Vallance B A, Galeazzi F, Collins S M, Snider D P
Intestinal Diseases Research Programme, McMaster University, Hamilton, Ontario, Canada.
Infect Immun. 1999 Nov;67(11):6090-7. doi: 10.1128/IAI.67.11.6090-6097.1999.
Expulsion of intestinal nematode parasites and the associated increased contraction by intestinal muscle are T cell dependent, since both are attenuated in athymic rodents. The CD4 T-cell subset has been strongly associated with worm expulsion; however, the relationship between these cells, antigen presentation, and worm expulsion is not definitive and the role of these factors in intestinal muscle hypercontractility has not been defined. We infected C57BL/6, athymic, CD4-deficient, CD8alpha-deficient, and major histocompatibility complex class II (MHC II)-deficient (C2d) mice with Trichinella spiralis larvae. We examined intestinal worm numbers, longitudinal muscle contraction, and MHC II expression. Numerous MHC II-positive cells were identified within the muscularis externa of infected but not uninfected C57BL/6 mice. C57BL/6 and CD8alpha-deficient mice developed large increases in muscle contraction, expelling the parasite by day 21. Athymic and C2d mice exhibited much smaller increases in muscle contraction and delayed parasite expulsion. CD4-deficient mice exhibited intermediate levels of muscle contraction and delayed parasite expulsion. To further examine the role of MHC II and CD4 T cells, we irradiated C2d mice and reconstituted them with C57BL/6 bone marrow alone or with C57BL/6 CD4 T cells. C57BL/6 bone marrow alone did not affect muscle function or worm expulsion in recipient C2d mice. Partial CD4 T-cell reconstitution was sufficient to restore increased muscle contraction but not worm expulsion. Thus, hematopoietic MHC II expression alone is insufficient for the development of muscle hypercontractility and worm expulsion, but the addition of even small numbers of CD4 T cells was sufficient to induce intestinal muscle pathophysiology.
肠道线虫寄生虫的排出以及肠道肌肉随之增强的收缩是T细胞依赖性的,因为在无胸腺啮齿动物中这两者都会减弱。CD4 T细胞亚群与蠕虫排出密切相关;然而,这些细胞、抗原呈递和蠕虫排出之间的关系并不明确,且这些因素在肠道肌肉过度收缩中的作用尚未明确。我们用旋毛虫幼虫感染了C57BL/6、无胸腺、CD4缺陷、CD8α缺陷和主要组织相容性复合体II类(MHC II)缺陷(C2d)小鼠。我们检查了肠道蠕虫数量、纵肌收缩和MHC II表达。在感染而非未感染的C57BL/6小鼠的肌层中发现了大量MHC II阳性细胞。C57BL/6和CD8α缺陷小鼠的肌肉收缩大幅增加,到第21天时排出了寄生虫。无胸腺和C2d小鼠的肌肉收缩增加幅度小得多,寄生虫排出延迟。CD4缺陷小鼠的肌肉收缩水平中等,寄生虫排出延迟。为了进一步研究MHC II和CD4 T细胞的作用,我们对C2d小鼠进行照射,然后单独用C57BL/6骨髓或用C57BL/6 CD4 T细胞对其进行重建。单独的C5/B6骨髓对受体C2d小鼠的肌肉功能或蠕虫排出没有影响。部分CD4 T细胞重建足以恢复肌肉收缩增强,但不能恢复蠕虫排出。因此,仅造血MHC II表达不足以发展肌肉过度收缩和蠕虫排出,但即使添加少量CD4 T细胞也足以诱导肠道肌肉病理生理变化。