2021
DOI: 10.1161/circulationaha.120.047375
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BMP9 and BMP10 Act Directly on Vascular Smooth Muscle Cells for Generation and Maintenance of the Contractile State

Abstract: Background: Vascular smooth muscle cells (VSMCs) show a remarkable phenotypic plasticity allowing acquisition of contractile or synthetic states but critical information is missing about the physiological signals, promoting formation and maintenance of contractile VSMCs in vivo . BMP9 and BMP10 are known to regulate endothelial quiescence after secretion from the liver and right atrium, whereas a direct role in the regulation of VSMCs was not investigated. Here, we studied t… Show more

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Cited by 41 publications
(30 citation statements)
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“…The PAVMs we observe in the homozygous p.[Glu279Ter];[Glu279Ter] patient combined with recent reports of PAVMs in a p.[Tyr354Argf-sTer15];[Tyr354ArgfsTer15] homozygote (Liu et al, 2020) and a p.[Gly291Ser] heterozygous mutation carrier (Topiwala et al, 2020) suggest that loss of BMP9 and BMP10 predispose individuals to the development of PAVMs. To date, studies of compound Bmp9:Bmp10 knockout mice have not specifically noted AVM development, although dilated vessels associated with altered vascular smooth muscle cell functionality have been reported (L. Wang et al, 2021). It remains to be determined whether additional events are required to promote PAVM formation, either via disruption of BMP signaling, or by affecting other signaling pathways.…”
Section: Assessment Of Alternate Codon Utilization In the P[gln26ter] Bmp9 Mutantmentioning
confidence: 99%
“…The PAVMs we observe in the homozygous p.[Glu279Ter];[Glu279Ter] patient combined with recent reports of PAVMs in a p.[Tyr354Argf-sTer15];[Tyr354ArgfsTer15] homozygote (Liu et al, 2020) and a p.[Gly291Ser] heterozygous mutation carrier (Topiwala et al, 2020) suggest that loss of BMP9 and BMP10 predispose individuals to the development of PAVMs. To date, studies of compound Bmp9:Bmp10 knockout mice have not specifically noted AVM development, although dilated vessels associated with altered vascular smooth muscle cell functionality have been reported (L. Wang et al, 2021). It remains to be determined whether additional events are required to promote PAVM formation, either via disruption of BMP signaling, or by affecting other signaling pathways.…”
Section: Assessment Of Alternate Codon Utilization In the P[gln26ter] Bmp9 Mutantmentioning
confidence: 99%
“…Interestingly, this effect in these cells takes place in pulmonary blood vessels but not in aortic and coronary arteries. The heterogeneity of this response is related to the differential expression of BMP type I receptors ALK1, ALK2, ALK3 and ALK6 [163]. All these findings have been shown in the context of pulmonary hypertension, but they evidence a possible effect of BMP9-ALK1 in mural cells, supporting cells which stabilize tumor blood vessels, especially pericytes.…”
Section: Bmp9 Induces Direct Effects On Tumor Cellsmentioning
confidence: 93%
“…After birth, BMP9 and BMP10 clearly play redundant roles in postnatal angiogenesis (retinal vascularization and closure of the ductus arteriosus 5,30,85 ) but also in adult vascular homeostasis (under physiological conditions) as only the double Bmp9/ Bmp10 deletion leads to a vascular phenotype. 108,109 Due to technical issues, the role of BMP9 has been addressed via a complete and constitutive KO while the role of BMP10 has been addressed via either neutralizing antibodies, or tamoxifen inducible knockdown in adult or tissue-specific deletion in the right atria in order to bypass cardiac embryonic lethality. In zebrafish, no transcriptional adaptation or genetic compensation was found for bmp9 or bmp10-like expression or in bmp10 mutants.…”
Section: Loss Of Bmp9 And/or Bmp10 In Pathological Contextsmentioning
confidence: 99%
“…It was shown that adult Bmp10 knockdown in the C57BL/6 background was not lethal and showed no obvious vascular phenotype 107,108 . More recently, a mouse model specifically deleted for Bmp10 in the right atrium was generated ( Bmp10 ANF ) 109 . These mice overcame embryonic cardiac lethality and were viable with no obvious phenotype, suggesting that cardiac BMP10 is not involved in postnatal vascular remodeling.…”
Section: Bmp9 and Bmp10 Functions In The Cardiovascular System: Specific And Redundant Rolesmentioning
confidence: 99%