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首例流浪猫 PRNP 基因 108bp 缺失和 5 个新 SNP 的报道及其与猫海绵状脑病关系的计算机分析。

First report of a novel 108 bp deletion and five novel SNPs in PRNP gene of stray cats and in silico analysis of their possible relation with feline spongiform encephalopathy.

机构信息

Ege University Faculty of Science, Department of Biology, Molecular Biology Section, İzmir, Türkiye.

Biruni University, Faculty of Engineering and Natural Sciences, Department of Molecular Biology and Genetics, İstanbul, Türkiye.

出版信息

Top Companion Anim Med. 2024 Mar-Apr;59:100859. doi: 10.1016/j.tcam.2024.100859. Epub 2024 Mar 18.

Abstract

Prion diseases are fatal neurodegenerative diseases affecting humans and animals. A relationship between variations in the prion gene of some species and susceptibility to prion diseases has been detected. However, variations in the prion protein of cats that have close contact with humans and their effect on prion protein are not well-known. Therefore, this study aimed to investigate the variations of prion protein-encoding gene (PRNP gene) in stray cats and to evaluate variants detected in terms of genetic factors associated with susceptibility or resistance to feline spongiform encephalopathy using bioinformatics tools. For this, cat DNA samples were amplified by a PCR targeting PRNP gene and then sequenced to reveal the variations. Finally, the effects of variants on prion protein were predicted by bioinformatics tools. According to the obtained results, a novel 108 bp deletion and nine SNPs were detected. Among SNPs, five (c314A>G, c.454T>A, c.579G>C, c.642G>C and c.672G>C) were detected for the first time in this study. Bioinformatics findings showed that c.579G>C (Q193H), c.454T>A (Y152N) and c.457G>A (E153K) variants have deleterious effects on prion protein and c.579G>C (Q193H) has high amyloid propensities. This study demonstrates prion protein variants of stray cats and their deleterious effects on prion protein for the first time.

摘要

朊病毒病是一种影响人类和动物的致命神经退行性疾病。已经检测到某些物种朊病毒基因的变异与易感性之间存在关系。然而,与人类密切接触的猫的朊蛋白变异及其对朊蛋白的影响尚不清楚。因此,本研究旨在调查流浪猫朊蛋白编码基因(PRNP 基因)的变异,并利用生物信息学工具评估与猫海绵状脑病易感性或抗性相关的遗传因素检测到的变异。为此,通过针对 PRNP 基因的 PCR 扩增猫 DNA 样本,然后对其进行测序以揭示变异。最后,通过生物信息学工具预测变异对朊蛋白的影响。根据获得的结果,检测到一个新的 108 bp 缺失和九个 SNPs。在 SNPs 中,有五个(c314A>G、c.454T>A、c.579G>C、c.642G>C 和 c.672G>C)是首次在本研究中检测到的。生物信息学研究结果表明,c.579G>C(Q193H)、c.454T>A(Y152N)和 c.457G>A(E153K)变异对朊蛋白具有有害影响,c.579G>C(Q193H)具有较高的淀粉样倾向。本研究首次证明了流浪猫的朊病毒蛋白变异及其对朊蛋白的有害影响。

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