Contribution of PKC-dependent and -independent processes in temporal ERK regulation by ET-1, PDGF, and EGF in rat myometrial cells

Robin, Philippe; Boulven, Isaline; Bôle‐Feysot, Christine; Tanfin, Zahra; Leiber, Denis

doi:10.1152/ajpcell.00465.2003

Cited by 30 publications

(34 citation statements)

References 46 publications

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“…In conclusion, our data support a model whereby PDGF pathway signaling via MEK 3369 RESEARCH ARTICLE PDGF signaling promotes expansion of ExEn and PKC plays a key role in XEN cell propagation. However, the exact and respective roles of MEK and PKC remain unclear, and we cannot exclude cross-talk, as has been reported in various cell systems (Lee et al, 2006;Okazaki et al, 2000;Robin et al, 2004). Future studies will be required to address the specific and combinatorial roles of these signal transducers.…”

Section: Discussionmentioning

confidence: 93%

A role for PDGF signaling in expansion of the extra-embryonic endoderm lineage of the mouse blastocyst

2010

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SUMMARYThe inner cell mass (ICM) of the implanting mammalian blastocyst comprises two lineages: the pluripotent epiblast (EPI) and primitive endoderm (PrE). We have identified platelet-derived growth factor receptor alpha (PDGFR) as an early marker of the PrE lineage and its derivatives in both mouse embryos and ex vivo paradigms of extra-embryonic endoderm (ExEn). By combining live imaging of embryos and embryo-derived stem cells expressing a histone H2B-GFP fusion reporter under the control of Pdgfra regulatory elements with the analysis of lineage-specific markers, we found that Pdgfra expression coincides with that of GATA6, the earliest expressed transcriptional regulator of the PrE lineage. We show that GATA6 is required for the activation of Pdgfra expression. Using pharmacological inhibition and genetic inactivation we addressed the role of the PDGF pathway in the PrE lineage. Our results demonstrate that PDGF signaling is essential for the establishment, and plays a role in the proliferation, of XEN cells, which are isolated from mouse blastocyst stage embryos and represent the PrE lineage. Implanting Pdgfra mutant blastocysts exhibited a reduced number of PrE cells, an effect that was exacerbated by delaying implantation. Surprisingly, we also noted an increase in the number of EPI cells in implantation-delayed Pdgfra-null mutants. Taken together, our data suggest a role for PDGF signaling in the expansion of the ExEn lineage. Our observations also uncover a possible role for the PrE in regulating the size of the pluripotent EPI compartment.

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Section: Discussionmentioning

confidence: 93%

A role for PDGF signaling in expansion of the extra-embryonic endoderm lineage of the mouse blastocyst

2010

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“…Clerk et al 2006 found that EGF increases cardiomyocyte Ras.GTP and activates c-Raf and ERK1/2 phosphorylation independently of PKC. Similarly, there is evidence that EGF activation of ERK1/2 in non-cardiac muscle is PKC-independent and Ras-dependent (Robin et al, 2004). These findings suggest that direct ligation of the EGFR removes the PKC dependence of signalling, implicating upstream functions of the kinase in regulating ligand levels and EGFR phosphorylation.…”

Section: Pkcmentioning

confidence: 86%

Transactivation of the epidermal growth factor receptor in responses to myocardial stress and cardioprotection

Reichelt

O’Brien

Thomas

et al. 2017

The International Journal of Biochemistry & Cell Biology

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“…EGF also activates the PI-3 kinase/Akt pathway in other tissues, synergizing with PLCγ activity in mediating EGF effects [27]. EGF activation of ERK in myometrium is PKC-independent and involves the conventional Ras pathway [28]. EGF has also been implicated in myometrial cell proliferation in a pathway involving PKC and eicosanoids [29].…”

Section: Contractant and Relaxant Signaling Pathways Stimulate Multipmentioning

confidence: 99%

Hormonal signaling and signal pathway crosstalk in the control of myometrial calcium dynamics

Sanborn

2007

Seminars in Cell & Developmental Biology

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Understanding the basis for the control of myometrial contractant and relaxant signaling pathways is important to understanding how to manage myometrial contractions. Signaling pathways are influenced by the level of expression of the signals and signal pathway components, the location of these components in the appropriate subcellular environment, and covalent modification. Crosstalk between these pathways regulates the effectiveness of signal transduction and represents an important way by which hormones can regulate phenotype. This review deals primarily with signaling pathways that control Ca 2+ entry and intracellular release, as well as the interplay between these pathways.

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Contribution of PKC-dependent and -independent processes in temporal ERK regulation by ET-1, PDGF, and EGF in rat myometrial cells

Cited by 30 publications

References 46 publications

A role for PDGF signaling in expansion of the extra-embryonic endoderm lineage of the mouse blastocyst

A role for PDGF signaling in expansion of the extra-embryonic endoderm lineage of the mouse blastocyst

Transactivation of the epidermal growth factor receptor in responses to myocardial stress and cardioprotection

Hormonal signaling and signal pathway crosstalk in the control of myometrial calcium dynamics

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