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Sphingosine 1-phosphate receptor 1 governs endothelial barrier function and angiogenesis by upregulating endoglin signaling. | LitMetric

AI Article Synopsis

  • The S1P/S1P receptor 1 (S1pr1) signaling pathway is crucial for maintaining vascular health and promoting angiogenesis, particularly in endothelial cells, but the relationship between S1pr1 and endoglin (Eng) requires further exploration.
  • Experimental methods including inhibitors and transgenic models were used to determine whether inhibiting S1pr1 affects vascular leakage and inflammation, as well as to investigate the interaction between S1P/S1pr1 and BMP9/Eng signaling in retinal angiogenesis.
  • Findings indicate that both S1pr1 and Eng are critical for postnatal retinal angiogenesis, with S1pr1 activation enhancing vascular barrier function through increased phosphorylation of Smad proteins, while inhibition

Article Abstract

Background: The sphingosine 1-phosphate (S1P)/S1P receptor (S1pr) 1 signaling plays an essential role in regulating vascular integrity and angiogenesis. We have previously shown that cell-surface expression of endoglin (Eng) is sustained by S1P/S1pr1 signaling in endothelial cells (ECs). However, whether S1pr1 mediates Eng signaling, or vice versa, remains unknown.

Methods: S1pr1 inhibitors were used to study whether pharmacological inhibition induces basal vascular leakage . An acute respiratory distress syndrome (ARDS) model was used to study whether S1pr1 inhibition evoked greater inflammation in lungs. A S1pr1 inhibitor, a bone morphogenetic protein 9 (BMP9) blocking antibody, or lentivirus-mediated expression of soluble extracellular domain of Eng (sEng) were used to test whether blocking both S1P/S1pr1 and BMP9/Eng signaling axes would impose any interaction in retinal angiogenesis. To clarify whether S1P and BMP9 function in a linear pathway, a study of trans-endothelial electrical resistance (TEER) measurement was carried out using a mouse islet EC line MS1; time course studies were executed to exam downstream effectors of S1P and BMP9 signaling pathways in ECs; two stable MS1 cell lines were generated, one with overexpression of human S1PR1 and the other with knockdown of Eng, to validate S1pr1 and Eng were the key players for the crosstalk. Inhibitor of extracellular regulated protein kinases (ERK) was used to check whether this signaling was involved in S1P-induced cell-surface localization of Eng.

Results: The present study elucidated that S1pr1 and Eng are both pivotal for angiogenesis in the postnatal mouse retina, and that the activation of S1pr1 or Eng increases vascular barrier function. Activation of S1pr1 enhanced the phosphorylation of Smad family members 1, 5, and 8 (pSmad1/5/8), while the inhibition of S1pr1 reduced the levels of pSma1/5/8 induced by BMP9 treatment. Activation or loss of Eng did not affect S1pr1 signaling. Moreover, activation of ERK was involved in promoting EC-surface expression of Eng by S1pr1.

Conclusions: Our data demonstrates for the first time that there exists a linear pathway of S1pr1-Eng signaling axis in ECs, which governs vascular homeostasis. Functional BMP9/Eng signaling requires S1P/S1pr1 activation, and S1pr1 signaling acts as a vascular protection mechanism upstream of Eng.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8904984PMC
http://dx.doi.org/10.21037/atm-21-6679DOI Listing

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