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朊病毒前体功能基因而非假基因中的多态性与白尾鹿慢性消耗病的易感性相关。

Polymorphisms in the prion precursor functional gene but not the pseudogene are associated with susceptibility to chronic wasting disease in white-tailed deer.

作者信息

O'Rourke Katherine I, Spraker Terry R, Hamburg Linda K, Besser Thomas E, Brayton Kelly A, Knowles Donald P

机构信息

Department of Veterinary Microbiology and Pathology, Washington State University, Pullman, WA, USA.

US Department of Agriculture, Agricultural Research Service, Animal Disease Research Unit, 3003 ADBF, Pullman, WA 99164, USA.

出版信息

J Gen Virol. 2004 May;85(Pt 5):1339-1346. doi: 10.1099/vir.0.79785-0.

Abstract

Chronic wasting disease (CWD) status and PrP genotypes were determined for a group of 133 wild white-tailed deer in a 780 acre enclosure in western Nebraska, USA. Approximately half of the deer tested showed evidence of PrPd in the brainstem or lymphoid tissues. Four PRNP alleles encoding amino acid substitutions were identified, with substitutions at residues 95 (Q-->H), 96 (G-->S) or 116 (A-->G), each with serine (S) at residue 138. In addition, a processed pseudogene with two alleles encoding five or six copies of the octapeptide repeat was identified in 26 % of the deer. Both alleles encoded asparagine (N) at residue 138. The functional gene alleles sorted into five major diploid genotypes and four rare genotypes. Although all five major diploid genotypes were found in deer with CWD, unaffected deer were less likely to have the allele QGAS and more likely to have QSAS compared with CWD-affected deer. Late-stage disease (PrPd in brainstem) was noted in deer less than 1 year of age, although no single genotype was associated with this rapid neuroinvasion. Early-stage disease (PrPd distribution limited to the lymphoid system) was observed in deer estimated to be more than 5 years old, suggesting that they were infected as adults or that the incubation time might be extremely long in some individuals. The pseudogene was found in deer of all major PRNP genotypes and was not correlated with CWD status. The large number of susceptible genotypes and the possibility of adult-to-adult transmission suggest that much of the white-tailed deer population may be at risk for disease following exposure to CWD, despite the association of specific genotypes with CWD noted here.

摘要

在美国内布拉斯加州西部一个780英亩的围栏内,对一组133只野生白尾鹿进行了慢性消耗病(CWD)状态和朊蛋白(PrP)基因型的测定。大约一半接受检测的鹿在脑干或淋巴组织中显示出PrPd的证据。鉴定出四个编码氨基酸替代的PRNP等位基因,其在第95位残基(谷氨酰胺(Q)→组氨酸(H))、第96位残基(甘氨酸(G)→丝氨酸(S))或第116位残基(丙氨酸(A)→甘氨酸(G))处发生替代,且在第138位残基处均为丝氨酸(S)。此外,在26%的鹿中鉴定出一个加工假基因,其有两个等位基因,分别编码五个或六个八肽重复序列拷贝。两个等位基因在第138位残基处均编码天冬酰胺(N)。功能性基因等位基因分为五种主要的二倍体基因型和四种罕见基因型。尽管在患有CWD的鹿中发现了所有五种主要的二倍体基因型,但与受CWD影响的鹿相比,未受影响的鹿携带QGAS等位基因的可能性较小,而携带QSAS等位基因的可能性较大。在不到1岁的鹿中发现了晚期疾病(脑干中有PrPd),尽管没有单一基因型与这种快速神经侵袭相关。在估计超过5岁的鹿中观察到早期疾病(PrPd分布限于淋巴系统),这表明它们是成年后感染的,或者某些个体的潜伏期可能极长。在所有主要PRNP基因型的鹿中都发现了该假基因,且与CWD状态无关。大量易感基因型以及成体到成体传播的可能性表明,尽管此处指出了特定基因型与CWD的关联,但许多白尾鹿种群在接触CWD后可能面临患病风险。

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