Macera M J, Godec C J, Sharma N, Verma R S
Institute of Molecular Biology and Genetics, Brooklyn, NY 11228, USA.
Cancer Genet Cytogenet. 1999 Jan 1;108(1):42-7. doi: 10.1016/s0165-4608(98)00109-5.
Mutation within the TP53 tumor suppressor gene is a frequent occurrence in human cancers, resulting in a poor prognosis, response to therapy, and overall survival time. Mutations have been primarily detected in advanced prostate cancer; however, the involvement of the gene through loss of heterozygosity (LOH) in primary prostate cancers has not been investigated due to lack of identifiable polymorphisms within this gene. Using the nonisotopic RNAse cleavage assay (NIRCA), we screened for point mutations and identified an ApaI restriction site polymorphism located in intron 7 within the TP53 gene. This polymorphism allowed us to detect LOH in informative samples in a population of patients that underwent prostate biopsies and a population that underwent radical prostatectomies. Within the combined study population, 31 of 80 patients (38.75%) were informative for the polymorphism. Loss of heterozygosity was detected in 10 of the 31 samples (32.3%). Point mutations were identified in two samples. The identification of LOH in these patients suggests that the TP53 tumor suppressor gene may play a more active role in prostate cancer than was previously believed.
TP53肿瘤抑制基因的突变在人类癌症中经常发生,导致预后不良、对治疗的反应不佳以及总体生存时间缩短。突变主要在晚期前列腺癌中被检测到;然而,由于该基因内缺乏可识别的多态性,原发性前列腺癌中该基因通过杂合性缺失(LOH)的参与情况尚未得到研究。我们使用非同位素RNA酶切割分析(NIRCA)筛选点突变,并在TP53基因的内含子7中鉴定出一个ApaI限制性位点多态性。这种多态性使我们能够在接受前列腺活检的患者群体和接受根治性前列腺切除术的患者群体中的信息样本中检测LOH。在合并的研究群体中,80名患者中有31名(38.75%)对该多态性具有信息性。在31个样本中的10个(32.3%)检测到杂合性缺失。在两个样本中鉴定出点突变。这些患者中LOH的鉴定表明,TP53肿瘤抑制基因在前列腺癌中可能比以前认为的发挥更积极的作用。
