Infections after chimeric antigen receptor (CAR)‐T‐cell therapy for hematologic malignancies-Reference-Cited by-同舟云学术

Infections after chimeric antigen receptor (CAR)‐T‐cell therapy for hematologic malignancies

Published:2023-10-03 Issue:S1 Volume:25 Page:
ISSN:1398-2273
Container-title:Transplant Infectious Disease
language:en
Short-container-title:Transplant Infectious Dis

Author:

Kampouri Eleftheria¹²^ORCID,Little Jessica S.³⁴,Rejeski Kai⁵⁶,Manuel Oriol²^ORCID,Hammond Sarah P.⁴⁷,Hill Joshua A.¹⁸⁹

Affiliation:

1. Vaccine and Infectious Disease Division Fred Hutchinson Cancer Center Seattle Washington USA

2. Infectious Diseases Service Lausanne University Hospital and University of Lausanne Lausanne Switzerland

3. Division of Infectious Diseases Brigham and Women's Hospital Harvard Medical School Boston Massachusetts USA

4. Division of Medical Oncology Dana‐Farber Cancer Institute Harvard Medical School Boston Massachusetts USA

5. Department of Medicine III—Hematology/Oncology LMU University Hospital, LMU Munich Munich Germany

6. German Cancer Consortium (DKTK) Munich site, and German Cancer Research Center Heidelberg Germany

7. Divisions of Hematology/Oncology and Infectious Diseases Massachusetts General Hospital Harvard Medical School Boston Massachusetts USA

8. Clinical Research Division Fred Hutchinson Cancer Center Seattle Washington USA

9. Department of Medicine University of Washington Seattle Washington USA

Abstract

AbstractBackgroundChimeric antigen receptor (CAR)‐T‐cell therapies have revolutionized the management of acute lymphoblastic leukemia, non‐Hodgkin lymphoma, and multiple myeloma but come at the price of unique toxicities, including cytokine release syndrome, immune effector cell‐associated neurotoxicity syndrome, and long‐term “on‐target off‐tumor” effects.MethodsAll of these factors increase infection risk in an already highly immunocompromised patient population. Indeed, infectious complications represent the key determinant of non‐relapse mortality after CAR‐T cells. The temporal distribution of these risk factors shapes different infection patterns early versus late post‐CAR‐T‐cell infusion. Furthermore, due to the expression of their targets on B lineage cells at different stages of differentiation, CD19, and B‐cell maturation antigen (BCMA) CAR‐T cells induce distinct immune deficits that could require different prevention strategies. Infection incidence is the highest during the first month post‐infusion and subsequently decreases thereafter. However, infections remain relatively common even a year after infusion.ResultsBacterial infections predominate early after CD19, while a more equal distribution between bacterial and viral causes is seen after BCMA CAR‐T‐cell therapy, and fungal infections are universally rare. Cytomegalovirus (CMV) and other herpesviruses are increasingly breported, but whether routine monitoring is warranted for all, or a subgroup of patients, remains to be determined. Clinical practices vary substantially between centers, and many areas of uncertainty remain, including CMV monitoring, antibacterial and antifungal prophylaxis and duration, use of immunoglobulin replacement therapy, and timing of vaccination.ConclusionRisk stratification tools are available and may help distinguish between infectious and non‐infectious causes of fever post‐infusion and predict severe infections. These tools need prospective validation, and their integration in clinical practice needs to be systematically studied.

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Publisher

Wiley

Subject

Infectious Diseases,Transplantation

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1111/tid.14157

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