Balish E, Vazquez-Torres F A, Jones-Carson J, Wagner R D, Warner T
Department of Surgery, University of Wisconsin Medical School, Madison 53706-1532, USA.
Infect Immun. 1996 Dec;64(12):5092-7. doi: 10.1128/iai.64.12.5092-5097.1996.
beta2-Microglobulin knockout (beta2m-/-) mice, which lack major histocompatibility complex class I expression and are deficient in CD8alpha/beta T-cell receptor alpha/beta (TcRalpha/beta) T cells, were as resistant to systemic (intravenous) challenge with Candida albicans as immunocompetent controls. Conversely, the beta2m-/- mutant mice were susceptible to systemic candidiasis of endogenous origin despite the induction of C. albicans-specific antibody and cell-mediated immune responses after colonization with a pure culture of C. albicans. Despite some superficial and transient infections of tongues and esophagi (detected by histology) at 1 to 2 weeks after oral colonization and gastric infections (cardia-antrum section) which were observed at 10 to 12 weeks after oral challenge, C. albicans-colonized beta2m-/- mice showed an overall resistance to candidiasis in other mucosal and cutaneous tissues. These data suggest that immune defects that accompany the loss of beta2-microglobulin play an important role in murine resistance to gastric and disseminated candidiasis of endogenous (intestinal tract) origin and that innate immunity and CD4 TcRalpha/beta as well as CD8alpha/alpha TcRalpha/beta (or -gamma/delta) T cells play an important role in resistance to systemic, cutaneous, and nongastric mucosal tissues.
β2-微球蛋白基因敲除(β2m-/-)小鼠缺乏主要组织相容性复合体I类表达,且缺乏CD8α/β T细胞受体α/β(TcRα/β)T细胞,它们对白色念珠菌的全身(静脉)攻击具有与免疫活性对照相同的抵抗力。相反,β2m-/-突变小鼠易患内源性系统性念珠菌病,尽管在用白色念珠菌纯培养物定植后诱导了白色念珠菌特异性抗体和细胞介导的免疫反应。尽管在口腔定植后1至2周出现了一些浅表和短暂的舌头和食管感染(通过组织学检测),以及在口腔攻击后10至12周观察到胃感染(贲门-胃窦部),但白色念珠菌定植的β2m-/-小鼠在其他黏膜和皮肤组织中总体上对念珠菌病具有抵抗力。这些数据表明,伴随β2-微球蛋白缺失的免疫缺陷在小鼠对内源性(肠道)来源的胃和播散性念珠菌病的抵抗力中起重要作用,并且固有免疫以及CD4 TcRα/β和CD8α/α TcRα/β(或-γ/δ)T细胞在对全身、皮肤和非胃黏膜组织的抵抗力中起重要作用。
