Microbiology & Immunology - Research Publications

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Author: Dougan, Gordon × End date: 2017 × Start date: 2012 ×

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    Induction of Cell Cycle and NK Cell Responses by Live-Attenuated Oral Vaccines against Typhoid Fever
    Blohmke, CJ ; Hill, J ; Darton, TC ; Carvalho-Burger, M ; Eustace, A ; Jones, C ; Schreiber, F ; Goodier, MR ; Dougan, G ; Nakaya, HI ; Pollard, AJ (FRONTIERS MEDIA SA, 2017-10-12)
    The mechanisms by which oral, live-attenuated vaccines protect against typhoid fever are poorly understood. Here, we analyze transcriptional responses after vaccination with Ty21a or vaccine candidate, M01ZH09. Alterations in response profiles were related to vaccine-induced immune responses and subsequent outcome after wild-type Salmonella Typhi challenge. Despite broad genetic similarity, we detected differences in transcriptional responses to each vaccine. Seven days after M01ZH09 vaccination, marked cell cycle activation was identified and associated with humoral immunogenicity. By contrast, vaccination with Ty21a was associated with NK cell activity and validated in peripheral blood mononuclear cell stimulation assays confirming superior induction of an NK cell response. Moreover, transcriptional signatures of amino acid metabolism in Ty21a recipients were associated with protection against infection, including increased incubation time and decreased severity. Our data provide detailed insight into molecular immune responses to typhoid vaccines, which could aid the rational design of improved oral, live-attenuated vaccines against enteric pathogens.
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    Genome Sequence of Porcine Escherichia coli Strain IMT8073, an Atypical Enteropathogenic E. coli Strain Isolated from a Piglet with Diarrhea.
    Semmler, T ; Eichhorn, I ; Bethe, A ; Bauerfeind, R ; Pickard, D ; Kingsley, RA ; Dougan, G ; Wieler, LH (American Society for Microbiology, 2013-08-01)
    Escherichia coli is a highly diverse bacterial species, with atypical enteropathogenic E. coli (aEPEC) causing intestinal disease in both human and animal hosts. Here, we report the first complete genome sequence of an aEPEC strain of sequence type ST794 and serotype Ont:H7, isolated from a diseased piglet.
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    Correction: Signatures of Adaptation in Human Invasive Salmonella Typhimurium ST313 Populations from Sub-Saharan Africa.
    Okoro, CK ; Barquist, L ; Connor, TR ; Harris, SR ; Clare, S ; Stevens, MP ; Arends, MJ ; Hale, C ; Kane, L ; Pickard, DJ ; Hill, J ; Harcourt, K ; Parkhill, J ; Dougan, G ; Kingsley, RA (Public Library of Science (PLoS), 2015-06)
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    Phylogenetic Analysis of Klebsiella pneumoniae from Hospitalized Children, Pakistan
    Ejaz, H ; Wang, N ; Wilksch, JJ ; Page, AJ ; Cao, H ; Gujaran, S ; Keane, JA ; Lithgow, T ; ul-Haq, I ; Dougan, G ; Strugnell, RA ; Heinz, E (CENTERS DISEASE CONTROL & PREVENTION, 2017-11)
    Klebsiella pneumoniae shows increasing emergence of multidrug-resistant lineages, including strains resistant to all available antimicrobial drugs. We conducted whole-genome sequencing of 178 highly drug-resistant isolates from a tertiary hospital in Lahore, Pakistan. Phylogenetic analyses to place these isolates into global context demonstrate the expansion of multiple independent lineages, including K. quasipneumoniae.
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    Multilocus Sequence Typing as a Replacement for Serotyping in Salmonella enterica
    Achtman, M ; Wain, J ; Weill, F-X ; Nair, S ; Zhou, Z ; Sangal, V ; Krauland, MG ; Hale, JL ; Harbottle, H ; Uesbeck, A ; Dougan, G ; Harrison, LH ; Brisse, S ; Bessen, DE (PUBLIC LIBRARY SCIENCE, 2012-06)
    Salmonella enterica subspecies enterica is traditionally subdivided into serovars by serological and nutritional characteristics. We used Multilocus Sequence Typing (MLST) to assign 4,257 isolates from 554 serovars to 1092 sequence types (STs). The majority of the isolates and many STs were grouped into 138 genetically closely related clusters called eBurstGroups (eBGs). Many eBGs correspond to a serovar, for example most Typhimurium are in eBG1 and most Enteritidis are in eBG4, but many eBGs contained more than one serovar. Furthermore, most serovars were polyphyletic and are distributed across multiple unrelated eBGs. Thus, serovar designations confounded genetically unrelated isolates and failed to recognize natural evolutionary groupings. An inability of serotyping to correctly group isolates was most apparent for Paratyphi B and its variant Java. Most Paratyphi B were included within a sub-cluster of STs belonging to eBG5, which also encompasses a separate sub-cluster of Java STs. However, diphasic Java variants were also found in two other eBGs and monophasic Java variants were in four other eBGs or STs, one of which is in subspecies salamae and a second of which includes isolates assigned to Enteritidis, Dublin and monophasic Paratyphi B. Similarly, Choleraesuis was found in eBG6 and is closely related to Paratyphi C, which is in eBG20. However, Choleraesuis var. Decatur consists of isolates from seven other, unrelated eBGs or STs. The serological assignment of these Decatur isolates to Choleraesuis likely reflects lateral gene transfer of flagellar genes between unrelated bacteria plus purifying selection. By confounding multiple evolutionary groups, serotyping can be misleading about the disease potential of S. enterica. Unlike serotyping, MLST recognizes evolutionary groupings and we recommend that Salmonella classification by serotyping should be replaced by MLST or its equivalents.
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    Intracontinental spread of human invasive Salmonella Typhimurium pathovariants in sub-Saharan Africa
    Okoro, CK ; Kingsley, RA ; Connor, TR ; Harris, SR ; Parry, CM ; Al-Mashhadani, MN ; Kariuki, S ; Msefula, CL ; Gordon, MA ; de Pinna, E ; Wain, J ; Heyderman, RS ; Obaro, S ; Alonso, PL ; Mandomando, I ; MacLennan, CA ; Tapia, MD ; Levine, MM ; Tennant, SM ; Parkhill, J ; Dougan, G (NATURE PUBLISHING GROUP, 2012-11)
    A highly invasive form of non-typhoidal Salmonella (iNTS) disease has recently been documented in many countries in sub-Saharan Africa. The most common Salmonella enterica serovar causing this disease is Typhimurium (Salmonella Typhimurium). We applied whole-genome sequence-based phylogenetic methods to define the population structure of sub-Saharan African invasive Salmonella Typhimurium isolates and compared these to global Salmonella Typhimurium populations. Notably, the vast majority of sub-Saharan invasive Salmonella Typhimurium isolates fell within two closely related, highly clustered phylogenetic lineages that we estimate emerged independently ∼52 and ∼35 years ago in close temporal association with the current HIV pandemic. Clonal replacement of isolates from lineage I by those from lineage II was potentially influenced by the use of chloramphenicol for the treatment of iNTS disease. Our analysis suggests that iNTS disease is in part an epidemic in sub-Saharan Africa caused by highly related Salmonella Typhimurium lineages that may have occupied new niches associated with a compromised human population and antibiotic treatment.
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    Emergence and global spread of epidemic healthcare-associated Clostridium difficile
    He, M ; Miyajima, F ; Roberts, P ; Ellison, L ; Pickard, DJ ; Martin, MJ ; Connor, TR ; Harris, SR ; Fairley, D ; Bamford, KB ; D'Arc, S ; Brazier, J ; Brown, D ; Coia, JE ; Douce, G ; Gerding, D ; Kim, HJ ; Koh, TH ; Kato, H ; Senoh, M ; Louie, T ; Michell, S ; Butt, E ; Peacock, SJ ; Brown, NM ; Riley, T ; Songer, G ; Wilcox, M ; Pirmohamed, M ; Kuijper, E ; Hawkey, P ; Wren, BW ; Dougan, G ; Parkhill, J ; Lawley, TD (NATURE PUBLISHING GROUP, 2013-01)
    Epidemic C. difficile (027/BI/NAP1) has rapidly emerged in the past decade as the leading cause of antibiotic-associated diarrhea worldwide. However, the key events in evolutionary history leading to its emergence and the subsequent patterns of global spread remain unknown. Here, we define the global population structure of C. difficile 027/BI/NAP1 using whole-genome sequencing and phylogenetic analysis. We show that two distinct epidemic lineages, FQR1 and FQR2, not one as previously thought, emerged in North America within a relatively short period after acquiring the same fluoroquinolone resistance-conferring mutation and a highly related conjugative transposon. The two epidemic lineages showed distinct patterns of global spread, and the FQR2 lineage spread more widely, leading to healthcare-associated outbreaks in the UK, continental Europe and Australia. Our analysis identifies key genetic changes linked to the rapid transcontinental dissemination of epidemic C. difficile 027/BI/NAP1 and highlights the routes by which it spreads through the global healthcare system.
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    Genomic Epidemiology of Vibrio cholerae O1 Associated with Floods, Pakistan, 2010
    Shah, MA ; Mutreja, A ; Thomson, N ; Baker, S ; Parkhill, J ; Dougan, G ; Bokhari, H ; Wren, BW (CENTERS DISEASE CONTROL & PREVENTION, 2014-01)
    In August 2010, Pakistan experienced major floods and a subsequent cholera epidemic. To clarify the population dynamics and transmission of Vibrio cholerae in Pakistan, we sequenced the genomes of all V. cholerae O1 El Tor isolates and compared the sequences to a global collection of 146 V. cholerae strains. Within the global phylogeny, all isolates from Pakistan formed 2 new subclades (PSC-1 and PSC-2), lying in the third transmission wave of the seventh-pandemic lineage that could be distinguished by signature deletions and their antimicrobial susceptibilities. Geographically, PSC-1 isolates originated from the coast, whereas PSC-2 isolates originated from inland areas flooded by the Indus River. Single-nucleotide polymorphism accumulation analysis correlated river flow direction with the spread of PSC-2. We found at least 2 sources of cholera in Pakistan during the 2010 epidemic and illustrate the value of a global genomic data bank in contextualizing cholera outbreaks.
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    Drug Resistance in Salmonella enterica ser. Typhimurium Bloodstream Infection, Malawi
    Feasey, NA ; Cain, AK ; Msefula, CL ; Pickard, D ; Alaerts, M ; Aslett, M ; Everett, DB ; Allain, TJ ; Dougan, G ; Gordon, MA ; Heyderman, RS ; Kingsley, RA (CENTERS DISEASE CONTROL, 2014-11)
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    Multidrug-Resistant Salmonella enterica, Serotype Typhi, Gulf of Guinea Region, Africa
    Baltazar, M ; Ngandjio, A ; Holt, KE ; Lepillet, E ; Pardos de la Gandara, M ; Collard, J-M ; Bercion, R ; Nzouankeu, A ; Le Hello, S ; Dougan, G ; Fonkoua, M-C ; Weill, F-X (CENTERS DISEASE CONTROL, 2015-04)
    We identified 3 lineages among multidrug-resistant (MDR) Salmonella enterica serotype Typhi isolates in the Gulf of Guinea region in Africa during the 2000s. However, the MDR H58 haplotype, which predominates in southern Asia and Kenya, was not identified. MDR quinolone-susceptible isolates contained a 190-kb incHI1 pST2 plasmid or a 50-kb incN pST3 plasmid.