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Young developmental age cardiac extracellular matrix promotes the expansion of neonatal cardiomyocytes in vitro

机译:年轻的发育年龄心脏细胞外基质可促进新生儿心肌细胞的体外扩增

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A major limitation to cardiac tissue engineering and regenerative medicine strategies is the lack of proliferation of postnatal cardiomyocytes. The extracellular matrix (ECM) is altered during heart development, and studies suggest that it plays an important role in regulating myocyte proliferation. Here, the effects of fetal, neonatal and adult cardiac ECM on the expansion of neonatal rat ventricular cells in vitro are studied. At 24 h, overall cell attachment was lowest on fetal ECM; however, ~80% of the cells were cardiomyocytes, while many non-myocytes attached to older ECM and poly-l-lysine controls. After 5 days, the cardiomyocyte population remained highest on fetal ECM, with a 4-fold increase in number. Significantly more cardiomyocytes stained positively for the mitotic marker phospho-histone H3 on fetal ECM compared with other substrates at 5 days, suggesting that proliferation may be a major mechanism of cardiomyocyte expansion on young ECM. Further study of the beneficial properties of early developmental aged cardiac ECM could advance the design of novel biomaterials aimed at promoting cardiac regeneration.
机译:心脏组织工程和再生医学策略的主要限制是出生后心肌细胞缺乏增殖。细胞外基质(ECM)在心脏发育过程中发生改变,研究表明它在调节心肌细胞增殖中起重要作用。在这里,研究了胎儿,新生儿和成年心脏ECM对新生大鼠心室细胞体外扩增的影响。在24 h时,胎儿ECM的总体细胞附着率最低;然而,约80%的细胞是心肌细胞,而许多非肌细胞则附着在较老的ECM和聚-1-赖氨酸对照上。 5天后,胎儿ECM上的心肌细胞数量仍然最高,数量增加了4倍。与其他底物相比,在5天时,胎儿ECM上的有丝分裂标记磷酸组蛋白H3阳性染色的心肌细胞明显更多,这表明增殖可能是年轻ECM上心肌细胞扩增的主要机制。对早期发育的老年心脏ECM的有益特性的进一步研究可以促进旨在促进心脏再生的新型生物材料的设计。

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