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通过单克隆抗体多参数流式细胞术评估膀胱肿瘤的临床癌症进展。拉瓦尔大学泌尿外科小组。

Clinical cancer progression in urinary bladder tumors evaluated by multiparameter flow cytometry with monoclonal antibodies. Laval University Urology Group.

作者信息

Fradet Y, Tardif M, Bourget L, Robert J

机构信息

Centre de Recherche en Cancérologie, Université Laval, Hôtel-Dieu de Québec, Canada.

出版信息

Cancer Res. 1990 Jan 15;50(2):432-7.

PMID:2295082
Abstract

Multiparameter flow cytometry studies were performed on clinical samples of human bladder tumors to simultaneously analyse DNA content and the expression of surface glycoproteins defined by monoclonal antibodies T16, Om5, T43, and T138. The results of tests performed on 80 samples of bladder irrigations and tumors from 68 patients were correlated with clinical findings at the time of sampling and with disease outcome prospectively (mean follow-up 2 years). Measuring the level of the panurothelial antigen T16 provided more precision in DNA analysis and served as an internal standard to measure the relative expression of the other cell surface antigens studied. The panel of monoclonal antibodies improved the analytical capacity to study the heterogeneity of antigenic phenotypes within individual samples. Aneuploidy frequently correlated with high stage cancers and with a high rate of clinical cancer progression defined as metastasis or death by cancer. However ploidy was not an entirely reliable prognostic indicator since a significant proportion of Ta and T1 nonprogressing tumors were aneuploid, while in 6/20 cases of cancer progression, the samples were near diploid. Contrary to Om5, T43 and T138 antigens were expressed significantly more often on aneuploid samples, although they appear to provide additional information. T138 was positive on 17/18 samples from patients with high stage cancers of which five were near diploid. It was also positive on 4/5 samples from patients with Ta and T1 tumors in whom disease progressed to metastasis and death. Overall, the expression of T138 antigen was a better single indicator of clinical cancer progression than was ploidy. Further stratification was obtained with combined results of DNA and T138 antigen studies. Within the near diploid group, the incidence of bladder cancer death was 0/26 for T138 negative and 5/13 (38%) for T138-positive patients (P less than 0.01). In the aneuploid group incidence of bladder cancer death was 2/10 (20%) for T138-negative and 12/19 (63%) for T138-positive patients (P less than 0.05). These results suggest that simultaneous flow cytometry measurements of DNA and surface antigens may better assess the prognostic behavior of human bladder tumors.

摘要

对人类膀胱肿瘤的临床样本进行了多参数流式细胞术研究,以同时分析DNA含量以及由单克隆抗体T16、Om5、T43和T138所定义的表面糖蛋白的表达。对68例患者的80份膀胱冲洗液和肿瘤样本进行检测的结果,与采样时的临床发现以及疾病预后进行了前瞻性关联(平均随访2年)。测量泛尿路上皮抗原T16的水平在DNA分析中提供了更高的精确度,并作为测量所研究的其他细胞表面抗原相对表达的内标。单克隆抗体组合提高了研究单个样本中抗原表型异质性的分析能力。非整倍体常与高分期癌症以及高临床癌症进展率相关,后者被定义为转移或癌症死亡。然而,倍性并非完全可靠的预后指标,因为相当一部分Ta和T1期无进展肿瘤为非整倍体,而在6/20例癌症进展病例中,样本接近二倍体。与Om5相反,T43和T138抗原在非整倍体样本上的表达明显更频繁,尽管它们似乎能提供额外信息。T138在17/18例高分期癌症患者的样本上呈阳性,其中5例接近二倍体。它在4/5例Ta和T1期肿瘤患者的样本上也呈阳性,这些患者的疾病进展为转移和死亡。总体而言,T138抗原的表达比倍性更能作为临床癌症进展的单一指标。通过DNA和T138抗原研究的联合结果获得了进一步的分层。在接近二倍体组中,T138阴性患者的膀胱癌死亡率为0/26,T138阳性患者为5/13(38%)(P<0.01)。在非整倍体组中,T138阴性患者的膀胱癌死亡率为2/10(20%),T138阳性患者为12/1

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