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I型和II型CD36缺乏症患者的心肌CD36表达及脂肪酸蓄积

Myocardial CD36 expression and fatty acid accumulation in patients with type I and II CD36 deficiency.

作者信息

Watanabe K, Ohta Y, Toba K, Ogawa Y, Hanawa H, Hirokawa Y, Kodama M, Tanabe N, Hirono S, Ohkura Y, Nakamura Y, Kato K, Aizawa Y, Fuse I, Miyajima S, Kusano Y, Nagamoto T, Hasegawa G, Naito M

机构信息

Department of Clinical Pharmacology, Niigata College of Pharmacy, Japan.

出版信息

Ann Nucl Med. 1998 Oct;12(5):261-6. doi: 10.1007/BF03164911.

Abstract

Long-chain fatty acids (LCFA) are one of the major cardiac energy substrates, so understanding LCFA metabolism may help in elucidating the mechanisms of various heart diseases. CD36 is a multifunctional membrane glycoprotein that acts not only as a receptor for thrombospondin, collagen and oxidized low density lipoprotein but also as a receptor for LCFA. We investigated the relationship between CD36 expression in myocardial capillary endothelial cells and myocardial LCFA uptake in patients with CD36 deficiency. We analyzed CD36 expression in blood cells from 250 patients with heart diseases by means of a flow cytometer. In 218 patients, myocardial LCFA scintigraphy was performed with 123I-beta-methyl-p-iodophenyl pentadecanoic acid (BMIPP). In 5 patients, myocardial capillary endothelial cells were examined immunohistochemically for CD36 expression. Eleven patients (4%) showed signs of type I CD36 deficiency (neither platelets nor monocytes expressed CD36). Twenty patients (8%) had type II CD36 deficiency (monocytes expressed CD36 but platelets did not). In all 11 patients with type I CD36 deficiency, no BMIPP accumulation was observed in the heart, but in 13 patients with type II CD36 deficiency, BMIPP accumulation in the heart was focally reduced, but there were no patients without BMIPP accumulation in the heart. Although the myocardial capillary endothelial cells from two CD36-positive patients expressed CD36, those from two patients with type I CD36 deficiency did not. In a patient with type II CD36 deficiency, some capillary endothelial cells displayed patchy CD36 expression. CD36 deficiency was documented in 31 (12%) patients with heart diseases. Because CD36 was not expressed in the myocardial capillary endothelial cells in patients with type I CD36 deficiency, type I CD36 deficiency is closely related to lack of myocardial LCFA accumulation and metabolism in the myocardium.

摘要

长链脂肪酸(LCFA)是心脏的主要能量底物之一,因此了解LCFA代谢可能有助于阐明各种心脏病的发病机制。CD36是一种多功能膜糖蛋白,不仅作为血小板反应蛋白、胶原蛋白和氧化型低密度脂蛋白的受体,还作为LCFA的受体。我们研究了CD36缺乏患者心肌毛细血管内皮细胞中CD36表达与心肌LCFA摄取之间的关系。我们通过流式细胞仪分析了250例心脏病患者血细胞中的CD36表达。在218例患者中,用123I-β-甲基-对-碘苯基十五烷酸(BMIPP)进行了心肌LCFA闪烁显像。在5例患者中,通过免疫组织化学检查心肌毛细血管内皮细胞的CD36表达。11例患者(4%)表现出I型CD36缺乏的迹象(血小板和单核细胞均不表达CD36)。20例患者(8%)患有II型CD36缺乏(单核细胞表达CD36但血小板不表达)。在所有11例I型CD36缺乏的患者中,心脏未观察到BMIPP蓄积,但在13例II型CD36缺乏的患者中,心脏中BMIPP的蓄积局部减少,但没有患者心脏中完全没有BMIPP蓄积。虽然两名CD36阳性患者的心肌毛细血管内皮细胞表达CD36,但两名I型CD36缺乏患者的心肌毛细血管内皮细胞不表达。在一名II型CD36缺乏的患者中,一些毛细血管内皮细胞显示出斑驳的CD36表达。在31例(12%)心脏病患者中记录到CD36缺乏。由于I型CD36缺乏患者的心肌毛细血管内皮细胞不表达CD36,因此I型CD36缺乏与心肌中LCFA蓄积和代谢的缺乏密切相关。

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