局部进展期直肠癌新辅助免疫治疗免疫相关不良反应的临床管理及分析

doi:10.19401/j.cnki.1007-3639.2025.07.005

摘要/Abstract

摘要：

背景和目的：目前，新辅助免疫治疗能够显著提升局部进展期直肠癌（locally advanced rectal cancer，LARC）新辅助治疗效果，但免疫相关不良反应（immune-related adverse events，irAEs）的临床管理尚缺乏充分证据。本研究拟探讨直肠癌新辅助免疫治疗中irAEs的发生特征、临床管理策略及转归，为优化irAEs监测与干预提供依据。方法：回顾性分析2022年7月—2024年6月于中国医学科学院北京协和医学院北京协和医院接受新辅助免疫治疗并出现irAEs的LARC患者的临床资料。记录irAEs类型、分级、发生时间、治疗措施及转归。所有患者均接受至少6个月的定期随访。本研究经中国医学科学院北京协和医院审批通过（伦理批件号：I-24PJ0024）。采用描述性统计总结irAEs的发生规律与治疗应对措施。结果：本研究共纳入30例患者，累计发生41例次irAEs，其中78%（32/41）为1~2级轻度不良反应，22%（9/41）为3~4级严重不良反应，5例（16.7%）因严重不良反应永久停药。内分泌系统不良反应最为常见（36.6%，15/41），以表现为甲状腺功能亢进到减退的动态演变为主，75%需甲状腺激素替代治疗，另有1例迟发性肾上腺皮质功能减退经糖皮质激素（glucocorticoid，GC）治疗后缓解。肝脏毒性（19.5%，8/41）中62.5%为3级损伤，37.5%需GC干预，2例术后辅助化疗期间复发。3例发生重症肌炎并伴发无症状心肌损伤，表现为肌酸激酶显著升高和心肌生物标志物同步变化，均需大剂量GC冲击联合免疫球蛋白或免疫抑制剂治疗，恢复周期2~4个月。9例发生皮肤反应，以局部治疗为主。2例发生胃肠道反应，其中1例为3级腹泻接受GC治疗。总体GC使用率为31.7%（13/41），76.9%用于3级以上irAEs管理。结论：LARC新辅助免疫治疗irAEs以轻中度为主，经过对症支持治疗可改善；但仍有部分患者发生3~4级严重不良反应，需多学科综合管理。GC使用集中于3级以上irAEs，其中重症肌炎及心脏受累虽罕见但需强化免疫抑制治疗。少数患者辅助化疗阶段出现irAEs复发，提示早期识别、分级治疗和全治疗周期管理的必要性。

关键词: 局部进展期直肠癌, 新辅助免疫治疗, 免疫相关不良反应, 糖皮质激素, 多学科综合管理

Abstract:

Background and Purpose: Neoadjuvant immunotherapy currently significantly enhances treatment efficacy for locally advanced rectal cancer (LARC); However, clinical management of immune-related adverse events (irAEs) lacks robust evidence. This study aimed to investigate the characteristics, clinical management strategies, and outcomes of irAEs during neoadjuvant immunotherapy for rectal cancer, providing a basis for optimizing irAEs monitoring and intervention. Methods: We retrospectively analyzed clinical data from LARC patients who developed irAEs after receiving neoadjuvant immunotherapy at Peking Union Medical College Hospital, Chinese Academy of Medical Sciences, between July 2022 and June 2024. Types of irAEs, severity, time of onset, management strategies, and outcomes were recorded. All patients underwent regular follow-up for at least 6 months. This study has been approved by Peking Union Medical College Hospital, Chinese Academy of Medical Sciences (ethical approval number: I-24PJ0024). Descriptive statistics were used to summarize irAEs patterns and management approaches. Results: A total of 41 irAE episodes occurred among the 30 patients. Mild irAEs (Grade 1-2) accounted for 78.0% (32/41), while severe irAEs (Grade 3-4) constituted 22.0% (9/41). Five patients (16.7%) permanently discontinued treatment due to severe toxicity. Endocrine toxicities were most frequent (36.6%, 15/41), primarily characterized by progression from hyperthyroidism to hypothyroidism; 75.0% required thyroid hormone replacement therapy. One case of delayed-onset adrenal insufficiency was alleviated with glucocorticoid (GC) therapy. Among hepatotoxicities (19.5%, 8/41), 62.5% were Grade 3 injury, and 37.5% required GC intervention; two patients experienced recurrence during adjuvant chemotherapy. Three cases of severe myositis occurred, accompanied by asymptomatic myocardial injury (evidenced by markedly elevated creatine kinase and concurrent changes in cardiac biomarkers), all requiring high-dose GC pulse therapy combined with intravenous immunoglobulin or immunosuppressants (recovery period: 2-4 months). Nine dermatological reactions were managed with topical therapy. Two gastrointestinal events occurred, including one Grade 3 diarrhea treated with GCs. The overall GC usage rate was 31.7% (13/41), with 76.9% administered for Grade ≥3 irAEs. Conclusion: irAEs during neoadjuvant immunotherapy for LARC are predominantly mild-to-moderate and manageable with supportive care. However, some patients develop severe (Grade 3-4) irAEs requiring multidisciplinary management. GC usage is concentrated in higher-grade irAEs, with severe myositis and cardiac involvement necessitating intensive immunosuppressive therapy despite their rarity. Recurrence of irAEs during adjuvant chemotherapy in a minority of patients underscores the necessity for early recognition, graded intervention, and comprehensive management throughout the entire treatment cycle.

Key words: Locally advanced rectal cancer, Neoadjuvant immunotherapy, Immune-related adverse events, Glucocorticoids, Multidisciplinary management

中图分类号:

R735.3+7

安杨, 王晨童, 邱小原, 周皎琳, 林国乐. 局部进展期直肠癌新辅助免疫治疗免疫相关不良反应的临床管理及分析[J]. 中国癌症杂志, 2025, 35(7): 665-671.

AN Yang, WANG Chentong, QIU Xiaoyuan, ZHOU Jiaolin, LIN Guole. Clinical management and analysis of immune-related adverse events in neoadjuvant immunotherapy for locally advanced rectal cancer[J]. China Oncology, 2025, 35(7): 665-671.

图/表 2

参考文献 21

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Characteristic	Case (n=30)
Gender
Male	20 (67)
Female	10 (33)
Age/year median (range)	60 (39-75）
cT stage
cT1	1 (3)
cT2	1 (3)
cT3	22 (74)
cT4	6 (20)
cN stage
cN1	8 (27)
cN2	22 (73)
MMR
dMMR	4 (13)
pMMR	26 (87)
Differentiation
Well-moderate	28 (94)
Poor	1 (3)
Mucinous	1 (3)
Treatment
Neoadjuvant radiochemotherapy and immunotherapy	26 (87)
Neoadjuvant immunotherapy	4 (13)
CEA>5 ng/mL
Yes	10 (33)
No	20 (67)
CA19-9>37 U/mL
Yes	2 (6)
No	28 (94)