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视网膜色素上皮中的微过氧化物酶体。

Microperoxisomes in retinal pigment epithelium.

作者信息

Robison W G, Kuwabara T

出版信息

Invest Ophthalmol. 1975 Nov;14(11):866-72.

PMID:810456
Abstract

Microperoxisomes were found to be abundant in the retinal pigment epithelium of the human, rhesus monkey, mice, rats, domestic fowl, and frog by ultrastructural histochemistry. They were rare in other cells of the retina and choroid. These organelles had a granular matrix, ranged in diameter from 0.15 mum to 0.30 mum, and were bound by a single tripartite membrane which often maintained slender connections with the smooth endoplasmic reticulum and other microperoxisomes. They exhibited a positive reaction (electron opaque product) following incubation in diaminobenzidine and H2O2 for the demonstration of the peroxidatic activity of catalase (Novikoff et al., J. Histochem. Cytochem. 20: 1006, 1972). The reaction was inhibited by: (1) aminotriazole; (2) dichlorophenol-indophenol; (3) preheating at 95 degrees C.; or (4) elimination of H2O2. Microperoxisomes, like the well-known peroxisomes (microbodies) of liver cells have been inplicated in various aspects of lipid metabolism and the detoxification of H2O2. We demonstrated for the first time that microperoxisomes respond to drug-induced changes in lipid metabolism, as previously shown for peroxisomes. Nafenopin is a recently utilized drug which greatly decreases serum lipids, increases hepatic catalase activity, and induces an increased size and number of hepatic peroxisomes. Black, beige, albino, and obese mutant mice of the C57BL/6J strain treated with nafenopin for several weeks showed a two- to threefold increase in the number of microperoxisomes in the retinal pigment epithelium. Microperoxisomes of the retinal pigment epithelium may be involved in the transport, storage, and rapid turnover of lipids associated with the maintenance of photoreceptor outer segment disc membranes.

摘要

通过超微结构组织化学发现,微过氧化物酶体在人类、恒河猴、小鼠、大鼠、家禽和青蛙的视网膜色素上皮中大量存在。它们在视网膜和脉络膜的其他细胞中很少见。这些细胞器具有颗粒状基质,直径在0.15μm至0.30μm之间,由单层三层膜包围,该膜通常与滑面内质网和其他微过氧化物酶体保持细长连接。在二氨基联苯胺和H2O2中孵育后,它们表现出阳性反应(电子不透明产物),用于证明过氧化氢酶的过氧化物活性(诺维科夫等人,《组织化学与细胞化学杂志》20: 1006, 1972)。该反应受到以下因素抑制:(1)氨基三唑;(2)二氯酚靛酚;(3)95℃预热;或(4)去除H2O2。微过氧化物酶体与肝细胞中著名的过氧化物酶体(微体)一样,参与脂质代谢的各个方面以及H2O2的解毒。我们首次证明,微过氧化物酶体对药物诱导的脂质代谢变化有反应,正如之前对过氧化物酶体的研究所示。萘酚平是一种最近使用的药物,它能大幅降低血脂、增加肝脏过氧化氢酶活性,并诱导肝脏过氧化物酶体的大小和数量增加。用萘酚平处理数周的C57BL/6J品系的黑色、米色、白化和肥胖突变小鼠,其视网膜色素上皮中的微过氧化物酶体数量增加了两到三倍。视网膜色素上皮的微过氧化物酶体可能参与与光感受器外节盘膜维持相关的脂质的运输、储存和快速周转。

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