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DOI10.1096/fj.12-225060
Dynamic changes in fetal Leydig cell populations influence adult Leydig cell populations in mice
Barsoum, Ivraym B.1; Kaur, Jaspreet1; Ge, Renshan S.2; Cooke, Paul S.1,3; Yao, Humphrey Hung-Chang1,4
通讯作者Yao, Humphrey Hung-Chang
来源期刊FASEB JOURNAL
ISSN0892-6638
EISSN1530-6860
出版年2013
卷号27期号:7页码:2657-2666
英文摘要

Testes contain two distinct Leydig cell populations during development: fetal and adult Leydig cells (FLCs and ALCs, respectively). ALCs are not derived from FLCs, and it is unknown whether these two populations share common progenitors. We discovered that hedgehog (Hh) signaling is responsible for transforming steroidogenic factor 1-positive (SF1(+)) progenitors into FLCs. However, not all SF1(+) progenitors become FLCs, and some remain undifferentiated through fetal development. We therefore hypothesized that if FLCs and ALCs share SF1(+) progenitors, increased Hh pathway activation in SF1(+) progenitor cells could change the dynamics and distribution of SF1(+) progenitors, FLCs, and ALCs. Using a genetic model involving constitutive activation of Hh pathway in SF1(+) cells, we observed reduced numbers of SF1(+) progenitor cells and increased FLCs. Conversely, increased Hh activation led to decreased ALC populations prepubertally, while adult ALC numbers were comparable to control testes. Hence, reduction in SF1(+) progenitors temporarily affects ALC numbers, suggesting that SF1(+) progenitors in fetal testes are a potential source of both FLCs and ALCs. Besides transient ALC defects, adult animals with Hh activation in SF1(+) progenitors had reduced testicular weight, oligospermia, and decreased sperm mobility. These defects highlight the importance of properly regulated Hh signaling in Leydig cell development and testicular functions.Barsoum, I. B., Kaur, J. Ge, R. S., Cooke, P. S., Yao, H. H.-C. Dynamic changes in fetal Leydig cell populations influence adult Leydig cell populations in mice.


英文关键词hedgehog pathway spermatogenesis steroidogenic factor 1 testis
类型Article
语种英语
国家USA
收录类别SCI-E
WOS记录号WOS:000328841000015
WOS关键词HEDGEHOG DHH GENE ; DESERT-HEDGEHOG ; MOUSE TESTIS ; GONADAL-DYSGENESIS ; PROGENITOR CELLS ; SERTOLI-CELLS ; DIFFERENTIATION ; IDENTIFICATION ; MUTATION ; PROLIFERATION
WOS类目Biochemistry & Molecular Biology ; Biology ; Cell Biology
WOS研究方向Biochemistry & Molecular Biology ; Life Sciences & Biomedicine - Other Topics ; Cell Biology
资源类型期刊论文
条目标识符http://119.78.100.177/qdio/handle/2XILL650/177108
作者单位1.Univ Illinois, Coll Vet Med, Dept Comparat Biosci, Urbana, IL USA;
2.Populat Council, New York, NY 10021 USA;
3.Univ Florida, Coll Vet Med, Dept Physiol Sci, Gainesville, FL 32610 USA;
4.NIEHS, Dev Reprod Biol Grp, Lab Reprod & Dev Toxicol, NIH, Res Triangle Pk, NC 27709 USA
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Barsoum, Ivraym B.,Kaur, Jaspreet,Ge, Renshan S.,et al. Dynamic changes in fetal Leydig cell populations influence adult Leydig cell populations in mice[J],2013,27(7):2657-2666.
APA Barsoum, Ivraym B.,Kaur, Jaspreet,Ge, Renshan S.,Cooke, Paul S.,&Yao, Humphrey Hung-Chang.(2013).Dynamic changes in fetal Leydig cell populations influence adult Leydig cell populations in mice.FASEB JOURNAL,27(7),2657-2666.
MLA Barsoum, Ivraym B.,et al."Dynamic changes in fetal Leydig cell populations influence adult Leydig cell populations in mice".FASEB JOURNAL 27.7(2013):2657-2666.
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