Teuscher C, Hickey W F, Korngold R
Division of Reproductive Biology, University of Pennsylvania, Philadelphia, Pennsylvania.
Immunogenetics. 1990;32(1):34-40. doi: 10.1007/BF01787326.
Previous studies have shown that differential susceptibility to actively induced experimental allergic orchitis (EAO) exists among various BALB/c substrains. Of 13 substrains studied, BALB/cJ mice consistently exhibit greater resistance to disease induction. Such resistance is associated with a single recessive genotypic difference in an immunoregulatory locus which is unlinked to any of the known alleles distinguishing the BALB/cJ substrain. In this study, gene complementation protocols were used to study the genetics of susceptibility and resistance to EAO. The results indicate that resistance in BALB/cJ mice is not due to a mutation in the H-2Dd linked gene which governs the phenotypic expression of autoimmune orchitis. The mechanistic basis for disease resistance was examined using reciprocal bone marrow radiation chimeras generated between the disease-susceptible BALB/cByJ (ByJ) substrain and BALB/cJ (Jax) mice. All constructs, including Jax----Jax and Jax----ByJ, developed severe EAO following inoculation with mouse testicular homogenate (MTH) and adjuvants whereas control chimeras immunized with adjuvants alone did not. These results suggest that an active immunoregulatory mechanism rather than a passive one, such as the lack of T cells and/or B cells with receptors for the aspermatogenic autoantigens relevant in the induction of EAO, is responsible for disease resistance in BALB/cJ mice. The role of immunoregulatory cells was examined by pretreating BALB/cJ mice with either cyclophosphamide (20 mg/kg) or low-dose whole body or total lymphoid irradiation (350 rads) 2 days prior to inoculation. BALB/cJ mice immunized with MTH plus adjuvants generate immunoregulatory spleen cells (SpCs) that, when transferred to naive BALB/cByJ recipients, significantly reduce the severity of autoimmune orchitis observed during actively induced EAO. Treatment of such cells with either cytotoxic monoclonal anti-Thy-1.2 or anti-CD4 plus C' before transfer abrogates the ability of BALB/cJ spleen cells to inhibit disease. In contrast, neither SpCs from adjuvant-immunized BALB/cJ nor MTH plus adjuvant-primed BALB/cByJ donors significantly influenced the severity of disease observed in recipients. Taken together, these results suggest that genetically controlled resistance to EAO in BALB/cJ mice is associated with a mutation in an immunoregulatory locus whose effects appear to be mediated through a cyclophosphamide and low-dose radiation-sensitive CD4+ T-cell population.
先前的研究表明,不同的BALB/c亚系对主动诱导的实验性过敏性睾丸炎(EAO)存在易感性差异。在研究的13个亚系中,BALB/cJ小鼠始终表现出对疾病诱导更强的抵抗力。这种抵抗力与免疫调节位点上的一个单一隐性基因型差异有关,该位点与区分BALB/cJ亚系的任何已知等位基因均无连锁关系。在本研究中,采用基因互补方案来研究对EAO的易感性和抗性遗传学。结果表明,BALB/cJ小鼠的抗性并非由于与自身免疫性睾丸炎表型表达相关的H-2Dd连锁基因发生突变。利用疾病易感的BALB/cByJ(ByJ)亚系和BALB/cJ(Jax)小鼠之间产生的相互骨髓辐射嵌合体,研究了疾病抗性的机制基础。所有构建体,包括Jax----Jax和Jax----ByJ,在接种小鼠睾丸匀浆(MTH)和佐剂后均发生了严重的EAO,而仅用佐剂免疫的对照嵌合体则未发生。这些结果表明,BALB/cJ小鼠的疾病抗性是由一种主动免疫调节机制而非被动机制(如缺乏对诱导EAO相关的生精自身抗原具有受体的T细胞和/或B细胞)所介导。通过在接种前2天用环磷酰胺(20mg/kg)或低剂量全身或全淋巴照射(350拉德)预处理BALB/cJ小鼠,研究了免疫调节细胞的作用。用MTH加佐剂免疫的BALB/cJ小鼠产生免疫调节性脾细胞(SpC),当将这些脾细胞转移到未免疫的BALB/cByJ受体小鼠时,可显著降低主动诱导EAO期间观察到的自身免疫性睾丸炎的严重程度。在转移前用细胞毒性单克隆抗Thy-1.2或抗CD4加补体C处理这些细胞,可消除BALB/cJ脾细胞抑制疾病的能力。相反,来自用佐剂免疫的BALB/cJ或用MTH加佐剂致敏的BALB/cByJ供体的SpC对受体小鼠中观察到的疾病严重程度均无显著影响。综上所述,这些结果表明,BALB/cJ小鼠对EAO的遗传控制抗性与免疫调节位点的突变有关,其作用似乎是通过环磷酰胺和低剂量辐射敏感的CD4+T细胞群体介导的。
