通过MART-1特异性CTL培养使黑色素瘤肿瘤细胞对非MHC Fas介导的杀伤产生免疫致敏。
Immunosensitization of melanoma tumor cells to non-MHC Fas-mediated killing by MART-1-specific CTL cultures.
作者信息
Frost P J, Butterfield L H, Dissette V B, Economou J S, Bonavida B
机构信息
Department of Microbiology, Immunology and Molecular Genetics, University of California School of Medicine, University of California, Los Angeles, CA 90095, USA.
出版信息
J Immunol. 2001 Mar 1;166(5):3564-73. doi: 10.4049/jimmunol.166.5.3564.
The discovery of human melanoma rejection Ags has allowed the rational design of immunotherapeutic strategies. One such Ag, MART-1, is expressed on >90% of human melanomas, and CTL generated against MART-1(27-35) kill most HLA A2.1(+) melanoma cells. However, variant tumor cells, which do not express MART-1, down-regulate MHC, or become resistant to apoptosis, will escape killing. Cytotoxic lymphocytes kill by two main mechanisms, the perforin/granzyme degranulation pathway and the TNF/Fas/TNF-related apoptosis-inducing ligand superfamily of apoptosis-inducing ligands. In this study, we examined whether cis-diaminedichloroplatinum (II) cisplatin (CDDP) sensitizes MART-1/HLA A2.1(+) melanoma and melanoma variant tumor cells to non-MHC-restricted, Fas ligand (FasL)-mediated killing by CTL. MART-1(27-35)-specific bulk CTL cultures were generated by pulsing normal PBL with MART-1(27-35) peptide. These CTL cultures specifically kill M202 melanoma cells (MART-1(+), HLA A2.1(+), FasR(-)), and MART-1(27-35) peptide-pulsed T2 cells (FasR(+)), but not M207 melanoma cells (MART-1(+), HLA A2.1(-), FasR(-)), FLU(58-66) peptide-pulsed T2 cells, or DU145 and PC-3 prostate cells (MART-1(-), HLA A2.1(-), FasR(+)). CDDP (0.1-10 microg/ml) sensitized non-MART-1(27-35) peptide-pulsed T2 to the CD8(+) subset of bulk MART-1-specific CTL, and killing was abolished by neutralizing anti-Fas Ab. Furthermore, CDDP up-regulated FasR expression and FasL-mediated killing of M202, and sensitized PC-3 and DU145 to killing by bulk MART-1-specific CTL cultures. These findings demonstrate that drug-mediated sensitization can potentiate FasL-mediated killing by MHC-restricted CTL cell lines, independent of MHC and MART-1 expression on tumor cells. This represents a novel approach for potentially controlling tumor cell variants found in primary heterogeneous melanoma tumor cell populations that would normally escape killing by MART-1-specific immunotherapy.
人类黑色素瘤排斥抗原的发现使得免疫治疗策略的合理设计成为可能。其中一种抗原MART-1在超过90%的人类黑色素瘤中表达,针对MART-1(27 - 35)产生的细胞毒性T淋巴细胞(CTL)可杀死大多数HLA A2.1(+)黑色素瘤细胞。然而,不表达MART-1、下调主要组织相容性复合体(MHC)或对凋亡产生抗性的变异肿瘤细胞将会逃脱杀伤。细胞毒性淋巴细胞通过两种主要机制杀伤,即穿孔素/颗粒酶脱颗粒途径以及肿瘤坏死因子(TNF)/Fas/TNF相关凋亡诱导配体超家族的凋亡诱导配体途径。在本研究中,我们检测了顺二氯二氨铂(II)(顺铂,CDDP)是否能使MART-1/HLA A2.1(+)黑色素瘤及黑色素瘤变异肿瘤细胞对非MHC限制性的、由CTL介导的Fas配体(FasL)杀伤作用敏感。通过用MART-1(27 - 35)肽刺激正常外周血淋巴细胞(PBL)产生MART-1(27 - 35)特异性的大量CTL培养物。这些CTL培养物能特异性杀死M202黑色素瘤细胞(MART-1(+),HLA A2.1(+),Fas受体(FasR)(-))以及MART-1(27 - 35)肽刺激的T2细胞(FasR(+)),但不能杀死M207黑色素瘤细胞(MART-1(+),HLA A .2(-),FasR(-))、FLU(58 - 66)肽刺激的T2细胞,或DU145和PC-3前列腺细胞(MART-1(-),HLA A2.1(-),FasR(+))。CDDP(0.1 - 10微克/毫升)使未用MART-1(27 - 35)肽刺激的T2细胞对大量MART-1特异性CTL的CD8(+)亚群敏感,并且通过中和抗Fas抗体可消除杀伤作用。此外,CDDP上调FasR表达以及FasL介导的对M202的杀伤作用,并使PC-3和DU145对大量MART-1特异性CTL培养物的杀伤作用敏感。这些发现表明药物介导的致敏作用可增强MHC限制性CTL细胞系介导的FasL杀伤作用,而与肿瘤细胞上的MHC和MART-1表达无关。这代表了一种潜在控制原发性异质性黑色素瘤肿瘤细胞群体中通常会逃脱MART-1特异性免疫治疗杀伤的肿瘤细胞变异体的新方法。
Zotero 插件