BMP signaling regulates PGC numbers and motility in organ culture

Dudley, Brian; Runyan, Chris; Takeuchi, Yutaka; Schaible, Kyle; Molyneaux, Kathleen

doi:10.1016/j.mod.2006.09.005

Cited by 57 publications

(67 citation statements)

References 55 publications

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“…Consistent with this, loss of function of the receptor for FGF7, FGFR2-3b results in reduced germ cell numbers (Takeuchi et al, 2005). In addition, BMPs regulate PGC numbers and motility in culture (Dudley et al, 2007;Ross et al, 2007). BMPs are also required for regulation of pluripotency in ES cells (Ying et al, 2003) and for recruitment of PGCs from the proximal epiblast during germ line specification (Lawson et al, 1999;de Sousa Lopes et al, 2004).…”

Section: Survival and Proliferation: Key Aspects Of Early Germ Cell Dmentioning

confidence: 71%

Foetal germ cells: striking the balance between pluripotency and differentiation

Western¹

2009

Int. J. Dev. Biol.

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Section: Survival and Proliferation: Key Aspects Of Early Germ Cell Dmentioning

confidence: 71%

Foetal germ cells: striking the balance between pluripotency and differentiation

Western¹

2009

Int. J. Dev. Biol.

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“…The murine testis is formed from genital swellings ventral to the mesonephros, which are populated by migrating primordial germ cells at E10.5 (Wilhelm and Koopman, 2006). BMP signaling regulates primordial germ cell number, proliferation and migration, yet no role had been defined in testicular somatic cells (Hu et al, 2004;Puglisi et al, 2004;Dudley et al, 2007). No germ cell defects were observed in Alk3 IMP null mice, consistent with lack of expression of Rarb2-Cre in these cells.…”

Section: Alk3 Signaling Regulates Mesonephric Derived Testicular Popumentioning

confidence: 97%

Alk3 controls nephron number and androgen production via lineage-specific effects in intermediate mesoderm

et al. 2011

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SUMMARYThe mammalian kidney and male reproductive system are both derived from the intermediate mesoderm. The spatial and temporal expression of bone morphogenetic protein (BMP) 2 and BMP4 and their cognate receptor, activin like kinase 3 (ALK3), suggests a functional role for BMP-ALK3 signaling during formation of intermediate mesoderm-derivative organs. Here, we define cell autonomous functions for Alk3 in the kidney and male gonad in mice with CRE-mediated Alk3 inactivation targeted to intermediate mesoderm progenitors (Alk3 IMP null ). Alk3-deficient mice exhibit simple renal hypoplasia characterized by decreases in both kidney size and nephron number but normal tissue architecture. These defects are preceded by a decreased contribution of Alk3-deleted cells to the metanephric blastema and reduced expression of Osr1 and SIX2, which mark nephron progenitor cells. Mutant mice are also characterized by defects in intermediate mesoderm-derived genital tissues with fewer mesonephric tubules and testicular Leydig cells, epithelial vacuolization in the postnatal corpus epididymis, and decreased serum testosterone levels and reduced fertility. Analysis of ALK3-dependent signaling effectors revealed lineage-specific reduction of phospho-p38 MAPK in metanephric mesenchyme and phospho-SMAD1/5/8 in the testis. Together, these results demonstrate a requirement for Alk3 in distinct progenitor cell populations derived from the intermediate mesoderm.

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“…Id1 is downstream of the BMP/phosphorylated Smad pathway and functions as a dominant-negative binding factor for HLH genes (Norton et al, 1998). However, phosphorylated Smad1, 5 and 8 are not detected in migrating PGCs (Dudley et al, 2007). Thus, Id1 has to be upregulated by another pathway.…”

Section: Research Articlementioning

confidence: 99%

“…S7A in the supplementary material). Although the mechanism of transcriptional regulation of Id1, which bypasses the BMP/phosphorylated Smad pathway (Dudley et al, 2007), is unclear, Id1 might be directly downstream of Nanog in PGCs, as shown by the binding of Nanog to Id1 in ESCs (Kim et al, 2008).…”

Section: Changes In Gene Expression Profile Upon Nanog Knockdown In Ementioning

confidence: 99%

Conditional knockdown of Nanog induces apoptotic cell death in mouse migrating primordial germ cells

Yamaguchi

Kurimoto²,

Yabuta³

et al. 2009

Development

115

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The pluripotency factor Nanog is expressed in peri-implantation embryos and primordial germ cells (PGCs). Nanog-deficient mouse embryos die soon after implantation. To explore the function of Nanog in germ cells, Nanog RNA was conditionally knocked down in vivo by shRNA. Nanog shRNA transgenic (NRi-Tg) mice were generated through the formation of germline chimeras with NRi-Tg embryonic stem cells. In E12.5 Cre-induced ER-Cre/NRi-Tg and TNAP-Cre/NRi-Tg double-transgenic embryos, the number of alkaline phosphatase-positive and SSEA1-positive PGCs decreased significantly. In the E9.5 and E10.5 migrating Nanog-knockdown PGCs, TUNEL-positive apoptotic cell death became prominent in vivo and in vitro, despite Oct4 expression. Single-cell microarray analysis of E10.5 Nanog-knockdown PGCs revealed significant up-and downregulation of a substantial number of genes, including Tial1, Id1 and Suz12. These data suggest that Nanog plays a key role in the proliferation and survival of migrating PGCs as a safeguard of the PGC-specific molecular network.

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BMP signaling regulates PGC numbers and motility in organ culture

Cited by 57 publications

References 55 publications

Foetal germ cells: striking the balance between pluripotency and differentiation

Foetal germ cells: striking the balance between pluripotency and differentiation

Alk3 controls nephron number and androgen production via lineage-specific effects in intermediate mesoderm

Conditional knockdown of Nanog induces apoptotic cell death in mouse migrating primordial germ cells

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