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鉴定 SPARC 作为各种癌症免疫治疗的候选靶抗原。

Identification of SPARC as a candidate target antigen for immunotherapy of various cancers.

机构信息

Department of Immunogenetics, Graduate School of Medical Sciences, Kumamoto University, Kumamoto, Japan.

出版信息

Int J Cancer. 2010 Sep 1;127(6):1393-403. doi: 10.1002/ijc.25160.

DOI:10.1002/ijc.25160
PMID:20063317
Abstract

To establish efficient anticancer immunotherary, it is important to identify tumor-associated antigens (TAAs) directing the immune system to attack cancer. A genome-wide cDNA microarray analysis identified that secreted protein acidic and rich in cysteine (SPARC) gene is overexpressed in the gastric, pancreatic and colorectal cancer tissues but not in their noncancerous counterparts. This study attempted to identify HLA-A24 (A2402)-restricted and SPARC-derived CTL epitopes. We previously identified H-2K(d)-restricted and SPARC-derived CTL epitope peptides in BALB/c mice, of which H-2K(d)-binding peptide motif is comparable with that of HLA-A24 binding peptides. By using these peptides, we tried to induce HLA-A24 (A2402)-restricted and SPARC-reactive human CTLs and demonstrated an antitumor immune response. The SPARC-A24-1(143-151) (DYIGPCKYI) and SPARC-A24-4(225-234) (MYIFPVHWQF) peptides-reactive CTLs were successfully induced from peripheral blood mononuclear cells by in vitro stimulation with these two peptides in HLA-A24 (A2402) positive healthy donors and cancer patients, and these CTLs exhibited cytotoxicity specific to cancer cells expressing both SPARC and HLA-A24 (A2402). Furthermore, the adoptive transfer of the SPARC-specific CTLs could inhibit the tumor growth in nonobese diabetic/severe combined immunodeficient mice bearing human cancer cells expressing both HLA-A24 (A*2402) and SPARC. These findings suggest that SPARC is a potentially useful target candidate for cancer immunotherapy.

摘要

为了建立有效的抗癌免疫疗法,识别引导免疫系统攻击癌症的肿瘤相关抗原(TAA)非常重要。全基因组 cDNA 微阵列分析表明,分泌富含半胱氨酸的酸性蛋白(SPARC)基因在胃癌、胰腺癌和结直肠癌组织中过度表达,但在其非癌组织中没有表达。本研究试图鉴定 HLA-A24(A2402)限制性和 SPARC 衍生的 CTL 表位。我们之前在 BALB/c 小鼠中鉴定了 H-2K(d)-限制性和 SPARC 衍生的 CTL 表位肽,其中 H-2K(d)结合肽基序与 HLA-A24 结合肽基序具有可比性。通过使用这些肽,我们试图诱导 HLA-A24(A2402)限制性和 SPARC 反应性人类 CTL,并证明了抗肿瘤免疫反应。通过体外用这两种肽刺激 HLA-A24(A2402)阳性健康供体和癌症患者的外周血单核细胞,成功诱导出对 SPARC-A24-1(143-151)(DYIGPCKYI)和 SPARC-A24-4(225-234)(MYIFPVHWQF)肽反应性 CTL,这些 CTL 对表达 SPARC 和 HLA-A24(A2402)的癌细胞具有特异性细胞毒性。此外,SPARC 特异性 CTL 的过继转移可抑制在表达 HLA-A24(A*2402)和 SPARC 的非肥胖糖尿病/严重联合免疫缺陷小鼠中携带人癌细胞的肿瘤生长。这些发现表明 SPARC 是癌症免疫治疗的一个有前途的候选靶标。

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