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Blogger's Note: does not relate to Lynch Syndrome women; for those who have had an interest in and/or followed the WHI trial and subsequent analyses; when the initial WHI trial was publicized very little attention was paid to this particular aspect (eg. estrogen/hrt/risk reduction); debatable if and/or when 'we' will ever get to an analysis in affected Lynch Syndrome women (eg. low numbers etc.)
abstract
"Worldwide, colorectal cancer has a higher
incidence rate in men than in women, suggesting a protective role for
sex hormones
in the development of the disease. Preclinical data
support a role for estrogen and its receptors in the initiation and
progression
of colorectal cancer and establishes that
protective effects of estrogen are exerted through ERβ. Hormone
replacement therapy
(HRT) in postmenopausal women as well as
consumption of soy reduces the incidence of colorectal cancer. In the
Women's Health
Initiative trial, use of HRT in postmenopausal
women reduced the risk of colon cancer by 56% [95% confidence interval
(CI),
0.38–0.81; P = 0.003]. A recent meta-analysis showed that in women, consumption of soy reduced the risk of colon cancer by 21% (95% CI,
0.03–0.35; P = 0.026). In this review,
using the preclinical data, we translate the findings in the clinical
trials and observational
studies to define the role of estrogen in the
prevention of colorectal cancer. We hypothesize that sometime during the
tumorigenesis
process ERβ expression in colonocytes is lost and
the estrogen ligand, HRT, or soy products, exerts its effects through
preventing
this loss. Thus, in the adenoma-to-carcinoma
continuum, timing of HRT is a significant determinant of the observed
benefit
from this intervention. We further argue that the
protective effects of estrogen are limited to certain molecular
subtypes.
Successful development of estrogen modulators for
prevention of colorectal cancer depends on identification of susceptible
colorectal cancer population(s). Thus, research to
better understand the estrogen pathway is fundamental for clinical
delivery
of these agents."
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