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16 April 2014 Regulation of the Proliferation and Differentiation of Leydig Stem Cells in the Adult Testis
Hana M. Odeh, Colin Kleinguetl, Renshan Ge, Barry R. Zirkin, Haolin Chen
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Abstract

We reported previously that stem cells associated with adult rat testis seminiferous tubules are able to give rise to differentiated Leydig cells in vitro. The regulatory mechanisms by which they do so, however, are uncertain. Herein, we hypothesized that the proliferation and differentiation of Leydig cell stem cells (stem Leydig cells, SLCs) depend upon locally produced factors from the seminiferous tubules. Microarray analysis revealed that platelet-derived growth factor receptor alpha (PDGFRalpha) is up-regulated and PDGFRbeta is down-regulated with postnatal differentiation of SLCs. This suggested that their ligands, PDGF-AA and PDGF-BB, respectively, might have important roles in SLC proliferation and differentiation. To test this, we developed a unique in vitro culture system in which SLCs proliferate on the surfaces of cultured seminiferous tubules largely during Week 1 of culture and their progeny subsequently differentiate to testosterone-forming Leydig cells during Weeks 2 through 4. Using this system, seminiferous tubules from adult rat testes were cultured with PDGF-AA or PDGF-BB for up to 4 wk. Both ligands stimulated SLC proliferation during the first week of culture, with PDGF-BB significantly more potent than PDGF-AA. Furthermore, PDGF-AA had a stimulatory effect on SLC differentiation from Weeks 2 through 4 of culture. In contrast, PDGF-BB, which stimulated cell proliferation during Week 1, had a significant inhibitory effect on differentiation during Weeks 2 through 4. These findings, made possible by the development of the seminiferous tubule culture system, reveal distinct roles by locally produced PDGFs in SLC regulation.

Hana M. Odeh, Colin Kleinguetl, Renshan Ge, Barry R. Zirkin, and Haolin Chen "Regulation of the Proliferation and Differentiation of Leydig Stem Cells in the Adult Testis," Biology of Reproduction 90(6), (16 April 2014). https://doi.org/10.1095/biolreprod.114.117473
Received: 8 January 2014; Accepted: 1 March 2014; Published: 16 April 2014
KEYWORDS
Leydig cells
PDGF
stem cells
testosterone
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