Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer

BACKGROUND: Statins preferentially promote tumor-specific apoptosis by depleting isoprenoid such as farnesyl pyrophosphate and geranylgeranyl pyrophosphate. However, statins have not yet been approved for clinical cancer treatment due, in part, to poor understanding of molecular determinants on stat...

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Autores principales: Nam, Gi-Hoon, Kwon, Minsu, Jung, Hanul, Ko, Eunbyeol, Kim, Seong A, Choi, Yoonjeong, Song, Su Jeong, Kim, Seohyun, Lee, Yeji, Kim, Gi Beom, Han, Jihoon, Woo, Jiwan, Cho, Yakdol, Jeong, Cherlhyun, Park, Seung-Yoon, Roberts, Thomas M., Cho, Yong Beom, Kim, In-San
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2021
Materias:
Basic Tumor Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8327837/
https://www.ncbi.nlm.nih.gov/pubmed/34330763
http://dx.doi.org/10.1136/jitc-2021-002474
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author Nam, Gi-Hoon
Kwon, Minsu
Jung, Hanul
Ko, Eunbyeol
Kim, Seong A
Choi, Yoonjeong
Song, Su Jeong
Kim, Seohyun
Lee, Yeji
Kim, Gi Beom
Han, Jihoon
Woo, Jiwan
Cho, Yakdol
Jeong, Cherlhyun
Park, Seung-Yoon
Roberts, Thomas M.
Cho, Yong Beom
Kim, In-San
author_facet Nam, Gi-Hoon
Kwon, Minsu
Jung, Hanul
Ko, Eunbyeol
Kim, Seong A
Choi, Yoonjeong
Song, Su Jeong
Kim, Seohyun
Lee, Yeji
Kim, Gi Beom
Han, Jihoon
Woo, Jiwan
Cho, Yakdol
Jeong, Cherlhyun
Park, Seung-Yoon
Roberts, Thomas M.
Cho, Yong Beom
Kim, In-San
author_sort Nam, Gi-Hoon
collection PubMed
description BACKGROUND: Statins preferentially promote tumor-specific apoptosis by depleting isoprenoid such as farnesyl pyrophosphate and geranylgeranyl pyrophosphate. However, statins have not yet been approved for clinical cancer treatment due, in part, to poor understanding of molecular determinants on statin sensitivity. Here, we investigated the potential of statins to elicit enhanced immunogenicity of KRAS-mutant (KRAS(mut)) tumors. METHODS: The immunogenicity of treated cancer cells was determined by western blot, flow cytometry and confocal microscopy. The immunotherapeutic efficacy of mono or combination therapy using statin was assessed in KRAS(mut) tumor models, including syngeneic colorectal cancer and genetically engineered lung and pancreatic tumors. Using NanoString analysis, we analyzed how statin influenced the gene signatures associated with the antigen presentation of dendritic cells in vivo and evaluated whether statin could induce CD8+ T-cell immunity. Multiplex immunohistochemistry was performed to better understand the complicated tumor-immune microenvironment. RESULTS: Statin-mediated inhibition of KRAS prenylation provoked severe endoplasmic reticulum (ER) stress by attenuating the anti-ER stress effect of KRAS mutation, thereby resulting in the immunogenic cell death (ICD) of KRAS(mut) cancer cells. Moreover, statin-mediated ICD enhanced the cross-priming ability of dendritic cells, thereby provoking CD8+ T-cell immune responses against KRAS(mut) tumors. Combination therapy using statin and oxaliplatin, an ICD inducer, significantly enhanced the immunogenicity of KRAS(mut) tumors and promoted tumor-specific immunity in syngeneic and genetically engineered KRAS(mut) tumor models. Along with immune-checkpoint inhibitors, the abovementioned combination therapy overcame resistance to PD-1 blockade therapies, improving the survival rate of KRAS(mut) tumor models. CONCLUSIONS: Our findings suggest that KRAS mutation could be a molecular target for statins to elicit potent tumor-specific immunity.
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spelling pubmed-83278372021-08-19 Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer Nam, Gi-Hoon Kwon, Minsu Jung, Hanul Ko, Eunbyeol Kim, Seong A Choi, Yoonjeong Song, Su Jeong Kim, Seohyun Lee, Yeji Kim, Gi Beom Han, Jihoon Woo, Jiwan Cho, Yakdol Jeong, Cherlhyun Park, Seung-Yoon Roberts, Thomas M. Cho, Yong Beom Kim, In-San J Immunother Cancer Basic Tumor Immunology BACKGROUND: Statins preferentially promote tumor-specific apoptosis by depleting isoprenoid such as farnesyl pyrophosphate and geranylgeranyl pyrophosphate. However, statins have not yet been approved for clinical cancer treatment due, in part, to poor understanding of molecular determinants on statin sensitivity. Here, we investigated the potential of statins to elicit enhanced immunogenicity of KRAS-mutant (KRAS(mut)) tumors. METHODS: The immunogenicity of treated cancer cells was determined by western blot, flow cytometry and confocal microscopy. The immunotherapeutic efficacy of mono or combination therapy using statin was assessed in KRAS(mut) tumor models, including syngeneic colorectal cancer and genetically engineered lung and pancreatic tumors. Using NanoString analysis, we analyzed how statin influenced the gene signatures associated with the antigen presentation of dendritic cells in vivo and evaluated whether statin could induce CD8+ T-cell immunity. Multiplex immunohistochemistry was performed to better understand the complicated tumor-immune microenvironment. RESULTS: Statin-mediated inhibition of KRAS prenylation provoked severe endoplasmic reticulum (ER) stress by attenuating the anti-ER stress effect of KRAS mutation, thereby resulting in the immunogenic cell death (ICD) of KRAS(mut) cancer cells. Moreover, statin-mediated ICD enhanced the cross-priming ability of dendritic cells, thereby provoking CD8+ T-cell immune responses against KRAS(mut) tumors. Combination therapy using statin and oxaliplatin, an ICD inducer, significantly enhanced the immunogenicity of KRAS(mut) tumors and promoted tumor-specific immunity in syngeneic and genetically engineered KRAS(mut) tumor models. Along with immune-checkpoint inhibitors, the abovementioned combination therapy overcame resistance to PD-1 blockade therapies, improving the survival rate of KRAS(mut) tumor models. CONCLUSIONS: Our findings suggest that KRAS mutation could be a molecular target for statins to elicit potent tumor-specific immunity. BMJ Publishing Group 2021-07-30 /pmc/articles/PMC8327837/ /pubmed/34330763 http://dx.doi.org/10.1136/jitc-2021-002474 Text en © Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ. https://creativecommons.org/licenses/by-nc/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) .
spellingShingle Basic Tumor Immunology
Nam, Gi-Hoon
Kwon, Minsu
Jung, Hanul
Ko, Eunbyeol
Kim, Seong A
Choi, Yoonjeong
Song, Su Jeong
Kim, Seohyun
Lee, Yeji
Kim, Gi Beom
Han, Jihoon
Woo, Jiwan
Cho, Yakdol
Jeong, Cherlhyun
Park, Seung-Yoon
Roberts, Thomas M.
Cho, Yong Beom
Kim, In-San
Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer
title Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer
title_full Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer
title_fullStr Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer
title_full_unstemmed Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer
title_short Statin-mediated inhibition of RAS prenylation activates ER stress to enhance the immunogenicity of KRAS mutant cancer
title_sort statin-mediated inhibition of ras prenylation activates er stress to enhance the immunogenicity of kras mutant cancer
topic Basic Tumor Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8327837/
https://www.ncbi.nlm.nih.gov/pubmed/34330763
http://dx.doi.org/10.1136/jitc-2021-002474
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