癌症合并系统性硬化症患者的免疫检查点抑制剂治疗。
Immune checkpoint inhibitor therapy in patients with cancer and pre-existing systemic sclerosis.
机构信息
Department of Medicine, Division of Rheumatology, Johns Hopkins School of Medicine, Baltimore, MD, United States.
Department of Medicine, Division of Rheumatology, University of Pennsylvania, Philadelphia, PA, United States.
出版信息
Semin Arthritis Rheum. 2024 Aug;67:152460. doi: 10.1016/j.semarthrit.2024.152460. Epub 2024 May 4.
OBJECTIVE
Immune checkpoint inhibitor (ICI) therapies have dramatically improved outcomes in multiple cancers. ICI's mechanism of action involves immune system activation to augment anti-tumor immunity. Patients with pre-existing autoimmune diseases, such as systemic sclerosis (SSc), were excluded from initial ICI clinical trials due to concern that such immune system activation could precipitate an autoimmune disease flare or new, severe immune related adverse events (irAE). In the present study, we report our experience with ICIs in patients with pre-existing SSc.
METHODS
Patients with SSc who received ICI therapy for cancer were identified from the Johns Hopkins Scleroderma Center Research Registry. Through chart review and prespecified definitions, we identified whether patients experienced worsening SSc activity or new irAEs. SSc disease activity worsening was pre-defined as an increase in modified Rodnan skin score (mRSS), new scleroderma renal crisis, progression of interstitial lung disease (ILD) on CT scan, increased Raynaud's phenomenon frequency or severity, new pulmonary hypertension, or myositis flare. IrAEs also included active inflammatory arthritis and dermatitis.
RESULTS
Eight patients with SSc who received ICI therapy for cancer were included. Overall, SSc symptoms remained stable during and after ICI therapy. None of the patients with long-standing sine or limited cutaneous SSc (lcSSc) had progressive skin thickening after ICI therapy. One patient, who was early in his diffuse cutaneous SSc (dcSSc) disease course, experienced worsening skin thickening and renal crisis. Three patients (38 %) experienced a total of five irAEs (grade 2: diarrhea, mucositis and dermatitis; grade 3: pneumonitis, and grade 4: nephritis). The patient with grade 4 nephritis developed scleroderma renal crisis and immune checkpoint related nephritis simultaneously. There were no deaths due to irAEs.
CONCLUSION
In this study, ICI therapy was well tolerated in patients with longstanding, sine or lcSSc. IrAE were common but generally manageable. Patients with early, active SSc may be at greater risk from ICI therapy, but more research is needed.
目的
免疫检查点抑制剂(ICI)疗法显著改善了多种癌症的预后。ICI 的作用机制涉及免疫系统的激活,以增强抗肿瘤免疫。由于担心这种免疫系统的激活会引发自身免疫疾病发作或新的、严重的免疫相关不良事件(irAE),最初的 ICI 临床试验排除了患有自身免疫性疾病(如系统性硬化症 [SSc])的患者。在本研究中,我们报告了我们在患有预先存在的 SSc 的患者中使用 ICI 的经验。
方法
从约翰霍普金斯硬皮病中心研究登记处确定接受 ICI 治疗癌症的 SSc 患者。通过图表审查和规定的定义,我们确定患者是否经历 SSc 活动恶化或新的 irAE。SSc 疾病活动恶化预先定义为改良罗德里格皮肤评分(mRSS)增加、新的硬皮病肾危象、CT 扫描上间质性肺病(ILD)进展、雷诺现象频率或严重程度增加、新的肺动脉高压或肌炎发作。irAE 还包括活动性炎症性关节炎和皮炎。
结果
纳入了 8 名接受 ICI 治疗癌症的 SSc 患者。总的来说,ICI 治疗期间和之后 SSc 症状保持稳定。没有接受 ICI 治疗的长期系统性或局限性 SSc(lcSSc)患者的皮肤增厚进展。一名处于弥漫性皮肤 SSc(dcSSc)疾病早期的患者经历了皮肤增厚和肾危象恶化。三名患者(38%)共发生了五例 irAE(2 级:腹泻、黏膜炎和皮炎;3 级:肺炎,4 级:肾炎)。4 级肾炎患者同时发生了硬皮病肾危象和免疫检查点相关肾炎。没有因 irAE 导致的死亡。
结论
在这项研究中,ICI 治疗在患有长期、系统性或局限性 SSc 的患者中耐受良好。irAE 很常见,但通常可以控制。早期、活动期 SSc 的患者可能面临更大的 ICI 治疗风险,但需要进一步研究。
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