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FHL5 Controls Vascular Disease-Associated Gene Programs in Smooth Muscle Cells.
Wong, Doris; Auguste, Gaëlle; Lino Cardenas, Christian L; Turner, Adam W; Chen, Yixuan; Song, Yipei; Ma, Lijiang; Perry, R Noah; Aherrahrou, Redouane; Kuppusamy, Maniselvan; Yang, Chaojie; Mosquera, Jose Verdezoto; Dube, Collin J; Khan, Mohammad Daud; Palmore, Meredith; Kalra, Jaspreet; Kavousi, Maryam; Peyser, Patricia A; Matic, Ljubica; Hedin, Ulf; Manichaikul, Ani; Sonkusare, Swapnil K; Civelek, Mete; Kovacic, Jason C; Björkegren, Johan L M; Malhotra, Rajeev; Miller, Clint L.
Afiliação
  • Wong D; Department of Biochemistry and Molecular Genetics (D.W., C.Y., J.V.M., A.M., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Auguste G; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Lino Cardenas CL; Robert M. Berne Cardiovascular Research Center (D.W., R.N.P., M. Kuppusamy, S.K.S., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Turner AW; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Chen Y; Cardiovascular Research Center, Cardiology Division, Department of Medicine, Massachusetts General Hospital, Harvard Medical School, Boston (C.L.L.C., R.M.).
  • Song Y; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Ma L; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Perry RN; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Aherrahrou R; Department of Genetics and Genomic Sciences, Icahn Institute for Genomics and Multiscale Biology (L. Ma, J.L.M.B.), Icahn School of Medicine at Mount Sinai, New York.
  • Kuppusamy M; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Yang C; Robert M. Berne Cardiovascular Research Center (D.W., R.N.P., M. Kuppusamy, S.K.S., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Mosquera JV; Department of Biomedical Engineering (R.N.P., M.C.), University of Virginia, Charlottesville. A.I.
  • Dube CJ; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Khan MD; Virtanen Institute for Molecular Sciences, University of Eastern Finland, Finland (R.A.).
  • Palmore M; Institute for Cardiogenetics, Universität zu Lübeck, DZHK (German Centre for Cardiovascular Research), Partner Site Hamburg/Kiel/Lübeck, Germany, University Heart Centre Lübeck, Lübeck, Germany (R.A.).
  • Kalra J; Robert M. Berne Cardiovascular Research Center (D.W., R.N.P., M. Kuppusamy, S.K.S., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Kavousi M; Department of Biochemistry and Molecular Genetics (D.W., C.Y., J.V.M., A.M., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Peyser PA; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Matic L; Department of Biochemistry and Molecular Genetics (D.W., C.Y., J.V.M., A.M., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Hedin U; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Manichaikul A; Department of Microbiology, Immunology, and Cancer Biology (C.J.D.), University of Virginia, Charlottesville. A.I.
  • Sonkusare SK; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Civelek M; Center for Public Health Genomics (D.W., G.A., A.W.T., Y.C., Y.S., R.N.P., R.A., C.Y., J.V.M., D.K., M.P., A.M., M.C., C.L.M.), University of Virginia, Charlottesville. A.I.
  • Kovacic JC; Department of Molecular Physiology and Biological Physics (J.K., S.K.S.), University of Virginia, Charlottesville. A.I.
  • Björkegren JLM; Department of Epidemiology, Erasmus University Medical Center, the Netherlands (M. Kavousi).
  • Malhotra R; Department of Epidemiology, University of Michigan, Ann Arbor (P.A.P.).
  • Miller CL; Department of Molecular Medicine and Surgery, Karolinska Institutet, Stockholm, Sweden (L. Matic, U.H.).
Circ Res ; 132(9): 1144-1161, 2023 04 28.
Article em En | MEDLINE | ID: mdl-37017084
ABSTRACT

BACKGROUND:

Genome-wide association studies have identified hundreds of loci associated with common vascular diseases, such as coronary artery disease, myocardial infarction, and hypertension. However, the lack of mechanistic insights for many GWAS loci limits their translation into the clinic. Among these loci with unknown functions is UFL1-four-and-a-half LIM (LIN-11, Isl-1, MEC-3) domain 5 (FHL5; chr6q16.1), which reached genome-wide significance in a recent coronary artery disease/ myocardial infarction GWAS meta-analysis. UFL1-FHL5 is also associated with several vascular diseases, consistent with the widespread pleiotropy observed for GWAS loci.

METHODS:

We apply a multimodal approach leveraging statistical fine-mapping, epigenomic profiling, and ex vivo analysis of human coronary artery tissues to implicate FHL5 as the top candidate causal gene. We unravel the molecular mechanisms of the cross-phenotype genetic associations through in vitro functional analyses and epigenomic profiling experiments in coronary artery smooth muscle cells.

RESULTS:

We prioritized FHL5 as the top candidate causal gene at the UFL1-FHL5 locus through expression quantitative trait locus colocalization methods. FHL5 gene expression was enriched in the smooth muscle cells and pericyte population in human artery tissues with coexpression network analyses supporting a functional role in regulating smooth muscle cell contraction. Unexpectedly, under procalcifying conditions, FHL5 overexpression promoted vascular calcification and dysregulated processes related to extracellular matrix organization and calcium handling. Lastly, by mapping FHL5 binding sites and inferring FHL5 target gene function using artery tissue gene regulatory network analyses, we highlight regulatory interactions between FHL5 and downstream coronary artery disease/myocardial infarction loci, such as FOXL1 and FN1 that have roles in vascular remodeling.

CONCLUSIONS:

Taken together, these studies provide mechanistic insights into the pleiotropic genetic associations of UFL1-FHL5. We show that FHL5 mediates vascular disease risk through transcriptional regulation of downstream vascular remodeling gene programs. These transacting mechanisms may explain a portion of the heritable risk for complex vascular diseases.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Doença da Artéria Coronariana / Hipertensão / Infarto do Miocárdio Tipo de estudo: Prognostic_studies / Risk_factors_studies / Systematic_reviews Limite: Humans Idioma: En Ano de publicação: 2023 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Doença da Artéria Coronariana / Hipertensão / Infarto do Miocárdio Tipo de estudo: Prognostic_studies / Risk_factors_studies / Systematic_reviews Limite: Humans Idioma: En Ano de publicação: 2023 Tipo de documento: Article