Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease

AIMS: Quiescent, differentiated adult vascular smooth muscle cells (VSMCs) can be induced to proliferate and switch phenotype. Such plasticity underlies blood vessel homeostasis and contributes to vascular disease development. Oligoclonal VSMC contribution is a hallmark of end-stage vascular disease...

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Autores principales: Worssam, Matt D, Lambert, Jordi, Oc, Sebnem, Taylor, James C K, Taylor, Annabel L, Dobnikar, Lina, Chappell, Joel, Harman, Jennifer L, Figg, Nichola L, Finigan, Alison, Foote, Kirsty, Uryga, Anna K, Bennett, Martin R, Spivakov, Mikhail, Jørgensen, Helle F
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10202649/
https://www.ncbi.nlm.nih.gov/pubmed/35994249
http://dx.doi.org/10.1093/cvr/cvac138
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author Worssam, Matt D
Lambert, Jordi
Oc, Sebnem
Taylor, James C K
Taylor, Annabel L
Dobnikar, Lina
Chappell, Joel
Harman, Jennifer L
Figg, Nichola L
Finigan, Alison
Foote, Kirsty
Uryga, Anna K
Bennett, Martin R
Spivakov, Mikhail
Jørgensen, Helle F
author_facet Worssam, Matt D
Lambert, Jordi
Oc, Sebnem
Taylor, James C K
Taylor, Annabel L
Dobnikar, Lina
Chappell, Joel
Harman, Jennifer L
Figg, Nichola L
Finigan, Alison
Foote, Kirsty
Uryga, Anna K
Bennett, Martin R
Spivakov, Mikhail
Jørgensen, Helle F
author_sort Worssam, Matt D
collection PubMed
description AIMS: Quiescent, differentiated adult vascular smooth muscle cells (VSMCs) can be induced to proliferate and switch phenotype. Such plasticity underlies blood vessel homeostasis and contributes to vascular disease development. Oligoclonal VSMC contribution is a hallmark of end-stage vascular disease. Here, we aim to understand cellular mechanisms underpinning generation of this VSMC oligoclonality. METHODS AND RESULTS: We investigate the dynamics of VSMC clone formation using confocal microscopy and single-cell transcriptomics in VSMC-lineage-traced animal models. We find that activation of medial VSMC proliferation occurs at low frequency after vascular injury and that only a subset of expanding clones migrate, which together drives formation of oligoclonal neointimal lesions. VSMC contribution in small atherosclerotic lesions is typically from one or two clones, similar to observations in mature lesions. Low frequency (<0.1%) of clonal VSMC proliferation is also observed in vitro. Single-cell RNA-sequencing revealed progressive cell state changes across a contiguous VSMC population at onset of injury-induced proliferation. Proliferating VSMCs mapped selectively to one of two distinct trajectories and were associated with cells showing extensive phenotypic switching. A proliferation-associated transitory state shared pronounced similarities with atypical SCA1+ VSMCs from uninjured mouse arteries and VSMCs in healthy human aorta. We show functionally that clonal expansion of SCA1+ VSMCs from healthy arteries occurs at higher rate and frequency compared with SCA1− cells. CONCLUSION: Our data suggest that activation of proliferation at low frequency is a general, cell-intrinsic feature of VSMCs. We show that rare VSMCs in healthy arteries display VSMC phenotypic switching akin to that observed in pathological vessel remodelling and that this is a conserved feature of mouse and human healthy arteries. The increased proliferation of modulated VSMCs from healthy arteries suggests that these cells respond more readily to disease-inducing cues and could drive oligoclonal VSMC expansion.
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spelling pubmed-102026492023-05-23 Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease Worssam, Matt D Lambert, Jordi Oc, Sebnem Taylor, James C K Taylor, Annabel L Dobnikar, Lina Chappell, Joel Harman, Jennifer L Figg, Nichola L Finigan, Alison Foote, Kirsty Uryga, Anna K Bennett, Martin R Spivakov, Mikhail Jørgensen, Helle F Cardiovasc Res Original Article AIMS: Quiescent, differentiated adult vascular smooth muscle cells (VSMCs) can be induced to proliferate and switch phenotype. Such plasticity underlies blood vessel homeostasis and contributes to vascular disease development. Oligoclonal VSMC contribution is a hallmark of end-stage vascular disease. Here, we aim to understand cellular mechanisms underpinning generation of this VSMC oligoclonality. METHODS AND RESULTS: We investigate the dynamics of VSMC clone formation using confocal microscopy and single-cell transcriptomics in VSMC-lineage-traced animal models. We find that activation of medial VSMC proliferation occurs at low frequency after vascular injury and that only a subset of expanding clones migrate, which together drives formation of oligoclonal neointimal lesions. VSMC contribution in small atherosclerotic lesions is typically from one or two clones, similar to observations in mature lesions. Low frequency (<0.1%) of clonal VSMC proliferation is also observed in vitro. Single-cell RNA-sequencing revealed progressive cell state changes across a contiguous VSMC population at onset of injury-induced proliferation. Proliferating VSMCs mapped selectively to one of two distinct trajectories and were associated with cells showing extensive phenotypic switching. A proliferation-associated transitory state shared pronounced similarities with atypical SCA1+ VSMCs from uninjured mouse arteries and VSMCs in healthy human aorta. We show functionally that clonal expansion of SCA1+ VSMCs from healthy arteries occurs at higher rate and frequency compared with SCA1− cells. CONCLUSION: Our data suggest that activation of proliferation at low frequency is a general, cell-intrinsic feature of VSMCs. We show that rare VSMCs in healthy arteries display VSMC phenotypic switching akin to that observed in pathological vessel remodelling and that this is a conserved feature of mouse and human healthy arteries. The increased proliferation of modulated VSMCs from healthy arteries suggests that these cells respond more readily to disease-inducing cues and could drive oligoclonal VSMC expansion. Oxford University Press 2022-08-22 /pmc/articles/PMC10202649/ /pubmed/35994249 http://dx.doi.org/10.1093/cvr/cvac138 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the European Society of Cardiology. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Worssam, Matt D
Lambert, Jordi
Oc, Sebnem
Taylor, James C K
Taylor, Annabel L
Dobnikar, Lina
Chappell, Joel
Harman, Jennifer L
Figg, Nichola L
Finigan, Alison
Foote, Kirsty
Uryga, Anna K
Bennett, Martin R
Spivakov, Mikhail
Jørgensen, Helle F
Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
title Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
title_full Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
title_fullStr Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
title_full_unstemmed Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
title_short Cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
title_sort cellular mechanisms of oligoclonal vascular smooth muscle cell expansion in cardiovascular disease
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10202649/
https://www.ncbi.nlm.nih.gov/pubmed/35994249
http://dx.doi.org/10.1093/cvr/cvac138
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