Tcf21<sup>+</sup>mesenchymal cells contribute to testis somatic cell development, homeostasis, and regeneration

Shen, Yannan; Larose, Hailey; Shami, Adrienne Niederriter; Moritz, Lindsay; Manske, Gabriel L.; Ma, Qianyi; Zheng, Xianing; Sukhwani, Meena; Czerwinski, Michael; Sultan, Caleb; Clements, Jourdan; Chen, Haolin; Spence, Jason R.; Orwig, Kyle E.; Tallquist, Michelle D.; Li, Jun Z.; Hammoud, Saher Sue

doi:10.1101/2020.05.02.074518

Cited by 6 publications

(8 citation statements)

References 113 publications

(148 reference statements)

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“…PMCs and LCs (Shen et al, 2020), while the fate of Wnt5a + progenitors is mainly restricted to FLCs and ALCs, as reported here.…”

Section: Discussionsupporting

confidence: 82%

“…Consistent with its expression profile, our findings confirm that Wnt5a + cells are true steroidogenic progenitors giving rise to most FLCs and ALCs. Other genes expressed in steroidogenic progenitors might also have been potential candidates to use for genetically tracing the lineage of these cells, including Nr5a1, Nr2f2/CouptfII, Pdgfra and Tcf21/Pod1 (Brennan et al, 2003;Shen et al, 2020). However, the expression of these genes is not restricted to the steroidogenic progenitors and they usually display a more widespread expression, either at earlier stages of development and/or in other cell types.…”

Section: Discussionmentioning

confidence: 99%

“…The dramatic increase in the number of FLCs between E12.5 and E15.5 occurs through the recruitment and differentiation of Leydig progenitor cells via paracrine factors, rather than by mitotic division of differentiated FLCs (Barsoum et al, 2009; Barsoum and Yao, 2010;Bitgood et al, 1996;Brennan et al, 2003;Byskov, 1986;Kerr and Knell, 1988;Migrenne et al, 2001). During the first postnatal days, FLCs involute gradually and are replaced by ALCs, although some may persist in the adult testis (Haider, 2004;Shima et al, 2015;Wen et al, 2016). ALCs are not derived from pre-existing FLCs but, like their fetal counterparts, arise from uncharacterized LC progenitors located in the testicular interstitium (Barsoum et al, 2013;Davidoff et al, 2004;Kilcoyne et al, 2014;Shima et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

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Expression ofWnt5adefines the major progenitors of fetal and adult Leydig cells

Ademi

Stévant

Rands

et al. 2020

Preprint

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SummaryLeydig cells (LCs) are the major androgen-producing cells in the testes. They arise from steroidogenic progenitors, whose origins, maintenance and differentiation dynamics remain largely unknown. Here, we identified Wnt5a as a specific marker of steroidogenic progenitors, whose expression begins at around E11.5-E12.5 in interstitial cells of the fetal mouse testis. In vivo lineage tracing indicates that Wnt5a-expressing progenitors are initially present in large numbers in the fetal testis and then progressively decrease as development progresses. We provide evidence that Wnt5a-expressing cells are bona fide progenitors of peritubular myoid cells as well as fetal and adult LCs, contributing to most of the LCs present in the fetal and adult testis. Additionally, we show in the adult testis that Wnt5a expression is restricted to a subset of LCs exhibiting a slow but noticeable clonal expansion, revealing hitherto unappreciated proliferation of fully differentiated LCs as a contribution to the adult LC pool.

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“…PMCs and LCs (Shen et al, 2020), while the fate of Wnt5a + progenitors is mainly restricted to FLCs and ALCs, as reported here.…”

Section: Discussionsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Expression ofWnt5adefines the major progenitors of fetal and adult Leydig cells

Ademi

Stévant

Rands

et al. 2020

Preprint

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“…Since PTMs and stromal cells were clustered into a single large cluster (Figure 1D) and PTMs are suggested to be derived from interstitial progenitors (Shen et al 2020) , PTMs and stromal cells were grouped together for subsequent analysis. Re-clustering of this cell group generated 10 clusters of cells (Supplementary Figure S11A and B).…”

Section: Stromal Cell Heterogeneity and Ptm Development During The Pementioning

confidence: 99%

The single-cell epigenetic regulatory landscape in mammalian perinatal testis development

Liao

et al. 2021

Preprint

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Spermatogenesis depends on an orchestrated series of developing events in germ cells and full maturation of the somatic microenvironment. To date, the majority of efforts to study cellular heterogeneity in testis has been focused on single-cell gene expression rather than the chromatin landscape shaping gene expression. To advance our understanding of the regulatory programs underlying testicular cell types, we analyzed single-cell chromatin accessibility profiles in more than 25,000 cells from mouse developing testis. We showed that scATAC-Seq allowed us to deconvolve distinct cell populations and identify cis-regulatory elements (CREs) underlying cell type specification. We identified sets of transcription factors associated with cell type-specific accessibility, revealing novel regulators of cell fate specification and maintenance. Pseudotime reconstruction revealed detailed regulatory dynamics coordinating the sequential developmental progressions of germ cells and somatic cells. This high-resolution data also revealed putative stem cells within the Sertoli and Leydig cell populations. Further, we defined candidate target cell types and genes of several GWAS signals, including those associated with testosterone levels and coronary artery disease. Collectively, our data provide a blueprint of the ‘regulon’ of the mouse male germline and supporting somatic cells.

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“…They arise from LC progenitors located in the testicular interstitium (Davidoff et al, 2004;Barsoum et al, 2013;Shima et al, 2013;Kilcoyne et al, 2014;Ademi et al, 2020). Two recent studies showed that both fetal and adult Leydig cells derive from a common pool of progenitor cells originating from the gonadal surface epithelium and mesonephric mesenchymal cells present from fetal life (Ademi et al, 2020;Shen et al, 2020). Evidence also shows that a subset of FLCs dedifferentiate at fetal stages to serve as potential ALC stem cells (Shima et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

Specific transcriptomic signatures and dual regulation of steroidogenesis between fetal and adult mouse Leydig cells

Sararols

Stévant

Neirijnck

et al. 2021

Preprint

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Leydig cells (LC) are the main testicular androgen-producing cells. In eutherian mammals, two types of LCs emerge successively during testicular development, fetal Leydig cells (FLCs) and adult Leydig cells (ALCs). Both display significant differences in androgen production and regulation. Using bulk RNA sequencing, we compared the transcriptomes of both LC populations to characterise their specific transcriptional and functional features. Despite similar transcriptomic profiles, a quarter of the genes show significant variations in expression between FLCs and ALCs. Non-transcriptional events, such as alternative splicing was also observed, including a high rate of intron retention in FLCs compared to ALCs. The use of single-cell RNA sequencing data also allowed the identification of nine FLC-specific genes and 50 ALC-specific genes. Expression of the corticotropin-releasing hormone 1 (Crhr1) receptor and the ACTH receptor melanocortin type 2 receptor (Mc2r) specifically in FLCs suggests a dual regulation of steroidogenesis. The androstenedione synthesis by FLCs is stimulated by luteinizing hormone (LH), CRH and ACTH whereas the testosterone synthesis by ALCs is dependent exclusively on LH. Overall, our study provides a useful database to explore LC development and function.

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

Cited by 6 publications

References 113 publications

Expression ofWnt5adefines the major progenitors of fetal and adult Leydig cells

Expression ofWnt5adefines the major progenitors of fetal and adult Leydig cells

The single-cell epigenetic regulatory landscape in mammalian perinatal testis development

Specific transcriptomic signatures and dual regulation of steroidogenesis between fetal and adult mouse Leydig cells

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

Cited by 6 publications

References 113 publications

Expression ofWnt5adefines the major progenitors of fetal and adult Leydig cells

Expression ofWnt5adefines the major progenitors of fetal and adult Leydig cells

The single-cell epigenetic regulatory landscape in mammalian perinatal testis development

Specific transcriptomic signatures and dual regulation of steroidogenesis between fetal and adult mouse Leydig cells

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