成肌细胞移植对心肌梗死后局部结构和功能的远期影响

S. Ghostine, C. Carrion, Luiz César Guarita Souza, P. Richard, P. Bruneval, J. Vilquin, B. Pouzet, K. Schwartz, P. Menasché, A. Hagège
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引用次数: 262

摘要

梗死心肌内骨骼肌母细胞(SM)移植(Tx)可改善左心室(LV)整体功能,尽管其直接收缩作用仍存在争议。方法和结果在梗死前(基线)、瘢痕内注射自体SM或培养基(CM)后4 (M4)和12 (M12)个月的绵羊模型(n=16)中研究了整体和局部左室功能。采用超声心动图结合组织多普勒成像测量左室舒张末容积(EDV)、射血分数(EF)、壁运动评分(WMS)和收缩心肌速度梯度(MVG)。各组间基线参数相似。在M4时,SM的Tx降低了梗死后EDV的增加(CM组为72±8 mL, CM组为105±13 mL, P <0.05), EF的降低(CM组为48±5,CM组为33±3%,P =0.006),尽管它改善了WMS (CM组为5.4±1.2,CM组为13±2.2,P <0.01)和SMVG(0.60±0.13,CM组为-0.04±)。CM组为13 s-1, P <0.05)。M12时的结果相似。所有Tx动物在M12之前都检测到肌管和SM的瘢痕内积累,肌球蛋白重链(MHC)的快速和缓慢亚型共表达(30%的纤维,而正常骨骼肌为0%),胶原密度降低(30±2%对73±3%,P <0.0001)。结论:在长达1年的时间里,SM的Tx限制了梗死后EF的恶化,并通过表达两种MHC亚型的骨骼肌细胞定殖纤维化改善收缩疤痕功能,这可能赋予移植物承受心脏型负荷的能力。
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Long-Term Efficacy of Myoblast Transplantation on Regional Structure and Function After Myocardial Infarction
BackgroundTransplantation (Tx) of skeletal myoblasts (SM) within an infarcted myocardium improves global left ventricular (LV) function, although a direct systolic effect remains controversial. Methods and ResultsGlobal and regional LV functions were studied in a sheep model (n=16) of infarction before (baseline), and 4 (M4), and 12 (M12) months after in-scar injections of autologous SM or culture medium (CM). LV end-diastolic volume (EDV), ejection fraction (EF), wall motion score (WMS), and systolic myocardial velocity gradient (MVG) across the scar were measured by echocardiography with tissue Doppler imaging. Parameters were similar at baseline between groups. At M4, Tx of SM reduced the postinfarction increase in EDV (72±8 versus 105±13 mL in the CM group, P <0.05) and the decrease in EF (48±5 versus 33±3% in the CM group, P =0.006) although it improved WMS (5.4±1.2 versus 13±2.2 in the CM group, P <0.01) and SMVG (0.60±0.13 versus –0.04±.13 seconds-1 in the CM group, P <0.05). Results were similar at M12. In-scar accumulation of myotubes and SM were detected in all Tx animals up to M12, with co-expression of fast and slow isoforms of the myosin heavy chain (MHC) (30% of the fibers versus 0% in the normal skeletal muscle) and decreased collagen density (30±2% versus 73±3%, P <0.0001). ConclusionFor up to 1 year, Tx of SM limits postinfarction EF deterioration and improves systolic scar function through colonization of fibrosis by skeletal muscle cells with expression of both MHC isoforms, which may confer to the graft the ability to withstand a cardiac-type workload.
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