WT1 Maintains Adrenal-Gonadal Primordium Identity and Marks a Population of AGP-like Progenitors within the Adrenal Gland

Bandiera, Roberto; Vidal, Valérie; Motamedi, Fariba Jian; Clarkson, Michael W.; Sahut‐Barnola, Isabelle; Gise, Alexander von; Pu, William T.; Hohenstein, Peter; Martinez, Antoine; Schedl, Andreas

doi:10.1016/j.devcel.2013.09.003

Cited by 104 publications

(117 citation statements)

References 46 publications

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“…We extracted expression levels of a list of 28 genes expressed or functionally linked to the progenitor compartment and found that 18 of them were significantly (t test, adjusted P < 0.05) downregulated in Prkar1a-knockout adrenals compared with WT adrenals (Supplemental Figure 4B). We further confirmed by qPCR that Prkar1a ablation in steroidogenic cells resulted in the downregulation of all stem/progenitor markers (12,14,(41)(42)(43) from either capsular or subcapsular compartments (Supplemental Figure 4C). The SHH and RSPO/WNT/β-catenin signaling pathways play an essential role in adult cortex maintenance and renewal (12,14).…”

Section: Pka-dependent Accelerated Cortex Renewal Is Counteracted By supporting

confidence: 54%

PKA signaling drives reticularis differentiation and sexually dimorphic adrenal cortex renewal

Dumontet¹,

Sahut‐Barnola²,

Septier³

et al. 2018

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Section: Pka-dependent Accelerated Cortex Renewal Is Counteracted By supporting

confidence: 54%

PKA signaling drives reticularis differentiation and sexually dimorphic adrenal cortex renewal

Dumontet¹,

Sahut‐Barnola²,

Septier³

et al. 2018

JCI Insight

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“…In the absence of Wt1, high Sf1 expression is induced by an unknown factor, which leads undifferentiated somatic cells to develop into steroidogenic cells. Interestingly, a recent study also showed that the differentiation of steroidogenic cells in the adrenal gland is repressed by Wt1 (Bandiera et al, 2013), implying that Wt1 plays a role in the differentiation of gonad somatic cells, most likely by inhibiting the development of steroidogenic cells.…”

Section: Discussionmentioning

confidence: 99%

Wt1 directs the lineage specification of sertoli and granulosa cells by repressing Sf1 expression

et al. 2016

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Supporting cells (Sertoli and granulosa) and steroidogenic cells (Leydig and theca-interstitium) are two major somatic cell types in mammalian gonads, but the mechanisms that control their differentiation during gonad development remain elusive. In this study, we found that deletion of Wt1 in the ovary after sex determination caused ectopic development of steroidogenic cells at the embryonic stage. Furthermore, differentiation of both Sertoli and granulosa cells was blocked when Wt1 was deleted before sex determination and most genital ridge somatic cells differentiated into steroidogenic cells in both male and female gonads. Further studies revealed that WT1 repressed Sf1 expression by directly binding to the Sf1 promoter region, and the repressive function was completely abolished when WT1 binding sites were mutated. This study demonstrates that Wt1 is required for the lineage specification of both Sertoli and granulosa cells by repressing Sf1 expression. Without Wt1, the expression of Sf1 was upregulated and the somatic cells differentiated into steroidogenic cells instead of supporting cells. Our study uncovers a novel mechanism of somatic cell differentiation during gonad development.

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“…The adrenal capsule consists of mesenchymal cells that are positive for the SHH mediator GLI1 (King et al 2009) and COUPTFII (also known as NR2F2) (Wood et al 2013) and surrounded by a thin layer of mesothelial lining expressing the Wilms tumor suppressor WT1 (Bandiera et al 2013). To determine whether Rspo1 and Rspo3 are expressed in the same cell population, we performed cell-sorting experiments on dissociated adult adrenals from Wt1-GFP animals (Hosen et al 2007).…”

Section: Resultsmentioning

confidence: 99%

“…By embryonic day 12.5 (E12.5) in mice, the developing organ becomes surrounded by condensing mesenchymal cells that ultimately form the capsule (Bandiera et al 2013). A second contribution to the capsule is likely derived from adrenal progenitor cells that have lost SF1 expression (Wood et al 2013).…”

mentioning

confidence: 99%

The adrenal capsule is a signaling center controlling cell renewal and zonation through Rspo3

Vidal¹,

Sacco²,

Rocha³

et al. 2016

Genes Dev.

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Adrenal glands are zonated endocrine organs that are essential in controlling body homeostasis. How zonation is induced and maintained and how renewal of the adrenal cortex is ensured remain a mystery. Here we show that capsular RSPO3 signals to the underlying steroidogenic compartment to induce β-catenin signaling and imprint glomerulosa cell fate. Deletion of RSPO3 leads to loss of SHH signaling and impaired organ growth. Importantly, Rspo3 function remains essential in adult life to ensure replenishment of lost cells and maintain the properties of the zona glomerulosa. Thus, the adrenal capsule acts as a central signaling center that ensures replacement of damaged cells and is required to maintain zonation throughout life.

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WT1 Maintains Adrenal-Gonadal Primordium Identity and Marks a Population of AGP-like Progenitors within the Adrenal Gland

Cited by 104 publications

References 46 publications

PKA signaling drives reticularis differentiation and sexually dimorphic adrenal cortex renewal

PKA signaling drives reticularis differentiation and sexually dimorphic adrenal cortex renewal

Wt1 directs the lineage specification of sertoli and granulosa cells by repressing Sf1 expression

The adrenal capsule is a signaling center controlling cell renewal and zonation through Rspo3

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