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来自171个代表肺癌、肺外小细胞癌和间皮瘤的细胞系的RB蛋白状态与临床相关性。

RB protein status and clinical correlation from 171 cell lines representing lung cancer, extrapulmonary small cell carcinoma, and mesothelioma.

作者信息

Shimizu E, Coxon A, Otterson G A, Steinberg S M, Kratzke R A, Kim Y W, Fedorko J, Oie H, Johnson B E, Mulshine J L

机构信息

National Cancer Institute-Navy Oncology Branch, National Cancer Institute, Bethesda, Maryland 20889.

出版信息

Oncogene. 1994 Sep;9(9):2441-8.

PMID:8058306
Abstract

We have studied RB protein expression in 171 cell lines derived from patients with small cell lung cancer (SCLC), non-small cell lung cancer (NSCLC), pulmonary carcinoid, mesothelioma, and extrapulmonary small cell cancer (EPSC) and have correlated this data with clinical outcome. We detected absent or aberrant RB protein expression in 66/75 SCLC, 12/80 NSCLC, 1/6 carcinoid, 0/5 mesothelioma, and 4/5 EPSC samples. In addition, we observed integration of human papilloma virus (HPV) DNA in the single EPSC cell line that retained wildtype RB protein. We did not detect integration of HPV, SV40 or adenoviral DNA in other tumor samples with wildtype RB status. We also noted a stable, hypophosphorylated mutant RB in 12 SCLC and 3 NSCLC samples which might have been falsely interpreted as wildtype by current immunohistochemical techniques. Analysis of the matched clinical data showed no associations between RB status and age, sex, extent of disease, performance status, smoking history, and previous treatment. In addition, retrospective analyses showed no consistent correlation of RB protein expression with either best clinical response, overall survival, or in vitro chemotherapeutic drug sensitivity. The stable expression of RB after gene transfection into RB(-) SCLC cells, however, resulted in a trend toward increased in vitro resistance to etoposide, cisplatin and doxorubicin.

摘要

我们研究了171株来源于小细胞肺癌(SCLC)、非小细胞肺癌(NSCLC)、肺类癌、间皮瘤和肺外小细胞癌(EPSC)患者的细胞系中的RB蛋白表达情况,并将这些数据与临床结果进行了关联分析。我们在66/75例SCLC、12/80例NSCLC、1/6例类癌、0/5例间皮瘤和4/5例EPSC样本中检测到RB蛋白表达缺失或异常。此外,我们在保留野生型RB蛋白的单一EPSC细胞系中观察到了人乳头瘤病毒(HPV)DNA的整合。在其他具有野生型RB状态的肿瘤样本中,我们未检测到HPV、SV40或腺病毒DNA的整合。我们还在12例SCLC和3例NSCLC样本中发现了一种稳定的、低磷酸化的突变型RB,目前的免疫组织化学技术可能会将其错误地解释为野生型。对匹配的临床数据进行分析后发现,RB状态与年龄、性别、疾病范围、体能状态、吸烟史及既往治疗之间无关联。此外,回顾性分析表明,RB蛋白表达与最佳临床反应、总生存期或体外化疗药物敏感性之间均无一致的相关性。然而,将基因转染至RB(-)SCLC细胞后RB的稳定表达导致对依托泊苷、顺铂和阿霉素的体外耐药性有增加的趋势。

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