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生长中的鸡和大鼠主动脉中赖氨酰氧化酶活性及弹性蛋白/糖胺聚糖相互作用

Lysyl oxidase activity and elastin/glycosaminoglycan interactions in growing chick and rat aortas.

作者信息

Fornieri C, Baccarani-Contri M, Quaglino D, Pasquali-Ronchetti I

机构信息

Institute of General Pathology, University of Modena, Italy.

出版信息

J Cell Biol. 1987 Sep;105(3):1463-9. doi: 10.1083/jcb.105.3.1463.

Abstract

Hydrophobic tropoelastin molecules aggregate in vitro in physiological conditions and form fibers very similar to natural ones (Bressan, G. M., I. Pasquali Ronchetti, C. Fornieri, F. Mattioli, I. Castellani, and D. Volpin, 1986, J. Ultrastruct. Molec. Struct. Res., 94:209-216). Similar hydrophobic interactions might be operative in in vivo fibrogenesis. Data are presented suggesting that matrix glycosaminoglycans (GAGs) prevent spontaneous tropoelastin aggregation in vivo, at least up to the deamination of lysine residues on tropoelastin by matrix lysyl oxidase. Lysyl oxidase inhibitors beta-aminopropionitrile, aminoacetonitrile, semicarbazide, and isonicotinic acid hydrazide were given to newborn chicks, to chick embryos, and to newborn rats, and the ultrastructural alterations of the aortic elastic fibers were analyzed and compared with the extent of the enzyme inhibition. When inhibition was greater than 65% all chemicals induced alterations of elastic fibers in the form of lateral aggregates of elastin, which were always permeated by cytochemically and immunologically recognizable GAGs. The number and size of the abnormal elastin/GAGs aggregates were proportional to the extent of lysyl oxidase inhibition. The phenomenon was independent of the animal species. All data suggest that, upon inhibition of lysyl oxidase, matrix GAGs remain among elastin molecules during fibrogenesis by binding to positively charged amino groups on elastin. Newly synthesized and secreted tropoelastin has the highest number of free epsilon amino groups, and, therefore, the highest capability of binding to GAGs. These polyanions, by virtue of their great hydration and dispersing power, could prevent random spontaneous aggregation of hydrophobic tropoelastin in the extracellular space.

摘要

在生理条件下,疏水性原弹性蛋白分子在体外聚集并形成与天然纤维非常相似的纤维(Bressan, G. M., I. Pasquali Ronchetti, C. Fornieri, F. Mattioli, I. Castellani, and D. Volpin, 1986, J. Ultrastruct. Molec. Struct. Res., 94:209 - 216)。类似的疏水相互作用可能在体内纤维生成过程中起作用。现有数据表明,基质糖胺聚糖(GAGs)可防止体内原弹性蛋白的自发聚集,至少在基质赖氨酰氧化酶使原弹性蛋白上的赖氨酸残基脱氨之前是这样。将赖氨酰氧化酶抑制剂β - 氨基丙腈、氨基乙腈、氨基脲和异烟肼分别给予新生雏鸡、鸡胚胎和新生大鼠,并分析主动脉弹性纤维的超微结构改变,并与酶抑制程度进行比较。当抑制率大于65%时,所有化学物质都会诱导弹性纤维发生改变,表现为弹性蛋白的横向聚集,这些聚集物总是被细胞化学和免疫可识别的GAGs渗透。异常弹性蛋白/GAGs聚集物的数量和大小与赖氨酰氧化酶的抑制程度成正比。该现象与动物物种无关。所有数据表明,在抑制赖氨酰氧化酶后,基质GAGs在纤维生成过程中通过与弹性蛋白上带正电荷的氨基结合而保留在弹性蛋白分子之间。新合成并分泌的原弹性蛋白具有最多的游离ε - 氨基,因此具有最高的与GAGs结合的能力。这些聚阴离子凭借其强大的水合和分散能力,可以防止疏水性原弹性蛋白在细胞外空间随机自发聚集。

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