Menon Usha ; Karpinskyj Chloe, Aleksandra Gentry-Maharaj;
Ovarian Cancer Prevention and Screening Obstetrics
& Gynecology. 131(5):909–927, MAY 2018
DOI: 10.1097/AOG.0000000000002580
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Abstract
There has been much progress in ovarian cancer screening and prevention
in recent years. Improved tools that combine genetic and epidemiologic factors
to predict an individual's ovarian cancer risk are set to become available for
tailoring preventive and screening approaches. The increasing evidence on tubal
origins of a proportion of ovarian cancer has paved the way to use of
opportunistic bilateral salpingectomy at tubal ligation and hysterectomy in the
general population. Clinical trials are in progress to estimate the long-term
effects on endocrine function. In women at high risk, risk reducing
salpingo-oophorectomy remains the standard of care with the current focus on
management of resulting noncancer outcomes, especially sexual dysfunction in
younger women. This has led to evaluation of early bilateral salpingectomy and
delayed oophorectomy in this population. Meanwhile, modeling suggests
that BRCA mutation carriers should consider using the oral
contraceptive pill for chemoprevention. In the general population, the largest
ovarian cancer screening trial to date, the UK Collaborative Trial of Ovarian
Cancer Screening reported a stage shift with annual multimodal screening using
the longitudinal CA 125 Risk of Ovarian Cancer Algorithm but not with annual
transvaginal ultrasound screening. There was no definitive mortality reduction
with either screening strategy compared with no screening. Further follow-up
until December 2018 in now underway. Stage shift and higher rates of optimal
cytoreduction were also reported during 3- to 4-monthly multimodal screening in
the United Kingdom and U.S. high-risk screening trials. Although all agree that
there is not yet evidence to support general population screening,
recommendations for high-risk screening vary between countries. A key finding
from the screening trials has been the better performance of longitudinal
algorithms compared with a single cutoff for CA 125. A major focus of ovarian
cancer biomarker discovery work has been tumor DNA markers in both plasma and
novel specimens such
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