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首页> 外文期刊>Journal of proteomics >Differential expression of Trypanosoma cruzi I associated with clinical forms of Chagas disease: overexpression of oxidative stress proteins in acute patient isolate.
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Differential expression of Trypanosoma cruzi I associated with clinical forms of Chagas disease: overexpression of oxidative stress proteins in acute patient isolate.

机译:锥虫锥虫I的差异表达与恰加斯病的临床形式有关:急性患者分离株中氧化应激蛋白的过表达。

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摘要

Chagas disease has a variable clinical course with different manifestations and heterogenous geographical distribution. Some studies suggest that this clinical variability could be influenced by the genetic variability of T. cruzi. Here we present the differential protein expression among trypomastigotes and amastigotes of T. cruzi group I isolates from patients with acute and chronic form of Chagas disease from Santander, Colombia. A total of 29 proteins were identified by MALDI-TOF and LC-MS/MS; twenty in trypomastigote and nine in amastigote stage. The 29 proteins identified were grouped in 7 functional categories: 1) metabolism 31%, 2) assembly of cytoskeleton 13.7%, 3) protein destination 13.7%, 4) defenses antioxidants 20.6%, 5) protein synthesis and cellular cycle 13.7%, 6) catabolism 6.8%, and 7) adhesion 3.4%. Tryparedoxin peroxidase, lipoamide dehydrogenase, tyrosine amino transferase and HSP70 were overexpressed in the acute Chagas isolate. Tryparedoxin peroxidase overexpression in the acute isolate was confirmed by Western blot analysis. Most of these proteins are associated with resistance to oxidative stress facilitating their survival within host cells. Therefore, these proteins may represent virulence factors associated with the development of the acute form of the disease and could be used as biomarkers of the clinical course of disease and as drug targets.
机译:恰加斯病具有可变的临床过程,具有不同的表现和异质的地理分布。一些研究表明,这种临床变异性可能受到克鲁氏锥虫遗传变异性的影响。在这里,我们介绍了来自哥伦比亚桑坦德银行的T. cruzi组I分离的锥虫和Amastigotes之间的差异蛋白表达,该细菌来自急性和慢性Chagas病患者。 MALDI-TOF和LC-MS / MS鉴定出29种蛋白质;在锥虫纲中有二十个,在a虫阶段中有九个。鉴定出的29种蛋白质分为7个功能类别:1)代谢31%,2)细胞骨架装配13.7%,3)蛋白质目的地13.7%,4)防御抗氧化剂20.6%,5)蛋白质合成和细胞周期13.7%,6 )分解代谢6.8%,以及7)附着力3.4%。 Trychaedoxin过氧化物酶,脂酰胺脱氢酶,酪氨酸氨基转移酶和HSP70在急性Chagas分离株中过表达。免疫印迹分析证实了急性分离物中Tryparedoxin过氧化物酶的过表达。这些蛋白质大多数与抗氧化应激有关,从而促进其在宿主细胞中的存活。因此,这些蛋白质可能代表与疾病急性形式发展有关的毒力因子,并可用作疾病临床过程的生物标志物和药物靶标。

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