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趋化因子受体 Duffy 基因多态性与印度芒格洛尔的疟疾。

Duffy antigen receptor for chemokines gene polymorphisms and malaria in Mangaluru, India.

机构信息

Charité-Universitätsmedizin Berlin, corporate member of Freie Universität Berlin, Humboldt-Universität zu Berlin, and Berlin Institute of Health; Institute of Tropical Medicine and International Health, Berlin, Germany.

Karnataka Institute for DNA Research, Dharwad, Karnataka, India.

出版信息

Malar J. 2019 Sep 24;18(1):328. doi: 10.1186/s12936-019-2966-9.

Abstract

BACKGROUND

Duffy blood group antigens serve as receptors for Plasmodium vivax invasion into erythrocytes, and they are determined by polymorphisms of the Duffy antigen receptor for chemokines (DARC), also known as Fy glycoprotein (FY). Duffy negativity, i.e., absence of the antigens, protects against P. vivax infection and is rare among non-African populations. However, data on DARC polymorphisms and their impact on Plasmodium infection in India are scarce.

METHODS

In a case-control study among 909 malaria patients and 909 healthy community controls in Mangaluru, southwestern India, DARC polymorphisms T-33C (rs2814778), G125A (rs12075), C265T (rs34599082), and G298A (rs13962) were genotyped. Associations of the polymorphisms with the odds of malaria, parasite species and manifestation were assessed.

RESULTS

Among patients, vivax malaria (70%) predominated over falciparum malaria (9%) and mixed species infections (21%). DARC T-33C was absent and C265T was rare (1%). FYB carriage (deduced from DARC G125A) was not associated with the risk of malaria per se but it protected against severe falciparum malaria (P = 0.03), and hospitalization (P = 0.006) due to falciparum malaria. Vice versa, carriage of DARC 298A was associated with increased odds of malaria (aOR, 1.46 (1.07-1.99), P = 0.015) and vivax malaria (aOR, 1.60 (1.14-2.22), P = 0.006) and with several reported symptoms and findings of the patients.

CONCLUSION

This report from southern India is the first to show an independent effect of the DARC 298A polymorphism on the risk of malaria. Functional studies are required to understand the underlying mechanism. Moreover, FYB carriage appears to protect against severe falciparum malaria in southern India.

摘要

背景

达菲血型抗原是间日疟原虫(Plasmodium vivax)入侵红细胞的受体,其由趋化因子达菲抗原受体(Duffy Antigen Receptor for Chemokines,DARC),也称为 Fy 糖蛋白(FY)的多态性决定。达菲阴性(即缺乏这些抗原)可预防间日疟原虫感染,在非非洲人群中较为罕见。然而,关于 DARC 多态性及其对印度疟疾感染的影响的数据却很少。

方法

在印度西南部芒格洛尔的一项疟疾患者(909 例)与健康社区对照者(909 例)的病例对照研究中,对 DARC 多态性 T-33C(rs2814778)、G125A(rs12075)、C265T(rs34599082)和 G298A(rs13962)进行了基因分型。评估了这些多态性与疟疾、寄生虫种类和临床表现的比值比(odds ratio,OR)的相关性。

结果

在患者中,以间日疟(70%)为主,恶性疟(9%)和混合感染(21%)较少。DARC T-33C 缺失,C265T 罕见(1%)。FYB 携带(由 DARC G125A 推断得出)本身与疟疾风险无关,但它可预防恶性疟(P=0.03)和因恶性疟所致的住院治疗(P=0.006)。相反,DARC 298A 携带与疟疾(优势比[aOR],1.46(1.07-1.99),P=0.015)和间日疟(aOR,1.60(1.14-2.22),P=0.006)的发病风险增加有关,且与患者的一些报告症状和发现有关。

结论

本报告来自印度南部,首次显示 DARC 298A 多态性对疟疾风险的独立影响。需要进行功能研究以了解潜在机制。此外,FYB 携带似乎可预防印度南部严重的恶性疟。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7816/6760058/dd9ef88ac40b/12936_2019_2966_Fig1_HTML.jpg

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