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在CAS-200图像分析系统上获取的定量细胞核形态测量学、马尔可夫纹理描述符和DNA含量,结合PCNA和HER-2/neu免疫组织化学用于预测前列腺癌进展。

Quantitative nuclear morphometry, Markovian texture descriptors, and DNA content captured on a CAS-200 Image analysis system, combined with PCNA and HER-2/neu immunohistochemistry for prediction of prostate cancer progression.

作者信息

Veltri R W, Partin A W, Epstein J E, Marley G M, Miller C M, Singer D S, Patton K P, Criley S R, Coffey D S

机构信息

CytoDiagnostics, Inc., Oklahoma City, OK 73112.

出版信息

J Cell Biochem Suppl. 1994;19:249-58.

PMID:7529856
Abstract

One hundred and twenty-four localized prostate cancer patients operated on at Johns Hopkins Hospital (JHH) since 1975 were identified. The sample was optimized for evaluation of prostate cancer progression. Based upon accurate clinical histories, these radical prostatectomy patients included 50 progressors and 74 non-progressors using appearance of serum PSA as an indication of recurrence (mean follow-up = 8.6 +/- 1.8 years, range 7-15 years). All patients included in the study had no involvement of their seminal vesicles or lymph nodes at the time of prostatectomy. Average time to progression was 3.6 +/- 2 years, range of 1-8 years. Using paraffin-embedded specimens, several five micron sections were cut and placed on Probe-On slides; one slide was H&E-stained and the other was Feulgen-stained. The H&E and Feulgen-stained slides were screened and "dotted" by pathologists at JHH and CytoDynostics, Inc. A CAS-200 Image analysis system (Cell Image Systems, Elmhurst, IL) equipped with a Cell Measurement Program version 1.2 beta, was used to capture the Feulgen-stained images and to perform the calculations. From the "dotted" areas, 150 cancer cells were selected for measurement of DNA content and 27 nuclear morphometric shape and size factors, including 21 Markovian chromatin texture variables. Additional sections were used for immunochemistry staining with an alkaline phosphatase streptavidin-biotin complex stain to detect and quantitate cancer cells binding monoclonal antibodies directed against proliferating cell nuclear antigen (PCNA) and HER-2/neu antigen. All data were entered into a statistical program (STATA) for further analysis and univariate and multivariate statistical analysis was performed using logistic regression and its stepwise variant. The biomarkers of greatest utility to detect progressors when analyzed univariately included post-operative Gleason score (p = < 0.0001), HER-2/neu antigenicity (p = 0.0147), CAS-200 DNA ploidy (p = 0.008), and twelve Markovian nuclear texture and shape features (p = < 0.0001), whereas PCNA (p = 0.160) failed. The optimal set of nuclear morphometry progression tumor features were selected using backward stepwise logistic regression estimate analysis which drops variables due to collinearity. Although post-operative Gleason score is a strong univariate predictor of progression, DNA ploidy and HER-2/neu contributed significantly to further stratification of higher risk groups within the low Gleason score subpopulation. The best Markovian features combined with post-operative Gleason score generated sensitivity = 90%, specificity = 96%, positive predictive value = 94%, negative predictive value = 93% and the area under the receiver operator curve was 0.975.

摘要

自1975年以来,在约翰·霍普金斯医院(JHH)接受手术的124例局限性前列腺癌患者被纳入研究。该样本针对前列腺癌进展评估进行了优化。基于准确的临床病史,这些接受根治性前列腺切除术的患者中,以血清PSA出现作为复发指标,有50例病情进展者和74例无进展者(平均随访时间 = 8.6±1.8年,范围7 - 15年)。所有纳入研究的患者在前列腺切除时精囊和淋巴结均未受累。平均进展时间为3.6±2年,范围为1 - 8年。使用石蜡包埋标本,切取数张5微米厚的切片并置于Probe-On载玻片上;一张载玻片进行苏木精 - 伊红(H&E)染色,另一张进行福尔根(Feulgen)染色。JHH和CytoDynostics公司的病理学家对H&E染色和福尔根染色的载玻片进行筛选并“打点标记”。使用配备Cell Measurement Program version 1.2 beta的CAS - 200图像分析系统(Cell Image Systems,伊利诺伊州埃尔姆赫斯特)来采集福尔根染色图像并进行计算。从“打点标记”区域中,选择150个癌细胞用于测量DNA含量以及27个核形态计量形状和大小因子,包括21个马尔可夫染色质纹理变量。额外的切片用于免疫化学染色,采用碱性磷酸酶链霉亲和素 - 生物素复合物染色法,以检测和定量癌细胞与针对增殖细胞核抗原(PCNA)和HER - 2/neu抗原的单克隆抗体的结合情况。所有数据输入统计程序(STATA)进行进一步分析,并使用逻辑回归及其逐步变体进行单变量和多变量统计分析。单变量分析时,对检测病情进展者最有用的生物标志物包括术后Gleason评分(p = < 0.0001)、HER - 2/neu抗原性(p = 0.0147)、CAS - 200 DNA倍体性(p = 0.008)以及12个马尔可夫核纹理和形状特征(p = < 0.0001),而PCNA(p = 0.160)未显示相关性。使用向后逐步逻辑回归估计分析选择最佳的核形态计量进展肿瘤特征集,该分析会因共线性而剔除变量。尽管术后Gleason评分是进展的强有力单变量预测指标,但DNA倍体性和HER - 2/neu对低Gleason评分亚组中高风险组的进一步分层有显著贡献。最佳的马尔可夫特征与术后Gleason评分相结合,产生的敏感性 = 90%,特异性 = 96%,阳性预测值 = 94%,阴性预测值 = 93%,受试者工作特征曲线下面积为0.975。

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