Foy B D, Magalhaes T, Injera W E, Sutherland I, Devenport M, Thanawastien A, Ripley D, Cárdenas-Freytag L, Beier J C
Department of Tropical Medicine, Tulane University, New Orleans, Louisiana, USA.
Infect Immun. 2003 Apr;71(4):2032-40. doi: 10.1128/IAI.71.4.2032-2040.2003.
Vaccines that induce mosquito-killing (mosquitocidal) activity could substantially reduce the transmission of certain mosquito-borne diseases, especially vaccines against African malaria vectors, such as the mosquito Anopheles gambiae. To generate and characterize antimosquito immunity we immunized groups of mice with two individual A. gambiae midgut cDNAs, Ag-Aper1 (a secreted peritrophic matrix protein) and AgMuc1 (a midgut-bound mucin), and an A. gambiae midgut cDNA library from blood-fed mosquitoes. We observed significantly increased mortality among mosquitoes that fed on either the AgMuc1- or the cDNA library-immunized mice compared to that of controls, but no differences were observed among those fed on Ag-Aper1-immunized mice. Analysis of the humoral and cellular immune responses from mice showed that the induced mosquitocidal effect was associated with immune profiles characterized by elevated tumor necrosis factor alpha and gamma interferon cytokine levels and very low antibody titers. Furthermore, an additional immunization of cDNA library-immunized mice with midgut protein shifted immunity toward a Th2-type immune response, characterized by elevated antibody titers and high interleukin-5 and interleukin-10 cytokine levels; importantly, mosquitoes feeding on these mice exhibited no undue mortality. Finally, when immune sera was ingested by mosquitoes through a membrane feeder, no effect on mosquito mortality was observed, indicating that serum factors alone were not responsible for the mosquitocidal effect. Our results demonstrate that mosquitocidal immunity in mice can be consistently generated by midgut cDNA immunization and suggest this cDNA-induced mosquitocidal immunity is cell mediated.
诱导杀蚊活性的疫苗可以大幅减少某些蚊媒疾病的传播,特别是针对非洲疟疾传播媒介的疫苗,比如冈比亚按蚊。为了产生并表征抗蚊免疫力,我们用两种冈比亚按蚊中肠cDNA(Ag-Aper1,一种分泌型围食膜蛋白;AgMuc1,一种中肠结合黏蛋白)以及来自吸食血液的蚊子的冈比亚按蚊中肠cDNA文库对几组小鼠进行免疫。我们观察到,与对照组相比,取食AgMuc1免疫小鼠或cDNA文库免疫小鼠血液的蚊子死亡率显著增加,但取食Ag-Aper1免疫小鼠血液的蚊子死亡率无差异。对小鼠体液免疫和细胞免疫反应的分析表明,诱导产生的杀蚊效应与以肿瘤坏死因子α和γ干扰素细胞因子水平升高以及抗体滴度极低为特征的免疫谱相关。此外,用中肠蛋白对cDNA文库免疫小鼠进行再次免疫会使免疫转向Th2型免疫反应,其特征为抗体滴度升高以及白细胞介素-5和白细胞介素-10细胞因子水平升高;重要的是,取食这些小鼠血液的蚊子没有出现异常死亡。最后,当通过膜饲器让蚊子摄取免疫血清时,未观察到对蚊子死亡率有影响,这表明仅血清因子并不负责杀蚊效应。我们的结果表明,通过中肠cDNA免疫可以在小鼠中持续产生杀蚊免疫力,并表明这种cDNA诱导的杀蚊免疫力是细胞介导的。