2014
DOI: 10.1007/s11693-014-9135-9
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Integrative immunoinformatics for Mycobacterial diseases in R platform

Abstract: The sequencing of genomes of the pathogenic Mycobacterial species causing pulmonary and extrapulmonary tuberculosis, leprosy and other atypical mycobacterial infections, offer immense opportunities for discovering new therapeutics and identifying new vaccine candidates. Enhanced RV, which uses additional algorithms to Reverse Vaccinology (RV), has increased potential to reduce likelihood of undesirable features including allergenicity and immune cross reactivity to host. The starting point for MycobacRV databa… Show more

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Cited by 24 publications
(16 citation statements)
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“…For tuberculosis vaccine policies, Zwerling et al has developed a tool [ 54 ]. MycobacRv is another database related to TB vaccine [ 55 ]. MycobacRv has limits its focus to adhesion proteins in the genomes of different mycobacterial species.…”
Section: Discussionmentioning
confidence: 99%
“…For tuberculosis vaccine policies, Zwerling et al has developed a tool [ 54 ]. MycobacRv is another database related to TB vaccine [ 55 ]. MycobacRv has limits its focus to adhesion proteins in the genomes of different mycobacterial species.…”
Section: Discussionmentioning
confidence: 99%
“…Molecules localized on the cell membrane or extracellularly are beter antigens because they are more exposed to host cells, speciically to those related to the immune system; thus, they have a greater probability of generating a protective response [15]. In addition to the software that can predict these characteristics, there are protein databases that generate information about protein subcellular localization, such as LOCATE, LocDB, and eSLDB.…”
Section: Protein Cellular Localizationmentioning
confidence: 99%
“…The RV process begins with the proteomic information in a database; then, the selection of vaccine candidates is performed by means of different bioinformatics tools that analyze the properties of each protein and the human immune response generated by them [ 8 10 , 15 ]. Good vaccine candidates are considered those that do not present homology with human proteins to avoid the generation of a potential autoimmune response [ 16 ]; these candidates must also lack transmembrane regions, in order to facilitate their expression. In addition, it is necessary to analyze the lack of cross-reaction among other pathogenic antigens [ 14 ].…”
Section: Introductionmentioning
confidence: 99%
“…Another characteristic a good vaccine candidate should have is to possess good antigenic and adhesin properties, which are important for the pathogenesis of the microorganism and for protection against the disease [ 13 , 17 ]. Extracellular or cell surface localized proteins are good vaccine candidates due to their increased accessibility to the immune system [ 14 , 16 ]. Currently, software useful for simulation of the immune response has been developed that could help in the search for novel vaccine candidates [ 15 ].…”
Section: Introductionmentioning
confidence: 99%