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p53免疫阳性与乳腺癌肿瘤增殖及其他预后指标的相关性

The association of p53 immunopositivity with tumor proliferation and other prognostic indicators in breast cancer.

作者信息

Bhargava V, Thor A, Deng G, Ljung B M, Moore D H, Waldman F, Benz C, Goodson W, Mayall B, Chew K

机构信息

Department of Pathology, University of California, San Francisco.

出版信息

Mod Pathol. 1994 Apr;7(3):361-8.

PMID:8058709
Abstract

Abnormal accumulation of the p53 tumor suppressor gene product was analyzed in 198 primary invasive human breast carcinomas. In 47 of these cases, single-strand conformational polymorphism was used to detect mutations in the highly conserved exons 5-9 of the gene. Mutations as determined by single-strand conformational polymorphism were found in 15 of 15 strongly immunopositive cases (100%) and 3 of 23 immunonegative cases (13%). There were also nine cases with < 1% immunopositive cells (borderline immunopositivity); p53 mutations were detected in seven of these cases. The results suggest that p53 immunopositivity is a highly specific, albeit somewhat insensitive surrogate for p53 mutations. p53 accumulation, detected by immunohistochemical methods using antibody PAb 1801, was noted in 29.8% of the cases and was associated with estrogen receptor (ER) negativity (P = 0.0003), progesterone receptor (PR) negativity (P = 0.008), and high histological grade (P = 0.037) by univariate analysis. Incorporation of bromodeoxyuridine was used to determine the percentage of cells synthesizing DNA (proliferative fraction). When bromodeoxyuridine was administered either in vivo (n = 93) or in vitro (n = 79), p53 accumulation was only marginally related to proliferative fraction (P = 0.067 by chi 2; P = 0.055 by Mann-Whitney). When tumors were segregated by ER status, the aforementioned associations of p53 immunopositivity with PR negativity, high histological grade, and increased proliferation rate lost their significance. p53 accumulation did not correlate with tumor size, clinical stage, axillary node metastases, or age at diagnosis.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在198例原发性浸润性人类乳腺癌中分析了p53肿瘤抑制基因产物的异常积聚情况。在其中47例病例中,采用单链构象多态性检测该基因高度保守的外显子5 - 9中的突变。通过单链构象多态性确定的突变在15例强免疫阳性病例中的15例(100%)以及23例免疫阴性病例中的3例(13%)被发现。还有9例免疫阳性细胞<1%(临界免疫阳性)的病例;其中7例检测到p53突变。结果表明,p53免疫阳性是p53突变的一种高度特异性但有点不敏感的替代指标。使用抗体PAb 1801通过免疫组化方法检测到p53积聚在29.8%的病例中存在,并且通过单因素分析与雌激素受体(ER)阴性(P = 0.0003)、孕激素受体(PR)阴性(P = 0.008)以及高组织学分级(P = 0.037)相关。采用溴脱氧尿苷掺入法确定合成DNA的细胞百分比(增殖分数)。当在体内(n = 93)或体外(n = 79)给予溴脱氧尿苷时,p53积聚与增殖分数仅存在微弱关联(卡方检验P = 0.067;曼 - 惠特尼检验P = 0.055)。当根据ER状态对肿瘤进行分类时,上述p53免疫阳性与PR阴性、高组织学分级以及增殖率增加之间的关联失去了意义。p53积聚与肿瘤大小、临床分期、腋窝淋巴结转移或诊断时的年龄无关。(摘要截断于250字)

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