Breast Cancer Clinical Trial
Official title:
Bone Mineral Density and Subsequent Cancer Risk
Recent cohort studies demonstrated reduced breast cancer risks among women with a history of
fractures or low bone mineral density (BMD). In the Study of Osteoporotic Fractures, each
standard deviation increase in distal radius BMD was associated with a 50% increased risk
over three years of follow-up, while in the Framingham study, women in the highest quartile
of metacarpal bone mass had a 3.5-fold higher risk than women in the lowest quartile. The
impact of the severity and timing of bone loss on risk has not yet been investigated, and the
extent to which other risk factors (family history, anthropometric factors, physical
activity, and exogenous hormones) modify the relationship with BMD is unknown.
To elaborate on these research questions, we are conducting a follow-up study of 22,695
postmenopausal women who volunteered for the Fracture Intervention Trial (FIT), a trial of
the bone-enhancing drug alendronate. This large cohort includes extensive baseline
information on major breast cancer risk factors, and thus is ideal for evaluating potential
interactions with BMD and the effects of BMD on other cancer sites. Endometrial cancer has
been reported to occur more frequently among women with a history of fracture, but no
previous studies have specifically investigated its relationship to BMD.
We are investigating whether BMD of the proximal femur predicts breast cancer risk; whether
breast cancer risk factors among postmenopausal women modify the relationship with BMD;
whether BMD predicts endometrial or other cancers; and whether measurable biomarkers offer
further etiologic clues about BMD and cancer risk.
We have contacted the surviving members of FIT to ascertain incident cancers. Risk factors
and fracture history are being updated through a self-administered questionnaire. To
supplement the serum samples collected at baseline, we are using a nested case-control study
approach to collect buccal cell specimens, which may be useful for measuring a variety of
biomarkers, including endogenous hormones and genetic polymorphisms involved in either bone
growth (e.g., vitamin D receptor) or hormone metabolism (e.g., CYP17, COMT). Retrieval of
operative and pathology reports is being used to validate self-reported cancers. The social
security numbers and contacts names provided by FIT participants when they completed the
baseline questionnaire are facilitating comprehensive follow-up and a National Death Index
search for those who cannot be located. The baseline data, the established cooperation of
this study population, and the collection of additional biospecimens should enable this study
to answer important questions about BMD in breast and endometrial cancers.
Recent cohort studies demonstrated reduced breast cancer risks among women with a history of
fractures or low bone mineral density (BMD). In the Study of Osteoporotic Fractures, each
standard deviation increase in distal radius BMD was associated with a 50% increased risk
over three years of follow-up, while in the Framingham study, women in the highest quartile
of metacarpal bone mass had a 3.5-fold higher risk than women in the lowest quartile. The
impact of the severity and timing of bone loss on risk has not been investigated, and the
extent to which other risk factors (family history, lifestyle, and exogenous hormones) modify
the relationship with BMD is unknown.
To elaborate on these research questions, we conducted a follow-up study of postmenopausal
women who volunteered for the Fracture Intervention Trial (FIT), a trial of the
bone-enhancing drug alendronate. The BFIT follow-up study includes 15,595 of the 22,695 FIT
volunteers. Surviving members of FIT were contacted to ascertain incident cancers and to
provide updated risk factor and fracture history through a self-administered questionnaire.
To supplement baseline serum samples, we used a nested case-control approach to collect
buccal cell specimens for biomarker measurement, including endogenous hormones and genetic
polymorphisms involved in either bone growth (e.g., vitamin D receptor) or hormone metabolism
(e.g., CYPI7, COMT). Operative and pathology reports were used to validate self-reported
cancers. The social security numbers and contact names provided by FIT participants at
baseline facilitated comprehensive follow-up and a National Death Index search for those who
could not be located.
This large cohort includes extensive baseline information on major breast cancer risk
factors, and thus is ideal for evaluating potential interactions with BMD and the effects of
BMD on other cancer sites. Endometrial cancer has been reported to occur more frequently
among women with a history of fracture, but no previous studies have investigated its
relationship to BMD. We are investigating whether proximal femur BMD predicts breast cancer
risk; whether breast cancer risk factors among postmenopausal women modify the relationship
with BMD; whether BMD predicts cancer risk; and whether biomarkers offer etiologic clues
about BMD and cancer risk. Currently, we are examining: 1) the relationship of serum
adipocytokines to endometrial cancer risk, and 2) the relationships of serum estrogens and
metabolites to postmenopausal breast cancer risk. The baseline and follow-up data and the
collection of additional biospecimens should enable us to answer important questions about
BMD and other cancers.
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