一项针对被转诊至早期临床试验的罕见癌症患者的单中心经验。
A single centre experience of patients with rare cancers referred for early phase clinical trials.
作者信息
Angelakas Angelos, Cook Natalie, Graham Donna M, Krebs Matthew, Thistlethwaite Fiona, Carter Louise
机构信息
Department of Medical Oncology, The Christie NHS Foundation Trust, Manchester, UK.
Division of Cancer Sciences, Faculty of Biology, Medicine and Health, University of Manchester, Manchester, UK.
出版信息
BMC Cancer. 2025 Mar 28;25(1):558. doi: 10.1186/s12885-025-13934-2.
BACKGROUND
Cancers affecting < 6/100,000/year are classified as rare, but they account for up to 25% of all cancers and are associated with worse 5-year survival than common cancers. Early-phase clinical trials (EPCTs) may represent a viable treatment option for patients with rare cancers as they have evolved significantly with novel designs and the increasing use of precision medicine.
METHODS
A retrospective study of patients with rare cancers referred to a large EPCT team at a UK specialist centre over 5 years (2016-2020) was conducted. Patient demographics, medical and oncological history, genomic variants, EPCT participation, responses and survival outcomes were analysed.
RESULTS
In total, 240 patients with rare cancers were included. The mean age at diagnosis was 51.7 years (range 16-84), 54.2% of the patients were female. The most frequent rare cancers originated from the digestive system (27.1%), female genital tract (20%) and head and neck (H + N) (18.3%). Molecular profiling was offered to 45.5% of the population, median number of gene alterations was 3 per patient (range 1-20) while actionable gene alterations were reported in 60.2% (n = 50) of those with identified gene aberrations. Fifty-one patients participated in EPCTs, with 39.2% achieving SD and 11.8% PR. Median PFS for trial participants was three months (95% CI 1.12 - 4.88) while median OS in the trial patients was 16 months (95% CI 9.10 - 22.90) compared to 7 months for non-trial participants (95% CI 5.50 - 8.51). Finally, poor Royal Marsden Hospital (RMH) prognostic score (2-3) was correlated with worse survival when controlling for age and sex (HR 1.714, 95% CI 1.19 - 2.46, p = 0.004).
CONCLUSIONS
Participation of patients with rare cancers in EPCTs may be associated with a survival benefit and lead to the development of new treatments for these patients. Moreover, expanded use of precision medicine is paramount as it can inform targeted treatment selection in this heterogenous group.
背景
每年发病率低于十万分之六的癌症被归类为罕见癌症,但它们占所有癌症的比例高达25%,并且与普通癌症相比,5年生存率更低。早期临床试验(EPCT)可能是罕见癌症患者可行的治疗选择,因为随着新设计的不断涌现以及精准医学的日益广泛应用,早期临床试验已经有了显著发展。
方法
对一家英国专科中心的大型早期临床试验团队在5年(2016 - 2020年)内收治的罕见癌症患者进行了回顾性研究。分析了患者的人口统计学特征、医学和肿瘤病史、基因组变异、参与早期临床试验的情况、反应及生存结果。
结果
总共纳入了240例罕见癌症患者。诊断时的平均年龄为51.7岁(范围16 - 84岁),54.2%的患者为女性。最常见的罕见癌症起源于消化系统(27.1%)、女性生殖道(20%)和头颈部(H + N)(18.3%)。45.5%的患者接受了分子谱分析,每位患者的基因改变中位数为3个(范围1 - 20个),而在那些已识别出基因异常的患者中,60.2%(n = 50)报告了可操作的基因改变。51例患者参与了早期临床试验,39.2%达到疾病稳定(SD),11.8%达到部分缓解(PR)。试验参与者的中位无进展生存期(PFS)为3个月(95%置信区间1.12 - 4.88),而试验患者的中位总生存期(OS)为16个月(95%置信区间9.10 - 22.90),相比之下,未参与试验的患者中位总生存期为7个月(95%置信区间5.50 - 8.51)。最后,在控制年龄和性别后,皇家马斯登医院(RMH)预后评分较差(2 - 3分)与较差的生存率相关(风险比1.714,95%置信区间1.19 - 2.46,p = 0.004)。
结论
罕见癌症患者参与早期临床试验可能与生存获益相关,并能为这些患者开发新的治疗方法。此外,扩大精准医学的应用至关重要,因为它可为这一异质性群体的靶向治疗选择提供依据。
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