Cargando…
The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity
Tuberculosis now exceeds HIV as the top infectious disease cause of mortality, and is caused by the Mycobacterium tuberculosis complex (MTBC). MTBC strains have highly conserved genome sequences (similarity >99%) but dramatically different phenotypes. To analyze the relationship between genotype...
| Autores principales: | , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Frontiers Media S.A.
2017
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5360109/ https://www.ncbi.nlm.nih.gov/pubmed/28377903 http://dx.doi.org/10.3389/fcimb.2017.00088 |
| _version_ | 1782516536434491392 |
|---|---|
| author | Jia, Xinmiao Yang, Li Dong, Mengxing Chen, Suting Lv, Lingna Cao, Dandan Fu, Jing Yang, Tingting Zhang, Ju Zhang, Xiangli Shang, Yuanyuan Wang, Guirong Sheng, Yongjie Huang, Hairong Chen, Fei |
| author_facet | Jia, Xinmiao Yang, Li Dong, Mengxing Chen, Suting Lv, Lingna Cao, Dandan Fu, Jing Yang, Tingting Zhang, Ju Zhang, Xiangli Shang, Yuanyuan Wang, Guirong Sheng, Yongjie Huang, Hairong Chen, Fei |
| author_sort | Jia, Xinmiao |
| collection | PubMed |
| description | Tuberculosis now exceeds HIV as the top infectious disease cause of mortality, and is caused by the Mycobacterium tuberculosis complex (MTBC). MTBC strains have highly conserved genome sequences (similarity >99%) but dramatically different phenotypes. To analyze the relationship between genotype and phenotype, we conducted the comparative genomic analysis on 12 MTBC strains representing different lineages (i.e., Mycobacterium bovis; M. bovis BCG; M. microti; M. africanum; M. tuberculosis H37Rv; M. tuberculosis H37Ra, and six M. tuberculosis clinical isolates). The analysis focused on the three aspects of pathogenicity: host association, virulence, and epitope variations. Host association analysis indicated that eight mce3 genes, two enoyl-CoA hydratases, and five PE/PPE family genes were present only in human isolates; these may have roles in host-pathogen interactions. There were 15 SNPs found on virulence factors (including five SNPs in three ESX secretion proteins) only in the Beijing strains, which might be related to their more virulent phenotype. A comparison between the virulent H37Rv and non-virulent H37Ra strains revealed three SNPs that were likely associated with the virulence attenuation of H37Ra: S219L (PhoP), A219E (MazG) and a newly identified I228M (EspK). Additionally, a comparison of animal-associated MTBC strains showed that the deletion of the first four genes (i.e., pe35, ppe68, esxB, esxA), rather than all eight genes of RD1, might play a central role in the virulence attenuation of animal isolates. Finally, by comparing epitopes among MTBC strains, we found that four epitopes were lost only in the Beijing strains; this may render them better capable of evading the human immune system, leading to enhanced virulence. Overall, our comparative genomic analysis of MTBC strains reveals the relationship between the highly conserved genotypes and the diverse phenotypes of MTBC, provides insight into pathogenic mechanisms, and facilitates the development of potential molecular targets for the prevention and treatment of tuberculosis. |
| format | Online Article Text |
| id | pubmed-5360109 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2017 |
| publisher | Frontiers Media S.A. |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-53601092017-04-04 The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity Jia, Xinmiao Yang, Li Dong, Mengxing Chen, Suting Lv, Lingna Cao, Dandan Fu, Jing Yang, Tingting Zhang, Ju Zhang, Xiangli Shang, Yuanyuan Wang, Guirong Sheng, Yongjie Huang, Hairong Chen, Fei Front Cell Infect Microbiol Microbiology Tuberculosis now exceeds HIV as the top infectious disease cause of mortality, and is caused by the Mycobacterium tuberculosis complex (MTBC). MTBC strains have highly conserved genome sequences (similarity >99%) but dramatically different phenotypes. To analyze the relationship between genotype and phenotype, we conducted the comparative genomic analysis on 12 MTBC strains representing different lineages (i.e., Mycobacterium bovis; M. bovis BCG; M. microti; M. africanum; M. tuberculosis H37Rv; M. tuberculosis H37Ra, and six M. tuberculosis clinical isolates). The analysis focused on the three aspects of pathogenicity: host association, virulence, and epitope variations. Host association analysis indicated that eight mce3 genes, two enoyl-CoA hydratases, and five PE/PPE family genes were present only in human isolates; these may have roles in host-pathogen interactions. There were 15 SNPs found on virulence factors (including five SNPs in three ESX secretion proteins) only in the Beijing strains, which might be related to their more virulent phenotype. A comparison between the virulent H37Rv and non-virulent H37Ra strains revealed three SNPs that were likely associated with the virulence attenuation of H37Ra: S219L (PhoP), A219E (MazG) and a newly identified I228M (EspK). Additionally, a comparison of animal-associated MTBC strains showed that the deletion of the first four genes (i.e., pe35, ppe68, esxB, esxA), rather than all eight genes of RD1, might play a central role in the virulence attenuation of animal isolates. Finally, by comparing epitopes among MTBC strains, we found that four epitopes were lost only in the Beijing strains; this may render them better capable of evading the human immune system, leading to enhanced virulence. Overall, our comparative genomic analysis of MTBC strains reveals the relationship between the highly conserved genotypes and the diverse phenotypes of MTBC, provides insight into pathogenic mechanisms, and facilitates the development of potential molecular targets for the prevention and treatment of tuberculosis. Frontiers Media S.A. 2017-03-21 /pmc/articles/PMC5360109/ /pubmed/28377903 http://dx.doi.org/10.3389/fcimb.2017.00088 Text en Copyright © 2017 Jia, Yang, Dong, Chen, Lv, Cao, Fu, Yang, Zhang, Zhang, Shang, Wang, Sheng, Huang and Chen. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms. |
| spellingShingle | Microbiology Jia, Xinmiao Yang, Li Dong, Mengxing Chen, Suting Lv, Lingna Cao, Dandan Fu, Jing Yang, Tingting Zhang, Ju Zhang, Xiangli Shang, Yuanyuan Wang, Guirong Sheng, Yongjie Huang, Hairong Chen, Fei The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity |
| title | The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity |
| title_full | The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity |
| title_fullStr | The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity |
| title_full_unstemmed | The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity |
| title_short | The Bioinformatics Analysis of Comparative Genomics of Mycobacterium tuberculosis Complex (MTBC) Provides Insight into Dissimilarities between Intraspecific Groups Differing in Host Association, Virulence, and Epitope Diversity |
| title_sort | bioinformatics analysis of comparative genomics of mycobacterium tuberculosis complex (mtbc) provides insight into dissimilarities between intraspecific groups differing in host association, virulence, and epitope diversity |
| topic | Microbiology |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5360109/ https://www.ncbi.nlm.nih.gov/pubmed/28377903 http://dx.doi.org/10.3389/fcimb.2017.00088 |
| work_keys_str_mv | AT jiaxinmiao thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT yangli thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT dongmengxing thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT chensuting thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT lvlingna thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT caodandan thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT fujing thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT yangtingting thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT zhangju thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT zhangxiangli thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT shangyuanyuan thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT wangguirong thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT shengyongjie thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT huanghairong thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT chenfei thebioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT jiaxinmiao bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT yangli bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT dongmengxing bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT chensuting bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT lvlingna bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT caodandan bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT fujing bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT yangtingting bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT zhangju bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT zhangxiangli bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT shangyuanyuan bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT wangguirong bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT shengyongjie bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT huanghairong bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity AT chenfei bioinformaticsanalysisofcomparativegenomicsofmycobacteriumtuberculosiscomplexmtbcprovidesinsightintodissimilaritiesbetweenintraspecificgroupsdifferinginhostassociationvirulenceandepitopediversity |