Malaria causes approximately 212 million cases and 429 thousand deaths annually. Plasmodium falciparum is responsible for the vast majority of deaths (99%) than others. The virulence of P. falciparum is mostly associated with immune response-evading ability. It has different mechanisms to evade both Anopheles mosquito and human host immune responses. Immune-evading mechanisms in mosquito depend mainly on the Pfs47 gene that inhibits Janus kinase-mediated activation. Host complement factor also protects human complement immune attack of extracellular gametes in Anopheles mosquito midgut. In the human host, evasion largely results from antigenic variation, polymorphism, and sequestration. They also induce Kupffer cell apoptosis at the preerythrocytic stage and interfere with phagocytic functions of macrophage by hemozoin in the erythrocytic stage. Lack of major histocompatibility complex-I molecule expression on the surface red blood cells also avoids recognition by CD8~(+) T cells. Complement proteins could allow for the entry of parasite into the red blood cell. Intracellular survival also assists the escape of malarial parasite. Invading, evading, and immune response mechanisms both in malaria vector and human host are critical to design appropriate vaccine. As a result, the receptors and ligands involved in different stages of malaria parasites should be elucidated.
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机译:疟疾每年导致约21200万个案件和429千人死亡。疟原虫疟原虫负责绝大多数死亡(99%)。 p. falciparum的毒力大多与免疫应答疏散能力相关。它有不同的机制,以逃避Anopheles蚊子和人宿主免疫反应。蚊子的免疫逃避机制主要取决于抑制Janus激酶介导的活化的PFS47基因。宿主补充因子还保护人类细胞外配子的人类补体免疫发作在蚊帐蚊子中肠。在人体宿主中,逃避主要是由抗原变异,多态性和封存产生的。他们还在血液化阶段诱导血液化阶段的Kupffer细胞凋亡,并干扰红细胞血液中血液素的吞噬功能。表面红细胞上缺乏主要的组织相容性络合物-I分子表达也避免了CD8〜(+)T细胞的识别。补体蛋白可以允许寄生虫进入红细胞。细胞内生存率也有助于疟疾寄生虫的逃脱。疟疾载体和人体宿主中的入侵,逃避和免疫应答机制对于设计适当的疫苗至关重要。结果,应阐明涉及疟疾寄生虫的不同阶段的受体和配体。
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