Activin A Balances Sertoli and Germ Cell Proliferation in the Fetal Mouse Testis

Mendis, Sirisha; Meachem, Sarah J; Sarraj, Mai; Loveland, Kate L

doi:10.1095/biolreprod.110.086231

Cited by 127 publications

(105 citation statements)

References 55 publications

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“…However, in the same study, RA was reported to slightly increase PND3 gonocyte numbers and have no effect on apoptosis. Moreover, activin A and androgen were reported to be negative regulators of fetal gonocyte proliferation, whereas we did not find any effect of testosterone on PND3 gonocyte proliferation in vitro (Merlet et al 2007, Thuillier et al 2010, Mendis et al 2011.…”

Section: Introductioncontrasting

confidence: 86%

Mammalian gonocyte and spermatogonia differentiation: recent advances and remaining challenges

Manku¹,

Culty²

2015

Reproduction

125

105

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The production of spermatozoa relies on a pool of spermatogonial stem cells (SSCs), formed in infancy from the differentiation of their precursor cells, the gonocytes. Throughout adult life, SSCs will either self-renew or differentiate, in order to maintain a stem cell reserve while providing cells to the spermatogenic cycle. By contrast, gonocytes represent a transient and finite phase of development leading to the formation of SSCs or spermatogonia of the first spermatogenic wave. Gonocyte development involves phases of quiescence, cell proliferation, migration, and differentiation. Spermatogonia, on the other hand, remain located at the basement membrane of the seminiferous tubules throughout their successive phases of proliferation and differentiation. Apoptosis is an integral part of both developmental phases, allowing for the removal of defective cells and the maintenance of proper germ-Sertoli cell ratios. While gonocytes and spermatogonia mitosis are regulated by distinct factors, they both undergo differentiation in response to retinoic acid. In contrast to postpubertal spermatogenesis, the early steps of germ cell development have only recently attracted attention, unveiling genes and pathways regulating SSC self-renewal and proliferation. Yet, less is known on the mechanisms regulating differentiation. The processes leading from gonocytes to spermatogonia have been seldom investigated. While the formation of abnormal gonocytes or SSCs could lead to infertility, defective gonocyte differentiation might be at the origin of testicular germ cell tumors. Thus, it is important to better understand the molecular mechanisms regulating these processes. This review summarizes and compares the present knowledge on the mechanisms regulating mammalian gonocyte and spermatogonial differentiation.

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Section: Introductioncontrasting

confidence: 86%

Mammalian gonocyte and spermatogonia differentiation: recent advances and remaining challenges

Manku¹,

Culty²

2015

Reproduction

125

105

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“…In contrast to these findings however, another study concluded that disruption of Activin/Nodal signaling affected fetal germ cell meiosis (although pluripotency was not investigated) (Souquet et al 2012). In that study, Activin/Nodal inhibitors disrupted Nodal signaling in germ cells but also Activin signaling in somatic cells, so it is possible that the observed meiosis is the result of inadvertent disruption of the gonadal environment: Activin is normally required for the induction of germ cell mitotic arrest and differentiation (Mendis et al 2010). Complete Nodal deletion in germ cells may be required to clarify whether the main role of Nodal signaling is to maintain pluripotency or to prevent meiosis.…”

Section: Model Of Nodal Signaling Nodal a Member Of The Tgfb Famimentioning

confidence: 82%

Nodal/Cripto signaling in fetal male germ cell development: implications for testicular germ cell tumors

Spiller

Bowles²,

Koopman

2013

Int. J. Dev. Biol.

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Testicular cancer is the most frequent cancer in young men aged 15-40 years and accounts for 1% of all cancer diagnosed in males. Testicular germ cell tumors (TGCT) encompass a broad group of cancers, each displaying different levels of pluripotency and differentiation as well as malignancy potential. The TGCT cell of origin is thought to be a fetal germ cell that failed to correctly differentiate during development: this is known as the 'fetal origins hypothesis' . This theory predicts that developmental pathways that control germ cell pluripotency or differentiation may be involved in the malignant transformation of these cells. Recently the Nodal/Cripto signaling pathway, known to control pluripotency and differentiation in embryonic stem (ES) cells, was implicated in regulating normal male fetal germ cell pluripotency. Although genes of this pathway are not normally expressed in germ cells during adult life, ectopic expression of this pathway was detected in several sub-groups of TGCTs. In this review, we consider the evidence for the fetal origins of TGCT and discuss the implications of Nodal/Cripto signaling in various aspects of germ cell development and cancer progression.

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“…Multiple Tgfβ superfamily members have also been associated with male germ cell differentiation, including Tgfβ2 (Miles et al, 2013;Moreno et al, 2010) and activin β 5 (InhbaMouse Genome Informatics) (Mendis et al, 2011). These factors repress germ cell proliferation, and participate in the entry into quiescence (Moreno et al, 2010) and probably also in its maintenance (Mendis et al, 2011;Moreno et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

Prostaglandin D2 acts through the Dp2 receptor to influence male germ cell differentiation in the foetal mouse testis

et al. 2014

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Through intercellular signalling, the somatic compartment of the foetal testis is able to program primordial germ cells to undergo spermatogenesis. Fibroblast growth factor 9 and several members of the transforming growth factor β superfamily are involved in this process in the foetal testis, counteracting the induction of meiosis by retinoic acid and activating germinal mitotic arrest. Here, using in vitro and in vivo approaches, we show that prostaglandin D 2 (PGD 2 ), which is produced through both L-Pgds and H-Pgds enzymatic activities in the somatic and germ cell compartments of the foetal testis, plays a role in mitotic arrest in male germ cells by activating the expression and nuclear localization of the CDK inhibitor p21Cip1 and by repressing pluripotency markers. We show that PGD 2 acts through its Dp2 receptor, at least in part through direct effects in germ cells, and contributes to the proper differentiation of male germ cells through the upregulation of the master gene Nanos2. Our data identify PGD 2 signalling as an early pathway that acts in both paracrine and autocrine manners, and contributes to the differentiation of germ cells in the foetal testis.

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Activin A Balances Sertoli and Germ Cell Proliferation in the Fetal Mouse Testis

Cited by 127 publications

References 55 publications

Mammalian gonocyte and spermatogonia differentiation: recent advances and remaining challenges

Mammalian gonocyte and spermatogonia differentiation: recent advances and remaining challenges

Nodal/Cripto signaling in fetal male germ cell development: implications for testicular germ cell tumors

Prostaglandin D2 acts through the Dp2 receptor to influence male germ cell differentiation in the foetal mouse testis

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