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GD2低聚糖:细胞毒性T淋巴细胞的靶点。

GD2 oligosaccharide: target for cytotoxic T lymphocytes.

作者信息

Zhao X J, Cheung N K

机构信息

Department of Pediatrics, Memorial Sloan Kettering Cancer Center, New York 10021, USA.

出版信息

J Exp Med. 1995 Jul 1;182(1):67-74. doi: 10.1084/jem.182.1.67.

Abstract

Carbohydrate antigens rarely provide target epitopes for cytotoxic T lymphocytes (CTL). Disialoganglioside GD2 is a glycolipid expressed at high levels in human tumors and a small group of murine lymphomas (EL4, RBL5, RMA, RMA-S, A13, and BALBRVE). Immunization of C57B1/6 mice with irradiated EL4 cells stimulated a specific CTL response and protected these animals from engraftment of EL4 lymphoma. The CTL activity resided in the CD4-CD8+ population, was dependent on T cell receptor alpha/beta, and was not removed by anti-natural killer cell immunoabsorption, but was restricted to GD2 and H-2b bearing targets. CTL activity could be completely inhibited by GD2-oligosaccharide-specific monoclonal antibodies and their F(ab')2 fragments, but not by immunoglobulin G3 myelomas or antibodies against GD3 or GM2. Soluble GD2 did not inhibit specific tumor lysis. RMA-S lymphoma cells (GD2+H-2b-TAP2 deficient) were resistant to GD2-specific CTL. Sialic acid-containing peptides eluted from EL4 lymphoma cells could (a) stabilize H-2 molecules on RMA-S cells and (b) sensitize them for GD2-specific CTL. Control peptides (derived from vesicular stomatitis virus nucleoprotein peptide and GD2-negative lymphomas) could also stabilize H-2 on RMA-S, but were resistant to GD2-specific CTL. These H-2-binding peptides could be purified by anti-GD2 affinity chromatography. We postulate a new class of naturally occurring epitopes for T cells where branched-chain oligosaccharides are linked to peptides with anchoring motifs for the major histocompatibility complex class I pocket. While analogous to the haptens trinitrophenyl and O-beta-linked acetyl-glucosamine, the potential implications of natural carbohydrates as antigenic epitopes for CTL in biology are considerable.

摘要

碳水化合物抗原很少为细胞毒性T淋巴细胞(CTL)提供靶表位。双唾液酸神经节苷脂GD2是一种糖脂,在人类肿瘤和一小部分鼠淋巴瘤(EL4、RBL5、RMA、RMA - S、A13和BALBRVE)中高水平表达。用经辐射的EL4细胞免疫C57B1/6小鼠可刺激特异性CTL反应,并保护这些动物免受EL4淋巴瘤的植入。CTL活性存在于CD4 - CD8 + 群体中,依赖于T细胞受体α/β,且不能通过抗自然杀伤细胞免疫吸附去除,但仅限于带有GD2和H - 2b的靶细胞。GD2 - 寡糖特异性单克隆抗体及其F(ab')2片段可完全抑制CTL活性,但免疫球蛋白G3骨髓瘤或抗GD3或GM2的抗体则不能。可溶性GD2不抑制特异性肿瘤溶解。RMA - S淋巴瘤细胞(GD2 + H - 2b - TAP2缺陷)对GD2特异性CTL具有抗性。从EL4淋巴瘤细胞洗脱的含唾液酸肽可(a)稳定RMA - S细胞上的H - 2分子,以及(b)使其对GD2特异性CTL敏感。对照肽(源自水泡性口炎病毒核蛋白肽和GD2阴性淋巴瘤)也可稳定RMA - S细胞上的H - 2,但对GD2特异性CTL具有抗性。这些H - 2结合肽可通过抗GD2亲和层析纯化。我们推测存在一类新的T细胞天然表位,其中支链寡糖与具有主要组织相容性复合体I类口袋锚定基序的肽相连。虽然类似于三硝基苯基和O - β - 连接的乙酰葡糖胺等半抗原,但天然碳水化合物作为CTL在生物学中的抗原表位的潜在意义重大。

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