Mutational landscape of atherosclerotic plaques reveals large clonal cell populations

Lasse Bach Steffensen; Stephanie Kavan; Pia Søndergaard Jensen; Matilde Kvist Pedersen; Steffen Møller Bøttger; Martin J Larsen; Maja Dembic; Otto Bergman; Ljubica Matic; Ulf Hedin; Lars vB Andersen; Jes Sanddal Lindholt; Kim Christian Houlind; Lars P Riber; Mads Thomassen; Lars Melholt Rasmussen

doi:10.1172/jci.insight.188281

Mutational landscape of atherosclerotic plaques reveals large clonal cell populations

Lasse Bach Steffensen^*, Stephanie Kavan, Pia Søndergaard Jensen, Matilde Kvist Pedersen, Steffen Møller Bøttger, Martin J Larsen, Maja Dembic, Otto Bergman, Ljubica Matic, Ulf Hedin, Lars vB Andersen, Jes Sanddal Lindholt, Kim Christian Houlind, Lars P Riber, Mads Thomassen, Lars Melholt Rasmussen

^*Kontaktforfatter

Karolinska Institutet

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

Abstract

The notion of clonal cell populations in human atherosclerosis has been suggested but not demonstrated. Somatic mutations are used to define cellular clones in tumors. Here, we characterized the mutational landscape of human carotid plaques through whole-exome sequencing to explore the presence of clonal cell populations. Somatic mutations were identified in 12 of 13 investigated plaques, while no mutations were detected in 11 non-atherosclerotic arteries. Mutated clones often constituted over 10% of the sample cell population, with genes related to the contractile apparatus enriched for mutations. In carriers of clonal hematopoiesis of indeterminate potential (CHIP), hematopoietic clones had infiltrated the plaque tissue and constituted substantial fractions of the plaque cell population alongside locally expanded clones. Our findings establish somatic mutations as a common feature of human atherosclerosis and demonstrate the existence of mutated clones expanding locally, as well as CHIP clones invading from the circulation. While our data do not support plaque monoclonality, we observed a pattern suggesting the coexistence of multiple mutated clones of considerable size spanning different regions of plaques. Mutated clones are likely to be relevant to disease development, and somatic mutations will serve as a convenient tool to uncover novel pathological processes of atherosclerosis in future studies.

Originalsprog	Engelsk
Artikelnummer	e188281
Tidsskrift	JCI Insight
Vol/bind	10
Udgave nummer	10
Antal sider	17
ISSN	2379-3708
DOI	https://doi.org/10.1172/jci.insight.188281 https://doi.org/10.1172/jci.insight.188281
Status	Udgivet - 22. maj 2025

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Steffensen, L. B., Kavan, S., Jensen, P. S., Pedersen, M. K., Bøttger, S. M., Larsen, M. J., Dembic, M., Bergman, O., Matic, L., Hedin, U., Andersen, L. VB., Lindholt, J. S., Houlind, K. C., Riber, L. P., Thomassen, M., & Rasmussen, L. M. (2025). Mutational landscape of atherosclerotic plaques reveals large clonal cell populations. JCI Insight, 10(10), Artikel e188281. https://doi.org/10.1172/jci.insight.188281, https://doi.org/10.1172/jci.insight.188281

@article{29d45eb1bcc641a6b6b181ebff653c04,

title = "Mutational landscape of atherosclerotic plaques reveals large clonal cell populations",

abstract = "The notion of clonal cell populations in human atherosclerosis has been suggested but not demonstrated. Somatic mutations are used to define cellular clones in tumors. Here, we characterized the mutational landscape of human carotid plaques through whole-exome sequencing to explore the presence of clonal cell populations. Somatic mutations were identified in 12 of 13 investigated plaques, while no mutations were detected in 11 non-atherosclerotic arteries. Mutated clones often constituted over 10% of the sample cell population, with genes related to the contractile apparatus enriched for mutations. In carriers of clonal hematopoiesis of indeterminate potential (CHIP), hematopoietic clones had infiltrated the plaque tissue and constituted substantial fractions of the plaque cell population alongside locally expanded clones. Our findings establish somatic mutations as a common feature of human atherosclerosis and demonstrate the existence of mutated clones expanding locally, as well as CHIP clones invading from the circulation. While our data do not support plaque monoclonality, we observed a pattern suggesting the coexistence of multiple mutated clones of considerable size spanning different regions of plaques. Mutated clones are likely to be relevant to disease development, and somatic mutations will serve as a convenient tool to uncover novel pathological processes of atherosclerosis in future studies.",

keywords = "Aged, Atherosclerosis/genetics, Carotid Arteries/pathology, Clonal Hematopoiesis/genetics, Clone Cells/pathology, Exome Sequencing, Female, Humans, Male, Middle Aged, Mutation, Plaque, Atherosclerotic/genetics",

author = "Steffensen, {Lasse Bach} and Stephanie Kavan and Jensen, {Pia S{\o}ndergaard} and Pedersen, {Matilde Kvist} and B{\o}ttger, {Steffen M{\o}ller} and Larsen, {Martin J} and Maja Dembic and Otto Bergman and Ljubica Matic and Ulf Hedin and Andersen, {Lars vB} and Lindholt, {Jes Sanddal} and Houlind, {Kim Christian} and Riber, {Lars P} and Mads Thomassen and Rasmussen, {Lars Melholt}",

year = "2025",

month = may,

day = "22",

doi = "10.1172/jci.insight.188281",

language = "English",

volume = "10",

journal = "JCI Insight",

issn = "2379-3708",

publisher = "American Society for Clinical Investigation",

number = "10",

}

Steffensen, LB, Kavan, S, Jensen, PS, Pedersen, MK , Bøttger, SM , Larsen, MJ , Dembic, M, Bergman, O, Matic, L, Hedin, U, Andersen, LVB, Lindholt, JS , Houlind, KC , Riber, LP , Thomassen, M & Rasmussen, LM 2025, 'Mutational landscape of atherosclerotic plaques reveals large clonal cell populations', JCI Insight, bind 10, nr. 10, e188281. https://doi.org/10.1172/jci.insight.188281, https://doi.org/10.1172/jci.insight.188281

TY - JOUR

T1 - Mutational landscape of atherosclerotic plaques reveals large clonal cell populations

AU - Steffensen, Lasse Bach

AU - Kavan, Stephanie

AU - Jensen, Pia Søndergaard

AU - Pedersen, Matilde Kvist

AU - Bøttger, Steffen Møller

AU - Larsen, Martin J

AU - Dembic, Maja

AU - Bergman, Otto

AU - Matic, Ljubica

AU - Hedin, Ulf

AU - Andersen, Lars vB

AU - Lindholt, Jes Sanddal

AU - Houlind, Kim Christian

AU - Riber, Lars P

AU - Thomassen, Mads

AU - Rasmussen, Lars Melholt

PY - 2025/5/22

Y1 - 2025/5/22

N2 - The notion of clonal cell populations in human atherosclerosis has been suggested but not demonstrated. Somatic mutations are used to define cellular clones in tumors. Here, we characterized the mutational landscape of human carotid plaques through whole-exome sequencing to explore the presence of clonal cell populations. Somatic mutations were identified in 12 of 13 investigated plaques, while no mutations were detected in 11 non-atherosclerotic arteries. Mutated clones often constituted over 10% of the sample cell population, with genes related to the contractile apparatus enriched for mutations. In carriers of clonal hematopoiesis of indeterminate potential (CHIP), hematopoietic clones had infiltrated the plaque tissue and constituted substantial fractions of the plaque cell population alongside locally expanded clones. Our findings establish somatic mutations as a common feature of human atherosclerosis and demonstrate the existence of mutated clones expanding locally, as well as CHIP clones invading from the circulation. While our data do not support plaque monoclonality, we observed a pattern suggesting the coexistence of multiple mutated clones of considerable size spanning different regions of plaques. Mutated clones are likely to be relevant to disease development, and somatic mutations will serve as a convenient tool to uncover novel pathological processes of atherosclerosis in future studies.

AB - The notion of clonal cell populations in human atherosclerosis has been suggested but not demonstrated. Somatic mutations are used to define cellular clones in tumors. Here, we characterized the mutational landscape of human carotid plaques through whole-exome sequencing to explore the presence of clonal cell populations. Somatic mutations were identified in 12 of 13 investigated plaques, while no mutations were detected in 11 non-atherosclerotic arteries. Mutated clones often constituted over 10% of the sample cell population, with genes related to the contractile apparatus enriched for mutations. In carriers of clonal hematopoiesis of indeterminate potential (CHIP), hematopoietic clones had infiltrated the plaque tissue and constituted substantial fractions of the plaque cell population alongside locally expanded clones. Our findings establish somatic mutations as a common feature of human atherosclerosis and demonstrate the existence of mutated clones expanding locally, as well as CHIP clones invading from the circulation. While our data do not support plaque monoclonality, we observed a pattern suggesting the coexistence of multiple mutated clones of considerable size spanning different regions of plaques. Mutated clones are likely to be relevant to disease development, and somatic mutations will serve as a convenient tool to uncover novel pathological processes of atherosclerosis in future studies.

KW - Aged

KW - Atherosclerosis/genetics

KW - Carotid Arteries/pathology

KW - Clonal Hematopoiesis/genetics

KW - Clone Cells/pathology

KW - Exome Sequencing

KW - Female

KW - Humans

KW - Male

KW - Middle Aged

KW - Mutation

KW - Plaque, Atherosclerotic/genetics

U2 - 10.1172/jci.insight.188281

DO - 10.1172/jci.insight.188281

M3 - Journal article

C2 - 40198128

SN - 2379-3708

VL - 10

JO - JCI Insight

JF - JCI Insight

IS - 10

M1 - e188281

ER -

Mutational landscape of atherosclerotic plaques reveals large clonal cell populations

Abstract

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