Epicardial retinoid X receptor α is required for myocardial growth and coronary artery formation

Merki, Esther; Zamora, Mónica; Raya, Ángel; Kawakami, Yasuhiko; Wang, Jianming; Zhang, Xiaoxue; Burch, John; Kubalak, Steven W.; Kaliman, Perla; Belmonte, Juan Carlos Izpisúa; Chien, Kenneth R.; Ruiz‐Lozano, Pilar

doi:10.1073/pnas.0504343102

Cited by 310 publications

(411 citation statements)

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“…Furthermore, the total level of mitogenic activity in rCM (measured by thymidine incorporation in NIH3T3 cells) was also not altered by these treatments. It is possible that our earlier results with EMC cells were in error, although we note that our general conclusions regarding the role of RA in the embryonic epicardium have been corroborated in several independent ways by other labs (Stuckmann et al, 2003;Lavine et al, 2005;Merki et al, 2005). As a possible explanation, we suspect that the phenotype of the EMC cell line may have shifted since our original investigations such that mitogen expression or secretion has become RAindependent.…”

Section: Discussionmentioning

confidence: 58%

“…RA is made by embryonic epicardium and by EMC cells, and we have proposed that RA signaling in vivo is required for the production of epicardial mitogens. Thus, mouse embryos lacking the RA receptor RXR␣ show a profoundly hypoplastic ventricular chamber wall (Sucov et al, 1994), and this phenotype is replicated (albeit to a less severe extent) in epicardium-specific RXR␣ mutants (Merki et al, 2005). With the identification of PDGF-A as a mitogen made by EMC cells, we addressed the potential role of RA in Pdgfa expression or PDGF-A secretion.…”

Section: Discussionmentioning

confidence: 99%

“…Fibroblast growth factors (FGFs) may be important, as combined mutation of the FGFR1 and FGFR2 receptor genes results in reduced regional myocardial proliferation and an underdeveloped ventricular wall (Lavine et al, 2005). Wnt9b has also been proposed as an epicardial factor (Merki et al, 2005), although its role may be more important in the formation of coronary vasculature rather than as a mitogenic signal; this may be true for FGF as well (Lavine et al, 2006). A hypoplastic ventricular chamber wall is observed in mouse knockout studies of several genes encoding regulatory or signaling components, although how these ultimately impact myocardial proliferation remains unclear.…”

Section: Introductionmentioning

confidence: 99%

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PDGF‐A as an epicardial mitogen during heart development

Kang

et al. 2008

Developmental Dynamics

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In the developing heart, reciprocal interactions between the epicardium and myocardium drive further sublineage specification and ventricular chamber morphogenesis. Several observations suggest that the epicardium is a source of secreted factors that influence cardiomyocyte proliferation, and these factors may have other roles as well. However, the identity of these epicardial factors remains mostly unknown. We have identified platelet-derived growth factor-A (PDGF-A) as one of several mitogens expressed by the rat EMC epicardial cell line (epicardial mesothelial cells), by embryonic epicardium and myocardium during mouse heart development, and by adult epicardium. Expression of the cognate receptor gene Pdgfra was detected in the epicardium, although a low level of expression in myocardium could not be ruled out. To address the potential role of PDGF signaling in heart development, we mutated both PDGF receptor genes in the myocardial and mesodermal compartments of the heart; however, this did not result in an observable cardiac phenotype. This finding suggests that mesodermal PDGF signaling is not essential in heart development, although its role may be redundant with other signaling pathways. Indeed, our results demonstrate the presence of additional mitogens that may have such an overlapping role. Developmental Dynamics 237:692-701, 2008.

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Section: Discussionmentioning

confidence: 58%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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PDGF‐A as an epicardial mitogen during heart development

Kang

et al. 2008

Developmental Dynamics

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“…Ablation of the epicardium or loss of the epicardially expressed genes, RXR␣ and BAF180, results in defects in cardiomyoblast proliferation and coronary development (Wang et al, 2004;Merki et al, 2005). Based on these data, we and others have proposed that the epicardium secretes factors that govern both of these processes Lavine et al, 2005).…”

Section: Introductionmentioning

confidence: 94%

Novel tool to suppress cell proliferation in vivo demonstrates that myocardial and coronary vascular growth represent distinct developmental programs

Lavine

Schmid

Smith

et al. 2008

Developmental Dynamics

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Cell proliferation, differentiation, and vascular growth are coordinated processes that are essential for embryonic development, tissue repair, and disease pathogenesis. Of interest, whether these critical processes are dependent upon each other has not been thoroughly explored. We have generated mice that conditionally express the cell cycle inhibitor p27 Kip1 , following Cre-mediated recombination, as a tool to separate tissue proliferation from other cellular processes. Using the embryonic heart as a model, we show that myocardial proliferation and coronary development are genetically separable processes. Forced expression of p27, in both a wild-type and in a genetically sensitized background, resulted in ventricular hypoplasia without having any substantial effects on coronary development. We further demonstrate that Hedgehog signaling, which is essential for coronary vascular growth, does not control myocardial proliferation. Together, these studies strongly suggest that myocardial cell proliferation and coronary development are genetically separable programs exemplifying one of the many potential uses of this genetic tool. Developmental Dynamics 237:713-724, 2008.

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“…Disturbing RA signaling in the epicardium by epicardial deletion of the retinoid X receptor-α (RXRα), results in defective epithelial-to-mesenchymal transition (EMT), thinning of the myocardium, disturbed coronary arteriogenesis and ventricular pre-excitation [34,35]. This phenotype is also seen after disturbance of epicardial outgrowth in avian embryos [36] and in Wt1-null mice [27,37].…”

Section: Discussionmentioning

confidence: 99%