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X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells

Immunotherapy, particularly CAR-T therapy has recently emerged as an innovator for cancer treatment. Gamma-irradiated K562 cells is a common and effective method to stimulated CAR-T cells prior to treatment. However, high cost and limited equipment of gamma-irradiation is drawback of this method. Th...

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Autores principales: Bui, Khac Cuong, Ho, Viet Hoanh, Nguyen, Hien Hanh, Dang, Thanh Chung, Ngo, Thu Hang, Nguyen, Thi Mai Ly, Nguyen, Linh Toan, Dang, Thuy Linh, Tran, Thanh Tung, Le, Quang Hoa, Pham, Hong Lam, Nguyen, Van Ba, Can, Van Mao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9719861/
https://www.ncbi.nlm.nih.gov/pubmed/36478893
http://dx.doi.org/10.1016/j.bbrep.2022.101399
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author Bui, Khac Cuong
Ho, Viet Hoanh
Nguyen, Hien Hanh
Dang, Thanh Chung
Ngo, Thu Hang
Nguyen, Thi Mai Ly
Nguyen, Linh Toan
Dang, Thuy Linh
Tran, Thanh Tung
Le, Quang Hoa
Pham, Hong Lam
Nguyen, Van Ba
Can, Van Mao
author_facet Bui, Khac Cuong
Ho, Viet Hoanh
Nguyen, Hien Hanh
Dang, Thanh Chung
Ngo, Thu Hang
Nguyen, Thi Mai Ly
Nguyen, Linh Toan
Dang, Thuy Linh
Tran, Thanh Tung
Le, Quang Hoa
Pham, Hong Lam
Nguyen, Van Ba
Can, Van Mao
author_sort Bui, Khac Cuong
collection PubMed
description Immunotherapy, particularly CAR-T therapy has recently emerged as an innovator for cancer treatment. Gamma-irradiated K562 cells is a common and effective method to stimulated CAR-T cells prior to treatment. However, high cost and limited equipment of gamma-irradiation is drawback of this method. This requires the establishment of CAR-T-expanding alternatives, such as X-ray-irradiated K562 cells. X-ray irradiation was used to deactivate K562 cells. The post-irradiative cell survival was investigated by counting of the number of cells, staining with Trypan Blue and PI. FACS analysis was applied to detect the expression of cell surface markers. The production of CD19-CAR-T cells were executed from fresh blood donor by CD19-CAR-plasmid transfection, followed by the stimulation with X-ray-irradiated K562 feeder cells. The function of produced CAR-T cells was checked by their ability to kill Daudi cells. X-ray-irradiation inhibited the propagation and viability of K562 cells in a dose- and time-dependent manner. Interestingly, CAR-T-stimulating effectors were remained on the surface of X-ray-irradiated K562 cells. CD-19-CAR-T cells were produced successfully, suggested by number of CAR-positive cells in transfected and stimulated population, compared to un-transfected group. Lastly, our data showed that engineered CAR-T cells effectively killed Daudi cells. Our data demonstrated the efficacy of X-ray on deactivation K562 feeder cells which subsequently stimulated and expanded functional CAR-T cells. Thus, X-ray can be used as an alternative to inactivate K562 cells prior to using as a feeder of CAR-T cells.
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spelling pubmed-97198612022-12-06 X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells Bui, Khac Cuong Ho, Viet Hoanh Nguyen, Hien Hanh Dang, Thanh Chung Ngo, Thu Hang Nguyen, Thi Mai Ly Nguyen, Linh Toan Dang, Thuy Linh Tran, Thanh Tung Le, Quang Hoa Pham, Hong Lam Nguyen, Van Ba Can, Van Mao Biochem Biophys Rep Short Communication Immunotherapy, particularly CAR-T therapy has recently emerged as an innovator for cancer treatment. Gamma-irradiated K562 cells is a common and effective method to stimulated CAR-T cells prior to treatment. However, high cost and limited equipment of gamma-irradiation is drawback of this method. This requires the establishment of CAR-T-expanding alternatives, such as X-ray-irradiated K562 cells. X-ray irradiation was used to deactivate K562 cells. The post-irradiative cell survival was investigated by counting of the number of cells, staining with Trypan Blue and PI. FACS analysis was applied to detect the expression of cell surface markers. The production of CD19-CAR-T cells were executed from fresh blood donor by CD19-CAR-plasmid transfection, followed by the stimulation with X-ray-irradiated K562 feeder cells. The function of produced CAR-T cells was checked by their ability to kill Daudi cells. X-ray-irradiation inhibited the propagation and viability of K562 cells in a dose- and time-dependent manner. Interestingly, CAR-T-stimulating effectors were remained on the surface of X-ray-irradiated K562 cells. CD-19-CAR-T cells were produced successfully, suggested by number of CAR-positive cells in transfected and stimulated population, compared to un-transfected group. Lastly, our data showed that engineered CAR-T cells effectively killed Daudi cells. Our data demonstrated the efficacy of X-ray on deactivation K562 feeder cells which subsequently stimulated and expanded functional CAR-T cells. Thus, X-ray can be used as an alternative to inactivate K562 cells prior to using as a feeder of CAR-T cells. Elsevier 2022-12-01 /pmc/articles/PMC9719861/ /pubmed/36478893 http://dx.doi.org/10.1016/j.bbrep.2022.101399 Text en © 2022 The Authors. Published by Elsevier B.V. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Short Communication
Bui, Khac Cuong
Ho, Viet Hoanh
Nguyen, Hien Hanh
Dang, Thanh Chung
Ngo, Thu Hang
Nguyen, Thi Mai Ly
Nguyen, Linh Toan
Dang, Thuy Linh
Tran, Thanh Tung
Le, Quang Hoa
Pham, Hong Lam
Nguyen, Van Ba
Can, Van Mao
X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells
title X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells
title_full X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells
title_fullStr X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells
title_full_unstemmed X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells
title_short X-ray-irradiated K562 feeder cells for expansion of functional CAR-T cells
title_sort x-ray-irradiated k562 feeder cells for expansion of functional car-t cells
topic Short Communication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9719861/
https://www.ncbi.nlm.nih.gov/pubmed/36478893
http://dx.doi.org/10.1016/j.bbrep.2022.101399
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