Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models

BACKGROUND: Liver cancer (LC) is the most devastating disease affecting a large set of populations in the world. The mortality due to LC is escalating, indicating the lack of effective therapeutic options. Immunotherapeutic agents may play an important role against cancer cells. As immune cells, esp...

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Autores principales: Zafar, Sidra, Bai, Baogang, Guo, Jinlei, Muhammad, Syed Aun, Naqvi, Syeda Tahira Qousain, Shabbir, Muhammad Nauman, Imran, Imran, Shaikh, Rehan Sadiq, Ali, Amjad
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9173915/
https://www.ncbi.nlm.nih.gov/pubmed/35686237
http://dx.doi.org/10.1155/2022/4792374
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author Zafar, Sidra
Bai, Baogang
Guo, Jinlei
Muhammad, Syed Aun
Naqvi, Syeda Tahira Qousain
Shabbir, Muhammad Nauman
Imran, Imran
Shaikh, Rehan Sadiq
Ali, Amjad
author_facet Zafar, Sidra
Bai, Baogang
Guo, Jinlei
Muhammad, Syed Aun
Naqvi, Syeda Tahira Qousain
Shabbir, Muhammad Nauman
Imran, Imran
Shaikh, Rehan Sadiq
Ali, Amjad
author_sort Zafar, Sidra
collection PubMed
description BACKGROUND: Liver cancer (LC) is the most devastating disease affecting a large set of populations in the world. The mortality due to LC is escalating, indicating the lack of effective therapeutic options. Immunotherapeutic agents may play an important role against cancer cells. As immune cells, especially T lymphocytes, which are part of cancer immunology, the design of vaccine candidates for cytotoxic T lymphocytes may be an effective strategy for curing liver cancer. RESULTS: In our study, based on an immunoinformatics approach, we predicted potential T cell epitopes of MHC class I molecules using integrated steps of data retrieval, screening of antigenic proteins, functional analysis, peptide synthesis, and experimental in vivo investigations. We predicted the binding affinity of epitopes LLECADDRADLAKY, VSEHRIQDKDGLFY, and EYILSLEELVNGMY of LC membrane-bounded extracellular proteins including butyrophilin-like protein-2 (BTNL2), glypican-3 (GPC3), and serum albumin (ALB), respectively, with MHC class I molecules (allele: HLA-A∗01:01). These T cell epitopes rely on the level of their binding energy and antigenic properties. We designed and constructed a trivalent immunogenic model by conjugating these epitopes with linkers to activate cytotoxic T cells. For validation, the nonspecific hematological assays showed a significant rise in the count of white blood cells (5 × 10(9)/l), lymphocytes (13 × 10(9)/l), and granulocytes (5 × 10(9)/l) compared to the control after administration of trivalent peptides. Specific immunoassays including granzyme B and IgG ELISA exhibited the significant concentration of these effector molecules in blood serum, indicating the activity of cytotoxic T cells. Granzyme concentration increased to 1050 pg/ml at the second booster dose compared to the control (95 pg/ml), while the concentration of IgG raised to 6 g/l compared to the control (2 g/l). CONCLUSION: We concluded that a potential therapeutic trivalent vaccine can activate and modulate the immune system to cure liver cancer on the basis of significant outcomes of specific and nonspecific assays.
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spelling pubmed-91739152022-06-08 Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models Zafar, Sidra Bai, Baogang Guo, Jinlei Muhammad, Syed Aun Naqvi, Syeda Tahira Qousain Shabbir, Muhammad Nauman Imran, Imran Shaikh, Rehan Sadiq Ali, Amjad Biomed Res Int Research Article BACKGROUND: Liver cancer (LC) is the most devastating disease affecting a large set of populations in the world. The mortality due to LC is escalating, indicating the lack of effective therapeutic options. Immunotherapeutic agents may play an important role against cancer cells. As immune cells, especially T lymphocytes, which are part of cancer immunology, the design of vaccine candidates for cytotoxic T lymphocytes may be an effective strategy for curing liver cancer. RESULTS: In our study, based on an immunoinformatics approach, we predicted potential T cell epitopes of MHC class I molecules using integrated steps of data retrieval, screening of antigenic proteins, functional analysis, peptide synthesis, and experimental in vivo investigations. We predicted the binding affinity of epitopes LLECADDRADLAKY, VSEHRIQDKDGLFY, and EYILSLEELVNGMY of LC membrane-bounded extracellular proteins including butyrophilin-like protein-2 (BTNL2), glypican-3 (GPC3), and serum albumin (ALB), respectively, with MHC class I molecules (allele: HLA-A∗01:01). These T cell epitopes rely on the level of their binding energy and antigenic properties. We designed and constructed a trivalent immunogenic model by conjugating these epitopes with linkers to activate cytotoxic T cells. For validation, the nonspecific hematological assays showed a significant rise in the count of white blood cells (5 × 10(9)/l), lymphocytes (13 × 10(9)/l), and granulocytes (5 × 10(9)/l) compared to the control after administration of trivalent peptides. Specific immunoassays including granzyme B and IgG ELISA exhibited the significant concentration of these effector molecules in blood serum, indicating the activity of cytotoxic T cells. Granzyme concentration increased to 1050 pg/ml at the second booster dose compared to the control (95 pg/ml), while the concentration of IgG raised to 6 g/l compared to the control (2 g/l). CONCLUSION: We concluded that a potential therapeutic trivalent vaccine can activate and modulate the immune system to cure liver cancer on the basis of significant outcomes of specific and nonspecific assays. Hindawi 2022-05-31 /pmc/articles/PMC9173915/ /pubmed/35686237 http://dx.doi.org/10.1155/2022/4792374 Text en Copyright © 2022 Sidra Zafar et al. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Zafar, Sidra
Bai, Baogang
Guo, Jinlei
Muhammad, Syed Aun
Naqvi, Syeda Tahira Qousain
Shabbir, Muhammad Nauman
Imran, Imran
Shaikh, Rehan Sadiq
Ali, Amjad
Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models
title Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models
title_full Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models
title_fullStr Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models
title_full_unstemmed Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models
title_short Experimental Study of Potential CD8(+) Trivalent Synthetic Peptides for Liver Cancer Vaccine Development Using Sprague Dawley Rat Models
title_sort experimental study of potential cd8(+) trivalent synthetic peptides for liver cancer vaccine development using sprague dawley rat models
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9173915/
https://www.ncbi.nlm.nih.gov/pubmed/35686237
http://dx.doi.org/10.1155/2022/4792374
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