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Background: Staphylococcus haemolyticus is a coagulase-negative commensal organism of both people and companion animals. It has pathogenic potential and when cultured is often meticillin- and multidrug-resistant.

Objectives: To characterise the clinical features of dogs and cats with clinical skin disease that had positive S. haemolyticus skin cultures, and to employ whole-genome sequencing (WGS) to identify resistance genes and characterise the genetic relatedness of strains.

Materials and Methods: Isolates were identified by the institutional clinical microbiology laboratory by routine aerobic culture and susceptibility from seven veterinary hospitals across the United States. Then, WGS and analysis of each isolate were performed and clinical data collected via a retrospective clinician questionnaire.

Results: S. haemolyticus was identified from superficial (seven of 12) and deep (five of 12) cutaneous infections in our study. Most animals had received antimicrobials (10 of 12) and/or immunomodulatory drugs (nine of 12) within the six months before culture. WGS analysis revealed a variety of genetic lineages and a wide array of antimicrobial resistance genes. Meticillin resistance was identified in nine of 12 isolates and four of 12 isolates demonstrated mupirocin tolerance.

Conclusions and Clinical Relevance: Staphylococcus haemolyticus may be an under-recognised pathogen in companion animals, and its demonstrated potential for multidrug-resistance, meticillin-resistance, and high-level mupirocin tolerance may create a therapeutic challenge. Further studies should evaluate the prior antimicrobial use and immunocompromised status as risk factors for infection with S. haemolyticus.

Titel:	Genomic and clinical case characterisation of Staphylococcus haemolyticus isolated from dogs and cats in the United States, including strains with high-level mupirocin tolerance.
Autor/in / Beteiligte Person:	Citron, LE ; Cain, CL ; Dietrich, J ; Cole, SD
Link:	Full Text Finder (Volltext)
Zeitschrift:	Veterinary dermatology, Jg. 34 (2023-08-01), Heft 4, S. 298-309
Veröffentlichung:	<1997->: Oxford, U.K. : Blackwell Science ; <i>Original Publication</i>: [England?] : Oxford, U.K. ; New York, U.S.A. : European Society of Veterinary Dermatology ; [Distributed by] Pergamon Press, 1989-, 2023
Medientyp:	academicJournal
ISSN:	1365-3164 (electronic)
DOI:	10.1111/vde.13154
Schlagwort:	Cats Dogs Animals United States epidemiology Mupirocin pharmacology Mupirocin therapeutic use Staphylococcus haemolyticus genetics Anti-Bacterial Agents pharmacology Anti-Bacterial Agents therapeutic use Methicillin Retrospective Studies Microbial Sensitivity Tests veterinary Genomics Cat Diseases drug therapy Cat Diseases microbiology Staphylococcal Infections drug therapy Staphylococcal Infections veterinary Staphylococcal Infections microbiology Dog Diseases drug therapy Dog Diseases microbiology
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article Language: English [Vet Dermatol] 2023 Aug; Vol. 34 (4), pp. 298-309. <i>Date of Electronic Publication: </i>2023 Mar 13. MeSH Terms: Cat Diseases* / drug therapy ; Cat Diseases* / microbiology ; Staphylococcal Infections* / drug therapy ; Staphylococcal Infections* / veterinary ; Staphylococcal Infections* / microbiology ; Dog Diseases* / drug therapy ; Dog Diseases* / microbiology ; Cats ; Dogs ; Animals ; United States / epidemiology ; Mupirocin / pharmacology ; Mupirocin / therapeutic use ; Staphylococcus haemolyticus / genetics ; Anti-Bacterial Agents / pharmacology ; Anti-Bacterial Agents / therapeutic use ; Methicillin ; Retrospective Studies ; Microbial Sensitivity Tests / veterinary ; Genomics References: Salgueiro VC, Seixas MDAL, Guimarães LC, Ferreira DC, Da Cunha DC, Nouér SA, et al. High rate of neonates colonized by methicillin-resistant Staphylococcus species in an intensive care unit. J Infect Dev Ctries. 2019;13:810-6. ; Abraham JL, Morris DO, Griffeth GC, Shofer FS, Rankin SC. Surveillance of healthy cats and cats with inflammatory skin disease for colonization of the skin by methicillin-resistant coagulase-positive staphylococci and Staphylococcus schleiferi ssp. schleiferi. Vet Dermatol. 2007;18:252-9. ; Griffeth GC, Morris DO, Abraham JL, Shofer FS, Rankin SC. Screening for skin carriage of methicillin-resistant coagulase-positive staphylococci and Staphylococcus schleiferi in dogs with healthy and inflamed skin. Vet Dermatol. 2008;19:142-9. ; Ruzauskas M, Siugzdiniene R, Klimiene I, Virgailis M, Mockeliunas R, Vaskeviciute L, et al. Prevalence of methicillin-resistant Staphylococcus haemolyticus in companion animals: a cross-sectional study. Ann Clin Microbiol Antimicrob. 2014;13:56. ; Barros EM, Ceotto H, Bastos MCF, Dos Santos KRN, Giambiagi-Demarval M. Staphylococcus haemolyticus as an important hospital pathogen and carrier of methicillin resistance genes. J Clin Microbiol. 2012;50:166-8. ; Takeuchi F, Watanabe S, Baba T, Yuzawa H, Ito T, Morimoto Y, et al. Whole-genome sequencing of Staphylococcus haemolyticus uncovers the extreme plasticity of its genome and the evolution of human-colonizing staphylococcal species. J Bacteriol. 2005;187:7292-308. ; Eltwisy HO, Abdel-Fattah M, Elsisi AM, Omar MM, Aly Abdelmoteleb A, El-Mokhtar MA. Pathogenesis of Staphylococcus haemolyticus on primary human skin fibroblast cells. Virulence. 2020;11:1142-57. ; Shittu A, Lin J, Morrison D, Kolawole D. Isolation and molecular characterization of multiresistant Staphylococcus sciuri and Staphylococcus haemolyticus associated with skin and soft-tissue infections. J Med Microbiol. 2004;53:51-5. ; Bierowiec K, Korzeniowska-Kowal A, Wzorek A, Rypuła K, Gamian A. Prevalence of Staphylococcus species colonization in healthy and sick cats. Biomed Res Int. 2019;2019:4360525. ; Tyson GH, Ceric O, Guag J, Nemser S, Borenstein S, Slavic D, et al. Genomics accurately predicts antimicrobial resistance in Staphylococcus pseudintermedius collected as part of Vet-LIRN resistance monitoring. Vet Microbiol. 2021;254:109006. ; CLSI. Performance standards for antimicrobial disk and dilution susceptibility tests for bacteria isolated from animals. 5th ed. CLSI supplement VET01S. Wayne, PA: Clinical and Laboratory Standards Institute 2020. ; Lavallée C, Rouleau D, Gaudreau C, Roger M, Tsimiklis C, Locas M-C, et al. Performance of an agar dilution method and a Vitek 2 card for detection of inducible clindamycin resistance in Staphylococcus spp. J Clin Microbiol. 2010;48:1354-7. ; Patel JB, Gorwitz RJ, Jernigan JA. Mupirocin resistance. Clin Infect Dis. 2009;49:935-41. ; Jones RN, Castanheira M, Rhomberg PR, Woosley LN, Pfaller MA. Performance of fusidic acid (CEM-102) susceptibility testing reagents: broth microdilution, disk diffusion, and Etest methods as applied to Staphylococcus aureus. J Clin Microbiol. 2010;48:972-6. ; Davis JJ, Wattam AR, Aziz RK, Brettin T, Butler R, Butler RM, et al. The PATRIC bioinformatics resource center: expanding data and analysis capabilities. Nucleic Acids Res. 2020;48:D606-12. ; Bankevich A, Nurk S, Antipov D, Gurevich AA, Dvorkin M, Kulikov AS, et al. SPAdes: a new genome assembly algorithm and its applications to single-cell sequencing. J Comput Biol. 2012;19:455-77. ; Jolley KA, Bray JE, Maiden MCJ. Open-access bacterial population genomics: BIGSdb software, the PubMLST.org website and their applications. Wellcome Open Res. 2018;3:124. ; Zankari E, Allesøe R, Joensen KG, Cavaco LM, Lund O, Aarestrup FM. PointFinder: a novel web tool for WGS-based detection of antimicrobial resistance associated with chromosomal point mutations in bacterial pathogens. J Antimicrob Chemother. 2017;72:2764-8. ; Bortolaia V, Kaas RS, Ruppe E, Roberts MC, Schwarz S, Cattoir V, et al. ResFinder 4.0 for predictions of phenotypes from genotypes. J Antimicrob Chemother. 2020;75:3491-500. ; Camacho C, Coulouris G, Avagyan V, Ma N, Papadopoulos J, Bealer K, et al. BLAST+: architecture and applications. BMC Bioinformatics. 2009;10:421. ; Carattoli A, Zankari E, Garciá-Fernández A, Larsen MV, Lund O, Villa L, et al. In Silico detection and typing of plasmids using plasmidfinder and plasmid multilocus sequence typing. Antimicrob Agents Chemother. 2014;58:3895-903. ; Price MN, Dehal PS, Arkin AP. FastTree 2 - approximately maximum-likelihood trees for large alignments. PLoS One. 2010;5:e9490. ; Katoh K, Misawa K, Kuma K-I, Miyata T. MAFFT: a novel method for rapid multiple sequence alignment based on fast Fourier transform. Nucleic Acids Res. 2002;30:3059-66. ; Page AJ, Cummins CA, Hunt M, Wong VK, Reuter S, Holden MTG, et al. Roary: rapid large-scale prokaryote pan genome analysis. Bioinformatics. 2015;31:3691-3. ; Sum S, Park HM, Oh JY. High-level mupirocin resistance in gram-positive bacteria isolated from diseased companion animals. J Vet Sci. 2020;21:e40. ; Ben-Ami R, Navon-Venezia S, Schwartz D, Schlezinger Y, Mekuzas Y, Carmeli Y. Erroneous reporting of coagulase-negative staphylococci as Kocuria spp. by the Vitek 2 system. J Clin Microbiol. 2005;43:1448-50. ; Martins KB, Ferreira AM, Mondelli AL, Rocchetti TT, Lr de S d, Cunha M d. Evaluation of MALDI-TOF VITEK®MS and VITEK® 2 system for the identification of Staphylococcus saprophyticus. Future Microbiol. 2018;13:1603-9. ; Cain CL, Morris DO, Rankin SC. Clinical characterization of Staphylococcus schleiferi infections and identification of risk factors for acquisition of oxacillin-resistant strains in dogs: 225 cases (2003-2009). J Am Vet Med Assoc. 2011;239:1566-73. ; Vincze S, Brandenburg AG, Espelage W, Stamm I, Wieler LH, Kopp PA, et al. Risk factors for MRSA infection in companion animals: results from a case-control study within Germany. Int J Med Microbiol. 2014;304:787-93. ; Misic AM, Cain CL, Morris DO, Rankin SC, Beiting DP. Divergent isoprenoid biosynthesis pathways in Staphylococcus species constitute a drug target for treating infections in companion animals. mSphere. 2016;1:e00258-16. ; Rook KA, Brown DC, Rankin SC, Morris DO. Case-control study of Staphylococcus lugdunensis infection isolates from small companion animals. Vet Dermatol. 2012;23:476-e90. ; Becker K, Heilmann C, Peters G. Coagulase-negative staphylococci. Clin Microbiol Rev. 2014;27:870-926. ; Tabe Y, Nakamura A, Oguri T, Igari J. Molecular characterization of epidemic multiresistant Staphylococcus haemolyticus isolates. Diagn Microbiol Infect Dis. 1998;32:177-83. ; High EJ, Olivry T. The prevalence of bacterial infections during cyclosporine therapy in dogs: a critically appraised topic. Can Vet J. 2020;61:1283-9. ; Cosgrove SB, Wren JA, Cleaver DM, Walsh KF, Follis SI, King VI, et al. A blinded, randomized, placebo-controlled trial of the efficacy and safety of the Janus kinase inhibitor oclacitinib (Apoquel®) in client-owned dogs with atopic dermatitis. Vet Dermatol. 2013;24:587-97. ; Cavanagh JP, Hjerde E, Holden MTG, Kahlke T, Klingenberg C, Flaegstad T, et al. Whole-genome sequencing reveals clonal expansion of multiresistant Staphylococcus haemolyticus in European hospitals. J Antimicrob Chemother. 2014;69:2920-7. ; Cavanagh JP, Klingenberg C, Hanssen A-M, Fredheim EA, Francois P, Schrenzel J, et al. Core genome conservation of Staphylococcus haemolyticus limits sequence based population structure analysis. J Microbiol Methods. 2012;89:159-66. ; Schmidt JS, Kuster SP, Nigg A, Dazio V, Brilhante M, Rohrbach H, et al. Poor infection prevention and control standards are associated with environmental contamination with carbapenemase-producing Enterobacterales and other multidrug-resistant bacteria in Swiss companion animal clinics. Antimicrob Resist Infect Control. 2020;9:93. ; Bathavatchalam YD, Solaimalai D, Amladi A, Dwarakanathan HT, Anandan S, Veeraraghavan B. Vancomycin heteroresistance in Staphylococcus haemolyticus: elusive phenotype. Futur Sci OA. 2021;7:FSO710. ; Werner AH, Russell AD. Mupirocin, fusidic acid and bacitracin: activity, action and clinical uses of three topical antibiotics. Vet Dermatol. 1999;10:225-40. ; Williamson DA, Carter GP, Howden BP. Current and emerging topical antibacterials and antiseptics: agents, action, and resistance patterns. Clin Microbiol Rev. 2017;30:827-60. ; Kizerwetter-Świda M, Chrobak-Chmiel D, Rzewuska M. High-level mupirocin resistance in methicillin-resistant staphylococci isolated from dogs and cats. BMC Vet Res. 2019;15:238. ; Rossi CC, Ferreira NC, Coelho MLV, Schuenck RP, Bastos M, do C de F, et al. Transfer of mupirocin resistance from Staphylococcus haemolyticus clinical strains to Staphylococcus aureus through conjugative and mobilizable plasmids. FEMS Microbiol Lett. 2016;363:fnw121. ; Seah C, Alexander DC, Louie L, Simor A, Low DE, Longtin J, et al. MupB, a new high-level mupirocin resistance mechanism in Staphylococcus aureus. Antimicrob Agents Chemother. 2012;56:1916-20. ; Rode H, Hanslo D, de Wet PM, Millar AJ, Cywes S. Efficacy of mupirocin in methicillin-resistant Staphylococcus aureus burn wound infection. Antimicrob Agents Chemother. 1989;33:1358-61. ; Hillier A, Lloyd DH, Weese JS, Blondeau JM, Boothe D, Breitschwerdt E, et al. Guidelines for the diagnosis and antimicrobial therapy of canine superficial bacterial folliculitis (antimicrobial guidelines working Group of the International Society for companion animal infectious diseases). Vet Dermatol. 2014;25:163-e43. ; Yu F, Liu Y, Lu C, Lv J, Qi X, Ding Y, et al. Dissemination of fusidic acid resistance among Staphylococcus aureus clinical isolates. BMC Microbiol. 2015;15:210. ; Frosini SM, Bond R, Loeffler A, Larner J. Opportunities for topical antimicrobial therapy: permeation of canine skin by fusidic acid. BMC Vet Res. 2017;13:345. Grant Information: This study was self-funded. Contributed Indexing: Keywords: Staphylococcus haemolyticus; antimicrobial drug resistance; meticillin resistance; mupirocin ; Local Abstract: [Publisher, French] Staphylococcus haemolyticus est une bactérie à coagulase négative, commensale des humains et des animaux de compagnie. Elle possède un potentiel pathogène et, en culture, présente souvent des résistances à la méticilline et à plusieurs autres familles d’antibiotiques (bactérie multirésistante). [Publisher, French] Étudier les caractéristiques cliniques des infections cutanées à S. haemolyticus canines et féline et utiliser le séquençage du génome entier (WGS) pour identifier les gènes de résistance et caractériser la parenté génétique des souches. MATÉRIELS ET MÉTHODES: Les isolats ont été identifiés par le laboratoire institutionnel de microbiologie clinique par culture aérobie de routine et antibiogramme dans sept hôpitaux vétérinaires américains. Ensuite, le WGS et l'analyse de chaque isolat ont été effectués et les données cliniques recueillies via un questionnaire clinique rétrospectif. RÉSULTATS: Dans notre étude Staphylococcus haemolyticus a été isolé dans des prélèvements provenant d'infections cutanées superficielles (sept sur 12) et profondes (cinq sur 12). La plupart des animaux ont reçu des antimicrobiens (10 sur 12) et/ou des médicaments immunomodulateurs (neuf sur 12) dans les six mois précédant la culture. L'analyse WGS révèle une variété de lignées génétiques et un large éventail de gènes de résistance aux antimicrobiens. La résistance à la méticilline a été identifiée dans neuf des 12 isolats et quatre des 12 isolats présentent une résistance élevée à la mupirocine. [Publisher, French] Staphylococcus haemolyticus est un agent pathogène mal connu chez les animaux de compagnie, et son potentiel de multirésistance aux antibiotiques, de résistance à la méticilline et de résistance élevée à la mupirocine peut se révéler un défi thérapeutique. D'autres études devraient évaluer les facteurs de risque d'infection à S. haemolyticus tels que l’utilisation antérieure d'antimicrobiens et le statut immunodéprimé. [Publisher, Spanish; Castilian] INTRODUCCIÓN: Staphylococcus haemolyticus es un organismo comensal coagulasa negativo tanto de personas como de animales de compañía. Tiene potencial patógeno y, cuando se cultiva, a menudo es resistente a la meticilina y a múltiples fármacos. OBJETIVOS: Caracterizar las características clínicas de perros y gatos con enfermedad clínica de la piel que tuviesen cultivos de piel positivos para S. haemolyticus y emplear la secuenciación del genoma completo (WGS) para identificar genes de resistencia y caracterizar la relación genética de las cepas. MATERIALES Y MÉTODOS: El laboratorio de microbiología clínica institucional identificó los aislamientos mediante cultivos aeróbicos de rutina y susceptibilidad de siete hospitales veterinarios en los Estados Unidos. Luego se realizó WGS y análisis de cada aislamiento y se recopilaron datos clínicos a través de un cuestionario clínico retrospectivo. RESULTADOS: Staphylococcus haemolyticus se identificó a partir de infecciones cutáneas superficiales (siete de 12) y profundas (cinco de 12) en nuestro estudio. La mayoría de los animales habían recibido antimicrobianos (10 de 12) y/o fármacos inmunomoduladores (nueve de 12) dentro de los seis meses anteriores al cultivo. El análisis WGS reveló una variedad de linajes genéticos y una amplia gama de genes de resistencia a los antimicrobianos. Se identificó resistencia a la meticilina en nueve de los 12 aislamientos y cuatro de los 12 aislamientos demostraron un alto nivel de resistencia a la mupirocina. CONCLUSIONES Y RELEVANCIA CLÍNICA: Staphylococcus haemolyticus puede ser un patógeno poco reconocido en los animales de compañía, y su potencial demostrado de resistencia a múltiples fármacos, resistencia a la meticilina y resistencia a la mupirocina de alto nivel puede crear un reto terapéutico. Estudios adicionales deberían evaluar el uso previo de antimicrobianos y un estado inmunocomprometido como factores de riesgo para la infección por S. haemolyticus. [Publisher, German] Staphylococcus haemolyticus ist ein Koagulase-negativer Kommensale sowohl vom Menschen wie auch von Haustieren. Es handelt sich dabei um einen potenziellen Krankheitserreger, der bei Bakterienkultur oft Methicillin- und Multidrug Resistenz zeigt. [Publisher, German] Eine Beschreibung der klinischen Merkmale von Hunden und Katzen mit einer klinischen Hauterkrankung, die eine positive S. haemolyticus Kultur der Haut aufwiesen. Eine Gesamt-Genom Sequenzierung (WGS) sollte eingesetzt werden, um die Resistenzgene zu identifizieren und die genetische Verwandtschaft der Stämme zu beschreiben. [Publisher, German] Die Isolate wurden in institutionellen klinischen Mikrobiologie Laboratorien durch routinemäßige aerobe Kulturen und Empfindlichkeitstests in sieben Veterinärmedizinischen Kliniken, verteilt über die gesamten Vereinigten Staaten, identifiziert. Danach wurde eine WGS und Analyse eines jeden Isolates durchgeführt und die klinischen Daten mittels retrospektiver klinischer Fragebogen gesammelt. [Publisher, German] Staphylococcus haemolyticus wurde in unserer Studie von oberflächlicher (sieben von 12) und tiefer (fünf von 12) Hautinfektionen identifiziert. Die meisten Tiere erhielten innerhalb der letzten sechs Monate vor der Kultur Antibiotika (10 von 12) und/oder immunmodulierende Medikamente (neun von 12). Die WGS-Analyse zeigte verschiedene genetische Linien und ein großes Ausmaß an antimikrobiellen Resistenzgenen. Eine Methicillin-Resistenz wurde bei neun von 12 Isolaten identifiziert und vier von 12 Isolaten zeigten ein hohes Level an Mupirocin Resistenz. [Publisher, German] Bei Staphylococcus haemolyticus könnte es sich um ein zu wenig anerkanntes Pathogen bei Haustieren handeln und sein bewiesenes Potential für eine Multidrug Resistenz, Methicillin Resistenz und ein hohes Level an Mupirocin Resistenz können eine therapeutische Herausforderung darstellen. Weitere Studien sollten die vorherige Verabreichung von Antibiotika und einen Immunkompromittierten Status als Risikofaktoren für eine Infektion mit Staphylococcus haemolyticus evaluieren. [Publisher, Japanese] 背景: Staphylococcus haemolyticusは、人およびコンパニオンアニマルの両方に存在するコアグラーゼ陰性常在菌である。この菌は病原性を持ち、培養するとメチシリン耐性や多剤耐性を示すことが多い。目的: 本研究の目的は、S. haemolyticusの皮膚培養が陽性であった臨床皮膚疾患の犬および猫の臨床的特徴を明らかにし、全ゲノム配列決定(WGS)を用いて耐性遺伝子を特定し、菌株の遺伝的近縁性を明らかにすることであった。材料と方法: 分離株は、米国内の7つの動物病院から、施設の臨床微生物学研究所がルーチン好気性培養検査および薬剤感受性試験により同定した。その後、各分離株のWGSと解析を行い、レトロスペクティブな臨床医アンケートにより臨床データを収集した。結果本研究では、表在性(12例中7例)および深在性(12例中5例)皮膚感染症からStaphylococcus haemolyticusが確認された。ほとんどの動物が培養前6カ月以内に抗菌薬(12例中10例)および/または免疫調節薬(12例中9例)を投与されていた。WGS解析により、多様な遺伝子系統および抗菌薬耐性遺伝子が検出された。12株中9株でメチシリン耐性が確認され、12株中4株で高レベルのムピロシン耐性が確認された。結論と臨床的関連性: Staphylococcus haemolyticusはコンパニオンアニマルにおいて十分に認存されていない病原体であり、多剤耐性、メチシリン耐性、高レベルのムピロシン耐性を示す可能性があることから、治療上の課題があると思われる。今後の研究では、S. haemolyticusに感染する危険因子として、抗菌薬の使用歴や免疫不全状態を評価する必要がある。. [Publisher, Chinese] 背景: 血葡萄球菌是人和伴侣动物的一种凝固酶阴性共生生物。它具有致病潜力，培养时通常对甲氧西林和多药耐药。目的: 述具有溶血性链球菌皮肤培养阳性的临床皮肤病的犬和猫的临床特征，并采用全基因组测序(WGS)来鉴定耐药基因和鉴定菌株的遗传相关性。材料和方法: 国七家兽医医院的机构临床微生物学实验室，通过常规需氧培养和敏感性鉴定分离物。然后进行WGS和每个分离物的分析，并通过回顾性临床医生问卷收集临床数据。结果: 我们的研究中，从浅表(12个中的7个)和深层(12中的5个)皮肤感染中鉴定出溶血葡萄球菌。大多数动物在培养前六个月内接受了抗菌药物(12个中的10个)和/或免疫调节药物(12中的9个)。WGS分析揭示了多种遗传谱系和广泛的抗微生物基因。12株分离株中有9株对甲氧西林耐药，其中4株表现出高水平的莫匹罗星耐药性。结论和临床相关性: 血葡萄球菌可能是伴侣动物中一种未被充分识别的病原体，其表现出的多药耐药性、甲氧西林耐药性和高水平莫匹罗星耐药性，这些可能会带来治疗挑战。进一步的研究应评估先前的抗菌药物使用情况和免疫功能低下状况，均应作为溶血性链球菌感染的危险因素。. [Publisher, Portuguese] Staphylococcus haemolyticus é um microrganismo comensal coagulase-negativo de pessoas e animais de companhia. Possui potencial patogênico, e quando cultivado, é frequentemente resistente à meticilina e multirresistente. [Publisher, Portuguese] Caracterizar as características clínicas de cães e gatos com doenças de pele com culturas de pele positivas para S. haemolyticus, e empregar o sequenciamento de genoma completo (WGS) para identificar genes de resistência e caracterizar o parentesco genético das cepas. MATERIAIS E MÉTODOS: Os isolados foram identificados pelo laboratório institucional de microbiologia clínica por cultura aeróbica de rotina e antibiograma de amostras oriundas de sete hospitais veterinários nos Estados Unidos. Posteriormente, WGS e análise de cada isolado foi realizada e os dados clínicos foram coletados por um questionário clínico retrospectivo. [Publisher, Portuguese] Staphylococcus haemolyticus foi identificado de infecções cutâneas superficiais (sete de 12) e profundas (cinco de 12) do nosso estudo. A maioria dos animais recebeu antimicrobianos (10 de 12) e/ou medicamentos imunomoduladores (nove de 12) durante os seis meses antes da cultura. Resistência à meticilina foi detectada em nove dos 12 isolados e quatro dos 12 isolados demonstraram alto nível de resistência à mupirocina. CONCLUSÕES E RELEVÂNCIA CLÍNICA: Staphylococcus haemolyticus pode ser um patógeno subdiagnosticado em animais de companhia, e o seu demonstrado potencial para desenvolver multirresistência, resistência à meticilina e alto grau de resistência à mupirocina pode criar um desafio terapêutico. Estudos futuros devem avaliar a utilização prévia de antibióticos e o status de imunocomprometimento como fatores de risco para infecção por S. haemolyticus. Substance Nomenclature: D0GX863OA5 (Mupirocin) ; 0 (Anti-Bacterial Agents) ; Q91FH1328A (Methicillin) Entry Date(s): Date Created: 20230313 Date Completed: 20230705 Latest Revision: 20230705 Update Code: 20240513

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Genomic and clinical case characterisation of Staphylococcus haemolyticus isolated from dogs and cats in the United States, including strains with high-level mupirocin tolerance.