Aveyard J S, Skilleter A, Habuchi T, Knowles M A
ICRF Cancer Medicine Research Unit, St James's University Hospital, Leeds, UK.
Br J Cancer. 1999 May;80(5-6):904-8. doi: 10.1038/sj.bjc.6690439.
The tumour suppressor gene PTEN/MMAC1, which is mutated or homozygously deleted in glioma, breast and prostate cancer, is mapped to a region of 10q which shows loss of heterozygosity (LOH) in bladder cancer. We screened 123 bladder tumours for LOH in the region of PTEN. In 53 informative muscle invasive tumours (> or = pT2), allele loss was detected in 13 (24.5%) and allelic imbalance in four tumours (overall frequency 32%). LOH was found in four of 60 (6.6%) informative, non-invasive tumours (pTa/pT1). We screened 63 muscle invasive tumours for PTEN mutations by single-strand conformation polymorphism (SSCP) analysis and for homozygous deletion by duplex quantitative polymerase chain reaction (PCR). Two homozygous deletions were identified but no mutations. Of 15 bladder tumour cell lines analysed, three showed homozygous deletion of all or part of the PTEN gene, but none had mutations detectable by SSCP analysis. Our results indicate that PTEN is involved in the development of some bladder tumours. The low frequency of mutation of the retained allele in tumours with 10q23 LOH suggests that there may be another predominant mechanism of inactivation of the second allele, for example small intragenic deletions, that hemizygosity may be sufficient for phenotypic effect, or that there is another target gene at 10q23.
肿瘤抑制基因PTEN/MMAC1在胶质瘤、乳腺癌和前列腺癌中发生突变或纯合缺失,该基因定位于10q区域,而此区域在膀胱癌中显示杂合性缺失(LOH)。我们对123例膀胱肿瘤进行了PTEN区域的LOH筛查。在53例信息充分的肌层浸润性肿瘤(≥pT2)中,13例(24.5%)检测到等位基因缺失,4例肿瘤存在等位基因失衡(总频率32%)。在60例信息充分的非浸润性肿瘤(pTa/pT1)中有4例(6.6%)发现LOH。我们通过单链构象多态性(SSCP)分析对63例肌层浸润性肿瘤进行PTEN突变筛查,并通过双重定量聚合酶链反应(PCR)检测纯合缺失。鉴定出2例纯合缺失,但未发现突变。在分析的15株膀胱肿瘤细胞系中,3株显示PTEN基因全部或部分纯合缺失,但通过SSCP分析均未检测到突变。我们的结果表明,PTEN参与了某些膀胱肿瘤的发生发展。在10q23 LOH的肿瘤中保留等位基因突变频率较低,这表明可能存在另一种使第二个等位基因失活的主要机制,例如小的基因内缺失,半合子状态可能足以产生表型效应,或者在10q23存在另一个靶基因。
