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p53和p21表达与膀胱原位癌患者临床结局的相关性

Association of p53 and p21 expression with clinical outcome in patients with carcinoma in situ of the urinary bladder.

作者信息

Shariat Shahrokh F, Kim JaHong, Raptidis Grigorios, Ayala Gustavo E, Lerner Seth P

机构信息

Scott Department of Urology, Baylor College of Medicine and Methodist Hospital, Houston, Texas, USA.

出版信息

Urology. 2003 Jun;61(6):1140-5. doi: 10.1016/s0090-4295(03)00236-x.

Abstract

OBJECTIVES

To determine whether p53 and p21 expression in bladder carcinoma in situ (CIS) with or without papillary disease can predict disease recurrence, progression, and survival.

METHODS

Immunohistochemical staining for p53 and p21 was carried out on paraffin-embedded tumor specimens from 47 and 39 patients, respectively, who had CIS with or without Ta or T1 disease, but without muscle-invasive cancer. Immunoreactivity was categorized as either positive (reactivity in 10% or more CIS cells) or negative.

RESULTS

Expression of p53 and p21 was positive in 28 (60%) of 47 and 12 (31%) of 39 CIS tumors, respectively. p53 expression was not associated with clinical outcome. Positive p21 expression was associated with bladder cancer recurrence (P = 0.035) and progression (P = 0.033) when adjusted for the effects of clinical stage and grade. The combined p53/p21 expression status was independently associated with disease recurrence (P = 0.022), progression (P = 0.042), and cancer-specific survival (P = 0.031). Patients with p53+/p21+ expression were at significantly greater risk of disease recurrence, progression, and mortality than those having a p53+/p21- or p53-/p21- phenotype (not significantly different from each other statistically).

CONCLUSIONS

In CIS without muscle-invasive disease, positive p21 expression was independently associated with bladder cancer recurrence and progression. Positive expression for both p53 and p21 puts patients with bladder CIS at the greatest risk of bladder cancer recurrence, progression, and, most importantly, mortality, suggesting a potential rationale for early definitive therapy in these patients. On the other hand, an intact pathway at the level of p21 seems to abrogate the detrimental effects of altered p53 immunoreactivity on the outcome of bladder CIS.

摘要

目的

确定伴或不伴乳头状病变的原位膀胱癌(CIS)中p53和p21的表达是否可预测疾病复发、进展及生存情况。

方法

分别对47例和39例患有伴或不伴Ta或T1期疾病的原位癌但无肌层浸润性癌的患者石蜡包埋肿瘤标本进行p53和p21的免疫组化染色。免疫反应性分为阳性(10%或更多CIS细胞有反应性)或阴性。

结果

47例CIS肿瘤中有28例(60%)p53表达阳性,39例中有12例(31%)p21表达阳性。p53表达与临床结局无关。校正临床分期和分级的影响后,p21阳性表达与膀胱癌复发(P = 0.035)和进展(P = 0.033)相关。p53/p21联合表达状态与疾病复发(P = 0.022)、进展(P = 0.042)及癌症特异性生存(P = 0.031)独立相关。p53+/p21+表达的患者比p53+/p21-或p53-/p21-表型的患者有更高的疾病复发、进展及死亡风险(二者在统计学上无显著差异)。

结论

在无肌层浸润性疾病的原位癌中,p21阳性表达与膀胱癌复发和进展独立相关。p53和p21均阳性表达使膀胱原位癌患者有最高的膀胱癌复发、进展风险,最重要的是死亡风险,提示对这些患者进行早期确定性治疗的潜在理论依据。另一方面,p21水平完整的通路似乎可消除p53免疫反应性改变对膀胱原位癌结局的有害影响。

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