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口腔癌进展过程中组织蛋白酶L mRNA和蛋白表达的定量分析。

Quantitative analysis of cathepsin L mRNA and protein expression during oral cancer progression.

作者信息

Macabeo-Ong Maricris, Shiboski Caroline H, Silverman Sol, Ginzinger David G, Dekker Nusi, Wong David T W, Jordan Richard C K

机构信息

Department of Stomatology, UCSF, San Francisco, CA 94143, USA.

出版信息

Oral Oncol. 2003 Oct;39(7):638-47. doi: 10.1016/s1368-8375(03)00034-4.

Abstract

Although an important risk factor for oral cancer is the presence of epithelial dysplasia, most of these lesions will not progress to malignancy. Presently, for the individual patient with dysplasia, there are few reliable markers that may indicate the likelihood of progression to oral cancer. Cathepsin L is a lysosomal protease that degrades extracellular matrix material. Because cathepsin L is frequently overexpressed in oral squamous cell carcinoma (SCC) we hypothesized that it is also overexpressed in oral premalignancy and that premalignant lesions that progressed to oral cancer expressed higher levels of cathepsin L than those premalignant lesions that did not. In this retrospective pilot study we examined changes in cathepsin L expression at the mRNA level using quantitative TaqMan RT-PCR and at the protein level by immunohistochemistry in 33 routinely processed oral dysplastic lesions and 14 SCCs obtained from 33 patients. Sixteen of the dysplastic lesions progressed to oral SCC and 17 did not after several years of follow-up. Cathepsin L mRNA was overexpressed in 16/33 (48%) dysplastic lesions and in 9/14 (64%) oral SCC. Cathepsin L protein was also overexpressed in a large proportion of dysplasias and cancers. Overexpression was independent of dysplasia grade and identified in both those patients who progressed to oral SCC and in those who did not. Levels of cathepsin L mRNA and protein did not differ significantly in the progressing versus non-progressing dysplasias (P=0.27). However, cathepsin L mRNA and protein were significantly lower in the non-progressing dysplasias when compared to the oral cancers (P=0.03) but not in the progressing dysplasias suggesting a trend for dysplasias with overexpressed cathepsin L to be more likely to progress to oral cancer.

摘要

虽然上皮发育异常是口腔癌的一个重要风险因素,但这些病变大多数不会发展为恶性肿瘤。目前,对于患有发育异常的个体患者,几乎没有可靠的标志物可以表明其发展为口腔癌的可能性。组织蛋白酶L是一种降解细胞外基质物质的溶酶体蛋白酶。由于组织蛋白酶L在口腔鳞状细胞癌(SCC)中经常过度表达,我们推测它在口腔癌前病变中也过度表达,并且发展为口腔癌的癌前病变比未发展为口腔癌的癌前病变表达更高水平的组织蛋白酶L。在这项回顾性试点研究中,我们使用定量TaqMan RT-PCR检测了33例常规处理的口腔发育异常病变和从33例患者中获取的14例SCC中组织蛋白酶L在mRNA水平的表达变化,并通过免疫组织化学检测了其在蛋白质水平的表达变化。经过数年的随访,16例发育异常病变发展为口腔SCC,17例未发展。组织蛋白酶L mRNA在16/33(48%)的发育异常病变和9/14(64%)的口腔SCC中过度表达。组织蛋白酶L蛋白在大部分发育异常病变和癌症中也过度表达。过度表达与发育异常分级无关,在发展为口腔SCC的患者和未发展为口腔SCC的患者中均有发现。发展性与非发展性发育异常病变中组织蛋白酶L mRNA和蛋白的水平没有显著差异(P = 0.27)。然而,与口腔癌相比,非发展性发育异常病变中组织蛋白酶L mRNA和蛋白显著更低(P = 0.03),但在发展性发育异常病变中并非如此,这表明组织蛋白酶L过度表达的发育异常病变更有可能发展为口腔癌的趋势。

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