Remission after CAR T‐cell therapy: Do lymphoma patients recover a normal life?

Author:

Perthus Alya1ORCID,Colin Fanny1,Charton Emilie2,Anota Amélie23,Lhomme Faustine1,Manson Guillaume1,De Guibert Sophie1,Daufresne Pierre1,Bellec Adeline1,Le Bars Laetitia1,De Barros Sandra4,Ysebaert Loïc4,Merceur Marianne5,Cogné Mélanie5,Lamy De La Chapelle Thierry16,Houot Roch16,Moignet Aline1

Affiliation:

1. Service d'Hématologie—CHU Pontchaillou, Department of Hematology University Hospital of Rennes Rennes France

2. Human and Social Sciences Department Leon Berard Center Lyon France

3. Department of Clinical Research and Innovation Leon Berard Center Lyon France

4. Department of Hematology Cancer University Institute of Toulouse Oncopole Toulouse France

5. Department of Physical and Rehabilitation Medicine University Hospital of Rennes Rennes France

6. UMR U1236, INSERM University of Rennes Rennes France

Abstract

AbstractChimeric antigen receptor T cells (CAR T cells) can induce prolonged remission in a substantial subset of patients with relapse/refractory lymphoma. However, little is known about patients' life after CAR T‐cell therapy. We prospectively assessed the multidimensional recovery of lymphoma patients in remission, before leukapheresis, before CAR T‐cell infusion, and 3, 6, and 12 months thereafter. Validated tools were used to measure lymphoma‐related and global health‐related quality of life (HRQoL; Functional Assessment of Cancer Therapy‐Lymphoma [FACT‐Lym] and EQ‐5D‐5L), cognitive complaint (FACT‐Cognition), fatigue (FACIT‐Fatigue subscale), psychological status (Hospital Anxiety and Depression Scale, Post‐Traumatic Check List Scale), and sexuality (Relationship and Sexuality Scale). Beyond 12 months of remission, we also surveyed physical, professional, sexual, and general life status. At 3, 6, and 12 months, 53, 35, and 23 patients were evaluable, respectively. Improvement in lymphoma‐related HRQoL was clinically relevant at 3, 6, and 12 months with a mean change from baseline of 10.9 (95% confidence interval [CI]: 5.8; 16.1), 12.2 (95% CI: 4.2; 20.1), and 11.72 (95% CI: 2.06; 21.38), respectively. Improvement in global HRQoL, fatigue, and anxiety was clinically relevant, but 20%–40% of patients experienced persistent fatigue, psychological distress, and cognitive complaints over time. Beyond 12 months after CAR T cells, 81.8% of 22 evaluable patients were satisfied with their daily life. Physical activity, professional, sexual, and global well‐being had returned to prediagnosis levels in nearly half of the patients. We found an improvement in HRQoL after CAR T‐cell therapy including anxiety, depression, sexual satisfaction, and general well‐being. However, not all patients recover a “normal life.” Further research is needed to determine which patients are at risk of quality‐of‐life impairment to improve recovery after CAR T‐cell infusion.

Publisher

Wiley

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