Clinical Features, Survival, and Burden of Toxicities in Survivors More Than One Year After Lung Cancer Immunotherapy

Author:

Hsu Melinda L12ORCID,Murray Joseph C12,Psoter Kevin J3,Zhang Jiajia12,Barasa Durrant12,Brahmer Julie R12,Ettinger David S12,Forde Patrick M12,Hann Christine L12,Lam Vincent K12,Levy Benjamin12,Marrone Kristen A12,Patel Tricia,Peterson Valerie,Sagorsky Sarah,Turner Michelle12,Anagnostou Valsamo12,Naidoo Jarushka124,Feliciano Josephine L12

Affiliation:

1. Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins University , Baltimore, MD , USA

2. Bloomberg-Kimmel institute for Cancer Immunotherapy , Baltimore, MD , USA

3. Department of Pediatrics, Johns Hopkins University , Baltimore, MD , USA

4. Beaumont Hospital Dublin and RCSI University of Health Sciences , Dublin , Ireland

Abstract

Abstract Introduction Anti-PD-(L)1 immune checkpoint inhibitors (ICI) improve survival in patients with advanced non-small cell lung cancer (aNSCLC). The clinical features, survival, and burden of toxicities of patients with aNSCLC alive >1 year from ICI initiation are poorly understood. Materials and Methods We defined ICI survivors as patients alive >1 year after ICI start and retrospectively reviewed demographics, treatment, and immune-related adverse events (irAEs). Long-term irAEs were defined as ongoing irAEs lasting >1 year; burden of toxicity measures were based on percentage of days a patient experienced toxicity. Using linear and logistic regression, we evaluated association between demographics and disease characteristics with burden of toxicity. Results We identified 114 ICI survivors from 317 patients with aNSCLC. Half (52%) experienced an irAE of any grade, and 23.7% developed long-term irAEs. More ICI survivors with irAES in the first year had never smoked (P = .018) or received ICIs as frontline therapy (P = .015). The burden of toxicity in the first year significantly correlated with the burden of toxicity afterward (ρ = 0.72; P < .001). No patients with progressive disease had a high burden of toxicity, and they experienced 30.6% fewer days with toxicity than those with stable disease. Increased duration of therapy was associated with higher odds of experiencing toxicity. Half of ICI survivors with irAEs were still receiving treatment for unresolved irAEs at time of death or last follow-up. Conclusion Significant proportions of ICI survivors have unresolved long-term toxicities. These data support a growing need to understand long-term toxicity to optimize management of those treated with ICIs.

Publisher

Oxford University Press (OUP)

Subject

Cancer Research,Oncology

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