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Fate of undifferentiated mouse embryonic stem cells within the rat heart: role of myocardial infarction and immune suppression

机译:大鼠心脏内未分化的小鼠胚胎干细胞的命运:心肌梗死和免疫抑制的作用

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摘要

It has recently been suggested that the infarcted rat heart microenvironment could direct pluripotent mouse embryonic stem cells to differentiate into cardiomyocytes through an in situ paracrine action. To investigate whether the heart can function as a cardiogenic niche and confer an immune privilege to embryonic stem cells, we assessed the cardiac differentiation potential of undifferentiated mouse embryonic stem cells (mESC) injected into normal, acutely or chronically infarcted rat hearts. We found that mESC survival depended on immunosuppression both in normal and infarcted hearts. However, upon Cyclosporin A treatment, both normal and infarcted rat hearts failed to induce selective cardiac differentiation of implanted mESC. Instead, teratomas developed in normal and infarcted rat hearts 1 week and 4 weeks (50% and 100%, respectively) after cell injection. Tight control of ESC commitment into a specific cardiac lineage is mandatory to avoid the risk of uncontrolled growth and tumourigenesis following transplantation of highly plastic cells into a diseased myocardium.
机译:最近有人提出,梗塞的大鼠心脏微环境可以指导多能小鼠胚胎干细胞通过原位旁分泌作用分化为心肌细胞。为了调查心脏是否可以充当心源性利基市场并赋予胚胎干细胞免疫特权,我们评估了注入正常,急性或慢性梗死大鼠心脏的未分化小鼠胚胎干细胞(mESC)的心脏分化潜能。我们发现,mESC的存活取决于正常心脏和梗塞心脏的免疫抑制。但是,在用环孢菌素A治疗后,正常和梗死的大鼠心脏均无法诱导植入的mESC的选择性心脏分化。相反,在细胞注射后1周和4周(分别为50%和100%),畸胎瘤在正常和梗死的大鼠心脏中发展。必须严格控制ESC对特定心脏谱系的表达,以避免将高度可塑性细胞移植到患病心肌中后不受控制的生长和肿瘤形成的风险。

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