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基于间日疟原虫环子孢子蛋白基因同源性分析对云南省间日疟复发患者的分子鉴定。

Molecular identification of vivax malaria relapse patients in the Yunnan Province based on homology analysis of the Plasmodium vivax circumsporozoite protein gene.

机构信息

Yunnan Institute of Parasitic Diseases Control, Yunnan Provincial Key Laboratory of Vector-Borne Diseases Control and Research, Yunnan Centre of Malaria Research, Pu'er, 665000, China.

Department of Basic Medical Sciences, Clinical College of Anhui Medical University, Hefei, 230031, China.

出版信息

Parasitol Res. 2023 Jan;122(1):85-96. doi: 10.1007/s00436-022-07700-7. Epub 2022 Nov 5.

Abstract

More than 85% of the malaria burden in the Yunnan Province is caused by imported vivax malaria, and Yunnan is also where the majority of vivax malaria patients are diagnosed in China. Timely removal of the infection sources of Plasmodium vivax and its breeding environment remains the key to eliminating the secondary transmission of imported malaria. To that end, blood samples were collected from cases diagnosed and revalidated as single species infection with P. vivax in the Yunnan Province from 2013 to 2020. Specifically, samples from vivax malaria patients with suspected relapses episodes were subjected to PCR amplification, product sequencing, and analysis of the P. vivax circumsporozoite protein (pvcsp) gene. In total, 77 suspected relapse patients were identified out of 2484 cases infected with P. vivax, with a total of 81 recurrent episodes. A total of 156 CDS (coding DNA sequence) chains were obtained through PCR amplification and sequencing of the pvcsp gene from 159 blood samples, 121 of which can be matched to the paired sequences of 59 vivax malaria patients with both primary attack and recurrent experience. Of the 59 pairs of pvcsp gene sequences, every one of 31 pairs showed only one haplotype and no variant sites (VS), meaning every two paired sequence was completely homologous. Every one of the remaining 28 paired sequences had two haplotypes but no length polymorphism, indicating that the paired sequences was "weakly heterologous" with no fragment insertions (or deletions). All 59 vivax malaria patients with recurrences were caused by the activation of P. vivax hypnozoites originated from the same population as the primary infection. The paired analysis of the similarity between high variant genes allowed the identification of relapse episodes caused by P. vivax homologous hypnozoites and also demonstrated pvcsp gene as one of the candidate molecular markers for tracing infection origin.

摘要

云南省 85%以上的疟疾负担是由输入性间日疟引起的,也是中国大多数间日疟患者的诊断地。及时消除间日疟原虫的感染源及其滋生环境仍然是消除输入性疟疾继发传播的关键。为此,从 2013 年至 2020 年,从云南省诊断并重新确认为间日疟单病种感染的病例中采集了血样。具体来说,从疑似复发的间日疟患者中采集血样,进行 PCR 扩增、产物测序,并分析间日疟原虫环子孢子蛋白(pvcsp)基因。在感染间日疟原虫的 2484 例患者中,共发现 77 例疑似复发患者,共发生 81 例复发。通过对 159 份血样的 pvcsp 基因进行 PCR 扩增和测序,共获得 156 条 CDS(编码 DNA 序列)链,其中 121 条可与 59 例初次发病和复发的间日疟患者的配对序列相匹配。在 59 对 pvcsp 基因序列中,31 对的每一对都只有一个单倍型且没有变异位点(VS),这意味着每两条配对序列完全同源。其余 28 对配对序列中的每一对都有两个单倍型但没有长度多态性,这表明配对序列与原发感染来自同一人群的间日疟休眠子“弱异源”,没有片段插入(或缺失)。所有 59 例复发的间日疟患者都是由原发感染相同人群的间日疟休眠子激活引起的。高变异基因的配对相似性分析可以识别由间日疟同源休眠子引起的复发,也证明 pvcsp 基因是追踪感染源的候选分子标记之一。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/238c/9816221/d9af9a0e791c/436_2022_7700_Fig1_HTML.jpg

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