Temporal Changes in Patient-Matched Staphylococcus epidermidis Isolates from Infections: towards Defining a ‘True’ Persistent Infection

Staphylococcus epidermidis is found naturally on the skin but is a common cause of persistent orthopaedic device-related infections (ODRIs). This study used a pan-genome and gene-by-gene approach to analyse the clonality of whole genome sequences (WGS) of 115 S. epidermidis isolates from 55 patients with persistent ODRIs. Analysis of the 522 gene core genome revealed that the isolates clustered into three clades, and MLST analysis showed that 83% of the isolates belonged to clonal complex 2 (CC2). Analysis also found 13 isolate pairs had different MLST types and less than 70% similarity within the genes; hence, these were defined as re-infection by a different S. epidermidis strain. Comparison of allelic diversity in the remaining 102 isolates (49 patients) revealed that 6 patients had microevolved infections (>7 allele differences), and only 37 patients (77 isolates) had a ‘true’ persistent infection. Analysis of the core genomes of isolate pairs from 37 patients found 110/841 genes had variations; mainly in metabolism associated genes. The accessory genome consisted of 2936 genes; with an average size of 1515 genes. To conclude, this study demonstrates the advantage of using WGS for identifying the accuracy of a persistent infection diagnosis. Hence, persistent infections can be defined as ‘true’ persistent infections if the core genome of paired isolates has ≤7 allele differences; microevolved persistent infection if the paired isolates have >7 allele differences but same MLST type; and polyclonal if they are the same species but a different MLST type.

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A Genomic Distance Based on MUM Indicates Discontinuity between Most Bacterial Species and Genera

Journal of Bacteriology ◽

10.1128/jb.01202-08 ◽

2008 ◽

Vol 191 (1) ◽

pp. 91-99 ◽

Cited By ~ 115

Author(s):

Marc Deloger ◽

Meriem El Karoui ◽

Marie-Agnès Petit

Keyword(s):

Dna Sequences ◽

Dna Content ◽

Core Genome ◽

Biological Diversity ◽

Bacterial Species ◽

Genomic Distance ◽

The Core ◽

Intraspecies Diversity ◽

Genome Level ◽

Definition Of

ABSTRACT The fundamental unit of biological diversity is the species. However, a remarkable extent of intraspecies diversity in bacteria was discovered by genome sequencing, and it reveals the need to develop clear criteria to group strains within a species. Two main types of analyses used to quantify intraspecies variation at the genome level are the average nucleotide identity (ANI), which detects the DNA conservation of the core genome, and the DNA content, which calculates the proportion of DNA shared by two genomes. Both estimates are based on BLAST alignments for the definition of DNA sequences common to the genome pair. Interestingly, however, results using these methods on intraspecies pairs are not well correlated. This prompted us to develop a genomic-distance index taking into account both criteria of diversity, which are based on DNA maximal unique matches (MUM) shared by two genomes. The values, called MUMi, for MUM index, correlate better with the ANI than with the DNA content. Moreover, the MUMi groups strains in a way that is congruent with routinely used multilocus sequence-typing trees, as well as with ANI-based trees. We used the MUMi to determine the relatedness of all available genome pairs at the species and genus levels. Our analysis reveals a certain consistency in the current notion of bacterial species, in that the bulk of intraspecies and intragenus values are clearly separable. It also confirms that some species are much more diverse than most. As the MUMi is fast to calculate, it offers the possibility of measuring genome distances on the whole database of available genomes.

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Nora virus, a persistent virus in Drosophila, defines a new picorna-like virus family

Journal of General Virology ◽

10.1099/vir.0.81997-0 ◽

2006 ◽

Vol 87 (10) ◽

pp. 3045-3051 ◽

Cited By ~ 68

Author(s):

Mazen S. Habayeb ◽

Sophia K. Ekengren ◽

Dan Hultmark

Keyword(s):

Persistent Infection ◽

Open Reading Frames ◽

Close Relative ◽

Virus Family ◽

Viral Genomes ◽

Persistent Infections ◽

New Family ◽

Nora Virus ◽

Persistent Virus ◽

Viral Sequences

Several viruses, including picornaviruses, are known to establish persistent infections, but the mechanisms involved are poorly understood. Here, a novel picorna-like virus, Nora virus, which causes a persistent infection in Drosophila melanogaster, is described. It has a single-stranded, positive-sense genomic RNA of 11879 nt, followed by a poly(A) tail. Unlike other picorna-like viruses, the genome has four open reading frames (ORFs). One ORF encodes a picornavirus-like cassette of proteins for virus replication, including an iflavirus-like RNA-dependent RNA polymerase and a helicase that is related to those of mammalian picornaviruses. The three other ORFs are not closely related to any previously described viral sequences. The unusual sequence and genome organization in Nora virus suggest that it belongs to a new family of picorna-like viruses. Surprisingly, Nora virus could be detected in all tested D. melanogaster laboratory stocks, as well as in wild-caught material. The viral titres varied enormously, between 104 and 1010 viral genomes per fly in different stocks, without causing obvious pathological effects. The virus was also found in Drosophila simulans, a close relative of D. melanogaster, but not in more distantly related Drosophila species. It will now be possible to use Drosophila genetics to study the factors that control this persistent infection.

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To catch a hijacker: abundance, evolution and genetic diversity of P4-like bacteriophage satellites

Philosophical Transactions of the Royal Society B Biological Sciences ◽

10.1098/rstb.2020.0475 ◽

2021 ◽

Vol 377 (1842) ◽

Author(s):

Jorge A. Moura de Sousa ◽

Eduardo P. C. Rocha

Keyword(s):

Escherichia Coli ◽

Molecular Mechanisms ◽

Core Genome ◽

Mobile Genetic Elements ◽

Abundance Distribution ◽

Theme Issue ◽

Genetic Elements ◽

The Core ◽

Antagonistic Interactions ◽

Variable Genes

Bacteriophages (phages) are bacterial parasites that can themselves be parasitized by phage satellites. The molecular mechanisms used by satellites to hijack phages are sometimes understood in great detail, but the origins, abundance, distribution and composition of these elements are poorly known. Here, we show that P4-like elements are present in more than 30% of the genomes of Enterobacterales, and in almost half of those of Escherichia coli , sometimes in multiple distinct copies. We identified over 1000 P4-like elements with very conserved genetic organization of the core genome and a few hotspots with highly variable genes. These elements are never found in plasmids and have very little homology to known phages, suggesting an independent evolutionary origin. Instead, they are scattered across chromosomes, possibly because their integrases are often exchanged with other elements. The rooted phylogenies of hijacking functions are correlated and suggest longstanding coevolution. They also reveal broad host ranges in P4-like elements, as almost identical elements can be found in distinct bacterial genera. Our results show that P4-like phage satellites constitute a very distinct, widespread and ancient family of mobile genetic elements. They pave the way for studying the molecular evolution of antagonistic interactions between phages and their satellites. This article is part of the theme issue ‘The secret lives of microbial mobile genetic elements’.

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Синтез и магнитные свойства наночастиц Fe-=SUB=-3-=/SUB=-O-=SUB=-4-=/SUB=-/CoFe-=SUB=-2-=/SUB=-O-=SUB=-4-=/SUB=- со структурой ядро/оболочка

Физика твердого тела ◽

10.21883/ftt.2020.02.48874.581 ◽

2020 ◽

Vol 62 (2) ◽

pp. 235

Author(s):

Д.А. Балаев ◽

С.В. Семенов ◽

А.А. Дубровский ◽

А.А. Красиков ◽

С.И. Попков ◽

...

Keyword(s):

Single Phase ◽

Hybrid Particles ◽

Soft Magnetic ◽

Cofe2o4 Nanoparticles ◽

The Core ◽

Core Shell Structure ◽

Magnetically Hard ◽

Co Precipitation ◽

Average Size ◽

Magnetic Fe3o4

Fe3O4 / CoFe2O4 nanoparticles with a core-shell structure with an average size of 5 nm were obtained by co-precipitation from solutions of iron and cobalt chlorides. An analysis of the magnetic properties of the resulting system and their comparison with the data for single-phase Fe3O4 (4 nm) and CoFe2O4 (6 nm) nanoparticles led to the conclusion that there is a noticeable interaction between the soft magnetic (Fe3O4) and magnetically hard (CoFe2O4) phases that form the core and the shell of hybrid particles, correspondingly.

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The core genome multi-locus sequence typing of Mycoplasma anserisalpingitidis

BMC Genomics ◽

10.1186/s12864-020-06817-2 ◽

2020 ◽

Vol 21 (1) ◽

Author(s):

Áron B. Kovács ◽

Zsuzsa Kreizinger ◽

Barbara Forró ◽

Dénes Grózner ◽

Alexa Mitter ◽

...

Keyword(s):

Core Genome ◽

Multi Locus Sequence Typing ◽

The Core

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Revisiting Bap Multidomain Protein: More Than Sticking Bacteria Together

Frontiers in Microbiology ◽

10.3389/fmicb.2020.613581 ◽

2020 ◽

Vol 11 ◽

Author(s):

Jaione Valle ◽

Xianyang Fang ◽

Iñigo Lasa

Keyword(s):

Biofilm Formation ◽

Core Genome ◽

Current Knowledge ◽

Surface Proteins ◽

Structure And Properties ◽

Diverse Range ◽

The Core ◽

Self Assembling ◽

Abiotic Surfaces ◽

Range Of Functions

One of the major components of the staphylococcal biofilm is surface proteins that assemble as scaffold components of the biofilm matrix. Among the different surface proteins able to contribute to biofilm formation, this review is dedicated to the Biofilm Associated Protein (Bap). Bap is part of the accessory genome of Staphylococcus aureus but orthologs of Bap in other staphylococcal species belong to the core genome. When present, Bap promotes adhesion to abiotic surfaces and induces strong intercellular adhesion by self-assembling into amyloid like aggregates in response to the levels of calcium and the pH in the environment. During infection, Bap enhances the adhesion to epithelial cells where it binds directly to the host receptor Gp96 and inhibits the entry of the bacteria into the cells. To perform such diverse range of functions, Bap comprises several domains, and some of them include several motifs associated to distinct functions. Based on the knowledge accumulated with the Bap protein of S. aureus, this review aims to summarize the current knowledge of the structure and properties of each domain of Bap and their contribution to Bap functionality.

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Why? – Successful Pseudomonas aeruginosa clones with a focus on clone C

FEMS Microbiology Reviews ◽

10.1093/femsre/fuaa029 ◽

2020 ◽

Vol 44 (6) ◽

pp. 740-762

Author(s):

Changhan Lee ◽

Jens Klockgether ◽

Sebastian Fischer ◽

Janja Trcek ◽

Burkhard Tümmler ◽

...

Keyword(s):

Pseudomonas Aeruginosa ◽

Core Genome ◽

Genomic Island ◽

Protein Quality ◽

Temperature Tolerance ◽

Protein Homeostasis ◽

Gene Products ◽

Accessory Genome ◽

The Core ◽

Conserved Core

ABSTRACT The environmental species Pseudomonas aeruginosa thrives in a variety of habitats. Within the epidemic population structure of P. aeruginosa, occassionally highly successful clones that are equally capable to succeed in the environment and the human host arise. Framed by a highly conserved core genome, individual members of successful clones are characterized by a high variability in their accessory genome. The abundance of successful clones might be funded in specific features of the core genome or, although not mutually exclusive, in the variability of the accessory genome. In clone C, one of the most predominant clones, the plasmid pKLC102 and the PACGI-1 genomic island are two ubiquitous accessory genetic elements. The conserved transmissible locus of protein quality control (TLPQC) at the border of PACGI-1 is a unique horizontally transferred compository element, which codes predominantly for stress-related cargo gene products such as involved in protein homeostasis. As a hallmark, most TLPQC xenologues possess a core genome equivalent. With elevated temperature tolerance as a characteristic of clone C strains, the unique P. aeruginosa and clone C specific disaggregase ClpG is a major contributor to tolerance. As other successful clones, such as PA14, do not encode the TLPQC locus, ubiquitous denominators of success, if existing, need to be identified.

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Core Genome Allelic Profiles of Clinical Klebsiella pneumoniae Strains Using a Random Forest Algorithm Based on Multilocus Sequence Typing Scheme for Hypervirulence Analysis

The Journal of Infectious Diseases ◽

10.1093/infdis/jiz562 ◽

2020 ◽

Vol 221 (Supplement_2) ◽

pp. S263-S271 ◽

Cited By ~ 1

Author(s):

Peng Lan ◽

Qiucheng Shi ◽

Ping Zhang ◽

Yan Chen ◽

Rushuang Yan ◽

...

Keyword(s):

Random Forest ◽

Klebsiella Pneumoniae ◽

Multilocus Sequence Typing ◽

Operating Characteristic ◽

Core Genome ◽

Characteristic Curve ◽

Random Forest Algorithm ◽

The Core ◽

Model Based ◽

Operating Characteristic Curve

Abstract Background Hypervirulent Klebsiella pneumoniae (hvKP) infections can have high morbidity and mortality rates owing to their invasiveness and virulence. However, there are no effective tools or biomarkers to discriminate between hvKP and nonhypervirulent K. pneumoniae (nhvKP) strains. We aimed to use a random forest algorithm to predict hvKP based on core-genome data. Methods In total, 272 K. pneumoniae strains were collected from 20 tertiary hospitals in China and divided into hvKP and nhvKP groups according to clinical criteria. Clinical data comparisons, whole-genome sequencing, virulence profile analysis, and core genome multilocus sequence typing (cgMLST) were performed. We then established a random forest predictive model based on the cgMLST scheme to prospectively identify hvKP. The random forest is an ensemble learning method that generates multiple decision trees during the training process and each decision tree will output its own prediction results corresponding to the input. The predictive ability of the model was assessed by means of area under the receiver operating characteristic curve. Results Patients in the hvKP group were younger than those in the nhvKP group (median age, 58.0 and 68.0 years, respectively; P < .001). More patients in the hvKP group had underlying diabetes mellitus (43.1% vs 20.1%; P < .001). Clinically, carbapenem-resistant K. pneumoniae was less common in the hvKP group (4.1% vs 63.8%; P < .001), whereas the K1/K2 serotype, sequence type (ST) 23, and positive string tests were significantly higher in the hvKP group. A cgMLST-based minimal spanning tree revealed that hvKP strains were scattered sporadically within nhvKP clusters. ST23 showed greater genome diversification than did ST11, according to cgMLST-based allelic differences. Primary virulence factors (rmpA, iucA, positive string test result, and the presence of virulence plasmid pLVPK) were poor predictors of the hypervirulence phenotype. The random forest model based on the core genome allelic profile presented excellent predictive power, both in the training and validating sets (area under receiver operating characteristic curve, 0.987 and 0.999 in the training and validating sets, respectively). Conclusions A random forest algorithm predictive model based on the core genome allelic profiles of K. pneumoniae was accurate to identify the hypervirulent isolates.

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Persistent Infection of Human Oligodendrocytic and Neuroglial Cell Lines by Human Coronavirus 229E

Journal of Virology ◽

10.1128/jvi.73.4.3326-3337.1999 ◽

1999 ◽

Vol 73 (4) ◽

pp. 3326-3337 ◽

Cited By ~ 74

Author(s):

Nathalie Arbour ◽

Sophie Ekandé ◽

Geneviève Côté ◽

Claude Lachance ◽

Fanny Chagnon ◽

...

Keyword(s):

Nervous System ◽

Cell Lines ◽

Persistent Infection ◽

Viral Antigen ◽

Infectious Virus ◽

Acute Infection ◽

Viral Rna ◽

Persistent Infections ◽

Virus Progeny

ABSTRACT Human coronaviruses (HuCV) cause common colds. Previous reports suggest that these infectious agents may be neurotropic in humans, as they are for some mammals. With the long-term aim of providing experimental evidence for the neurotropism of HuCV and the establishment of persistent infections in the nervous system, we have evaluated the susceptibility of various human neural cell lines to acute and persistent infection by HuCV-229E. Viral antigen, infectious virus progeny and viral RNA were monitored during both acute and persistent infections. The astrocytoma cell lines U-87 MG, U-373 MG, and GL-15, as well as neuroblastoma SK-N-SH, neuroglioma H4, and oligodendrocytic MO3.13 cell lines, were all susceptible to an acute infection by HuCV-229E. The CHME-5 immortalized fetal microglial cell line was not susceptible to infection by this virus. The MO3.13 and H4 cell lines also sustained a persistent viral infection, as monitored by detection of viral antigen and infectious virus progeny. Sequencing of the S1 gene from viral RNA after ∼130 days of infection showed two point mutations, suggesting amino acid changes during persistent infection of MO3.13 cells but none for H4 cells. Thus, persistent in vitro infection did not generate important changes in the S1 portion of the viral spike protein, which was shown for murine coronaviruses to bear hypervariable domains and to interact with cellular receptor. These results are consistent with the potential persistence of HuCV-229E in cells of the human nervous system, such as oligodendrocytes and possibly neurons, and the virus’s apparent genomic stability.

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Genome Organization and Adaptive Potential of Archetypal Organophosphate Degrading Sphingobium fuliginis ATCC 27551

Genome Biology and Evolution ◽

10.1093/gbe/evz189 ◽

2019 ◽

Vol 11 (9) ◽

pp. 2557-2562 ◽

Cited By ~ 2

Author(s):

Sarwar Azam ◽

Sunil Parthasarathy ◽

Chhaya Singh ◽

Shakti Kumar ◽

Dayananda Siddavattam

Keyword(s):

Core Genome ◽

Gc Content ◽

Mobile Element ◽

Membrane Receptors ◽

Harsh Environments ◽

Adaptive Potential ◽

Gene Encoding ◽

Organophosphate Hydrolase ◽

The Core ◽

Close Relationship

Abstract Sphingobium fuliginis ATCC 27551, previously classified as Flavobacterium sp. ATCC 27551, degrades neurotoxic organophosphate insecticides and nerve agents through the activity of a membrane-associated organophosphate hydrolase. This study was designed to determine the complete genome sequence of S. fuliginis ATCC 27551 to unravel its degradative potential and adaptability to harsh environments. The 5,414,624 bp genome with a GC content of 64.4% is distributed between two chromosomes and four plasmids and encodes 5,557 proteins. Of the four plasmids, designated as pSF1, pSF2, pSF3, and pSF4, only two (pSF1 and pSF2) are self-transmissible and contained the complete genetic repertoire for a T4SS. The other two plasmids (pSF3 and pSF4) are mobilizable and both showed the presence of an oriT and relaxase-encoding sequences. The sequence of plasmid pSF3 coincided with the previously determined sequence of pPDL2 and included an opd gene encoding organophosphate hydrolase as a part of the mobile element. About 15,455 orthologous clusters were identified from among the cumulatively annotated genes of 49 Sphingobium species. Phylogenetic analysis done using the core genome consisting of 802 orthologous clusters revealed a close relationship between S. fuliginis ATCC 27551 and bacteria capable of degradation of polyaromatic hydrocarbon compounds. Genes coding for transposases, efflux pumps conferring resistance to heavy metals, and TonR-type outer membrane receptors are selectively enriched in the genome of S. fuliginis ATCC 27551 and appear to contribute to the adaptive potential of the organism to challenging and harsh environments.

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