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新辅助激素治疗高危前列腺癌后的肿瘤消退:一项随机 II 期试验的病理结果。

Tumor regression after neoadjuvant hormonal therapy in high risk prostate cancer: pathological outcomes from a randomized phase II trial.

机构信息

Department of Pathology, Instituto do Câncer do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, São Paulo, SP, Brazil.

Department of Clinical Oncology, Instituto do Câncer do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, São Paulo, SP, Brazil.

出版信息

World J Urol. 2024 Nov 2;42(1):618. doi: 10.1007/s00345-024-05323-4.

Abstract

PURPOSE

High-risk localized prostate cancer (HRLPC) commonly progresses to metastatic disease after local treatment. Neoadjuvant androgen deprivation therapy (nADT) before radical prostatectomy (RP) has recently been suggested to improve early oncological outcomes in HRLPC. We aimed to perform an exploratory analysis of the pathological outcomes from a prospective trial testing nADT before RP.

METHODS

Prospective, single-centered, phase II, randomized trial performed between October 2018 and July 2021. Random assignment (1:1) for nADT modalities: goserelin (10.8 mg) plus abiraterone acetate (1000 mg/d) plus prednisone (5 mg/d), with or without apalutamide (240 mg/d) for 12 weeks, followed by RP (within 30 days) and extended lymph node dissection. Baseline clinical and pathological variables were assessed in needle biopsies before nADT. Tumor regression was histologically evaluated in surgical specimens using the residual cancer burden index (RCB).

RESULTS

Sixty-two patients reached the surgical phase. Good response (RCB ≤ 0.25 cm³) was achieved in 14 patients (22.5%). Overall stage migration rate between baseline status (MRI before nADT) and final status (after surgery) was 27.4%. Late stage detection (high tumor burden, perineural invasion) and altered PTEN/ERG immunostatus showed significant association with poor response in univariate analysis. Higher baseline tumor burden was the only independent factor related to poor response in multivariate analysis.

CONCLUSIONS

There are subgroups of patients, such as those with low baseline cancer burden and PTEN/ERG wild-type status, more likely to achieve good response with nADT. In the case of long term oncological benefit to be proven, nADT might be an additional therapeutic resource for these patients.

摘要

目的

高危局限性前列腺癌(HRLPC)在局部治疗后常进展为转移性疾病。新辅助去势治疗(nADT)在根治性前列腺切除术(RP)前的应用最近被认为可以改善 HRLPC 的早期肿瘤学结果。我们旨在对一项前瞻性试验的病理结果进行探索性分析,该试验检测了 nADT 在 RP 前的应用。

方法

这是一项于 2018 年 10 月至 2021 年 7 月进行的前瞻性、单中心、II 期、随机试验。nADT 模式(1:1 随机分配):戈舍瑞林(10.8mg)+醋酸阿比特龙(1000mg/d)+泼尼松(5mg/d),加或不加阿帕鲁胺(240mg/d),持续 12 周,随后进行 RP(在 30 天内)和扩大淋巴结清扫。在 nADT 前的针吸活检中评估基线临床和病理变量。使用残留癌负担指数(RCB)在手术标本中评估肿瘤退缩情况。

结果

62 例患者达到手术阶段。14 例(22.5%)患者达到良好反应(RCB≤0.25cm³)。基线状态(nADT 前 MRI)与最终状态(手术后)之间的总体分期迁移率为 27.4%。单因素分析显示,晚期检测(高肿瘤负荷、神经周围侵犯)和改变的 PTEN/ERG 免疫状态与不良反应显著相关。多因素分析显示,较高的基线肿瘤负荷是与不良反应相关的唯一独立因素。

结论

在 nADT 治疗中,存在一些亚组患者,如基线癌症负担较低和 PTEN/ERG 野生型状态的患者,更有可能获得良好的反应。在长期肿瘤学获益得到证实的情况下,nADT 可能成为这些患者的额外治疗资源。

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