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Maspin(在肺癌中18q21.3丝氨酸蛋白酶抑制剂基因簇中最常表达的基因)在肿瘤前支气管病变中强烈表达。

Maspin - the most commonly-expressed gene of the 18q21.3 serpin cluster in lung cancer - is strongly expressed in preneoplastic bronchial lesions.

作者信息

Smith Shirley L, Watson Suzanne G, Ratschiller Daniel, Gugger Mathias, Betticher Daniel C, Heighway Jim

机构信息

Target Identification Group, Roy Castle International Centre for Lung Cancer Research, University of Liverpool, 200 London Rd, Liverpool L3 9TA, UK.

出版信息

Oncogene. 2003 Nov 27;22(54):8677-87. doi: 10.1038/sj.onc.1207127.

DOI:10.1038/sj.onc.1207127
PMID:14647462
Abstract

Maspin, SCCA1/2 and hurpin were identified by cDNA microarray analyses as dramatically differentially expressed transcripts in primary non-small cell lung cancer (NSCLC). These sequences are located within a 10-gene serpin cluster on 18q21.3. Using comparative RT-PCR, we have investigated the expression of each of these serpins, including their flanking loci, in an independent NSCLC series. Whereas six of the genes (maspin, SCCA1, SCCA2, hurpin, megsin and pAI-2) were commonly differentially expressed in primary lesions, each significantly more often in squamous cell tumours, maspin was identified as the most frequently over-represented sequence in both squamous cell carcinoma and adenocarcinoma. Using a well-characterized monoclonal antibody, we have shown strong maspin expression in tumour protein extracts, detected multiple isoforms of the 42 kDa protein and shown that maspin is localized specifically to the tumour cells within neoplastic lesions. In contrast, most cells in non-neoplastic lung tissue appear not to express the gene, with the exception of the multipotent basal epithelial cells that line the bronchial airway. These reserve cells generally show strong predominantly nuclear localization of maspin. Strong nuclear expression of maspin within primary tumour cells is correlated with increased survival (P=0.05) and a longer remission duration (P=0.02) in resectable-staged patients. However, within the airways of cancer patients and somewhat in contrast to this observation, such expression was more frequently detected in the superficial cells of preneoplastic over non-neoplastic epithelia (P<0.0001), consistent with a role for the protein in early neoplasia.

摘要

通过cDNA微阵列分析,在原发性非小细胞肺癌(NSCLC)中,maspin、SCCA1/2和hurpin被鉴定为差异表达显著的转录本。这些序列位于18q21.3上的一个包含10个基因的丝氨酸蛋白酶抑制剂(serpin)基因簇内。我们利用比较逆转录-聚合酶链反应(RT-PCR),在一个独立的NSCLC系列中研究了这些丝氨酸蛋白酶抑制剂及其侧翼基因座的表达情况。虽然其中六个基因(maspin、SCCA1、SCCA2、hurpin、megsin和pAI-2)在原发性病变中普遍存在差异表达,且在鳞状细胞肿瘤中差异表达更为显著,但maspin被确定为在鳞状细胞癌和腺癌中最常过度表达的序列。使用一种特性明确的单克隆抗体,我们在肿瘤蛋白提取物中检测到maspin的强表达,发现了42 kDa蛋白的多种异构体,并表明maspin特异性定位于肿瘤病变内的肿瘤细胞。相比之下,非肿瘤性肺组织中的大多数细胞似乎不表达该基因,但支气管气道内衬的多能基底上皮细胞除外。这些储备细胞通常显示maspin主要定位于细胞核。原发性肿瘤细胞内maspin的强核表达与可切除分期患者的生存率提高(P = 0.05)和缓解期延长(P = 0.02)相关。然而,在癌症患者的气道中,与这一观察结果有所不同的是,在癌前上皮细胞的表层细胞中比在非肿瘤性上皮细胞中更频繁地检测到这种表达(P < 0.0001),这与该蛋白在早期肿瘤形成中的作用一致。

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