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在杜氏利什曼原虫恰加斯前鞭毛体发育为感染性形式的过程中,表面蛋白酶gp63的三种不同RNA呈现出差异表达。

Three distinct RNAs for the surface protease gp63 are differentially expressed during development of Leishmania donovani chagasi promastigotes to an infectious form.

作者信息

Ramamoorthy R, Donelson J E, Paetz K E, Maybodi M, Roberts S C, Wilson M E

机构信息

Veterans Administration Medical Center, Iowa City, Iowa 52242.

出版信息

J Biol Chem. 1992 Jan 25;267(3):1888-95.

PMID:1370484
Abstract

Leishmania sp. protozoa contain an abundant surface protease (gp63) that is important for the virulence of the parasite. We found that the average amount of gp63 expressed by Leishmania donovani chagasi promastigotes increases 6-11-fold as they develop from a less infectious form in logarithmic phase to a highly infectious form during stationary phase of cultivation in vitro. The predominant gp63 RNA switches from a 2.7 to a 3.0 kilobase (kb) RNA during the transition from log to stationary phase. Sequence analysis of gp63 cDNAs reveals that three different classes of gp63 RNAs, containing unique 3'-untranslated regions (3' UTRs), are expressed during growth to stationary phase. The predominant 2.7-(log) and 3.0-kb (stationary) class gp63 RNAs possess nearly identical coding regions, but they diverge in their 3' UTRs. A third class, consisting of 3.1- and 2.6-kb (constitutive) gp63 RNAs, is expressed at low levels throughout cultivation. This latter class encodes a gp63 with an additional 41 amino acids at its C terminus, replacing a potential signal for attachment of a glycolipid membrane anchor with a sequence that could be a transmembrane region. These findings are consistent with the regulated expression of different gp63 genes, resulting in different amounts of gp63 protein, during the promastigote's in vitro development to an infectious form.

摘要

利什曼原虫属的原生动物含有一种丰富的表面蛋白酶(gp63),它对该寄生虫的毒力很重要。我们发现,杜氏利什曼原虫恰加斯亚种前鞭毛体所表达的gp63平均量,在其从对数期传染性较低的形态发育为体外培养稳定期传染性很强的形态过程中增加了6至11倍。在从对数期向稳定期转变期间,主要的gp63 RNA从2.7千碱基(kb)的RNA转变为3.0 kb的RNA。gp63 cDNA的序列分析表明,在生长至稳定期的过程中表达了三类不同的gp63 RNA,它们含有独特的3'非翻译区(3'UTR)。主要的2.7 kb(对数期)和3.0 kb(稳定期)类gp63 RNA具有几乎相同的编码区,但它们的3'UTR不同。第三类由3.1 kb和2.6 kb(组成型)的gp63 RNA组成,在整个培养过程中低水平表达。后一类编码的gp63在其C末端有额外的41个氨基酸,用一个可能是跨膜区的序列取代了糖脂膜锚定附着的潜在信号。这些发现与不同gp63基因的调控表达一致,导致前鞭毛体在体外发育为感染性形态过程中gp63蛋白量不同。

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