Research Highlights - 2002 and 2003
Below are highlights of research reported by grantees supported by the
Epidemiology and Genetics Research Program (EGRP). We can't begin to capture
all the research contributions of our grantees and apologize for this.
Your suggestions
on additions to make to the Web page are welcome. (The names that appear
in boldface are those of the principal investigators of the EGRP-supported
grants cited in the published reports.)
Breast Cancer
Colorectal Cancer
Lung Cancer
Melanoma
Non-Hodgkin's Lymphoma
Prostate Cancer
Viruses
Study Design
Methods
Some Breast Cancers May Be Due to Inherited Susceptibility to Hormones
at Puberty
Thomas
Mack, M.D., M.P.H., and Ann Hamilton, Ph.D., of the University of
Southern California at Los Angeles, have found that certain breast cancers
may be linked to an unusual inherited sensitivity to the ovarian hormones
that flood the body at puberty. Among identical female twins who both
were diagnosed with breast cancer, the twin who began menstruating earlier
was more than five times as likely as the other twin to develop breast
cancer first. Females who started menstruating before age 12 were especially
susceptible to getting breast cancer first within the pair. In contrast,
some of the well-known risk factors for breast cancer, such as late age
at first pregnancy and at menopause, were associated with increased risk
for breast cancer only among pairs of identical and fraternal twins in
which one twin had breast cancer, but not among those in which both twins
had the disease. These findings suggest that there may be another pathway
to development of breast cancer that is related to genetic susceptibility.
In some genetically susceptible women, elevated ovarian hormone levels
at puberty might affect breast cells when they are still immature and
vulnerable, and the damage may manifest itself as cancer decades later.
Hamilton AS, Mack TM. Puberty and genetic susceptibility
to breast cancer in a case control study in twins. N Engl J Med 2003
Jun 5;348(23):2313-22.
Lobular Breast Carcinoma on the Increase
Research
has suggested that combined estrogen and progestin hormone replacement
therapy (CHRT) may be associated with increased risk for breast cancer,
particularly invasive lobular breast carcinoma. The finding is noteworthy
because lobular carcinoma is more difficult to detect by physical examination
and mammography. Janet Daling, Ph.D., of Fred Hutchinson Cancer
Research Center, and colleagues now report that incidence rates for lobular
carcinoma increased steadily from 1987 to 1999 (the proportion increasing
from 9.5 to 15.6 percent of all breast cancer cases), while rates for
ductal carcinoma remained constant. The increase in rates for lobular
carcinoma was most pronounced for women ages 50 and older.
In further research focusing on postmenopausal women, Daling and others
found that the risk for invasive lobular breast carcinoma and other histologic
types of breast cancer increased among women who were currently taking
CHRT. Unopposed estrogen replacement therapy (ERT) was not associated
with increased risk for any histologic type of breast cancer. Neither
CHRT nor ERT substantially increased the risk for ductal breast carcinoma.
They also found that incidence rates for lobular carcinoma in situ have
steadily increased over the past 25 years among postmenopausal women.
These findings suggest the need for further research to explore reasons
for these trends.
Li CI, Anderson BO, Daling JR, Moe RE. Trends in incidence
rates of invasive lobular and ductal breast carcinoma. JAMA 2003
Mar 19;289(11):1421-4.
Daling JR, Malone KE, Doody DR, Voigt LF, Bernstein
L, Coates RJ, Marchbanks PA, Norman SA, Weiss LK, Ursin G, Berlin JA,
Burkman RT, Deapen D, Folger SG, McDonald JA, Simon MS, Strom BL, Wingo
PA, Spirtas R. Relation of regimens of combined hormone replacement
therapy to lobular, ductal, and other histologic types of breast carcinoma.
Cancer 2002 Dec 15;95(12):2455-64.
Li CI, Anderson BO, Daling JR, Moe RE. Changing incidence
of lobular carcinoma in situ of the breast. Breast Cancer Res Treat
2002 Oct;75(3):259-68.
Obesity, Tamoxifen, and Outcomes in Women with ER-Positive Early-Stage
Breast Cancer
James
Dignam, Ph.D., of The University of Chicago, and colleagues have found
that obesity is not associated with an increased risk of recurrence among
women with early-stage, hormone-responsive breast cancer, and does not
appear to decrease the effectiveness of the drug tamoxifen. This finding
supports use of tamoxifen for women of all body types. Earlier studies
suggested that risk for breast cancer recurrence and death was increased
for obese women compared with lean women, but these studies included women
with different stages of breast cancer. Further, obesity was found to
be associated with increased risk for contralateral breast cancer, other
new primary cancers, and overall mortality. The findings are from analysis
of data on 3,385 women enrolled in a National Surgical Adjuvant Breast
and Bowel Project (NSABP) randomized, placebo-controlled clinical trial
(B-14) evaluating the effectiveness of tamoxifen following surgery for
lymph node-negative, estrogen receptor (ER)-positive breast cancer.
Dignam JJ, Wieand K, Johnson KA, Fisher B, Xu L, Mamounas
EP. Obesity, tamoxifen use, and outcomes in women with estrogen receptor-positive
early-stage breast cancer. J Natl Cancer Inst 2003 Oct 1;95(19):1467-76.
Estrogen Associated With Increased Risk for Breast Cancer in Asian Women
Most
epidemiologic studies on estrogen and breast cancer have been conducted
in white populations. A new study assessed the association in Asian women
whose levels of estrogen are substantially lower than those of white women.
Herbert Yu, M.D., Ph.D., of Yale University, and Wei Zheng,
Ph.D., of Vanderbilt University, and colleagues found that elevated
sex hormones in the circulation, both estrogen and androgen, were associated
with increased risk for breast cancer even in the Asian population with
relatively low sex hormone levels. The finding suggests that the role
of endogenous sex hormones in breast cancer is the same in the Asian population
as in white women. Dr. Yu is pictured far left, and Dr. Zheng is to his
right.
Yu H, Shu XO, Shi R, Dai Q, Jin F, Gao YT, Li BD, Zheng
W. Plasma sex steroid hormones and breast cancer risk in Chinese women.
Int J Cancer 2003 May 20;105(1):92-7.
Electromagnetic Fields Not Associated With Risk for Breast Cancer
M.
Cristina Leske, M.D., M.P.H., of Stony Brook University, and colleagues
found no indication that electromagnetic fields (EMFs) increase risk for
breast cancer in a study that included comprehensive measurements of EMFs
in and around the outside of the homes of study participants, and data
collected by interview. The findings offer reassurance to individuals
who have been concerned about a possible link between EMFs and risk for
breast cancer. The results are consistent with an earlier NCI-funded study
of EMFs and breast cancer that included in-home measurements, adding further
weight to the strength of the evidence.
Schoenfeld ER, O'Leary ES, Henderson K, Grimson G,
Kabat GC, Ahnn S, Kaune WT, Gammon MD, Leske MC. Electromagnetic fields
and breast cancer on Long Island: A case-control study. Am J Epidemiol
2003 July 158(1):47-58.
Dietary Changes Associated With Colorectal Cancer in Mexican Americans
Kristine
Monroe, Ph.D., of the University of Southern California at Los Angeles,
and Laurence Kolonel, M.D., Ph.D., of the University of Hawaii,
and colleagues examined changes in dietary practices that might be consistent
with the increasing incidence of colorectal cancer in the Mexican-American
migrant population of Los Angeles. Some food traditions were retained
by Mexican Americans, but the dietary changes resulting from acculturation
were significant and support an association between colorectal cancer
risk and certain dietary components, especially alcohol as a risk factor
and vegetables as protective factors. The scientists found an 11 percent
and 9 percent decrease in calorie-adjusted mean intake of vegetables,
excluding legumes, in U.S.-born men and women, respectively, compared
with Mexican-born study participants. The decline in mean vegetable intake
was lower, 18 percent and 15 percent, respectively, when legumes were
included in the vegetable category. There also was a decrease in intake
of nonstarch polysaccharides (dietary fiber) from vegetables, 13 percent
in men and 10 percent in women. The study is based on data from the EGRP-funded
Multiethnic Cohort Study.
Monroe KR, Hankin JH, Pike MC, Henderson BE, Stram
DO, Park S, Nomura AM, Wilkens LR, Kolonel LN. Correlation
of dietary intake and colorectal cancer incidence among Mexican-American
migrants: The Multiethnic Cohort Study. Nutr Cancer 2003;45(2):133-47.
Loss of DNA Repair Capability in Colorectal Cancer Patients Increases
With Age
The
frequency of loss of expression of the DNA repair gene hMLH1 in
colorectal cancer patients is strongly associated with increasing age,
according to research by Noralane Lindor, M.D., of the Mayo Clinic,
and colleagues. The loss was most pronounced in tumors of female patients,
and in tumors that originated on the right side of the colon. Loss of
gene expression in right-sided tumors occurred in almost 50 percent of
patients who were more than 90 years of age. The age-related trend also
was seen in males and in tumors that originated in the left colon. The
findings suggest the need for additional research on possible environmental
or genetic reasons for the damage, and the possibility of developing a
non-invasive method to screen for the disease. The study population was
drawn from the EGRP-funded Colon Cancer Family Registries.
Kakar S, Burgart LJ, Thibodeau SN, Rabe KG, Petersen
GM, Goldberg RM, Lindor NM. Frequency of loss of hMLH1 expression in
colorectal carcinoma increases with advancing age. Cancer 2003
Mar 15;97(6):1421-7.
New Lead Found on Genetics of Familial Colorectal Cancer
New
research points to a chromosomal region responsible for forms of familial
colorectal cancer unrelated to well known hereditary forms of the disease.
Familial adenomatous polyposis (FAP) and hereditary nonpolyposis colorectal
cancer (HNPCC) account for about 5 percent of colorectal cancers, but
an additional 20 percent of individuals with the cancer report having
a first-degree relative with the disease. Whole genome scans were conducted
to test for genetic linkage in 53 kindreds in which two or more siblings
were diagnosed with colorectal by age 65 or younger, or who had advanced
colon adenomas of greater than one centimeter, or showed high-grade dysplasia.
Kindreds with FAP, HNPCC, or other known hereditary forms of the cancer
were excluded.
Sanford Markowitz, M.D., Ph.D., of Case Western Reserve University,
and colleagues found that a single locus (9q22.2-31.2) can contribute
to susceptibility in patients with familial colorectal cancer unrelated
to known syndromes. Additional research will be needed to determine if
the findings are generalizable to larger populations.
Wiesner GL, Daley D, Lewis S, Ticknor C, Platzer P,
Lutterbaugh J, MacMillen M, Baliner B, Willis J, Elston RC, Markowitz
SD. A subset of familial colorectal neoplasia kindreds linked to chromosome
9q22.2-31.2. Proc Natl Acad Sci 2003 Oct 28;100(22):12961-5.
Searching for Reasons for Elevated Rates of Colon Cancer Among African
Americans
African
Americans have the highest incidence rate for colon cancer among U.S.
racial ethnic groups, and the reasons are largely unknown. The North Carolina
Colon Cancer Study, which is a large case-control study with similar numbers
of African Americans and whites, provides a unique opportunity to search
for clues. Jessie Satia-Abouta, Ph.D., and Robert Sandler, M.D.,
M.P.H., of the University of North Carolina at Chapel Hill, and colleagues
found that total energy intake consistently was positively associated
with increased risk for colon cancer for both whites and African Americans.
However, associations with individual macronutrients (fat, carbohydrate,
protein) varied somewhat by race and adjustment for energy intake.
For African Americans, saturated fat was associated with increased risk
for colon cancer when risk estimates were not adjusted for total energy
intake, and dietary fiber was statistically significantly associated with
reduced risk both with and without adjustment for total energy intake.
These findings, coupled with those from an earlier study specific to African
Americans, suggest that a high-fiber, low saturated fat diet may decrease
risk for colon cancer for this group. For whites, when risk estimates
were not adjusted for total energy, high intakes of total energy and most
macronutrients were positively associated with increased risk for colon
cancer, but the associations largely disappeared when total energy was
taken into account. Alcohol intake was not associated with increased risk
for colon cancer in either racial group.
In other analyses on this study population, vitamins E and C from food
sources were associated with a reduction in risk for colon cancer among
African Americans when comparing individuals with intake in the highest
quartile to those in the lowest quartile. Beta-carotene, vitamin C, and
calcium were associated with a reduction in risk for colon cancer among
whites when comparing individuals in the highest to the lowest quartile.
This research suggests that micronutrients may be independently associated
with 30-70 percent reductions in risk for colon cancer in the two groups.
Satia-Abouta J, Galanko JA, Potter JD, Ammerman A,
Martin CF, Sandler RS; North Carolina Colon Cancer Study. Associations
of total energy and macronutrients with colon cancer risk in African
Americans and Whites: results from the North Carolina Colon Cancer Study.
Am J Epidemiol 2003 Nov 15;158(10):951-62.
Satia-Abouta J, Galanko JA, Martin CF, Potter JD, Ammerman
A, Sandler RS. Associations of micronutrients with Colon Cancer risk
in African Americans and whites: results from the North Carolina Colon
Cancer Study. Cancer Epidemiol Biomarkers Prev 2003 Aug;12(8):747-54.
The Dietary Folate and Lung Cancer Connection Explored
Folate
deficiency increasingly is believed to be associated with altered DNA
methylation and synthesis and disruption of DNA repair, which might explain
reports of a link between folate deficiency and risk of different types
of cancer. Qingyi Wei, M.D., Ph.D., and Margaret Spitz, M.D.,
M.P.H., of The University of Texas M.D. Anderson Cancer Center, and
colleagues found low dietary intake of folate to be associated with suboptimal
DNA repair capability (as measured by the host cell reactivation assay).
Studying a cancer-free population, they found that individuals in the
lowest tertile of dietary folate intake had a greater reduction in DNA
repair capability than those in the upper tertile of intake. The association
also was more pronounced in individuals who did not use folate supplements
than in those who did.
In other research, Hongbing Shen, Ph.D., Dr. Spitz, and colleagues found
that dietary folate may protect against lung cancer in an analysis of
data on 470 lung cancer patients who were former smokers and 472 former
smoker controls. Former smokers were studied to avoid confounding bias
from smoking. There was an inverse dose-response relationship between
increasing intake of dietary folate and decreased risk of lung cancer.
The association was especially apparent among those who drank alcoholic
beverages, were former heavy smokers, reported having a family history
of lung cancer, and those who did not take folate supplements. Dietary
folate intake above the control median level was associated with a 40
percent decreased risk of lung cancer. If confirmed by other studies,
the findings could have important public health implications for use of
folate supplements or diet modification to increase intake of the vitamin
in at-risk populations.
Wei Q, Shen H, Wang LE, Duphorne CM, Pillow PC, Guo
Z, Qiao Y, Spitz MR. Association
between low dietary folate intake and suboptimal cellular DNA repair
capacity. Cancer Epidemiol Biomarkers Prev 2003 Oct;12(10):963-9.
Shen H, Wei Q, Pillow PC, Amos CI, Hong WK, Spitz MR.
Dietary
folate intake and lung cancer risk in former smokers: A case-control
analysis. Cancer Epidemiol Biomarkers Prev 2003 Oct;12(10):980-6.
DNA Repair Gene Polymorphisms and Cigarette Smoking Interaction Found
David
Christiani, M.D., of Harvard School of Public Health, and colleagues
have published the first report demonstrating gene-smoking interaction
between the joint effects of the DNA repair genes XRCC1 and ERCC2
and cumulative cigarette smoking exposure in risk for lung cancer. The
magnitudes of these interactions appear to be associated with the number
of variant alleles of the ERCC2 polymorphisms Asp312ASN
and Lys751Gln and the XRCC1 Arg399Gln polymorphism.
How cigarette smoking changes the DNA repair capability of the polymorphisms
is not known.
Zhou W, Liu G, Miller DP, Thurston SW, Xu LL, Wain
JC, Lynch TJ, Su L, Christiani DC. Polymorphisms in the DNA repair genes
XRCC1 and ERCC2, smoking, and lung cancer risk. Cancer Epidemiol
Biomarkers Prev 2003 Apr;12(4):359-65.
XPA Polymorphism Associated With Decreased Risk for Lung Cancer
Margaret Spitz, M.D., M.P.H., of the University of Texas M.D.
Anderson Cancer Center (pictured
elsewhere on the page), and colleagues have shown that an XPA
polymorphism modulates nucleotide excision repair (NER) capacity and is
associated with decreased risk for lung cancer, particularly among ever
smokers. Individuals with the AG
substitution in the 5-end
of the non-coding region had a reduced risk of lung cancer. This pattern
was statistically significant for Caucasians and Mexican Americans, but
not for African Americans.
Wu X, Zhao H, Wei Q, Amos CI, Zhang K, Guo Z, Qiao
Y, Hong WK, Spitz MR. XPA polymorphism associated with reduced lung
cancer risk and a modulating effect on nucleotide excision repair capacity.
Carcinogenesis 2003 Mar;24(3):505-9.
GST Detoxifying Gene Variant Linked to Lung Cancer in Men, Younger
Individuals
Research
suggests that polymorphisms of glutathion transferases (GST), which
are involved in detoxification of carcinogens, may alter the ability to
detoxify and increase risk for certain cancers. Research by Xifeng
Wu, M.D., Ph.D., and Margaret Spitz, M.D., M.P.H., of the University
of Texas M.D. Anderson Cancer Center, and colleagues indicates that the
GSTP1 exon 6 polymorphism is associated with increased risk for
lung cancer especially in men, younger individuals, and ever smokers.
This finding suggests that having the polymorphism may be an important
genetic susceptibility factor. The scientists did not find that the exon
5 polymorphism, which also has been implicated in lung cancer, to be associated
with increased risk for the disease.
Wang Y, Spitz MR, Schabath MB, Ali-Osman F, Mata H,
Wu X. Association between glutathione S-transferase p1polymorphisms
and lung cancer risk in Caucasians: a case-control study. Lung Cancer
2003 Apr;40(1):25-32.
Sunlight-Induced DNA Damage Associated With Increased Risk for Melanoma
Qingyi
Wei, M.D., Ph.D., of the University of Texas M.D. Anderson Cancer
Center, and colleagues have found that reduced DNA repair capability caused
by ultraviolet light is associated with increased risk for melanoma. They
also found a dose-response relationship between the DNA damage and risk
for melanoma. This hospital-based case-control study is the largest and
first epidemiologic study to show that reduced DNA repair capability may
play a role in causation of sunlight-induced melanoma. Sunlight exposure,
particularly intermittent bursts of exposure early in life, is directly
associated with risk for melanoma. A relatively small proportion of individuals
exposed to sunlight develop melanoma, however, suggesting that genetic
susceptibility plays a role in causation of the cancer.
Wei Q, Lee JE, Gershenwald JE, Ross MI, Mansfield PF,
Strom SS, Wang LE, Guo Z, Qiao Y, Amos CI, Spitz MR, Duvic M. Repair
of UV light induced DNA damage and risk of cutaneous malignant melanoma.
J Natl Cancer Inst 2003 Feb 19;95(4):308-15
Some Medications Associated With Decreased Risk of Non-Hodgkin's Lymphoma
The
incidence of non-Hodgkin's lymphoma has been increasing steadily worldwide,
and little is known about risk factors for the disease. Some studies have
suggested that certain medications may have a protective effect against
the cancer, but drug exposures were assessed in different ways in the
studies. In research drawing upon the drug-dispensing records from community
pharmacies and hospital records in the Netherlands, Elizabeth Holly,
Ph.D., M.P.H., of the University of California at San Francisco, and
colleagues report an inverse relationship between occurrence of non-Hodgkin's
lymphoma and use of antihistamine medications (histamine2
blockers) and analgesics among women. They also found reductions in risk
among women that were not statistically significant and may have been
due to chance for other drugs studied. However, the inverse associations
tended to increase with increasing duration of use of the drugs, suggesting
reason for further study. The other drugs studied included nonsteroidal
anti-inflammatory drugs, cholesterol-lowering drugs, and antibiotics.
Beiderbeck AB, Holly EA, Sturkenboom MC, Coebergh JW,
Stricker BH, Leufkens HG. Prescription medications associated with a
decreased risk of non-Hodgkin's lymphoma. Am J Epidemiol 2003
Mar 15;157(6):510-6.
A Y Chromosome May Play Role in Risk of Prostate Cancer Among Asians
Silvia Paracchini, Ph.D., of the University of Oxford, Laurence Kolonel,
M.D., Ph.D., of the University of Hawaii, and Brian Henderson,
M.D., of the University of Southern California at Los Angeles, and
colleagues investigated the role of the Y chromosome in prostate cancer
in a case-control study nested within the Multiethnic Cohort Study. The
analysis included data on 930 prostate cancer cases and 1,208 controls.
The men were African American, white, Latino, and Japanese. Only the Y
lineage O3, which was present almost exclusively in the Japanese study
participants, was associated with a 63 percent increased risk of prostate
cancer. The risk was modified by age and severity of disease. Japanese
men under age 65 who had the Y lineage O3 had nearly a fourfold increased
risk of developing severe prostate cancer. If studies of other Japanese
or Asian populations yield similar findings, the scientists suggest that
a systematic evaluation of the genetic changes in this lineage is warranted.
(Drs. Kolonel and Henderson
are pictured elsewhere on the page.)
Paracchini S, Pearce CL, Kolonel LN, Altshuler D, Henderson
BE, Tyler-Smith C. A
Y chromosomal influence on prostate cancer risk: The multi-ethnic cohort
study. J Med Genet 2003 Nov;40(11):815-9.
New Clues Found on Genetic Susceptibility for Aggressive Prostate Cancer
A
variety of genetic epidemiologic studies are investigating how better
to identify men at risk for aggressive prostate cancer. These studies
have important implications for improving diagnosis and treatment, and
for identifying ways to prevent the disease. Previous research has suggested
that chromosome 19q harbors a gene for aggressiveness of prostate cancer.
Research by Stephen Thibodeau, Ph.D., of the Mayo Clinic, and colleagues
confirms this finding and provides strong evidence of the association.
The scientists analyzed genome scan data from men in 161 families among
whom there was a family history of prostate cancer. The study also suggested
that chromosome 4q may be involved in tumor aggressiveness.
In
other research, Sara Strom, Ph.D., of the University of Texas M.D.
Anderson Cancer Center, and colleagues found that the presence of a certain
allele was strongly associated with younger age at diagnosis of prostate
cancer. This "A" allele of the cell cycle regulating gene cyclin
D1 also has been associated with early onset colorectal cancer and poorer
prognosis for lung cancer. Still other research by Richard Everson,
M.D., Ph.D., of Wayne State University, and colleagues indicates that
certain polymorphisms in the androgen receptor and in genes that influence
androgen metabolism are associated with increased risk for being diagnosed
with prostate cancer and with more aggressive disease.
Slager SL, Schaid DJ, Cunningham JM, McDonnell SK,
Marks AF, Peterson BJ, Hebbring SJ, Anderson S, French AJ, Thibodeau
SN. Confirmation of linkage of prostate cancer aggressiveness with chromosome
19q. Am J Hum Genet 2003 Mar;72(3):759-62.
Sanchez-Ortiz RF, Yamamura Y, Frazier ML, Babalan RJ,
Troncoso P, Pettaway CA, Strom S. Relationship between cyclin D1 polymorphism
and age at diagnosis of prostate cancer. Proc Annu Meet Am Assoc
Cancer Res 2003.
Powell IJ, Land SJ, Zhou J, Sun Y, Dey J, Patel NP,
Sakr WA, Hughes MR, Everson RB. Influence of androgen receptor and androgen
metabolism polymorphisms on prostate cancer prognosis after prostactectomy
in an ethnically diverse population. Proc Annu Meet Am Assoc Cancer
Res 2003.
The Hunt for Prostate Cancer Susceptibility Genes Proves Difficult
Despite
strong evidence for the existence of prostate cancer susceptibility genes,
the search for such genes has been frustrating. The International Consortium
for Prostate Cancer Genetics (ICPCG) demonstrates how difficult this research
has been in a review of eight genome-wide linkage searches for chromosomal
regions associated with development of the cancer. The ICPCG, with William
Isaacs, Ph.D., of Johns Hopkins University as principal investigator,
is funded through a grant from EGRP.
The review was based on 1,293 families with multiple cases of prostate
cancer, but even with these numbers, no chromosomal region was found to
be especially promising. Eleven linkage peaks with LOD scores in excess
of 2 were identified, but no chromosomal region was reported as significant
at this level by more than one study. Further, only one of these linkage
peaks corresponded to a peak previously suggested by another group.
The ICPCG's review shows that prostate cancer is genetically complex,
and that combined analyses of large family sets will be needed to evaluate
reliably the linkage evidence. The consortium plans such analyses with
a combined dataset on more than 2,000 families, which will provide the
statistical power to detect genes of much smaller effect, and allow a
more reliable evaluation of subsets based on family history, disease aggressiveness,
and co-occurrence of other types of cancer.
Easton DF, Schaid DJ, Whittemore AS, Isaacs WJ. Where
are the prostate cancer genes? A summary of eight genome wide
searches. Prostate 2003 Dec 1;57(4):261-9.
Mononucleosis Related to Epstein-Barr Virus and Risk for Hodgkin's Lymphoma
Infectious
mononucleosis related to infection with Epstein-Barr virus (EBV) is associated
with an increased risk for Hodgkin's lymphoma in young adults. This finding
is from a study of more than 60,000 young adults in two Danish cohorts
of patients who tested positive for infectious mononucleosis. Mads
Melbye, M.D., Ph.D., of the Statens Serum Institut in Copenhagen,
and colleagues found no evidence of an increased risk of EBV-negative
Hodgkin's lymphoma following infectious mononucleosis. However, there
was a 4-fold increased risk of EBV-positive Hodgkin's lymphoma after infectious
mononucleosis. The estimated median incubation time from mononucleosis
to diagnosis of EBV-positive Hodgkin's lymphoma was 4.1 years.
This study makes a convincing connection among infectious mononucleosis,
EBV, and the development of Hodgkin's disease. The risk of Hodgkin's disease
after infectious mononucleosis is low about 1 case per 1,000 persons
with EBV-related mononucleosis, suggesting that other co-factors are involved.
Hjalgrim H, Askling J, Rostgaard K, Hamilton-Dutoit
S, Frisch M, Zhang JS, Madsen M, Rosdahl N, Konradsen HB, Storm HH,
Melbye M. Characteristics of Hodgkin's lymphoma after infectious mononucleosis.
N Engl J Med 2003 Oct 2;349(14):1324-32.
Explanation Found for HPV 16's Strong Association With Cervical Cancer
Human
papillomavirus (HPV) 16, which is responsible for about one-half of all
cervical cancers, appears to be more successful in escaping immune surveillance
than other HPV types. The findings may explain why HPV 16 plays a major
role in causing cervical cancer. Howard Strickler, M.D., M.P.H.,
of the Albert Einstein College of Medicine, and colleagues compared the
prevalence and incidence of different HPV types among HIV-positive women
who had varying levels of T cells, an indicator of immune status.
Strickler HD, Palefsky JM, Shah KV, Anastos K, Klein
RS, Minkoff H, Duerr A, Massad LS, Celentano DD, Hall C, Fazzari M,
Cu-Uvin S, Bacon M, Schuman P, Levine AM, Durante AJ, Gange S, Melnick
S, Burk RD. Human papillomavirus type 16 and immune status in human
immunodeficiency virus-seropositive women. J Natl Cancer Inst
2003 Jul 16;95(14):1062-71.
Oncogenic Human Papilloma Virus Infection and Progression to Cervical
Cancer
Precursor
lesions of the cervix detected by cytology persist longer and are more
likely to progress in women who have oncogenic types of human papilloma
virus infections (HPV) than in women with non-oncogenic types of HPV infections
or in uninfected women. These findings reported by Eduardo Franco,
Dr.P.H., of McGill University, and colleagues, suggest that testing
for HPV in women who have abnormal PAP smears may help identify patients
who would benefit from more intensive follow-up and chemopreventive treatment.
Other patients might be followed at longer intervals and potentially could
avoid invasive diagnostic and therapeutic procedures.
Schlecht NF, Platt RW, Duarte-Franco E, Costa MC, Sobrinho
JP, Prado JC, Ferenczy A, Rohan TE, Villa LL, Franco EL. Human papillomavirus
infection and time to progression and regression of cervical intraepithelial
neoplasia. J Natl Cancer Inst 2003 Sep 3;95(17):1336-43.
Clinic-Based Study Designs Give More Accurate Estimates of Penetrance
Alice
Whittemore, Ph.D., and Gail Gong, Ph.D., of Stanford University School
of Medicine, used computer simulations to compare the performance of two
study designs based on family data for estimating the disease risk associated
with mutations of known disease-susceptibility genes. The scientists found
that clinic-based designs, where families are ascertained because they
meet certain criteria for multiple disease occurrence in the family, yielded
more accurate estimates than did population-based designs, where families
are sampled through population-based registries of affected individuals.
The reason may be that clinic-based designs include more identified mutation
carriers. The study was conducted with assistance from the EGRP-funded
Cancer Family Registries.
Gong G, Whittemore AS. Optimal designs for estimating
penetrance of rare mutations of a disease susceptibility gene. Genet
Epidemiol 2003 Apr;24(3):173-80.
Research Methods
|
Two papers on research methods may be of interest to epidemiologists:
- University of Southern California at Los Angeles scientists
Daniel Stram, Ph.D., and Brian Henderson, M.D.
(pictured elsewhere on the page),
and colleagues outline issues involved in choosing a method of
estimating haplotype-specific risk estimates from genotype data
for case-control studies of unrelated individuals.
- The EGRP-funded Cancer Genetics Network (CGN)
has published a paper describing recruitment results and pilot
studies from this resource for researchers.
Stram DO, Leigh Pearce C, Bretsky P, Freedman
M, Hirschhorn JN, Altshuler D, Kolonel LN, Henderson BE, Thomas
DC. Modeling
and E-M estimation of haplotype-specific relative risks from
genotype data for a case-control study of unrelated individuals.
Hum Hered 2003;55(4):179-90.
Anton-Culver H, Ziogas A, Bowen D, Finkelstein
D, Griffin C, Hanson J, Isaacs C, Kasten-Sportes C, Mineau G,
Nadkarni P, Rimer B, Schildkraut J, Strong L, Weber B, Winn
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