Your search keyword '"genome degradation"' showing total 34 results

1. Pseudogenization of the Secreted Effector Gene sseI Confers Rapid Systemic Dissemination of S. Typhimurium ST313 within Migratory Dendritic Cells

Author

Carden, Sarah E, Walker, Gregory T, Honeycutt, Jared, Lugo, Kyler, Pham, Trung, Jacobson, Amanda, Bouley, Donna, Idoyaga, Juliana, Tsolis, Renee M, and Monack, Denise

Subjects

Microbiology, Medical Microbiology, Biomedical and Clinical Sciences, Biological Sciences, Digestive Diseases, Foodborne Illness, Hematology, Prevention, Biodefense, Vaccine Related, Infectious Diseases, Emerging Infectious Diseases, Aetiology, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, Infection, Animals, Bacteremia, Cell Movement, Dendritic Cells, Disease Models, Animal, Female, Gastroenteritis, Gene Expression Regulation, Bacterial, Genes, Bacterial, Host-Pathogen Interactions, Lymph Nodes, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Receptors, CCR7, Salmonella Infections, Salmonella typhimurium, NTS, SrfH, T3SS effectors, evolution, genome degradation, iNTS, niche adaptation, nontyphoidal Salmonella, pathogenesis, pseudogene, Immunology, Biochemistry and cell biology, Medical microbiology

Abstract

Genome degradation correlates with host adaptation and systemic disease in Salmonella. Most lineages of the S. enterica subspecies Typhimurium cause gastroenteritis in humans; however, the recently emerged ST313 lineage II pathovar commonly causes systemic bacteremia in sub-Saharan Africa. ST313 lineage II displays genome degradation compared to gastroenteritis-associated lineages; yet, the mechanisms and causal genetic differences mediating these infection phenotypes are largely unknown. We find that the ST313 isolate D23580 hyperdisseminates from the gut to systemic sites, such as the mesenteric lymph nodes (MLNs), via CD11b+ migratory dendritic cells (DCs). This hyperdissemination was facilitated by the loss of sseI, which encodes an effector that inhibits DC migration in gastroenteritis-associated isolates. Expressing functional SseI in D23580 reduced the number of infected migratory DCs and bacteria in the MLN. Our study reveals a mechanism linking pseudogenization of effectors with the evolution of niche adaptation in a bacterial pathogen.

Published

2017

2. A New Family of DNA Viruses Causing Disease in Crustaceans from Diverse Aquatic Biomes

Author

Kuttichantran Subramaniam, Donald C. Behringer, Jamie Bojko, Natalya Yutin, Abigail S. Clark, Kelly S. Bateman, Ronny van Aerle, David Bass, Rose C. Kerr, Eugene V. Koonin, Grant D. Stentiford, and Thomas B. Waltzek

Subjects

Crustacea, genome degradation, large nucleocytoplasmic DNA viruses, low-complexity sequences, virus evolution, Microbiology, QR1-502

Abstract

ABSTRACT Panulirus argus virus 1 (PaV1) is the only known virus infecting the Caribbean spiny lobster (Panulirus argus) from the Caribbean Sea. Recently, related viruses, Dikerogammarus haemobaphes virus 1 (DhV1) and Carcinus maenas virus 1 (CmV1), have been detected in the demon shrimp (Dikerogammarus haemobaphes) and the European shore crab (Carcinus maenas), respectively, from sites in the United Kingdom. The virion morphology of these crustacean viruses is similar to that of iridoviruses. However, unlike iridoviruses and other nucleocytoplasmic large DNA viruses (NCLDVs), these viruses complete their morphogenesis in the host cell nucleus rather than in the cytoplasm. To date, these crustacean viruses have remained unclassified due to a lack of genomic data. Using an Illumina MiSeq sequencer, we sequenced the complete genomes of PaV1, CmV1, and DhV1. Comparative genome analysis shows that these crustacean virus genomes encode the 10 hallmark proteins previously described for the NCLDVs of eukaryotes, strongly suggesting that they are members of this group. With a size range of 70 to 74 kb, these are the smallest NCLDV genomes identified to date. Extensive gene loss, divergence of gene sequences, and the accumulation of low-complexity sequences reflect the extreme degradation of the genomes of these “minimal” NCLDVs rather than any direct relationship with the NCLDV ancestor. Phylogenomic analysis supports the classification of these crustacean viruses as a distinct family, “Mininucleoviridae,” within the pitho-irido-Marseille branch of the NCLDVs. IMPORTANCE Recent genomic and metagenomic studies have led to a dramatic expansion of the known diversity of nucleocytoplasmic large DNA viruses (NCLDVs) of eukaryotes, which include giant viruses of protists and important pathogens of vertebrates, such as poxviruses. However, the characterization of viruses from nonmodel hosts still lags behind. We sequenced the complete genomes of three viruses infecting crustaceans, the Caribbean spiny lobster, demon shrimp, and European shore crab. These viruses have the smallest genomes among the known NCLDVs, with losses of many core genes, some of which are shared with iridoviruses. The deterioration of the transcription apparatus is compatible with microscopic and ultrastructural observations indicating that these viruses replicate in the nucleus of infected cells rather than in the cytoplasm. Phylogenomic analysis indicates that these viruses are sufficiently distinct from all other NCLDVs to justify the creation of a separate family, for which we propose the name “Mininucleoviridae” (i.e., small viruses reproducing in the cell nucleus).

Published

2020

3. Loss and Gain in the Evolution of the Salmonella enterica Serovar Gallinarum Biovar Pullorum Genome

Author

Yachen Hu, Zhenyu Wang, Bin Qiang, Yaohui Xu, Xiang Chen, Qiuchun Li, and Xinan Jiao

Subjects

Salmonella enterica serovar Gallinarum biovar Pullorum, evolution, genome degradation, genomic epidemiology, multidrug resistance, Microbiology, QR1-502

Abstract

ABSTRACT Salmonella enterica subspecies enterica serovar Gallinarum biovar Pullorum (S. Pullorum) is the etiological agent of pullorum disease, causing white diarrhea with high mortality in chickens. There are many unsolved issues surrounding the epidemiology of S. Pullorum, including its origin and transmission history as well as the discordance between its phenotypic heterogeneity and genetic monomorphism. In this paper, we report the results of whole-genome sequencing of a panel of 97 S. Pullorum strains isolated between 1962 and 2014 from four countries across three continents. We utilized 6,795 core genome single nucleotide polymorphisms (SNPs) to reconstruct a phylogenetic tree within a spatiotemporal Bayesian framework, estimating that the most recent common ancestor of S. Pullorum emerged in ∼914 CE (95% confidence interval [95%CI], 565 to 1273 CE). The extant S. Pullorum strains can be divided into four distinct lineages, each of which is significantly associated with geographical distribution. The intercontinental transmissions of lineages III and IV can be traced to the mid-19th century and are probably related to the “Hen Fever” prevalent at that time. Further genomic analysis indicated that the loss or pseudogenization of functional genes involved in metabolism and virulence in S. Pullorum has been ongoing since before and after divergence from the ancestor. In contrast, multiple prophages and plasmids have been acquired by S. Pullorum, and these have endowed it with new characteristics, especially the multidrug resistance conferred by two large plasmids in lineage I. The results of this study provide insight into the evolution of S. Pullorum and prove the efficiency of whole-genome sequencing in epidemiological surveillance of pullorum disease. IMPORTANCE Pullorum disease, an acute poultry septicemia caused by Salmonella Gallinarum biovar Pullorum, is fatal for young chickens and is a heavy burden on poultry industry. The pathogen is rare in most developed countries but still extremely difficult to eliminate in China. Efficient epidemiological surveillance necessitates clarifying the origin of the isolates from different regions and their phylogenic relationships. Genomic epidemiological analysis of 97 S. Pullorum strains was carried out to reconstruct the phylogeny and transmission history of S. Pullorum. Further analysis demonstrated that functional gene loss and acquisition occurred simultaneously throughout the evolution of S. Pullorum, both of which reflected adaptation to the changing environment. The result of our study will be helpful in surveillance and prevention of pullorum disease.

Published

2019

4. Genetic Markers in S. Paratyphi C Reveal Primary Adaptation to Pigs

Author

Satheesh Nair, Maria Fookes, Craig Corton, Nicholas R. Thomson, John Wain, and Gemma C. Langridge

Subjects

host adaptation, convergent evolution, genome degradation, genomic lesions, Biology (General), QH301-705.5

Abstract

Salmonella enterica with the identical antigenic formula 6,7:c:1,5 can be differentiated biochemically and by disease syndrome. One grouping, Salmonella Paratyphi C, is currently considered a typhoidal serovar, responsible for enteric fever in humans. The human-restricted typhoidal serovars (S. Typhi and Paratyphi A, B and C) typically display high levels of genome degradation and are cited as an example of convergent evolution for host adaptation in humans. However, S. Paratyphi C presents a different clinical picture to S. Typhi/Paratyphi A, in a patient group with predisposition, raising the possibility that its natural history is different, and that infection is invasive salmonellosis rather than enteric fever. Using whole genome sequencing and metabolic pathway analysis, we compared the genomes of 17 S. Paratyphi C strains to other members of the 6,7:c:1,5 group and to two typhoidal serovars: S. Typhi and Paratyphi A. The genome degradation observed in S. Paratyphi C was much lower than S. Typhi/Paratyphi A, but similar to the other 6,7:c:1,5 strains. Genomic and metabolic comparisons revealed little to no overlap between S. Paratyphi C and the other typhoidal serovars, arguing against convergent evolution and instead providing evidence of a primary adaptation to pigs in accordance with the 6,7:c:1.5 strains.

Published

2020

5. Ca. Endozoicomonas cretensis: A Novel Fish Pathogen Characterized by Genome Plasticity.

Author

Weihong Qi, Cascarano, Maria Chiara, Schlapbach, Ralph, Katharios, Pantelis, Vaughan, Lloyd, and Seth-Smith, Helena M. B.

Subjects

*FISH pathogens, *GENOMES, *BACTERIA, *SYMBIOSIS, *MARINE invertebrates, *SPONGES (Invertebrates)

Abstract

Endozoicomonas bacteria are generally beneficial symbionts of diverse marine invertebrates including reef-building corals, sponges, sea squirts, sea slugs, molluscs, and Bryozoans. In contrast, the recently reported Ca. Endozoicomonas cretensiswas identified as a vertebrate pathogen, causing epitheliocystis in fish larvae resulting inmassivemortality. Here, we described the Ca. E. cretensis draft genome, currently undergoing genome decay as evidenced by massive insertion sequence (IS element) expansion and pseudogene formation. Many of the insertion sequences are also predicted to carry outward-directed promoters, implying that they may be able to modulate the expression of neighbouring coding sequences (CDSs). Comparative genomic analysis has revealed many Ca. E. cretensis-specific CDSs, phage integration and novel gene families. Potential virulence related CDSs and machineries were identified in the genome, including secretion systems and related effector proteins, and systems related to biofilmformation and directed cellmovement. Mucin degradation would be of importance to a fish pathogen, and many candidate CDSs associated with this pathway have been identified. The genome may reflect a bacteriumin the process of changing niche fromsymbiont to pathogen, through expansion of virulence genes and some loss of metabolic capacity. [ABSTRACT FROM AUTHOR]

Published

2018

6. Cladogenesis and Genomic Streamlining in Extracellular Endosymbionts of Tropical Stink Bugs.

Author

Otero-Bravo, Alejandro, Goffredi, Shana, and Sabree, Zakee L.

Subjects

*ADAPTIVE radiation, *ENDOSYMBIOSIS, *STINKBUGS, *INSECT phylogeny, *INSECT genomes

Abstract

Phytophagous stink bugs are globally distributed and many harbor vertically inherited bacterial symbionts that are extracellular, yet little is known about how the symbiont's genomes have evolved under this transmission strategy. Genome reduction is common in insect intracellular symbionts but limited genome sampling of the extracellular symbionts of distantly related stink bugs has precluded inferring patterns of extracellular symbiont genome evolution. To address this knowledge gap, we completely sequenced the genomes of the uncultivable bacterial symbionts of four neotropical stink bugs of the Edessa genus. Phylogenetic and comparative analyses indicated that the symbionts form a clade within the Pantoea genus and their genomes are highly reduced (~0.8 Mb). Furthermore, genome synteny analysis and a jackknife approach for phylogenetic reconstruction, which corrected for long branch attraction artifacts, indicated that the Edessa symbionts were the result of a single symbiotic event that was distinct from the symbiosis event giving rise to Candidatus "Pantoea carbekii," the extracellular symbiont of the invasive pentatomid stink bug, Halyomorpha halys. Metabolic functions inferred from the Edessa symbiont genomes suggests a shift in genomic composition characteristic of its lifestyle in that they retained many host-supportive functions while undergoing dramatic gene loss and establishing a stable relationship with their host insects. Given the undersampled nature of extracellular insect symbionts, this study is the first comparative analysis of these symbiont genomes from four distinct Edessa stink bug species. Finally, we propose the candidate name "Candidatus Pantoea edessiphila" for the species of these symbionts with strain designations according to their host species. [ABSTRACT FROM AUTHOR]

Published

2018

7. Brucella Genetic Variability in Wildlife Marine Mammals Populations Relates to Host Preference and Ocean Distribution.

Author

Suárez-Esquivel, Marcela, Baker, Kate S., Ruiz-Villalobos, Nazareth, Hernández-Mora, Gabriela, Barquero-Calvo, Elías, González-Barrientos, Rocío, Castillo-Zeledón, Amanda, Jiménez-Rojas, César, Chacón-Díaz, Carlos, Cloeckaert, Axel, Chaves-Olarte, Esteban, Thomson, Nicholas R., Moreno, Edgardo, and Guzmán-Verri, Caterina

Subjects

*BRUCELLA, *PATHOGENIC microorganisms, *SINGLE nucleotide polymorphisms, *METABOLITE synthesis, *BACTERIAL diseases

Abstract

Intracellular bacterial pathogens probably arose when their ancestor adapted from a free-living environment to an intracellular one, leading to clonal bacteria with smaller genomes and less sources of genetic plasticity. Still, this plasticity is needed to respond to the challenges posed by the host. Members of the Brucella genus are facultative-extracellular intracellular bacteria responsible for causing brucellosis in a variety of mammals. The various species keep different host preferences, virulence, and zoonotic potential despite having 97-99% similarity at genome level. Here, we describe elements of genetic variation in Brucella ceti isolated from wildlife dolphins inhabiting the Pacific Ocean and the Mediterranean Sea. Comparison with isolates obtained from marine mammals from the Atlantic Ocean and the broader Brucella genus showed distinctive traits according to oceanic distribution and preferred host. Marine mammal isolates display genetic variability, represented by an important number of IS711 elements as well as specific IS711 and SNPs genomic distribution clustering patterns. Extensive pseudogenization was found among isolates from marine mammals as compared with terrestrial ones, causing degradation in pathways related to energy, transport of metabolites, and regulation/transcription. Brucella ceti isolates infecting particularly dolphin hosts, showed further degradation of metabolite transport pathways as well as pathways related to cell wall/membrane/envelope biogenesis and motility. Thus, gene loss through pseudogenization is a source of genetic variation in Brucella, which in turn, relates to adaptation to different hosts. This is relevant to understand the natural history of bacterial diseases, their zoonotic potential, and the impact of human interventions such as domestication. [ABSTRACT FROM AUTHOR]

Published

2017

8. Winding paths to simplicity: genome evolution in facultative insect symbionts.

Author

Wen-Sui Lo, Ya-Yi Huang, and Chih-Horng Kuo

Abstract

Symbiosis between organisms is an important driving force in evolution. Among the diverse relationships described, extensive progress has been made in insect–bacteria symbiosis, which improved our understanding of the genome evolution in host-associated bacteria. Particularly, investigations on several obligate mutualists have pushed the limits of what we know about the minimal genomes for sustaining cellular life. To bridge the gap between those obligate symbionts with extremely reduced genomes and their non-host-restricted ancestors, this review focuses on the recent progress in genome characterization of facultative insect symbionts. Notable cases representing various types and stages of host associations, including those from multiple genera in the family Enterobacteriaceae (class Gammaproteobacteria), Wolbachia (Alphaproteobacteria) and Spiroplasma (Mollicutes), are discussed. Although several general patterns of genome reduction associated with the adoption of symbiotic relationships could be identified, extensive variation was found among these facultative symbionts. These findings are incorporated into the established conceptual frameworks to develop a more detailed evolutionary model for the discussion of possible trajectories. In summary, transitions from facultative to obligate symbiosis do not appear to be a universal one-way street; switches between hosts and lifestyles (e.g. commensalism, parasitism or mutualism) occur frequently and could be facilitated by horizontal gene transfer. [ABSTRACT FROM AUTHOR]

Published

2016

9. Attenuation and Degeneration of SARS-CoV-2 Despite Adaptive Evolution.

Author

Liu Y

Abstract

The evolution of severe acute respiratory syndrome coronavirus 2 (SARS‑CoV‑2) has followed similar trends as other RNA viruses, such as human immunodeficiency virus type 1 and the influenza A virus. Rapid initial diversification was followed by strong competition and a rapid succession of dominant variants. Host-initiated RNA editing has been the primary mechanism for introducing mutations. A significant number of mutations detrimental to viral replication have been quickly purged. Fixed mutations are mostly diversifying mutations selected for host adaptation and immune evasion, with the latter accounting for the majority of the mutations. However, immune evasion often comes at the cost of functionality, and thus, optimal functionality is still far from being accomplished. Instead, selection for antibody-escaping variants and accumulation of near-neutral mutations have led to suboptimal codon usage and reduced replicative capacity, as demonstrated in non-respiratory cell lines. Beneficial adaptation of the virus includes reduced infectivity in lung tissues and increased tropism for the upper airway, resulting in shorter incubation periods, milder diseases, and more efficient transmission between people., Competing Interests: The authors have declared that no competing interests exist., (Copyright © 2023, Liu et al.)

Published

2023

10. Found and Lost: The Fates of Horizontally Acquired Genes in Arthropod-Symbiotic Spiroplasma.

Author

Wen-Sui Lo, Gasparich, Gail E., and Chih-Horng Kuo

Subjects

*SPIROPLASMAS, *HORIZONTAL gene transfer, *BIODIVERSITY research, *NUCLEOTIDE sequencing, *NUCLEOTIDE sequence, *DELETION mutation

Abstract

Horizontal gene transfer (HGT) is an important mechanism that contributed to biological diversity, particularly in bacteria. Through acquisition of novel genes, the recipient cell may change its ecological preference and the process could promote speciation. In this study, we determined the complete genome sequence of two Spiroplasma species for comparative analyses and inferred the putative gene gains and losses. Although most Spiroplasma species are symbionts of terrestrial insects, Spiroplasma eriocheiris has evolved to be a lethal pathogen of freshwater crustaceans. We found that approximately 7%of the genes in this genome may have originated from HGT and these genes expanded the metabolic capacity of this organism. Through comparison with the closely related Spiroplasma atrichopogonis, as well as other more divergent lineages, our results indicated that these HGT events could be traced back to the most recent common ancestor of these two species. However, most of these horizontally acquired genes have been pseudogenized in S. atrichopogonis, suggesting that they did not contribute to the fitness of this lineage that maintained the association with terrestrial insects. Thus, accumulation of small deletions that disrupted these foreign genes was not countered by natural selection. On the other hand, the long-term survival of these horizontally acquired genes in the S. eriocheiris genome hinted that they might play a role in the ecological shift of this species. Finally, the implications of these findings and the conflicts among gene content, 16S rRNA gene sequencing, and serological typing, are discussed in light of defining bacterial species. [ABSTRACT FROM AUTHOR]

Published

2015

11. Kinetoplast adaptations in American strains from Trypanosoma vivax.

Author

Greif, Gonzalo, Rodriguez, Matías, Reyna-Bello, Armando, Robello, Carlos, and Alvarez-Valin, Fernando

Subjects

*KINETOPLASTS, *BIOLOGICAL adaptation, *TRYPANOSOMA, *PHYSIOLOGIC strain, *PHOSPHORYLATION, *BIOLOGICAL evolution

Abstract

The mitochondrion role changes during the digenetic life cycle of African trypanosomes. Owing to the low abundance of glucose in the insect vector (tsetse flies) the parasites are dependent upon a fully functional mitochondrion, capable of performing oxidative phosphorylation. Nevertheless, inside the mammalian host (bloodstream forms), which is rich in nutrients, parasite proliferation relies on glycolysis, and the mitochondrion is partially redundant. In this work we perform a comparative study of the mitochondrial genome (kinetoplast) in different strains of Trypanosoma vivax . The comparison was conducted between a West African strain that goes through a complete life cycle and two American strains that are mechanically transmitted (by different vectors) and remain as bloodstream forms only. It was found that while the African strain has a complete and apparently fully functional kinetoplast, the American T. vivax strains have undergone a drastic process of mitochondrial genome degradation, in spite of the recent introduction of these parasites in America. Many of their genes exhibit different types of mutations that are disruptive of function such as major deletions, frameshift causing indels and missense mutations. Moreover, all but three genes (A6-ATPase, RPS12 and MURF2) are not edited in the American strains, whereas editing takes place normally in all (editable) genes from the African strain. Two of these genes, A6-ATPase and RPS12, are known to play an essential function during bloodstream stage. Analysis of the minicircle population shows that its diversity has been greatly reduced, remaining mostly those minicircles that carry guide RNAs necessary for the editing of A6-ATPase and RPS12. The fact that these two genes remain functioning normally, as opposed to that reported in Trypanosoma brucei -like trypanosomes that restrict their life cycle to the bloodstream forms, along with other differences, is indicative that the American T. vivax strains are following a novel evolutionary pathway. [ABSTRACT FROM AUTHOR]

Published

2015

12. Rekonstrukce metabolických drah bakterií Legionella polyplacis a Candidatus Riesia pediculischaeffi, symbiontů vší

Author

ZADINOVÁ, Zuzana

Subjects

degradace genomu, puriny, sucking lice, pyrimidiny, vitamíny B, citrátový cyklus, pentose phosphate pathway, endosymbióza, glykolýza, symbionti hmyzu, pyrimidines, amino acids, B vitamins, Legionella polyplacis, pentózofosfátový cyklus, obsah GC, metabolism, citrate cycle, insect symbionts, glycolysis, GC content, aminokyseliny, metabolismus, vši, Candidatus Riesia pediculischaeffi, endosymbiosis, oxidační fosforylace, oxidative phosphorylation, genome degradation, purines

Abstract

The genomes of two bacteria, Legionella polyplacis and Candidatus Riesia pediculischaeffi, lice endosymbionts, were examined and compared. Preserved genes were identified, assigned to appropriate metabolic pathways, and listed in an electronic attachment table. Completeness and functionality were assessed for individual metabolic pathways. Based on the results, metabolic maps were created for both bacteria

Published

2021

13. Genetic markers in s. Paratyphi c reveal primary adaptation to pigs

Author

Gemma C. Langridge, Maria Fookes, John Wain, Craig Corton, Satheesh Nair, and Nicholas R. Thomson

Subjects

Microbiology (medical), Serotype, genome degradation, Microbiology, Genome, complex mixtures, Article, 03 medical and health sciences, fluids and secretions, Antigen, Virology, convergent evolution, lcsh:QH301-705.5, 030304 developmental biology, Genetics, Whole genome sequencing, 0303 health sciences, biology, 030306 microbiology, host adaptation, biology.organism_classification, genomic lesions, lcsh:Biology (General), Salmonella enterica, Genetic marker, bacteria, Host adaptation, Adaptation

Abstract

Salmonella enterica with the identical antigenic formula 6,7:c:1,5 can be differentiated biochemically and by disease syndrome. One grouping, Salmonella Paratyphi C, is currently considered a typhoidal serovar, responsible for enteric fever in humans. The human-restricted typhoidal serovars (S. Typhi and Paratyphi A, B and C) typically display high levels of genome degradation and are cited as an example of convergent evolution for host adaptation in humans. However, S. Paratyphi C presents a different clinical picture to S. Typhi/Paratyphi A, in a patient group with predisposition, raising the possibility that its natural history is different, and that infection is invasive salmonellosis rather than enteric fever. Using whole genome sequencing and metabolic pathway analysis, we compared the genomes of 17 S. Paratyphi C strains to other members of the 6,7:c:1,5 group and to two typhoidal serovars: S. Typhi and Paratyphi A. The genome degradation observed in S. Paratyphi C was much lower than S. Typhi/Paratyphi A, but similar to the other 6,7:c:1,5 strains. Genomic and metabolic comparisons revealed little to no overlap between S. Paratyphi C and the other typhoidal serovars, arguing against convergent evolution and instead providing evidence of a primary adaptation to pigs in accordance with the 6,7:c:1.5 strains.

Published

2020

14. A New Family of DNA Viruses Causing Disease in Crustaceans from Diverse Aquatic Biomes

Author

Rose Kerr, Jamie Bojko, Grant D. Stentiford, Kuttichantran Subramaniam, David Bass, Thomas B. Waltzek, Kelly S. Bateman, Natalya Yutin, Abigail S. Clark, Donald C. Behringer, Eugene V. Koonin, and Ronny van Aerle

Subjects

low-complexity sequences, large nucleocytoplasmic DNA viruses, Brachyura, viruses, genome degradation, Oceans and Seas, Ecological and Evolutionary Science, Genome, Viral, 030312 virology, Biology, Nucleocytoplasmic large DNA viruses, Genome, Microbiology, Virus, Evolution, Molecular, 03 medical and health sciences, Penaeidae, Virology, Crustacea, Animals, Giant Virus, Palinuridae, Gene, Host cell nucleus, Ecosystem, Phylogeny, 030304 developmental biology, virus evolution, 0303 health sciences, fungi, DNA Viruses, Genomics, biology.organism_classification, QR1-502, United Kingdom, Metagenomics, Evolutionary biology, Viral evolution, Research Article

Abstract

Recent genomic and metagenomic studies have led to a dramatic expansion of the known diversity of nucleocytoplasmic large DNA viruses (NCLDVs) of eukaryotes, which include giant viruses of protists and important pathogens of vertebrates, such as poxviruses. However, the characterization of viruses from nonmodel hosts still lags behind. We sequenced the complete genomes of three viruses infecting crustaceans, the Caribbean spiny lobster, demon shrimp, and European shore crab. These viruses have the smallest genomes among the known NCLDVs, with losses of many core genes, some of which are shared with iridoviruses. The deterioration of the transcription apparatus is compatible with microscopic and ultrastructural observations indicating that these viruses replicate in the nucleus of infected cells rather than in the cytoplasm. Phylogenomic analysis indicates that these viruses are sufficiently distinct from all other NCLDVs to justify the creation of a separate family, for which we propose the name “Mininucleoviridae” (i.e., small viruses reproducing in the cell nucleus)., Panulirus argus virus 1 (PaV1) is the only known virus infecting the Caribbean spiny lobster (Panulirus argus) from the Caribbean Sea. Recently, related viruses, Dikerogammarus haemobaphes virus 1 (DhV1) and Carcinus maenas virus 1 (CmV1), have been detected in the demon shrimp (Dikerogammarus haemobaphes) and the European shore crab (Carcinus maenas), respectively, from sites in the United Kingdom. The virion morphology of these crustacean viruses is similar to that of iridoviruses. However, unlike iridoviruses and other nucleocytoplasmic large DNA viruses (NCLDVs), these viruses complete their morphogenesis in the host cell nucleus rather than in the cytoplasm. To date, these crustacean viruses have remained unclassified due to a lack of genomic data. Using an Illumina MiSeq sequencer, we sequenced the complete genomes of PaV1, CmV1, and DhV1. Comparative genome analysis shows that these crustacean virus genomes encode the 10 hallmark proteins previously described for the NCLDVs of eukaryotes, strongly suggesting that they are members of this group. With a size range of 70 to 74 kb, these are the smallest NCLDV genomes identified to date. Extensive gene loss, divergence of gene sequences, and the accumulation of low-complexity sequences reflect the extreme degradation of the genomes of these “minimal” NCLDVs rather than any direct relationship with the NCLDV ancestor. Phylogenomic analysis supports the classification of these crustacean viruses as a distinct family, “Mininucleoviridae,” within the pitho-irido-Marseille branch of the NCLDVs.

Published

2020

15. Cladogenesis and Genomic Streamlining in Extracellular Endosymbionts of Tropical Stink Bugs

Author

Zakee L. Sabree, Shana K. Goffredi, and Alejandro Otero-Bravo

Subjects

0301 basic medicine, Genome evolution, animal structures, Genetic Speciation, genome degradation, Citric Acid Cycle, 030106 microbiology, genome evolution, Biology, Genome, Heteroptera, 03 medical and health sciences, Terminology as Topic, primary symbiont, Genetics, Animals, Symbiosis, Ecology, Evolution, Behavior and Systematics, Long branch attraction, Phylogenetic tree, Pantoea, Host (biology), fungi, food and beverages, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, 030104 developmental biology, Cladogenesis, Evolutionary biology, Candidatus, bacteria, neotropical stink bug, Genome, Bacterial, Research Article

Abstract

Phytophagous stink bugs are globally distributed and many harbor vertically inherited bacterial symbionts that are extracellular, yet little is known about how the symbiont’s genomes have evolved under this transmission strategy. Genome reduction is common in insect intracellular symbionts but limited genome sampling of the extracellular symbionts of distantly related stink bugs has precluded inferring patterns of extracellular symbiont genome evolution. To address this knowledge gap, we completely sequenced the genomes of the uncultivable bacterial symbionts of four neotropical stink bugs of the Edessa genus. Phylogenetic and comparative analyses indicated that the symbionts form a clade within the Pantoea genus and their genomes are highly reduced (∼0.8 Mb). Furthermore, genome synteny analysis and a jackknife approach for phylogenetic reconstruction, which corrected for long branch attraction artifacts, indicated that the Edessa symbionts were the result of a single symbiotic event that was distinct from the symbiosis event giving rise to Candidatus “Pantoea carbekii,” the extracellular symbiont of the invasive pentatomid stink bug, Halyomorpha halys. Metabolic functions inferred from the Edessa symbiont genomes suggests a shift in genomic composition characteristic of its lifestyle in that they retained many host-supportive functions while undergoing dramatic gene loss and establishing a stable relationship with their host insects. Given the undersampled nature of extracellular insect symbionts, this study is the first comparative analysis of these symbiont genomes from four distinct Edessa stink bug species. Finally, we propose the candidate name “Candidatus Pantoea edessiphila” for the species of these symbionts with strain designations according to their host species.

Published

2018

16. How does the 'ancient' asexual Philodina roseola (Rotifera: Bdelloidea) handle potential UVB-induced mutations?

Author

Fischer, Claus, Ahlrichs, Wilko H., Buma, Anita G. J., van de Poll, Willem H., and Bininda-Emonds, Olaf R. P.

Subjects

*ASEXUAL reproduction, *GENOMES, *GENETIC mutation, *ULTRAVIOLET radiation, *REPAIRING, *DNA

Abstract

Like other obligate asexuals, bdelloid rotifers are expected to suffer from degradation of their genomes through processes including the accumulation of deleterious mutations. However, sequence-based analyses in this regard remain inconclusive. Instead of looking for historical footprints of mutations in these ancient asexuals, we directly examined the susceptibility and ability to repair point mutations by the bdelloid Philodina roseola by inducing cyclobutane-pyrimidine dimers (CPDs) via exposure to UVB radiation (280-320nm). For comparison, we performed analogous experiments with the facultative asexual monogonont rotifer Brachionus rubens. Different strategies were found for the two species. Philodina roseola appeared to shield itself from CPD induction through uncharacterized UV-absorbing compounds and, except for the genome reconstruction that occurs after desiccation, was largely unable to repair UVB-induced damage. By contrast, B. rubens was more susceptible to UVB irradiation, but could repair all induced damage in ~2h. In addition, whereas UV irradiation had a significant negative impact on the reproductive output of P. roseola, and especially so after desiccation, that of B. rubens was unaffected. Although the strategy of P. roseola might suffice under natural conditions where UVB irradiation is less intense, the lack of any immediate CPD repair mechanisms in this species remains perplexing. It remains to be investigated how typical these results are for bdelloids as a group and therefore how reliant these animals are on desiccation-dependent genome repair to correct potential DNA damage given their obligate asexual lifestyle. [ABSTRACT FROM AUTHOR]

Published

2013

17. Factors Behind Junk DNA in Bacteria.

Author

Gil, Rosario and Latorre, Amparo

Subjects

*DNA analysis, *BACTERIAL genomes, *COMPARATIVE genomics, *GENOMES, *MOLECULAR genetics

Abstract

Although bacterial genomes have been traditionally viewed as being very compact, with relatively low amounts of repetitive and non-coding DNA, this view has dramatically changed in recent years. The increase of available complete bacterial genomes has revealed that many species present abundant repetitive DNA (i.e., insertion sequences, prophages or paralogous genes) and that many of these sequences are not functional but can have evolutionary consequences as concerns the adaptation to specialized host-related ecological niches. Comparative genomics analyses with close relatives that live in non- specialized environments reveal the nature and fate of this bacterial junk DNA. In addition, the number of insertion sequences and pseudogenes, as well as the size of the intergenic regions, can be used as markers of the evolutionary stage of a genome. [ABSTRACT FROM AUTHOR]

Published

2012

18. Symbiosis as an adaptive process and source of phenotypic complexity.

Author

Moran, Nancy A.

Subjects

*SYMBIOSIS, *BIOLOGY, *GENOMICS, *GENES, *GENOMES, *PROKARYOTES

Abstract

Genomics has revealed that inheritance systems of separate species are often not well segregated: genes and capabilities that evolve in one lineage are often stably acquired by another lineage. Although direct gene transfer between species has occurred at some level in all major groups, it appears to be far more frequent in prokaryotes than in multicellular eukaryotes. An alternative to incorporating novel genes into a recipient genome is acquiring a stable, possibly heritable, symbiotic association and thus enjoying benefits of complementary metabolic capabilities. These kinds of symbioses have arisen frequently in animals; for example, many insect groups have diversified on the basis of symbiotic associations acquired early in their evolutionary histories. The resulting associations are highly complex, often involving specialized cell types and organs, developmental mechanisms that ensure transfer of symbionts between generations, and mechanisms for controlling symbiont proliferation and location. The genomes of long-term obligate symbionts often undergo irreversible gene loss and deterioration even as hosts evolve dependence on them. In some cases, animal genomes may have acquired genes from symbionts, mirroring the gene uptake from mitochondrial and plastid genomes. Multiple symbionts often coexist in the same host, resulting in coadaptation among several phylogenetically distant genomes. [ABSTRACT FROM AUTHOR]

Published

2007

19. Genome deterioration: loss of repeated sequences and accumulation of junk DNA.

Author

Carolin Frank, A., Amiri, Haleh, and Andersson, Siv

Abstract

A global survey of microbial genomes reveals a correlation between genome size, repeat content and lifestyle. Free-living bacteria have large genomes with a high content of repeated sequences and self-propagating DNA, such as transposons and bacteriophages. In contrast, obligate intracellular bacteria have small genomes with a low content of repeated sequences and no or few genetic parasites. In extreme cases, such as in the 650 kb-genomes of aphid endosymbionts of the genus Buchnera all repeated sequences above 200 bp have been eliminated. We speculate that the initial downsizing of the genomes of obligate symbionts and parasites occurred by homologous recombination at repeated genes, leading to the loss of large blocks of DNA as well as to the consumption of repeated sequences. Further sequence elimination in these small genomes seems primarily to result from the accumulation of short deletions within genic sequences. This process may lead to temporary increases in the genomic content of pseudogenes and ‘junk’ DNA. We discuss causes and long-term consequences of extreme genome size reductions in obligate intracellular bacteria. [ABSTRACT FROM AUTHOR]

Published

2002

20. Loss and Gain in the Evolution of the Salmonella enterica Serovar Gallinarum Biovar Pullorum Genome

Author

Qiuchun Li, Xinan Jiao, Yaohui Xu, Zhenyu Wang, Yachen Hu, Bin Qiang, and Xiang Chen

Subjects

Serotype, China, Biovar, animal diseases, genome degradation, lcsh:QR1-502, Virulence, Ecological and Evolutionary Science, genomic epidemiology, Serogroup, Polymorphism, Single Nucleotide, Microbiology, lcsh:Microbiology, Evolution, Molecular, 03 medical and health sciences, Bacterial Proteins, Phylogenetics, multidrug resistance, evolution, Animals, Molecular Biology, Phylogeny, Poultry Diseases, Prophage, 030304 developmental biology, Genetics, Salmonella Infections, Animal, 0303 health sciences, Whole Genome Sequencing, biology, Phylogenetic tree, 030306 microbiology, Genetic heterogeneity, Salmonella enterica, Bayes Theorem, biology.organism_classification, QR1-502, Salmonella enterica serovar Gallinarum biovar Pullorum, Chickens, Genome, Bacterial, Research Article

Abstract

Pullorum disease, an acute poultry septicemia caused by Salmonella Gallinarum biovar Pullorum, is fatal for young chickens and is a heavy burden on poultry industry. The pathogen is rare in most developed countries but still extremely difficult to eliminate in China. Efficient epidemiological surveillance necessitates clarifying the origin of the isolates from different regions and their phylogenic relationships. Genomic epidemiological analysis of 97 S. Pullorum strains was carried out to reconstruct the phylogeny and transmission history of S. Pullorum. Further analysis demonstrated that functional gene loss and acquisition occurred simultaneously throughout the evolution of S. Pullorum, both of which reflected adaptation to the changing environment. The result of our study will be helpful in surveillance and prevention of pullorum disease., Salmonella enterica subspecies enterica serovar Gallinarum biovar Pullorum (S. Pullorum) is the etiological agent of pullorum disease, causing white diarrhea with high mortality in chickens. There are many unsolved issues surrounding the epidemiology of S. Pullorum, including its origin and transmission history as well as the discordance between its phenotypic heterogeneity and genetic monomorphism. In this paper, we report the results of whole-genome sequencing of a panel of 97 S. Pullorum strains isolated between 1962 and 2014 from four countries across three continents. We utilized 6,795 core genome single nucleotide polymorphisms (SNPs) to reconstruct a phylogenetic tree within a spatiotemporal Bayesian framework, estimating that the most recent common ancestor of S. Pullorum emerged in ∼914 CE (95% confidence interval [95%CI], 565 to 1273 CE). The extant S. Pullorum strains can be divided into four distinct lineages, each of which is significantly associated with geographical distribution. The intercontinental transmissions of lineages III and IV can be traced to the mid-19th century and are probably related to the “Hen Fever” prevalent at that time. Further genomic analysis indicated that the loss or pseudogenization of functional genes involved in metabolism and virulence in S. Pullorum has been ongoing since before and after divergence from the ancestor. In contrast, multiple prophages and plasmids have been acquired by S. Pullorum, and these have endowed it with new characteristics, especially the multidrug resistance conferred by two large plasmids in lineage I. The results of this study provide insight into the evolution of S. Pullorum and prove the efficiency of whole-genome sequencing in epidemiological surveillance of pullorum disease. IMPORTANCE Pullorum disease, an acute poultry septicemia caused by Salmonella Gallinarum biovar Pullorum, is fatal for young chickens and is a heavy burden on poultry industry. The pathogen is rare in most developed countries but still extremely difficult to eliminate in China. Efficient epidemiological surveillance necessitates clarifying the origin of the isolates from different regions and their phylogenic relationships. Genomic epidemiological analysis of 97 S. Pullorum strains was carried out to reconstruct the phylogeny and transmission history of S. Pullorum. Further analysis demonstrated that functional gene loss and acquisition occurred simultaneously throughout the evolution of S. Pullorum, both of which reflected adaptation to the changing environment. The result of our study will be helpful in surveillance and prevention of pullorum disease.

Published

2019

21. Adaptation and genomic erosion in fragmented Pseudomonas aeruginosa populations in the sinuses of people with cystic fibrosis.

Author

Armbruster, Catherine R., Marshall, Christopher W., Garber, Arkadiy I., Melvin, Jeffrey A., Zemke, Anna C., Moore, John, Zamora, Paula F., Li, Kelvin, Fritz, Ian L., Manko, Christopher D., Weaver, Madison L., Gaston, Jordan R., Morris, Alison, Methé, Barbara, DePas, William H., Lee, Stella E., Cooper, Vaughn S., and Bomberger, Jennifer M.

Abstract

Pseudomonas aeruginosa notoriously adapts to the airways of people with cystic fibrosis (CF), yet how infection-site biogeography and associated evolutionary processes vary as lifelong infections progress remains unclear. Here we test the hypothesis that early adaptations promoting aggregation influence evolutionary-genetic trajectories by examining longitudinal P. aeruginosa from the sinuses of six adults with CF. Highly host-adapted lineages harbored mutator genotypes displaying signatures of early genome degradation associated with recent host restriction. Using an advanced imaging technique (MiPACT-HCR [microbial identification after passive clarity technique]), we find population structure tracks with genome degradation, with the most host-adapted, genome-degraded P. aeruginosa (the mutators) residing in small, sparse aggregates. We propose that following initial adaptive evolution in larger populations under strong selection for aggregation, P. aeruginosa persists in small, fragmented populations that experience stronger effects of genetic drift. These conditions enrich for mutators and promote degenerative genome evolution. Our findings underscore the importance of infection-site biogeography to pathogen evolution. [Display omitted] • Selection favors P. aeruginosa mutations that promote aggregation in the CF sinuses • Aggregation and bottlenecks fragment populations, amplifying effects of genetic drift • Mutators persist in small populations and drive early genome degradation • Population size and infection-site biogeography impact evolutionary trajectories Armbruster et al. find that infection-site biogeography impacts evolution of the opportunistic pathogen, Pseudomonas aeruginosa. In the sinuses of adults with cystic fibrosis, P. aeruginosa residing in large, dense aggregates adaptively evolves, whereas small, sparse aggregates experience greater effects of genetic drift and early stages of degenerative genome evolution. [ABSTRACT FROM AUTHOR]

Published

2021

22. Ca. Endozoicomonas cretensis: A Novel Fish Pathogen Characterized by Genome Plasticity

Author

Maria Chiara Cascarano, Weihong Qi, Helena M. B. Seth-Smith, Ralph Schlapbach, Pantelis Katharios, Lloyd Vaughan, University of Zurich, and Seth-Smith, Helena M B

Subjects

0301 basic medicine, Aquatic Organisms, mobile elements, Sequence analysis, genome degradation, Pseudogene, Cell Plasticity, Virulence, 610 Medicine & health, 10071 Functional Genomics Center Zurich, Biology, Genome, host–pathogen, resistance, virulence, genome decay, 03 medical and health sciences, 1311 Genetics, Genetics, Animals, 14. Life underwater, Insertion sequence, Symbiosis, Pathogen, Gene, Phylogeny, Ecology, Evolution, Behavior and Systematics, Bacteria, Coral Reefs, Effector, Fishes, Sequence Analysis, DNA, Genome Report, 1105 Ecology, Evolution, Behavior and Systematics, 030104 developmental biology, Vertebrates, DNA Transposable Elements, 570 Life sciences, biology, Genome, Bacterial, Pseudogenes

Abstract

Endozoicomonas bacteria are generally beneficial symbionts of diverse marine invertebrates including reef-building corals, sponges, sea squirts, sea slugs, molluscs, and Bryozoans. In contrast, the recently reported Ca. Endozoicomonas cretensis was identified as a vertebrate pathogen, causing epitheliocystis in fish larvae resulting in massive mortality. Here, we described the Ca. E. cretensis draft genome, currently undergoing genome decay as evidenced by massive insertion sequence (IS element) expansion and pseudogene formation. Many of the insertion sequences are also predicted to carry outward-directed promoters, implying that they may be able to modulate the expression of neighbouring coding sequences (CDSs). Comparative genomic analysis has revealed many Ca. E. cretensis-specific CDSs, phage integration and novel gene families. Potential virulence related CDSs and machineries were identified in the genome, including secretion systems and related effector proteins, and systems related to biofilm formation and directed cell movement. Mucin degradation would be of importance to a fish pathogen, and many candidate CDSs associated with this pathway have been identified. The genome may reflect a bacterium in the process of changing niche from symbiont to pathogen, through expansion of virulence genes and some loss of metabolic capacity. ISSN:1759-6653

Published

2018

23. Brucella genetic variability in wildlife marine mammals populations relates to host preference and ocean distribution

Author

Rocío González-Barrientos, Esteban Chaves-Olarte, Nazareth Ruiz-Villalobos, Amanda Castillo-Zeledón, Elías Barquero-Calvo, Edgardo Moreno, Carlos Chacón-Díaz, César Jiménez-Rojas, Kate S. Baker, Caterina Guzmán-Verri, Marcela Suárez-Esquivel, Gabriela Hernández-Mora, Axel Cloeckaert, Nicholas R. Thomson, Universidad Nacional, Heredia, The Wellcome Trust Sanger Institute [Cambridge], University of Liverpool, Ministerio de Agricultura y Ganadería, Partenaires INRAE, Universidad de Costa Rica (UCR), Infectiologie et Santé Publique (UMR ISP), Institut National de la Recherche Agronomique (INRA)-Université de Tours (UT), Univ Costa Rica, Fac Microbiol, Ctr Invest Enfermedades Trop, San Jose, Costa Rica, FEES-CONARE, Costa Rica, Ministry of Science and Technology of Costa Rica Forinves FV-004-13, Wellcome Trust 098051, UCR scholarships, Wellcome Trust Postdoctoral Training Fellowship for Clinicians 106690/Z/14/Z, and Institut National de la Recherche Agronomique (INRA)-Université de Tours

Subjects

0301 basic medicine, DNA, Bacterial, phylogénétique, [SDV.OT]Life Sciences [q-bio]/Other [q-bio.OT], caractère phénotypique, Dolphins, genome degradation, variabilité génétique, Virulence, Animals, Wild, Brucella, Genome, Brucellosis, 03 medical and health sciences, MARINE MAMMALS, Genetic variation, Genetics, Animals, BRUCELLA, 14. Life underwater, Genetic variability, marine mammals, Ecology, Evolution, Behavior and Systematics, Phylogeny, Phenotypic plasticity, GENOTIPOS, biology, Ecology, Intracellular parasite, adn, Genetic Variation, mammifère marin, Gene Expression Regulation, Bacterial, 15. Life on land, biology.organism_classification, MAMIFEROS MARINOS, 030104 developmental biology, BRUCELOSIS, Evolutionary biology, Brucella ceti, Host-Pathogen Interactions, bactérie intracellulaire, souche bactérienne, GENOME DEGRADATION, Research Article, Autre (Sciences du Vivant)

Abstract

Intracellular bacterial pathogens probably arose when their ancestor adapted from a free-living environment to an intracellular one, leading to clonal bacteria with smaller genomes and less sources of genetic plasticity. Still, this plasticity is needed to respond to the challenges posed by the host. Members of the Brucella genus are facultative-extracellularintracellularbacteriaresponsibleforcausing brucellosis in a variety of mammals. The various species keep different host preferences, virulence, and zoonotic potential despite having 97–99% similarity at genome level. Here, we describe elements of genetic variation in Brucella ceti isolated from wildlife dolphins inhabiting the Pacific Ocean and the Mediterranean Sea. Comparison with isolates obtained from marine mammals from the Atlantic Ocean and the broader Brucella genus showed distinctive traits according to oceanic distribution and preferred host. Marine mammal isolates display genetic variability, represented by an important number of IS711 elements as well as specific IS711 and SNPs genomic distribution clustering patterns. Extensive pseudogenization was found among isolates from marine mammals as compared with terrestrial ones, causing degradation in pathways related to energy, transport of metabolites, and regulation/transcription. Brucella ceti isolates infecting particularly dolphin hosts, showed further degradation of metabolite transport pathways as well as pathways related to cell wall/membrane/envelope biogenesis and motility. Thus, gene loss through pseudogenization is a source of genetic variation in Brucella, which in turn, relates to adaptation to different hosts. This is relevant to understand the natural history of bacterial diseases, their zoonotic potential, and the impact of human interventions such as domestication. Los patógenos bacterianos intracelulares probablemente surgieron cuando su antepasado se adaptó de un entorno de vida libre a uno intracelular, lo que dio lugar a bacterias clonales con genomas más pequeños y menos fuentes de plasticidad genética. Aún así, esta plasticidad es necesaria para responder a los desafíos que plantea el huésped. Los miembros del género Brucella son bacterias facultativas-extracelulares-intracelulares responsables de causar brucelosis en una variedad de mamíferos. Las diversas especies mantienen diferentes preferencias en cuanto a huéspedes, virulencia y potencial zoonótico a pesar de que tienen una similitud del 97 al 99% a nivel del genoma. Aquí describimos elementos de la variación genética en Brucella ceti aislados de los delfines salvajes que habitan en el Océano Pacífico y el Mar Mediterráneo. La comparación con los aislamientos obtenidos de mamíferos marinos del Océano Atlántico y del género Brucella, más amplio, mostró rasgos distintivos según la distribución oceánica y el huésped preferido. Los aislados de mamíferos marinos muestran una variabilidad genética, representada por un número importante de elementos IS711, así como por patrones de agrupación de la distribución genómica específicos de IS711 y SNPs. Se encontró una amplia pseudogenización entre los aislados de mamíferos marinos en comparación con los terrestres, lo que causó una degradación en las vías relacionadas con la energía, el transporte de metabolitos y la regulación/transcripción. Los aislamientos de Brucella ceti que infectan particularmente a los delfines huéspedes, mostraron una mayor degradación de las vías de transporte de metabolitos así como de las vías relacionadas con la biogénesis y la motilidad de la pared celular/membrana/superficie. Así pues, la pérdida de genes por pseudogenización es una fuente de variación genética en Brucella, que a su vez, se relaciona con la adaptación a diferentes huéspedes. Esto es pertinente para comprender la historia natural de las enfermedades bacterianas, su potencial zoonótico y el impacto de las intervenciones humanas, como la domesticación. Universidad Nacional, Costa Rica Escuela de Medicina Veterinaria

Published

2017

24. Genetic Markers in S. Paratyphi C Reveal Primary Adaptation to Pigs.

Author

Nair, Satheesh, Fookes, Maria, Corton, Craig, Thomson, Nicholas R., Wain, John, and Langridge, Gemma C.

Subjects

GENETIC markers, TYPHOID fever, CONVERGENT evolution, SALMONELLA enterica, PHYSIOLOGICAL adaptation

Abstract

Salmonella enterica with the identical antigenic formula 6,7:c:1,5 can be differentiated biochemically and by disease syndrome. One grouping, Salmonella Paratyphi C, is currently considered a typhoidal serovar, responsible for enteric fever in humans. The human-restricted typhoidal serovars (S. Typhi and Paratyphi A, B and C) typically display high levels of genome degradation and are cited as an example of convergent evolution for host adaptation in humans. However, S. Paratyphi C presents a different clinical picture to S. Typhi/Paratyphi A, in a patient group with predisposition, raising the possibility that its natural history is different, and that infection is invasive salmonellosis rather than enteric fever. Using whole genome sequencing and metabolic pathway analysis, we compared the genomes of 17 S. Paratyphi C strains to other members of the 6,7:c:1,5 group and to two typhoidal serovars: S. Typhi and Paratyphi A. The genome degradation observed in S. Paratyphi C was much lower than S. Typhi/Paratyphi A, but similar to the other 6,7:c:1,5 strains. Genomic and metabolic comparisons revealed little to no overlap between S. Paratyphi C and the other typhoidal serovars, arguing against convergent evolution and instead providing evidence of a primary adaptation to pigs in accordance with the 6,7:c:1.5 strains. [ABSTRACT FROM AUTHOR]

Published

2020

25. Pseudogenization of the Secreted Effector Gene sseI Confers Rapid Systemic Dissemination of S. Typhimurium ST313 within Migratory Dendritic Cells

Author

Trung H.M. Pham, Kyler A. Lugo, Donna M. Bouley, Renée M. Tsolis, Jared Honeycutt, Denise M. Monack, Gregory T. Walker, Amanda Jacobson, Sarah Carden, and Juliana Idoyaga

Subjects

0301 basic medicine, Male, Salmonella typhimurium, pseudogene, Bacteremia, Inbred C57BL, Genome, iNTS, Mice, Cell Movement, Receptors, Mesenteric lymph nodes, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, Aetiology, Genetics, Mice, Knockout, Effector, pathogenesis, Bacterial, Hematology, Foodborne Illness, Phenotype, Gastroenteritis, medicine.anatomical_structure, T3SS effectors, Infectious Diseases, Medical Microbiology, Host-Pathogen Interactions, Salmonella Infections, Female, Host adaptation, Infection, NTS, nontyphoidal Salmonella, Receptors, CCR7, Lineage (genetic), Knockout, genome degradation, 030106 microbiology, Immunology, Biology, Communicable Diseases, Microbiology, Article, Vaccine Related, 03 medical and health sciences, SrfH, Virology, Biodefense, evolution, medicine, Humans, Animals, Gene, niche adaptation, Animal, Prevention, Biological Transport, Dendritic Cells, Gene Expression Regulation, Bacterial, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Emerging Infectious Diseases, Gene Expression Regulation, Genes, Genes, Bacterial, Disease Models, Parasitology, Lymph Nodes, Niche adaptation, Digestive Diseases, CCR7

Abstract

© 2017 Elsevier Inc. Genome degradation correlates with host adaptation and systemic disease in Salmonella. Most lineages of the S. enterica subspecies Typhimurium cause gastroenteritis in humans; however, the recently emerged ST313 lineage II pathovar commonly causes systemic bacteremia in sub-Saharan Africa. ST313 lineage II displays genome degradation compared to gastroenteritis-associated lineages; yet, the mechanisms and causal genetic differences mediating these infection phenotypes are largely unknown. We find that the ST313 isolate D23580 hyperdisseminates from the gut to systemic sites, such as the mesenteric lymph nodes (MLNs), via CD11b+ migratory dendritic cells (DCs). This hyperdissemination was facilitated by the loss of sseI, which encodes an effector that inhibits DC migration in gastroenteritis-associated isolates. Expressing functional SseI in D23580 reduced the number of infected migratory DCs and bacteria in the MLN. Our study reveals a mechanism linking pseudogenization of effectors with the evolution of niche adaptation in a bacterial pathogen.

Published

2016

26. Factors Behind Junk DNA in Bacteria

Author

Rosario Gil and Amparo Latorre

Subjects

Comparative genomics, Genetics, lcsh:QH426-470, Pseudogene, genome degradation, junk DNA, pseudogenes, Bacterial genome size, Review, Biology, intergenic regions (IGR), Genome, Noncoding DNA, lcsh:Genetics, Intergenic region, insertion sequences (IS), Insertion sequence, Gene, Genetics (clinical)

Abstract

Although bacterial genomes have been traditionally viewed as being very compact, with relatively low amounts of repetitive and non-coding DNA, this view has dramatically changed in recent years. The increase of available complete bacterial genomes has revealed that many species present abundant repetitive DNA (i.e., insertion sequences, prophages or paralogous genes) and that many of these sequences are not functional but can have evolutionary consequences as concerns the adaptation to specialized host-related ecological niches. Comparative genomics analyses with close relatives that live in non-specialized environments reveal the nature and fate of this bacterial junk DNA. In addition, the number of insertion sequences and pseudogenes, as well as the size of the intergenic regions, can be used as markers of the evolutionary stage of a genome.

Published

2012

27. A New Family of DNA Viruses Causing Disease in Crustaceans from Diverse Aquatic Biomes.

Author

Subramaniam K, Behringer DC, Bojko J, Yutin N, Clark AS, Bateman KS, van Aerle R, Bass D, Kerr RC, Koonin EV, Stentiford GD, and Waltzek TB

Subjects

Animals, Brachyura virology, DNA Viruses isolation & purification, DNA Viruses pathogenicity, Ecosystem, Evolution, Molecular, Genomics, Oceans and Seas, Palinuridae virology, Penaeidae virology, United Kingdom, Crustacea virology, DNA Viruses classification, Genome, Viral, Phylogeny

Abstract

Panulirus argus virus 1 (PaV1) is the only known virus infecting the Caribbean spiny lobster ( Panulirus argus ) from the Caribbean Sea. Recently, related viruses, Dikerogammarus haemobaphes virus 1 (DhV1) and Carcinus maenas virus 1 (CmV1), have been detected in the demon shrimp ( Dikerogammarus haemobaphes ) and the European shore crab ( Carcinus maenas ), respectively, from sites in the United Kingdom. The virion morphology of these crustacean viruses is similar to that of iridoviruses. However, unlike iridoviruses and other nucleocytoplasmic large DNA viruses (NCLDVs), these viruses complete their morphogenesis in the host cell nucleus rather than in the cytoplasm. To date, these crustacean viruses have remained unclassified due to a lack of genomic data. Using an Illumina MiSeq sequencer, we sequenced the complete genomes of PaV1, CmV1, and DhV1. Comparative genome analysis shows that these crustacean virus genomes encode the 10 hallmark proteins previously described for the NCLDVs of eukaryotes, strongly suggesting that they are members of this group. With a size range of 70 to 74 kb, these are the smallest NCLDV genomes identified to date. Extensive gene loss, divergence of gene sequences, and the accumulation of low-complexity sequences reflect the extreme degradation of the genomes of these "minimal" NCLDVs rather than any direct relationship with the NCLDV ancestor. Phylogenomic analysis supports the classification of these crustacean viruses as a distinct family, "Mininucleoviridae," within the pitho-irido-Marseille branch of the NCLDVs. IMPORTANCE Recent genomic and metagenomic studies have led to a dramatic expansion of the known diversity of nucleocytoplasmic large DNA viruses (NCLDVs) of eukaryotes, which include giant viruses of protists and important pathogens of vertebrates, such as poxviruses. However, the characterization of viruses from nonmodel hosts still lags behind. We sequenced the complete genomes of three viruses infecting crustaceans, the Caribbean spiny lobster, demon shrimp, and European shore crab. These viruses have the smallest genomes among the known NCLDVs, with losses of many core genes, some of which are shared with iridoviruses. The deterioration of the transcription apparatus is compatible with microscopic and ultrastructural observations indicating that these viruses replicate in the nucleus of infected cells rather than in the cytoplasm. Phylogenomic analysis indicates that these viruses are sufficiently distinct from all other NCLDVs to justify the creation of a separate family, for which we propose the name "Mininucleoviridae" (i.e., small viruses reproducing in the cell nucleus)., (Copyright © 2020 Subramaniam et al.)

Published

2020

28. Loss and Gain in the Evolution of the Salmonella enterica Serovar Gallinarum Biovar Pullorum Genome.

Author

Hu Y, Wang Z, Qiang B, Xu Y, Chen X, Li Q, and Jiao X

Subjects

Animals, Bacterial Proteins metabolism, Bayes Theorem, Chickens, China epidemiology, Phylogeny, Polymorphism, Single Nucleotide, Poultry Diseases microbiology, Salmonella Infections, Animal transmission, Serogroup, Whole Genome Sequencing, Evolution, Molecular, Genome, Bacterial, Poultry Diseases transmission, Salmonella enterica genetics

Abstract

Salmonella enterica subspecies enterica serovar Gallinarum biovar Pullorum ( S Pullorum) is the etiological agent of pullorum disease, causing white diarrhea with high mortality in chickens. There are many unsolved issues surrounding the epidemiology of S Pullorum, including its origin and transmission history as well as the discordance between its phenotypic heterogeneity and genetic monomorphism. In this paper, we report the results of whole-genome sequencing of a panel of 97 S Pullorum strains isolated between 1962 and 2014 from four countries across three continents. We utilized 6,795 core genome single nucleotide polymorphisms (SNPs) to reconstruct a phylogenetic tree within a spatiotemporal Bayesian framework, estimating that the most recent common ancestor of S Pullorum emerged in ∼914 CE (95% confidence interval [95%CI], 565 to 1273 CE). The extant S Pullorum strains can be divided into four distinct lineages, each of which is significantly associated with geographical distribution. The intercontinental transmissions of lineages III and IV can be traced to the mid-19th century and are probably related to the "Hen Fever" prevalent at that time. Further genomic analysis indicated that the loss or pseudogenization of functional genes involved in metabolism and virulence in S Pullorum has been ongoing since before and after divergence from the ancestor. In contrast, multiple prophages and plasmids have been acquired by S Pullorum, and these have endowed it with new characteristics, especially the multidrug resistance conferred by two large plasmids in lineage I. The results of this study provide insight into the evolution of S Pullorum and prove the efficiency of whole-genome sequencing in epidemiological surveillance of pullorum disease. IMPORTANCE Pullorum disease, an acute poultry septicemia caused by Salmonella Gallinarum biovar Pullorum, is fatal for young chickens and is a heavy burden on poultry industry. The pathogen is rare in most developed countries but still extremely difficult to eliminate in China. Efficient epidemiological surveillance necessitates clarifying the origin of the isolates from different regions and their phylogenic relationships. Genomic epidemiological analysis of 97 S Pullorum strains was carried out to reconstruct the phylogeny and transmission history of S Pullorum. Further analysis demonstrated that functional gene loss and acquisition occurred simultaneously throughout the evolution of S Pullorum, both of which reflected adaptation to the changing environment. The result of our study will be helpful in surveillance and prevention of pullorum disease., (Copyright © 2019 Hu et al.)

Published

2019

29. Muller’s ratchet in symbiont populations

Author

Pettersson, Mats E. and Berg, Otto G.

Published

2007

30. Pseudogenes, junk DNA, and the dynamics of Rickettsia genomes

Author

Andersson, Jan O, Andersson, Siv GE, Andersson, Jan O, and Andersson, Siv GE

Abstract

Studies of neutrally evolving sequences suggest that differences in eukaryotic genome sizes result from different rates of DNA loss. However, very few pseudogenes have been identified in microbial species, and the processes whereby genes and genomes deteriorate in bacteria remain largely unresolved. The typhus-causing agent, Rickettsia prowazekii, is exceptional in that as much as 24% of its 1.1-Mb genome consists of noncoding DNA and pseudogenes. To test the hypothesis that the noncoding DNA in the R. prowazekii genome represents degraded remnants of ancestral genes, we systematically examined all of the identified pseudogenes and their flanking sequences in three additional Rickettsia species. Consistent with the hypothesis, we observe sequence similarities between genes and pseudogenes in one species and intergenic DNA in another species. We show that the frequencies and average sizes of deletions are larger than insertions in neutrally evolving pseudogene sequences. Our results suggest that inactivated genetic material in the Rickettsia genomes deteriorates spontaneously due to a mutation bias for deletions and that the noncoding sequences represent DNA in the final stages of this degenerative process., Addresses: Andersson SGE, Uppsala Univ, Evolutionary Biol Ctr, Dept Mol Evolut, Norbyvagen 18C, S-75236 Uppsala, Sweden. Uppsala Univ, Evolutionary Biol Ctr, Dept Mol Evolut, S-75236 Uppsala, Sweden.

Published

2001

31. Winding paths to simplicity: genome evolution in facultative insect symbionts.

Author

Lo WS, Huang YY, and Kuo CH

Subjects

Animals, Enterobacteriaceae genetics, Gene Transfer, Horizontal genetics, Proteobacteria genetics, Spiroplasma genetics, Evolution, Molecular, Genome, Bacterial genetics, Insecta genetics, Insecta microbiology, Symbiosis genetics

Abstract

Symbiosis between organisms is an important driving force in evolution. Among the diverse relationships described, extensive progress has been made in insect–bacteria symbiosis, which improved our understanding of the genome evolution in host-associated bacteria. Particularly, investigations on several obligate mutualists have pushed the limits of what we know about the minimal genomes for sustaining cellular life. To bridge the gap between those obligate symbionts with extremely reduced genomes and their non-host-restricted ancestors, this review focuses on the recent progress in genome characterization of facultative insect symbionts. Notable cases representing various types and stages of host associations, including those from multiple genera in the family Enterobacteriaceae (class Gammaproteobacteria), Wolbachia (Alphaproteobacteria) and Spiroplasma (Mollicutes), are discussed. Although several general patterns of genome reduction associated with the adoption of symbiotic relationships could be identified, extensive variation was found among these facultative symbionts. These findings are incorporated into the established conceptual frameworks to develop a more detailed evolutionary model for the discussion of possible trajectories. In summary, transitions from facultative to obligate symbiosis do not appear to be a universal one-way street; switches between hosts and lifestyles (e.g. commensalism, parasitism or mutualism) occur frequently and could be facilitated by horizontal gene transfer.

Published

2016

32. Found and Lost: The Fates of Horizontally Acquired Genes in Arthropod-Symbiotic Spiroplasma.

Author

Lo WS, Gasparich GE, and Kuo CH

Subjects

Animals, Arthropods microbiology, Evolution, Molecular, Genes, Bacterial, Genome, Bacterial, Interspersed Repetitive Sequences, Phylogeny, Spiroplasma classification, Symbiosis, Gene Transfer, Horizontal, Spiroplasma genetics

Abstract

Horizontal gene transfer (HGT) is an important mechanism that contributed to biological diversity, particularly in bacteria. Through acquisition of novel genes, the recipient cell may change its ecological preference and the process could promote speciation. In this study, we determined the complete genome sequence of two Spiroplasma species for comparative analyses and inferred the putative gene gains and losses. Although most Spiroplasma species are symbionts of terrestrial insects, Spiroplasma eriocheiris has evolved to be a lethal pathogen of freshwater crustaceans. We found that approximately 7% of the genes in this genome may have originated from HGT and these genes expanded the metabolic capacity of this organism. Through comparison with the closely related Spiroplasma atrichopogonis, as well as other more divergent lineages, our results indicated that these HGT events could be traced back to the most recent common ancestor of these two species. However, most of these horizontally acquired genes have been pseudogenized in S. atrichopogonis, suggesting that they did not contribute to the fitness of this lineage that maintained the association with terrestrial insects. Thus, accumulation of small deletions that disrupted these foreign genes was not countered by natural selection. On the other hand, the long-term survival of these horizontally acquired genes in the S. eriocheiris genome hinted that they might play a role in the ecological shift of this species. Finally, the implications of these findings and the conflicts among gene content, 16S rRNA gene sequencing, and serological typing, are discussed in light of defining bacterial species., (© The Author(s) 2015. Published by Oxford University Press on behalf of the Society for Molecular Biology and Evolution.)

Published

2015

33. Mechanistic insight into virus disinfection influence of virus characteristics, solution composition and surface interactions

Author

Sigstam, Anne Thérèse and Kohn, Tamar

Subjects

tailing effect, genome degradation, copper, virus inactivation, inactivation mechanisms by oxidants, protein degradation, self-assembled monolayers (SAMs), chlorine dioxide, virus-surface interaction

34. Ca. Endozoicomonas cretensis: A Novel Fish Pathogen Characterized by Genome Plasticity

Author

Qi, Weihong, Cascarano, Maria C., Schlapbach, Ralph, Katharios, Pantelis, Vaughan, Lloyd, and Seth-Smith, Helena M.B.

Subjects

resistance, virulence, mobile elements, genome degradation, genome decay, 14. Life underwater, host–pathogen

Abstract

Endozoicomonas bacteria are generally beneficial symbionts of diverse marine invertebrates including reef-building corals, sponges, sea squirts, sea slugs, molluscs, and Bryozoans. In contrast, the recently reported Ca. Endozoicomonas cretensis was identified as a vertebrate pathogen, causing epitheliocystis in fish larvae resulting in massive mortality. Here, we described the Ca. E. cretensis draft genome, currently undergoing genome decay as evidenced by massive insertion sequence (IS element) expansion and pseudogene formation. Many of the insertion sequences are also predicted to carry outward-directed promoters, implying that they may be able to modulate the expression of neighbouring coding sequences (CDSs). Comparative genomic analysis has revealed many Ca. E. cretensis-specific CDSs, phage integration and novel gene families. Potential virulence related CDSs and machineries were identified in the genome, including secretion systems and related effector proteins, and systems related to biofilm formation and directed cell movement. Mucin degradation would be of importance to a fish pathogen, and many candidate CDSs associated with this pathway have been identified. The genome may reflect a bacterium in the process of changing niche from symbiont to pathogen, through expansion of virulence genes and some loss of metabolic capacity., Genome Biology and Evolution, 10 (6), ISSN:1759-6653