Leandro J. Benevides
Universidade Federal de Minas Gerais
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Publication
Featured researches published by Leandro J. Benevides.
Frontiers in Microbiology | 2017
Rebeca Martín; Sylvie Miquel; Leandro J. Benevides; Chantal Bridonneau; Véronique Robert; Sylvie Hudault; Florian Chain; Olivier Berteau; Vasco Azevedo; Jean M. Chatel; Harry Sokol; Luis G. Bermúdez-Humarán; Muriel Thomas; Philippe Langella
Faecalibacterium prausnitzii is a major member of the Firmicutes phylum and one of the most abundant bacteria in the healthy human microbiota. F. prausnitzii depletion has been reported in several intestinal disorders, and more consistently in Crohns disease (CD) patients. Despite its importance in human health, only few microbiological studies have been performed to isolate novel F. prausnitzii strains in order to better understand the biodiversity and physiological diversity of this beneficial commensal species. In this study, we described a protocol to isolate novel F. prausnitzii strains from feces of healthy volunteers as well as a deep molecular and metabolic characterization of these isolated strains. These F. prausnitzii strains were classified in two phylogroups and three clusters according to 16S rRNA sequences and results support that they would belong to two different genomospecies or genomovars as no genome sequencing has been performed in this work. Differences in enzymes production, antibiotic resistance and immunomodulatory properties were found to be strain-dependent. So far, all F. prausnitzii isolates share some characteristic such as (i) the lack of epithelial cells adhesion, plasmids, anti-microbial, and hemolytic activity and (ii) the presence of DNAse activity. Furthermore, Short Chain Fatty Acids (SCFA) production was assessed for the novel isolates as these products influence intestinal homeostasis. Indeed, the butyrate production has been correlated to the capacity to induce IL-10, an anti-inflammatory cytokine, in peripheral blood mononuclear cells (PBMC) but not to the ability to block IL-8 secretion in TNF-α-stimulated HT-29 cells, reinforcing the hypothesis of a complex anti-inflammatory pathway driven by F. prausnitzii. Altogether, our results suggest that some F. prausnitzii strains could represent good candidates as next-generation probiotic.
Genome Announcements | 2014
Rafael A. Baraúna; Luis Carlos Guimarães; Adonney A. O. Veras; Pablo H.C.G. de Sá; Diego Assis das Graças; Kenny C. Pinheiro; Andréia do Socorro de Sousa Silva; Edson L. Folador; Leandro J. Benevides; Marcus Vinicius Canário Viana; Adriana Ribeiro Carneiro; Maria Paula Cruz Schneider; Sharon J. Spier; Judy M. Edman; Rommel Thiago Jucá Ramos; Vasco Azevedo; Artur Silva
ABSTRACT The genome of Corynebacterium pseudotuberculosis MB20 bv. equi was sequenced using the Ion Personal Genome Machine (PGM) platform, and showed a size of 2,363,089 bp, with 2,365 coding sequences and a GC content of 52.1%. These results will serve as a basis for further studies on the pathogenicity of C. pseudotuberculosis bv. equi.
PLOS ONE | 2017
Letícia de Castro Oliveira; Tessália Diniz Luerce Saraiva; Wanderson M. Silva; Ulisses de Pádua Pereira; Bruno C. Campos; Leandro J. Benevides; Flávia Souza Rocha; Henrique César Pereira Figueiredo; Vasco Azevedo; Siomar de Castro Soares
Lactococcus lactis subsp. lactis NCDO 2118 was recently reported to alleviate colitis symptoms via its anti-inflammatory and immunomodulatory activities, which are exerted by exported proteins that are not produced by L. lactis subsp. lactis IL1403. Here, we used in vitro and in silico approaches to characterize the genomic structure, the safety aspects, and the immunomodulatory activity of this strain. Through comparative genomics, we identified genomic islands, phage regions, bile salt and acid stress resistance genes, bacteriocins, adhesion-related and antibiotic resistance genes, and genes encoding proteins that are putatively secreted, expressed in vitro and absent from IL1403. The high degree of similarity between all Lactococcus suggests that the Symbiotic Islands commonly shared by both NCDO 2118 and KF147 may be responsible for their close relationship and their adaptation to plants. The predicted bacteriocins may play an important role against the invasion of competing strains. The genes related to the acid and bile salt stresses may play important roles in gastrointestinal tract survival, whereas the adhesion proteins are important for persistence in the gut, culminating in the competitive exclusion of other bacteria. Finally, the five secreted and expressed proteins may be important targets for studies of new anti-inflammatory and immunomodulatory proteins. Altogether, the analyses performed here highlight the potential use of this strain as a target for the future development of probiotic foods.
Frontiers in Microbiology | 2017
Leandro J. Benevides; Sriti Burman; Rebecca Martin; Véronique Robert; Muriel Thomas; Sylvie Miquel; Florian Chain; Harry Sokol; Luis G. Bermúdez-Humarán; Mark Morrison; Philippe Langella; Vasco Azevedo; Jean-Marc Chatel; Siomar de Castro Soares
Faecalibacterium prausnitzii is a commensal bacterium, ubiquitous in the gastrointestinal tracts of animals and humans. This species is a functionally important member of the microbiota and studies suggest it has an impact on the physiology and health of the host. F. prausnitzii is the only identified species in the genus Faecalibacterium, but a recent study clustered strains of this species in two different phylogroups. Here, we propose the existence of distinct species in this genus through the use of comparative genomics. Briefly, we performed analyses of 16S rRNA gene phylogeny, phylogenomics, whole genome Multi-Locus Sequence Typing (wgMLST), Average Nucleotide Identity (ANI), gene synteny, and pangenome to better elucidate the phylogenetic relationships among strains of Faecalibacterium. For this, we used 12 newly sequenced, assembled, and curated genomes of F. prausnitzii, which were isolated from feces of healthy volunteers from France and Australia, and combined these with published data from 5 strains downloaded from public databases. The phylogenetic analysis of the 16S rRNA sequences, together with the wgMLST profiles and a phylogenomic tree based on comparisons of genome similarity, all supported the clustering of Faecalibacterium strains in different genospecies. Additionally, the global analysis of gene synteny among all strains showed a highly fragmented profile, whereas the intra-cluster analyses revealed larger and more conserved collinear blocks. Finally, ANI analysis substantiated the presence of three distinct clusters—A, B, and C—composed of five, four, and four strains, respectively. The pangenome analysis of each cluster corroborated the classification of these clusters into three distinct species, each containing less variability than that found within the global pangenome of all strains. Here, we propose that comparison of pangenome subsets and their associated α values may be used as an alternative approach, together with ANI, in the in silico classification of new species. Altogether, our results provide evidence not only for the reconsideration of the phylogenetic and genomic relatedness among strains currently assigned to F. prausnitzii, but also the need for lineage (strain-based) differentiation of this taxon to better define how specific members might be associated with positive or negative host interactions.
Genome Announcements | 2015
Thiago J. Sousa; Diego C. B. Mariano; Doglas Parise; Mariana T D Parise; Marcus Vinicius Canário Viana; Luis Carlos Guimarães; Leandro J. Benevides; Flávia Souza Rocha; Priscilla Bagano; Rommel Thiago Jucá Ramos; Artur Silva; Henrique César Pereira Figueiredo; Sintia Almeida; Vasco Azevedo
ABSTRACT We present here the complete genome sequence of Corynebacterium pseudotuberculosis strain 12C, isolated from a sheep abscess in the Brazil. The sequencing was performed with the Ion Torrent Personal Genome Machine (PGM) system, a fragment library, and a coverage of ~48-fold. The genome presented is a circular chromosome with 2,337,451 bp in length, 2,119 coding sequences, 12 rRNAs, 49 tRNAs, and a G+C content of 52.83%.
Genome Announcements | 2014
Marcus Vinicius Canário Viana; Leandro J. Benevides; Diego César Batista Mariano; Flávia Souza Rocha; Priscilla C. B. Vilas Boas; Edson L. Folador; Felipe L. Pereira; Fernanda Alves Dorella; Carlos Augusto Gomes Leal; Alex F. Carvalho; Artur Silva; Siomar de Castro Soares; Henrique César Pereira Figueiredo; Vasco Azevedo; Luis Carlos Guimarães
ABSTRACT In this work, we present the complete genome sequence of Corynebacterium ulcerans strain 210932, isolated from a human. The species is an emergent pathogen that infects a variety of wild and domesticated animals and humans. It is associated with a growing number of cases of a diphtheria-like disease around the world.
PLOS ONE | 2017
Syed Babar Jamal; Syed Shah Hassan; Sandeep Tiwari; Marcus Vinicius Canário Viana; Leandro J. Benevides; Asad Ullah; Adrián G. Turjanski; Debmalya Barh; Preetam Ghosh; Daniela Arruda Costa; Artur Silva; Richard Röttger; Jan Baumbach; Vasco Azevedo
Corynebacterium diphtheriae (Cd) is a Gram-positive human pathogen responsible for diphtheria infection and once regarded for high mortalities worldwide. The fatality gradually decreased with improved living standards and further alleviated when many immunization programs were introduced. However, numerous drug-resistant strains emerged recently that consequently decreased the efficacy of current therapeutics and vaccines, thereby obliging the scientific community to start investigating new therapeutic targets in pathogenic microorganisms. In this study, our contributions include the prediction of modelome of 13 C. diphtheriae strains, using the MHOLline workflow. A set of 463 conserved proteins were identified by combining the results of pangenomics based core-genome and core-modelome analyses. Further, using subtractive proteomics and modelomics approaches for target identification, a set of 23 proteins was selected as essential for the bacteria. Considering human as a host, eight of these proteins (glpX, nusB, rpsH, hisE, smpB, bioB, DIP1084, and DIP0983) were considered as essential and non-host homologs, and have been subjected to virtual screening using four different compound libraries (extracted from the ZINC database, plant-derived natural compounds and Di-terpenoid Iso-steviol derivatives). The proposed ligand molecules showed favorable interactions, lowered energy values and high complementarity with the predicted targets. Our proposed approach expedites the selection of C. diphtheriae putative proteins for broad-spectrum development of novel drugs and vaccines, owing to the fact that some of these targets have already been identified and validated in other organisms.
Frontiers in Microbiology | 2017
Alberto Oliveira; Letícia de Castro Oliveira; Flavia Aburjaile; Leandro J. Benevides; Sandeep Tiwari; Syed Babar Jamal; Arthur Silva; Henrique César Pereira Figueiredo; Preetam Ghosh; Ricardo Wagner Portela; Vasco Azevedo; Alice R. Wattam
This review gathers recent information about genomic and transcriptomic studies in the Corynebacterium genus, exploring, for example, prediction of pathogenicity islands and stress response in different pathogenic and non-pathogenic species. In addition, is described several phylogeny studies to Corynebacterium, exploring since the identification of species until biological speciation in one species belonging to the genus Corynebacterium. Important concepts associated with virulence highlighting the role of Pld protein and Tox gene. The adhesion, characteristic of virulence factor, was described using the sortase mechanism that is associated to anchorage to the cell wall. In addition, survival inside the host cell and some diseases, were too addressed for pathogenic corynebacteria, while important biochemical pathways and biotechnological applications retain the focus of this review for non-pathogenic corynebacteria. Concluding, this review broadly explores characteristics in genus Corynebacterium showing to have strong relevance inside the medical, veterinary, and biotechnology field.
BMC Bioinformatics | 2016
Diego C. B. Mariano; Felipe L. Pereira; Edgar L. Aguiar; Letícia de Castro Oliveira; Leandro J. Benevides; Luis Carlos Guimarães; Edson L. Folador; Thiago J. Sousa; Preetam Ghosh; Debmalya Barh; Henrique César Pereira Figueiredo; Artur Silva; Rommel Thiago Jucá Ramos; Vasco Azevedo
BackgroundThe evolution of Next-Generation Sequencing (NGS) has considerably reduced the cost per sequenced-base, allowing a significant rise of sequencing projects, mainly in prokaryotes. However, the range of available NGS platforms requires different strategies and software to correctly assemble genomes. Different strategies are necessary to properly complete an assembly project, in addition to the installation or modification of various software. This requires users to have significant expertise in these software and command line scripting experience on Unix platforms, besides possessing the basic expertise on methodologies and techniques for genome assembly. These difficulties often delay the complete genome assembly projects.ResultsIn order to overcome this, we developed SIMBA (SImple Manager for Bacterial Assemblies), a freely available web tool that integrates several component tools for assembling and finishing bacterial genomes. SIMBA provides a friendly and intuitive user interface so bioinformaticians, even with low computational expertise, can work under a centralized administrative control system of assemblies managed by the assembly center head. SIMBA guides the users to execute assembly process through simple and interactive pages. SIMBA workflow was divided in three modules: (i) projects: allows a general vision of genome sequencing projects, in addition to data quality analysis and data format conversions; (ii) assemblies: allows de novo assemblies with the software Mira, Minia, Newbler and SPAdes, also assembly quality validations using QUAST software; and (iii) curation: presents methods to finishing assemblies through tools for scaffolding contigs and close gaps. We also presented a case study that validated the efficacy of SIMBA to manage bacterial assemblies projects sequenced using Ion Torrent PGM.ConclusionBesides to be a web tool for genome assembly, SIMBA is a complete genome assemblies project management system, which can be useful for managing of several projects in laboratories. SIMBA source code is available to download and install in local webservers at http://ufmg-simba.sourceforge.net.
Genome Announcements | 2015
Leandro J. Benevides; Marcus Vinicius Canário Viana; Diego César Batista Mariano; Flávia Souza Rocha; Priscilla Bagano; Edson L. Folador; Felipe L. Pereira; Fernanda Alves Dorella; Carlos Augusto Gomes Leal; Alex F. Carvalho; Siomar de Castro Soares; Adriana Ribeiro Carneiro; Rommel Thiago Jucá Ramos; Edgar Badell-Ocando; Nicole Guiso; Artur Silva; Henrique César Pereira Figueiredo; Vasco Azevedo; Luis Carlos Guimarães
ABSTRACT Here, we present the genome sequence of Corynebacterium ulcerans strain FRC11. The genome includes one circular chromosome of 2,442,826 bp (53.35% G+C content), and 2,210 genes were predicted, 2,146 of which are putative protein-coding genes, with 12 rRNAs and 51 tRNAs; 1 pseudogene was also identified.