Magistrado Pamela A, Lusingu John, Vestergaard Lasse S, Lemnge Martha, Lavstsen Thomas, Turner Louise, Hviid Lars, Jensen Anja T R, Theander Thor G
Centre for Medical Parasitology at Department of Medical Microbiology and Immunology, University of Copenhagen, Denmark.
Infect Immun. 2007 May;75(5):2415-20. doi: 10.1128/IAI.00951-06. Epub 2007 Feb 5.
Variant surface antigens (VSA) on the surface of Plasmodium falciparum-infected red blood cells play a major role in the pathogenesis of malaria and are key targets for acquired immunity. The best-characterized VSA belong to the P. falciparum erythrocyte membrane protein 1 (PfEMP1) family. In areas where P. falciparum is endemic, parasites causing severe malaria and malaria in young children with limited immunity tend to express semiconserved PfEMP1 molecules encoded by group A var genes. Here we investigated antibody responses of Tanzanians who were 0 to 19 years old to PF11_0008, a group A PfEMP1. PF11_0008 has previously been found to be highly transcribed in a nonimmune Dutch volunteer experimentally infected with NF54 parasites. A high proportion of the Tanzanian donors had antibodies against recombinant PF11_0008 domains, and in children who were 4 to 9 years old the presence of antibodies to the PF11_0008 CIDR2beta domain was associated with reduced numbers of malaria episodes. These results indicate that homologues of PF11_0008 are present in P. falciparum field isolates and suggest that PF11_0008 CIDR2beta-reactive antibodies might be involved in protection against malaria episodes.
恶性疟原虫感染的红细胞表面的变异表面抗原(VSA)在疟疾发病机制中起主要作用,并且是获得性免疫的关键靶点。特征最明确的VSA属于恶性疟原虫红细胞膜蛋白1(PfEMP1)家族。在恶性疟原虫流行地区,导致严重疟疾的寄生虫以及免疫力有限的幼儿中的疟原虫往往表达由A组var基因编码的半保守PfEMP1分子。在此,我们调查了0至19岁坦桑尼亚人对A组PfEMP1的PF11_0008的抗体反应。先前已发现PF11_0008在实验性感染NF54寄生虫的非免疫荷兰志愿者中高度转录。很大比例的坦桑尼亚献血者具有针对重组PF11_0008结构域的抗体,并且在4至9岁的儿童中,针对PF11_0008 CIDR2β结构域的抗体的存在与疟疾发作次数减少有关。这些结果表明PF11_0008的同源物存在于恶性疟原虫野外分离株中,并表明PF11_0008 CIDR2β反应性抗体可能参与预防疟疾发作。
