A whole-genome microarray reveals genetic diversity among
            <i>Helicobacter pylori</i>
            strains

Salama, Nina R.; Guillemin, Karen; McDaniel, Timothy K.; Sherlock, Gavin; Tompkins, Lucy S.; Falkow, Stanley

doi:10.1073/pnas.97.26.14668

Cited by 528 publications

(477 citation statements)

References 35 publications

(24 reference statements)

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“…Ratios between 0.3 and 0.8 indicated moderate sequence variability. Finally, ratios between 0.8 and 1.5 indicated conservation of the gene (Read et al, 2003;Salama et al, 2000).…”

Section: Methodsmentioning

confidence: 99%

Genomic and antigenic characterization of monomeric autotransporters of Haemophilus parasuis: an ongoing process of reductive evolution

et al. 2012

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The genome of the highly pathogenic Haemophilus parasuis Nagasaki strain (serovar 5) was sequenced to 99 % completion. A genomic comparison with two other pathogenic serovar 5 H. parasuis strains identified six genes per genome (bmaA1-bmaA6) encoding b-barrel monomeric autotransporters, bmaA2 and bmaA3 being pseudogenes in at least one strain. The remaining encoded proteins were predicted to belong to the subtilisin (BmaA1 and BmaA4) and cysteine (BmaA5 and BmaA6) protease families. Allelic polymorphism was detected in other H. parasuis strains by comparative genomic hybridization using microarrays. Recombination events were observed, some of them leading to gene disruption in one of the three strains, although synteny around bmaA genes was conserved. These results suggest that bmaA genes are undergoing a process of reductive evolution. To evaluate their use as potential vaccine antigens, the products of the passenger domains of bmaA1, bmaA4, bmaA5 and bmaA6 were produced in Escherichia coli as recombinant proteins. They were detected by immunoblotting using sera of colostrum-deprived piglets recovering from a sublethal infection with H. parasuis (Nagasaki). The existence of specific antibodies after infection with H. parasuis also demonstrated in vivo expression. Using proteomics, only BmaA6 was detected in the in vitro-grown Nagasaki strain. Interestingly, the translocator domain was found in the outer membrane, while the passenger domain was located in supernatants. These results indicate that BmaA proteins could be considered as immunogen candidates to improve H. parasuis vaccines. However, their capacity to confer protective immunity needs to be studied further.

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“…Ratios between 0.3 and 0.8 indicated moderate sequence variability. Finally, ratios between 0.8 and 1.5 indicated conservation of the gene (Read et al, 2003;Salama et al, 2000).…”

Section: Methodsmentioning

confidence: 99%

Genomic and antigenic characterization of monomeric autotransporters of Haemophilus parasuis: an ongoing process of reductive evolution

et al. 2012

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“…It is one of the most genetically diverse bacterial species: independent clinical isolates typically differ by some 2-5 % in sequences of essential genes and by some 5 % or more in gene content (Achtman et al, 1999;Alm et al, 1999;Israel et al, 2001;Salama et al, 2000). This diversity probably reflects a combination of factors including: (i) mutation (Bjorkholm et al, 2001;Wang & Taylor, 1999); (ii) recombination among divergent lineages (Achtman et al, 1999;Kersulyte et al, 1999;Suerbaum et al, 1998); (iii) gene transfer from unrelated species (Tomb et al, 1997); (iv) preferential transmission among family members, and thus little chance of selection for any one or few potentially optimal genotypes (Mukhopadhyay et al, 2003);and (v) diversity among hosts in traits that are important to individual strains, and selection for adaptive changes after transmission to new hosts (Dubois et al, 1999).…”

Section: Introductionmentioning

confidence: 99%

Helicobacter pylori tissue tropism: mouse-colonizing strains can target different gastric niches

et al. 2003

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Studies with the mouse-adapted Helicobacter pylori strain SS1 had supported an idea that infections by this pathogen start in the gastric antrum and spread to the corpus after extensive mucosal damage. This paper shows that the unrelated strain X47 colonizes the corpus preferentially. Differences between strains in preferred gastric region were detected by co-inoculating mice with a mixture of SS1 and X47, and genotyping H. pylori recovered after 2-8 weeks of infection by vacA s allele PCR and RAPD fingerprinting. Mixed infections were found in each of 59 co-inoculated young C57BL/6J mice. On average, however, SS1 was fourfold more abundant than X47 in the antrum and X47 was threefold more abundant than SS1 in the corpus. Similar results were obtained in mice inoculated first with one strain and then the other strain 2 weeks later. SS1 was even more abundant in the antrum of elderly (>1 year old) mice (97 % of isolates). Qualitatively similar SS1 and X47 tissue distributions were seen using unrelated mouse lines (AKR/J, A/J, DBA/2J, BALB/cJ, LG/J, SM/J), but with significantly different SS1 : X47 ratios in some cases. These results suggest the existence of at least two distinct gastric niches whose characteristics may be affected by host genotype and age (physiology), and indicate that strains differ in how effectively they colonize each niche. Differences among gastric regions and the mixed infections that these allow may contribute to H. pylori diversity and genome evolution.

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“…In other species, such as Mycobacterium tuberculosis, the comparison of complete genome sequences has identified large-sequence polymorphisms (LSPs) and singlenucleotide polymorphisms (SNPs), but the molecular basis of variability in virulence and transmissibility remains undefined (6,7). A distinct but complementary approach to comparative genomics involves the interrogation of unsequenced genomes by DNA microarray to identify sequences present in a fully sequenced isolate, but absent from interrogated isolates (8)(9)(10)(11)(12)(13)(14)(15)(16). Although this approach is limited to the identification of relatively large sequence polymorphisms, it allows for the comparison of a large number of genomes, and thus provides information on the diversity and frequency of polymorphisms in the population.…”

mentioning

confidence: 99%

Functional and evolutionary genomics of Mycobacterium tuberculosis : Insights from genomic deletions in 100 strains

Tsolaki

Hirsh

DeRiemer

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

325

301

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To better understand genome function and evolution in Mycobacterium tuberculosis, the genomes of 100 epidemiologically well characterized clinical isolates were interrogated by DNA microarrays and sequencing. We identified 68 different large-sequence polymorphisms (comprising 186,137 bp, or 4.2% of the genome) that are present in H37Rv, but absent from one or more clinical isolates. A total of 224 genes (5.5%), including genes in all major functional categories, were found to be partially or completely deleted. Deletions are not distributed randomly throughout the genome but instead tend to be aggregated. The distinct deletions in some aggregations appear in closely related isolates, suggesting a genomically disruptive process specific to an individual mycobacterial lineage. Other genomic aggregations include distinct deletions that appear in phylogenetically unrelated isolates, suggesting that a genomic region is vulnerable throughout the species. Although the deletions identified here are evidently inessential to the causation of disease (they are found in active clinical cases), their frequency spectrum suggests that most are weakly deleterious to the pathogen. For some deletions, short-term evolutionary pressure due to the host immune system or antibiotics may favor the elimination of genes, whereas longer-term physiological requirements maintain the genes in the population.

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A whole-genome microarray reveals genetic diversity among Helicobacter pylori strains

Cited by 528 publications

References 35 publications

Genomic and antigenic characterization of monomeric autotransporters of Haemophilus parasuis: an ongoing process of reductive evolution

Genomic and antigenic characterization of monomeric autotransporters of Haemophilus parasuis: an ongoing process of reductive evolution

Helicobacter pylori tissue tropism: mouse-colonizing strains can target different gastric niches

Functional and evolutionary genomics of Mycobacterium tuberculosis : Insights from genomic deletions in 100 strains

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