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Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3

BACKGROUND: Bone marrow stem cell clonal dysfunction by somatic mutation is suspected to affect post-infarction myocardial regeneration after coronary bypass surgery (CABG). METHODS: Transcriptome and variant expression analysis was studied in the phase 3 PERFECT trial post myocardial infarction CAB...

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Autores principales: Wolfien, Markus, Klatt, Denise, Salybekov, Amankeldi A., Ii, Masaaki, Komatsu-Horii, Miki, Gaebel, Ralf, Philippou-Massier, Julia, Schrinner, Eric, Akimaru, Hiroshi, Akimaru, Erika, David, Robert, Garbade, Jens, Gummert, Jan, Haverich, Axel, Hennig, Holger, Iwasaki, Hiroto, Kaminski, Alexander, Kawamoto, Atsuhiko, Klopsch, Christian, Kowallick, Johannes T., Krebs, Stefan, Nesteruk, Julia, Reichenspurner, Hermann, Ritter, Christian, Stamm, Christof, Tani-Yokoyama, Ayumi, Blum, Helmut, Wolkenhauer, Olaf, Schambach, Axel, Asahara, Takayuki, Steinhoff, Gustav
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7339012/
https://www.ncbi.nlm.nih.gov/pubmed/32629392
http://dx.doi.org/10.1016/j.ebiom.2020.102862
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author Wolfien, Markus
Klatt, Denise
Salybekov, Amankeldi A.
Ii, Masaaki
Komatsu-Horii, Miki
Gaebel, Ralf
Philippou-Massier, Julia
Schrinner, Eric
Akimaru, Hiroshi
Akimaru, Erika
David, Robert
Garbade, Jens
Gummert, Jan
Haverich, Axel
Hennig, Holger
Iwasaki, Hiroto
Kaminski, Alexander
Kawamoto, Atsuhiko
Klopsch, Christian
Kowallick, Johannes T.
Krebs, Stefan
Nesteruk, Julia
Reichenspurner, Hermann
Ritter, Christian
Stamm, Christof
Tani-Yokoyama, Ayumi
Blum, Helmut
Wolkenhauer, Olaf
Schambach, Axel
Asahara, Takayuki
Steinhoff, Gustav
author_facet Wolfien, Markus
Klatt, Denise
Salybekov, Amankeldi A.
Ii, Masaaki
Komatsu-Horii, Miki
Gaebel, Ralf
Philippou-Massier, Julia
Schrinner, Eric
Akimaru, Hiroshi
Akimaru, Erika
David, Robert
Garbade, Jens
Gummert, Jan
Haverich, Axel
Hennig, Holger
Iwasaki, Hiroto
Kaminski, Alexander
Kawamoto, Atsuhiko
Klopsch, Christian
Kowallick, Johannes T.
Krebs, Stefan
Nesteruk, Julia
Reichenspurner, Hermann
Ritter, Christian
Stamm, Christof
Tani-Yokoyama, Ayumi
Blum, Helmut
Wolkenhauer, Olaf
Schambach, Axel
Asahara, Takayuki
Steinhoff, Gustav
author_sort Wolfien, Markus
collection PubMed
description BACKGROUND: Bone marrow stem cell clonal dysfunction by somatic mutation is suspected to affect post-infarction myocardial regeneration after coronary bypass surgery (CABG). METHODS: Transcriptome and variant expression analysis was studied in the phase 3 PERFECT trial post myocardial infarction CABG and CD133(+) bone marrow derived hematopoetic stem cells showing difference in left ventricular ejection fraction (∆LVEF) myocardial regeneration Responders (n=14; ∆LVEF +16% day 180/0) and Non-responders (n=9; ∆LVEF -1.1% day 180/0). Subsequently, the findings have been validated in an independent patient cohort (n=14) as well as in two preclinical mouse models investigating SH2B3/LNK antisense or knockout deficient conditions. FINDINGS: 1. Clinical: R differed from NR in a total of 161 genes in differential expression (n=23, q<0•05) and 872 genes in coexpression analysis (n=23, q<0•05). Machine Learning clustering analysis revealed distinct RvsNR preoperative gene-expression signatures in peripheral blood acorrelated to SH2B3 (p<0.05). Mutation analysis revealed increased specific variants in RvsNR. (R: 48 genes; NR: 224 genes). 2. Preclinical:SH2B3/LNK-silenced hematopoietic stem cell (HSC) clones displayed significant overgrowth of myeloid and immune cells in bone marrow, peripheral blood, and tissue at day 160 after competitive bone-marrow transplantation into mice. SH2B3/LNK(−/−) mice demonstrated enhanced cardiac repair through augmenting the kinetics of bone marrow-derived endothelial progenitor cells, increased capillary density in ischemic myocardium, and reduced left ventricular fibrosis with preserved cardiac function. 3. Validation: Evaluation analysis in 14 additional patients revealed 85% RvsNR (12/14 patients) prediction accuracy for the identified biomarker signature. INTERPRETATION: Myocardial repair is affected by HSC gene response and somatic mutation. Machine Learning can be utilized to identify and predict pathological HSC response. FUNDING: German Ministry of Research and Education (BMBF): Reference and Translation Center for Cardiac Stem Cell Therapy - FKZ0312138A and FKZ031L0106C, German Ministry of Research and Education (BMBF): Collaborative research center - DFG:SFB738 and Center of Excellence - DFG:EC-REBIRTH), European Social Fonds: ESF/IV-WM-B34-0011/08, ESF/IV-WM-B34-0030/10, and Miltenyi Biotec GmbH, Bergisch-Gladbach, Germany. Japanese Ministry of Health : Health and Labour Sciences Research Grant (H14-trans-001, H17-trans-002) TRIAL REGISTRATION: ClinicalTrials.gov NCT00950274
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spelling pubmed-73390122020-07-14 Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3 Wolfien, Markus Klatt, Denise Salybekov, Amankeldi A. Ii, Masaaki Komatsu-Horii, Miki Gaebel, Ralf Philippou-Massier, Julia Schrinner, Eric Akimaru, Hiroshi Akimaru, Erika David, Robert Garbade, Jens Gummert, Jan Haverich, Axel Hennig, Holger Iwasaki, Hiroto Kaminski, Alexander Kawamoto, Atsuhiko Klopsch, Christian Kowallick, Johannes T. Krebs, Stefan Nesteruk, Julia Reichenspurner, Hermann Ritter, Christian Stamm, Christof Tani-Yokoyama, Ayumi Blum, Helmut Wolkenhauer, Olaf Schambach, Axel Asahara, Takayuki Steinhoff, Gustav EBioMedicine Research paper BACKGROUND: Bone marrow stem cell clonal dysfunction by somatic mutation is suspected to affect post-infarction myocardial regeneration after coronary bypass surgery (CABG). METHODS: Transcriptome and variant expression analysis was studied in the phase 3 PERFECT trial post myocardial infarction CABG and CD133(+) bone marrow derived hematopoetic stem cells showing difference in left ventricular ejection fraction (∆LVEF) myocardial regeneration Responders (n=14; ∆LVEF +16% day 180/0) and Non-responders (n=9; ∆LVEF -1.1% day 180/0). Subsequently, the findings have been validated in an independent patient cohort (n=14) as well as in two preclinical mouse models investigating SH2B3/LNK antisense or knockout deficient conditions. FINDINGS: 1. Clinical: R differed from NR in a total of 161 genes in differential expression (n=23, q<0•05) and 872 genes in coexpression analysis (n=23, q<0•05). Machine Learning clustering analysis revealed distinct RvsNR preoperative gene-expression signatures in peripheral blood acorrelated to SH2B3 (p<0.05). Mutation analysis revealed increased specific variants in RvsNR. (R: 48 genes; NR: 224 genes). 2. Preclinical:SH2B3/LNK-silenced hematopoietic stem cell (HSC) clones displayed significant overgrowth of myeloid and immune cells in bone marrow, peripheral blood, and tissue at day 160 after competitive bone-marrow transplantation into mice. SH2B3/LNK(−/−) mice demonstrated enhanced cardiac repair through augmenting the kinetics of bone marrow-derived endothelial progenitor cells, increased capillary density in ischemic myocardium, and reduced left ventricular fibrosis with preserved cardiac function. 3. Validation: Evaluation analysis in 14 additional patients revealed 85% RvsNR (12/14 patients) prediction accuracy for the identified biomarker signature. INTERPRETATION: Myocardial repair is affected by HSC gene response and somatic mutation. Machine Learning can be utilized to identify and predict pathological HSC response. FUNDING: German Ministry of Research and Education (BMBF): Reference and Translation Center for Cardiac Stem Cell Therapy - FKZ0312138A and FKZ031L0106C, German Ministry of Research and Education (BMBF): Collaborative research center - DFG:SFB738 and Center of Excellence - DFG:EC-REBIRTH), European Social Fonds: ESF/IV-WM-B34-0011/08, ESF/IV-WM-B34-0030/10, and Miltenyi Biotec GmbH, Bergisch-Gladbach, Germany. Japanese Ministry of Health : Health and Labour Sciences Research Grant (H14-trans-001, H17-trans-002) TRIAL REGISTRATION: ClinicalTrials.gov NCT00950274 Elsevier 2020-07-04 /pmc/articles/PMC7339012/ /pubmed/32629392 http://dx.doi.org/10.1016/j.ebiom.2020.102862 Text en © 2020 The Author(s) http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research paper
Wolfien, Markus
Klatt, Denise
Salybekov, Amankeldi A.
Ii, Masaaki
Komatsu-Horii, Miki
Gaebel, Ralf
Philippou-Massier, Julia
Schrinner, Eric
Akimaru, Hiroshi
Akimaru, Erika
David, Robert
Garbade, Jens
Gummert, Jan
Haverich, Axel
Hennig, Holger
Iwasaki, Hiroto
Kaminski, Alexander
Kawamoto, Atsuhiko
Klopsch, Christian
Kowallick, Johannes T.
Krebs, Stefan
Nesteruk, Julia
Reichenspurner, Hermann
Ritter, Christian
Stamm, Christof
Tani-Yokoyama, Ayumi
Blum, Helmut
Wolkenhauer, Olaf
Schambach, Axel
Asahara, Takayuki
Steinhoff, Gustav
Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3
title Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3
title_full Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3
title_fullStr Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3
title_full_unstemmed Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3
title_short Hematopoietic stem-cell senescence and myocardial repair - Coronary artery disease genotype/phenotype analysis of post-MI myocardial regeneration response induced by CABG/CD133+ bone marrow hematopoietic stem cell treatment in RCT PERFECT Phase 3
title_sort hematopoietic stem-cell senescence and myocardial repair - coronary artery disease genotype/phenotype analysis of post-mi myocardial regeneration response induced by cabg/cd133+ bone marrow hematopoietic stem cell treatment in rct perfect phase 3
topic Research paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7339012/
https://www.ncbi.nlm.nih.gov/pubmed/32629392
http://dx.doi.org/10.1016/j.ebiom.2020.102862
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