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2. Emergence and spread of a human-transmissible multidrug-resistant nontuberculous mycobacterium.

Author

Bryant, J.M., Grogono, D.M., Rodriguez-Rincon, D., Everall, I., Brown, K.P., Moreno, P., Verma, D., Hill, E., Drijkoningen, J., Gilligan, P., Esther, C.R., Noone, P.G., Giddings, O., Bell, S.C., Thomson, R., Wainwright, C.E., Coulter, C., Pandey, S., Wood, M.E., Stockwell, R.E., Ramsay, K.A., Sherrard, L.J., Kidd, T.J., Jabbour, N., Johnson, G.R., Knibbs, L.D., Morawska, L., Sly, P.D., Jones, A., Bilton, D., Laurenson, I., Ruddy, M., Bourke, S., Bowler, I.C., Chapman, S.J., Clayton, A., Cullen, M., Dempsey, O., Denton, M., Desai, M., Drew, R.J., Edenborough, F., Evans, J., Folb, J., Daniels, T., Humphrey, H., Isalska, B., Jensen-Fangel, S., Jönsson, B., Jones, A.M., Katzenstein, T.L., Lillebaek, T., MacGregor, G., Mayell, S., Millar, M., Modha, D., Nash, E.F., O'Brien, C., O'Brien, D., Ohri, C., Pao, C.S., Peckham, D., Perrin, F., Perry, A., Pressler, T., Prtak, L., Qvist, T., Robb, A., Rodgers, H., Schaffer, K., Shafi, N., Ingen, J. van, Walshaw, M., Watson, D., West, N., Whitehouse, J., Haworth, C.S., Harris, S.R., Ordway, D., Parkhill, J., Floto, R.A., Bryant, J.M., Grogono, D.M., Rodriguez-Rincon, D., Everall, I., Brown, K.P., Moreno, P., Verma, D., Hill, E., Drijkoningen, J., Gilligan, P., Esther, C.R., Noone, P.G., Giddings, O., Bell, S.C., Thomson, R., Wainwright, C.E., Coulter, C., Pandey, S., Wood, M.E., Stockwell, R.E., Ramsay, K.A., Sherrard, L.J., Kidd, T.J., Jabbour, N., Johnson, G.R., Knibbs, L.D., Morawska, L., Sly, P.D., Jones, A., Bilton, D., Laurenson, I., Ruddy, M., Bourke, S., Bowler, I.C., Chapman, S.J., Clayton, A., Cullen, M., Dempsey, O., Denton, M., Desai, M., Drew, R.J., Edenborough, F., Evans, J., Folb, J., Daniels, T., Humphrey, H., Isalska, B., Jensen-Fangel, S., Jönsson, B., Jones, A.M., Katzenstein, T.L., Lillebaek, T., MacGregor, G., Mayell, S., Millar, M., Modha, D., Nash, E.F., O'Brien, C., O'Brien, D., Ohri, C., Pao, C.S., Peckham, D., Perrin, F., Perry, A., Pressler, T., Prtak, L., Qvist, T., Robb, A., Rodgers, H., Schaffer, K., Shafi, N., Ingen, J. van, Walshaw, M., Watson, D., West, N., Whitehouse, J., Haworth, C.S., Harris, S.R., Ordway, D., Parkhill, J., and Floto, R.A.

Abstract

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Published
2016

5. Act now against new NHS competition regulations

Author

Davis, J., primary, Banks, I., additional, Wrigley, D., additional, Peedell, C., additional, Pollock, A., additional, McPherson, K., additional, McKee, M., additional, Irving, W. L., additional, Crome, P., additional, Greenhalgh, T., additional, Holland, W., additional, Evans, D., additional, Maryon-Davis, A., additional, Smyth, A., additional, Fleming, P., additional, Coleman, M., additional, Sharp, D. J., additional, Whincup, P., additional, Logan, S., additional, Cook, D., additional, Moore, R., additional, Rawaf, S., additional, McEewen, J., additional, West, R., additional, Yudkin, J. S., additional, Clarke, A., additional, Finer, N., additional, Domizio, P., additional, Bambra, C., additional, Jones, A., additional, Feder, G., additional, Scott-Samuel, A., additional, Irvine, L., additional, Sharma, A., additional, Fitchett, M., additional, Boomla, K., additional, Folb, J., additional, Paul, A., additional, McCoy, D., additional, Tallis, R., additional, Burgess-Allen, J., additional, Edwards, M., additional, Tomlinson, J., additional, Colvin, D., additional, Gore, J., additional, Brown, K., additional, Mitchel, S., additional, Lau, A., additional, Sayer, M., additional, Clark, L., additional, Silverman, R., additional, Marmot, S., additional, Rainbow, D., additional, Carter, L., additional, Mann, N., additional, Fielding, R., additional, Logan, J., additional, Tebboth, L., additional, Arnold, N., additional, Stobbart, K., additional, Cabot, K., additional, Finer, S., additional, Davies, D., additional, Buttivant, H., additional, Kraemer, S., additional, Newell, J., additional, Griffiths, A., additional, FitzGerald, R., additional, MacGibbon, R., additional, Lee, A., additional, Macklon, A. F., additional, Hobson, E., additional, Jenner, D., additional, Jacobson, B., additional, Timmis, A., additional, Salim, A., additional, Evans-Jones, J., additional, Caan, W., additional, Awsare, N., additional, Pride, N., additional, Suckling, R., additional, Bratty, C., additional, Rossiter, B., additional, Hawkins, D., additional, Currie, J., additional, Camilleri-Ferrante, C., additional, Fluxman, J., additional, Bhatti, O., additional, Anson, J., additional, Etherington, R., additional, Lawrence, D., additional, Fell, H., additional, Clarke, E., additional, Ormerod, J., additional, Ormerod, O., additional, Ireland, M., additional, Duncan, J. A. T., additional, Chandy, R., additional, Mindell, J., additional, Mullen, P., additional, Bennett-Richards, P., additional, Hirst, J., additional, Murphy, E., additional, Martin, P., additional, Lowes, S., additional, Grunewald, R., additional, Reeve, J., additional, Schweiger, M., additional, Coates, J., additional, Farrelly, G., additional, Chamberlain, M. A., additional, Lewis, G., additional, Young, J., additional, Scott, B., additional, Gibbs, J., additional, Landers, A., additional, Deveson, P., additional, Ingrams, G., additional, Leigh, M., additional, Gawler, J., additional, Ford, A., additional, Nixon, J., additional, McCartney, M., additional, Bareford, D., additional, Singh, S., additional, Lockwood, K., additional, Cripwell, M., additional, Ehrhardt, P., additional, Bell, D., additional, Wortley, P., additional, Tomlinson, L., additional, Hotchkiss, J., additional, Ford, S., additional, Turner, G., additional, Reissman, G., additional, Lewis, D., additional, Johnstone, C., additional, Tomson, M., additional, Torabi, P., additional, Tomson, D., additional, Tulloch, A., additional, Johnston, S., additional, Dickinson, J., additional, McElderry, E., additional, Ross, W., additional, Holt, K., additional, Logan, M., additional, Klonin, H., additional, Danby, J., additional, Goodger, V., additional, Puntis, J., additional, Dickson, H., additional, Gould, D. A., additional, Livingstone, A., additional, Lefevre, D., additional, Kendall, B., additional, Singh, G., additional, Hall, P., additional, Darling, J., additional, Hamlyn, A. N., additional, Patel, A., additional, Erskine, J., additional, Fisher, B., additional, Hughes, R., additional, Highton, C., additional, Venning, H., additional, Singer, R., additional, Brearey, S., additional, Sikorski, J., additional, Paintin, D., additional, Feehally, J., additional, Savage, W., additional, Freud, K. M., additional, Holt, V. J., additional, Gill, A., additional, Waterston, T., additional, Souza, R. d., additional, Hopkinson, N., additional, Beadsworth, M., additional, Franks, A., additional, Daley, H., additional, Cullinan, P., additional, Basarab, A., additional, Gurling, H., additional, Zinkin, P., additional, Kirwin, S., additional, Buhrs, E., additional, Brown, R., additional, West, A., additional, Marlowe, G., additional, Fellows, G., additional, Main, J., additional, Applebee, J., additional, Koperski, M., additional, Jones, P., additional, Macfarlane, A., additional, Beer, N., additional, Mason, R., additional, Eisner, M., additional, Smailes, A., additional, Timms, P., additional, Knight, D., additional, Jones, C., additional, Wesby, B., additional, Lyttelton, L., additional, Morrison, R., additional, Bossano, D., additional, Walker, J., additional, Davies, G., additional, Godfrey, P., additional, Wolfe, I., additional, Nsutebu, E., additional, Stevenson, N., additional, Cheeroth, S., additional, Miller, J., additional, Johnson, G., additional, Noor, R., additional, Hall, A., additional, Bostock, D., additional, Michael, B., additional, Sharvill, J., additional, Macpherson, J., additional, Ma, R., additional, Middleton,, J., additional, Jeffreys, A., additional, Cole, J., additional, Boswell, J. P., additional, Bury, B., additional, Mitchison, S., additional, Kinmonth, A.-L., additional, Young, G., additional, Maclennan, I., additional, and Munday, P., additional

Published
2013
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8. Emergence and spread of a human-transmissible multidrug-resistant nontuberculous mycobacterium

Author

Bryant, JM, Grogono, DM, Rodriguez-Rincon, D, Everall, I, Brown, KP, Moreno, P, Verma, D, Hill, E, Drijkoningen, J, Gilligan, P, Esther, CR, Noone, PG, Giddings, O, Bell, SC, Thomson, R, Wainwright, CE, Coulter, C, Pandey, S, Wood, ME, Stockwell, RE, Ramsay, KA, Sherrard, LJ, Kidd, TJ, Jabbour, N, Johnson, GR, Knibbs, LD, Morawska, L, Sly, PD, Jones, A, Bilton, D, Laurenson, I, Ruddy, M, Bourke, S, Bowler, ICJW, Chapman, SJ, Clayton, A, Cullen, M, Dempsey, O, Denton, M, Desai, M, Drew, RJ, Edenborough, F, Evans, J, Folb, J, Daniels, T, Humphrey, H, Isalska, B, Jensen-Fangel, S, Jönsson, B, Jones, AM, Katzenstein, TL, Lillebaek, T, MacGregor, G, Mayell, S, Millar, M, Modha, D, Nash, EF, O'Brien, C, O'Brien, D, Ohri, C, Pao, CS, Peckham, D, Perrin, F, Perry, A, Pressler, T, Prtak, L, Qvist, T, Robb, A, Rodgers, H, Schaffer, K, Shafi, N, Van Ingen, J, Walshaw, M, Watson, D, West, N, Whitehouse, J, Haworth, CS, Harris, Ordway, D, Parkhill, J, and Floto, RA

Subjects
Cystic Fibrosis, Incidence, Mycobacterium Infections, Nontuberculous, Nontuberculous Mycobacteria, Genomics, Mice, SCID, Sequence Analysis, DNA, bacterial infections and mycoses, Communicable Diseases, Emerging, Polymorphism, Single Nucleotide, 3. Good health, Mice, Drug Resistance, Multiple, Bacterial, Pneumonia, Bacterial, bacteria, Animals, Humans, Lung, Genome, Bacterial, Phylogeny
Abstract

Lung infections with $\textit{Mycobacterium abscessus}$, a species of multidrug-resistant nontuberculous mycobacteria, are emerging as an important global threat to individuals with cystic fibrosis (CF), in whom $\textit{M. abscessus}$ accelerates inflammatory lung damage, leading to increased morbidity and mortality. Previously, $\textit{M. abscessus}$ was thought to be independently acquired by susceptible individuals from the environment. However, using whole-genome analysis of a global collection of clinical isolates, we show that the majority of $\textit{M. abscessus}$ infections are acquired through transmission, potentially via fomites and aerosols, of recently emerged dominant circulating clones that have spread globally. We demonstrate that these clones are associated with worse clinical outcomes, show increased virulence in cell-based and mouse infection models, and thus represent an urgent international infection challenge.

9. The role of antibiotics in the surgical management of paediatric obstructive sleep apnoea (OSA): a cohort study.

Author

Pandey G, Harris-Folb J, Murkin C, Sutton L, Flynn WP, Orban N, and Bajaj Y

Subjects
Adenoidectomy, Anti-Bacterial Agents therapeutic use, Child, Cohort Studies, Humans, Quality of Life, Retrospective Studies, Sleep Apnea, Obstructive surgery, Tonsillectomy
Abstract

Purpose: Obstructive sleep apnoea (OSA) describes an irregular night-time breathing pattern that is present in approximately 1.8% of children and can have a negative impact on quality of life. The use of antibiotics postoperatively is controversial. They are commonly prescribed; however, they can also be associated with side effects and resistance. This study explores the role of antibiotics in the post-operative management of children with OSA in a cohort of children., Methods: We conducted a retrospective cohort study of children undergoing surgery for OSA or sleep disordered breathing (SDB) at a tertiary paediatric ENT referral centre from November 2018 to November 2019., Results: This study identified 382 children who had undergone surgical treatment for OSA or sleep disordered breathing (SDB); 319 underwent adenotonsillectomy, 53 adenoidectomy and 10 tonsillectomies. Antibiotics were given post-operatively to 158 (41%) patients and 18 (11%) of these patients presented to hospital with post-operative complications. A higher number of patients re-presented to hospital from the group who did not receive antibiotics (p = 0.982). Bleeding (p = 0.886) and infection (p = 0.823) were also more common in those children who did not receive antibiotics., Conclusion: Antibiotics led to fewer complications and re-presentations to hospital in children undergoing operative management of OSA; however, this trend was not found to be statistically significant., (© 2021. Crown.)

Published
2021
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10. A prospective surveillance study to determine the prevalence of 16S rRNA methyltransferase-producing Gram-negative bacteria in the UK.

Author

Taylor E, Bal AM, Balakrishnan I, Brown NM, Burns P, Clark M, Diggle M, Donaldson H, Eltringham I, Folb J, Gadsby N, Macleod M, Ratnaraja NVDV, Williams C, Wootton M, Sriskandan S, Woodford N, and Hopkins KL

Subjects
Anti-Bacterial Agents pharmacology, Bacterial Proteins genetics, Humans, Male, Methyltransferases genetics, Microbial Sensitivity Tests, Prevalence, Prospective Studies, RNA, Ribosomal, 16S genetics, United Kingdom epidemiology, beta-Lactamases genetics, Drug Resistance, Bacterial, Gram-Negative Bacteria genetics
Abstract

Objectives: To determine the prevalence of 16S rRNA methyltransferase- (16S RMTase-) producing Gram-negative bacteria in patients in the UK and to identify potential risk factors for their acquisition., Methods: A 6 month prospective surveillance study was conducted from 1 May to 31 October 2016, wherein 14 hospital laboratories submitted Acinetobacter baumannii, Enterobacterales and Pseudomonas aeruginosa isolates that displayed high-level amikacin resistance according to their testing methods, e.g. no zone of inhibition with amikacin discs. Isolates were linked to patient travel history, medical care abroad, and previous antibiotic exposure using a surveillance questionnaire. In the reference laboratory, isolates confirmed to grow on Mueller-Hinton agar supplemented with 256 mg/L amikacin were screened by PCR for 16S RMTase genes armA, rmtA-rmtH and npmA, and carbapenemase genes (blaKPC, blaNDM, blaOXA-48-like and blaVIM). STs and total antibiotic resistance gene complement were determined via WGS. Prevalence was determined using denominators for each bacterial species provided by participating hospital laboratories., Results: Eighty-four isolates (44.7%), among 188 submitted isolates, exhibited high-level amikacin resistance (MIC >256 mg/L), and 79 (94.0%) of these harboured 16S RMTase genes. armA (54.4%, 43/79) was the most common, followed by rmtB (17.7%, 14/79), rmtF (13.9%, 11/79), rmtC (12.7%, 10/79) and armA + rmtF (1.3%, 1/79). The overall period prevalence of 16S RMTase-producing Gram-negative bacteria was 0.1% (79/71 063). Potential risk factors identified through multivariate statistical analysis included being male and polymyxin use., Conclusions: The UK prevalence of 16S RMTase-producing Gram-negative bacteria is low, but continued surveillance is needed to monitor their spread and inform intervention strategies., (© Crown copyright 2021.)

Published
2021
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11. Oral versus intravenous antibiotics for bone and joint infections: the OVIVA non-inferiority RCT.

Author

Scarborough M, Li HK, Rombach I, Zambellas R, Walker AS, McNally M, Atkins B, Kümin M, Lipsky BA, Hughes H, Bose D, Warren S, Mack D, Folb J, Moore E, Jenkins N, Hopkins S, Seaton RA, Hemsley C, Sandoe J, Aggarwal I, Ellis S, Sutherland R, Geue C, McMeekin N, Scarborough C, Paul J, Cooke G, Bostock J, Khatamzas E, Wong N, Brent A, Lomas J, Matthews P, Wangrangsimakul T, Gundle R, Rogers M, Taylor A, Thwaites GE, and Bejon P

Subjects
Administration, Intravenous, Administration, Oral, Adult, Anti-Bacterial Agents adverse effects, Bacterial Infections microbiology, Bone Diseases, Infectious microbiology, Clinical Protocols, Cost-Benefit Analysis economics, Female, Humans, Joint Diseases microbiology, Male, Middle Aged, Quality-Adjusted Life Years, Technology Assessment, Biomedical, Treatment Outcome, United Kingdom, Anti-Bacterial Agents administration & dosage, Bacterial Infections drug therapy, Bone Diseases, Infectious drug therapy, Drug Administration Schedule, Joint Diseases drug therapy
Abstract

Background: Management of bone and joint infection commonly includes 4-6 weeks of intravenous (IV) antibiotics, but there is little evidence to suggest that oral (PO) therapy results in worse outcomes., Objective: To determine whether or not PO antibiotics are non-inferior to IV antibiotics in treating bone and joint infection., Design: Parallel-group, randomised (1 : 1), open-label, non-inferiority trial. The non-inferiority margin was 7.5%., Setting: Twenty-six NHS hospitals., Participants: Adults with a clinical diagnosis of bone, joint or orthopaedic metalware-associated infection who would ordinarily receive at least 6 weeks of antibiotics, and who had received ≤ 7 days of IV therapy from definitive surgery (or start of planned curative treatment in patients managed non-operatively)., Interventions: Participants were centrally computer-randomised to PO or IV antibiotics to complete the first 6 weeks of therapy. Follow-on PO therapy was permitted in either arm., Main Outcome Measure: The primary outcome was the proportion of participants experiencing treatment failure within 1 year. An associated cost-effectiveness evaluation assessed health resource use and quality-of-life data., Results: Out of 1054 participants (527 in each arm), end-point data were available for 1015 (96.30%) participants. Treatment failure was identified in 141 out of 1015 (13.89%) participants: 74 out of 506 (14.62%) and 67 out of 509 (13.16%) of those participants randomised to IV and PO therapy, respectively. In the intention-to-treat analysis, using multiple imputation to include all participants, the imputed risk difference between PO and IV therapy for definitive treatment failure was -1.38% (90% confidence interval -4.94% to 2.19%), thus meeting the non-inferiority criterion. A complete-case analysis, a per-protocol analysis and sensitivity analyses for missing data each confirmed this result. With the exception of IV catheter complications [49/523 (9.37%) in the IV arm vs. 5/523 (0.96%) in the PO arm)], there was no significant difference between the two arms in the incidence of serious adverse events. PO therapy was highly cost-effective, yielding a saving of £2740 per patient without any significant difference in quality-adjusted life-years between the two arms of the trial., Limitations: The OVIVA (Oral Versus IntraVenous Antibiotics) trial was an open-label trial, but bias was limited by assessing all potential end points by a blinded adjudication committee. The population was heterogenous, which facilitated generalisability but limited the statistical power of subgroup analyses. Participants were only followed up for 1 year so differences in late recurrence cannot be excluded., Conclusions: PO antibiotic therapy is non-inferior to IV therapy when used during the first 6 weeks in the treatment for bone and joint infection, as assessed by definitive treatment failure within 1 year of randomisation. These findings challenge the current standard of care and provide an opportunity to realise significant benefits for patients, antimicrobial stewardship and the health economy., Future Work: Further work is required to define the optimal total duration of therapy for bone and joint infection in the context of specific surgical interventions. Currently, wide variation in clinical practice suggests significant redundancy that likely contributes to the excess and unnecessary use of antibiotics., Trial Registration: Current Controlled Trials ISRCTN91566927., Funding: This project was funded by the National Institute for Health Research (NIHR) Health Technology Assessment programme and will be published in full in Health Technology Assessment ; Vol. 23, No. 38. See the NIHR Journals Library website for further project information., Competing Interests: Adrian Taylor reports personal fees from Zimmer Inc., Corin Group and DePuy Synthes Companies outside the submitted work. Martin McNally reports personal fees from Bonesupport AB outside the submitted work. R Andrew Seaton reports personal fees from previous consultancy and funding for speaking at educational meetings (Novartis Pharma) and consultancy for Merck Sharp & Dohme Corp. (MSD) outside the submitted work. Harriet Hughes reports other competing interests from Gilead Sciences Inc., MSD, Biocomposites, and personal fees from Biocomposites and Cubist Pharmaceuticals outside the submitted work. Jennifer Bostock was a member of the Health Services and Delivery Research Commissioned Panel Members during this project.

Published
2019
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12. Oral versus Intravenous Antibiotics for Bone and Joint Infection.

Author

Li HK, Rombach I, Zambellas R, Walker AS, McNally MA, Atkins BL, Lipsky BA, Hughes HC, Bose D, Kümin M, Scarborough C, Matthews PC, Brent AJ, Lomas J, Gundle R, Rogers M, Taylor A, Angus B, Byren I, Berendt AR, Warren S, Fitzgerald FE, Mack DJF, Hopkins S, Folb J, Reynolds HE, Moore E, Marshall J, Jenkins N, Moran CE, Woodhouse AF, Stafford S, Seaton RA, Vallance C, Hemsley CJ, Bisnauthsing K, Sandoe JAT, Aggarwal I, Ellis SC, Bunn DJ, Sutherland RK, Barlow G, Cooper C, Geue C, McMeekin N, Briggs AH, Sendi P, Khatamzas E, Wangrangsimakul T, Wong THN, Barrett LK, Alvand A, Old CF, Bostock J, Paul J, Cooke G, Thwaites GE, Bejon P, and Scarborough M

Subjects
Administration, Intravenous, Adolescent, Adult, Aged, Aged, 80 and over, Anti-Bacterial Agents adverse effects, Anti-Bacterial Agents pharmacokinetics, Female, Humans, Intention to Treat Analysis, Male, Medication Adherence, Middle Aged, Treatment Outcome, Young Adult, Administration, Oral, Anti-Bacterial Agents administration & dosage, Bone Diseases, Infectious drug therapy, Joint Diseases drug therapy
Abstract

Background: The management of complex orthopedic infections usually includes a prolonged course of intravenous antibiotic agents. We investigated whether oral antibiotic therapy is noninferior to intravenous antibiotic therapy for this indication., Methods: We enrolled adults who were being treated for bone or joint infection at 26 U.K. centers. Within 7 days after surgery (or, if the infection was being managed without surgery, within 7 days after the start of antibiotic treatment), participants were randomly assigned to receive either intravenous or oral antibiotics to complete the first 6 weeks of therapy. Follow-on oral antibiotics were permitted in both groups. The primary end point was definitive treatment failure within 1 year after randomization. In the analysis of the risk of the primary end point, the noninferiority margin was 7.5 percentage points., Results: Among the 1054 participants (527 in each group), end-point data were available for 1015 (96.3%). Treatment failure occurred in 74 of 506 participants (14.6%) in the intravenous group and 67 of 509 participants (13.2%) in the oral group. Missing end-point data (39 participants, 3.7%) were imputed. The intention-to-treat analysis showed a difference in the risk of definitive treatment failure (oral group vs. intravenous group) of -1.4 percentage points (90% confidence interval [CI], -4.9 to 2.2; 95% CI, -5.6 to 2.9), indicating noninferiority. Complete-case, per-protocol, and sensitivity analyses supported this result. The between-group difference in the incidence of serious adverse events was not significant (146 of 527 participants [27.7%] in the intravenous group and 138 of 527 [26.2%] in the oral group; P=0.58). Catheter complications, analyzed as a secondary end point, were more common in the intravenous group (9.4% vs. 1.0%)., Conclusions: Oral antibiotic therapy was noninferior to intravenous antibiotic therapy when used during the first 6 weeks for complex orthopedic infection, as assessed by treatment failure at 1 year. (Funded by the National Institute for Health Research; OVIVA Current Controlled Trials number, ISRCTN91566927 .).

Published
2019
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13. Emergence and spread of a human-transmissible multidrug-resistant nontuberculous mycobacterium.

Author

Bryant JM, Grogono DM, Rodriguez-Rincon D, Everall I, Brown KP, Moreno P, Verma D, Hill E, Drijkoningen J, Gilligan P, Esther CR, Noone PG, Giddings O, Bell SC, Thomson R, Wainwright CE, Coulter C, Pandey S, Wood ME, Stockwell RE, Ramsay KA, Sherrard LJ, Kidd TJ, Jabbour N, Johnson GR, Knibbs LD, Morawska L, Sly PD, Jones A, Bilton D, Laurenson I, Ruddy M, Bourke S, Bowler IC, Chapman SJ, Clayton A, Cullen M, Daniels T, Dempsey O, Denton M, Desai M, Drew RJ, Edenborough F, Evans J, Folb J, Humphrey H, Isalska B, Jensen-Fangel S, Jönsson B, Jones AM, Katzenstein TL, Lillebaek T, MacGregor G, Mayell S, Millar M, Modha D, Nash EF, O'Brien C, O'Brien D, Ohri C, Pao CS, Peckham D, Perrin F, Perry A, Pressler T, Prtak L, Qvist T, Robb A, Rodgers H, Schaffer K, Shafi N, van Ingen J, Walshaw M, Watson D, West N, Whitehouse J, Haworth CS, Harris SR, Ordway D, Parkhill J, and Floto RA

Subjects
Animals, Communicable Diseases, Emerging epidemiology, Communicable Diseases, Emerging pathology, Communicable Diseases, Emerging transmission, Cystic Fibrosis epidemiology, Cystic Fibrosis pathology, Genome, Bacterial, Genomics, Humans, Incidence, Lung microbiology, Lung pathology, Mice, Mice, SCID, Mycobacterium Infections, Nontuberculous epidemiology, Mycobacterium Infections, Nontuberculous pathology, Mycobacterium Infections, Nontuberculous transmission, Nontuberculous Mycobacteria genetics, Nontuberculous Mycobacteria isolation & purification, Phylogeny, Pneumonia, Bacterial epidemiology, Pneumonia, Bacterial microbiology, Pneumonia, Bacterial pathology, Pneumonia, Bacterial transmission, Polymorphism, Single Nucleotide, Sequence Analysis, DNA, Communicable Diseases, Emerging microbiology, Cystic Fibrosis microbiology, Drug Resistance, Multiple, Bacterial, Mycobacterium Infections, Nontuberculous microbiology, Nontuberculous Mycobacteria classification
Abstract

Lung infections with Mycobacterium abscessus, a species of multidrug-resistant nontuberculous mycobacteria, are emerging as an important global threat to individuals with cystic fibrosis (CF), in whom M. abscessus accelerates inflammatory lung damage, leading to increased morbidity and mortality. Previously, M. abscessus was thought to be independently acquired by susceptible individuals from the environment. However, using whole-genome analysis of a global collection of clinical isolates, we show that the majority of M. abscessus infections are acquired through transmission, potentially via fomites and aerosols, of recently emerged dominant circulating clones that have spread globally. We demonstrate that these clones are associated with worse clinical outcomes, show increased virulence in cell-based and mouse infection models, and thus represent an urgent international infection challenge., (Copyright © 2016, American Association for the Advancement of Science.)

Published
2016
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14. Brucella melitensis prosthetic joint infection in a traveller returning to the UK from Thailand: Case report and review of the literature.

Author

Lewis JM, Folb J, Kalra S, Squire SB, Taegtmeyer M, and Beeching NJ

Subjects
Adult, Aged, Animals, Brucella melitensis drug effects, Brucellosis drug therapy, Brucellosis epidemiology, Doxycycline therapeutic use, Female, Humans, Male, Middle Aged, Prosthesis-Related Infections drug therapy, Prosthesis-Related Infections microbiology, Rifampin therapeutic use, Thailand epidemiology, United Kingdom, Young Adult, Brucella melitensis isolation & purification, Brucellosis blood, Brucellosis diagnosis, Joints microbiology, Prosthesis-Related Infections diagnosis, Travel
Abstract

Background: Brucella spp. prosthetic joint infections are infrequently reported in the literature, particularly in returning travellers, and optimal treatment is unknown., Method: We describe a prosthetic joint infection (PJI) caused by Brucella melitensis in a traveller returning to the UK from Thailand, which we believe to be the first detailed report of brucellosis in a traveller returning from this area. The 23 patients with Brucella-related PJI reported in the literature are summarised, together with our case., Results: The diagnosis of Brucella-related PJI is difficult to make; only 30% of blood cultures and 75% of joint aspiration cultures were positive in the reported cases. Culture of intraoperative samples provides the best diagnostic yield. In the absence of radiological evidence of joint loosening, combination antimicrobial therapy alone may be appropriate treatment in the first instance; this was successful in 6/7 [86%] of patients, though small numbers of patients and the likelihood of reporting bias warrant caution in drawing any firm conclusions about optimal treatment. Aerosolisation of synovial fluid during joint aspiration procedures and nosocomial infection has been described., Conclusions: Brucella-related PJI should be considered in the differential of travellers returning from endemic areas with PJI, including Thailand. Personal protective equipment including fit tested filtering face piece-3 (FFP3) mask or equivalent is recommended for personnel carrying out joint aspiration when brucellosis is suspected. Travellers can reduce the risk of brucellosis by avoiding unpasteurised dairy products and animal contact (particularly on farms and abattoirs) in endemic areas and should be counselled regarding these risks as part of their pre-travel assessment., (Copyright © 2016 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published
2016
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15. Idiopathic annular submitral aneurysm associated with Takayasu's aortitis. A report of two cases.

Author

Rose AG, Folb J, Sinclair-Smith CC, and Schneider JW

Subjects
Adolescent, Child, Coronary Aneurysm complications, Female, Humans, Male, Takayasu Arteritis complications, Aorta, Abdominal pathology, Coronary Aneurysm pathology, Takayasu Arteritis pathology
Abstract

The pathologic findings in two patients with idiopathic annular submitral left ventricular aneurysms and coexistent Takayasu's aortitis are documented. The evidence of chronic persistent myocarditis in one patient and marked myocardial fibrosis in the other supports two theoretical possibilities: first, the aneurysms may have an inflammatory etiology and, second, a common inflammatory process may have accounted for both the myocardial and the aortic lesions.

Published
1995

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