Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii: A Computational-Based Subtractive Proteomics Approach

Muhammad Naveed; Jawad Ul Hassan; Muneeb Ahmad; Nida Naeem; Muhammad Saad Mughal; Ali A. Rabaan; Mohammed Aljeldah; Basim R.Al Shammari; Mohammed Alissa; Amal A. Sabour; Rana A. Alaeq; Maha A. Alshiekheid; Safaa A. Turkistani; Abdirahman Hussein Elmi; Naveed Ahmed

doi:10.3390/medicina58101356

Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii: A Computational-Based Subtractive Proteomics Approach

Muhammad Naveed
, Jawad Ul Hassan
, Muneeb Ahmad
, Nida Naeem
, Muhammad Saad Mughal
, Ali A. Rabaan
, Mohammed Aljeldah
, Basim R.Al Shammari
, Mohammed Alissa
, Amal A. Sabour
, Rana A. Alaeq
, Maha A. Alshiekheid
, Safaa A. Turkistani
, Abdirahman Hussein Elmi
, Naveed Ahmed

Medical Laboratory Sciences

Research output: Contribution to journal › Article › peer-review

13 Scopus citations

Abstract

Background and Objectives: Citrobacter freundii (C. freundii) is an emerging and opportunistic Gram-negative bacteria of the human gastrointestinal tract associated with nosocomial and severe respiratory tract infections. It has also been associated with pneumonia, bloodstream, and urinary tract infections. Intrinsic and adaptive virulence characteristics of C. freundii have become a significant source of diarrheal infections and food poisoning among immune-compromised patients and newborns. Impulsive usage of antibiotics and these adaptive virulence characteristics has modulated the C. freundii into multidrug-resistant (MDR) bacteria. Conventional approaches are futile against MDR C. freundii. Materials and Methods: The current study exploits the modern computational-based vaccine design approach to treat infections related to MDR C. freundii. A whole proteome of C. freundii (strain: CWH001) was retrieved to screen pathogenic and nonhomologous proteins. Six proteins were shortlisted for the selection of putative epitopes for vaccine construct. Highly antigenic, nonallergen, and nontoxic eleven B-cell, HTL, and TCL epitopes were selected for mRNA- and peptide-based multi-epitope vaccine construct. Secondary and tertiary structures of the multi-epitope vaccine (MEVC) were designed, refined, and validated. Results: Evaluation of population coverage of MHC-I and MHC-II alleles were 72% and 90%, respectively. Docking MEVC with TLR-3 receptor with the binding affinity of 21.46 (kcal/mol) occurred through the mmGBSA process. Further validations include codon optimization with an enhanced CAI value of 0.95 and GC content of about 51%. Immune stimulation and molecular dynamic simulation ensure the antibody production upon antigen interaction with the host and stability of the MEVC construct, respectively. Conclusions: These interpretations propose a new strategy to combat MDR C. freundii. Further, in vivo and in vitro trials of this vaccine will be valuable in combating MDR pathogens.

Original language	English
Article number	1356
Journal	Medicina (Lithuania)
Volume	58
Issue number	10
DOIs	https://doi.org/10.3390/medicina58101356
State	Published - Oct 2022

Keywords

AMR
antibiotic resistance
bioinformatics
global hazards
health issues

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3390/medicina58101356

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Naveed, M., Hassan, J. U., Ahmad, M., Naeem, N., Mughal, M. S., Rabaan, A. A., Aljeldah, M., Shammari, B. R. A., Alissa, M., Sabour, A. A., Alaeq, R. A., Alshiekheid, M. A., Turkistani, S. A., Elmi, A. H., & Ahmed, N. (2022). Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii: A Computational-Based Subtractive Proteomics Approach. Medicina (Lithuania), 58(10), Article 1356. https://doi.org/10.3390/medicina58101356

@article{6b39673514b7406ca8050b7e0d76eaac,

title = "Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii: A Computational-Based Subtractive Proteomics Approach",

abstract = "Background and Objectives: Citrobacter freundii (C. freundii) is an emerging and opportunistic Gram-negative bacteria of the human gastrointestinal tract associated with nosocomial and severe respiratory tract infections. It has also been associated with pneumonia, bloodstream, and urinary tract infections. Intrinsic and adaptive virulence characteristics of C. freundii have become a significant source of diarrheal infections and food poisoning among immune-compromised patients and newborns. Impulsive usage of antibiotics and these adaptive virulence characteristics has modulated the C. freundii into multidrug-resistant (MDR) bacteria. Conventional approaches are futile against MDR C. freundii. Materials and Methods: The current study exploits the modern computational-based vaccine design approach to treat infections related to MDR C. freundii. A whole proteome of C. freundii (strain: CWH001) was retrieved to screen pathogenic and nonhomologous proteins. Six proteins were shortlisted for the selection of putative epitopes for vaccine construct. Highly antigenic, nonallergen, and nontoxic eleven B-cell, HTL, and TCL epitopes were selected for mRNA- and peptide-based multi-epitope vaccine construct. Secondary and tertiary structures of the multi-epitope vaccine (MEVC) were designed, refined, and validated. Results: Evaluation of population coverage of MHC-I and MHC-II alleles were 72\% and 90\%, respectively. Docking MEVC with TLR-3 receptor with the binding affinity of 21.46 (kcal/mol) occurred through the mmGBSA process. Further validations include codon optimization with an enhanced CAI value of 0.95 and GC content of about 51\%. Immune stimulation and molecular dynamic simulation ensure the antibody production upon antigen interaction with the host and stability of the MEVC construct, respectively. Conclusions: These interpretations propose a new strategy to combat MDR C. freundii. Further, in vivo and in vitro trials of this vaccine will be valuable in combating MDR pathogens.",

keywords = "AMR, antibiotic resistance, bioinformatics, global hazards, health issues",

author = "Muhammad Naveed and Hassan, \{Jawad Ul\} and Muneeb Ahmad and Nida Naeem and Mughal, \{Muhammad Saad\} and Rabaan, \{Ali A.\} and Mohammed Aljeldah and Shammari, \{Basim R.Al\} and Mohammed Alissa and Sabour, \{Amal A.\} and Alaeq, \{Rana A.\} and Alshiekheid, \{Maha A.\} and Turkistani, \{Safaa A.\} and Elmi, \{Abdirahman Hussein\} and Naveed Ahmed",

note = "Publisher Copyright: {\textcopyright} 2022 by the authors.",

year = "2022",

month = oct,

doi = "10.3390/medicina58101356",

language = "English",

volume = "58",

journal = "Medicina (Lithuania)",

issn = "1010-660X",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "10",

}

Naveed, M, Hassan, JU, Ahmad, M, Naeem, N, Mughal, MS, Rabaan, AA, Aljeldah, M, Shammari, BRA, Alissa, M, Sabour, AA, Alaeq, RA, Alshiekheid, MA, Turkistani, SA, Elmi, AH & Ahmed, N 2022, 'Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii: A Computational-Based Subtractive Proteomics Approach', Medicina (Lithuania), vol. 58, no. 10, 1356. https://doi.org/10.3390/medicina58101356

TY - JOUR

T1 - Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii

T2 - A Computational-Based Subtractive Proteomics Approach

AU - Naveed, Muhammad

AU - Hassan, Jawad Ul

AU - Ahmad, Muneeb

AU - Naeem, Nida

AU - Mughal, Muhammad Saad

AU - Rabaan, Ali A.

AU - Aljeldah, Mohammed

AU - Shammari, Basim R.Al

AU - Alissa, Mohammed

AU - Sabour, Amal A.

AU - Alaeq, Rana A.

AU - Alshiekheid, Maha A.

AU - Turkistani, Safaa A.

AU - Elmi, Abdirahman Hussein

AU - Ahmed, Naveed

PY - 2022/10

Y1 - 2022/10

N2 - Background and Objectives: Citrobacter freundii (C. freundii) is an emerging and opportunistic Gram-negative bacteria of the human gastrointestinal tract associated with nosocomial and severe respiratory tract infections. It has also been associated with pneumonia, bloodstream, and urinary tract infections. Intrinsic and adaptive virulence characteristics of C. freundii have become a significant source of diarrheal infections and food poisoning among immune-compromised patients and newborns. Impulsive usage of antibiotics and these adaptive virulence characteristics has modulated the C. freundii into multidrug-resistant (MDR) bacteria. Conventional approaches are futile against MDR C. freundii. Materials and Methods: The current study exploits the modern computational-based vaccine design approach to treat infections related to MDR C. freundii. A whole proteome of C. freundii (strain: CWH001) was retrieved to screen pathogenic and nonhomologous proteins. Six proteins were shortlisted for the selection of putative epitopes for vaccine construct. Highly antigenic, nonallergen, and nontoxic eleven B-cell, HTL, and TCL epitopes were selected for mRNA- and peptide-based multi-epitope vaccine construct. Secondary and tertiary structures of the multi-epitope vaccine (MEVC) were designed, refined, and validated. Results: Evaluation of population coverage of MHC-I and MHC-II alleles were 72% and 90%, respectively. Docking MEVC with TLR-3 receptor with the binding affinity of 21.46 (kcal/mol) occurred through the mmGBSA process. Further validations include codon optimization with an enhanced CAI value of 0.95 and GC content of about 51%. Immune stimulation and molecular dynamic simulation ensure the antibody production upon antigen interaction with the host and stability of the MEVC construct, respectively. Conclusions: These interpretations propose a new strategy to combat MDR C. freundii. Further, in vivo and in vitro trials of this vaccine will be valuable in combating MDR pathogens.

AB - Background and Objectives: Citrobacter freundii (C. freundii) is an emerging and opportunistic Gram-negative bacteria of the human gastrointestinal tract associated with nosocomial and severe respiratory tract infections. It has also been associated with pneumonia, bloodstream, and urinary tract infections. Intrinsic and adaptive virulence characteristics of C. freundii have become a significant source of diarrheal infections and food poisoning among immune-compromised patients and newborns. Impulsive usage of antibiotics and these adaptive virulence characteristics has modulated the C. freundii into multidrug-resistant (MDR) bacteria. Conventional approaches are futile against MDR C. freundii. Materials and Methods: The current study exploits the modern computational-based vaccine design approach to treat infections related to MDR C. freundii. A whole proteome of C. freundii (strain: CWH001) was retrieved to screen pathogenic and nonhomologous proteins. Six proteins were shortlisted for the selection of putative epitopes for vaccine construct. Highly antigenic, nonallergen, and nontoxic eleven B-cell, HTL, and TCL epitopes were selected for mRNA- and peptide-based multi-epitope vaccine construct. Secondary and tertiary structures of the multi-epitope vaccine (MEVC) were designed, refined, and validated. Results: Evaluation of population coverage of MHC-I and MHC-II alleles were 72% and 90%, respectively. Docking MEVC with TLR-3 receptor with the binding affinity of 21.46 (kcal/mol) occurred through the mmGBSA process. Further validations include codon optimization with an enhanced CAI value of 0.95 and GC content of about 51%. Immune stimulation and molecular dynamic simulation ensure the antibody production upon antigen interaction with the host and stability of the MEVC construct, respectively. Conclusions: These interpretations propose a new strategy to combat MDR C. freundii. Further, in vivo and in vitro trials of this vaccine will be valuable in combating MDR pathogens.

KW - AMR

KW - antibiotic resistance

KW - bioinformatics

KW - global hazards

KW - health issues

UR - https://www.scopus.com/pages/publications/85140649928

U2 - 10.3390/medicina58101356

DO - 10.3390/medicina58101356

M3 - Article

C2 - 36295517

AN - SCOPUS:85140649928

SN - 1010-660X

VL - 58

JO - Medicina (Lithuania)

JF - Medicina (Lithuania)

IS - 10

M1 - 1356

ER -

Designing mRNA- and Peptide-Based Vaccine Construct against Emerging Multidrug-Resistant Citrobacter freundii: A Computational-Based Subtractive Proteomics Approach

Abstract

Keywords

UN SDGs

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