Dennis S Chan, Aran L Kanagaratnam, Nick Pavlakis, David L Chan
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Endpoints included overall survival (OS), progression-free survival (PFS) and adverse events (AEs); summarised qualitatively because of the marked heterogeneity in patient populations, trial designs and treatments administered. Eligible studies (24) included: 14 retrospective studies (643 patients) and 10 prospective studies (521 patients). For PRRT, most studies used <sup>177</sup> Lu (n = 21), with combination <sup>177</sup> Lu + <sup>90</sup> Y (n = 2), <sup>111</sup> In (n = 1) and <sup>225</sup> Ac (n = 1). Chemotherapy regimens included capecitabine (n = 8), capecitabine and temozolomide (n = 5), 5-fluorouracil (n = 4) or a mixture of regimens (n = 6). Most studies included Grade 1-2 NENs. In prospective studies, median OS exceeded 2 years in most studies (range not reached by end of follow-up-86 months). In retrospective studies, median OS ranged from 7 months to 55 months and was not reached in many studies. 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引用次数: 0
摘要
肽受体放化核素治疗(PRCRT)是在肽受体放化核素治疗(PRRT)的基础上增加的放化化疗,已在神经内分泌肿瘤(NENs)的个别中心使用,但迄今为止关于其疗效和安全性的数据很少。我们进行了系统的回顾,以记录该组合的疗效和副作用。我们检索了包括≥5例接受PRCRT的晚期NENs患者的研究。检索各大数据库,并通过手工检索2019 - 2023年各大会议进行补充。提取的数据包括临床病理特征、试验环境、化疗和PRRT的剂量。终点包括总生存期(OS)、无进展生存期(PFS)和不良事件(ae);由于患者群体、试验设计和治疗方法的显著异质性,对其进行了定性总结。符合条件的研究(24项)包括:14项回顾性研究(643例)和10项前瞻性研究(521例)。对于PRRT,大多数研究使用177 Lu (n = 21), 177 Lu + 90 Y (n = 2), 111 In (n = 1)和225 Ac (n = 1)的组合。化疗方案包括卡培他滨(n = 8)、卡培他滨联合替莫唑胺(n = 5)、5-氟尿嘧啶(n = 4)或混合方案(n = 6)。大多数研究包括1-2年级nen。在前瞻性研究中,大多数研究的中位生存期超过2年(随访结束时为86个月)。在回顾性研究中,中位生存期从7个月到55个月不等,在许多研究中没有达到。PFS数据范围从前瞻性队列中31个月未达到,到回顾性队列中4个月未达到。3/4级ae通常是血液学的,大多数是可逆的或没有持续的临床影响。对于晚期NENs, PRCRT治疗已显示出有希望的临床结果,并且耐受性良好,尽管已确定的研究是异质的。需要进一步的随机试验数据来阐明这种联合治疗方式在NEN治疗范例中的地位。
Peptide receptor chemoradionuclide therapy for neuroendocrine neoplasms: A systematic review.
Peptide receptor chemoradionuclide therapy (PRCRT), the addition of radiosensitising chemotherapy to peptide receptor radionuclide therapy (PRRT), has been used in individual centres for neuroendocrine neoplasms (NENs), but there are few data to date regarding its efficacy and safety. We conducted a systematic review to document the efficacy and side effect profile of this combination. We searched for studies including ≥5 patients with advanced NENs who received PRCRT. Major databases were searched and supplemented by handsearching of major conferences from 2019 to 2023. Data extracted included clinicopathological characteristics, trial setting and doses of chemotherapy and PRRT administered. Endpoints included overall survival (OS), progression-free survival (PFS) and adverse events (AEs); summarised qualitatively because of the marked heterogeneity in patient populations, trial designs and treatments administered. Eligible studies (24) included: 14 retrospective studies (643 patients) and 10 prospective studies (521 patients). For PRRT, most studies used 177 Lu (n = 21), with combination 177 Lu + 90 Y (n = 2), 111 In (n = 1) and 225 Ac (n = 1). Chemotherapy regimens included capecitabine (n = 8), capecitabine and temozolomide (n = 5), 5-fluorouracil (n = 4) or a mixture of regimens (n = 6). Most studies included Grade 1-2 NENs. In prospective studies, median OS exceeded 2 years in most studies (range not reached by end of follow-up-86 months). In retrospective studies, median OS ranged from 7 months to 55 months and was not reached in many studies. PFS data ranged from 31 months-not reached in prospective cohorts and from 4 months-not reached in retrospective cohorts. Grade 3/4 AEs were commonly haematological, with majority being reversible or having no ongoing clinical impact. For advanced NENs, PRCRT treatment has demonstrated promising clinical outcomes and was well tolerated, although identified studies were heterogeneous. Further randomised trial data are required to clarify the place of this combination modality in the NEN treatment paradigm.
期刊介绍:
Journal of Neuroendocrinology provides the principal international focus for the newest ideas in classical neuroendocrinology and its expanding interface with the regulation of behavioural, cognitive, developmental, degenerative and metabolic processes. Through the rapid publication of original manuscripts and provocative review articles, it provides essential reading for basic scientists and clinicians researching in this rapidly expanding field.
In determining content, the primary considerations are excellence, relevance and novelty. While Journal of Neuroendocrinology reflects the broad scientific and clinical interests of the BSN membership, the editorial team, led by Professor Julian Mercer, ensures that the journal’s ethos, authorship, content and purpose are those expected of a leading international publication.
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