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p53 immunohistochemistry in transitional cell carcinoma and dysplasia of the urinary bladder correlates with disease progression

机译:移行细胞癌和膀胱发育不良中的p53免疫组化与疾病进展相关

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Immunohistochemically detectable p53 protein using a polyclonal antibody (CM-1) was studied in 42 carcinomas of which 11 were grade I, 22 grade II and nine grade III carcinomas. Additionally 14 urothelial dysplasias were studied. In 11 of these a diagnosis of transitional cell carcinoma was established before and in one after the dysplasia diagnosis. Twenty-one out of 42 (50%) cases of transitional cell carcinoma were positive for the p53 protein. Eleven out of 14 (78%) dysplasias and 10/12 (83%) related carcinomas were p53 positive. One out of 11 grade I (9%), 12/22 grade II (55%) and 8/9 grade III (89%) tumours showed positivity for p53. There were significantly more p53 positive cases in grade II-III tumours than in grade I tumours (P = 0.004). There were significantly more p53 positive cases in stage T2-T4 tumours than in stage T1 tumours (P = 0.035). In only one case among the 11 dysplastic lesions following the treatment of a carcinoma the dysplastic lesion was p53 negative while the preceding carcinoma was p53 positive. All dysplasias and 28 carcinomas were also immunostained for laminin and type IV collagen to evaluate the continuity of basement membranes (BMs). Clearly disrupted BMs were observed only in grade III carcinomas. These cases showed the most p53 immunopositivity. The results show a strong association of p53 staining between dysplasias and transitional cell carcinomas of the urinary bladder indicating that these lesions might share similar p53 changes. The correlation to grade, clinical stage and to disrupted BM suggests that p53 mutations may be associated with the evolution of aggressive growth characteristics in transitional cell carcinomas or, alternatively, that p53 positive tumours of a more aggressive type from the start. Whether p53 staining can be used as an adjunct in the assessment and follow-up of epithelial changes of patients treated for a p53 positive bladder carcinoma deserves to be studied.
机译:在42例癌症中研究了使用多克隆抗体(CM-1)进行免疫组织化学检测的p53蛋白,其中11例为I级,22例II级和9例III级癌。另外研究了14例尿路上皮发育不良。在其中的11例中,在异型增生诊断之前和之后均确定了对移行细胞癌的诊断。 42例(50%)移行细胞癌中有21例p53蛋白阳性。 14例(78%)发育不良和10/12(83%)相关癌中有11例是p53阳性。在11个I级肿瘤中(9%),12/22 II级肿瘤(55%)和8/9 III级肿瘤(89%)中有1个显示p53阳性。 II-III级肿瘤中的p53阳性病例明显多于I级肿瘤(P = 0.004)。在T2-T4期肿瘤中,p53阳性病例明显多于T1期肿瘤(P = 0.035)。在癌症治疗后的11例增生性病变中,只有1例增生性病变为p53阴性,而先前的癌为p53阳性。所有不典型增生和28个癌也进行了层粘连蛋白和IV型胶原蛋白的免疫染色,以评估基底膜(BMs)的连续性。仅在III级癌中观察到明显破坏的BM。这些病例显示出最大的p53免疫阳性。结果显示,异型增生与膀胱移行细胞癌之间的p53染色密切相关,表明这些病变可能共享相似的p53变化。与等级,临床阶段和破坏的BM的相关性表明,p53突变可能与移行细胞癌中侵袭性生长特征的演变有关,或者从一开始就具有更具侵略性的p53阳性肿瘤。 p53染色是否可以作为评估p53阳性膀胱癌患者的上皮变化的辅助手段和随访手段,值得研究。

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