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Altering Sphingolipid Metabolism Attenuates Cell Death and Inflammatory Response After Myocardial Infarction.
Hadas, Yoav; Vincek, Adam S; Youssef, Elias; Zak, Magdalena M; Chepurko, Elena; Sultana, Nishat; Sharkar, Mohammad Tofael Kabir; Guo, Ningning; Komargodski, Rinat; Kurian, Ann Anu; Kaur, Keerat; Magadum, Ajit; Fargnoli, Anthony; Katz, Michael G; Hossain, Nadia; Kenigsberg, Ephraim; Dubois, Nicole C; Schadt, Eric; Hajjar, Roger; Eliyahu, Efrat; Zangi, Lior.
Afiliação
  • Hadas Y; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Vincek AS; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Youssef E; Black Family Stem Cell Institute (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., N.C.D.), Icahn School of Medicine at Mount Sinai, New York.
  • Zak MM; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Chepurko E; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Sultana N; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Sharkar MTK; Black Family Stem Cell Institute (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., N.C.D.), Icahn School of Medicine at Mount Sinai, New York.
  • Guo N; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Komargodski R; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Kurian AA; Black Family Stem Cell Institute (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., N.C.D.), Icahn School of Medicine at Mount Sinai, New York.
  • Kaur K; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Magadum A; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Fargnoli A; Black Family Stem Cell Institute (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., N.C.D.), Icahn School of Medicine at Mount Sinai, New York.
  • Katz MG; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Hossain N; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Kenigsberg E; Black Family Stem Cell Institute (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., N.C.D.), Icahn School of Medicine at Mount Sinai, New York.
  • Dubois NC; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Schadt E; Black Family Stem Cell Institute (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., N.C.D.), Icahn School of Medicine at Mount Sinai, New York.
  • Hajjar R; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
  • Eliyahu E; Cardiovascular Research Center (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.F, M.G.K.), Icahn School of Medicine at Mount Sinai, New York.
  • Zangi L; Department of Genetics and Genomic Sciences (Y.H., E.Y., M.M.Z., E.C., N.S., M.T.K.S., R.K., A.A.K., K.K., A.M., N.H., L.Z., A.S.V., N.G., E.K., E.S., E.E.), Icahn School of Medicine at Mount Sinai, New York.
Circulation ; 141(11): 916-930, 2020 03 17.
Article em En | MEDLINE | ID: mdl-31992066
ABSTRACT

BACKGROUND:

Sphingolipids have recently emerged as a biomarker of recurrence and mortality after myocardial infarction (MI). The increased ceramide levels in mammalian heart tissues during acute MI, as demonstrated by several groups, is associated with higher cell death rates in the left ventricle and deteriorated cardiac function. Ceramidase, the only enzyme known to hydrolyze proapoptotic ceramide, generates sphingosine, which is then phosphorylated by sphingosine kinase to produce the prosurvival molecule sphingosine-1-phosphate. We hypothesized that Acid Ceramidase (AC) overexpression would counteract the negative effects of elevated ceramide and promote cell survival, thereby providing cardioprotection after MI.

METHODS:

We performed transcriptomic, sphingolipid, and protein analyses to evaluate sphingolipid metabolism and signaling post-MI. We investigated the effect of altering ceramide metabolism through a loss (chemical inhibitors) or gain (modified mRNA [modRNA]) of AC function post hypoxia or MI.

RESULTS:

We found that several genes involved in de novo ceramide synthesis were upregulated and that ceramide (C16, C20, C201, and C24) levels had significantly increased 24 hours after MI. AC inhibition after hypoxia or MI resulted in reduced AC activity and increased cell death. By contrast, enhancing AC activity via AC modRNA treatment increased cell survival after hypoxia or MI. AC modRNA-treated mice had significantly better heart function, longer survival, and smaller scar size than control mice 28 days post-MI. We attributed the improvement in heart function post-MI after AC modRNA delivery to decreased ceramide levels, lower cell death rates, and changes in the composition of the immune cell population in the left ventricle manifested by lowered abundance of proinflammatory detrimental neutrophils.

CONCLUSIONS:

Our findings suggest that transiently altering sphingolipid metabolism through AC overexpression is sufficient and necessary to induce cardioprotection post-MI, thereby highlighting the therapeutic potential of AC modRNA in ischemic heart disease.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Esfingolipídeos / RNA Mensageiro / Terapia Genética / Ceramidase Ácida / Hipóxia / Infarto do Miocárdio Tipo de estudo: Etiology_studies Limite: Animals / Female / Humans / Male Idioma: En Ano de publicação: 2020 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Esfingolipídeos / RNA Mensageiro / Terapia Genética / Ceramidase Ácida / Hipóxia / Infarto do Miocárdio Tipo de estudo: Etiology_studies Limite: Animals / Female / Humans / Male Idioma: En Ano de publicação: 2020 Tipo de documento: Article