Your search keyword '"Kellam, Paul"' showing total 7 results

1. Gene expression subtypes in patients with chronic fatigue syndrome/myalgic encephalomyelitis

Author

Kerr, Jonathan R., Petty, Robert, Burke, Beverley, Gough, John, Fear, David, Sinclair, Lindsey I., Mattey, Derek L., Richards, Selwyn C.M., Montgomery, Jane, Baldwin, Don A., Kellam, Paul, Griffin, George E., Main, Janice, Enlander, Derek, Nutt, David J., and Holgate, Stephen T.

Subjects

Gene expression -- Research, Gene expression -- Physiological aspects, Chronic fatigue syndrome -- Research, Chronic fatigue syndrome -- Genetic aspects, Chronic fatigue syndrome -- Development and progression, Health

Published

2008

2. Genome-Wide Sequence Analysis of Kaposi Sarcoma-Associated Herpesvirus Shows Diversification Driven by Recombination.

Author

Sallah, Neneh, Palser, Anne L, Watson, Simon J, Labo, Nazzarena, Asiki, Gershim, Marshall, Vickie, Newton, Robert, Whitby, Denise, Kellam, Paul, and Barroso, Inês

Subjects

KAPOSI'S sarcoma-associated herpesvirus, GENOMES, DNA, GENOTYPES, GEOGRAPHY

Abstract

Background: Kaposi sarcoma-associated herpesvirus (KSHV) establishes lifelong infection in the human host and has been associated with a variety of malignancies. KSHV displays striking geographic variation in prevalence, which is highest in sub-Saharan Africa. The current KSHV genome sequences available are all tumor cell line-derived or primary tumor-associated viruses, which have provided valuable insights into KSHV genetic diversity.Methods: Here, we sequenced 45 KSHV genomes from a Ugandan population cohort in which KSHV is endemic; these are the only genome sequences obtained from nondiseased individuals and of KSHV DNA isolated from saliva.Results: Population structure analysis, along with the 25 published genome sequences from other parts of the world, showed whole-genome variation, separating sequences and variation within the central genome contributing to clustering of genomes by geography. We reveal new evidence for the presence of intragenic recombination and multiple recombination events contributing to the divergence of genomes into at least 5 distinct types.Discussion: This study shows that large-scale genome-wide sequencing from clinical and epidemiological samples is necessary to capture the full extent of genetic diversity of KSHV, including recombination, and provides evidence to suggest a revision of KSHV genotype nomenclature. [ABSTRACT FROM AUTHOR]

Published

2018

3. Human Coronavirus NL63 Molecular Epidemiology and Evolutionary Patterns in Rural Coastal Kenya.

Author

Kiyuka, Patience K., Agoti, Charles N., Munywoki, Patrick K., Njeru, Regina, Bett, Anne, Otieno, James R., Otieno, Grieven P., Kamau, Everlyn, Clark, Taane G., van der Hoek, Lia, Kellam, Paul, Nokes, D. James, and Cotten, Matthew

Subjects

CORONAVIRUSES, CORONAVIRUS diseases, MOLECULAR epidemiology, IMMUNE response, EPIDEMIOLOGY

Abstract

Background: Human coronavirus NL63 (HCoV-NL63) is a globally endemic pathogen causing mild and severe respiratory tract infections with reinfections occurring repeatedly throughout a lifetime.Methods: Nasal samples were collected in coastal Kenya through community-based and hospital-based surveillance. HCoV-NL63 was detected with multiplex real-time reverse transcription PCR, and positive samples were targeted for nucleotide sequencing of the spike (S) protein. Additionally, paired samples from 25 individuals with evidence of repeat HCoV-NL63 infection were selected for whole-genome virus sequencing.Results: HCoV-NL63 was detected in 1.3% (75/5573) of child pneumonia admissions. Two HCoV-NL63 genotypes circulated in Kilifi between 2008 and 2014. Full genome sequences formed a monophyletic clade closely related to contemporary HCoV-NL63 from other global locations. An unexpected pattern of repeat infections was observed with some individuals showing higher viral titers during their second infection. Similar patterns for 2 other endemic coronaviruses, HCoV-229E and HCoV-OC43, were observed. Repeat infections by HCoV-NL63 were not accompanied by detectable genotype switching.Conclusions: In this coastal Kenya setting, HCoV-NL63 exhibited low prevalence in hospital pediatric pneumonia admissions. Clade persistence with low genetic diversity suggest limited immune selection, and absence of detectable clade switching in reinfections indicates initial exposure was insufficient to elicit a protective immune response. [ABSTRACT FROM AUTHOR]

Published

2018

4. Evaluating the Impact of Functional Genetic Variation on HIV-1 Control.

Author

McLaren, Paul J., Pulit, Sara L., Gurdasani, Deepti, Bartha, Istvan, Shea, Patrick R., Pomilla, Cristina, Gupta, Namrata, Gkrania-Klotsas, Effrossyni, Young, Elizabeth H., Bannert, Norbert, Del Amo, Julia, Gill, M. John, Gilmour, Jill, Kellam, Paul, Kelleher, Anthony D., Sönnerborg, Anders, Zangerle, Robert, Post, Frank A., Fisher, Martin, and Haas, David W.

Subjects

HUMAN genetic variation, HIV, DISEASE progression, EXOMES, NUCLEOTIDE sequencing, VIRAL load

Abstract

Background: Previous genetic association studies of human immunodeficiency virus-1 (HIV-1) progression have focused on common human genetic variation ascertained through genome-wide genotyping.Methods: We sought to systematically assess the full spectrum of functional variation in protein coding gene regions on HIV-1 progression through exome sequencing of 1327 individuals. Genetic variants were tested individually and in aggregate across genes and gene sets for an influence on HIV-1 viral load.Results: Multiple single variants within the major histocompatibility complex (MHC) region were observed to be strongly associated with HIV-1 outcome, consistent with the known impact of classical HLA alleles. However, no single variant or gene located outside of the MHC region was significantly associated with HIV progression. Set-based association testing focusing on genes identified as being essential for HIV replication in genome-wide small interfering RNA (siRNA) and clustered regularly interspaced short palindromic repeats (CRISPR) studies did not reveal any novel associations.Conclusions: These results suggest that exonic variants with large effect sizes are unlikely to have a major contribution to host control of HIV infection. [ABSTRACT FROM AUTHOR]

Published

2017

5. Respiratory Tract Samples, Viral Load, and Genome Fraction Yield in Patients With Middle East Respiratory Syndrome

Author

Memish, Ziad A., primary, Al-Tawfiq, Jaffar A., additional, Makhdoom, Hatem Q., additional, Assiri, Abdullah, additional, Alhakeem, Raafat F., additional, Albarrak, Ali, additional, Alsubaie, Sarah, additional, Al-Rabeeah, Abdullah A., additional, Hajomar, Waleed H., additional, Hussain, Raheela, additional, Kheyami, Ali M., additional, Almutairi, Abdullah, additional, Azhar, Esam I., additional, Drosten, Christian, additional, Watson, Simon J., additional, Kellam, Paul, additional, Cotten, Matthew, additional, and Zumla, Alimuddin, additional

Published

2014

6. Immediate T-Helper 17 Polarization Upon Triggering CD11b/c on HIV-Exposed Dendritic Cells.

Author

Wilflingseder, Doris, Schroll, Andrea, Hackl, Hubert, Gallasch, Ralf, Frampton, Dan, Lass-Flörl, Cornelia, Pancino, Gianfranco, Saez-Cirion, Asier, Lambotte, Olivier, Weiss, Laurence, Kellam, Paul, Trajanoski, Zlatko, Geijtenbeek, Teunis, Weiss, Günter, and Posch, Wilfried

Subjects

THERAPEUTICS, HIV infections, T helper cells, DENDRITIC cells, ANTIVIRAL agents, CELL compartmentation, IMMUNOCOMPROMISED patients, COMPLEMENT (Immunology)

Abstract

Early on in human immunodeficiency virus (HIV) type 1 infection, gut T-helper (Th) 17 cells are massively depleted leading eventually to compromised intestinal barrier function and excessive immune activation. In contrast, the functional Th17 cell compartment of the gut is well-maintained in nonpathogenic simian immunodeficiency virus infection as well as HIV-1 long-term nonprogressors. Here, we show that dendritic cells (DCs) loaded with HIV-1 bearing high surface complement levels after incubation in plasma from HIV-infected individuals secreted significantly higher concentrations of Th17-polarizing cytokines than DCs exposed to nonopsonized HIV-1. The enhanced Th17-polarizing capacity of in vitro-generated and BDCA-1+ DCs directly isolated from blood was linked to activation of ERK. In addition, C3a produced from DCs exposed to complement- opsonized HIV was associated with the higher Th17 polarization. Our in vitro and ex vivo data, therefore, indicate that complement opsonization of HIV-1 strengthens DC-mediated antiviral immune functions by simultaneously triggering Th17 expansion and intrinsic C3 formation via DC activation. [ABSTRACT FROM AUTHOR]

Published

2015

7. Ordered appearance of zidovudine resistance mutations during treatment of 18 human immunodeficiency virus-positive subjects.

Author

Boucher, Charles A. B., O'Sullivan, Eithne, Mulder, Jan W., Ramautarsing, Chitra, Kellam, Paul, Darby, Graham, Lange, Joep M. A., Goudsmit, Jaap, Larder, Brendan A., Boucher, C A, O'Sullivan, E, Mulder, J W, Ramautarsing, C, Kellam, P, Darby, G, Lange, J M, Goudsmit, J, and Larder, B A

Abstract

The order of appearance in the reverse transcriptase gene of four mutations implicated in the development of resistance to zidovudine was investigated by selective polymerase chain reaction. Serial human immunodeficiency virus isolates were studied from 18 initially asymptomatic individuals who had been treated with zidovudine for 2 years. Most subjects had similar patterns. The first mutation occurred transiently at codon 70; its disappearance was paralleled by the appearance of a mutation at codon 215. Subsequently, in some individuals, the mutation at codon 70 reappeared. During the 2 years of treatment, no mutations developed at codon 219 and only one at codon 67, suggesting that most individuals developed only partly resistant virus. This was confirmed by plaque-reduction assay. Six subjects progressed to AIDS within the 2-year study period, confirming that the development of highly resistant isolates is not required for progression in treated individuals. No clear temporal relationship was found between the development of partial resistance and progression. [ABSTRACT FROM AUTHOR]

Published

1992