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SDF1 gradient associates with the distribution of c-Kit+ cardiac cells in the heart.


ABSTRACT: Identification of the adult cardiac stem cells (CSCs) has offered new therapeutic possibilities for treating ischemic myocardium. CSCs positive for the cell surface antigen c-Kit are known as the primary source for cardiac regeneration. Accumulating evidence shows that chemokines play important roles in stem cell homing. Here we investigated molecular targets to be utilized in modulating the mobility of endogenous CSCs. In a four week follow-up after experimental acute myocardial infarction (AMI) with ligation of the left anterior descending (LAD) coronary artery of Sprague-Dawley rats c-Kit+ CSCs redistributed in the heart. The number of c-Kit+ CSCs in the atrial c-Kit niche was diminished, whereas increased amount was observed in the left ventricle and apex. This was associated with increased expression of stromal cell-derived factor 1 alpha (SDF1?), and a significant positive correlation was found between c-Kit+ CSCs and SDF1? expression in the heart. Moreover, the migratory capacity of isolated c-Kit+ CSCs was induced by SDF1 treatment in vitro. We conclude that upregulation of SDF1? after AMI associates with increased expression of endogenous c-Kit+ CSCs in the injury area, and show induced migration of c-Kit+ cells by SDF1.

SUBMITTER: Renko O 

PROVIDER: S-EPMC5773575 | biostudies-literature | 2018 Jan

REPOSITORIES: biostudies-literature

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SDF1 gradient associates with the distribution of c-Kit+ cardiac cells in the heart.

Renko Outi O   Tolonen Anna-Maria AM   Rysä Jaana J   Magga Johanna J   Mustonen Erja E   Ruskoaho Heikki H   Serpi Raisa R  

Scientific reports 20180118 1


Identification of the adult cardiac stem cells (CSCs) has offered new therapeutic possibilities for treating ischemic myocardium. CSCs positive for the cell surface antigen c-Kit are known as the primary source for cardiac regeneration. Accumulating evidence shows that chemokines play important roles in stem cell homing. Here we investigated molecular targets to be utilized in modulating the mobility of endogenous CSCs. In a four week follow-up after experimental acute myocardial infarction (AMI  ...[more]

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