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首页> 外文期刊>Chinese journal of cancer >Phase I/II trial evaluating concurrent carbon-ion radiotherapy plus chemotherapy for salvage treatment of locally recurrent nasopharyngeal carcinoma
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Phase I/II trial evaluating concurrent carbon-ion radiotherapy plus chemotherapy for salvage treatment of locally recurrent nasopharyngeal carcinoma

机译:I / II期试验评估同时碳离子放疗加化疗对局部复发性鼻咽癌的挽救治疗

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Background After definitive chemoradiotherapy for non-metastatic nasopharyngeal carcinoma (NPC), more than 10% of patients will experience a local recurrence. Salvage treatments present significant challenges for locally recurrent NPC. Surgery, stereotactic ablative body radiotherapy, and brachytherapy have been used to treat locally recurrent NPC. However, only patients with small-volume tumors can benefit from these treatments. Re-irradiation with X-ray—based intensity-modulated radiotherapy (IMXT) has been more widely used for salvage treatment of locally recurrent NPC with a large tumor burden, but over-irradiation to the surrounding normal tissues has been shown to cause frequent and severe toxicities. Furthermore, locally recurrent NPC represents a clinical entity that is more radio-resistant than its primary counterpart. Due to the inherent physical advantages of heavy-particle therapy, precise dose delivery to the target volume(s), without exposing the surrounding organs at risk to extra doses, is highly feasible with carbon-ion radiotherapy (CIRT). In addition, CIRT is a high linear energy transfer (LET) radiation and provides an increased relative biological effectiveness compared with photon and proton radiotherapy. Our prior work showed that CIRT alone to 57.5 GyE (gray equivalent), at 2.5 GyE per daily fraction, was well tolerated in patients who were previously treated for NPC with a definitive dose of IMXT. The short-term response rates at 3–6?months were also acceptable. However, no patients were treated with concurrent chemotherapy. Whether the addition of concurrent chemotherapy to CIRT can benefit locally recurrent NPC patients over CIRT alone has never been addressed. It is possible that the benefits of high-LET CIRT may make radiosensitizing chemotherapy unnecessary. We therefore implemented a phase I/II clinical trial to address these questions and present our methodology and results. Methods and design The maximal tolerated dose (MTD) of re-treatment using raster-scanning CIRT plus concurrent cisplatin will be determined in the phase I, dose-escalating stage of this study. CIRT dose escalation from 52.5 to 65 GyE (2.5 GyE?×?21–26 fractions) will be delivered, with the primary endpoints being acute and subacute toxicities. Efficacy in terms of overall survival (OS) and local progression-free survival of patients after concurrent chemotherapy plus CIRT at the determined MTD will then be studied in the phase II stage of the trial. We hypothesize that CIRT plus chemotherapy can improve the 2-year OS rate from the historical 50% to at least 70%. Conclusions Re-treatment of locally recurrent NPC using photon radiation techniques, including IMXT, provides moderate efficacy but causes potentially severe toxicities. Improved outcomes in terms of efficacy and toxicity profile are expected with CIRT plus chemotherapy. However, the MTD of CIRT used concurrently with cisplatin-based chemotherapy for locally recurrent NPC remains to be determined. In addition, whether the addition of chemotherapy to CIRT is needed remains unknown. These questions will be evaluated in the dose-escalating phase I and randomized phase II trials.
机译:背景对于非转移性鼻咽癌(NPC)进行了明确的放化疗之后,超过10%的患者会出现局部复发。打捞治疗对局部复发的鼻咽癌提出了重大挑战。外科手术,立体定向消融身体放疗和近距离放射治疗已用于治疗局部复发的鼻咽癌。但是,只有患有小体积肿瘤的患者才能从这些治疗中受益。基于X射线的强度调制放射疗法(IMXT)进行的再照射已被广泛用于挽救具有较大肿瘤负担的局部复发NPC,但已证明对周围正常组织的过度照射会导致频繁和复发。剧毒。此外,局部复发的鼻咽癌代表的临床实体比主要的鼻咽癌更耐放射。由于重颗粒疗法的内在物理优势,使用碳离子放射疗法(CIRT)在不使周围器官面临额外剂量风险的情况下,精确地将剂量递送至目标体积非常可行。此外,与光子和质子放射疗法相比,CIRT是高线性能量转移(LET)辐射,并提供增强的相对生物学有效性。我们以前的工作表明,以前接受过确定剂量的IMXT接受NPC治疗的患者,对单独的CIRT至57.5 GyE(灰色当量)/每天2.5 GyE的耐受性良好。 3-6个月的短期反应率也是可以接受的。但是,没有患者接受同步化疗。与CIRT相比,在CIRT上同时进行化疗是否能使局部复发的NPC患者受益?高LET CIRT的益处可能使放射增敏化学治疗变得不必要。因此,我们实施了I / II期临床试验来解决这些问题,并介绍我们的方法和结果。方法和设计在本研究的第一阶段(剂量递增阶段),将确定使用光栅扫描CIRT加同步顺铂进行再治疗的最大耐受剂量(MTD)。 CIRT剂量将从52.5 GyE(2.5 GyE?×?21–26分数)逐步提高,主要终点是急性和亚急性毒性。然后,将在试验的II期阶段研究同时进行的化疗加CIRT(确定的MTD)后患者的总生存期(OS)和局部无进展生存期的疗效。我们假设CIRT加化疗可以将2年OS率从历史的50%提高到至少70%。结论使用包括IMXT在内的光子辐射技术对局部复发的NPC进行再治疗可提供中等疗效,但可能引起严重的毒性反应。 CIRT加化疗有望改善疗效和毒性。然而,CIRT的MTD与基于顺铂的化疗同时用于局部复发的NPC尚待确定。此外,是否需要在CIRT中增加化疗尚不清楚。这些问题将在剂量递增I期和随机II期试验中进行评估。

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