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用脊髓免疫的SJL/J小鼠的淋巴细胞对蛋白脂质蛋白的一种肽产生选择性反应,并传递复发性脱髓鞘实验性自身免疫性脑脊髓炎。

Lymphocytes from SJL/J mice immunized with spinal cord respond selectively to a peptide of proteolipid protein and transfer relapsing demyelinating experimental autoimmune encephalomyelitis.

作者信息

Whitham R H, Bourdette D N, Hashim G A, Herndon R M, Ilg R C, Vandenbark A A, Offner H

机构信息

Neuroimmunology Research, Veterans Administration Medical Center, Portland, OR 97207.

出版信息

J Immunol. 1991 Jan 1;146(1):101-7.

PMID:1701788
Abstract

Relapsing experimental autoimmune encephalomyelitis (R-EAE) can be induced in SJL/J mice by immunization with spinal cord homogenate and adjuvant. The specific Ag(s) responsible for acute disease and subsequent relapses in this model is unknown. Myelin basic protein (BP), an encephalitogenic peptide of BP (BP 87-99), and proteolipid protein (PLP) can each induce R-EAE in SJL/J mice, and a peptide of PLP (PLP 139-151) has been reported to induce acute EAE. To determine the encephalitogens in cord-immunized mice with R-EAE, the in vitro proliferative responses of lymph node cells (LNC) and central nervous system mononuclear cells to BP, BP peptides, and PLP peptides were examined during acute EAE and during relapses. LNC responded only to PLP peptides 139-151 and 141-151 and did not respond to BP or its peptides during acute or chronic disease. Central nervous system mononuclear cells also preferentially responded to PLP 139-151 and 141-151 during acute and relapsing disease. A PLP 139-151 peptide-specific Th cell line was selected from LNC of cord-immunized donors. Five million peptide-specific line cells transferred severe relapsing demyelinating EAE to naive recipients. We conclude that PLP peptide 139-151 is the major encephalitogen for R-EAE in cord-immunized SJL/J mice. We demonstrate for the first time that Th cells specific for this peptide are sufficient to transfer relapsing demyelinating EAE. The predominance of a PLP immune response rather than a BP response in SJL/J mice suggests that genetic background may determine the predominant myelin Ag response in human demyelinating diseases such as multiple sclerosis.

摘要

复发性实验性自身免疫性脑脊髓炎(R-EAE)可通过用脊髓匀浆和佐剂免疫SJL/J小鼠诱导产生。该模型中导致急性疾病及随后复发的特异性抗原尚不清楚。髓鞘碱性蛋白(BP)、BP的一种致脑炎性肽(BP 87-99)以及蛋白脂蛋白(PLP)均可在SJL/J小鼠中诱导R-EAE,并且据报道一种PLP肽(PLP 139-151)可诱导急性EAE。为了确定患有R-EAE的经脊髓免疫小鼠中的致脑炎性抗原,在急性EAE期间及复发期间检测了淋巴结细胞(LNC)和中枢神经系统单核细胞对BP、BP肽以及PLP肽的体外增殖反应。在急性或慢性疾病期间,LNC仅对PLP肽139-151和141-151有反应,而对BP或其肽无反应。在急性和复发疾病期间,中枢神经系统单核细胞也优先对PLP 139-151和141-151有反应。从经脊髓免疫供体的LNC中筛选出一种PLP 139-151肽特异性Th细胞系。五百万个肽特异性系细胞将严重复发性脱髓鞘性EAE转移给未免疫的受体。我们得出结论,PLP肽139-151是经脊髓免疫的SJL/J小鼠中R-EAE的主要致脑炎性抗原。我们首次证明针对该肽的Th细胞足以转移复发性脱髓鞘性EAE。SJL/J小鼠中PLP免疫反应而非BP免疫反应占主导地位,这表明遗传背景可能决定人类脱髓鞘疾病如多发性硬化症中主要的髓鞘抗原反应。

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