阿法扎对有疾病进展风险的症状性良性前列腺增生男性的疗效和安全性：一项多中心、双盲、安慰剂对照、随机临床试验。

Efficacy and safety of Afalaza in men with symptomatic benign prostatic hyperplasia at risk of progression: a multicenter, double-blind, placebo-controlled, randomized clinical trial.

作者信息

Pushkar Dmitry, Vinarov Andrey, Spivak Leonid, Kolontarev Konstantin, Putilovskiy Mikhail, Andrianova Elena, Epstein Oleg

机构信息

Moscow State University of Medicine and Dentistry, Department of Urology, Moscow, Russian Federation.

Sechenov University, Moscow, Russian Federation.

出版信息

Cent European J Urol. 2018;71(4):427-435. doi: 10.5173/ceju.2018.1803. Epub 2018 Dec 27.

INTRODUCTION

In order to investigate the efficacy and safety of Afalaza in men with benign prostatic hyperplasia (BPH) at risk of progression, this multicenter, double-blind, placebo-controlled, randomized clinical trial was performed. Derived by technological treatment of antibodies to prostate-specific antigen (PSA) and endothelial nitric oxide synthase (eNOs), Afalaza was previously proved to modulate its molecular targets. The mechanism of action of the drug is associated with the modulating effect of the antibiodies (RA-Abs) on the molecular targets (PSA and eNOS) by way of conformational changes.

MATERIAL AND METHODS

A total of 49 patients aged 45-60 years with BPH and moderate lower urinary tract symptoms (LUTS), total prostate volume (TPV) ≥30 cm, Qmax 10-15 ml/s, and serum PSA<4 ng/ml were randomly assigned to receive either Afalaza (n = 125) or placebo (n = 124) for 12 months. Changes in BPH/LUTS symptoms (according to the International Prostate Symptom Score), Qmax, TPV, PSA, BPH clinical progression, occurrence of acure urinary retention (AUR) events or BPH-related surgery were estimated as the study endpoints.

RESULTS

IPSS mean change was -3.7 ±3.0 (95% CI -4.3 to -3.2) after 12 months of Afalaza (vs. -2.9 ±2.4; 95% CI -3.3 to -2.4 in placebo; р = 0.02). Qmax growth was 2.5 ±4.3 ml/s (vs. 1.4 ±3.3 in placebo; p = 0.049), TPV reduced by 11.8 ±16.0% (vs. 6.5 ±14.7%; p = 0.01, and PSA remained unchanged. Afalaza therapy resulted in a significant decrease in the total sum of BPH progression symptoms (p = 0.01). The maximum effect of Afalaza was registered after 12 months without a tendency to form a 'plateau'. During the study, no patients experienced AUR or BPH-related surgery.

CONCLUSIONS

A 12-month course of Afalaza therapy is effective and safe for patients with BPH. The results of end points measurements revealed asignificant advantage of Afalaza compared to placebo in the overall symptoms benefit and a decline in the risk of BPH progression.ClinicalTrials.gov: NCT01716104.

引言

为了研究阿法扎（Afalaza）对有疾病进展风险的良性前列腺增生（BPH）男性患者的疗效和安全性，开展了这项多中心、双盲、安慰剂对照的随机临床试验。阿法扎是通过对前列腺特异性抗原（PSA）和内皮型一氧化氮合酶（eNOs）抗体进行技术处理而得到的，先前已证明其可调节分子靶点。该药物的作用机制与抗体（RA-Abs）通过构象变化对分子靶点（PSA和eNOS）的调节作用有关。

材料与方法

总共49例年龄在45至60岁之间、患有BPH且有中度下尿路症状（LUTS）、总前列腺体积（TPV）≥30 cm、最大尿流率（Qmax）为10 - 15 ml/s且血清PSA<4 ng/ml的患者被随机分配接受阿法扎（n = 125）或安慰剂（n = 124）治疗12个月。将BPH/LUTS症状的变化（根据国际前列腺症状评分）、Qmax、TPV、PSA、BPH临床进展、急性尿潴留（AUR）事件的发生情况或与BPH相关的手术作为研究终点进行评估。

结果

服用阿法扎12个月后，国际前列腺症状评分（IPSS）的平均变化为-3.7±3.0（95%可信区间-4.3至-3.2）（相比之下，安慰剂组为-2.9±2.4；95%可信区间-3.3至-2.4；p = 0.02）。Qmax增加了2.5±4.3 ml/s（安慰剂组为1.4±3.3；p = 0.049），TPV减少了11.8±16.0%（安慰剂组为6.5±14.7%；p = 0.01），而PSA保持不变。阿法扎治疗使BPH进展症状的总和显著降低（p = 0.01）。阿法扎在12个月后达到最大效果，且没有形成“平台期”的趋势。在研究期间，没有患者经历AUR或与BPH相关的手术。