Literature DB >> 14764454

Regeneration of the infarcted heart with stem cells derived by nuclear transplantation.

Robert Lanza1, Malcolm A S Moore, Teruhiko Wakayama, Anthony C F Perry, Jae-Hung Shieh, Jan Hendrikx, Annarosa Leri, Stefano Chimenti, Alyssa Monsen, Daria Nurzynska, Michael D West, Jan Kajstura, Piero Anversa.   

Abstract

Nuclear transfer techniques have been proposed as a strategy for generating an unlimited supply of rejuvenated and histocompatible stem cells for the treatment of cardiac diseases. For this purpose, c-kit-positive fetal liver stem cells obtained from cloned embryos were injected in the border zone of infarcted mice to induce tissue reconstitution. Cloned embryos were derived from somatic cell fusion between nuclei of cultured LacZ-positive fibroblasts and enucleated oocytes of a different mouse strain. We report that regenerating myocardium replaced 38% of the scar at 1 month. The rebuilt tissue expressed LacZ and was composed of myocytes and vessels connected with the coronary circulation. Myocytes were functionally competent and expressed contractile proteins, desmin, connexin43, and N-cadherin. These structural characteristics indicated that the new myocytes were electrically and mechanically coupled. Similarly, the formed coronary arterioles and capillary structures contained blood and contributed, therefore, to tissue oxygenation. Cardiac replacement resulted in an improvement of ventricular hemodynamics and in a reduction of diastolic wall stress. These beneficial effects were obtained by stem cell transdifferentiation and commitment to the cardiac cell lineages. Myocardial growth was independent from fusion of the injected stem cells with preexisting partner cells. In conclusion, c-kit-positive stem cells derived by nuclear transfer cloning restore infarcted myocardium. Although problems currently plague nuclear transplantation, including the potential for epigenetic and imprinting abnormalities, stem cells derived from cloned embryos are sufficiently normal to repair damaged tissue in vivo. Importantly, the magnitude of myocardial regeneration obtained in this study is significantly superior to that achieved with adult bone marrow cells.

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Year:  2004        PMID: 14764454     DOI: 10.1161/01.RES.0000120863.53562.DF

Source DB:  PubMed          Journal:  Circ Res        ISSN: 0009-7330            Impact factor:   17.367


  16 in total

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Authors:  Jonathan H Dinsmore; Nabil Dib
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Review 4.  Stem cell treatment of the heart: a review of its current status on the brink of clinical experimentation.

Authors:  Paolo Angelini; Roger R Markwald
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Review 5.  Stem cell therapies for heart disease: why do we need bioengineers?

Authors:  Nenad Bursac
Journal:  IEEE Eng Med Biol Mag       Date:  2007 Jul-Aug

Review 6.  The problem of deception in embryonic stem cell research.

Authors:  R M Doerflinger
Journal:  Cell Prolif       Date:  2008-02       Impact factor: 6.831

7.  Embryonic stem cells attenuate myocardial dysfunction and inflammation after surgical global ischemia via paracrine actions.

Authors:  Paul R Crisostomo; Aaron M Abarbanell; Meijing Wang; Tim Lahm; Yue Wang; Daniel R Meldrum
Journal:  Am J Physiol Heart Circ Physiol       Date:  2008-08-22       Impact factor: 4.733

Review 8.  Stem cell therapy for heart failure.

Authors:  Robert E Michler
Journal:  Methodist Debakey Cardiovasc J       Date:  2013 Oct-Dec

Review 9.  The future of human nuclear transfer?

Authors:  Lyle Armstrong; Majlinda Lako
Journal:  Stem Cell Rev       Date:  2006       Impact factor: 5.739

10.  Lin-c-kit(+) BM-derived stem cells repair Infarcted Heart.

Authors:  M Khan; S Mohsin; Sn Khan; S Riazuddin
Journal:  J Stem Cells Regen Med       Date:  2010-04-05
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