Taniguchi Tomoyo, Tachikawa Saoko, Kanda Yasuhiro, Kawamura Toshihiko, Tomiyama-Miyaji Chikako, Li Changchun, Watanabe Hisami, Sekikawa Hiroho, Abo Toru
Department of Immunology, Niigata University School of Medicine, Niigata, Japan.
Immunology. 2007 Dec;122(4):514-21. doi: 10.1111/j.1365-2567.2007.02661.x. Epub 2007 Oct 3.
It is still controversial whether malaria protection is mediated by conventional immunity associated with T and B cells or by innate immunity associated with extrathymic T cells and autoantibody-producing B cells. Given this situation, it is important to examine the mechanism of malaria protection in beta(2)-microglobulin-deficient (beta(2)m(-/-)) mice. These mice lack major histocompatibility complex class I and CD1d antigens, which results in the absence of CD8(+) T cells and natural killer T (NKT) cells. When C57BL/6 and beta(2)m(-/-) mice were injected with parasitized (Plasmodium yoelii 17XNL) erythrocytes, both survived from the infection and showed a similar level of parasitaemia. The major expanding T cells were NK1.1(-) alphabeta T-cell receptor(int) cells in both mice. The difference was a compensatory expansion of NK and gammadelta T cells in beta(2)m(-/-) mice, and an elimination experiment showed that these lymphocytes were critical for protection in these mice. These results suggest that malaria protection might be events of the innate immunity associated with multiple subsets with autoreactivity. CD8(+) T and NKT cells may be partially related to this protection.
疟疾的保护作用是由与T细胞和B细胞相关的传统免疫介导,还是由与胸腺外T细胞和产生自身抗体的B细胞相关的先天免疫介导,目前仍存在争议。鉴于这种情况,研究β2-微球蛋白缺陷(β2m-/-)小鼠的疟疾保护机制很重要。这些小鼠缺乏主要组织相容性复合体I类和CD1d抗原,导致CD8+T细胞和自然杀伤T(NKT)细胞缺失。当给C57BL/6和β2m-/-小鼠注射感染疟原虫(约氏疟原虫17XNL)的红细胞时,两者均从感染中存活下来,且寄生虫血症水平相似。两种小鼠中主要扩增的T细胞均为NK1.1-αβT细胞受体int细胞。不同之处在于β2m-/-小鼠中NK细胞和γδT细胞的代偿性扩增,一项清除实验表明这些淋巴细胞对这些小鼠的保护至关重要。这些结果表明,疟疾保护可能是与具有自身反应性的多个亚群相关的先天免疫事件。CD8+T细胞和NKT细胞可能与这种保护有部分关联。