Author:
Fraser Hamish M.,Wulff Christine
Abstract
The ovary is distinctive in undergoing cyclic changes in angiogenesis that
play a critical role in the normal functioning of the female reproductive
system. The current paper describes the use of the marmoset monkey as an
in vivo model in which the cellular and molecular
regulation of angiogenesis in the ovary can be investigated and the effects of
manipulation of angiogenic factors elucidated. The studies are based on
quantifying changes in blood vessel area and endothelial cell proliferation,
monitoring changes in expression patterns of putative angiogenic regulatory
factors and targeting these factors by antagonists
in vivo. Quantification of endothelial cell
proliferation shows that angiogenesis commences in the pre-antral follicle,
increases with follicular development and becomes intense in the early corpus
luteum. Vascular endothelial growth factor (VEGF), a principal angiogenic
factor, is synthesized by the developing follicle and corpus luteum.
Administration of specific antagonists in vivo for
selected periods of the ovulatory cycle shows that inhibition of VEGF results
in a marked decrease in endothelial cell proliferation in the follicle and is
accompanied by a decline in granulosa cell proliferation. Inhibition during
the early or mid-luteal phase results in a marked suppression in luteal
angiogenesis, failure of development of the microvascular tree and suppression
of luteal function. Manipulation of angiogenesis should be a novel approach to
either promoting or inhibiting the normal processes of folliculogenesis,
ovulation and corpus luteum function.
Subject
Developmental Biology,Endocrinology,Genetics,Molecular Biology,Animal Science and Zoology,Reproductive Medicine,Biotechnology
Cited by
69 articles.
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