A perivascular niche for multipotent progenitors in the fetal testis

Kumar, Deepti Lava; DeFalco, Tony

doi:10.1038/s41467-018-06996-3

Cited by 70 publications

(125 citation statements)

References 69 publications

(128 reference statements)

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“…Multiple interstitial cell (CD90/PDGFRA/CoupTFII/Nes) populations can re-enter the cell cycle upon EDS-induced Leydig cell death. This suggests that the interstitial compartment contains a reserve Leydig or a general somatic cell progenitor population that can be activated in response to damage (Chen et al, 1996;Chen et al, 2010;Davidoff et al, 2004;Ge et al, 2006;Jiang et al, 2014;Kilcoyne et al, 2014;Kumar and DeFalco, 2018;Landreh et al, 2013;Qin et al, 2008). However, whether the reported molecular markers are expressed universally by a single population of Leydig stem cells or by distinct cell populations that all have the ability to regenerate remains difficult to tease apart.…”

Section: Introductionmentioning

confidence: 99%

“…However, whether the reported molecular markers are expressed universally by a single population of Leydig stem cells or by distinct cell populations that all have the ability to regenerate remains difficult to tease apart. This is due to the difficulty of performing single-cell transplantation and reconstitution experiments in the testis and the lack of multiplexed molecular barcoding tools for lineage tracing (Kumar and DeFalco, 2018;Rotgers et al, 2018;Shima et al, 2018). It is also unclear if a common somatic progenitor could give rise to additional cell types that persists in the adult, and what the role of such stem/progenitors would be in the normal adult testis.…”

Section: Introductionmentioning

confidence: 99%

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Tcf21⁺mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Shen

Larose

Shami

et al. 2020

Preprint

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2 Highlights • Multipotent Tcf21 + MPs can differentiate into somatic testis cell types • Tcf21 + cells contribute to testis and ovary somatic cells during gonadal development • Tcf21 + cells replenish somatic cells of the aging testis and in response to tissue injury • Testis Tcf21 cells resemble resident fibroblast populations in multiple organs 3 Summary Testicular development and function relies on interactions between somatic cells and the germline, but similar to other organs, regenerative capacity decline in aging and disease. Whether the adult testis maintains a reserve progenitor population with repair or regenerative capacity remains uncertain. Here, we characterized a recently identified mouse testis interstitial population expressing the transcription factor Tcf21. We found that Tcf21 + cells are bipotential somatic progenitors present in fetal testis and ovary, maintain adult testis homeostasis during aging, and act as reserve somatic progenitors following injury. In vitro, Tcf21 + cells are multipotent mesenchymal progenitors which form multiple somatic lineages including Leydig and myoid cells. Additionally, Tcf21 + cells resemble resident fibroblast populations reported in other organs having roles in tissue homeostasis, fibrosis, and regeneration. Our findings reveal that the testis, like other organs, maintains multipotent mesenchymal progenitors that can be leveraged in development of future therapies for hypoandrogenism and/or infertility.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Tcf21⁺mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Shen

Larose

Shami

et al. 2020

Preprint

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“…Previous studies demonstrated that FLCs were developed from stem Leydig cells [8,24]. Stem Leydig cells in the fetal testis are spindle-shaped and express NR2F2, also called COUP-TFII [8,[24][25][26]. We used NR2F2 as the biomarker to identify the stem Leydig cell and SOX9 as the biomarker to draw a boundary for the seminiferous cord.…”

Section: Measurement Of Stem Leydig Cell Numbermentioning

confidence: 99%

Gestational vinclozolin exposure suppresses fetal Leydig cell development in rats

Pan

et al. 2020

Preprint

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Background: Vinclozolin is not only a common dicarboximide fungicide used to protect crops against diseases but also an endocrine disruptor. This study aimed to investigate the effects of gestational vinclozolin exposure on the development of rat fetal Leydig cells.Methods: Female pregnant Sprague-Dawley rats were exposed to vinclozolin (0, 25, 50, and 100 mg/kg body weight/day) by oral gavage from gestational day 14 to 21.Results: Vinclozolin dose-dependently depressed serum testosterone levels at doses of 50 and 100 mg/kg and anogenital distance at 100 mg/kg. RNA-seq, qPCR, and Western blot showed that vinclozolin down-regulated the expression of Nr5a1 , Sox9 , Lhcgr , Cyp11a1 , Hsd3b1 , Hsd17b3 , Amh , Pdgfa , and Dhh and their encoded proteins. Vinclozolin depressed NR2F2-positive stem Leydig cell number at a dose of 100 mg/kg and also enhanced autophagy in the testis.Conclusion: Vinclozolin disrupts fetal Leydig cell development via several pathways.

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“…The vascular niche is also important for the regulation of the steroidogenic progenitors that give rise to Leydig cells (Tang et al 2008, Defalco et al 2013. These progenitors arise both from the CE and from specialized cells along the gonad-mesonephros border (Defalco et al 2011, Kumar & DeFalco 2018.…”

Section: Recruitment Of Other Cell Types In the Gonadmentioning

confidence: 99%

WOMEN IN REPRODUCTIVE SCIENCE: To be or not to be a testis

Capel

2019

Reproduction

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Work that established the testis as the driver of male development, and the Y chromosome as the bearer of the male-determining gene, established a working model, and set the stage for the molecular age of mammalian sex determination. The discovery and characterization of Sry/SRY at the top of the hierarchy in mammals launched the field in two major directions. The first was to identify the downstream transcription factors and other molecular players that drive the bifurcation of Sertoli and granulosa cell differentiation. The second major direction was to understand organogenesis of the early bipotential gonad, and how divergence of its two distinct morphogenetic pathways (testis and ovary) is regulated at the cellular level. This review will summarize the early discoveries soon after Sry was identified and focus on my study of the gonad as a model of organogenesis.

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A perivascular niche for multipotent progenitors in the fetal testis

Cited by 70 publications

References 69 publications

Tcf21⁺mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Tcf21⁺mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Gestational vinclozolin exposure suppresses fetal Leydig cell development in rats

WOMEN IN REPRODUCTIVE SCIENCE: To be or not to be a testis

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A perivascular niche for multipotent progenitors in the fetal testis

Cited by 70 publications

References 69 publications

Tcf21+mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Tcf21+mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Gestational vinclozolin exposure suppresses fetal Leydig cell development in rats

WOMEN IN REPRODUCTIVE SCIENCE: To be or not to be a testis

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Tcf21⁺mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Tcf21⁺mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration