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源自YACUT T细胞淋巴瘤与在二次混合淋巴细胞培养中激活的正常淋巴细胞之间增殖受抑制的体细胞杂种的新型杀伤性杂交瘤的产生。

Generation of novel killer hybridomas derived from proliferation-suppressed somatic cell hybrids between YACUT T cell lymphoma and normal lymphocytes activated in secondary mixed lymphocyte cultures.

作者信息

Kubota K, Nakazato K, Tamauchi H, Sasahara T, Katoh H

机构信息

Department of Microbiology, Kitasato University School of Medicine, Kanagawa, Japan.

出版信息

J Immunol Methods. 1996 Jun 10;192(1-2):137-47. doi: 10.1016/0022-1759(96)00030-0.

Abstract

Somatic cell hybridization between the YACUT T cell lymphoma cell line with normal lymphocytes activated in secondary mixed lymphocyte cultures (MLCs) consistently yielded IL-2-dependent CD4- CD8 alpha+ beta- Fc gamma RIII+ hybrids with cytotoxic function. The hybrids expressed T cell receptors other than that of YACUT origin, and fusion of the YACUT with a CD8 alpha+ beta+ Fc gamma RIII- T cell line also yielded hybrids with an unexpected CD8 alpha+ beta- Fc gamma RIII+ phenotype, which two observations strongly suggested that CD8+ T cells became the parental cell of the hybrids. Prolonged growth of the hybrids with IL-2 resulted in the generation of autonomously growing hybrids (hybridomas) without abrogating the cytotoxic function. The hybridomas exhibited MHC-unrestricted cytotoxicity in a Ca(2+)-dependent manner without prior stimulation and also mediated antibody-dependent cellular cytotoxicity. These results indicate that novel killer hybridomas can be produced following cell transformation of proliferation-suppressed cytotoxic YACUT x MLC cell hybrids. The killer hybridomas may be of value for analyzing recognition mechanisms and molecules involved in MHC-unrestricted cell-mediated cytotoxicity.

摘要

YACUT T细胞淋巴瘤细胞系与在二次混合淋巴细胞培养物(MLC)中被激活的正常淋巴细胞进行体细胞杂交,始终产生具有细胞毒性功能的白细胞介素-2依赖性CD4-CD8α+β-FcγRIII+杂交细胞。这些杂交细胞表达的T细胞受体并非源自YACUT,并且将YACUT与CD8α+β+FcγRIII-T细胞系融合也产生了具有意外的CD8α+β-FcγRIII+表型的杂交细胞,这两个观察结果强烈表明CD8+T细胞成为了杂交细胞的亲代细胞。用白细胞介素-2长时间培养杂交细胞导致产生自主生长的杂交细胞(杂交瘤),且未消除其细胞毒性功能。这些杂交瘤在无预先刺激的情况下以钙依赖方式表现出MHC非限制性细胞毒性,并且还介导抗体依赖性细胞毒性。这些结果表明,增殖受抑制的细胞毒性YACUT×MLC细胞杂交细胞在细胞转化后可产生新型杀伤杂交瘤。这些杀伤杂交瘤对于分析参与MHC非限制性细胞介导的细胞毒性的识别机制和分子可能具有价值。

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