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PTEN 缺失与早期膀胱癌的疾病进展和不良预后相关。

PTEN deletions are related to disease progression and unfavourable prognosis in early bladder cancer.

机构信息

Institute of Pathology, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.

出版信息

Histopathology. 2013 Nov;63(5):670-7. doi: 10.1111/his.12209. Epub 2013 Sep 5.

Abstract

AIMS

This study aimed to determine the prevalence and clinical significance of deletions of the tumour suppressor gene PTEN in bladder cancer.

METHODS AND RESULTS

A tissue microarray with 686 bladder cancers was analysed for PTEN deletions by fluorescence in-situ hybridization. PTEN mutations were analysed in nine tumours with heterozygous PTEN deletion. Heterozygous PTEN deletions were present in 16.5% of tumours and were associated with grade (P = 0.0024) and p53 status (P = 0.0141), but not linked to stage (P = 0.0965). PTEN deletions were seen in 5.8% of pTaG1, 10.9% of pTaG2, 29.0% of pTaG3, 16.7% of pT1G2, 22.2% of pT1G3, 17.7% of pT2-4G2 and 20.9% of pT2-4G3 tumours (P = 0.0235). PTEN deletions were associated significantly with recurrences in pTa tumours (P = 0.0173), progression in pT1 tumours (P = 0.0016), but not with overall or cancer-specific survival in pT2 tumours. Multivariate analyses including grade and PTEN deletions revealed that PTEN deletions but not grade were associated independently with recurrence in pTa tumours (P = 0.0377) and progression in pT1 tumours (P = 0.0030). No inactivating PTEN mutations were found.

CONCLUSIONS

PTEN is linked to aggressive tumour phenotype and to unfavourable outcome in early bladder cancer. Heterozygous PTEN loss, i.e. reduced PTEN gene dosage, might be sufficient to cause aggressive tumour behaviour in bladder cancer cells.

摘要

目的

本研究旨在确定抑癌基因 PTEN 缺失在膀胱癌中的发生率和临床意义。

方法和结果

采用荧光原位杂交技术分析了 686 例膀胱癌组织微阵列中 PTEN 缺失情况。对 9 例杂合性 PTEN 缺失肿瘤进行了 PTEN 突变分析。肿瘤存在杂合性 PTEN 缺失的比例为 16.5%,与分级(P = 0.0024)和 p53 状态(P = 0.0141)相关,但与分期无关(P = 0.0965)。PTEN 缺失见于 5.8%的 pTaG1、10.9%的 pTaG2、29.0%的 pTaG3、16.7%的 pT1G2、22.2%的 pT1G3、17.7%的 pT2-4G2 和 20.9%的 pT2-4G3 肿瘤(P = 0.0235)。PTEN 缺失与 pTa 肿瘤的复发显著相关(P = 0.0173),与 pT1 肿瘤的进展显著相关(P = 0.0016),但与 pT2 肿瘤的总生存或肿瘤特异性生存无关。包括分级和 PTEN 缺失在内的多变量分析显示,PTEN 缺失而不是分级与 pTa 肿瘤的复发(P = 0.0377)和 pT1 肿瘤的进展(P = 0.0030)独立相关。未发现失活的 PTEN 突变。

结论

PTEN 与膀胱癌侵袭性表型和不良预后相关。杂合性 PTEN 缺失(即 PTEN 基因剂量减少)可能足以导致膀胱癌细胞的侵袭性行为。

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