LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling

BACKGROUND: The genesis of SMAC mimetic drugs is founded on the observation that many cancers amplify IAP proteins to facilitate their survival, and therefore removal of these pathways would re-sensitize the cells towards apoptosis. It has become increasingly clear that SMAC mimetics also interface...

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Autores principales: Afsahi, Arya, Silvestri, Christopher M., Moore, Allyson E., Graham, Carly F., Bacchiochi, Kaylyn, St-Jean, Martine, Baker, Christopher L., Korneluk, Robert G., Beug, Shawn T., LaCasse, Eric C., Bramson, Jonathan L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10150108/
https://www.ncbi.nlm.nih.gov/pubmed/37138866
http://dx.doi.org/10.3389/fimmu.2023.1179827
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author Afsahi, Arya
Silvestri, Christopher M.
Moore, Allyson E.
Graham, Carly F.
Bacchiochi, Kaylyn
St-Jean, Martine
Baker, Christopher L.
Korneluk, Robert G.
Beug, Shawn T.
LaCasse, Eric C.
Bramson, Jonathan L.
author_facet Afsahi, Arya
Silvestri, Christopher M.
Moore, Allyson E.
Graham, Carly F.
Bacchiochi, Kaylyn
St-Jean, Martine
Baker, Christopher L.
Korneluk, Robert G.
Beug, Shawn T.
LaCasse, Eric C.
Bramson, Jonathan L.
author_sort Afsahi, Arya
collection PubMed
description BACKGROUND: The genesis of SMAC mimetic drugs is founded on the observation that many cancers amplify IAP proteins to facilitate their survival, and therefore removal of these pathways would re-sensitize the cells towards apoptosis. It has become increasingly clear that SMAC mimetics also interface with the immune system in a modulatory manner. Suppression of IAP function by SMAC mimetics activates the non-canonical NF-κB pathway which can augment T cell function, opening the possibility of using SMAC mimetics to enhance immunotherapeutics. METHODS: We have investigated the SMAC mimetic LCL161, which promotes degradation of cIAP-1 and cIAP-2, as an agent for delivering transient costimulation to engineered BMCA-specific human TAC T cells. In doing so we also sought to understand the cellular and molecular effects of LCL161 on T cell biology. RESULTS: LCL161 activated the non-canonical NF-κB pathway and enhanced antigen-driven TAC T cell proliferation and survival. Transcriptional profiling from TAC T cells treated with LCL161 revealed differential expression of costimulatory and apoptosis-related proteins, namely CD30 and FAIM3. We hypothesized that regulation of these genes by LCL161 may influence the drug’s effects on T cells. We reversed the differential expression through genetic engineering and observed impaired costimulation by LCL161, particularly when CD30 was deleted. While LCL161 can provide a costimulatory signal to TAC T cells following exposure to isolated antigen, we did not observe a similar pattern when TAC T cells were stimulated with myeloma cells expressing the target antigen. We questioned whether FasL expression by myeloma cells may antagonize the costimulatory effects of LCL161. Fas-KO TAC T cells displayed superior expansion following antigen stimulation in the presence of LCL161, suggesting a role for Fas-related T cell death in limiting the magnitude of the T cell response to antigen in the presence of LCL161. CONCLUSIONS: Our results demonstrate that LCL161 provides costimulation to TAC T cells exposed to antigen alone, however LCL161 did not enhance TAC T cell anti-tumor function when challenged with myeloma cells and may be limited due to sensitization of T cells towards Fas-mediated apoptosis.
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spelling pubmed-101501082023-05-02 LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling Afsahi, Arya Silvestri, Christopher M. Moore, Allyson E. Graham, Carly F. Bacchiochi, Kaylyn St-Jean, Martine Baker, Christopher L. Korneluk, Robert G. Beug, Shawn T. LaCasse, Eric C. Bramson, Jonathan L. Front Immunol Immunology BACKGROUND: The genesis of SMAC mimetic drugs is founded on the observation that many cancers amplify IAP proteins to facilitate their survival, and therefore removal of these pathways would re-sensitize the cells towards apoptosis. It has become increasingly clear that SMAC mimetics also interface with the immune system in a modulatory manner. Suppression of IAP function by SMAC mimetics activates the non-canonical NF-κB pathway which can augment T cell function, opening the possibility of using SMAC mimetics to enhance immunotherapeutics. METHODS: We have investigated the SMAC mimetic LCL161, which promotes degradation of cIAP-1 and cIAP-2, as an agent for delivering transient costimulation to engineered BMCA-specific human TAC T cells. In doing so we also sought to understand the cellular and molecular effects of LCL161 on T cell biology. RESULTS: LCL161 activated the non-canonical NF-κB pathway and enhanced antigen-driven TAC T cell proliferation and survival. Transcriptional profiling from TAC T cells treated with LCL161 revealed differential expression of costimulatory and apoptosis-related proteins, namely CD30 and FAIM3. We hypothesized that regulation of these genes by LCL161 may influence the drug’s effects on T cells. We reversed the differential expression through genetic engineering and observed impaired costimulation by LCL161, particularly when CD30 was deleted. While LCL161 can provide a costimulatory signal to TAC T cells following exposure to isolated antigen, we did not observe a similar pattern when TAC T cells were stimulated with myeloma cells expressing the target antigen. We questioned whether FasL expression by myeloma cells may antagonize the costimulatory effects of LCL161. Fas-KO TAC T cells displayed superior expansion following antigen stimulation in the presence of LCL161, suggesting a role for Fas-related T cell death in limiting the magnitude of the T cell response to antigen in the presence of LCL161. CONCLUSIONS: Our results demonstrate that LCL161 provides costimulation to TAC T cells exposed to antigen alone, however LCL161 did not enhance TAC T cell anti-tumor function when challenged with myeloma cells and may be limited due to sensitization of T cells towards Fas-mediated apoptosis. Frontiers Media S.A. 2023-04-17 /pmc/articles/PMC10150108/ /pubmed/37138866 http://dx.doi.org/10.3389/fimmu.2023.1179827 Text en Copyright © 2023 Afsahi, Silvestri, Moore, Graham, Bacchiochi, St-Jean, Baker, Korneluk, Beug, LaCasse and Bramson https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Afsahi, Arya
Silvestri, Christopher M.
Moore, Allyson E.
Graham, Carly F.
Bacchiochi, Kaylyn
St-Jean, Martine
Baker, Christopher L.
Korneluk, Robert G.
Beug, Shawn T.
LaCasse, Eric C.
Bramson, Jonathan L.
LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling
title LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling
title_full LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling
title_fullStr LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling
title_full_unstemmed LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling
title_short LCL161 enhances expansion and survival of engineered anti-tumor T cells but is restricted by death signaling
title_sort lcl161 enhances expansion and survival of engineered anti-tumor t cells but is restricted by death signaling
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10150108/
https://www.ncbi.nlm.nih.gov/pubmed/37138866
http://dx.doi.org/10.3389/fimmu.2023.1179827
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