Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach

Human Parainfluenza Virus (HPIV) Type-1, which is an anti-sense ribonucleic acid (RNA) virus belonging to the paramyxoviridae family, induces upper and lower respiratory tract infections. The infections caused by the HPIV Type-1 virus are usually confined to northwestern regions of America. HPIV-1 c...

Descripción completa

Detalles Bibliográficos
Autores principales: Naveed, Muhammad, Yaseen, Allah Rakha, Khalid, Hira, Ali, Urooj, Rabaan, Ali A., Garout, Mohamed, Halwani, Muhammad A., Al Mutair, Abbas, Alhumaid, Saad, Al Alawi, Zainab, Alhashem, Yousef N., Ahmed, Naveed, Yean, Chan Yean
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9228812/
https://www.ncbi.nlm.nih.gov/pubmed/35746477
http://dx.doi.org/10.3390/vaccines10060869
_version_ 1784734573697957888
author Naveed, Muhammad
Yaseen, Allah Rakha
Khalid, Hira
Ali, Urooj
Rabaan, Ali A.
Garout, Mohamed
Halwani, Muhammad A.
Al Mutair, Abbas
Alhumaid, Saad
Al Alawi, Zainab
Alhashem, Yousef N.
Ahmed, Naveed
Yean, Chan Yean
author_facet Naveed, Muhammad
Yaseen, Allah Rakha
Khalid, Hira
Ali, Urooj
Rabaan, Ali A.
Garout, Mohamed
Halwani, Muhammad A.
Al Mutair, Abbas
Alhumaid, Saad
Al Alawi, Zainab
Alhashem, Yousef N.
Ahmed, Naveed
Yean, Chan Yean
author_sort Naveed, Muhammad
collection PubMed
description Human Parainfluenza Virus (HPIV) Type-1, which is an anti-sense ribonucleic acid (RNA) virus belonging to the paramyxoviridae family, induces upper and lower respiratory tract infections. The infections caused by the HPIV Type-1 virus are usually confined to northwestern regions of America. HPIV-1 causes infections through the virulence of the hemagglutinin-neuraminidase (HN) protein, which plays a key role in the attachment of the viral particle with the host’s receptor cells. To the best of our knowledge, there is no effective antiviral drugs or vaccines being developed to combat the infection caused by HPIV-1. In the current study, a multiple epitope-based vaccine was designed against HPIV-1 by taking the viral HN protein as a probable vaccine candidate. The multiple epitopes were selected in accordance with their allergenicity, antigenicity and toxicity scoring. The determined epitopes of the HN protein were connected simultaneously using specific conjugates along with an adjuvant to construct the subunit vaccine, with an antigenicity score of 0.6406. The constructed vaccine model was docked with various Toll-like Receptors (TLRs) and was computationally cloned in a pET28a (+) vector to analyze the expression of vaccine sequence in the biological system. Immune stimulations carried out by the C-ImmSim Server showed an excellent result of the body’s defense system against the constructed vaccine model. The AllerTop tool predicted that the construct was non-allergen with and without the adjuvant sequence, and the VaxiJen 2.0 with 0.4 threshold predicted that the construct was antigenic, while the Toxinpred predicted that the construct was non-toxic. Protparam results showed that the selected protein was stable with 36.48 instability index (II) scores. The Grand average of Hydropathicity or GRAVY score indicated that the constructed protein was hydrophilic in nature. Aliphatic index values (93.53) confirmed that the construct was thermostable. This integrated computational approach shows that the constructed vaccine model has a potential to combat laryngotracheobronchitis infections caused by HPIV-I.
format Online
Article
Text
id pubmed-9228812
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-92288122022-06-25 Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach Naveed, Muhammad Yaseen, Allah Rakha Khalid, Hira Ali, Urooj Rabaan, Ali A. Garout, Mohamed Halwani, Muhammad A. Al Mutair, Abbas Alhumaid, Saad Al Alawi, Zainab Alhashem, Yousef N. Ahmed, Naveed Yean, Chan Yean Vaccines (Basel) Article Human Parainfluenza Virus (HPIV) Type-1, which is an anti-sense ribonucleic acid (RNA) virus belonging to the paramyxoviridae family, induces upper and lower respiratory tract infections. The infections caused by the HPIV Type-1 virus are usually confined to northwestern regions of America. HPIV-1 causes infections through the virulence of the hemagglutinin-neuraminidase (HN) protein, which plays a key role in the attachment of the viral particle with the host’s receptor cells. To the best of our knowledge, there is no effective antiviral drugs or vaccines being developed to combat the infection caused by HPIV-1. In the current study, a multiple epitope-based vaccine was designed against HPIV-1 by taking the viral HN protein as a probable vaccine candidate. The multiple epitopes were selected in accordance with their allergenicity, antigenicity and toxicity scoring. The determined epitopes of the HN protein were connected simultaneously using specific conjugates along with an adjuvant to construct the subunit vaccine, with an antigenicity score of 0.6406. The constructed vaccine model was docked with various Toll-like Receptors (TLRs) and was computationally cloned in a pET28a (+) vector to analyze the expression of vaccine sequence in the biological system. Immune stimulations carried out by the C-ImmSim Server showed an excellent result of the body’s defense system against the constructed vaccine model. The AllerTop tool predicted that the construct was non-allergen with and without the adjuvant sequence, and the VaxiJen 2.0 with 0.4 threshold predicted that the construct was antigenic, while the Toxinpred predicted that the construct was non-toxic. Protparam results showed that the selected protein was stable with 36.48 instability index (II) scores. The Grand average of Hydropathicity or GRAVY score indicated that the constructed protein was hydrophilic in nature. Aliphatic index values (93.53) confirmed that the construct was thermostable. This integrated computational approach shows that the constructed vaccine model has a potential to combat laryngotracheobronchitis infections caused by HPIV-I. MDPI 2022-05-29 /pmc/articles/PMC9228812/ /pubmed/35746477 http://dx.doi.org/10.3390/vaccines10060869 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Naveed, Muhammad
Yaseen, Allah Rakha
Khalid, Hira
Ali, Urooj
Rabaan, Ali A.
Garout, Mohamed
Halwani, Muhammad A.
Al Mutair, Abbas
Alhumaid, Saad
Al Alawi, Zainab
Alhashem, Yousef N.
Ahmed, Naveed
Yean, Chan Yean
Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach
title Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach
title_full Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach
title_fullStr Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach
title_full_unstemmed Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach
title_short Execution and Design of an Anti HPIV-1 Vaccine with Multiple Epitopes Triggering Innate and Adaptive Immune Responses: An Immunoinformatic Approach
title_sort execution and design of an anti hpiv-1 vaccine with multiple epitopes triggering innate and adaptive immune responses: an immunoinformatic approach
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9228812/
https://www.ncbi.nlm.nih.gov/pubmed/35746477
http://dx.doi.org/10.3390/vaccines10060869
work_keys_str_mv AT naveedmuhammad executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT yaseenallahrakha executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT khalidhira executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT aliurooj executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT rabaanalia executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT garoutmohamed executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT halwanimuhammada executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT almutairabbas executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT alhumaidsaad executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT alalawizainab executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT alhashemyousefn executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT ahmednaveed executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach
AT yeanchanyean executionanddesignofanantihpiv1vaccinewithmultipleepitopestriggeringinnateandadaptiveimmuneresponsesanimmunoinformaticapproach

Ejemplares similares