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Regional Myocardial Perfusion Disturbance in Experimental Chronic Chagas Cardiomyopathy

机译:实验性慢性Chagas心肌病的区域心肌灌注扰动

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Altered myocardial perfusion is a common finding in chronic Chagas cardiomyopathy (CCC), but its underlying histologic changes have not been elucidated. We investigated the occurrence of myocardial perfusion defects (MPDs) and the correlated regional changes to histology in an experimental model of CCC in hamsters. Methods: Female Syrian hamsters (n = 34) were infected with 3.5 x 10(4) to 10(5) trypomastigote forms of Trypanosoma cruzi, Y strain, and 6-10 mo afterward underwent in vivo imaging including resting Tc-99m-sestamibi SPECT, segmental and global left ventricular function assessment using 2-dimensional echocardiography, and F-18-FDG PET for evaluation of myocardial viability. Histologic analysis included quantification of fibrosis, inflammatory infiltration, and the diameter and density of myocardial microcirculation. Results: MPDs were present in 17 (50%) of the infected animals. Histologic analysis revealed no transmural scar in segments with an MPD, and normal or mildly reduced F-18-FDG uptake, indicating viable myocardium. Infected animals with an MPD, in comparison to infected animals without an MPD and control animals, showed a lower left ventricular ejection fraction (P = 0.012), a higher wall motion score index (P = 0.004), and a higher extent of inflammatory infiltration (P = 0.018) but a similar extent of fibrosis (P = 0.15) and similar microvascular diameter and density (P 0.05). Segments with an MPD (n = 65), as compared with normally perfused regions in the same animal (n = 156), showed a higher wall motion score index (P = 0.005) but a similar extent of inflammatory infiltration, a similar extent of fibrosis, and a similar microvascular diameter and density. Conclusion: Resting MPDs are frequent in experimental CCC and are associated with myocardial inflammation but do not designate scar tissue, corresponding to regions with metabolically viable myocardium.
机译:改变的心肌灌注是慢性噬菌体心肌病(CCC)的常见发现,但其潜在的组织学变化尚未阐明。我们调查了心肌灌注缺陷(MPDS)的发生以及在仓鼠CCC实验模型中对组织学的相关区域变化。方法:雌性叙利亚仓鼠(n = 34)感染3.5×10(4)至10(5)个胰蛋白酶瘤瘤瘤,Y菌株和6-10莫在体内成像后6-10莫,包括休息的TC-99M-Sestamibi使用二维超声心动图和F-18-FDG PET进行SPECT,节段性和全球左心室功能评估,用于评估心肌活力。组织学分析包括纤维化,炎症浸润和心肌微循环直径和密度的定量。结果:MPDS存在于17个(50%)的受感染的动物中。组织学分析显示出具有MPD的区段中的透际瘢痕,以及正常或轻度降低的F-18-FDG吸收,表明可行的心肌。与没有MPD和对照动物的感染的动物相比,具有MPD的感染动物显示出较低的左心室喷射部分(P = 0.012),更高的壁运动得分指数(P = 0.004),以及更高程度的炎性渗透(p = 0.018)但相似的纤维化程度(p = 0.15)和类似的微血管直径和密度(p& 0.05)。与MPD(n = 65)的区段与相同动物中的正常灌注区域相比(n = 156)相比,显示出更高的壁运动得分指数(p = 0.005),但相似的炎性渗透程度,类似的程度纤维化和类似的微血管直径和密度。结论:在实验CCC中频繁静息MPD,与心肌炎症有关,但不指定与具有代谢可行心肌的区域对应的瘢痕组织。

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