首页> 外文期刊>Urology >Blinded evaluation of reverse transcriptase-polymerase chain reaction prostate-specific antigen peripheral blood assay for molecular staging of prostate cancer.
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Blinded evaluation of reverse transcriptase-polymerase chain reaction prostate-specific antigen peripheral blood assay for molecular staging of prostate cancer.

机译:前列腺癌分子分期的逆转录酶-聚合酶链反应前列腺特异性抗原外周血分析的盲法评估。

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OBJECTIVES: The reverse transcriptase-polymerase chain reaction (RT-PCR)-prostate-specific antigen (PSA) assay to detect presumed occult micrometastatic prostate cancer has been controversial, and this molecular staging has been thought to be clinically useful by some groups but not others. METHODS: We used a sensitive nested RT-PCR assay with specific primers derived from the PSA sequence and a very stringent two-step PCR protocol with denaturing temperature of 94 degrees C annealing and extension temperature of 68 degrees C. This method enabled us to detect PSA-expressing LNCaP prostate cancer (PC) cells as low as one cell of 10 million lymphocytes (1/10(7)). Ninety-six patients with PC were studied, including 85 before radical prostatectomy (RP), and 22 controls, including healthy men and women and men with benign prostatic hyperplasia. RESULTS: In 85 patients undergoing RP, a minimum of two independent RT-PCR-PSA assays detected circulating prostate cells preoperatively in 27 patients (31.8%). Of 12 patients with locally advanced or advanced stage cancer, RT-PCR-PSA was positive in 5 (41.7%); of the 22 controls, no patient was RT-PCR-PSA positive. In 10 randomly selected cases, the RT-PCR product was confirmed as PSA by DNA sequencing. Of the 27 patients undergoing RP who were RT-PCR positive, 11 (40.7%) had non-organ-confined disease (pT3a or greater), and of the 58 patients who were RT-PCR negative, 32 (55.2%) had non-organ-confined disease. Patients with RT-PCR positive results also had lower margin positivity (9 of 27, 33.3%) than did patients with RT-PCR negative results (21 of 58, 36.2%). Finally, at a mean follow-up of 25.7 months, 5 (18.5%) of 27 RT-PCR positive patients had recurrence (PSA) compared with 14 (24.1%) of 58 RT-PCR negative patients. CONCLUSIONS: On the basis of this blinded study, RT-PCR for PSA-expressing cells in 85 patients before RP is not related to clinical stage, age, race, grade, Gleason sum, serum PSA or prostatic acid phosphatase, tumor volume, or tumor multifocality. RT-PCR positivity did not predict pathologic stage or early PSA recurrence. A standardized RT-PCR assay needs to be developed to account for interlaboratory discrepancies.
机译:目的:逆转录酶-聚合酶链反应(RT-PCR)-前列腺特异性抗原(PSA)测定法可用于检测隐匿性微转移性前列腺癌,一直存在争议,某些小组认为这种分子分期在临床上有用,但并非如此其他。方法:我们使用灵敏的巢式RT-PCR分析方法,并使用源自PSA序列的特异性引物和非常严格的两步PCR方案,变性温度为94℃退火,延伸温度为68℃。这种方法使我们能够检测表达PSA的LNCaP前列腺癌(PC)细胞低至一千万个淋巴细胞中的一细胞(1/10(7))。对96例PC患者进行了研究,其中包括85例行根治性前列腺切除术(RP)之前的患者和22例对照,包括健康的男性和女性以及前列腺增生的男性。结果:在进行RP的85例患者中,至少有两次独立的RT-PCR-PSA分析在27例患者中术前检测到了循环中的前列腺细胞(31.8%)。在12例局部晚期或晚期癌症患者中,RT-PCR-PSA阳性5例(41.7%);在22位对照中,没有患者是RT-PCR-PSA阳性的。在10个随机选择的病例中,通过DNA测序将RT-PCR产物确认为PSA。在接受RT-PCR阳性的RP的27例患者中,有11例(40.7%)患有非器官受限疾病(pT3a或更高),而在进行RT-PCR阴性的58例患者中,有32例(55.2%)未患有-器官受限疾病。与RT-PCR阴性结果的患者(21的58,36.2%)相比,RT-PCR阳性结果的患者的边缘阳性(27的9,33.3%)低。最后,在平均随访25.7个月时,27例RT-PCR阳性患者中有5例(18.5%)复发(PSA),而58例RT-PCR阴性患者中有14例(24.1%)。结论:在这项盲研究的基础上,RP前85名患者的PSA表达细胞的RT-PCR与临床阶段,年龄,种族,等级,格里森总和,血清PSA或前列腺酸磷酸酶,肿瘤体积或肿瘤多灶性。 RT-PCR阳性不能预测病理阶段或PSA早期复发。需要开发标准化的RT-PCR分析法以解决实验室间的差异。

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