Department of Cancer Medicine and INSERM U981, Université Paris-Sud, Université Paris-Saclay, Gustave Roussy, Villejuif, France.
San Camillo and Forlanini Hospitals, Rome, Italy; Weill Cornell Medicine, New York, NY, USA.
Eur J Cancer. 2020 Oct;138:202-211. doi: 10.1016/j.ejca.2020.07.023. Epub 2020 Sep 6.
Patients with pre-existing autoimmune disease (AID) are typically excluded from clinical trials of immune checkpoint inhibitors, and there are limited data on outcomes in this population. The single-arm international SAUL study of atezolizumab enrolled a broader 'real-world' patient population. We present outcomes in patients with a history of AID.
Patients with locally advanced/metastatic urinary tract carcinoma received atezolizumab 1200 mg every 3 weeks until loss of clinical benefit or unacceptable toxicity. The primary end-point was safety. Overall survival (OS) was a secondary end-point. Subgroup analyses of AID patients were prespecified.
Thirty-five of 997 treated patients had AID at baseline, most commonly psoriasis (n = 15). Compared with non-AID patients, AID patients experienced numerically more adverse events (AEs) of special interest (46% versus 30%; grade ≥3 14% versus 6%) and treatment-related grade 3/4 AEs (26% versus 12%), but without relevant increases in treatment-related deaths (0% versus 1%) or AEs necessitating treatment discontinuation (9% versus 6%). Pre-existing AID worsened in four patients (11%; two flares in two patients); three of the six flares resolved, one was resolving, and two were unresolved. Efficacy was similar in AID and non-AID patients (median OS, 8.2 versus 8.8 months, respectively; median progression-free survival, 4.4 versus 2.2 months; disease control rate, 51% versus 39%).
In 35 atezolizumab-treated patients with pre-existing AID, incidences of special- interest and treatment-related AEs appeared acceptable. AEs were manageable, rarely requiring atezolizumab discontinuation. Treating these patients requires caution, but pre-existing AID does not preclude atezolizumab therapy.
NCT02928406.
患有自身免疫性疾病(AID)的患者通常被排除在免疫检查点抑制剂的临床试验之外,而针对该人群的研究数据有限。单臂国际 SAUL 研究纳入了更广泛的“真实世界”患者人群。我们报告了既往患有 AID 的患者的结局。
局部晚期/转移性尿路上皮癌患者接受阿替利珠单抗 1200mg,每 3 周一次,直至临床获益丧失或不可接受的毒性。主要终点是安全性。总生存期(OS)是次要终点。预先设定了 AID 患者的亚组分析。
997 例接受治疗的患者中有 35 例在基线时有 AID,最常见的是银屑病(n=15)。与非 AID 患者相比,AID 患者经历了更多的特殊关注不良事件(46%对 30%;≥3 级 14%对 6%)和治疗相关的 3/4 级不良事件(26%对 12%),但治疗相关死亡(0%对 1%)或需要停药的不良事件(9%对 6%)没有相应增加。4 例患者(11%)的原有 AID 恶化;2 例患者出现 2 次发作;6 次发作中有 3 次缓解,1 次正在缓解,2 次未缓解。AID 和非 AID 患者的疗效相似(中位 OS,分别为 8.2 个月和 8.8 个月;中位无进展生存期,分别为 4.4 个月和 2.2 个月;疾病控制率,分别为 51%和 39%)。
在 35 例接受阿替利珠单抗治疗的患有既往 AID 的患者中,特殊关注和治疗相关不良事件的发生率似乎可以接受。不良事件可管理,很少需要停止使用阿替利珠单抗。治疗这些患者需要谨慎,但既往 AID 并不排除阿替利珠单抗治疗。
NCT02928406。
