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L552S是XAGE-1的一种选择性剪接异构体,在肺腺癌中过度表达。

L552S, an alternatively spliced isoform of XAGE-1, is over-expressed in lung adenocarcinoma.

作者信息

Wang T, Fan L, Watanabe Y, McNeill P, Fanger G R, Persing D H, Reed S G

机构信息

Department of Tumor Antigen Discovery, Corixa Corporation, 1124 Columbia Street, Seattle, WA 98104, USA.

出版信息

Oncogene. 2001 Nov 22;20(53):7699-709. doi: 10.1038/sj.onc.1204939.

Abstract

Using a combination of cDNA subtraction and microarray analysis, we report here the identification and characterization of L552S, an over-expressed, alternatively spliced isoform of XAGE-1 in lung adenocarcinoma. Real-time RT-PCR analysis shows that L552S is expressed at levels greater than 10-fold in 12 of 25 lung adenocarcinoma tumors compared with the highest expression level found in all normal tissues tested. L552S is expressed in both early and late stages of lung adenocarcinoma, but it was not detected in large cell carcinoma, small cell carcinoma, or atypical lung neuroendocrine carcinoid. The full-length cDNA for L552S comprises 770 bp and encodes a polypeptide of 160 amino acids. C-terminal 94 amino acids of L552S are identical to a cancer testis antigen, XAGE-1, found in Ewing's sarcoma. Genomic sequence analysis has revealed that L552S and XAGE-1 are alternatively spliced isoforms, and expression of both L552S and XAGE-1 isoforms are present in lung adenocarcinoma. Immunohistochemistry analysis using affinity purified L552S polyclonal antibodies demonstrated specific nuclear staining in 10 of 12 lung adenocarcinoma samples. Furthermore, antibody responses to recombinant L552S protein were observed in seven of 17 lung pleural effusion fluids of lung cancer patients. These results strongly imply that L552S protein is immunogenic and suggest that it might have use as a vaccine target for lung cancer.

摘要

通过结合cDNA消减和微阵列分析,我们在此报告了L552S的鉴定和特征,L552S是肺腺癌中一种过度表达的、可变剪接的XAGE-1同种型。实时RT-PCR分析表明,与所有测试的正常组织中发现的最高表达水平相比,25例肺腺癌肿瘤中有12例L552S的表达水平高出10倍以上。L552S在肺腺癌的早期和晚期均有表达,但在大细胞癌、小细胞癌或非典型肺神经内分泌类癌中未检测到。L552S的全长cDNA包含770 bp,编码一个160个氨基酸的多肽。L552S的C末端94个氨基酸与在尤因肉瘤中发现的一种癌胚抗原XAGE-1相同。基因组序列分析表明,L552S和XAGE-1是可变剪接的同种型,且L552S和XAGE-1同种型在肺腺癌中均有表达。使用亲和纯化的L552S多克隆抗体进行的免疫组织化学分析显示,12例肺腺癌样本中有10例出现特异性核染色。此外,在17例肺癌患者的肺胸积液中有7例观察到对重组L552S蛋白的抗体反应。这些结果强烈表明L552S蛋白具有免疫原性,并提示它可能用作肺癌的疫苗靶点。

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