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A multi-institutional evaluation of active surveillance for low risk prostate cancer.

机译:对低风险前列腺癌进行积极监测的多机构评估。

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PURPOSE: For select men with low risk prostate cancer active surveillance is more often being considered a management strategy. In a multicenter retrospective study we evaluated the actuarial rates and predictors of remaining on active surveillance, the incidence of cancer progression and the pathological findings of delayed radical prostatectomy. MATERIALS AND METHODS: A cohort of 262 men from 4 institutions met the inclusion criteria of age 75 years or younger, prostate specific antigen 10 ng/ml or less, clinical stage T1-T2a, biopsy Gleason sum 6 or less, 3 or less positive cores at diagnostic biopsy, repeat biopsy before active surveillance and no treatment for 6 months following the repeat biopsy. Active surveillance started on the date of the second biopsy. Actuarial rates of remaining on active surveillance were calculated and univariate Cox regression was used to assess predictors of discontinuing active surveillance. RESULTS: With a median followup of 29 months 43 patients ultimately received active treatment. The 2 and 5-year probabilities of remaining on active surveillance were 91% and 75%, respectively. Patients with cancer on the second biopsy (HR 2.23, 95% CI 1.23-4.06, p = 0.007) and a higher number of cancerous cores from the 2 biopsies combined (p = 0.002) were more likely to undergo treatment. Age, prostate specific antigen, clinical stage, prostate volume and number of total biopsy cores sampled were not predictive of outcome. Skeletal metastases developed in 1 patient 38 months after starting active surveillance. Of the 43 patients undergoing delayed treatment 41 (95%) are without disease progression at a median of 23 months following treatment. CONCLUSIONS: With a median followup of 29 months active surveillance for select patients appears to be safe and associated with a low risk of systemic progression. Cancer at restaging biopsy and a higher total number of cancerous cores are associated with a lower likelihood of remaining on active surveillance. A restaging biopsy should be strongly considered to finalize eligibility for active surveillance.
机译:目的:对于低危前列腺癌的精选男性,主动监测通常被认为是一种管理策略。在一项多中心回顾性研究中,我们评估了主动监测时的精算率和预测指标,癌症进展的发生率以及延迟根治性前列腺切除术的病理学发现。材料与方法:来自4个机构的262名男性患者符合纳入标准,年龄为75岁以下,前列腺特异抗原为10 ng / ml或以下,临床分期T1-T2a,活检格里森总和为6或以下,3或以下为阳性诊断活检的核心,在主动监测之前重复活检,重复活检后6个月未进行任何治疗。在第二次活检之日开始主动监测。计算主动监测剩余的精算率,并使用单变量Cox回归评估停止主动监测的预测因子。结果:中位随访29个月,最终有43例患者接受了积极治疗。保持主动监视的2年和5年概率分别为91%和75%。在第二次活检中患有癌症的患者(HR 2.23,95%CI 1.23-4.06,p = 0.007),并且两次活检中合并有更多癌芯的患者(p = 0.002)更可能接受治疗。年龄,前列腺特异抗原,临床分期,前列腺体积和取样的总活检芯数不能预测结果。开始主动监测后38个月,有1位患者发生了骨骼转移。在接受延迟治疗的43位患者中,有41位(95%)在治疗后的23个月中位无疾病进展。结论:中位随访29个月,对某些患者进行主动监护似乎是安全的,而且全身进展风险较低。重新进行活检时的癌症和更多的癌核心总数与保持主动监测的可能性降低有关。应强烈考虑进行再分期活检,以最终确定主动监测的资格。

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