PT - JOURNAL ARTICLE AU - Beattie, Jason AU - Rizvi, Hira AU - Fuentes, Paige AU - Luo, Jia AU - Schoenfeld, Adam AU - Lin, I-Hsin AU - Postow, Michael AU - Callahan, Margaret AU - Voss, Martin H AU - Shah, Neil J AU - Betof Warner, Allison AU - Chawla, Mohit AU - Hellmann, Matthew D TI - Success and failure of additional immune modulators in steroid-refractory/resistant pneumonitis related to immune checkpoint blockade AID - 10.1136/jitc-2020-001884 DP - 2021 Feb 01 TA - Journal for ImmunoTherapy of Cancer PG - e001884 VI - 9 IP - 2 4099 - http://jitc.bmj.com/content/9/2/e001884.short 4100 - http://jitc.bmj.com/content/9/2/e001884.full SO - J Immunother Cancer2021 Feb 01; 9 AB - Background Pneumonitis related to immune checkpoint blockade is uncommon but can be severe, fatal or chronic. Steroids are first-line treatment, however, some patients are refractory or become resistant to steroids. Like many immune-related adverse events, little is known regarding the outcomes and optimal management of patients in whom steroids are ineffective.Methods We performed a single-center retrospective cohort study at a high-volume tertiary cancer center to evaluate the clinical course, management strategies and outcomes of patients treated for immune checkpoint pneumonitis with immune modulatory medications in addition to systemic steroids. Pharmacy records were queried for patients treated with both immune checkpoint blockade and receipt of additional immune modulators. Records were then manually reviewed to identify patients who received the additional immune modulators for immune checkpoint pneumonitis.Results From 2013 to 2020, we identified 26 patients treated for immune checkpoint pneumonitis with additional immune modulators in addition to steroids. Twelve patients (46%) were steroid-refractory and 14 (54%) were steroid-resistant. Pneumonitis severity included grade 2 (42%) or grade 3–4 (58%). Additional immune modulation consisted of tumor necrosis factor-alpha inhibitor (77%) and/or mycophenolate (23%). Durable improvement in pneumonitis following initiation of additional immune modulators occurred in 10 patients (38%), including three patients (12%) in whom pneumonitis resolved and all immunosuppressants ceased. The rate of 90-day all-cause mortality/hospice referral was 50%. At last follow-up, mortality attributable to pneumonitis was 23%. In addition to mortality from pneumonitis and cancer, 3 patients (12%) died due to infections possibly associated with immunosuppression.Conclusions Steroid-refractory or -resistant immune checkpoint pneumonitis is uncommon but associated with significant morbidity and mortality. Additional immunomodulators can yield durable improvement, attained in over one third of patients. An improved understanding of the underlying biology of immune-related pneumonitis will be crucial to guide more precise and effective treatment strategies in the future.