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In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer

BACKGROUND: Breast cancer is one of the most prevalent cancers among women. Common cancer treatment methods are not effective enough, and there is a need for a more efficient treatment procedure. Cancer vaccine is a novel immunotherapy method that stimulates humoral and/or cellular immunity against...

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Autores principales: Taheri-Anganeh, Mortaza, Amiri, Ahmad, Movahedpour, Ahmad, Khatami, Seyyed Hossein, Ghasemi, Younes, Savardashtaki, Amir, Mostafavi-Pour, Zohreh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Pasteur Institute of Iran 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7275624/
https://www.ncbi.nlm.nih.gov/pubmed/31952435
http://dx.doi.org/10.29252/ibj.24.3.173
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author Taheri-Anganeh, Mortaza
Amiri, Ahmad
Movahedpour, Ahmad
Khatami, Seyyed Hossein
Ghasemi, Younes
Savardashtaki, Amir
Mostafavi-Pour, Zohreh
author_facet Taheri-Anganeh, Mortaza
Amiri, Ahmad
Movahedpour, Ahmad
Khatami, Seyyed Hossein
Ghasemi, Younes
Savardashtaki, Amir
Mostafavi-Pour, Zohreh
author_sort Taheri-Anganeh, Mortaza
collection PubMed
description BACKGROUND: Breast cancer is one of the most prevalent cancers among women. Common cancer treatment methods are not effective enough, and there is a need for a more efficient treatment procedure. Cancer vaccine is a novel immunotherapy method that stimulates humoral and/or cellular immunity against cancer. PLAC1 is a cancer/testis antigen, prevalent in breast cancer and rarely found in normal tissues. FliC, as a bacterial adjuvant, when fused to PLAC1 can elicit humoral and cellular responses. Therefore, PLAC1-fliC is a chimeric protein, which can be considered a suitable candidate against breast cancer. METHODS: ProtParam was used to evaluate the physicochemical properties of PLAC1-fliC. Second structures were determined using the GOR V server. PLAC1-fliC 3D structure was modeled by Phyre2, and it was refined using GalaxyWEB. The refined model was submitted to RAMPAGE, PROCHECK, and ProSA-web for validation. Antigenicity and allergenicity of the construct were predicted by ANTIGENpro, VaxiJen, AllergenFP, and SDAP databases. Then MHC-I- and MHC-II-binding epitopes of PLAC1-fliC were forecasted by NetMHC 4.0 and NetMHCII 2.3 Servers. Finally, Ellipro and CTLpred were employed to predict B-cell and CTL epitopes. RESULTS: The construct was evaluated as a stable fusion protein, which could be antigenic and could stimulate B and T cells against breast cancer. CONCLUSION: PLAC1-fliC, as a cancer vaccine candidate, might be suitable and specific for breast cancer, which could evoke humoral and cellular immunity against this type of tumor.
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spelling pubmed-72756242020-06-15 In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer Taheri-Anganeh, Mortaza Amiri, Ahmad Movahedpour, Ahmad Khatami, Seyyed Hossein Ghasemi, Younes Savardashtaki, Amir Mostafavi-Pour, Zohreh Iran Biomed J Full Length BACKGROUND: Breast cancer is one of the most prevalent cancers among women. Common cancer treatment methods are not effective enough, and there is a need for a more efficient treatment procedure. Cancer vaccine is a novel immunotherapy method that stimulates humoral and/or cellular immunity against cancer. PLAC1 is a cancer/testis antigen, prevalent in breast cancer and rarely found in normal tissues. FliC, as a bacterial adjuvant, when fused to PLAC1 can elicit humoral and cellular responses. Therefore, PLAC1-fliC is a chimeric protein, which can be considered a suitable candidate against breast cancer. METHODS: ProtParam was used to evaluate the physicochemical properties of PLAC1-fliC. Second structures were determined using the GOR V server. PLAC1-fliC 3D structure was modeled by Phyre2, and it was refined using GalaxyWEB. The refined model was submitted to RAMPAGE, PROCHECK, and ProSA-web for validation. Antigenicity and allergenicity of the construct were predicted by ANTIGENpro, VaxiJen, AllergenFP, and SDAP databases. Then MHC-I- and MHC-II-binding epitopes of PLAC1-fliC were forecasted by NetMHC 4.0 and NetMHCII 2.3 Servers. Finally, Ellipro and CTLpred were employed to predict B-cell and CTL epitopes. RESULTS: The construct was evaluated as a stable fusion protein, which could be antigenic and could stimulate B and T cells against breast cancer. CONCLUSION: PLAC1-fliC, as a cancer vaccine candidate, might be suitable and specific for breast cancer, which could evoke humoral and cellular immunity against this type of tumor. Pasteur Institute of Iran 2020-05 2019-11-18 /pmc/articles/PMC7275624/ /pubmed/31952435 http://dx.doi.org/10.29252/ibj.24.3.173 Text en This is an Open Access article distributed under the terms of the Creative Commons Attribution License, (http://creativecommons.org/licenses/by/3.0/) which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Full Length
Taheri-Anganeh, Mortaza
Amiri, Ahmad
Movahedpour, Ahmad
Khatami, Seyyed Hossein
Ghasemi, Younes
Savardashtaki, Amir
Mostafavi-Pour, Zohreh
In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer
title In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer
title_full In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer
title_fullStr In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer
title_full_unstemmed In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer
title_short In silico Evaluation of PLAC1-fliC As a Chimeric Vaccine against Breast Cancer
title_sort in silico evaluation of plac1-flic as a chimeric vaccine against breast cancer
topic Full Length
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7275624/
https://www.ncbi.nlm.nih.gov/pubmed/31952435
http://dx.doi.org/10.29252/ibj.24.3.173
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