Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG

Natural Killer cell receptors allow this heterogeneous immune population to efficiently fight both tumors and infection, so their use as immunotherapy agents is an active field of research. Cytokine activation, particularly by myeloid cell-derived IL15, can induce potent NK anti-tumor responses. Whi...

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Main Authors: Gloria Esteso, Nacho Aguiló, Esther Julián, Omodele Ashiru, Mei. M. Ho, Carlos Martín, Mar Valés-Gómez
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-02-01
Series:Frontiers in Immunology
Subjects:
Online Access:https://www.frontiersin.org/articles/10.3389/fimmu.2021.622995/full
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spelling doaj-be1ae3a0c3704bdf810a75ce97369ceb2021-02-23T06:04:00ZengFrontiers Media S.A.Frontiers in Immunology1664-32242021-02-011210.3389/fimmu.2021.622995622995Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCGGloria Esteso0Nacho Aguiló1Esther Julián2Omodele Ashiru3Mei. M. Ho4Carlos Martín5Mar Valés-Gómez6Department of Immunology and Oncology, Spanish National Centre for Biotechnology (CNB), Consejo Superior de Investigaciones Científicas (CSIC), Madrid, SpainMycobacteria Genetics Group, University of Zaragoza Medical School, IIS Aragón, CIBERES, Zaragoza, SpainDepartament de Genètica i Microbiologia, Facultat de Biociències, Universitat Autònoma de Barcelona, Barcelona, SpainCustom Solutions Department, Bacteriology Division, Medicines and Healthcare Products Regulatory Agency – National Institute for Biological Standards and Control (MHRA-NIBSC), Potters Bar, United KingdomCustom Solutions Department, Bacteriology Division, Medicines and Healthcare Products Regulatory Agency – National Institute for Biological Standards and Control (MHRA-NIBSC), Potters Bar, United KingdomMycobacteria Genetics Group, University of Zaragoza Medical School, IIS Aragón, CIBERES, Zaragoza, SpainDepartment of Immunology and Oncology, Spanish National Centre for Biotechnology (CNB), Consejo Superior de Investigaciones Científicas (CSIC), Madrid, SpainNatural Killer cell receptors allow this heterogeneous immune population to efficiently fight both tumors and infection, so their use as immunotherapy agents is an active field of research. Cytokine activation, particularly by myeloid cell-derived IL15, can induce potent NK anti-tumor responses. While studying the mechanism of action of intravesical instillations of Bacille Calmette-Guérin (BCG) as therapy for patients with high risk non-muscle invasive bladder cancer, we showed that BCG can activate a cytotoxic CD56bright NK cell population which efficiently recognized bladder cancer cells. This pioneer immunotherapy provides an invaluable model to understand the role of different immune populations in tumor elimination. However, during the propagation of BCG worldwide a large number of genetically diverse BCG substrains developed. Here, we investigated the capacity of different BCG substrains to promote NK cell activation and confirmed that they were able to activate lymphocytes. Tice, Connaught and Moreau were the substrains with a stronger NK activation effect as measured by CD56 upregulation. Surprisingly, dead mycobacteria also stimulated PBMC cultures and we further demonstrate here that subcellular fractions of BCG-Tice, in the absence of live mycobacteria, could also induce an NK cell response. Lipids from BCG-Tice, but not from Mycobacterium bovis, stimulated NK cell activation and degranulation, whereas the aqueous fraction of either bacteria did not activate lymphocytes. However, delipidated BCG-Tice bacteria were able to activate effector cells (CD3+CD56+ and NK, CD3-CD56+). These data demonstrate that different components of mycobacteria can stimulate different immune subpopulations resulting in phenotypes suitable for cancer elimination.https://www.frontiersin.org/articles/10.3389/fimmu.2021.622995/fullcancer immunologyBCG strainsNK activationCD56brightbladder cancermycobacterial fractions
collection DOAJ
language English
format Article
sources DOAJ
author Gloria Esteso
Nacho Aguiló
Esther Julián
Omodele Ashiru
Mei. M. Ho
Carlos Martín
Mar Valés-Gómez
spellingShingle Gloria Esteso
Nacho Aguiló
Esther Julián
Omodele Ashiru
Mei. M. Ho
Carlos Martín
Mar Valés-Gómez
Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG
Frontiers in Immunology
cancer immunology
BCG strains
NK activation
CD56bright
bladder cancer
mycobacterial fractions
author_facet Gloria Esteso
Nacho Aguiló
Esther Julián
Omodele Ashiru
Mei. M. Ho
Carlos Martín
Mar Valés-Gómez
author_sort Gloria Esteso
title Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG
title_short Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG
title_full Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG
title_fullStr Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG
title_full_unstemmed Natural Killer Anti-Tumor Activity Can Be Achieved by In Vitro Incubation With Heat-Killed BCG
title_sort natural killer anti-tumor activity can be achieved by in vitro incubation with heat-killed bcg
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2021-02-01
description Natural Killer cell receptors allow this heterogeneous immune population to efficiently fight both tumors and infection, so their use as immunotherapy agents is an active field of research. Cytokine activation, particularly by myeloid cell-derived IL15, can induce potent NK anti-tumor responses. While studying the mechanism of action of intravesical instillations of Bacille Calmette-Guérin (BCG) as therapy for patients with high risk non-muscle invasive bladder cancer, we showed that BCG can activate a cytotoxic CD56bright NK cell population which efficiently recognized bladder cancer cells. This pioneer immunotherapy provides an invaluable model to understand the role of different immune populations in tumor elimination. However, during the propagation of BCG worldwide a large number of genetically diverse BCG substrains developed. Here, we investigated the capacity of different BCG substrains to promote NK cell activation and confirmed that they were able to activate lymphocytes. Tice, Connaught and Moreau were the substrains with a stronger NK activation effect as measured by CD56 upregulation. Surprisingly, dead mycobacteria also stimulated PBMC cultures and we further demonstrate here that subcellular fractions of BCG-Tice, in the absence of live mycobacteria, could also induce an NK cell response. Lipids from BCG-Tice, but not from Mycobacterium bovis, stimulated NK cell activation and degranulation, whereas the aqueous fraction of either bacteria did not activate lymphocytes. However, delipidated BCG-Tice bacteria were able to activate effector cells (CD3+CD56+ and NK, CD3-CD56+). These data demonstrate that different components of mycobacteria can stimulate different immune subpopulations resulting in phenotypes suitable for cancer elimination.
topic cancer immunology
BCG strains
NK activation
CD56bright
bladder cancer
mycobacterial fractions
url https://www.frontiersin.org/articles/10.3389/fimmu.2021.622995/full
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