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AbstractW and Steel mutant mice exhibit similar developmental defects in melanogenesis, haematopoiesis, and gametogenesis. Consistent with the cell autonomous and microenvironmental nature of W and Sl mutations, respectively, W encodes the c‐kit receptor tyrosine kinase while Steel enclodes the Kit ligand. Both c‐kit and Steel are expressed in various cells in which no corresponding mutant phenotype has yet been demonstrated. In the adult ovary, certain stromal‐derived cells (theca and interstitial), as well as oocytes, express c‐kit, while granulosa cells express Steel. We show here that the cessation of oocyte growth, at the transition of the follicle to the antral stage, is associated with the cessation of Steel expression in the cumulus granulosa cells in the vicinity of the oocyte. These observations suggest a role for the Kit signaling pathway in oocyte growth or in meiotic arrest. In addition, the cyclic secretion of luteinizing hormone immediately and dramatically results in elevated Steel expression in mural granulosa cells and decreased levels of c‐kit transcripts in stromal‐derived cells. This influence of the estrous reproductive cycle on c‐kit/Steel expression suggests that the Kit signaling pathway, in addition to its previously described role in primordial germ cell development, is involved in follicular development in the adult female. © 1993 Wiley‐Liss, Inc.

Original publication

DOI

10.1002/aja.1001970107

Type

Journal article

Journal

Developmental Dynamics

Publisher

Wiley

Publication Date

05/1993

Volume

197

Pages

69 - 79