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首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >Pro-prostate-specific antigen measurements in serum and tissue are associated with treatment necessity among men enrolled in expectant management for prostate cancer.
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Pro-prostate-specific antigen measurements in serum and tissue are associated with treatment necessity among men enrolled in expectant management for prostate cancer.

机译:血清和组织中前列腺特异性抗原的测量与参加前列腺癌预期治疗的男性的治疗必要性相关。

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摘要

PURPOSE: We assessed the association of quantitative clinical and pathologic information, including serum and tissue pro-prostate-specific antigen (proPSA) measurements, with outcomes among men with prostate cancer in an expectant management (active surveillance) program. EXPERIMENTAL DESIGN: We identified 71 men enrolled in expectant management with frozen serum and tissue available from diagnosis: 39 subsequently developed unfavorable biopsies (Gleason score > or =7, > or =3 cores positive for cancer, >50% of any core involved with cancer), whereas 32 maintained favorable biopsies (median follow-up, 3.93 years). Serum total PSA, free PSA (fPSA), and [-2]proPSA were measured by the Beckman Coulter immunoassay. [-5/-7]proPSA was evaluated in cancer and benign-adjacent areas (BAA) by quantitative immunohistochemistry. Cox proportional hazards and Kaplan-Meier analyses were used to identify significant associations with unfavorable biopsy conversion. RESULTS: The ratio [-2]proPSA/% fPSA in serum was significantly higher at diagnosis (0.87 +/- 0.44 versus 0.65 +/- 0.36 pg/mL; P = 0.02) in men developing unfavorable biopsies. [-5/-7]proPSA tissue staining was more intense (4104.09 +/- 3033.50 versus 2418.06 +/- 1606.04; P = 0.03) and comprised a greater fractional area (11.58 +/- 7.08% versus 6.88 +/- 5.20%; P = 0.01) in BAA of these men. Serum [-2]proPSA/% fPSA [hazard ratio, 2.53 (1.18-5.41); P = 0.02], BAA [-5/-7]proPSA % area [hazard ratio, 1.06 (1.01-1.12); P = 0.02] and BAA [-5/-7]proPSA stain intensity [hazard ratio, 1.000213 (1.000071-1.000354); P = 0.003] were significantly associated with unfavorable biopsy in Kaplan-Meier and Cox analyses. Serum [-2]proPSA/% fPSA significantly correlated with BAA [-5/-7]proPSA % area (rho = 0.40; P = 0.002) and BAA [-5/-7]proPSA stain intensity (rho = 0.33; P = 0.016). CONCLUSIONS: In a prospective cohort of men enrolled into expectant management for prostate cancer, serum and tissue levels of proPSA at diagnosis are associated with need for subsequent treatment. The increase in serum proPSA/% fPSA might be driven by increased proPSA production from "premalignant" cells in the prostate BAA.
机译:目的:我们评估了定量临床和病理学信息(包括血清和组织前列腺特异性抗原(proPSA)的测量结果)与预期管理(积极监测)计划中前列腺癌男性的结局。实验设计:我们确定了71名接受诊断的男性,他们的冷冻血清和组织可从诊断中入选:39名随后发展为不利的活检组织(格里森评分>或= 7,>或= 3癌阳性,> 50%涉及的核心癌症),其中32例活检良好(中位随访时间为3.93年)。通过贝克曼库尔特免疫测定法测量血清总PSA,游离PSA(fPSA)和[-2] proPSA。 [-5 / -7] proPSA在癌症和良性邻近区域(BAA)中通过定量免疫组织化学评估。使用Cox比例风险和Kaplan-Meier分析来确定不良活检转换之间的显着相关性。结果:患有不良活检的男性在诊断时血清中的[-2] proPSA /%fPSA比率显着更高(0.87 +/- 0.44比0.65 +/- 0.36 pg / mL; P = 0.02)。 [-5 / -7] proPSA组织染色更强(4104.09 +/- 3033.50对2418.06 +/- 1606.04; P = 0.03),并且包含更大的分数区域(11.58 +/- 7.08%对6.88 +/- 5.20% ; P = 0.01)。血清[-2] proPSA /%fPSA [危险比,2.53(1.18-5.41); P = 0.02],BAA [-5 / -7] proPSA%面积[危险比,1.06(1.01-1.12); P = 0.02]和BAA [-5 / -7] proPSA染色强度[危险比,1.000213(1.000071-1.000354); P = 0.003]与Kaplan-Meier和Cox分析中的不良活检显着相关。血清[-2] proPSA /%fPSA与BAA [-5 / -7] proPSA%面积显着相关(rho = 0.40; P = 0.002)和BAA [-5 / -7] proPSA染色强度(rho = 0.33; P = 0.016)。结论:在预期参加前列腺癌治疗的一组预期人群中,诊断时proPSA的血清和组织水平与后续治疗的需要有关。血清proPSA /%fPSA的增加可能是由前列腺BAA中“癌变前”细胞产生的proPSA增加所驱动的。

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