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Immunodominant, protective response to the parasite Toxoplasma gondii requires antigen processing in the endoplasmic reticulum.

机译:对刚体弓形虫的免疫保护性保护反应需要在内质网中进行抗原处理。

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摘要

The parasite Toxoplasma gondii replicates in a specialized intracellular vacuole and causes disease in many species. Protection from toxoplasmosis is mediated by CD8(+) T cells, but the T. gondii antigens and host genes required for eliciting protective immunity are poorly defined. Here we identified GRA6, a polymorphic protein secreted in the parasitophorous vacuole, as the source of the immunodominant and protective decapeptide HF10 presented by the H-2L(d) major histocompatibility complex class I molecule. Presentation of the HF10-H-2L(d) ligand required proteolysis by ERAAP, the endoplasmic reticulum aminopeptidase associated with antigen processing. Consequently, expansion of protective CD8(+) T cell populations was impaired in T. gondii-infected ERAAP-deficient mice, which were more susceptible to toxoplasmosis. Thus, endoplasmic reticulum proteolysis is critical for eliciting protective immunity to a vacuolar parasite.
机译:弓形虫弓形虫在特殊的细胞内液泡中复制,并在许多物种中引起疾病​​。保护免受弓形虫病的CD8(+)T细胞介导,但弓形虫抗原和引发保护性免疫所需的宿主基因定义不清。在这里,我们确定了GRA6,一种在寄生虫液泡中分泌的多态蛋白,是H-2L(d)主要组织相容性复合体I类分子呈现的免疫显性和保护性十肽HF10的来源。呈现HF10-H-2L(d)配体需要通过ERAAP进行蛋白水解,ERAAP是一种与抗原加工相关的内质网氨基肽酶。因此,在弓形虫感染的ERAAP缺陷型小鼠中,保护性CD8(+)T细胞群的扩增受到损害,而后者更容易感染弓形虫病。因此,内质网蛋白水解对于引发对液泡寄生虫的保护性免疫至关重要。

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