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Myocardial lipid accumulation in patients with pressure-overloaded heart and metabolic syndrome

机译:压力超负荷的心脏代谢综合征患者的心肌脂质蓄积

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摘要

We evaluated the role of sterol-regulatory element binding protein (SREBP)-1c/peroxisome proliferator activated receptor-γ (PPARγ) pathway on heart lipotoxicity in patients with metabolic syndrome (MS) and aortic stenosis (AS). Echocardiographic parameters of heart function and structural alterations of LV specimens were studied in patients with (n = 56) and without (n = 61) MS undergoing aortic valve replacement. Tissues were stained with hematoxylin-eosin (H and E) and oil red O for evidence of intramyocyte lipid accumulation. The specimens were also analyzed with PCR, Western blot, and immunohistochemical analysis for SREBP-1c and PPARγ. Ejection fraction (EF) was lower in MS compared with patients without MS (P < 0.001); no difference was found in aortic orifice surface among the groups. H and E and oil red O staining of specimens from MS patients revealed several myocytes with intracellular accumulation of lipid, whereas these alterations were not detected in biopsies from patients without MS. Patients without MS have low levels and weak immunostaining of SREBP-1c and PPARγ in heart specimens. In contrast, strong immunostaining and higher levels of SREBP-1c and PPARγ were seen in biopsies from the MS patients. Moreover, we evidenced a significative correlation between both SREBP-1c and PPARγ and EF and intramyocyte lipid accumulation (P < 0.001). SREBP-1c may contribute to heart dysfunction by promoting lipid accumulation within myocytes in MS patients with AS; SREBP-1c may do it by increasing the levels of PPARγ protein.
机译:我们评估了固醇调节元件结合蛋白(SREBP)-1c /过氧化物酶体增殖物激活受体-γ(PPARγ)途径对代谢综合征(MS)和主动脉瓣狭窄(AS)患者心脏脂质毒性的作用。在有(n = 56)和没有(n = 61)MS接受主动脉瓣置换的患者中研究了心脏功能的超声心动图参数和LV标本的结构改变。组织用苏木精-曙红(H和E)和油红O染色,以显示肌内脂质积聚。还用PCR,蛋白质印迹和SREBP-1c和PPARγ的免疫组织化学分析了标本。与没有MS的患者相比,MS的射血分数(EF)更低(P <0.001);各组之间主动脉口表面无差异。 MS患者标本的H和E以及油红O染色显示,一些心肌细胞中脂质蓄积,而无MS患者的活检中未检测到这些改变。没有MS的患者心脏样本中SREBP-1c和PPARγ的水平较低且免疫染色较弱。相反,在MS患者的活检中发现强免疫染色和较高水平的SREBP-1c和PPARγ。此外,我们证明了SREBP-1c和PPARγ与EF与肌内脂质积聚之间存在显着相关性(P <0.001)。 SREBP-1c可能通过促进AS的MS患者的心肌细胞内脂质蓄积而导致心脏功能障碍。 SREBP-1c可以通过增加PPARγ蛋白的水平来实现。

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