Your search keyword '"Leigh Brown, A"' showing total 790 results

201. Instability in the ct MR2 strain of Drosophila melanogaster: Role of P element functions and structure of revertants

Author

Leigh Brown, Andrew J., Ross, Sarah J., Alphey, Luke S., Flavell, Andrew J., and Gerasimova, Tatiana I.

Published

1989

202. Persistence of HIV-1 transmitted drug resistance mutations

Author

Castro, H., Pillay, D., Cane, P., Asboe, D., Cambiano, V., Phillips, A., Dunn, D. T., Aitken, C., Webster, D., Chadwick, D., Churchill, D., Clark, D., Collins, S., Delpech, V., Geretti, A. M., Goldberg, D., Hale, A., Hue, S., Kaye, S., Kellam, P., Lazarus, L., Leigh-Brown, A., Mackie, N., Orkin, C., Rice, P., Smit, E., Templeton, K., Tilston, P., Tong, W., Williams, I., Zhang, H., Zuckerman, M., Greatorex, J., Wildfire, A., O'Shea, S., Mullen, J., Mbisa, T., Cox, A., Tandy, R., Hale, T., Fawcett, T., Hopkins, M., Ashton, L., Garcia-Diaz, A., Shepherd, J., Schmid, M. L., Payne, B., Hay, P., Paynter, M., Bibby, D., Kirk, S., MacLean, A., and Gunson, R.

Subjects

Male, FITNESS, Human immunodeficiency virus (HIV), HIV Infections, Drug resistance, VARIANTS, medicine.disease_cause, THERAPY, Persistence (computer science), 0302 clinical medicine, Immunology and Allergy, 030212 general & internal medicine, Hiv transmission, 11 Medical and Health Sciences, media_common, transmitted, 0303 health sciences, Mutation, Thymidine analogue, persistence, IMMUNODEFICIENCY-VIRUS TYPE-1, ABSENCE, 3. Good health, Infectious Diseases, HIV/AIDS, Female, Life Sciences & Biomedicine, Drug, Adult, Adolescent, Anti-HIV Agents, media_common.quotation_subject, Immunology, Exponential regression, Biology, Microbiology, UK Collaborative Group on HIV Drug Resistance, resistance, 03 medical and health sciences, Major Articles and Brief Reports, Young Adult, Drug Resistance, Viral, medicine, Humans, 030304 developmental biology, Science & Technology, 06 Biological Sciences, mutations, Virology, HIV-1

Abstract

There are few data on the persistence of individual human immunodeficiency virus type 1 (HIV-1) transmitted drug resistance (TDR) mutations in the absence of selective drug pressure. We studied 313 patients in whom TDR mutations were detected at their first resistance test and who had a subsequent test performed while ART-naive. The rate at which mutations became undetectable was estimated using exponential regression accounting for interval censoring. Most thymidine analogue mutations (TAMs) and T215 revertants (but not T215F/Y) were found to be highly stable, with NNRTI and PI mutations being relatively less persistent. Our estimates are important for informing HIV transmission models.

Published

2013

203. Molecular phylogeny of the planktic foraminifera

Author

Dick Kroon, A. J. Leigh Brown, Kathryn Darling, and Christopher M. Wade

Subjects

Foraminifera, Paleontology, biology, Molecular phylogenetics, biology.organism_classification, Microbiology

Published

1996

204. Evolution of Zidovudine Resistance-Associated Genotypes in Human Immunodeficiency Virus Type 1-Infected Patients

Author

A Cleland, Pamela Robertson, Christopher A. Ludlam, Andrew J. Leigh Brown, and Henry G. Watson

Subjects

Genotype, Molecular Sequence Data, Immunology, Population, HIV Infections, Genome, Viral, Drug resistance, Virus Replication, Antiviral Agents, Polymerase Chain Reaction, Peripheral blood mononuclear cell, Virus, Evolution, Molecular, Zidovudine, Proviruses, Virology, medicine, Humans, Immunology and Allergy, Amino Acid Sequence, education, Sida, DNA Primers, education.field_of_study, Base Sequence, biology, Drug Resistance, Microbial, RNA-Directed DNA Polymerase, biology.organism_classification, Genes, pol, CD4 Lymphocyte Count, Mutation, HIV-1, Leukocytes, Mononuclear, RNA, Viral, Viral disease, medicine.drug

Abstract

Substantial differences have been described in the response of individual patients to zidovudine (ZDV) therapy, both in the clinical impact and in virus load. Genotypic changes associated with the appearance of drug resistance may also be different or occur at different rates. We have obtained the nucleotide sequence of the RT domain of individual HIV-1 genomes extracted from 10 plasma and peripheral blood mononuclear cell (PBMC) samples donated by two haemophiliac patients before, during, and after long-term ZDV therapy. Although the plasma virus load was similar throughout, the order and timing of appearance of resistance-associated substitutions differed in the two patients. In patient p74, K70R appeared after 4 months, T215Y at 5.5 months, and M41L at 13 months. In p87, K70R also appeared at 4 months, but T215Y and K219Q were not observed until 18 months and M41L not at all. Much greater sequence change overall occurred in p74. The evolution of the viral population in that patient was dominated by the unique appearance of T215Y and subsequently M41L, with all sequences from the last time point being descended by a single path from the pretreatment samples. However, in p87, several different lineages of RT sequences were found to persist throughout treatment. We propose that these differences in outcome may be determined by differences in genetic background at sites other than the five generally considered to be associated with ZDV sensitivity.

Published

1996

205. No change in hepatitis C virus-specific T cell functionality after successful DAA treatment in chronic hepatitis C patients

Author

S.B. Willemse, M.J. Sinnige, M.H. van der Ree, M. van der Valk, J.M.L. de Vree, Paul Klenerman, E Barnes, Neeltje A. Kootstra, Leo Swadling, Andrew J. Leigh Brown, F. Stelma, and H. W. Reesink

Subjects

medicine.anatomical_structure, Hepatology, Chronic hepatitis, business.industry, Hepatitis C virus, T cell, Immunology, Medicine, business, medicine.disease_cause, Virology

Published

2017

206. The evolutionary dynamics of influenza A virus adaptation to mammalian hosts

Author

Bhatt, S., Lam, T. T., Lycett, S. J., Leigh Brown, A. J., Bowden, T. A., Holmes, E. C., Guan, Y., Wood, J. L. N., Brown, I. H., Kellam, P., Pybus, O. G., Brown, Ian, Brookes, Sharon, Germundsson, Anna, Cook, Alex, Williamson, Susanna, Essen, Stephen, Garcon, Fanny, Gunn, George, Sanchez, Manuel, Marques, Diogo, Wood, James, Tucker, Dan, McCrone, Ian, Gog, Julia, Saenz, Roberto, Staff, Meg, Murcia, Pablo, Barclay, Wendy, Donnelly, Christl, Elderfield, Ruth A., Kellam, Paul, Baillie, Greg, Coulter, Eve, Wieland, Barbara, Mastin, Alex, McCauley, John, Brown, Andy Leigh, Lycett, Sam, Woolhouse, Mark, Pybus, Oliver, Bhatt, Samir, Hayward, Andrew, Ishola, David, Archibald, Alan, Freeman, Tom, Charleston, Bryan, LeFevre, Eric, Bailey, Mick, Inman, Charlotte, Stokes, Chris, Chang, Kin Chow, Dunham, Stephen, White, Gavin, Nguyen-Van-Tam, Jonathan, and Enstone, Joanne

Subjects

Swine, Adaptation, Biological, Hemagglutinins, Viral, Neuraminidase, medicine.disease_cause, Genome, General Biochemistry, Genetics and Molecular Biology, Virus, Host Specificity, Evolution, Molecular, Orthomyxoviridae Infections, Zoonoses, Evolution of influenza, Databases, Genetic, medicine, Influenza A virus, Animals, Humans, Phylogeny, Genetics, Swine Diseases, Likelihood Functions, biology, Models, Genetic, Zoonosis, Articles, medicine.disease, Virology, Influenza A virus subtype H5N1, Viral phylodynamics, biology.protein, General Agricultural and Biological Sciences

Abstract

Few questions on infectious disease are more important than understanding how and why avian influenza A viruses successfully emerge in mammalian populations, yet little is known about the rate and nature of the virus’ genetic adaptation in new hosts. Here, we measure, for the first time, the genomic rate of adaptive evolution of swine influenza viruses (SwIV) that originated in birds. By using a curated dataset of more than 24 000 human and swine influenza gene sequences, including 41 newly characterized genomes, we reconstructed the adaptive dynamics of three major SwIV lineages (Eurasian, EA; classical swine, CS; triple reassortant, TR). We found that, following the transfer of the EA lineage from birds to swine in the late 1970s, EA virus genes have undergone substantially faster adaptive evolution than those of the CS lineage, which had circulated among swine for decades. Further, the adaptation rates of the EA lineage antigenic haemagglutinin and neuraminidase genes were unexpectedly high and similar to those observed in human influenza A. We show that the successful establishment of avian influenza viruses in swine is associated with raised adaptive evolution across the entire genome for many years after zoonosis, reflecting the contribution of multiple mutations to the coordinated optimization of viral fitness in a new environment. This dynamics is replicated independently in the polymerase genes of the TR lineage, which established in swine following separate transmission from non-swine hosts.

Published

2013

207. Dissembling Images: Electronic Media and Writing

Author

Alison Leigh Brown

Published

2013

208. Evolutionary interactions between haemagglutinin and neuraminidase in avian influenza

Author

Melissa J. Ward, Jonathan P. Bollback, Dorita Avila, Andrew J. Leigh Brown, and Samantha Lycett

Subjects

Evolution, Reassortment, Neuraminidase, Subtype, Hemagglutinin Glycoproteins, Influenza Virus, Biology, medicine.disease_cause, Virus, Birds, Viral life cycle, Phylogenetics, Evolution of influenza, Influenza A virus, medicine, Animals, Selection, Phylogeny, Ecology, Evolution, Behavior and Systematics, Stochastic Processes, 576 Genetics and evolution, Bayes Theorem, Biological Evolution, Virology, Influenza, Influenza A virus subtype H5N1, Influenza in Birds, biology.protein, Reassortant Viruses, Research Article

Abstract

Reassortment between the RNA segments encoding haemagglutinin (HA) and neuraminidase (NA), the major antigenic influenza proteins, produces viruses with novel HA and NA subtype combinations and has preceded the emergence of pandemic strains. It has been suggested that productive viral infection requires a balance in the level of functional activity of HA and NA, arising from their closely interacting roles in the viral life cycle, and that this functional balance could be mediated by genetic changes in the HA and NA. Here, we investigate how the selective pressure varies for H7 avian influenza HA on different NA subtype backgrounds. By extending Bayesian stochastic mutational mapping methods to calculate the ratio of the rate of non-synonymous change to the rate of synonymous change (d N /d S ), we found the average d N /d S across the avian influenza H7 HA1 region to be significantly greater on an N2 NA subtype background than on an N1, N3 or N7 background. Observed differences in evolutionary rates of H7 HA on different NA subtype backgrounds could not be attributed to underlying differences between avian host species or virus pathogenicity. Examination of d N /d S values for each subtype on a site-by-site basis indicated that the elevated d N /d S on the N2 NA background was a result of increased selection, rather than a relaxation of selective constraint. Our results are consistent with the hypothesis that reassortment exposes influenza HA to significant changes in selective pressure through genetic interactions with NA. Such epistatic effects might be explicitly accounted for in future models of influenza evolution.

Published

2013

209. Analysis of envelope sequence variants suggests multiple mechanisms of mother-to-child transmission of human immunodeficiency virus type 1

Author

J. Puel, Andrew J. Leigh Brown, Christopher M. Wade, M. Guyader, and Laurence Briant

Subjects

Adult, Glycosylation, Molecular Sequence Data, Immunology, HIV Infections, Biology, medicine.disease_cause, Microbiology, law.invention, Genetic Heterogeneity, Pregnancy, law, Phylogenetics, Virology, Genetic variation, medicine, Humans, Amino Acid Sequence, Peptide sequence, Phylogeny, DNA Primers, Sequence (medicine), Genetics, Mutation, Base Sequence, Sequence Homology, Amino Acid, Phylogenetic tree, Genetic heterogeneity, Infant, Newborn, Gene Products, env, Infectious Disease Transmission, Vertical, Phenotype, Transmission (mechanics), Insect Science, HIV-1, Female, Research Article

Abstract

In order to elucidate the molecular mechanisms involved in human immunodeficiency virus type 1 (HIV-1) mother-to-child transmission, we have analyzed the genetic variation within the V3 hypervariable domain and flanking regions of the HIV-1 envelope gene in four mother-child transmission pairs. Phylogenetic analysis and amino acid sequence comparison were performed on cell-associated viral sequences derived from maternal samples collected at different time points during pregnancy, after delivery, and from child samples collected from the time of birth until the child was approximately 1 year of age. Heterogeneous sequence populations were observed to be present in all maternal samples collected during pregnancy and postdelivery. In three newborns, viral sequence populations obtained within 2 weeks after birth revealed a high level of V3 sequence variability. In contrast, V3 sequences obtained from the fourth child (diagnosed at the age of 1 month) displayed a more restricted heterogeneity. The phylogenetic analysis performed for each mother-child sequence set suggested that several mechanisms may potentially be involved in HIV-1 vertical transmission. For one pair, child sequences were homogeneous and clustered in a single branch within the phylogenetic tree, consistent with selective transmission of a single maternal variant. For the other three pairs, the child sequences were more heterogeneous and clustered in several separate branches within the tree. In these cases, it appeared likely that more than one maternal variant was responsible for infection of the child. In conclusion, no single mechanism can account for mother-to-child HIV-1 transmission; both the selective transmission of a single maternal variant and multiple transmission events may occur.

Published

1995

210. Book reviews

Author

Ralph Acampora and Alison Leigh Brown

Subjects

Philosophy, Sociology and Political Science

Published

1995

211. Extensive compensatory cis-trans regulation in the evolution of mouse gene expression

Author

David Thybert, John C. Marioni, Alvis Brazma, Klara Stefflova, Paul Flicek, Duncan T. Odom, Angela Goncalves, Ernest Turro, and Sarah Leigh-Brown

Subjects

Male, Models, Molecular, Sequence analysis, Mice, Inbred Strains, Biology, Evolution, Molecular, 03 medical and health sciences, Genomic Imprinting, Mice, 0302 clinical medicine, Gene expression, Genetics, Gene silencing, Animals, Gene, Genetics (clinical), Alleles, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Sequence Analysis, RNA, Research, Phenotype, Circadian Rhythm, Mice, Inbred C57BL, Gene Expression Regulation, Female, Trans-acting, Genomic imprinting, 030217 neurology & neurosurgery

Abstract

Gene expression levels are thought to diverge primarily via regulatory mutations in trans within species, and in cis between species. To test this hypothesis in mammals we used RNA-sequencing to measure gene expression divergence between C57BL/6J and CAST/EiJ mouse strains and allele-specific expression in their F1 progeny. We identified 535 genes with parent-of-origin specific expression patterns, although few of these showed full allelic silencing. This suggests that the number of imprinted genes in a typical mouse somatic tissue is relatively small. In the set of nonimprinted genes, 32% showed evidence of divergent expression between the two strains. Of these, 2% could be attributed purely to variants acting in trans, while 43% were attributable only to variants acting in cis. The genes with expression divergence driven by changes in trans showed significantly higher sequence constraint than genes where the divergence was explained by variants acting in cis. The remaining genes with divergent patterns of expression (55%) were regulated by a combination of variants acting in cis and variants acting in trans. Intriguingly, the changes in expression induced by the cis and trans variants were in opposite directions more frequently than expected by chance, implying that compensatory regulation to stabilize gene expression levels is widespread. We propose that expression levels of genes regulated by this mechanism are fine-tuned by cis variants that arise following regulatory changes in trans, suggesting that many cis variants are not the primary targets of natural selection.

Published

2012

212. Time trends in drug resistant HIV-1 infections in the United Kingdom up to 2009: multicentre observational study

Author

David, Dolling, Caroline, Sabin, Valerie, Delpech, Erasmus, Smit, Anton, Pozniak, David, Asboe, Andrew Leigh, Brown, Duncan, Churchill, Ian, Williams, Anna Maria, Geretti, Andrew, Phillips, Nicola, Mackie, Gary, Murphy, Hannah, Castro, Deenan, Pillay, Patricia, Cane, David, Dunn, and Kholoud, Porter

Subjects

Drug, Adult, Male, medicine.medical_specialty, Adolescent, media_common.quotation_subject, HIV Infections, Drug resistance, Microbial Sensitivity Tests, Cohort Studies, 03 medical and health sciences, Zidovudine, Young Adult, 0302 clinical medicine, Mutation Rate, Internal medicine, Drug Resistance, Viral, medicine, Prevalence, Humans, 030212 general & internal medicine, Young adult, media_common, Aged, Aged, 80 and over, 0303 health sciences, 030306 microbiology, Transmission (medicine), business.industry, Stavudine, General Medicine, Middle Aged, Virology, Reverse transcriptase, United Kingdom, 3. Good health, Logistic Models, Anti-Retroviral Agents, HIV-1, Linear Models, Female, business, Cohort study, medicine.drug

Abstract

Objective To evaluate whether the prevalence of HIV-1 transmitted drug resistance has continued to decline in infections probably acquired within the United Kingdom. Design Multicentre observational study. Setting All UK public laboratories conducting tests for genotypic HIV resistance as a part of routine care. Participants 14584 patients infected with HIV-1 subtype B virus, who were first tested for resistance before receiving antiretroviral therapy between January 2002 and December 2009. Main outcome measure Prevalence of transmitted drug resistance, defined as one or more resistance mutations from the surveillance list recommended by the World Health Organization. Results 1654 (11.3%, 95% confidence interval 10.8% to 11.9%) patients had one or more mutations associated with transmitted HIV-1 drug resistance; prevalence was found to decline from 15.5% in 2002 to 9.6% in 2007, followed by a slight increase to 10.9% in 2009 (P=0.21). This later rise was mainly a result of increases in resistance to nucleos(t)ide reverse transcriptase inhibitors (from 5.4% in 2007 to 6.6% in 2009, P=0.24) and protease inhibitors (1.5% to 2.1%, P=0.12). Thymidine analogue mutations, including T215 revertants, remained the most frequent mutations associated with nucleos(t)ide reverse transcriptase inhibitors, despite a considerable fall in stavudine and zidovudine use between 2002 and 2009 (from 29.4% of drug regimens in 2002 to 0.8% in 2009, from 47.9% to 8.8%, respectively). Conclusions The previously observed decline in the prevalence of transmitted drug resistance in HIV-1 infections probably acquired in the UK seems to have stabilised. The continued high prevalence of thymidine analogue mutations suggests that the source of this resistance may be increasingly from patients who have not undergone antiretroviral therapy and who harbour resistant viruses. Testing of all newly diagnosed HIV-1 positive people should be continued.

Published

2012

213. Compensatory cis-trans regulation dominates the evolution of mouse gene expression

Author

A. Goncalves, S. Leigh-Brown, D. Thybert, K. Stefflova, E. Turro, P. Flicek, A. Brazma, D. T. Odom, and J. Marioni

Published

2012

214. The HIV Epidemic: High-Income Countries

Author

Sten H. Vermund and Andrew J. Leigh-Brown

Subjects

Male, Alcohol Drinking, media_common.quotation_subject, Ethnic group, HIV Infections, General Biochemistry, Genetics and Molecular Biology, Men who have sex with men, Risk Factors, Drug Resistance, Viral, medicine, Humans, Needle Sharing, Homosexuality, Homosexuality, Male, Epidemics, Heterosexuality, Substance Abuse, Intravenous, media_common, Needle sharing, Molecular Epidemiology, Unsafe Sex, Transmission (medicine), business.industry, Developed Countries, Transfusion Reaction, medicine.disease, Virology, Infectious Disease Transmission, Vertical, Substance abuse, Income, Female, business, Developed country, Demography, Perspectives

Abstract

The HIV epidemic in higher-income nations is driven by receptive anal intercourse, injection drug use through needle/syringe sharing, and, less efficiently, vaginal intercourse. Alcohol and noninjecting drug use increase sexual HIV vulnerability. Appropriate diagnostic screening has nearly eliminated blood/blood product-related transmissions and, with antiretroviral therapy, has reduced mother-to-child transmission radically. Affected subgroups have changed over time (e.g., increasing numbers of Black and minority ethnic men who have sex with men). Molecular phylogenetic approaches have established historical links between HIV strains from central Africa to those in the United States and thence to Europe. However, Europe did not just receive virus from the United States, as it was also imported from Africa directly. Initial introductions led to epidemics in different risk groups in Western Europe distinguished by viral clades/sequences, and likewise, more recent explosive epidemics linked to injection drug use in Eastern Europe are associated with specific strains. Recent developments in phylodynamic approaches have made it possible to obtain estimates of sequence evolution rates and network parameters for epidemics.

Published

2012

215. Immune responses in pigs vaccinated with adjuvanted and non-adjuvanted A(H1N1)pdm/09 influenza vaccines used in human immunization programmes

Author

Lefevre, Eric A, Carr, B Veronica, Inman, Charlotte F, Prentice, Helen, Brown, Ian H, Brookes, Sharon M, Garcon, Fanny, Hill, Michelle L, Iqbal, Munir, Elderfield, Ruth A, Barclay, Wendy S, Gubbins, Simon, Bailey, Mick, Charleston, Bryan, Leigh Brown, Andrew, Woolhouse, Mark, Archibald, Alan, Hill, Michelle L [0000-0002-9289-5811], Iqbal, Munir [0000-0001-5165-5339], Gubbins, Simon [0000-0003-0538-4173], and Apollo - University of Cambridge Repository

Subjects

Viral Diseases, Enzyme-Linked Immunospot Assay, viruses, PATHOGENESIS, Sus scrofa, lcsh:Medicine, EXPERIMENTAL-INFECTION, 0302 clinical medicine, Influenza A Virus, H1N1 Subtype, Interferon, T-Lymphocyte Subsets, Zoonoses, Cytotoxic T cell, PROTECTION, SWINE, lcsh:Science, 0303 health sciences, Multidisciplinary, Reverse Transcriptase Polymerase Chain Reaction, Viral Vaccine, Vaccination, Flow Cytometry, Fluoresceins, 3. Good health, Infectious Diseases, Veterinary Diseases, Influenza Vaccines, Science & Technology - Other Topics, Medicine, COSI, medicine.drug, Research Article, TRANSMISSION, General Science & Technology, Animal Types, Immunology, Succinimides, Enzyme-Linked Immunosorbent Assay, VIRUS-INFECTION, H1N1 VACCINE, Biology, Real-Time Polymerase Chain Reaction, Microbiology, Virus, Statistics, Nonparametric, Cell Line, 03 medical and health sciences, Immune system, Dogs, Adjuvants, Immunologic, Orthomyxoviridae Infections, Virology, MD Multidisciplinary, medicine, Animals, 030304 developmental biology, Cell Proliferation, Science & Technology, Interferon-gamma production, MULTIDISCIPLINARY SCIENCES, lcsh:R, Immunity, EVOLUTION, Immunization, Immunoglobulin G, REPLICATION, CELLS, Leukocytes, Mononuclear, lcsh:Q, Clinical Immunology, Veterinary Science, 030215 immunology

Abstract

Following the emergence and global spread of a novel H1N1 influenza virus in 2009, two A(H1N1)pdm/09 influenza vaccines produced from the A/California/07/09 H1N1 strain were selected and used for the national immunisation programme in the United Kingdom: an adjuvanted split virion vaccine and a non-adjuvanted whole virion vaccine. In this study, we assessed the immune responses generated in inbred large white pigs (Babraham line) following vaccination with these vaccines and after challenge with A(H1N1)pdm/09 virus three months post-vaccination. Both vaccines elicited strong antibody responses, which included high levels of influenza-specific IgG1 and haemagglutination inhibition titres to H1 virus. Immunisation with the adjuvanted split vaccine induced significantly higher interferon gamma production, increased frequency of interferon gamma-producing cells and proliferation of CD4(-)CD8(+) (cytotoxic) and CD4(+)CD8(+) (helper) T cells, after in vitro re-stimulation. Despite significant differences in the magnitude and breadth of immune responses in the two vaccinated and mock treated groups, similar quantities of viral RNA were detected from the nasal cavity in all pigs after live virus challenge. The present study provides support for the use of the pig as a valid experimental model for influenza infections in humans, including the assessment of protective efficacy of therapeutic interventions.

Published

2012

216. EVOLUTIONARY BIOLOGY OF HUMAN IMMUNODEFICIENCY VIRUS

Author

J. Leigh Brown and Edward C. Holmes

Subjects

Genetics, Genetic diversity, Ecology, Phylogenetic tree, biology, Molecular epidemiology, medicine.disease, biology.organism_classification, Virology, Virus, Phylogenetics, medicine, Sooty mangabey, Genetic variability, Immunodeficiency

Abstract

The human immunodeficiency viruses. HIV-l and HIV-2. are members of a group of closely related viruses found in a number of different African primate species. More distantly related lentiviruses are found in several different mam­ malian orders. All are associated with long-term infections, but the outcome of infection ranges from a complete absence of symptoms to a rapidly devel­ oping immunodeficiency and death. While HIV-2 is probably directly related to a virus that is responsible for an asymptomatic infection in the Sooty Mangabey, no obvious candidate for the progenitor of HIV-1 has yet been found. Substantial genetic diversity is present in all immunodeficiency viruses, and phylogenetic analysis of HIV -1 sequences obtained from a wide range of geographic locations has revealed 5-7 groups of viral strains, all equally distant from each other. All groups have been found in Africa, but their distribution elsewhere reflects chance links between individuals at high risk of infection. In some areas large epidemics have spread through groups of such individuals to infect thousands within a few months, resulting in an increase in the global frequency of the particular strain

Published

1994

217. Residual Human Immunodeficiency Virus (HIV) Type 1 RNA and DNA in Lymph Nodes and HIV RNA in Genital Secretions and in Cerebrospinal Fluid after Suppression of Viremia for 2 Years

Author

Gunthard, Huldrych F., Havlir, Diane V., Fiscus, Susan, Zhang, Zhi-Qiang, Eron, Joseph, Mellors, John, Gulick, Roy, Frost, Simon D. W., Leigh Brown, Andrew J., Schleif, William, Valentine, Fred, Jonas, Leslie, Meibohm, Anne, Ignacio, Caroline C., Isaacs, Robin, Gamagami, Reza, Emini, Emilio, Haase, Ashley, Richman, Douglas D., and Wong, Joseph K.

Subjects

HIV (Viruses) -- Reproduction, HIV infection -- Research, Health

Published

2001

218. Transmission Network Parameters Estimated From HIV Sequences for a Nationwide Epidemic

Author

Samantha Lycett, Andrew J. Leigh Brown, Gareth Hughes, Esther Fearnhill, David Dunn, and Lucy A. Weinert

Subjects

Male, Population, Molecular Sequence Data, Human immunodeficiency virus (HIV), HIV Infections, Biology, medicine.disease_cause, Men who have sex with men, law.invention, Major Articles and Brief Reports, Acquired immunodeficiency syndrome (AIDS), law, medicine, Cluster Analysis, Humans, Immunology and Allergy, education, Epidemics, Phylogeny, education.field_of_study, Molecular Epidemiology, Sequence Analysis, DNA, Degree distribution, medicine.disease, Virology, United Kingdom, Molecular Typing, Transmission (mechanics), Infectious Diseases, Etiology, HIV-1, HIV/AIDS, Contact Tracing, Contact tracing, Demography

Abstract

Human immunodeficiency virus (HIV) infection, like all sexually transmitted infections, spreads along the sexual contact network, and contact tracing played a key role in establishing the etiology of AIDS [1]. However, more recent studies have struggled to achieve any reconciliation between contact networks revealed by interview data and transmission networks reconstructed from the viral phylogeny [2, 3]. There are several possible reasons for this but 2 important factors are the long period of infectiousness (in the absence of therapy) and the low average risk of transmission per sexual contact [4]. The consequence of the first factor is that although sexual contact networks constructed from interview data usually work within a time frame of 1 year [5, 6], the HIV infection of the subject may have occurred at any time over a period of several years. The consequence of the second factor is reduction of the confidence that any particular contact was associated with infection. Other possible reasons for the lack of agreement that may be associated with particular risk groups include network complexity and anonymous sex. In addition, earlier studies of HIV-infected communities using sequence data were generally based on a small sample of the infected population, reducing the probability of including individuals from the same transmission network [7]. More recently, often working within defined risk groups, a number of studies have identified transmission networks by means of sequence analysis [8–10]. However, this static picture alone does not permit the quantitative description of the network through which HIV has been transmitted [11]. We have introduced an approach to estimating the HIV transmission network structure of a population based on the analysis of HIV sequences generated in the course of routine clinical care to test for antiretroviral resistance [12, 13]. Under UK guidelines from 2003, such tests are now performed for all patients entering therapy, which is recommended for patients with a CD4 cell count of ≤350 cells/μL [14]. Central collection of the assay results from the majority of clinics performing the assays in the United Kingdom allowed a data set of sequences from >26 000 patients to be constructed, including approximately two-thirds of the total number of men who have sex with men (MSM) receiving care for HIV infection in the United Kingdom [15]. We have already demonstrated that phylogenetic analysis of large population-based data sets reveals much more of the transmission pattern than has been seen before [12] and that in combination with relaxed clock models it has shed new light on the dynamics of the HIV infection epidemic in both the MSM and heterosexual contact risk groups. Here we extend our earlier analysis [12] to the MSM population of the entire United Kingdom. Using viral sequences from almost 60% of MSM diagnosed with HIV infection in 2009, we infer the degree distribution of the transmission networks, based on the time-resolved viral phylogenies, for a range of time depths. We have already shown that that the degree distribution inferred in this way can be approximated by a power law [13], as shown earlier for sexual contact networks inferred from interview data [5]. We here test a series of distributions for fit to the data to determine whether a preferential attachment model is, as has been suggested, the most appropriate model for transmission in this group.

Published

2011

219. Evolutionary relationships of the human immunodeficiency viruses

Author

Andrew J. Leigh Brown

Subjects

Genetics, viruses, Human immunodeficiency virus (HIV), Viral Genes, Nucleic acid sequence, Biology, medicine.disease_cause, medicine.disease, Virus, Acquired immunodeficiency syndrome (AIDS), Viral evolution, medicine, Human virome, Ecology, Evolution, Behavior and Systematics, Immunodeficiency

Abstract

The rapid accumulation of nucleotide sequence data on viral genes has allowed, for the first time, the development of detailed phylogenies of viruses based on an objective criterion. This has been demonstrated clearly in the recent analysis of the evolutionary relationships of HIV - the AIDS virus. When first characterized, HIV seemed aberrant and almost unique in many features. Now it is known to be one of a large group of immunodeficiency viruses, which are widely distributed among primates and other mammals.

Published

2011

220. Resistance of a human serum-selected human immunodeficiency virus type 1 escape mutant to neutralization by CD4 binding site monoclonal antibodies is conferred by a single amino acid change in gp120

Author

Andrew J. Leigh Brown, Ja Mckeating, Susan Zolla-Pazner, S Ashelford, M Schutten, J Bennett, and Peter Balfe

Subjects

medicine.drug_class, Molecular Sequence Data, Restriction Mapping, Immunology, Mutant, Mutagenesis (molecular biology technique), HIV Envelope Protein gp120, Ligands, Transfection, Monoclonal antibody, Microbiology, Epitope, Neutralization, Cell Line, Conserved sequence, Epitopes, Antigens, CD, Neutralization Tests, Virology, medicine, Humans, Point Mutation, Amino Acid Sequence, Cloning, Molecular, Binding site, Conserved Sequence, Binding Sites, Base Sequence, biology, Antibodies, Monoclonal, Molecular biology, Recombinant Proteins, Oligodeoxyribonucleotides, Insect Science, CD4 Antigens, HIV-1, Mutagenesis, Site-Directed, biology.protein, Antibody, Research Article

Abstract

We have selected an HXB2 variant which can replicate in the presence of a neutralizing human serum. Sequencing of the gp120 region of the env gene from the variant and parental viruses identified a single amino acid substitution in the third conserved region of gp120 at residue 375 (AGT-->AAT, Ser-->Asn; designated 375 S/N). The escape mutant was found to be resistant to neutralization by soluble CD4 (sCD4) and four monoclonal antibodies (MAbs), 39.13g, 1.5e, G13, and 448, binding to epitopes overlapping that of the CD4 binding site (CD4 b.s.). Introduction of the 375 S/N mutation into HXB2 by site-directed mutagenesis confirmed that this mutation is responsible for the neutralization-resistant phenotype. Both sCD4 and three of the CD4 b.s. MAbs (39.13g, 1.5e, and G13) demonstrated reduced binding to the native 375 S/N mutant gp120. The ability to select for an escape variant resistant to multiple independent CD4 b.s. MAbs by a human serum confirms the reports that antibodies to the discontinuous CD4 b.s. are a major component of the group-specific neutralizing activity in human sera.

Published

1993

221. Selection for specific sequences in the external envelope protein of human immunodeficiency virus type 1 upon primary infection

Author

Peter Simmonds, Edward C. Holmes, A Cleland, Lin Qi Zhang, Andrew J. Leigh Brown, and P. Mackenzie

Subjects

Male, Time Factors, Sequence analysis, Molecular Sequence Data, Immunology, Population, HIV Core Protein p24, HIV Infections, V3 loop, Biology, Genes, env, Polymerase Chain Reaction, Microbiology, Virus, Sequence Homology, Nucleic Acid, Virology, HIV Seropositivity, Humans, Amino Acid Sequence, Selection, Genetic, Seroconversion, education, Genetics, education.field_of_study, Base Sequence, Sequence Homology, Amino Acid, Nucleic acid sequence, Genetic Variation, Provirus, Genes, gag, Hypervariable region, Phenotype, Insect Science, HIV-1, Leukocytes, Mononuclear, Female, Sequence Analysis, Research Article

Abstract

Viral RNA was extracted from plasma samples collected from five individuals during the period of viremia before seroconversion in primary infection with human immunodeficiency virus type 1 (HIV-1) and amplified by polymerase chain reaction. Nucleotide sequence analysis of amplified DNA from the V3 and V4 hypervariable regions indicated that the initial virus population of each acutely infected individual was completely homogeneous in sequence. No intrasample variability was found among the 44,090 nucleotides sequenced in this region of env, contrasting with the high degree of variability normally found in seropositive individuals. Paradoxically, substantial sequence variability was found in the normally high conserved gag gene (encoding p17) in most of the preseroconversion samples. The diversity of p17 sequences in samples that were homogeneous in V3 and V4 can most readily be explained by the existence of strong selection for specific env sequences either upon transmission or in the interval between exposure and seroconversion in the exposed individual. Evidence that localizes the selected region upon transmission to V3 is provided by the similarity or identity of V3 loop sequences in five individuals with epidemiologically unrelated HIV-1 infections, while regions flanking the V3 loop and the V4 hypervariable region were highly divergent. The actual V3 sequences were similar to those associated with macrophage tropism in primary isolates of HIV, irrespective of whether infection was acquired by sexual contact or parenterally through transfusion of contaminated factor VIII. Proviral DNA sequences in peripheral blood mononuclear cells remained homogeneous in the V3 and V4 regions (and variable in p17gag) for several months after seroconversion. The persistence of HIV sequences in peripheral blood mononuclear cells identical to those found at primary infection in the absence of continued virus expression provides an explanation for the previously observed differences in the composition of circulating DNA and RNA populations in sequential samples from seropositive individuals.

Published

1993

222. The significance of the micropores at the stem-cement interface in total hip replacement

Author

Leigh Brown, Simon Barrans, Xiangqian Jiang, Hongyu Zhang, and Liam Blunt

Subjects

musculoskeletal diseases, medicine.medical_specialty, Materials science, medicine.medical_treatment, Arthroplasty, Replacement, Hip, Biomedical Engineering, Biophysics, Total hip replacement, Aseptic loosening, Dentistry, Bioengineering, Osteoarthritis, Prosthesis, Biomaterials, medicine, Humans, Femur, Cement, business.industry, technology, industry, and agriculture, Bone Cements, equipment and supplies, Bone cement, medicine.disease, Arthroplasty, Surgery, Prosthesis Failure, surgical procedures, operative, Stress, Mechanical, business, Porosity

Abstract

Cemented total hip replacement has been performed worldwide to treat patients with osteoarthritis and osteonecrosis, with aseptic loosening as its primary reason for revision. It has been indicated that the stem-cement interfacial porosity may contribute to the early loosening of cemented hip prosthesis. In addition, it is generally accepted that the micropores in bone cement surface and in the bulk material are detrimental to the mechanical integrity of bone cement and act as stress concentrators, resulting in generation of fatigue cracks in the cement mantle. Furthermore, it was demonstrated that the micropores also play an important part in initiation and propagation of fretting wear on polished femoral stems. Taking this into consideration, a detailed review of the potential significance of the micropores in bone cement and the methods that could be employed to reduce porosity is given in this article. It was considered that modern cementing techniques are clinically beneficial and should be applied in surgery to further improve the survivorship of cemented total hip replacement.

Published

2010

223. Regulatory Divergence of Transcript Isoforms in a Mammalian Model System

Author

Leigh-Brown, Sarah, primary, Goncalves, Angela, additional, Thybert, David, additional, Stefflova, Klara, additional, Watt, Stephen, additional, Flicek, Paul, additional, Brazma, Alvis, additional, Marioni, John C., additional, and Odom, Duncan T., additional

Published

2015

224. Re-emergence of HIV in the PWID population of Glasgow

Author

Jackson, C., primary, Bradley-Stewart, A., additional, Gunson, R.N., additional, Shepherd, S., additional, Aitken, C., additional, Ragonnet-Cronin, M., additional, Leigh-Brown, A., additional, Milosevic, C., additional, and Goldberg, D., additional

Published

2015

225. Grave voices: A discussion about praxis

Author

Alison Leigh Brown

Subjects

Phenomenology (philosophy), Philosophy, Praxis, Psychoanalysis, Sociology and Political Science, media_common.quotation_subject, Political philosophy, media_common

Published

1992

226. Detection of Mammalian Virulence Determinants in Highly Pathogenic Avian Influenza H5N1 Viruses: Multivariate Analysis of Published Data

Author

Samantha Lycett, Art F. Y. Poon, Melissa J. Ward, S. L. Kosakovsky Pond, A. J. Leigh Brown, and Fraser I Lewis

Subjects

viruses, animal diseases, Immunology, Orthomyxoviridae, Hemagglutinin (influenza), Virulence, Genome, Viral, medicine.disease_cause, Microbiology, Genome, Mice, Virology, medicine, Influenza A virus, Animals, Humans, Amino Acids, Gene, Probability, Genetics, Mutation, Models, Statistical, biology, Influenza A Virus, H5N1 Subtype, Computational Biology, virus diseases, Bayes Theorem, biology.organism_classification, Influenza A virus subtype H5N1, Phenotype, Genetic Diversity and Evolution, Insect Science, Multivariate Analysis, biology.protein, Gene Deletion

Abstract

Highly pathogenic avian influenza (HPAI) virus H5N1 infects water and land fowl and can infect and cause mortality in mammals, including humans. However, HPAI H5N1 strains are not equally virulent in mammals, and some strains have been shown to cause only mild symptoms in experimental infections. Since most experimental studies of the basis of virulence in mammals have been small in scale, we undertook a meta-analysis of available experimental studies and used Bayesian graphical models (BGM) to increase the power of inference. We applied text-mining techniques to identify 27 individual studies that experimentally determined pathogenicity in HPAI H5N1 strains comprising 69 complete genome sequences. Amino acid sequence data in all 11 genes were coded as binary data for the presence or absence of mutations related to virulence in mammals or nonconsensus residues. Sites previously implicated as virulence determinants were examined for association with virulence in mammals in this data set, and the sites with the most significant association were selected for further BGM analysis. The analyses show that virulence in mammals is a complex genetic trait directly influenced by mutations in polymerase basic 1 (PB1) and PB2, nonstructural 1 (NS1), and hemagglutinin (HA) genes. Several intra- and intersegment correlations were also found, and we postulate that there may be two separate virulence mechanisms involving particular combinations of polymerase and NS1 mutations or of NS1 and HA mutations.

Published

2009

227. Understanding initiation and propagation of fretting wear on the femoral stem in total hip replacement

Author

Hongyu Zhang, Leigh Brown, Xiang Jiang, Simon Barrans, and Liam Blunt

Subjects

musculoskeletal diseases, Cement, Materials science, Total hip replacement, Fretting, 02 engineering and technology, Surfaces and Interfaces, Tribology, Femoral stem, 021001 nanoscience & nanotechnology, Condensed Matter Physics, Bone cement, Surfaces, Coatings and Films, Fretting wear, 020303 mechanical engineering & transports, 0203 mechanical engineering, Mechanics of Materials, Wear simulation, Materials Chemistry, Forensic engineering, Composite material, 0210 nano-technology

Abstract

The femoral stem–bone cement interface in total hip replacement is supposed to experience low amplitude oscillatory micromotion under physiological loading, consequently leading to fretting wear on the stem surface, which nowadays is considered to play an important part in the overall wear of cemented prosthesis. However, initiation and propagation of fretting wear has been poorly documented and a better understanding concerning this issue has not been established as yet. This present study, on the basis of a profound surface investigation of a polished Exeter V40™ femoral stem and Simplex P bone cement obtained from an in vitro wear simulation, demonstrated that the edges of the micropores in the cement surface matched pretty well to the boundaries of the worn areas on the stem surface. This would indicate that these micropores contributed significantly to the fretting process at the stem–cement interface.

Published

2009

228. Crystallographic and cellular characterisation of two mutations stabilising the native fold of alpha1-antitrypsin: implications for rational drug design

Author

Gooptu, B, MIRANDA BANOS, MARIA ELENA, Nobeli, I, Mallya, M, Purkiss, A, LEIGH BROWN SC, Summers, C, Phillips, Rl, Lomas, Da, and Barrett, Te

Published

2009

229. Detection, quantification and sequencing of HIV-1 from the plasma of seropositive individuals and from factor VIII concentrates

Author

Peter Simmonds, Christopher A. Ludlam, Andrew J. Leigh Brown, and Lin Qi Zhang

Subjects

Molecular Sequence Data, Immunology, HIV Infections, Biology, Hemophilia A, Genes, env, Polymerase Chain Reaction, Virus, law.invention, chemistry.chemical_compound, law, RNA polymerase, HIV Seropositivity, Humans, Immunology and Allergy, Amino Acid Sequence, Gene, Polymerase chain reaction, Factor VIII, Base Sequence, RNA-Directed DNA Polymerase, RNA, Genes, pol, Virology, Infectious Diseases, Viral replication, chemistry, HIV-1, RNA, Viral, Viral disease, Drug Contamination

Abstract

A highly sensitive and reliable RNA polymerase chain reaction method has been developed which has been used to detect, quantify and sequence cell-free HIV RNA directly from the plasma of seropositive individuals. Plasma from 10 out of 12 haemophiliacs tested was found to contain detectable levels of HIV-1 RNA [log mean value: 1.2 x 10(3) copies for Centers for Disease Control (CDC) group II patients, 5.5 x 10(3) copies for CDC group IV patients]. The presence of cell-free circulating virus in both symptomatic and asymptomatic individuals suggests that viral replication continues throughout the course of infection. The same procedure has been used to detect and sequence HIV-1 RNA in two batches of unheated commercial factor VIII concentrate distributed in 1981 and 1983. The sequences obtained revealed a closer relationship to North American than to African strains of HIV-1.

Published

1991

230. Sequence variability in human immunodeficiency viruses

Author

Andrew J. Leigh Brown

Subjects

Immunology, Human immunodeficiency virus (HIV), Biology, medicine.disease_cause, Virology, Genome, Infectious Diseases, Viral evolution, Genetic variation, medicine, Consensus sequence, Immunology and Allergy, Base sequence, Peptide sequence, Sequence (medicine)

Published

1991

231. Femoral stem wear in cemented total hip replacement

Author

Simon Barrans, Hongyu Zhang, Leigh Brown, Xiang Jiang, Liam Blunt, and Y. Zhao

Subjects

musculoskeletal diseases, medicine.medical_specialty, Materials science, Surface Properties, medicine.medical_treatment, Arthroplasty, Replacement, Hip, Aseptic loosening, Total hip replacement, Dentistry, New materials, Osteoarthritis, Femoral stem, Prosthesis Design, Prosthesis, Tensile Strength, Materials Testing, medicine, Humans, Cementation, business.industry, Mechanical Engineering, Femur Head, General Medicine, Bone cement, medicine.disease, Arthroplasty, Surgery, Prosthesis Failure, Equipment Failure Analysis, TJ, Hip Prosthesis, business, human activities

Abstract

The great success of cemented total hip replacement to treat patients with end-stage osteoarthritis and osteonecrosis has been well documented. However, its long-term survivorship has been compromised by progressive development of aseptic loosening, and few hip prostheses could survive beyond 25 years. Aseptic loosening is mainly attributed to bone resorption which is activated by an in-vivo macrophage response to particulate debris generated by wear of the hip prosthesis. Theoretically, wear can occur not only at the articulating head—cup interface but also at other load-bearing surfaces, such as the stem—cement interface. Recently, great progress has been made in reducing wear at the head—cup interface through the introduction of new materials and improved manufacture; consequently femoral stem wear is considered to be playing an increasingly significant role in the overall wear of cemented total hip replacement. In this review article, the clinical incidences of femoral stem wear are comprehensively introduced, and its significance is highlighted as a source of generation of wear debris and corrosion products. Additionally, the relationship between femoral stem surface finish and femoral stem wear is discussed and the primary attempts to reproduce femoral stem wear through in-vitro wear testing are summarized. Furthermore, the initiation and propagation processes of femoral stem wear are also proposed and a better understanding of the issue is considered to be essential to reduce femoral stem wear and to improve the functionality of cemented total hip replacement.

Published

2008

232. Genetic basis of variation in tenofovir drug susceptibility in HIV-1

Author

Fraser I Lewis, Robert J Murray, Michael D. Miller, and Andrew J. Leigh Brown

Subjects

Mean squared error, Genotype, Anti-HIV Agents, Immunology, Decision tree, Organophosphonates, HIV Infections, Biology, Logistic regression, Models, Biological, Lethal Dose 50, Predictive Value of Tests, Genetic variation, Statistics, Drug Resistance, Viral, Immunology and Allergy, Humans, Amino Acid Sequence, Tenofovir, Categorical variable, Genetics, Decision tree learning, Adenine, Genetic Variation, Stepwise regression, Random forest, Infectious Diseases, Phenotype, HIV-1

Abstract

Objective To develop an improved model for the genetic basis of reduced susceptibility to tenofovir in vitro. Methods A dataset of 532 HIV-1 subtype B reverse transcriptase genotypes for which matched phenotypic susceptibility data were available was assembled, both as a continuous (transformed) dataset and a categorical dataset generated by imposing a cut-off on the basis of earlier studies of in-vivo response of 1.4-fold. Models were generated using stepwise regression, decision tree and random forest approaches on both the continuous and categorical data. Models were compared by mean squared error (continuous models), or by misclassification rates by nested crossvalidation. Results From the continuous dataset, stepwise linear regression, regression tree and regression forest methods yielded models with MSE of 0.46, 0.48 and 0.42 respectively. Amino acids 215, 65, 41, 67, 184 and 151 in HIV-1 reverse transcriptase were identified in all three models and amino acid 210 in two. The categorical data yielded logistic regression, classification tree and forest models with misclassification rates of 26, 24 and 23%, respectively. Amino acids 215, 65 and 67 appeared in all; 41, 184, 210 and 151 were also included in the classification forest model. Conclusion The random forests approach has yielded a substantial improvement in the available models to describe the genetic basis of reduced susceptibility to tenofovir in vitro. The most important sites in these models are amino acid sites 215, 65, 41, 67, 184, 151 and 210 in HIV-1 reverse transcriptase.

Published

2008

233. Estimating selection pressures on HIV-1 using phylogenetic likelihood models

Author

Ronald J. Ellis, Selene Zárate, A. J. Leigh Brown, Satish K. Pillai, Joseph K. Wong, S. L. Kosakovsky Pond, Simon D. W. Frost, Douglas D. Richman, Art F. Y. Poon, Susan J. Little, and Davey M. Smith

Subjects

Statistics and Probability, Likelihood Functions, Models, Statistical, Phylogenetic tree, Epidemiology, Extramural, Human immunodeficiency virus (HIV), virus diseases, Computational biology, Group-specific antigen, Biology, medicine.disease_cause, Virology, gag Gene Products, Human Immunodeficiency Virus, Virus, Article, Data sequences, Phylogenetics, medicine, HIV-1, Humans, Selection, Genetic, Selection (genetic algorithm), Phylogeny

Abstract

Human immunodeficiency virus (HIV-1) can rapidly evolve due to selection pressures exerted by HIV-specific immune responses, antiviral agents, and to allow the virus to establish infection in different compartments in the body. Statistical models applied to HIV-1 sequence data can help to elucidate the nature of these selection pressures through comparisons of non-synonymous (or amino acid changing) and synonymous (or amino acid preserving) substitution rates. These models also need to take into account the non-independence of sequences due to their shared evolutionary history. We review how we have developed these methods and have applied them to characterize the evolution of HIV-1 in vivo. To illustrate our methods, we present an analysis of compartment-specific evolution of HIV-1 env in blood and cerebrospinal fluid and of site-to-site variation in the gag gene of subtype C HIV-1.

Published

2008

234. General anaesthesia versus local anaesthesia for carotid surgery (GALA): a multicentre, randomised controlled trial

Author

GALA Trial Collaborative Group, C Lewis, S, P Warlow, C, R Bodenham, A, Colam, B, M Rothwell, P, Torgerson, D, Dellagrammaticas, D, Horrocks, M, Liapis, C, P Banning, A, Gough, M, J Gough, M, Fraser, A, Grant, S, Hunter, J, Leigh-Brown, A, Paterson, M, Soosay, V, Young, A, Williamson, A, Dean, Z, Mazzoli, T, Ricci, S, Valenti, D, Bamford, J, Beard, J, Dearden, M, Murray, G, Ruckley, V, E Norman, P, Sedivy, P, Idla, A, Schmitz-Rixen, T, Maritati, G, Bodenham, A, Cokic, N, Doppler, W, Hlatky, P, Koelblinger, C, Raith, C, Zölss, C, Dimmitt, S, Gharbi, R, Hankey, G, Maden, A, P Mwipatayi, B, Sieunarine, K, Tan, A, Turner, G, Wesseldine, A, T M, E Davis, Audzei, P, Davidovski, I, Dedul, D, Hetsiuk, A, Kornievich, S, Gao, J, Y-G, Huang, Jing, G, H, Li, Y-J, Li, Liu, B, C-W, Liu, J-D, Wu, W, Ye, C-H, Yu, Ban, T, Buljan, K, Candrlic, K, Dapic, D, Ilijasevic, M, Istvanic, T, Kovac, B, Kvolik, S, Lehner, V, Pinotic, K, Hudorović, N, Ivanec, Z, Lovricević, I, Mazul-Sunko, B, Novotny, Z, D De Syo, Vuković, V, Biebl, O, Dolecek, L, C El Samman, Kalasova, H, Kubricht, V, Matous, P, Michalek, P, Stajnrt, M, Stern, M, Svec, M, Vitasek, P, Vrzal, J, Weiss, K, Janousek, L, Kieslichova, E, Mazarova, V, Piza, P, Vychodil, P, Dulovcova, V, Fiksa, J, Hruby, J, Maresch, M, Mathias, M, Rubes, D, Tosenovsky, P, Vidim, T, Henzl, M, Riman, J, Ziegler, Z, Drabek, P, Hrbac, T, Reguli, S, Stigler, J, Bachleda, P, Drac, P, Hudecek, M, Koutna, J, Sanak, D, Utikal, P, Goldemund, D, Gregor, Z, Pavlikova, J, Podlaha, J, Privara, M, Staffa, R, Vlachovsky, R, Barankova, L, Chlouba, V, Fiedler, J, Prazak, P, Priban, V, Wierer, A, Ellervee, T, Järve, H, Sell, A, Taba, P, Kolbassov, V, Kullamaa, S, Paavel, T, Abramishvili, N, Bokuchava, M, Kachapuridze, N, Kipiani, K, Papashvili, K, Pargalava, N, Adili, F, Dietz, A, Neidhart, G, Nentwig, G, M Sitzer, O, Beno, M, Essink-Hassels, M, Lander, K, Ruemenapf, G, Breuer, P, Heldt, R, Melichar, G, Rieper, J, H Eckstein, H, Poppert, H, Schneider, G, Andrikopoulos, V, Angel, A, Bakogiannis, K, Dermitzaki, M, Georgakis, P, Lioupis, C, Maras, D, G Moulakakis, K, Sfyroeras, G, Arato, E, Gyevnar, Z, Hardi, P, Kasza, G, Kollar, L, Menyhei, G, Pal, E, Sinay, L, Verzar, Z, Volgyi, E, S Elmakias, S, Harah, E, Kristal, K, Lebi, D, Leonty, Y, Levy, D, Milo, R, Yoffe, B, Bissi, M, Cappellini, B, Cassamali, T, Corino, L, Denkewitz, T, Ghilardi, G, Massetto, N, P Di Mauro, Tommasino, C, Bartolucci, R, Buffa, V, M Corsi, F, D'Avino, E, F Di Cesare, L Di Pirro, Lappa, A, Luzzi, S, Menichetti, A, Nesi, F, Pannone, A, Picozzi, P, Pogany, G, Rabitti, G, Severi, L, Avella, R, Biandolino, P, P Giomarelli, P, R Monfregola, M, Palasciano, G, Peccianti, V, Pieragalli, D, Setacci, C, Setacci, F, Sirignano, P, Bordoni, M, Casadei, V, Cugnasca, M, A De Troia, Geremia, L, Guffanti, P, G Lo Guercio, V Maniaci, M, Mauri, Morbidelli, A, Aletta, A, Costanzo, E, D'Arrigo, G, F Di Stefano, Lomeo, A, Maugeri, S, C Monea, M, Scardavilli, G, Scolaro, A, Aloisi, P, Ciccozzi, A, Manno, M, Marrelli, A, Martinazzo, C, Mastromarino, A, Petrassi, C, Piroli, A, Spartera, C, Ventura, M, Alessandrini, F, Carissimi, C, M Centritto, E, Cinelli, G, C De Filippo, Liberatoscioli, G, Modugno, P, Rossi, M, T Attanzio, M, Bajardi, G, Bellisi, M, Machi, P, Salemi, S, Savettieri, G, A Crea, M, V di Lazzaro, Ferrante, A, Guarneri, S, Manni, R, Snider, F, Stefanuto, C, Berardi, G, Bianchi, A, Comis, M, Cumbo, P, Fadde, M, Ferrero, E, Ferri, M, Filardo, A, Gaggiano, A, Ganzaroli, M, Labate, C, Maggio, D, Mennuti, G, Minicucci, S, Musso, A, Nessi, F, Pasquino, M, Perretta, L, Piazza, S, Verdecchia, C, Viazzo, A, Antico, A, Battan, E, Ciarlo, M, Giardini, G, G Luca Iob, Marinello, C, Piccolo, D, Bove, R, Castrucci, T, Lorido, A, Sammarco, S, Bruzzone, B, Cannata, D, Colotto, P, Finocchi, C, Giudici, N, Mambrini, S, Mazzei, R, Palombo, D, Pellegrino, A, Rousas, N, Viacava, A, Ermirio, D, Faga, D, Simoni, G, Benedetti-Valentini, F, Gabrielli, R, Garofano, R, Gossetti, B, Guerricchio, R, Irace, L, Lenzi, G, Gedins, M, Kisis, K, Krievins, D, Krustina, I, Lietuvietis, E, Malina, M, Morlata, N, Rits, J, Thor, S, Ivanova, P, Kikule, I, Liepa, V, Ligers, A, Stengrevica, N, Vnukova, N, Zvirgzdins, V, P J A, M Brouwers, H Geelkerken, R, Stam, A, M A, M Simon, T den Hoed, P, Oltmans, M, Rettig, H, F Veen, H, Zuidgeest, D, Feldo, M, Kesik, J, Kobusiewicz, W, Łatkiewicz, D, Myślinski, W, Przywara, S, Terlecki, P, Wroński, J, Zubilewicz, T, Alfonso, G, Azevedo, E, R de Albuquerque, Mansilha, A, Al-Salman, M, K Aldaif, A, A Alnasr, T, A El Dawlatly, A, Elkayali, A, M Rabee, H, Chudikova, E, Chudá, I, Dulka, T, Goldenberg, Z, Lofaj, P, Pavlikova, M, Pisar, M, Sefranek, V, Slysko, R, Tomka, J, Tóthová, Z, Zita, Z, A Cairols, M, Iborra, E, Mercadal, M, Rubio, F, Canovas, D, Cobo, L, Gimenez-Gaibar, A, Gonzalez, E, Gonzalo, B, Guilera, N, Hospedales, J, J Laso, M, Perez, J, Solanich, T, Hensater, M, Karlström, L, Kjällman, L, Rosengren, L, C-A, Ewaldsson, Gillgren, P, T-B, Käll, Konrad, P, Lindkvist, M, Nilsson, L, Takolander, R, E von Zweigbergk, Cinar, B, Coruh, T, Kurc, E, Ozsoy, D, Sargin, M, Tutkavul, K, Yekeler, I, Aksoy, M, Aksoy, S, Kurtoglu, M, Arar, C, Canbaz, S, Celik, Y, Ege, T, Ketenc, S, Sunar, H, Unal, S, Asik, I, Bengisun, U, Koksoy, C, Yucemen, N, C Berridge, D, Caldicott, L, Cooper, J, Cross, M, Ford, H, Fuller, R, Gamlin, F, Homer-Vanniasinkum, S, Howell, S, Kent, P, Lumb, A, A I, D Mavor, D J, A Scott, Shah, M, Wanklyn, P, S Budd, J, Mcateer, P, Shaw, L, Dewar, R, H Lewis, M, Potter, C, Richards, H, Roberts, R, Townsend, E, Wagle, A, Woodford, P, Hall, G, Holdsworth, R, Macleod, M, Michels, L, P A, G Sandercock, Sudlow, C, Woods, A, S Abraham, J, Bukhari, M, Bush, A, Calvey, J, Chadwick, I, Krishnaprasad, K, Oldham, T, Tomlinson, M, Vickers, A, Wilson, D, Wilson, P, Greystone, S, C Grocott, E, Hayes, W, Haynes, S, Jenkins, C, Jenkins, D, Moore, W, Nyamekye, I, Overstall, P, Riseboro, S, Williams, H, Boyle, J, Duane, D, Gaunt, M, J Kirkpatrick, P, Martin, P, E Risdall, J, Scurrah, N, L Turner, C, Varty, K, T Ferguson, I, Horsfall, S, C Mitchell, D, Robinson, S, Frankel, J, E Morris, G, Phillips, M, Sansome, A, J Sparkes, D, Williams, J, Ashton, W, Baker, S, Clark, M, G Darke, S, Dunnill, R, Hargreaves, M, Jenkinson, D, Thomson, C, White, N, D Wijesinghe, L, Bapat, P, A Barrett, J, D Blair, S, Chandrasekar, R, Lawrence, G, Lowe, D, Sangster, G, Smith, M, M Van Miert, K Das, S, Malik, O, Nel, M, Rakowicz, W, Aukett, M, Carmichael, M, Colchester, A, R Taylor, P, Wood, C, Ageed, A, J Boom, S, Ghosh, S, Godfrey, J, Hewitt-Gray, J, Mcdiarmid, I, Yousif, S, Ziarkowski, A, Al-Din, A, Carpenter, M, Ch'Ng, K, J Curley, P, Davey, R, Henderson, B, F Hossain, J, D Irvine, C, Loizou, L, Main, A, Stanners, A, Muldoon, T, V Soong, C, Wiggam, I, P Armon, M, Burrows, M, Holmes, L, K Metcalf, A, Nunn, D, Abdul-Hamid, A, Akomalafe, B, Bryce, J, Chetter, I, Samaan, A, Briley, D, Collin, J, Darby, C, Dobson, M, Foex, P, Grange, C, Handa, A, Hands, L, E Higham, H, J M, T Perkins, Sear, J, Stoneham, M, Hamilton, G, Judge, C, Morris-Vincent, P, Pegg, M, A Wilson, L, I Aldoori, M, B E, A Dafalla, Kumar, N, I F, C Hay, Jefferson, P, Muir, I, Peel, W, Rutherford, J, Sathianathan, J, Wight, S, Williams, D, Wrathall, W, Bachoo, P, Brittenden, J, Counsell, C, Patey, R, Read, J, L de Cossart, K Dimitri, S, Edwards, P, Fergusson, N, Jameson, P, Somauroo, J, Taylor, V, D Aravindan, P, Brocklehurst, I, Mirza, S, N Namushi, R, O Oshodi, T, Ruff, D, A Solomon, S, Vassallo, J, Egbe, M, Halstead, G, Onwudike, M, Putland, A, Roberts, N, A Salaman, R, Watson, D, Caine, S, Day, J, Lamont, P, J Murphy, P, Smith, F, Beacham, K, J Dorman, P, Lambert, D, Rodgers, H, Collas, D, Sarin, S, Shah, J, S Baht, H, Banks, J, Cowie, L, Gunathilagan, G, Hargroves, D, Insall, R, G Smithard, D, K Chadha, D, R Pillay, W, Rashid, J, Sayles, J, Hill, S, Lawton, G, M Lloyd, C, Marsh, A, Clarke, G, J Lonsdale, R, Venables, G, Cross, R, Lord, B, Mcilmoyle, J, Y Osman, H, Robinson, J, Chant, H, Mate, A, Sim, D, Upton, P, Thomas, D, H Wolfe, J, Mccollum, C, O'Neill, P, Bernatsky, V, Bondar, L, Karpenko, A, Mamonova, M, Muz, N, and Yavorsky, V

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Carotid endarterectomy, general anesthesia, local anesthesia, carotid surgery, Anesthesia, General, law.invention, Postoperative Complications, Randomized controlled trial, law, medicine, Humans, Carotid Stenosis, General anaesthesia, general anaesthesia, Stroke, Aged, Endarterectomy, Endarterectomy, Carotid, local anaesthesia, Intention-to-treat analysis, business.industry, General Medicine, Perioperative, Vascular surgery, medicine.disease, Surgery, Anesthesia, Female, business, Anesthesia, Local

Abstract

BACKGROUND: The effect of carotid endarterectomy in lowering the risk of stroke ipsilateral to severe atherosclerotic carotid-artery stenosis is offset by complications during or soon after surgery. We compared surgery under general anaesthesia with that under local anaesthesia because prediction and avoidance of perioperative strokes might be easier under local anaesthesia than under general anaesthesia. METHODS: We undertook a parallel group, multicentre, randomised controlled trial of 3526 patients with symptomatic or asymptomatic carotid stenosis from 95 centres in 24 countries. Participants were randomly assigned to surgery under general (n=1753) or local (n=1773) anaesthesia between June, 1999 and October, 2007. The primary outcome was the proportion of patients with stroke (including retinal infarction), myocardial infarction, or death between randomisation and 30 days after surgery. Analysis was by intention to treat. The trial is registered with Current Control Trials number ISRCTN00525237. FINDINGS: A primary outcome occurred in 84 (4.8%) patients assigned to surgery under general anaesthesia and 80 (4.5%) of those assigned to surgery under local anaesthesia; three events per 1000 treated were prevented with local anaesthesia (95% CI -11 to 17; risk ratio [RR] 0.94 [95% CI 0.70 to 1.27]). The two groups did not significantly differ for quality of life, length of hospital stay, or the primary outcome in the prespecified subgroups of age, contralateral carotid occlusion, and baseline surgical risk. INTERPRETATION: We have not shown a definite difference in outcomes between general and local anaesthesia for carotid surgery. The anaesthetist and surgeon, in consultation with the patient, should decide which anaesthetic technique to use on an individual basis. FUNDING: The Health Foundation (UK) and European Society of Vascular Surgery.

Published

2008

235. GALA: an international multicentre randomised trial comparing general anaesthesia versus local anaesthesia for carotid surgery

Author

Gough, Michael J. Bodenham, Andrew Horrocks, Michael Colam, Bridget Lewis, Steff C. Rothwell, Peter M. Banning, Adrian P. Torgerson, David Gough, Moira Dellagrammaticas, Demosthenes Leigh-Brown, Anne Liapis, Christos Warlow, Charles

Abstract

Background: Patients who have severe narrowing at or near the origin of the internal carotid artery as a result of atherosclerosis have a high risk of ischaemic stroke ipsilateral to the arterial lesion. Previous trials have shown that carotid endarterectomy improves long-term outcomes, particularly when performed soon after a prior transient ischaemic attack or mild ischaemic stroke. However, complications may occur during or soon after surgery, the most serious of which is stroke, which can be fatal. It has been suggested that performing the operation under local anaesthesia, rather than general anaesthesia, may be safer. Therefore, a prospective, randomised trial of local versus general anaesthesia for carotid endarterectomy was proposed to determine whether type of anaesthesia influences peri-operative morbidity and mortality, quality of life and longer term outcome in terms of stroke-free survival. Methods/design: A two-arm, parallel group, multicentre randomised controlled trial with a recruitment target of 5000 patients. For entry into the study, in the opinion of the responsible clinician, the patient requiring an endarterectomy must be suitable for either local or general anaesthesia, and have no clear indication for either type. All patients with symptomatic or asymptomatic internal carotid stenosis for whom open surgery is advised are eligible. There is no upper age limit. Exclusion criteria are: no informed consent; definite preference for local or general anaesthetic by the clinician or patient; patient unlikely to be able to co-operate with awake testing during local anaesthesia; patient requiring simultaneous bilateral carotid endarterectomy; carotid endarterectomy combined with another operation such as coronary bypass surgery; and, the patient has been randomised into the trial previously. Patients are randomised to local or general anaesthesia by the central trial office. The primary outcome is the proportion of patients alive, stroke free ( including retinal infarction) and without myocardial infarction 30 days post-surgery. Secondary outcomes include the proportion of patients alive and stroke free at one year; health related quality of life at 30 days; surgical adverse events, re-operation and re-admission rates; the relative cost of the two methods of anaesthesia; length of stay and intensive and high dependency bed occupancy.

Published

2008

236. Estimating selection pressures on HIV-1 using phylogenetic likelihood models

Author

Pond, S. L. Kosakovsky, Poon, A. F. Y., Zarate, S., Smith, D. M., Little, S. J., Pillai, S. K., Ellis, R. J., Wong, J. K., Leigh Brown, Andrew, Richman, D. D., and Frost, S. D. W.

Abstract

Human immunodeficiency virus (HIV-1) can rapidly evolve due to selection pressures exerted by HIV-specific immune responses, antiviral agents, and to allow the virus to establish infection in different compartments in the body. Statistical models applied to HIV-1 sequence data can help to elucidate the nature of these selection pressures through comparisons of non-synonymous (or amino acid changing) and synonymous (or amino acid preserving) substitution rates. These models also need to take into account the non-independence of sequences due to their shared evolutionary history. We review how we have developed these methods and have applied them to characterize the evolution of HIV-1 in vivo. To illustrate our methods, we present an analysis of compartment-specific evolution of HIV-1 em) in blood and cerebrospinal fluid and of site-to-site variation in the gag gene of subtype C HIV-1. Copyright (C) 2008 John Wiley & Sons, Ltd.

Published

2008

237. HCV T Cell Re-Vaccination Strategies using Simian Adeno and MVA Viral Vectors to Enhance and Maintain Anti-Viral Immunity

Author

Alfredo Nicosia, E Barnes, Andrew J. Leigh Brown, Leo Swadling, Riccardo Cortese, Antonella Folgori, Stefania Capone, Stefano Colloca, and Felicity Hartnell

Subjects

Vaccination, medicine.anatomical_structure, Hepatology, T cell, Anti viral immunity, medicine, Biology, Simian, biology.organism_classification, Virology, Viral vector

Published

2016

238. Characterisation of the Specificity, Functionality and Durability of Host T-Cell Responses against the Full HEV Genome

Author

David Smith, Jacques Izopet, Katie Jeffery, J. Maggs, John Halliday, Leo Swadling, L. Vine, Andrew J. Leigh Brown, Harry R. Dalton, Richie G. Madden, R. Bendall, E Barnes, Nassim Kamar, Paul Klenerman, S. Jubb, J.G. Hunter, Jane Collier, Peter Simmonds, and C. Mclaughlin

Subjects

Genetics, medicine.anatomical_structure, Hepatology, Host (biology), T cell, medicine, Biology, Durability, Genome

Published

2016

239. Efficacy and Tolerability of Simeprevir and Daclatasvir for 12 or 24 Weeks in HCV Genotype 1b-Infected Treatment-Naïve Patients with Advanced Fibrosis or Compensated Cirrhosis

Author

M. Diago, Piero Luigi Almasio, S. Zeuzem, Ferenc Szalay, Ralph DeMasi, Ramon Planas, L. Gilles, I. Lonjon-Domanec, Suzanne Bourgeois, M. Schlag, Christophe Hézode, Giovanni Battista Gaeta, Peter Buggisch, Lawrence Serfaty, Andrew J. Leigh Brown, and Y. Horsmans

Subjects

Simeprevir, medicine.medical_specialty, Daclatasvir, Cirrhosis, Hepatology, business.industry, medicine.disease, 030226 pharmacology & pharmacy, Gastroenterology, Advanced fibrosis, Therapy naive, 03 medical and health sciences, 0302 clinical medicine, Genotype 1b, Tolerability, Internal medicine, medicine, 030211 gastroenterology & hepatology, business, medicine.drug

Published

2016

240. Transposable element-induced response to artificial selection in Drosophila melanogaster: molecular analysis of selection lines

Author

Anthony E. Shrimpton, Trudy F. C. Mackay, and Andrew J. Leigh Brown

Subjects

Male, Genetics, Genetic Variation, Investigations, Biology, Heritability, biology.organism_classification, Bristle, P element, Transposition (music), Drosophila melanogaster, Phenotype, Evolutionary biology, Genetic variation, DNA Transposable Elements, Animals, Female, Genetic variability, Selection, Genetic, Crosses, Genetic, Selection (genetic algorithm)

Abstract

Artificial selection lines for abdominal bristle score of Drosophila melanogaster established from P-M hybrid dysgenic crosses showed increases in selection response, heritability and phenotypic variance compared to similar lines started from nondysgenic crosses. To determine whether this increased genetic variance could be due to enhanced transposition of P elements following the dysgenic cross, the cytological locations (sites) of P elements were determined by in situ hybridization for the whole genome of samples of 20 individuals from the parental P strain, 20 individuals from each of the eight dysgenic selection lines, and ten individuals from each of the eight nondysgenic selection lines. Variation among and within the selection lines and the parental P strain in P element insertion sites was exceptionally high. A total of 601 sites were identified, but there was no difference in total number of sites per line, mean number of sites per individual, mean copy number per individual, or site frequency between dysgenic and nondysgenic selection lines, or between lines selected for high and low bristle score. Transposition following nondysgenic crosses may explain additional observations of accelerated selection responses in nondysgenic selection lines. It was not possible to deduce which, if any, of the several hundred insertions in the dysgenic selection lines were responsible for their extreme bristle phenotypes.

Published

1990

241. The polymerase chain reaction in the diagnosis of vertically transmitted HIV infection

Author

Paul Williams, Peter Simmonds, Peng Lee Yap, Peter Balfe, John Bishop, Ray Brettle, Rosie Hague, David Hargreaves, James Inglis, Andrew Leigh Brown, John Peutherer, Selma Rebus, and Jacqueline Mok

Subjects

Immunology, HIV Core Protein p24, Human immunodeficiency virus (HIV), Gene Products, gag, HIV Infections, Biology, medicine.disease_cause, Polymerase Chain Reaction, Peripheral blood mononuclear cell, DNA sequencing, Serology, law.invention, chemistry.chemical_compound, Pregnancy, law, medicine, Humans, Immunology and Allergy, Pregnancy Complications, Infectious, Gene, Polymerase chain reaction, Viral Core Proteins, Infant, Virology, Hypervariable region, Infectious Diseases, chemistry, Child, Preschool, DNA, Viral, Female, DNA

Abstract

The presence of HIV-1 DNA sequences in DNA from peripheral blood mononuclear cells (PBMCs) was investigated in a two-stage polymerase chain reaction ('double' PCR) using four sets of nested primers. The PBMCs tested were obtained from 46 children born to HIV-seropositive mothers, seven 'control' children born to HIV-seronegative mothers and seropositive fathers, and 45 healthy adult blood donors who were HIV seronegative. Nine of the children had symptomatic HIV infection and other laboratory features characteristic of HIV infection: all nine were PCR-positive with each set of primers in each of their 22 blood samples tested. The remaining 44 children had no clinical or laboratory evidence of HIV infection, and each of their 50 samples was PCR-negative with each set of primers, as were all blood donor samples. PCR-positive samples were tested in more detail using two of the sets of primers, which spanned hypervariable regions in the env gene. Polyacrylamide gel electrophoresis of DNA amplified from these regions yielded patterns of amplified DNA length variation which were characteristic for each child, and which changed little with time (in serial samples obtained over periods of 3-7 months). This excluded contamination as a cause of PCR positivity. This is the first report of the use of a double PCR for the diagnosis of HIV infection. The results demonstrate the specificity of this PCR method in diagnosis, with failure to reveal in this cohort any cases of vertically transmitted HIV-1 infection in addition to those already confirmed by conventional laboratory techniques.

Published

1990

242. HIV phylogenetics

Author

Andrew J. Leigh Brown, Deenan Pillay, Anna Maria Geretti, and Andrew Rambaut

Subjects

Human immunodeficiency virus (HIV), ComputingMilieux_LEGALASPECTSOFCOMPUTING, HIV Infections, Data_CODINGANDINFORMATIONTHEORY, Biology, Criminology, medicine.disease_cause, law.invention, InformationSystems_GENERAL, Phylogenetics, law, medicine, Humans, Phylogeny, General Environmental Science, General Engineering, Editorials, General Medicine, Virology, DNA Fingerprinting, Transmission (mechanics), TheoryofComputation_LOGICSANDMEANINGSOFPROGRAMS, HIV-1, General Earth and Planetary Sciences, ComputingMilieux_COMPUTERSANDSOCIETY, Crime

Abstract

Criminal convictions relying solely on this to establish transmission are unsafe

Published

2007

243. Reproduction of fretting wear at the stem—cement interface in total hip replacement

Author

Simon Barrans, Leigh Brown, Hongyu Zhang, and Liam Blunt

Subjects

Cement, musculoskeletal diseases, Materials science, Internationality, T1, Surface Properties, Mechanical Engineering, Metallurgy, Total hip replacement, Bone Cements, technology, industry, and agriculture, Reproducibility of Results, Fretting, General Medicine, Surface finish, Bone cement, Sensitivity and Specificity, Prosthesis Failure, Equipment Failure Analysis, Fretting wear, TA, Wear simulation, Cement mantle, Hip Prosthesis, Cementation

Abstract

The stem-cement interface experiences fretting wear in vivo due to low-amplitude oscillatory micromotion under physiological loading, as a consequence it is considered to play an important part in the overall wear of cemented total hip replacement. Despite its potential significance, in-vitro simulation to reproduce fretting wear has seldom been attempted and even then with only limited success. In the present study, fretting wear was successfully reproduced at the stem-cement interface through an in-vitro wear simulation, which was performed in part with reference to ISO 7206-4: 2002. The wear locations compared well with the results of retrieval studies. There was no evidence of bone cement transfer films on the stem surface and no fatigue cracks in the cement mantle. The cement surface was severely damaged in those areas in contact with the fretting zones on the stem surface, with retention of cement debris in the micropores. Furthermore, it was suggested that these micropores contributed to initiation and propagation of fretting wear. This study gave scope for further comparative study of the influence of stem geometry, stem surface finish, and bone cement brand on generation of fretting wear.

Published

2007

244. Adaptation to human populations is revealed by within-host polymorphisms in HIV-1 and hepatitis C virus

Author

Sergei L. Kosakovsky Pond, Andrew J. Leigh Brown, Phil Bennett, Simon D. W. Frost, Art F. Y. Poon, Douglas D. Richman, and Koup, Richard A

Subjects

Nonsynonymous substitution, Adaptation, Biological, Epitopes, T-Lymphocyte, HIV Infections, Hepacivirus, CD8-Positive T-Lymphocytes, Epitope, Hepatitis, Epitopes, Theoretical, Models, 2.2 Factors relating to the physical environment, Biology (General), Aetiology, Genetics, 0303 health sciences, education.field_of_study, Reverse Transcriptase Polymerase Chain Reaction, Liver Disease, Hepatitis C, 3. Good health, Fixation (population genetics), Infectious Diseases, Medical Microbiology, Viruses, HIV/AIDS, Infection, Biotechnology, Research Article, QH301-705.5, Population, Chronic Liver Disease and Cirrhosis, Immunology, Molecular Sequence Data, Biology, Microbiology, Models, Biological, Virus, Vaccine Related, 03 medical and health sciences, Hepatitis - C, Genetic, Clinical Research, Virology, Genetic variation, Humans, Adaptation, Polymorphism, education, Molecular Biology, Selection (genetic algorithm), 030304 developmental biology, Evolutionary Biology, Stochastic Processes, Polymorphism, Genetic, 030306 microbiology, Prevention, Human Genome, Genetics and Genomics, RC581-607, Models, Theoretical, Biological, CTL, Emerging Infectious Diseases, Good Health and Well Being, T-Lymphocyte, HIV-1, Parasitology, Immunization, Immunologic diseases. Allergy, Digestive Diseases

Abstract

CD8+ cytotoxic T-lymphocytes (CTLs) perform a critical role in the immune control of viral infections, including those caused by human immunodeficiency virus type 1 (HIV-1) and hepatitis C virus (HCV). As a result, genetic variation at CTL epitopes is strongly influenced by host-specific selection for either escape from the immune response, or reversion due to the replicative costs of escape mutations in the absence of CTL recognition. Under strong CTL-mediated selection, codon positions within epitopes may immediately “toggle” in response to each host, such that genetic variation in the circulating virus population is shaped by rapid adaptation to immune variation in the host population. However, this hypothesis neglects the substantial genetic variation that accumulates in virus populations within hosts. Here, we evaluate this quantity for a large number of HIV-1– (n ≥ 3,000) and HCV-infected patients (n ≥ 2,600) by screening bulk RT-PCR sequences for sequencing “mixtures” (i.e., ambiguous nucleotides), which act as site-specific markers of genetic variation within each host. We find that nonsynonymous mixtures are abundant and significantly associated with codon positions under host-specific CTL selection, which should deplete within-host variation by driving the fixation of the favored variant. Using a simple model, we demonstrate that this apparently contradictory outcome can be explained by the transmission of unfavorable variants to new hosts before they are removed by selection, which occurs more frequently when selection and transmission occur on similar time scales. Consequently, the circulating virus population is shaped by the transmission rate and the disparity in selection intensities for escape or reversion as much as it is shaped by the immune diversity of the host population, with potentially serious implications for vaccine design., Author Summary The rapid accumulation of genetic variation in human viruses, such as human immunodeficiency virus type 1 (HIV-1) and hepatitis C virus (HCV), enables these pathogens to elude the immune system and forestalls the development of effective vaccines. This variation may be shaped by selection due to host-specific immune responses, such that the total virus population mirrors the immune diversity of the host population. However, the often-neglected viral genetic variation within hosts may also play an important role in shaping variation in the total virus population. We carry out an innovative analysis of bulk HIV-1 and HCV sequences isolated from over 4,000 human patients, exploiting “mixtures” (i.e., ambiguous nucleotides) as a site-specific marker of within-host genetic variation. We find that nonsynonymous mixtures are disproportionately abundant at codon positions under strong host-specific immune selection. Because existing models of virus evolution provide no explanation for this outcome, we have formulated a new model supplemented with stochastic simulations to demonstrate that the rapid transmission of viruses through diverse selective environments creates a positive correlation between nonsynonymous variation within and among hosts.

Published

2007

245. HIV phylogenetics:Criminal convictions relying solely on this to establish transmission are unsafe

Author

Pillay, Deenan, Rambaut, Andrew, Geretti, Anna Maria, and Leigh Brown, Andrew J.

Published

2007

246. A Better Understanding of the Surface Topography at the Stem-Cement Interface

Author

Hongyu Zhang, Leigh Brown, and Liam Blunt

Subjects

musculoskeletal diseases, Cement, Materials science, business.industry, Interface (computing), technology, industry, and agriculture, Structural engineering, Surface finish, Bone cement, Durability, Finite element method, Rod, Shear strength, Composite material, business

Abstract

The long term stabilization and durability of cemented total hip replacement (THR) depends on not only the bulk properties of the components but also the interfaces through which they interact. The stem-cement interface has been consistently considered as a weak link in the stem-cement-bone system, being a transitional zone between two materials with significantly different mechanical properties. Previous research concerning this interface has been limited to investigation of interfacial shear strength through in vitro test and finite element analysis (FEA). Until now, a deep insight into the contact characteristics at this interface, especially the interaction between femoral stems with various surface finishes and bone cement, has not been established. In addition, it is still an area of debate whether a permanent fixation can be achieved by utilizing a matt femoral stem, and furthermore it is another matter of concern that a matt femoral stem would cause much more damage to the cement mantle, resulting in an acceleration of aseptic loosening of the femoral stem. This present study investigated the surface topography of stainless steel rods and Simplex P bone cement obtained from a series of pull out tests in order to gain a better understanding of the interaction at the stem-cement interface.Copyright © 2007 by ASME

Published

2007

247. Principles of Multi-Enzyme Purification by Affinity Chromatography

Author

Lee, C.-Y., primary, Leigh-Brown, A., additional, Langley, C., additional, Pegoraro, B., additional, Lopez-Barea, J., additional, and Charles, D., additional

Published

1978

248. A high HIV-1 strain variability in London, UK, revealed by full-genome analysis: Results from the ICONIC project.

Author

Yebra, Gonzalo, Frampton, Dan, Gallo Cassarino, Tiziano, Raffle, Jade, Hubb, Jonathan, Ferns, R. Bridget, Waters, Laura, Tong, C. Y. William, Kozlakidis, Zisis, Hayward, Andrew, Kellam, Paul, Pillay, Deenan, Clark, Duncan, Nastouli, Eleni, Leigh Brown, Andrew J., and null, null

Subjects

HIV, VIRAL genomes, GENETIC recombination, NUCLEOTIDE sequence

Abstract

Background & methods: The ICONIC project has developed an automated high-throughput pipeline to generate HIV nearly full-length genomes (NFLG, i.e. from gag to nef) from next-generation sequencing (NGS) data. The pipeline was applied to 420 HIV samples collected at University College London Hospitals NHS Trust and Barts Health NHS Trust (London) and sequenced using an Illumina MiSeq at the Wellcome Trust Sanger Institute (Cambridge). Consensus genomes were generated and subtyped using COMET, and unique recombinants were studied with jpHMM and SimPlot. Maximum-likelihood phylogenetic trees were constructed using RAxML to identify transmission networks using the Cluster Picker. Results: The pipeline generated sequences of at least 1Kb of length (median = 7.46Kb, IQR = 4.01Kb) for 375 out of the 420 samples (89%), with 174 (46.4%) being NFLG. A total of 365 sequences (169 of them NFLG) corresponded to unique subjects and were included in the down-stream analyses. The most frequent HIV subtypes were B (n = 149, 40.8%) and C (n = 77, 21.1%) and the circulating recombinant form CRF02_AG (n = 32, 8.8%). We found 14 different CRFs (n = 66, 18.1%) and multiple URFs (n = 32, 8.8%) that involved recombination between 12 different subtypes/CRFs. The most frequent URFs were B/CRF01_AE (4 cases) and A1/D, B/C, and B/CRF02_AG (3 cases each). Most URFs (19/26, 73%) lacked breakpoints in the PR+RT pol region, rendering them undetectable if only that was sequenced. Twelve (37.5%) of the URFs could have emerged within the UK, whereas the rest were probably imported from sub-Saharan Africa, South East Asia and South America. For 2 URFs we found highly similar pol sequences circulating in the UK. We detected 31 phylogenetic clusters using the full dataset: 25 pairs (mostly subtypes B and C), 4 triplets and 2 quadruplets. Some of these were not consistent across different genes due to inter- and intra-subtype recombination. Clusters involved 70 sequences, 19.2% of the dataset. Conclusions: The initial analysis of genome sequences detected substantial hidden variability in the London HIV epidemic. Analysing full genome sequences, as opposed to only PR+RT, identified previously undetected recombinants. It provided a more reliable description of CRFs (that would be otherwise misclassified) and transmission clusters. [ABSTRACT FROM AUTHOR]

Published

2018

249. Human Immunodeficiency Virus Type 1 Clade B Superinfection: Evidence for Differential Immune Containment of Distinct Clade B Strains

Author

Arumugam Balamurugan, Jacqueline A. Pitt, Andrew J. Leigh Brown, Otto O. Yang, Christos J. Petropoulos, Davey M. Smith, Susan J. Little, Eric S. Daar, Beth D. Jamieson, and Douglas D. Richman

Subjects

Adult, Male, Genotype, viruses, Immunology, Molecular Sequence Data, Epitopes, T-Lymphocyte, Viremia, HIV superinfection, Biology, medicine.disease_cause, Microbiology, Virus, Epitope, Immune system, Virology, Immunopathology, medicine, Humans, Amino Acid Sequence, Seroconversion, Phylogeny, AIDS Vaccines, Recombination, Genetic, Acquired Immunodeficiency Syndrome, virus diseases, medicine.disease, Phenotype, Insect Science, Superinfection, HIV-1, Pathogenesis and Immunity, T-Lymphocytes, Cytotoxic

Abstract

Sequential infection with different strains of human immunodeficiency virus type 1 (HIV-1) is a rarely identified phenomenon with important implications for immunopathogenesis and vaccine development. Here, we identify an individual whose good initial control of viremia was lost in association with reduced containment of a superinfecting strain. Subject 2030 presented with acute symptoms of HIV-1 infection with high viremia and an incomplete seroconversion as shown by Western blotting. A low set point of viremia (∼1,000 HIV-1 copies/ml) was initially established without drug therapy, but a new higher set point (∼40,000 HIV-1 copies/ml) manifested about 5 months after infection. Drug susceptibility testing demonstrated a multidrug-resistant virus initially but a fully sensitive virus after 5 months, and an analysis of pol genotypes showed that these were two phylogenetically distinct strains of virus (strains A and B). Replication capacity assays suggested that the outgrowth of strain B was not due to higher fitness conferred by pol , and env sequences indicated that the two strains had the same R5 coreceptor phenotype. Delineation of CD8 + -T-lymphocyte responses against HIV-1 showed a striking pattern of decay of the initial cellular immune responses after superinfection, followed by some adaptation of targeting to new epitopes. An examination of targeted sequences suggested that differences in the recognized epitopes contributed to the poor immune containment of strain B. In conclusion, the rapid overgrowth of a superinfecting strain of HIV-1 of the same subtype raises major concerns for effective vaccine development.

Published

2005

250. 974 SEROPREVALENCE OF HEPATITIS E IN THE SOUTH PACIFIC ISLANDS

Author

G.L.A. Harrison, Andrew J. Leigh Brown, P. Klenerman, J.G. Hunter, John Halliday, E Barnes, Harry R. Dalton, D. Penny, and R. Bendall

Subjects

Geography, Hepatology, medicine, Seroprevalence, Hepatitis E, medicine.disease, Demography

Published

2013