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间日疟原虫确诊复发病例的分子和免疫学分析。

Molecular and immunological analyses of confirmed Plasmodium vivax relapse episodes.

作者信息

Maneerattanasak Sarunya, Gosi Panita, Krudsood Srivicha, Chimma Pattamawan, Tongshoob Jarinee, Mahakunkijcharoen Yuvadee, Sukasem Chonlaphat, Imwong Mallika, Snounou Georges, Khusmith Srisin

机构信息

Department of Microbiology and Immunology, Faculty of Tropical Medicine, Mahidol University, 420/6 Rajvithi Road, Bangkok, 10400, Thailand.

Department of Immunology and Medicine, Armed Forces Research Institute of Medical Science-United States Army Military Component, Bangkok, Thailand.

出版信息

Malar J. 2017 May 30;16(1):228. doi: 10.1186/s12936-017-1877-x.

Abstract

BACKGROUND

Relapse infections resulting from the activation hypnozoites produced by Plasmodium vivax and Plasmodium ovale represent an important obstacle to the successful control of these species. A single licensed drug, primaquine is available to eliminate these liver dormant forms. To date, investigations of vivax relapse infections have been few in number.

RESULTS

Genotyping, based on polymorphic regions of two genes (Pvmsp1F3 and Pvcsp) and four microsatellite markers (MS3.27, MS3.502, MS6 and MS8), of 12 paired admission and relapse samples from P. vivax-infected patients were treated with primaquine, revealed that in eight of the parasite populations in the admission and relapse samples were homologous, and heterologous in the remaining four patients. The patients' CYP2D6 genotypes did not suggest that any were poor metabolisers of primaquine. Parasitaemia tended to be higher in the heterologous as compared to the homologous relapse episodes as was the IgG3 response. For the twelve pro- and anti-inflammatory cytokine levels measured for all samples, only those of IL-6 and IL-10 tended to be higher in patients with heterologous as compared to homologous relapses in both admission and relapse episodes.

CONCLUSIONS

The data from this limited number of patients with confirmed relapse episodes mirror previous observations of a significant proportion of heterologous parasites in relapses of P. vivax infections in Thailand. Failure of the primaquine treatment that the patients received is unlikely to be due to poor drug metabolism, and could indicate the presence of P. vivax populations in Thailand with poor susceptibility to 8-aminoquinolines.

摘要

背景

间日疟原虫和卵形疟原虫产生的休眠子激活导致的复发感染是成功控制这些疟原虫种类的一个重要障碍。目前有一种获得许可的药物伯氨喹可用于清除这些肝脏休眠形式。迄今为止,对间日疟复发感染的研究数量很少。

结果

对12例接受伯氨喹治疗的间日疟感染患者的配对入院和复发样本,基于两个基因(Pvmsp1F3和Pvcsp)的多态性区域以及四个微卫星标记(MS3.27、MS3.502、MS6和MS8)进行基因分型,结果显示在入院和复发样本中的八个疟原虫群体是同源的,其余四个患者的是异源的。患者的CYP2D6基因型并未表明有任何患者是伯氨喹的代谢不良者。与同源复发发作相比,异源复发发作时的寄生虫血症往往更高,IgG3反应也是如此。对于所有样本测量的12种促炎和抗炎细胞因子水平,在入院和复发发作中,只有白细胞介素-6(IL-6)和白细胞介素-10(IL-10)在异源复发患者中往往高于同源复发患者。

结论

来自这少数确诊复发发作患者的数据反映了泰国之前观察到的间日疟感染复发中相当一部分异源寄生虫的情况。患者接受的伯氨喹治疗失败不太可能是由于药物代谢不良,这可能表明泰国存在对8-氨基喹啉敏感性较差的间日疟原虫群体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b1b3/5450361/67892afe9c0e/12936_2017_1877_Fig1_HTML.jpg

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