Open Access
Development of Multivalent CAR T Cells as Dual Immunotherapy and Conditioning Agents
Quenton Bubb
1, 2, 3
,
Mohammad Balood
2
,
Gabe Eduardo Seir
2, 4
,
Leah Swartzrock
2, 3
,
Ethan Haslett
2, 3
,
Katie Ho
2, 3
,
Peng Xu
5
,
Saida G. Wiltz
2, 3
,
Elena Sotillo
5
,
Tanja A. Gruber
2
,
Rebecca M Richards
6
,
Crystal L Mackall
2, 5, 7
,
Agnieszka Czechowicz
2, 3
Publication type: Journal Article
Publication date: 2025-03-01
scimago Q1
wos Q1
SJR: 1.716
CiteScore: 11.1
Impact factor: 5.3
ISSN: 29503299
Abstract
Hematopoietic stem cell transplantation (HSCT) is the only definitive cure for pediatric acute myeloid leukemia (AML). Despite adjustments in HSCT protocols and improvements in supportive care, 30% of high-risk patients who receive HSCT as part of their therapy still experience disease relapse with high transplant-related mortality. Relapsed AML has a dismal prognosis, and novel therapies are needed. To improve upon the status quo, HSCT would more effectively eliminate relapse-initiating leukemic cells and be delivered with safer, non-genotoxic conditioning. Here, we investigate hematopoietic cytokine receptors (HCRs) and identify that KIT, MPL, and FLT3 are collectively highly expressed in virtually all pediatric AML samples studied. Further, we establish proof-of-concept of a first-in-class chimeric antigen receptor (CAR) T cell that enables simultaneous targeting of KIT, MPL, and FLT3 through a single receptor, which we term the extracellularly linked concatemeric trivalent cytokine (ELECTRIC) CAR. ELECTRIC CARs exhibit potent cytotoxicity against normal and malignant hematopoietic cells in vitro and display anti-HCR activity in a murine xenograft model. We propose that the ELECTRIC system can be the foundation to developing a non-genotoxic, anti-leukemic conditioning regimen to enable safer, more durable efficacy with minimal toxicity.
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Metrics
7
Total citations:
7
Citations from 2024:
7
(100%)
Cite this
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RIS |
BibTex |
MLA
Cite this
GOST
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Bubb Q. et al. Development of Multivalent CAR T Cells as Dual Immunotherapy and Conditioning Agents // Molecular Therapy Oncology. 2025. Vol. 33. No. 1. p. 200944.
GOST all authors (up to 50)
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Bubb Q., Balood M., Seir G. E., Swartzrock L., Haslett E., Ho K., Xu P., Wiltz S. G., Sotillo E., Gruber T. A., Richards R. M., Mackall C. L., Czechowicz A. Development of Multivalent CAR T Cells as Dual Immunotherapy and Conditioning Agents // Molecular Therapy Oncology. 2025. Vol. 33. No. 1. p. 200944.
Cite this
RIS
Copy
TY - JOUR
DO - 10.1016/j.omton.2025.200944
UR - https://linkinghub.elsevier.com/retrieve/pii/S295032992500013X
TI - Development of Multivalent CAR T Cells as Dual Immunotherapy and Conditioning Agents
T2 - Molecular Therapy Oncology
AU - Bubb, Quenton
AU - Balood, Mohammad
AU - Seir, Gabe Eduardo
AU - Swartzrock, Leah
AU - Haslett, Ethan
AU - Ho, Katie
AU - Xu, Peng
AU - Wiltz, Saida G.
AU - Sotillo, Elena
AU - Gruber, Tanja A.
AU - Richards, Rebecca M
AU - Mackall, Crystal L
AU - Czechowicz, Agnieszka
PY - 2025
DA - 2025/03/01
PB - Elsevier
SP - 200944
IS - 1
VL - 33
SN - 2950-3299
ER -
Cite this
BibTex (up to 50 authors)
Copy
@article{2025_Bubb,
author = {Quenton Bubb and Mohammad Balood and Gabe Eduardo Seir and Leah Swartzrock and Ethan Haslett and Katie Ho and Peng Xu and Saida G. Wiltz and Elena Sotillo and Tanja A. Gruber and Rebecca M Richards and Crystal L Mackall and Agnieszka Czechowicz},
title = {Development of Multivalent CAR T Cells as Dual Immunotherapy and Conditioning Agents},
journal = {Molecular Therapy Oncology},
year = {2025},
volume = {33},
publisher = {Elsevier},
month = {mar},
url = {https://linkinghub.elsevier.com/retrieve/pii/S295032992500013X},
number = {1},
pages = {200944},
doi = {10.1016/j.omton.2025.200944}
}
Cite this
MLA
Copy
Bubb, Quenton, et al. “Development of Multivalent CAR T Cells as Dual Immunotherapy and Conditioning Agents.” Molecular Therapy Oncology, vol. 33, no. 1, Mar. 2025, p. 200944. https://linkinghub.elsevier.com/retrieve/pii/S295032992500013X.