
Even sophisticated, educated persons will remain convinced of the
efficacy of echinacea for colds.
It is almost impossible to prove a negative. Advocates can cite numerous
reasons why this study does not disprove effectiveness—they can avow that
extracts from different varieties of plant, different parts of the plant,
different preparations, different extraction procedures and manufacturing
processes, location and season of cultivation will be effective. And treating
cold viruses other than rhinovirus will also be effective.
The investigators are correct in
stating that the burden of proof of effectiveness and safety should be placed
on manufacturers of various alternative herbal preparations touted for a myriad
of ills. I believe that the Congress made a serious error when it exempted
these nostrums from surveillance by the FDA. There have been grave
misapplications of these over-the-counter products: false advertising and
egregious promotion, surreptitious addition with standard efficacious
drugs, contamination with dangerous
substances such as arsenic and mercury.
Increasing Consumption Associated
With A Reduced Risk
7-11 COFFEE CONSUMPTION AND RISK OF
TYPE 2 DIABETES: A Systematic
Review
Epidemiological evidence has
suggested that higher coffee consumption may reduce the risk of type 2 diabetes
(DM2). Coffee contains numerous
substances beside caffeine some of which have been shown to have an effect on
glucose metabolism
This systematic review of cohort
studies contained a total of over 199 000 subjects. And 8394 cases of DM2.
Determined daily coffee consumption
Relative risk of DM2: coffee vs no
coffee: RR Confidence
interval
Six or more cups 0.54 0.54-0.78
4 to 5 cups 0.72 0.62-0.83
1 to 3 cups 0.94 0.88-1.01
All levels combined 0.65
This supports a significant inverse
association between coffee consumption and risk of DM2. Participants who drank
4 to 6 cups and over 6 cups daily had a 28% to 35% lower risk of DM2
Mechanisms? The authors speculate that various
components of coffee other than caffeine may have beneficial effects by
increasing insulin sensitivity, reducing hepatic glucose output, inhibiting
glucose absorption, and enhancing insulin secretion. They suggest that caffeine
is not the cause of the inverse association between coffee and DM2. Indeed,
some studies report that caffeine acutely increases
post-load glucose concentrations and lowers
insulin sensitivity.
I included this abstract because the conclusions of the study were
provocative. I do not believe there is any clinical message at present, except
that coffee is not harmful in this respect.
Another interesting connection between coffee and risk of dyslipidemia
concerned the difference between pot-boiled coffee (once common in
ABSTRACTS JULY 2005
Antibiotic Therapy Shortened The Time To Resolution Of
Symptoms.
7-1 RESPONSE TO ANTIBIOTICS OF WOMEN
WITH SYMPTOMS OF URINARY TRACT INFECTION BUT NEGATIVE DIPSTICK URINE TEST
RESULTS.
Urine is commonly tested by dipstick
for the presence of leukocytes and nitrites to predict a subsequent diagnosis
of urinary tract infection (UTI)
confirmed by culture.
In primary care practice, the
presence of leukocytes or nitrites in a turbid urine has a positive predictive
value1 of about 66% of finding a pure growth on subsequent culture. Conversely, a negative dipstick for both
leukocytes and nitrites has a negative predictive value of finding a pure
growth on subsequent culture of 80% to 98%.
One approach to women with symptoms
of uncomplicated UTI who have a positive dipstick is to give antibiotics
empirically.
A sizable group of women with urinary
symptoms who subsequently have UTI established by culture are dipstick
negative.
This pragmatic trial (as in primary
care practice) compared the effectiveness of antibiotic treatment vs placebo in
women with symptoms of UTI who had a negative dipstick.
Conclusion: Antibiotic therapy significantly
shortened the time to resolution of symptoms.
STUDY
1. Double-blind placebo-controlled study followed 59 women
presenting to primary care with a history of dysuria and frequency. All had a
negative dipstick for both leukocytes and nitrites.
The urine was sent for culture.
2. All were treated with: 1) Trimethoprim 300 mg daily for 3
days, or 2) placebo.
3. Main outcome = resolution of symptoms at 3 and 7 days. And
median time to resolution.
RESULTS
1. The median time to resolution of dysuria: Trimethoprim—3 days;
placebo—5 days.
2. Ongoing symptoms At
3 days At
7 days
Trimethoprim 24% 10%
Placebo 74% 41%
(Number needed to treat with
trimethoprim to benefit one patient = 4.)
3. The median duration of
constitutional symptoms (feverishness, shivers) was reduced by 4 days in the
trimethoprim group.
4. What did the cultures
show? Only 5 (of 59) women had
microbiological evidence of bacterial infection when standard criteria were
used—a pure growth of 100 000 organisms per mL. Three were in the
treatment group; 2 in the placebo group.
DISCUSSION
1. “These results
indicate a bacterial or other infectious cause for the symptoms that was missed
by dipstick testing, and standard testing in a diagnostic laboratory.”
2. The resolution of
symptoms that generally accompany infection would provide some support for an
atypical or occult cause, implying that these women do not have “urethral
syndrome”, a diagnosis of exclusion.
3. A past history of UTI
increases the risk of subsequent infection. Ninety % of the women in the study
reported a history of similar symptoms. This high rate is consistent with other
studies of women presenting in primary care with UTI. An alternative, but less
likely hypothesis is that trimethoprim has an effect other than its
bactericidal one in reducing symptoms.
4. Chlamydia trachomatis has been implicated as a cause of UTI and
dysuria. It does not respond to trimethoprim and would not have contributed to
the observed effect.
5. The pragmatic design
(ie, of typical patients seen in primary care) is its strength.
6. Implications for
clinical practice: “If these
finding are confirmed, empirical treatment with antibiotics of (dipstick
positive or dipstick negative) patients presenting in primary care is justified
irrespective of dipstick findings.”
7. An infectious cause
which is not being diagnosed by using the current approach is likely. This
further highlights the tension between relieving symptoms expeditiously with
the desire to minimize unnecessary antibiotic use.
CONCLUSION
Although a negative dipstick test
accurately predicted absence of infection, confirmed by a negative culture, it
did not predict response to antibiotic treatment.
Three days treatment with
trimethoprim significantly reduced dysuria in women whose dipstick test was
negative. This supports empirical use of antibiotics, guided by symptoms.
BMJ July 16, 2005; 331: 143-46 original investigation, first author Dee
Richards,
1
Positive predictive value:
Number of true positive tests divided
by the total number of positive tests
True positive plus sum of true
positive + false positive = 66 divided by (66 + 34) = 66 divided by 100 = 66%.
Many Elderly Women Experience Recurrence Of Symptoms
7-2 SYMPTOM EXPERIENCE AFTER
DISCONTINUING USE OF ESTROGEN PLUS PROGESTIN
The publication of the Women Health
Initiative (WHI) Trial 1 led to a change in the clinical use of
combined estrogen + progestin (E + P)
in symptomatic post-menopausal women. Previous observational studies suggested
a significant protective effect against cardiovascular disease. This
randomized, placebo-controlled trial not only disproved any protective effect,
but reported a slight increase in risks. The trial was discontinued early
because the overall health risks exceeded the benefits.
Women frequently cite relief of
vasomotor symptoms (hot flashes and night sweats), vaginal dryness, and
improvement in well-being as reasons for continuing menopausal hormone therapy.
This study asks: What is the effect
of discontinuing E + P therapy and placebo on older women who have taken it for
considerable time?
Conclusion: More than half of the women who
discontinued use reported return of some symptoms.
STUDY
1. This study began after
the WHI study was terminated in July 2002.Women had been taking conjugated
equine estrogens (0.625 mg) + medroxyprogesterone acetate (2.5 mg),or placebo, (CEE
+ MPA) for a mean of 5.6 years. All discontinued use at a mean age
of 69.
2. Eight to 12 months
after termination of the WHI study, and both E + P and placebo were suddenly
stopped, a survey asked the subjects (n = 8400) to describe any recurrence of
symptoms.
RESULTS
1. Over half of the women
who had been taking CEE + MPA reported recurrence of at least one moderate or
severe symptom 8 to 12 months after discontinuing use. Many who had been taking
placebo also reported symptoms:
CEE + MPA (%) Placebo (%)
Hot flashes and night sweats 21 5
Pain and stiffness
(joint, general, low back) 37 22
Feeling tired 21 12
Difficulty sleeping 18 8
Mood swings
8 3
Vaginal dryness 10 5
(Would not the recurrence of menopausal symptoms after discontinuing
placebo indicate a powerful placebo effect? RTJ )
2. After discontinuation,
women who developed symptoms adopted a wide variety of management strategies,
both lifestyle (eg, drinking more fluids, exercising, changing diet) and medical (talking to their clinician,
vitamin E, alternative medical techniques). The majority believed these were helpful.
(Perhaps
another indication of a placebo effect. RTJ)
3. Recurrence of
vasomotor symptoms was more common in women who reported these symptoms at
baseline (1993 to 1998) in the WHI
trial.
4. Recurrence of
vasomotor symptoms diminished with age of subjects who had previously taken CEE
+ MPA: 55-59 age group
(35%); 60-69 group (28%); 70 and
over (12%).
DISCUSSION
1. The study provides
insights about symptom experience after postmenopausal women discontinue CEE +
MPA after taking it for a number of years.
2. The mean age (63) of
women who began the WHI study in 1993 to 1998 was considerably older than the
age at which women typically begin menopausal hormone treatment.. The present
study judged symptom recurrence at mean age 69.
3. Women in this study
who discontinued CEE + MPA therapy after 5 to 6 years of use were more likely
to report recurrence of symptoms than women who discontinued placebo. However,
a significant number of women who had been taking placebo also reported
symptoms.
4. Troublesome recurrent
symptoms were more common in women in the WHI trial who had been experiencing
vasomotor symptoms in the past compared with those who had not. Few women who
did not have vasomotor symptoms before they started therapy developed symptoms
after discontinuing.
5. The higher prevalence
of pain and stiffness in respondents who were formerly taking CEE + MPA suggest
an additional benefit. This withdrawal symptom had not been documented in the
past. This warrants further investigation.
6. After treatment was
discontinued women used a wide variety of lifestyle and medical strategies to
manage symptoms. They were considered helpful.
CONCLUSION
Many participants (now mean age 69)
who terminated use of CEE + MPA after using it for 5-years experienced recurrence
of a range of symptoms.
Symptoms also recurred in women who
had been taking placebo although to a lesser extent than women who had taken
active hormones.
JAMA July 13, 2005; 294:
183-93 Original investigation,
first author Judith K Ockene, University of Massachusetts Medical School,
Worcester.
1 The Women’s Heath Initiative
trial determined the “Risks and Benefits of Estrogen plus Progestin in
Healthy Postmenopausal Women”
JAMA July17, 2002; 288: 321-33.
The study enrolled women between 1993
and 1998. It was designed to
determine if estrogen + progesterone given to a cross section of postmenopausal
women mean age 63 would reduce risk of cardiovascular events or protect against
them. It was not designed to determine effects on postmenopausal symptoms.
The harms over 5 years slightly
outweighed the benefits:
For 10 000 women over one year:
CHD events +
7 (harm)
Stroke +
8 (harm)
Pulmonary embolism +
8 (harm)
Invasive breast cancer +
8 (harm)
Colorectal cancer -
6 (benefit)
Hip fracture -
5 (benefit)
Global index +
19 (harm)
The main conclusion was that E + P
did not protect against
cardiovascular disease. The increased risk of breast cancer was confirmed.
“Not A Totally Benign Condition.”
7-3 WHITE-COAT
HYPERTENSION AS A RISK FACTOR OF TE DEVELOPMENT OF HOME HYPERTENSION
White-coat hypertension (WCHT) is characterized by an elevated
BP in medical settings, and a normal BP when self-recorded at home, or
determined by ambulatory recorders.
Sustained hypertension is the
presence of an elevated BP regardless of the setting.
Is WCHT related to later development
of sustained (home) hypertension?
Studies have been contradictory.
This present study was designed to
quantitatively determine the risk of transition from WCHT to sustained
hypertension.
Conclusion: WCHT is a transitional condition which
proceeds to sustained hypertension.
STUDY
1. This longitudinal observation study from
WCHT (defined as home BP < 135/85;
and office BP > 140/90) . N = 128
Sustained normotension (defined as
home BP < 135/85 and office BP < 140/90). N = 777
(Home BP determined by the HEM401C
Omron Health-Care company device.)
2. At baseline, subjects were mean age 56.
3. Mean baseline BP Home Office
WCHT 124/74 150/84
Sustained normotension 115/70 121/70
4. Follow-up for 8 years, compared risk of progression of
WCHT to sustained (home) hypertension.
RESULTS
1. During the 8-year
follow-up, 47% of the WCHT group progressed to home hypertension, vs 22% of the
sustained normotension group. (Odds ratio= 2.9)
2. In both groups, rates
of development of sustained home hypertension was greater as the baseline home
BP increased. (Ie, a baseline home BP of 110/70 was less likely to progress to
sustained hypertension than a baseline home BP of 120/80.)
3. Older age, obesity,
and male sex predicted development of home hypertension.
DISCUSSION
1. WCHT was a significant
predictor of the development of sustained home hypertension, independent of
other confounding factors and baseline home BP levels. “WCHT is not a
totally benign condition.”
2. Home BP measurements
are now widely used in clinical settings. The Japanese are particularly keen on
home BP determinations. Over 30 million devices for self-determination of BP
have been distributed in
3. Some studies have
reported that home BP better predicts cardiovascular events. WCHT may carry a
poor cardiovascular prognosis.
CONCLUSION
Over 8-years, WCHT often progressed
to sustained home hypertension. Progression was about twice the rate compared
with subjects with normal office BP.
Archives Int Med July
11, 2005; 165: 1541-46 Original
investigation, first author Takashi Ugajin,
Use Of High Doses Of Single Nutrients To Prevent Disease Has
Been Disappointing
7-4 ESSENTIAL NUTRIENTS: FOOD OR SUPPLEMENTS. Where Should The Emphasis Be?
Advance in our understanding of
essential nutrients has led to the ability to quickly and inexpensively treat
nutritional deficiencies. But it has allowed the possibility that the proper
balance of purified vitamins could supplant the need for a varied diet. We must
determine how best to advise the public in developed countries with respect to
nutrient supplements in an era which nutrient deficiencies are rare, chronic
disease rates are high, and overweight and obesity have reached epidemic
levels.
The government has issued recommended
dietary allowances (RDAs) ever since 1943. They have been revised
periodically. A new system
establishes dietary reference intakes (DRIs) for each nutrient. This includes
the RDAs and estimated average requirements, along with tolerable upper intake
levels. As scientific evidence accumulates, recommendations have changed.
In the
Single-nutrient interventions; Disappointing results.
Low fat and sodium diets which are
high in fruits and vegetables are associated with a decrease in BP and risk of
cardiovascular diseases. However, instead of focusing on dietary patterns, most
intervention trials have used high doses of single nutrients, or nutrient
cocktails, in an attempt to prevent disease. These results for the most part
have been disappointing.
Vitamin E, vitamin C, and beta carotene:
Recommendations for use were
supported by in-vitro studies in which addition of these vitamins reduced the
susceptibility of isolated LDL-cholesterol to oxidation. As with other examples
of observational studies, subsequent intervention studies did not support the
putative benefits. The American Heart Association now concludes
that…“There is currently no basis for recommending that patients
take vitamin C or E supplements or other antioxidants for the express purpose
of preventing or treating coronary artery disese”.
Another example of discordance
between the observational associations and single-nutrient intervention by
beta-carotene dispelled the notion that high-dose supplements would reduce risk
of lung cancer in smokers.
A recent meta-analysis of vitamin E
supplements suggested that doses greater than 400 IU daily (10 times RDA) increased all-cause mortality.
Folic acid:
In 1991, a large-scale study
concluded that folate supplements do indeed reduce risk of neural tube defects
in newborns. This led to fortification of flour and other dietary grains. A
general reduction of homocysteine levels and an increase in folate levels
resulted.
Epidemiological and clinical data
suggest that elevated plasma homocysteine levels are associated with increased
risk of cardiovascular disease.
Folic acid reduces homocysteine levels. In 1999, authors concluded that...
“Higher folic acid intake, by reducing homocysteine levels promises to
prevent atherosclerotic vascular disease”. However, the relationship between diet
and plasma homocysteine is complex, and does not rely solely on folate status.
Recent studies have reported that
folic acid, B12, and B6 given to patients who had experienced a non-disabling
stroke had no significant benefit on vascular outcomes. Others studies have warned
that high does of folate may interfere with B12 metabolism and thus increase
cognitive decline. Supplemental folic acid can precipitate vitamin B12 dementia
in patients who have minimal B12 levels.
“A final assessment...awaits
the results of ongoing placebo-controlled intervention trials.”
Although observational data are
valuable in identifying areas in which to conduct intervention studies, they
should not be used to draw premature conclusions.
Good data suggest that certain
dietary and lifestyle patterns are associated with decreased risk of chronic
disease. However, providing nutrient supplementation to mimic these effects has
failed to result in the efficacy that
was originally anticipated.
There remain, however, some strong
reasons to make targeted recommendations for use of specific supplements:
1) Folic acid to prevent neural tube
defects.
2) Vitamin B12 (high
dose) in the elderly who often have atrophic gastritis and do not absorb food
B12 adequately.
3) Vitamin D and calcium intakes
are often deficient in Americans of all ages, especially in older persons.
Supplements are the most practical way to meet the RDAs.
The article concludes: “There are insufficient data to
justify an alteration in public health policy from one that emphasizes a food
and diet to one that emphasizes nutrient supplements.”
JAMA July 20, 2005; 294:
351-58 “Special
Communication”, first author Alice J Lichenstein,
Comment:
Our pharmacy shelves are replete with
stocks of individual vitamins. Vitamin E is a favorite.
Some examples from my cursory
examination:
Content PER tablet Times
RDA
Vitamin A 8000
IU 2
Vitamin
E 1000
IU 25
Vitamin
B1 100
mg 66
Vitamin
B2 100
mg 59
Vitamin
C 500
mg 8
Vitamin B6 50
mg 25
Vitamin D 400
IU 1
Vitamin B12 500 mcg 83
Folic acid 800 mcg 2
Although the costs are generally
modest, costs will far exceed that of a daily multivitamin supplement
containing up to 100% of the RDAs of all. Not only are the above a waste of
money, but some of them may be toxic.
I
do not believe the authors were talking about the daily use of supplements
containing the RDAs of vitamins and minerals. I do not believe the authors of the
article infer that supplements which mimic daily requirements are harmful. Many
of the individual components will be unnecessary, but I do not believe they are
harmful.
Note the possible benefits of daily
low-dose supplements—containing up to 100% of RDA:
1) Vitamin D 400 IU: Many persons are deficient. In low
dose, daily use is very safe. This, I believe should be supplemented by added
calcium.
2) Folic acid 400
mcg: Already is considered
essential to prevent neural tube defects. I would not yet discount studies
relating lowering of homocysteine levels to benefit by reducing risk of
cardiovascular disease.
3) Vitamin B12 6
mcg: Crystalline B12 is absorbed in
elderly persons with atrophic gastritis who lack ability to absorb food B12. This
would negate the possible harmful effects of folate in obscuring neurological
effects of B12 deficiency. However,
a dose of 6 mcg is not sufficient since only about 1% of cyanocobalamin is
absorbed. This may be one instance where a much higher dose (eg 1000 mcg) will
be beneficial. The 6 mcg dose adds nothing except to look good on the label.
No one argues against a balanced
diet. The problem is—most Americans simply will not change to, or
maintain, a more healthful diet to ensure adequate nutrient intakes.
I believe daily supplements
containing the RDAs of vitamin D and folic acid are helpful because the diets
of many Americans are deficient. I
am not willing to give up on the putative benefits of folic acid on lessening
risk of cardiovascular disease by decreasing levels of homocysteine.
Vitamin B12 as an individual
supplement is an exception in some circumstances. Some elderly persons who lack
the ability to absorb B12 from food will absorb enough from high doses of
crystalline cyanocobalamin (1 mg) to maintain a normal blood level. The RDA
amount is not sufficient in these individuals.
Admittedly, most of the contents of
the daily supplement are a waste. The RDAs of Vitamin D and folic acid are
likely to be beneficial.
At a cost of 3 cents a day, I will
continue to take my supplement in addition to trying to maintain a healthy
diet.
There Is No Cutpoint Of PSA With Simultaneous High
Sensitivity And High Specificity
7-5 OPERATING CHARACTERISTICS OF
PROSTATE-SPECIFIC ANTIGEN
In 2001, approximately 75% of men in
the
Currently men in the
PSA screening has become
controversial. No studies have proven that it leads to a reduction in mortality
from prostate cancer (PC). After 2
decades of screening, mortality from PC has decreased, but it is not known if
this is due to screening or other factors such as treatment efficacy. PC
mortality rates have also declined in countries where PSA screening is
uncommon. In the
A potential explanation for these observations
may be due to the characteristics of PSA measurement as a screening test. In
general, biopsy has not been recommended unless PSA levels exceed a threshold
of 4.0 ng/mL. Other studies have reported that as many as 15% of men with a PSA
less than 4.0 have PC, and that 15% of these are high grade.
This study estimated the relation
between true positive PSA tests and true negative PSA tests over a range of PSA
cutpoints. (Sensitivity vs specificity.)
Conclusion: For monitoring healthy men, there is no cutpoint of PSA with simultaneous
high sensitivity and high specificity:
A. Setting the cutpoint high will
result in:
More men with cancer being missed.
Fewer men without cancer being
falsely considered positive for cancer and subject to biopsy.
B. Setting the cutpoint low will
result in:
More men with cancer being diagnosed.
More men without cancer being falsely
considered as having cancer and subject to biopsy.
STUDY
1. This present study is an
extension of the Prostate Cancer Prevention Trial which entered over 18 000
healthy men age 55 and older (mean age = 62) in 1994-2003.
A. At baseline, no one
was considered to have PC. All had normal digital rectal examinations. All had
a PSA under 3.0
B. Subjects were followed
for up to 7 years with annual PSA determinations and rectal examinations. If the PSA exceeded 4.0 and/or the
digital rectal examination was abnormal, a biopsy was recommended.
C. After 7 years, an
end-of-study biopsy was recommended in all cancer-free subjects regardless of
PSA values and results of digital rectal examination.
2. At the end of the
study, the authors calculated the sensitivities and specificities of 9 PSA
levels arbitrarily set at increasing cutpoints from 1.1 to 10.1. From these
they plotted a receiver operating characteristic (ROC) curve.
3. Main outcome measures
= operating characteristics of PSA for PC detection, including sensitivity,
specificity, and the ROC curve.
RESULTS
1. Of the participants
who underwent biopsy (n = 5587), 22% (n = 1225) had PC.
2. Of the 1213 PCs with
Gleason scores recorded, 21% were Gleason grade 7 or greater, and 5% were
Gleason grade 8 or greater.
3. Determining a clear-cut rule for prostate biopsy from
these results would be challenging.
A. Sensitivities: various cutpoints of PSA in men who have PC
PSAs for men with PC True
+ % False
negative %
1.1 83 17
2.6 40 60
4.1 20 80
10.1 1 99
According to these figures, for every
1000 men with prostate cancer:
830 (83%) had a PSA 1.1 and above;
and 170 (17%) had a PSA less than 1.1
400 (40%) had a PSA 2.6 and above; and 600 (60%) had a PSA less
than 2.6
200 (20%) had a PSA 4.1 and above; and 800
(80%) had a PSA less than 4.1
10 (1%) had a PSA 10.1 and above; and 990 (99%) had a PSA less
than 10.1
B.
Specificities of various cutpoints of PSA in men who do not have PC
PSAs for men without PC True
negative % False
positive %
1.1 40 60
2.6 81 19
4.1 94 6
10.1 99 1
According to these figures, for every
1000 men without prostate cancer:
600 (60%) had a PSA 1.1 and above;
and 400 (40%) had a PSA less than 1.1
190 (19%) had a PSA 2.6 and above; and 810 (81%) had a PSA less
than 2.6
60 (6%) had a PSA 4.1 and above; and 940
(94%) had a PSA less than 4.1
10 (1%) had a PSA 10.1 and above; and 990 (99%) had a PSA less
than 10.1
3. The area under the ROC curve for
prostate cancer vs no prostate cancer (true positive rate on the vertical axis
vs false positive rate on the horizontal axis charted at all cut-points) was
0.678. (Not very discriminating. An area
of 0.500 would indicate no ability to diagnose PC. As many subjects with PC
would have a positive test as those without PC. The test would be useless. RTJ
.)
DISCUSSION
1. Use of PSA for detection of early PC
with the commonly recommended cut-point of 4.0 may result in delayed detection
of PC. “It will be a challenge to the medical community to change the
long-held notion that there is a ‘normal’ PSA.” There is a
continuum of risk and no clearly defined PSA
cut-point at which to advise biopsy.
2. Many PCs, even those with high-grade,
are missed even at low levels of PSA. This...”Could explain the
discrepancy between the rate of PSA screening and the [lack of] change in prostate mortality over the past 15
years”.
3. The delay in diagnosis of high-grade
tumors until PSA levels exceed the current threshold of “normal”
values could also explain why there is a 35% risk of subsequent treatment after
radical prostatectomy, presumably due to disease recurrence.
4. Lowering the PSA threshold would have 2
consequences: 1) increased biopsy rates; and 2) the possibility of increased
detection of biologically inconsequential cancers.
5. An inherent property of all screening
tests is that they disproportionately enhance the detection of slower-growing
cancers because more-aggressive tumors have a greater likelihood of becoming
clinically apparent between screenings. While lowering the PSA threshold is
likely to increase the detection of such aggressive tumors at an earlier stage,
the unavoidable tradeoff is the increased detection of biologically
inconsequential cancers.
6. Patients, in concert with their
physicians will ultimately have to weigh the sensitivity-specificity trade-offs,
in combination with the uncertain natural history of the disease, to determine
whether further evaluation with a biopsy is appropriate.
JAMA July 6, 2005; 294: 66-70
Original investigation, first author Ian M Thompson, University of Texas Health
Sciences Center,
7-6 TREATMENT OF MENOPAUSAL SYMPTOMS:
What Shall We Do Now?
In the past few years, many studies have reported on the benefit/harm-cost
ratio of hormone replacement therapy and other interventions for treatment of
menopausal symptoms. Confusion remains.
This article permits us to step back and gain an overlook. RTJ
Almost all women who reach the
menopause will have symptoms at some point. Almost 80% have hot flashes and
night sweats. About 20% of these find them intolerable. Many will request
treatment. Hot flashes may continue for up to 5 years and, in some individuals,
even longer. Effective long-term as
well as short-term safe and effective therapy is needed.
During the past few years, a
substantial number of women have discontinued hormone replacement therapy (HRT)—the most effective therapy,
because of concerns about adverse effects.
Numerous alternatives have been
suggested. But, assessment of the
quality of evidence about the safety and effectiveness of different treatments
has been difficult.
This review article (based on a
PubMed search of randomized controlled trials and observational studies)
summarizes data from studies addressing the efficacy, risks, and benefits of
frequently prescribed treatments.
Hormone replacement therapy (HRT):
Evidence-based guidelines for HRT for
menopausal symptoms:
Indications:
Systemic HRT for moderate to severe
vasomotor symptoms (hot flashes).
Systematic HRT for night
sweats, insomnia, poor sleep quality (indirectly improving wellbeing and
symptoms of depression).
Urogenital symptoms (vaginal estrogen
if systemic HRT is not taken).
General advice:
Benefits should be offset against
risks. For otherwise healthy women, benefits of short term
HRT are likely to outweigh risks.
Women who take HRT for longer than 5 years should be told about potential risks
Advice should be individualized.
Lifestyle and alternative therapies
should be discussed.
Treatment should be at the lowest
effective dose.
Potential risks:
Breast cancer:
The absolute risk of breast cancer is
small, but it is the greatest concern. Risk probably increases after use of
combined E + P after 5 years. There
may be no risk for estrogen-alone.
Women with a history of breast cancer should not take HRT.
Coronary heart disease:
No evidence of benefit in reducing
risk. HRT should not be given for primary or secondary prevention. It should
generally be avoided in women at increased risk for CVD. There may be a slight increase in risk in women taking
combined E + P (7 per 10 000 per year). There may be a slight reduction in risk in women taking
estrogen alone (5 per 10 000 per year).
Stroke
HRT may be associated with increased
risk of ischemic stroke. (8 per 10 000 women taking E + P vs 12 in those taking
estrogen alone).
Venous thromboembolism
VTE is the major risk factor in the
first 5 years of use of both estrogen-alone and E + P. Oral HRT increases risk. (18 per 10 000
women per year for combined E + P; 7 per 10 000 per year for estrogen alone).
Osteoporosis
HRT is not recommended as first line
therapy. When used for treatment of menopausal symptoms, there may be an added
benefit in reducing risk of osteoporotic fractures.
Although the beneficial effects of
estrogen therapy on the skeleton are not reduced by increasing age, once
treatment stops, bone loss resumes.
Endometrial cancer
Estrogen alone increases risk.
Combined HRT should be used in women with a uterus.
Dementia
No role for HRT
Selective serotonin reuptake inhibitors
Slow-release venlafaxine [Effexor] might be effective in the short term
(<12 week).
Life style changes
Increased exercise, achieving a
normal body mass index, and discontinuing smoking are reasonable, since these
changes will benefit long-term health.
Alternative and complimentary therapies
There is not enough evidence that any
of the complimentary therapies available are any better than placebo for vasomotor
symptoms. Few safety data exist.
Lancet July 30, 2005;
366: 409-21 Review
article, first author Martha Hickley,
Right-Sided Stroke Or TIA May Be “Silent”, At
Least As Far As Recognition Goes.
7-7 UNDERDIAGNOSIS OF RIGHT-BRAIN
STROKE
“Recognizing a stroke should be
relatively simple, right?
Wrong!”
A study in this issue of Lancet1 included over 20 000
patients with stroke or TIA. It reported a striking difference in the rate of
diagnosis of left-sided and right-sided ischemic events. Symptoms of
cerebrovascular events due to anterior (carotid) circulation deficits differ
depending on the hemisphere involved.
Right-sided stroke was often
overlooked. Why?—The
perceived severity or significance of symptoms is the dominant factor.
The major difference between
hemispheres is the lateralization of cognitive functions, particularly the
left-hemisphere dominance of language. Patients, families, and physicians might
be more likely to recognize a disturbance of speech or language, and apraxia of
the right hand due to left-hemisphere ischemia than more difficult-to-define
cognitive deficits (sudden confusion) or apraxia of the non-dominate left hand
from a corresponding lesion in the right hemisphere. Neglect (defined as a
reduction in awareness of neurological deficits) is associated with
right-hemisphere lesions.
There are deficiencies in knowledge
about the signs and symptoms of stroke. Non-language deficits in particular may
get little mention. Even complex clinical severity rating scales, such as the
National Institutes of Health Stroke Scale systematically emphasize deficits
associated with left-hemisphere lesions. Imaging studies show that patients
with right hemisphere stroke can have a low NIHSS score despite substantial
infarct volume.
Assuming that right- and left-sided
strokes have equal frequency, the German study suggested that, for every eight patients currently
hospitalized for anterior-circulation
stroke or TIA, one patient with
right-sided ischemia will be overlooked. These patients are unlikely to
receive the same standard of management for secondary prevention. Patients with
right-hemisphere events are underrepresented in major trials of endarterectomy
for symptomatic carotid stenosis.
The effect on cognitive impairment
due to right-hemisphere dysfunction on day-to-day living is no less than that
of left-hemisphere dysfunction. Important unrecognized consequences
include: influences on relationships,
maintenance of employment, appropriate advice about driving, and access to
rehabilitation.
Imaging by MRI is valuable when the
clinical picture is uncertain. Up to half of patients with clinical TIA will
have positive images.
Lancet July 30, 2005;
366: 349-50 Commentary by John N Fink, Christchurch School of Medicine and
Health Sciences, Christchurch, New Zealand.
1 “Difference In Recognition Of Right
And Left Hemispheric Stroke”
Lancet
Cerebrovascular events are frequently
accompanied by characteristic, but different, neuropsychological deficits, depending
on the side of the lesion—aphasia due to lesions in the left hemisphere,
and neglect (diminished awareness) associated with lesions in the right
hemisphere. Self-recognition of symptoms is especially important in patients
with TIA.
Most stroke scales emphasize deficits
associated with lesions in the left hemisphere. In this study, left-hemisphere TIAs were
recorded in over 2100 patients vs 1300 right-hemisphere TIAs
The probable explanation is that
symptoms attributable to cerebral ischemia are more noticeable if language or
right hand function is affected. Both of these functions are controlled by the
left hemisphere.
In contrast, right-hemisphere lesions
are associated with a reduction in awareness of neurological deficits
(neglect). They are therefore perceived by patient and physician as being less
severe, or are not identified at all as stroke symptoms.
The asymmetry of symptoms and
awareness (right vs left hemisphere) is most striking in individuals with
mild-to-moderate defects. This lends support to the effect of awareness-related
factors. The asymmetry does not apply to cerebral hemorrhage, which causes more
severe symptoms.
Selection effects might lead to fewer
prophylactic interventions in patients with right-hemisphere lesions.
“All Women Should Have A Measurement Of Bone Mineral
Density At The Age Of 65.”
7-8 SCREENING FOR OSTEOPOROSIS
Osteoporosis is a favored subject in the current literature. This article
presents details about recommendations for screening. I abstracted a few
highlights. RTJ
Fewer than 1/3 of patients who have
had fragility fractures are appropriately evaluated and treated for
osteoporosis. The rates of diagnosis are even lower for those who have not yet
had a fracture.
Clinicians should routinely recommend
that patients have an adequate total intake of calcium (1200 mg per day), and
of vitamin D (400 to 800 IU per day), and participate in weight bearing
exercises. Many patients will not lose bone if they have an adequate intake of
calcium and vitamin D and exercise regularly. Nevertheless, the rates of
fractures remain high in individuals who receive these interventions.
It is important to identify high-risk
persons by appropriate screening.
Dual x-ray absorptiometry at the
lumbar spine and hip is a reliable and safe way of assessing fracture risk in
postmenopausal women. Peripheral measurements (eg, ultrasonography) should not
be used for decision making.
The 10-year risk of a fragility
fracture in a postmenopausal woman with a T-score at -2.5 standard deviations
or less (compared with a normal young woman), and no other risk factors is more
than 20% at age 65.
Factors other than T-score which
indicate elevated risk include: a previous fragility fracture, family history
of fracture, low body weight, loss of 5% or more of baseline weight and loss of
height, silent vertebral fracture, discontinuation of postmenopausal estrogen
therapy, increased tendency to fall, and drugs such as corticosteroids which
increase bone resorption. Indeed,
“Any fracture in a postmenopausal woman should prompt consideration of
bone-density measurement”.
“Low bone mass”
(osteopenia) is defined by a T-score between -1.0 and -2.5. About half of
fragility fractures occur in the osteopenic group.
“All women should have a
measurement of bone mineral density at the age of 65.”
The possibility of osteoporosis in men who have a fragility fracture or
other risk factors should not be forgotten.
Despite the recommendations for
screening, there is little evidence of its effectiveness in enhancing
prevention and treatment programs.
NEJM July 14, 2005; 353:
164-71 “Clinical
Practice”, review article by Lawrence G Raisz, University of Connecticut
Heath Center,
7-9 INSULIN RESISTANCE AND RISK OF
CONGESTIVE HEART FAILURE
Diabetes and obesity are established
risk factors for congestive heart failure (CHF).
Both are related to insulin resistance.
In patients with established CHF,
insulin resistance is associated with more severe disease and a worse
prognosis.
This study explored if insulin
resistance might predict CHF and provide the link between obesity and CHF.
Conclusion: Insulin resistance (recorded in a number
of ways, including the 2-hour glucose level measured on an oral glucose tolerance
test) predicted incidence of CHF
independently of established risk factors.
STUDY
1. The
2. Analyzed a number of
variables reflecting insulin sensitivity together with established risk
factors.
3. Main outcome measure =
first hospitalization for CHF.
RESULTS
1. One hundred and four
men of 1187 developed CHF over 9 years. As expected, prior myocardial
infarction, hypertension, diabetes, left ventricular hypertrophy, and current
cigarette smoking were significant risk factors for CHF.
2. After adjusting for
presence of diabetes at baseline, 5 indicators of insulin resistance remained
significant predictors of subsequent CHF:
clamp glucose disposal rate; fasting insulin levels; fasting proinsulin
levels; BMI; waist circumference: and 2-hour
glucose level.
3. After adjusting for
multiple established risk factors, an increase of 1 standard deviation in the
2-hour
glucose value was
associated with an increased hazard ratio of 1.44 in incidence of CHF.
4. After adjusting for
diabetes, fasting glucose levels were not predictive.
DISCUSSION
1. Insulin resistance,
measured by the 2-hour glucose level on the oral glucose tolerance test,
predicted incidence of CHF independently of diabetes, truncal and overall
obesity, and other risk factors.
2. The previously
described association between obesity and CHF may be mediated, in part, by
insulin resistance.
3. The authors cite a
number of possible mechanisms for the association. (page 339).
CONCLUSION
Insulin resistance (as determined by
the 2-hour glucose levels) independently predicted incidence of CHF in this
group of elderly men.
JAMA July 20 2005; 334-41
Original investigation, first author Erik Ingelson,
7-10 AN EVALUATION OF ECHINACEA ANGUSTIFOLIA IN EXPERIMENTAL
RHINOVIRUS INFECTIONS.
Echinacea is widely used as a herbal
remedy for the common cold. It was recently endorsed by the WHO for treatment
of the common cold. Efficacy studies have produced conflicting results.
A variety of Echinacea products are on
the market. This study concerned E
angustifolia roots. E angustifolia is the species originally
used by Native Americans in the
This study produced 3 different
preparations with distinct phytochemical profiles by extraction.
About 400 volunteers were randomized
to either: 1) prophylaxis with echinacea beginning 7 days before viral
challenge with rhinovirus), or 2) treatment of the experimental infection
(beginning on the day of challenge), or 3) placebo.
Results: There were no significant effects of
echinacea extracts on severity of symptoms, volume of nasal secretions,
polymorphonuclear leukocytes, interleukin-8 concentrations in nasal-lavage
specimens, or on quantitative virus titers.
Conclusion: The results indicate that these
extracts, either alone or in combination, do not have clinically significant
effects on rhinovirus infection, or on the resultant clinical illness.
The investigators conclude that the
burden of proof of effectiveness should now lie with those who advocate this
treatment.
NEJM July 28, 2005; 353:
341-48 Original investigation,
first author Ronald B Turner, University of Virginia School of Medicine,
Increasing Consumption Associated
With A Reduced Risk
7-11 COFFEE CONSUMPTION AND RISK OF
TYPE 2 DIABETES: A Systematic
Review
Epidemiological evidence has
suggested that higher coffee consumption may reduce the risk of type 2 diabetes
(DM2). Coffee contains numerous
substances beside caffeine some of which have been shown to have an effect on
glucose metabolism. Not until recently has a relation to risk of DM2 been
studied. A Dutch study reported that higher consumption of coffee was
associated with a lower risk of DM2. 1
This systematic review examined the
association between habitual coffee consumption and risk of DM2.
Conclusion: The review supports the
hypothesis that habitual coffee consumption is associated with a substantially
lower risk of DM2.
STUDY
1. MEDLINE search through
January 2005 identified 9 cohort studies of habitual coffee consumption
associated with and risk of DM2.
DM1 was excluded.
2. Extracted data on
study design, participant characteristics, measurements of coffee consumption,
and outcomes adjusted for confounders.
3. Distinguished 4 levels of daily consumption:
1) Six or more cups
2) 4 to 5 cups
3) 1 to 3 cups
4) No coffee consumption (Reference
category)
RESULTS
1. Cohort studies contained a total of over 199 000 subjects.
And 8394 cases of DM2.
A. Relative risk of DM2: coffee vs no
coffee: RR Confidence
interval
Level 1) 0.54 0.54-0.78
Level 2) 0.72 0.62-0.83
Level 3) 0.94 0.88-1.01
All levels combined 0.65
B. One study reported an
inverse association between coffee consumption of 6 or more cups daily vs 2 or
fewer cups and incidence of impaired
glucose tolerance. (RR = 0.37)
C. No study reported an
association with impaired fasting
glucose.
D. Two
E. Adding sugar and/or
cream made no difference.
DISCUSSION
1. These cohort studies
support a significant inverse association between coffee consumption and risk
of DM2. Participants who drank 4 to 6 cups and over 6 cups daily had a 285 to
35% lower risk of DM2.
2. Mechanisms? The authors speculate that various
components of coffee other than caffeine may have beneficial effects by
increasing insulin sensitivity, reducing hepatic glucose output, inhibiting
glucose absorption, and enhancing insulin secretion. They suggest that caffeine
is not the cause of the inverse association between coffee and DM2. Indeed,
some studies report that caffeine acutely increases
post-load glucose concentrations and lowers
insulin sensitivity.
3. Residual confounding
cannot be fully excluded as a potential explanation of findings in
observational studies. Observational studies cannot prove causality
4. It is premature to
recommend increasing coffee consumption as a public health strategy.
CONCLUSION
This systematic review supports the
hypothesis that habitual coffee consumption is associated with a substantially
lower risk of DM2.
JAMA July 6, 2005; 294: 97-104 Original investigation, first author Rob
M van Dam, Vrije Universiteit,
1 Lancet 2002; 360: 1477-78