视神经脊髓炎中的水通道蛋白 4 特异性 T 细胞表现出 Th17 偏向,并识别梭菌 ABC 转运蛋白。
Aquaporin 4-specific T cells in neuromyelitis optica exhibit a Th17 bias and recognize Clostridium ABC transporter.
机构信息
Departments of Neurology, University of California at San Francisco, USA.
出版信息
Ann Neurol. 2012 Jul;72(1):53-64. doi: 10.1002/ana.23651. Epub 2012 Jul 17.
OBJECTIVE
Aquaporin 4 (AQP4)-specific autoantibodies in neuromyelitis optica (NMO) are immunoglobulin (Ig)G1, a T cell-dependent Ig subclass, indicating that AQP4-specific T cells participate in NMO pathogenesis. Our goal was to identify and characterize AQP4-specific T cells in NMO patients and healthy controls (HC).
METHODS
Peripheral blood T cells from NMO patients and HC were examined for recognition of AQP4 and production of proinflammatory cytokines. Monocytes were evaluated for production of T cell-polarizing cytokines and expression of costimulatory molecules.
RESULTS
T cells from NMO patients and HC proliferated to intact AQP4 or AQP4 peptides (p11-30, p21-40, p61-80, p131-150, p156-170, p211-230, and p261-280). T cells from NMO patients demonstrated greater proliferation to AQP4 than those from HC, and responded most vigorously to p61-80, a naturally processed immunodominant determinant of intact AQP4. T cells were CD4(+), and corresponding to association of NMO with human leukocyte antigen (HLA)-DRB1*0301 and DRB3, AQP4 p61-80-specific T cells were HLA-DR restricted. The T-cell epitope within AQP4 p61-80 was mapped to 63-76, which contains 10 residues with 90% homology to a sequence within Clostridium perfringens adenosine triphosphate-binding cassette (ABC) transporter permease. T cells from NMO patients proliferated to this homologous bacterial sequence, and cross-reactivity between it and self-AQP4 was observed, supporting molecular mimicry. In NMO, AQP4 p61-80-specific T cells exhibited Th17 polarization, and furthermore, monocytes produced more interleukin 6, a Th17-polarizing cytokine, and expressed elevated CD40 and CD80 costimulatory molecules, suggesting innate immunologic dysfunction.
INTERPRETATION
AQP4-specific T-cell responses are amplified in NMO, exhibit a Th17 bias, and display cross-reactivity to a protein of an indigenous intestinal bacterium, providing new perspectives for investigating NMO pathogenesis.
目的
视神经脊髓炎(NMO)中特异的水通道蛋白 4(AQP4)自身抗体是 IgG1,这是一种 T 细胞依赖性的免疫球蛋白亚类,表明 AQP4 特异性 T 细胞参与了 NMO 的发病机制。我们的目标是鉴定和描述 NMO 患者和健康对照者(HC)中的 AQP4 特异性 T 细胞。
方法
检测 NMO 患者和 HC 的外周血 T 细胞对 AQP4 的识别和促炎细胞因子的产生。评估单核细胞产生 T 细胞极化细胞因子和表达共刺激分子的情况。
结果
NMO 患者和 HC 的 T 细胞对完整的 AQP4 或 AQP4 肽(p11-30、p21-40、p61-80、p131-150、p156-170、p211-230 和 p261-280)均有增殖反应。与 HC 相比,NMO 患者的 T 细胞增殖更强烈,对自然加工的完整 AQP4 的免疫优势决定簇 p61-80 反应最为强烈。T 细胞是 CD4+的,与 NMO 与人类白细胞抗原(HLA)-DRB1*0301 和 DRB3 的关联有关,AQP4 p61-80 特异性 T 细胞受 HLA-DR 限制。AQP4 p61-80 内的 T 细胞表位定位于 63-76,其中包含与梭状芽胞杆菌腺苷三磷酸结合盒(ABC)转运体通透酶内一段序列有 90%同源性的 10 个残基。NMO 患者的 T 细胞对该同源细菌序列有增殖反应,并且观察到其与自身 AQP4 之间的交叉反应性,支持分子模拟。在 NMO 中,AQP4 p61-80 特异性 T 细胞表现出 Th17 极化,此外,单核细胞产生更多的白细胞介素 6,一种 Th17 极化细胞因子,并表达升高的 CD40 和 CD80 共刺激分子,提示固有免疫功能障碍。
解释
AQP4 特异性 T 细胞反应在 NMO 中被放大,表现出 Th17 偏向性,并显示对一种内源性肠道细菌蛋白的交叉反应性,为研究 NMO 的发病机制提供了新的视角。
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