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Expression of apoptosis-regulatory genes in lung tumour cell lines: relationship to p53 expression and relevance to acquired drug resistance.

机译:凋亡调节基因在肺肿瘤细胞系中的表达:与p53表达的关系以及与获得性耐药的相关性。

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摘要

As a first step towards elucidating the potential role(s) of bcl-2 and bcl-2-related genes in lung tumorigenesis and therapeutic responsiveness, the expression of these genes has been examined in a panel of lung cancer cell lines derived from untreated and treated patients, and in cell lines selected in vitro for multidrug resistance. Bcl-2 was hyperexpressed in 15 of 16 small-cell lung cancer (SCLC) cell lines and two of five non-small-cell lung cancer (NSCLC) lines compared with normal lung and brain, and hyperexpression was not chemotherapy related. Bcl-x was hyperexpressed in the majority of SCLC and NSCLC cell lines as compared with normal tissues, and all lung tumour lines preferentially expressed bcl-x1-mRNA, the splice variant form that inhibits apoptosis. Bax gene transcripts were hyperexpressed in most SCLC and NSCLC cell lines examined compared with normal adult tissues. Mutant p53 gene expression was detected in the majority of the cell lines and no relationship between p53 gene expression and the expression of either bcl-2, bcl-x or bax was observed. No changes in bcl-2, bcl-x and bax gene expression were observed in multidrug-resistant cell lines compared with their drug-sensitive counterparts.
机译:阐明bcl-2和bcl-2相关基因在肺癌发生和治疗反应中的潜在作用的第一步,已经在一组未经治疗和治疗的肺癌细胞系中检查了这些基因的表达。治疗的患者,并在体外选择具有多重耐药性的细胞系。与正常的肺和脑相比,Bcl-2在16个小细胞肺癌(SCLC)细胞系中的15个和5个非小细胞肺癌(NSCLC)细胞系中的两个中高表达,并且高表达与化疗无关。与正常组织相比,Bcl-x在大多数SCLC和NSCLC细胞系中均过表达,并且所有肺肿瘤系均优先表达bcl-x1-mRNA(一种抑制凋亡的剪接变体形式)。与正常的成人组织相比,Bax基因转录本在大多数经检查的SCLC和NSCLC细胞系中均过表达。在大多数细胞系中检测到突变的p53基因表达,并且未观察到p53基因表达与bcl-2,bcl-x或bax表达之间的关系。与多药耐药细胞系相比,在多药耐药细胞系中未观察到bcl-2,bcl-x和bax基因表达的变化。

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