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SnSAG5是刚地弓形虫菌株的一种替代表面抗原,与SnSAG1相互排斥。 (注:原文中“刚地弓形虫”疑似有误,根据前文推测应为“犬新孢子虫”,以下是纠正后的译文) SnSAG5是犬新孢子虫菌株的一种替代表面抗原,与SnSAG1相互排斥。

SnSAG5 is an alternative surface antigen of Sarcocystis neurona strains that is mutually exclusive to SnSAG1.

作者信息

Crowdus Carolyn A, Marsh Antoinette E, Saville Willliam J, Lindsay David S, Dubey J P, Granstrom David E, Howe Daniel K

机构信息

Department of Veterinary Science, University of Kentucky, Lexington, KY 40546-0099, USA.

出版信息

Vet Parasitol. 2008 Nov 25;158(1-2):36-43. doi: 10.1016/j.vetpar.2008.08.012. Epub 2008 Aug 26.

Abstract

Sarcocystis neurona is an obligate intracellular parasite that causes equine protozoal myeloencephalitis (EPM). Previous work has identified a gene family of paralogous surface antigens in S. neurona called SnSAGs. These surface proteins are immunogenic in their host animals, and are therefore candidate molecules for development of diagnostics and vaccines. However, SnSAG diversity exists in strains of S. neurona, including the absence of the major surface antigen gene SnSAG1. Instead, sequence for an alternative SnSAG has been revealed in two of the SnSAG1-deficient strains. Herein, we present data characterizing this new surface protein, which we have designated SnSAG5. The results indicated that the protein encoded by the SnSAG5 sequence is indeed a surface-associated molecule that has characteristics consistent with the other SAGs identified in S. neurona and related parasites. Importantly, Western blot analyses of a collection of S. neurona strains demonstrated that 6 of 13 parasite isolates express SnSAG5 as a dominant surface protein instead of SnSAG1. Conversely, SnSAG5 was not detected in SnSAG1-positive strains. One strain, which was isolated from the brain of a sea otter, did not express either SnSAG1 or SnSAG5. Genetic analysis with SnSAG5-specific primers confirmed the presence of the SnSAG5 gene in Western blot-positive strains, while also suggesting the presence of a novel SnSAG sequence in the SnSAG1-deficient, SnSAG5-deficient otter isolate. The findings provide further indication of S. neurona strain diversity, which has implications for diagnostic testing and development of vaccines against EPM as well as the population biology of Sarcocystis cycling in the opossum definitive host.

摘要

犬新孢子虫是一种专性细胞内寄生虫,可引起马属动物原虫性脑脊髓炎(EPM)。先前的研究在犬新孢子虫中鉴定出了一个由同源表面抗原组成的基因家族,称为SnSAGs。这些表面蛋白在其宿主动物中具有免疫原性,因此是开发诊断方法和疫苗的候选分子。然而,犬新孢子虫菌株中存在SnSAG多样性,包括主要表面抗原基因SnSAG1的缺失。相反,在两个缺乏SnSAG1的菌株中发现了一种替代SnSAG的序列。在此,我们展示了表征这种新表面蛋白的数据,我们将其命名为SnSAG5。结果表明,由SnSAG5序列编码的蛋白确实是一种与表面相关的分子,其特征与在犬新孢子虫和相关寄生虫中鉴定出的其他SAGs一致。重要的是,对一组犬新孢子虫菌株的蛋白质印迹分析表明,13个寄生虫分离株中有6个表达SnSAG5作为主要表面蛋白,而不是SnSAG1。相反,在SnSAG1阳性菌株中未检测到SnSAG5。从一只海獭大脑中分离出的一个菌株既不表达SnSAG1也不表达SnSAG5。用SnSAG5特异性引物进行基因分析证实了蛋白质印迹阳性菌株中存在SnSAG5基因,同时也表明在缺乏SnSAG1、缺乏SnSAG5的水獭分离株中存在一种新的SnSAG序列。这些发现进一步表明了犬新孢子虫菌株的多样性,这对EPM的诊断检测和疫苗开发以及负鼠终末宿主中肉孢子虫循环的种群生物学具有重要意义。

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