Description

Nasopharyngeal carcinoma is a highly prevalent malignant tumor in the southern regions of China, with approximately 4% to 10% of patients presenting with distant metastasis at the initial diagnosis. The five-year survival rate of traditional sole systemic chemotherapy is less than 10%, and there is an urgent need to explore more effective treatment strategies. Our team previously conducted a single-center study (402 cases) and a national multicenter retrospective study (794 cases) and first revealed that local regional radiotherapy combined with systemic chemotherapy resulted in a 60% reduction in mortality compared to systemic chemotherapy alone (HR = 0.40) (Chen MY, Chin J Cancer, 2013; Eur J Cancer, 2015). To verify this finding, with the support of the 5010 project of Sun Yat-sen University, our team initiated the world's first phase III prospective clinical trial for newly diagnosed distant metastatic nasopharyngeal carcinoma in 2014. This trial confirmed that after 6 courses of adequate systemic chemotherapy, the control group was followed up, while the experimental group received local regional full-target area adequate radiotherapy, covering the gross tumor volume (GTV), high-risk clinical target area 1 (CTV1), and low-risk clinical target area 2 (CTV2), with a total radical dose of 70 Gy, 60 Gy and 54 Gy for prophylactic radiotherapy, extending the median progression-free survival (mPFS) from 6.7 months to 12.4 months, and the 2-year PFS rate from 3.6% to 35.0%. This "adequate chemotherapy + full-target adequate radiotherapy" dual-model achieved the "Global ASCO 17 Major Clinical Oncology Breakthrough" by the American Society of Clinical Oncology in 2021, directly promoting the inclusion of local radiotherapy in the standard recommended treatment for metastatic nasopharyngeal carcinoma in the US NCCN treatment guidelines, European ESMO guidelines, Chinese CSCO guidelines and CACA guidelines (Chen MY, JAMA Oncology, 2020).

With the widespread application of PD-1 monoclonal antibodies, GP chemotherapy combined with immunotherapy (with a maximum mPFS of 21.4 months and 2-year PFS of 44.8%) has become the first-line chemotherapy regimen for recurrent/metastatic nasopharyngeal carcinoma. However, these single-drug studies did not combine local-region radiotherapy, and its value in newly diagnosed distant metastatic nasopharyngeal carcinoma has not been optimized. Therefore, our team further conducted a phase II clinical trial, sequentially administering local-region full-target radiotherapy and PD-1 monoclonal antibody during and after systemic adequate chemotherapy, and the results showed that the mPFS exceeded 30.6 months, and the 2-year PFS rate reached 54%, confirming the outstanding efficacy of the "adequate chemotherapy + half-course immunotherapy + full-target radiotherapy" triple model (Chen MY, Cell Reports Medicine, 2023).

However, the preventive irradiation area CTV2 in full-target radiotherapy has a wide coverage and is irradiated with a dose of 54 Gy or more, resulting in a 33.9% incidence of grade 3 acute mucositis and 5.2% of late hearing damage and other adverse events, severely restricting treatment tolerance. Moreover, basic research has revealed that lymph node integrity is crucial for immunotherapy, and excessive destruction of draining lymph nodes (>30 Gy) will deplete the Tim-3-TCF-1⁺ CD8+ T cell subset (with stem cell characteristics, driving long-term responses to PD-1 monoclonal antibodies), while weakening the ability of antigen-presenting cells to activate T cells, leading to impaired systemic anti-tumor immunity. Clinical retrospective analysis also indicates that patients undergoing extensive preventive lymph node dissection who received PD-1 monoclonal antibody treatment had significantly shorter PFS (HR = 0.46). Based on this, we propose the following hypothesis: In the era of immunotherapy, omitting the traditional CTV2 for the irradiation area, and exempting the low-risk invasion area of the primary lesion and the lymphatic drainage areas such as the neck II-IV zone from the preventive irradiation, can not only reduce toxicity but also preserve the lymph node immune microenvironment, thereby potentially enhancing the systemic anti-tumor response and being more conducive to the control of systemic metastatic lesions. Therefore, our team has further carried out a phase II clinical trial. After 6 courses of full-dose chemotherapy and immunotherapy, sequential local-region reduced-CTV2 radiotherapy and concurrent and maintenance immunotherapy of PD-1 monoclonal antibody were administered. The results showed that the 1-year PFS rate was as high as 77%, preliminarily suggesting that the "full-dose chemotherapy + full-course immunotherapy + reduced target radiotherapy" new triad model may be superior to the conventional full-target radiotherapy original triad model.

To further verify the effectiveness of this new model, our team intends to conduct the world's first phase III non-inferiority clinical trial for the initial treatment of advanced nasopharyngeal carcinoma. Patients with newly diagnosis distant metastatic nasopharyngeal carcinoma who respond sensitively to chemoradiotherapy will be included. Under the full-course PD-1 treatment, they will randomly receive reduced-target radiotherapy (GTV + CTV1) or full-target radiotherapy (GTV + CTV1 + CTV2). The primary endpoints are the 2-year PFS rate (non-inferiority threshold HR = 1.5) and the incidence of grade 3 or higher radiotherapy-related adverse events.

The innovation of this research lies in: pioneering a new radiotherapy strategy under nasopharyngeal carcinoma immunotherapy that exempts the preventive irradiation of low-risk areas; revealing the mechanism correlation between reduced-target radiotherapy and the dynamics of immune cell subgroups; providing evidence-based evidence for "minimal irradiation" in immunotherapy for solid tumors.

If the study confirms non-inferiority, it will achieve three major translational values: clinical level, establishing a new standard of "reduced-target radiotherapy - immune synergy"; scientific level, clarifying the regulatory role of lymph node microenvironment in radiotherapy and immunotherapy; social level, optimizing the allocation of medical resources by improving the quality of life of patients and their treatment compliance. The implementation of this study will challenge the traditional full-target radiotherapy paradigm, providing a more efficient and less toxic reduced-target radiotherapy scheme for metastasis nasopharyngeal carcinoma, as well as locally advanced nasopharyngeal carcinoma and even other solid tumors, with significant clinical and scientific significance.