RENO Study: Clinical characteristics, treatment patterns and survival results in patients with metastatic renal cell carcinoma in Northern Spain

IF 3 3区 医学 Q2 ONCOLOGY Seminars in oncology Pub Date : 2024-06-01 DOI:10.1053/j.seminoncol.2024.02.002
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Abstract

Background

The current available evidence on the management of metastatic renal cell cancer (mRCC) in real life is scarce in our environment. We present a summary of the existing real-world data and the results of an analysis describing the clinical characteristics, treatments, and health outcomes of patients with mRCC in northern Spain.

Methods

Retrospective observational study. Adult patients diagnosed with mRCC between Jan 2007 and Dec 2019 were included. Epidemiological, efficacy and toxicity data were collected. Median overall survival (OS) and progression-free survival (PFS) were determined using the Kaplan-Meier method.

Results

A total of 829 patients were included (median age at diagnosis:63 years;73% men). Median follow-up was 180 months. The preponderant histology was clear cell (85%). In 50% the initial diagnosis was advanced disease. The distribution according to IMDC prognosis was good (24%), intermediate (50%) and poor (26%). The most frequent metastatic locations were lung (68.3%) and lymph node (41.0%). Most patients (95%) received a first line (1L) systemic treatment, 60% were treated with a second line (2L) of therapy and 37% received third line (3L). A VEGFR-TKIs was the most common treatment (1L: 90%, n = 507; 2L: 49%, n = 233; 3L: 54%, n = 156) followed by mTOR inhibitors (1L: 2%, n = 4; 2L: 27%, n = 126; 3L: 23%, n = 68) and immunotherapy (1L: 3.7%, n = 25; 2L: 27%, n = 126). Median OS was 24.5 months in the general population. According to IMDC prognostic groups, OS was 52.5, 25.7 and 9 months respectively. From the start of the 1L, 2L, and 3L treatment, median PFS was: 1L: 7.8 (6.8–9.0); 2L: 4.9 (4.3–5.5); 3L: 4.3 (3.8–4.8) months. No unexpected toxicity was reported.

Conclusions

The Real-World Data on the management of mRCC in Northern Spain are comparable in epidemiology, efficacy, and safety to studies conducted in other areas of the world. The significant reduction in the number of patients receiving second and subsequent lines of therapy hampers the access to new therapies developed in this context.

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RENO 研究:西班牙北部转移性肾细胞癌患者的临床特征、治疗模式和生存结果
在现实生活中,有关转移性肾细胞癌(mRCC)治疗的现有证据并不多。我们总结了现有的真实世界数据,并对西班牙北部 mRCC 患者的临床特征、治疗方法和健康结果进行了分析。回顾性观察研究。研究纳入了 2007 年 1 月至 2019 年 12 月期间确诊为 mRCC 的成年患者。收集了流行病学、疗效和毒性数据。采用卡普兰-梅耶法确定中位总生存期(OS)和无进展生存期(PFS)。共纳入 829 名患者(诊断时的中位年龄:63 岁;73% 为男性)。中位随访时间为 180 个月。组织学特征以透明细胞为主(85%)。50%的患者最初诊断为晚期疾病。IMDC预后分布为良好(24%)、中等(50%)和较差(26%)。最常见的转移部位是肺部(68.3%)和淋巴结(41.0%)。大多数患者(95%)接受一线(1L)系统治疗,60%接受二线(2L)治疗,37%接受三线(3L)治疗。VEGFR-TKIs是最常见的治疗方法(1L:90%,507例;2L:49%,233例;3L:54%,156例),其次是mTOR抑制剂(1L:2%,4例;2L:27%,126例;3L:23%,68例)和免疫疗法(1L:3.7%,25例;2L:27%,126例)。一般人群的中位 OS 为 24.5 个月。根据IMDC预后分组,OS分别为52.5个月、25.7个月和9个月。从1L、2L和3L治疗开始,中位PFS分别为:1L:7.8(6.8-9.0)个月;2L:4.9(4.3-5.5)个月;3L:4.3(3.8-4.8)个月。无意外毒性报告。西班牙北部治疗 mRCC 的真实世界数据在流行病学、疗效和安全性方面与世界其他地区进行的研究相当。接受二线及后续治疗的患者人数大幅减少,阻碍了在此背景下开发的新疗法的使用。
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来源期刊
Seminars in oncology
Seminars in oncology 医学-肿瘤学
CiteScore
6.60
自引率
0.00%
发文量
58
审稿时长
104 days
期刊介绍: Seminars in Oncology brings you current, authoritative, and practical reviews of developments in the etiology, diagnosis and management of cancer. Each issue examines topics of clinical importance, with an emphasis on providing both the basic knowledge needed to better understand a topic as well as evidence-based opinions from leaders in the field. Seminars in Oncology also seeks to be a venue for sharing a diversity of opinions including those that might be considered "outside the box". We welcome a healthy and respectful exchange of opinions and urge you to approach us with your insights as well as suggestions of topics that you deem worthy of coverage. By helping the reader understand the basic biology and the therapy of cancer as they learn the nuances from experts, all in a journal that encourages the exchange of ideas we aim to help move the treatment of cancer forward.
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