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RBPMS promotes contractile smooth muscle splicing and alters phenotypic behaviour of human embryonic stem cell derived vascular smooth muscle cells

Aishwarya G Jacob, Ilias Moutsopoulous, Alex Petchey, Irina Mohorianu, Sanjay Sinha, Christopher WJ Smith
doi: https://doi.org/10.1101/2022.11.27.516868
Aishwarya G Jacob
1Department of Biochemistry, University of Cambridge, CB2 1QW
2MRC-Wellcome Trust Cambridge Stem Cell Institute, CB2 0AW
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Ilias Moutsopoulous
2MRC-Wellcome Trust Cambridge Stem Cell Institute, CB2 0AW
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Alex Petchey
2MRC-Wellcome Trust Cambridge Stem Cell Institute, CB2 0AW
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Irina Mohorianu
2MRC-Wellcome Trust Cambridge Stem Cell Institute, CB2 0AW
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  • For correspondence: cwjs1@cam.ac.uk
Sanjay Sinha
2MRC-Wellcome Trust Cambridge Stem Cell Institute, CB2 0AW
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  • For correspondence: cwjs1@cam.ac.uk
Christopher WJ Smith
1Department of Biochemistry, University of Cambridge, CB2 1QW
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  • For correspondence: cwjs1@cam.ac.uk
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Abstract

Differentiated Vascular Smooth Muscle Cells (VSMCs) express a unique network of splice isoforms (smooth muscle specific alternative splicing - SM-AS) in functionally critical genes including those comprising the contractile machinery. We previously described RNA Binding Protein Multiple Splicing (RBPMS) as a potent driver of contractile, aortic tissue like SM-AS in VSMCs using rodent models. What is unknown is how RBPMS affects VSMC phenotype and behaviour. Here, we use human embryonic stem cell-derived VSMCs (hES-VSMCs) to dissect the role of RBPMS in SM-AS in human cells and determine the impact on VSMC phenotypic properties. hES-VSMCs are inherently immature and display only partially differentiated SM-AS patterns while RBPMS levels are undetectable endogenously. Hence, we used an over-expression system and found that RBPMS induces SM-AS patterns in hES-VSMCs akin to the contractile tissue VSMC splicing patterns in multiple events. We present in silico and experimental findings that support RBPMS’ splicing activity as mediated through direct binding and via functional cooperativity with splicing factor RBFOX2 on a significant subset of targets. Finally, we demonstrate that RBPMS is capable of altering the motility and the proliferative properties of hES-VSMCs to mimic a more differentiated state. Overall, this study emphasizes a critical splicing regulatory role for RBPMS in human VSMCs and provides evidence of phenotypic modulation by RBPMS.

Competing Interest Statement

The authors have declared no competing interest.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. All rights reserved. No reuse allowed without permission.
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Posted November 28, 2022.
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RBPMS promotes contractile smooth muscle splicing and alters phenotypic behaviour of human embryonic stem cell derived vascular smooth muscle cells
Aishwarya G Jacob, Ilias Moutsopoulous, Alex Petchey, Irina Mohorianu, Sanjay Sinha, Christopher WJ Smith
bioRxiv 2022.11.27.516868; doi: https://doi.org/10.1101/2022.11.27.516868
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RBPMS promotes contractile smooth muscle splicing and alters phenotypic behaviour of human embryonic stem cell derived vascular smooth muscle cells
Aishwarya G Jacob, Ilias Moutsopoulous, Alex Petchey, Irina Mohorianu, Sanjay Sinha, Christopher WJ Smith
bioRxiv 2022.11.27.516868; doi: https://doi.org/10.1101/2022.11.27.516868

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