扩展核心取样与主动监测患者延迟干预和病理结果的关系：基于人群的分析。

IF 1.9 4区医学 Q3 UROLOGY & NEPHROLOGY

Cuaj-Canadian Urological Association Journal Pub Date : 2024-05-01 DOI:10.5489/cuaj.8563

Rashid K Sayyid, Rui Bernardino, Zizo Al-Daqqaq, Raj Tiwari, Majed Al-Rumayyan, Tiiu Sildva, Jessica G Cockburn, Zachary Klaassen, Neil E Fleshner

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引用次数: 0

摘要

前言：结合系统性和靶向性活检取样可提高对有临床意义的前列腺癌（PCa）的检出率。我们的目的是评估主动监测（AS）患者首次活检时扩大核心取样是否与随后的AS终止和病理结果有关：方法：从监测、流行病学和最终结果（SEER）前列腺守候数据库中确定了2010年至2015年期间确诊的国家综合癌症网络（NCCN）低风险和良好中度风险（FIR）AS患者。前列腺活检取样分为标准取样（10-12个核芯）、扩展取样（13-20个核芯）或超扩展取样（21个核芯以上）。使用不同的临界值进行了敏感性分析。研究结果包括延迟明确干预（根治性前列腺切除术[RP]/放射治疗）和延迟根治性前列腺切除术患者的病理升级和/或降级。根据社会人口学/肿瘤学变量进行了多变量逻辑回归建模：该队列包括 42 459 例患者（低风险：28 411 例；FIR：14 048 例）；25%-29% 和 3%- 5% 的患者在诊断时分别进行了扩展和超扩展核心取样。在低风险（几率比 [OR] 0.89，P=0.003）和等级组 2 (GG2) FIR（OR 0.83，P=0.002）患者中，扩展核心取样与明确干预的几率降低有关。在 PSA 10-20 FIR 患者中，超扩展取样与最终干预几率降低相关（OR 0.65，P=0.02）。超扩展取样与低危患者≥GG2疾病（OR 0.45，p=0.032）和GG2 FIR患者≥GG3疾病（OR 0.67，p=0.044）的升级几率降低有关：这项基于人群的分析表明，诊断时延长/超延长取样与低/FIR AS 患者中断 AS 和病理升级的几率显著降低有关。这凸显了在初次活检时扩大组织取样的意义，以便对AS患者进行适当的风险分层，并最大限度地降低AS停药率。

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Association of extended core sampling with delayed intervention and pathologic outcomes for active surveillance patients A population-based analysis.

Introduction: Combined systematic plus targeted biopsy sampling improves detection of clinically significant prostate cancer (PCa). Our objective was to evaluate whether extended core sampling at initial biopsy in active surveillance (AS) patients is associated with subsequent AS discontinuation and pathologic outcomes.

Methods: National Comprehensive Cancer Network (NCCN) low- and favorable-intermediate-risk (FIR) AS patients diagnosed between 2010 and 2015 were identified from the Surveillance, Epidemiology, and End Results (SEER) Prostate with Watchful Waiting database. Prostate biopsy sampling was operationalized as: standard (10-12 cores), extended (13-20 cores), or super-extended (21+ cores). Sensitivity analyses using differing cutoffs was performed. Outcomes included delayed definitive intervention (radical prostatectomy [RP]/radiotherapy) and pathologic upgrading and/or downgrading in delayed RP patients. Multivariable logistic regression modelling adjusted for sociodemographic/oncologic variables was performed.

Results: This cohort included 42 459 patients (low-risk: 28 411; FIR:14 048); 25-29% and 3-5% of patients underwent extended and super-extended core sampling, respectively, at diagnosis. Extended core sampling was associated with decreased odds of definitive intervention in low (odds ratio [OR] 0.89, p=0.003) and grade group 2 (GG2) FIR (OR 0.83, p=0.002) patients. Super-extended sampling was associated with decreased odds of definitive intervention in prostate-specific antigen (PSA) 10-20 FIR patients (OR 0.65, p=0.02). Super-extended sampling was associated with decreased odds of upgrading to ≥GG2 disease in low-risk (OR 0.45, p=0.032) and to ≥GG3 disease in GG2 FIR patients (OR 0.67, p=0.044).

Conclusions: This population-based analysis demonstrates that extended/super-extended sampling at diagnosis is associated with significantly decreased odds of AS discontinuation and pathologic upgrading in low/FIR AS patients. This highlights the significance of extended tissue sampling at initial biopsy to appropriately risk-stratify AS patients and minimize AS discontinuation rates.

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来源期刊

Cuaj-Canadian Urological Association Journal 医学-泌尿学与肾脏学

CiteScore

2.80

自引率

10.50%

发文量

167

审稿时长

>12 weeks

期刊介绍： CUAJ is a a peer-reviewed, open-access journal devoted to promoting the highest standard of urological patient care through the publication of timely, relevant, evidence-based research and advocacy information.