Urban J L, Kumar V, Kono D H, Gomez C, Horvath S J, Clayton J, Ando D G, Sercarz E E, Hood L
Division of Biology, California Institute of Technology Pasadena 91125.
Cell. 1988 Aug 12;54(4):577-92. doi: 10.1016/0092-8674(88)90079-7.
Experimental allergic encephalomyelitis (EAE) is a paralytic autoimmune disease induced in susceptible animals by active immunization with myelin basic protein (MBP) or by passive transfer of MBP-specific T helper (TH) lymphocytes. We have analyzed the T cell receptor genes of 33 clonally distinct TH cells specific for a nonapeptide of MBP inducing EAE in B10.PL (H-2u) mice. All 33 TH cells used two alpha variable gene segments (V alpha 2.3, 61%; V alpha 4.2, 39%), the same alpha joining gene segment (J alpha 39), and two V beta and J beta gene segments (V beta 8.2-J beta 2.6, 79%; V beta 13-J beta 2.2, 21%). The anti-V beta 8 monoclonal antibody F23.1 was found to block completely recognition of the nonapeptide by V beta 8 TH cells in vitro and to reduce significantly the susceptibility of B10.PL mice to peptide-induced EAE.
实验性变应性脑脊髓炎(EAE)是一种麻痹性自身免疫疾病,可通过用髓磷脂碱性蛋白(MBP)进行主动免疫或通过MBP特异性T辅助(TH)淋巴细胞的被动转移在易感动物中诱发。我们分析了33个克隆性不同的TH细胞的T细胞受体基因,这些细胞对在B10.PL(H-2u)小鼠中诱导EAE的MBP九肽具有特异性。所有33个TH细胞都使用了两个α可变基因片段(Vα2.3,61%;Vα4.2,39%)、相同的α连接基因片段(Jα39)以及两个Vβ和Jβ基因片段(Vβ8.2-Jβ2.6,79%;Vβ13-Jβ2.2,21%)。发现抗Vβ8单克隆抗体F23.1在体外可完全阻断Vβ8 TH细胞对九肽的识别,并显著降低B10.PL小鼠对肽诱导的EAE的易感性。
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