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在患有陈旧性心肌梗死的小鼠中,重复剂量的心脏间充质细胞在治疗上优于单次剂量。

Repeated doses of cardiac mesenchymal cells are therapeutically superior to a single dose in mice with old myocardial infarction.

作者信息

Guo Yiru, Wysoczynski Marcin, Nong Yibing, Tomlin Alex, Zhu Xiaoping, Gumpert Anna M, Nasr Marjan, Muthusamy Senthikumar, Li Hong, Book Michael, Khan Abdur, Hong Kyung U, Li Qianhong, Bolli Roberto

机构信息

Institute of Molecular Cardiology, University of Louisville School of Medicine, Louisville, KY, USA.

出版信息

Basic Res Cardiol. 2017 Mar;112(2):18. doi: 10.1007/s00395-017-0606-5. Epub 2017 Feb 16.

Abstract

We have recently demonstrated that repeated administrations of c-kit cardiac progenitor cells (CPCs) have cumulative beneficial effects in rats with old myocardial infarction (MI), resulting in markedly greater improvement in left ventricular (LV) function compared with a single administration. To determine whether this paradigm applies to other species and cell types, mice with a 3-week-old MI received one or three doses of cardiac mesenchymal cells (CMCs), a novel cell type that we have recently described. CMCs or vehicle were infused percutaneously into the LV cavity, 14 days apart. Compared with vehicle-treated mice, the single-dose group exhibited improved LV ejection fraction (EF) after the 1st infusion (consisting of CMCs) but not after the 2nd and 3rd (vehicle). In contrast, in the multiple-dose group, LV EF improved after each CMC infusion, so that at the end of the study, LV EF averaged 35.5 ± 0.7% vs. 32.7 ± 0.6% in the single-dose group (P < 0.05). The multiple-dose group also exhibited less collagen in the non-infarcted region vs. the single-dose group. Engraftment and differentiation of CMCs were negligible in both groups, indicating paracrine effects. These results demonstrate that, in mice with ischemic cardiomyopathy, the beneficial effects of three doses of CMCs are significantly greater than those of one dose, supporting the concept that multiple treatments are necessary to properly evaluate the full therapeutic potential of cell therapy. Thus, the repeated-treatment paradigm is not limited to c-kit CPCs or to rats, but applies to other cell types and species. The generalizability of this concept dramatically augments its significance.

摘要

我们最近证明,对患有陈旧性心肌梗死(MI)的大鼠反复给予c-kit心脏祖细胞(CPCs)具有累积有益效果,与单次给药相比,左心室(LV)功能有显著更大改善。为了确定这种模式是否适用于其他物种和细胞类型,对患有3周龄MI的小鼠给予一剂或三剂心脏间充质细胞(CMCs),这是我们最近描述的一种新型细胞类型。将CMCs或赋形剂经皮注入LV腔,间隔14天。与赋形剂处理的小鼠相比,单剂量组在第一次输注(由CMCs组成)后左心室射血分数(EF)有所改善,但在第二次和第三次输注(赋形剂)后没有改善。相比之下,在多剂量组中,每次CMCs输注后左心室EF均有所改善,因此在研究结束时,左心室EF平均为35.5±0.7%,而单剂量组为32.7±0.6%(P<0.05)。与单剂量组相比,多剂量组在非梗死区域的胶原蛋白也更少。两组中CMCs的植入和分化都可以忽略不计,表明存在旁分泌效应。这些结果表明,在患有缺血性心肌病的小鼠中,三剂CMCs的有益效果明显大于一剂,支持了多次治疗对于正确评估细胞治疗的全部治疗潜力是必要的这一概念。因此,重复治疗模式不仅限于c-kit CPCs或大鼠,也适用于其他细胞类型和物种。这一概念的普遍性极大地增强了其重要性。

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