首页> 美国卫生研究院文献>Cancer Science >p53 Mutations in Prostatic Intraepithelial Neoplasia and Concurrent Carcinoma: Analysis of Laser Capture Microdissected Specimens from Non‐transition and Transition Zones
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p53 Mutations in Prostatic Intraepithelial Neoplasia and Concurrent Carcinoma: Analysis of Laser Capture Microdissected Specimens from Non‐transition and Transition Zones

机译:前列腺上皮内瘤变和并发癌中的p53突变:来自非过渡区和过渡区的激光捕获显微解剖标本分析

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摘要

Prostatic intraepithelial neoplasia (PIN) is characterized by intraluminal proliferation of epithelial cells and is divided into high‐grade (HGPIN) and low‐grade (LGPIN) lesions. HGPIN is regarded as the most likely precursor of prostatic cancer (PCA). Microdissected DNA selectively extracted from paraffin‐embedded sections of 27 cases with PCA were analyzed for p53 mutation in exons 5–8 by single‐strand conformation polymorphism of polymerase chain reaction‐amplified DNA fragments (PCR‐SSCP) followed by direct sequencing. These patients received total prostatectomy (27 cases). After a review of histologic sections, DNA was extracted from 193 locations; 111 lesions from 27 cases with HGPIN (75 lesions from non‐transition zone and 36 from transition zone), 55 lesions from 27 cases with PCA (30 lesions from non‐transition zone and 25 from transition zone), and 27 from 27 benign glands. Analysis revealed 27 mutations of the p53 gene in 24 lesions from 12 cases. Benign glands adjoining PIN and/or PCA had no mutations. All mutations were point mutations: 17 missense, 7 silent, and 2 nonsense. Mutations were detected in 6 cases (22.2%) or 13 of 111 lesions (11.7%) with HGPIN and 8 cases (29.6%) or 11 of 55 lesions (20.0%) with PCA. In a given case, HGPIN and PCA lesions had different p53 mutations from each other, suggesting multiclonal development of prostatic precancerous lesions. The frequency of p53 mutation of PCA was significantly higher in the non‐transition zone (33.3%) than in the transition zone (4%), and higher in the stage T3 cases (30.3%) than in the stage T2 cases (4.5%, 1 of 22 lesions) (both P < 0.05). Frequency of p53 mutation of PIN in the non‐transition zone (14.7%) was higher than that in the transition zone (5.6%), although the difference was not significant. The frequency rate of p53 mutation in HGPIN close to PCA (≤2 mm) was significantly higher (24%) than that in HGPIN lesions > 2 mm from PCA (3%). All these findings indicate that the p53 gene mutations are involved in prostatic carcinogenesis and explain why the non‐transition zone is the predominant site of PCA.
机译:前列腺上皮内瘤变(PIN)的特征是上皮细胞腔内增生,分为高级别(HGPIN)和低级别(LGPIN)病变。 HGPIN被认为是最可能的前列腺癌(PCA)的前体。通过聚合酶链反应扩增的DNA片段的单链构象多态性(PCR-SSCP),然后直接测序,从27例PCA的石蜡包埋切片中选择性提取的显微切割DNA进行了外显子5-8中p53突变的分析。这些患者接受了全前列腺切除术(27例)。经过组织切片检查后,从193个位置提取了DNA。 HGPIN的27例中有111处病变(非过渡区为75处病变,过渡区为36处),PCA的27例患者为55处病变(非过渡区为30处病变,过渡区为25处),27例良性腺为27 。分析显示在12例患者的24个病变中有27个p53基因突变。与PIN和/或PCA相邻的良性腺无突变。所有突变均为点突变:17个错义,7个沉默和2个废话。 HGPIN的6例(22.2%)或111个病灶中的13个(11.7%)和PCA的8例(29.6%)或55个病灶中的11个(20.0%)检测到突变。在给定的情况下,HGPIN和PCA病变的p53突变彼此不同,表明前列腺癌前病变的多克隆发展。非过渡区PCA p53突变的频率(33.3%)显着高于过渡区(4%),T3期病例(30.3%)高于T2期病例(4.5%) ,共22个病变中的1个)(均P <0.05)。非过渡区PIN的p53突变频率(14.7%)高于过渡区(5.6%),尽管差异不显着。 HGPIN接近PCA(≤2 mm)的p53突变发生率显着高于(24%),高于距PCA> 2 mm的HGPIN病变(3%)。所有这些发现表明,p53基因突变与前列腺癌发生有关,并解释了为什么非过渡区是PCA的主要位点。

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