Association between serum concentrations of vancomycin and acute kidney injury in critically ill children

Afrin, Rubina

05 1900

Résumé : Objectifs : La vancomycine est un antibiotique néphrotoxique couramment utilisé chez les enfants gravement malades. L'objectif de l’étude était de mesurer l'association entre la vancomycine sérique (Vs) et l'insuffisance rénale aiguë (IRA) chez les enfants en unité de soins intensifs pédiatriques (USIP). Méthode : Notre cohorte comprend les admissions à l’USIP entre 2017 et 2022, ayant reçu de la vancomycine pendant ≥48 heures, avec les Vs mesurées selon la norme de soins clinique. La Vs la plus élevée dans les sept jours suivant la vancomycine a été considérée comme l'exposition et catégorisée en deux groupes : ≤20 mg/L and >20 mg/L. L’issue principale était le développement de l’IRA stade 1(augmentation de créatinine >50%) et l’issue secondaire était le changement de créatinine sérique entre avant et après le début de la vancomycine (24 heures à sept jours). Nous avons utilisé des modèles de régression logistique et linéaire ajustés en fonction de l'âge, du diagnostic, du score de gravité clinique des patients, des médicaments concomitants et de la durée du séjour en USIP. Résultats : Nous avons inclus 161 admissions chez 149 patients, dont 18 (11.18 %) ont développé une IRA dans les sept jours après la vancomycine. Le rapport de cotes ajusté pour l'association entre l’IRA et un niveau de Vs de >20 mg/L était de 5.86 [95% CI : 1.70-22.65]. Conclusion : Une mesure de vancomycine sérique >20 mg/L était associé à un risque accru d’IRA et justifie une surveillance de la Vs chez les enfants gravement malade. Mots-clés : Antibiotiques néphrotoxiques, Vancomycine, Insuffisance rénale aiguë, Enfants gravement malades, Unité de soins intensifs pédiatriques. / Abstract: Objectives: Vancomycin is a nephrotoxic antibiotic commonly used in critically ill children. The objective of the study was to measure the association between serum vancomycin (Vs) and acute kidney injury (AKI) in children in the pediatric intensive care unit (PICU). Method: Our cohort included PICU admissions between 2017 and 2022, having received vancomycin for ≥48 hours, with Vs measured according to clinical care standards. The highest Vs within seven days following vancomycin administration was considered as the exposure and categorized into two groups: ≤20 mg/L and >20 mg/L. The primary outcome was the development of stage 1 AKI (creatinine increase >50%) and the secondary outcome was the change in serum creatinine between before and after the start of vancomycin (24 hours to seven days). We used logistic and linear regression models adjusted for age, diagnosis, patient clinical severity score, concomitant medications, and length of stay in the PICU. Results: We included 161 admissions of 149 patients, of whom 18 (11.18%) developed AKI within seven days after vancomycin. The adjusted odds ratio for the association between AKI and a Vs level of >20 mg/L was 5.86 [95% CI: 1.70-22.65]. Conclusion: A serum vancomycin measurement of >20 mg/L was associated with an increased risk of AKI, justifying the monitoring of Vs in critically ill children. Keywords: Nephrotoxic antibiotics, Vancomycin, Acute Kidney Injury, Critically ill children, Pediatric Intensive Care Unit.

Antibiotiques néphrotoxiques

Vancomycine

Insuffisance rénale aiguë

Enfants gravement malades

Unité de soins intensifs pédiatriques

Nephrotoxic antibiotics

Vancomycin

Acute Kidney Injury

Critically ill children

Pediatric Intensive Care Unit

Κλινικοεργαστηριακή διερεύνηση της φορείας και των λοιμώξεων από πολυανθεκτικά στελέχη σε ασθενείς της Μονάδας Εντατικής Θεραπείας και των Μονάδων Αυξημένης Φροντίδας

Παπαδημητρίου-Ολιβγέρης, Ματθαίος

11 October 2013

Σκοπός της παρούσας ερευνητικής εργασίας ήταν η επιδημιολογική επιτήρηση της φορείας και των λοιμώξεων από Klebsiella pneumoniae που παράγει καρβαπενεμάση KPC (KPC-Kp), ανθεκτικό σε βανκομυκίνη Enterococcus (VRE) και ανθεκτικό σε μεθικιλλίνη Staphylococccus aureus (MRSA) σε ασθενείς που νοσηλεύονται στις Μονάδες Εντατικής Θεραπείας (ΜΕΘ) του Πανεπιστημιακού Γενικού Νοσοκομείου Πατρών (ΜΕΘ Α) και του Νοσοκομείου «Άγιος Ανδρέας» (ΜΕΘ Β) τη χρονική περίοδο Οκτώβριος 2009 έως Φεβρουάριος 2012. H διασπορά της KPC-Kp αποτελεί το σημαντικότερο πρόβλημα στις Ελληνικές ΜΕΘ, με τα ποσοστά της να αυξάνονται στις παθολογικές και χειρουργικές κλινικές. Κατά τη διάρκεια της παρούσας μελέτης, 12.8% των ασθενών που εισήχθηκαν στη ΜΕΘ Α (52 από 405 ασθενείς) ήταν αποικισμένοι από KPC-Kp κατά την εισαγωγή τους με την προηγηθείσα νοσηλεία σε ΜΕΘ, την χρόνια αποφρακτική πνευμονοπάθεια, τη διάρκεια προηγηθείσας νοσηλείας και την προηγηθείσα χορήγηση καρβαπενέμης ή συνδυασμού β-λακτάμης/αναστολέα λακταμάσης να συμβάλλουν στον αποικισμό. Παρατηρήθηκε μία σταδιακή αύξηση των αποικισμένων ασθενών που εισάγονται στη ΜΕΘ με 3.9% (4 από 102 ασθενείς) τους πρώτους 6 μήνες σε σύγκριση με 15.8% (48 από 300 ασθενείς) τους επόμενους 16 μήνες που αντικατοπτρίζει τη σταδιακή διασπορά της KPC-Kp σε κλινικές εκτός ΜΕΘ. Από τους 226 μη αποικισμένους ασθενείς κατά την εισαγωγή στη ΜΕΘ Α, 164 (72.6%) αποικίστηκαν κατά τη διάρκεια της νοσηλείας τους με σημαντικότερους παράγοντες που επηρεάζουν τον αποικισμό να είναι η παρουσία αποικισμένων ασθενών σε διπλανές κλίνες και η νοσηλεία σε κλίνη προηγουμένως αποικισμένου ασθενή, ενώ δε βρέθηκε συσχέτιση ανάμεσα στον αποικισμό και τη θνησιμότητα. Το υψηλό ποσοστό αποικισμού σε συνδυασμό με τους προηγούμενους παράγοντες υποδεικνύει την σημασία της διασποράς της KPC-Kp από ασθενή σε ασθενή μέσω του ιατρονοσηλευτικού προσωπικού και υποδηλώνει τη σημασία πιο αυστηρής εφαρμογής της πολιτικής ελέγχου λοιμώξεων. Συνολικά 53 ασθενείς της ΜΕΘ Α ανέπτυξαν βακτηριαιμία από KPC-Kp με 43.4% θνησιμότητα. Οι σημαντικότεροι παράγοντες που επηρεάζουν τη θνησιμότητα είναι η αντοχή του στελέχους σε κολιστίνη/τιγεκυκλίνη/γενταμικίνη και η σηπτική καταπληξία, ενώ η θεραπεία με συνδυασμό τουλάχιστον δύο δραστικών αντιβιοτικών σχετίζεται με καλύτερη πρόγνωση επιβεβαιώνοντας τα αποτελέσματα προηγούμενων μελετών υπέρ της συνδυαστικής θεραπείας στην καταπολέμηση των λοιμώξεων από KPC-Kp. Η ανάπτυξη αντοχής των στελεχών KPC-Kp έναντι της κολιστίνης ή της τιγεκυκλίνης, οι οποίες αποτελούν τις τελευταίες θεραπευτικές επιλογές για το συγκεκριμένο παθογόνο, είναι ένα ανησυχητικό φαινόμενο. Συνολικά, 24.4% και 17.9% των ασθενών της ΜΕΘ Α αποικίστηκαν από στέλεχος KPC-Kp ανθεκτικό στην κολιστίνη και τιγεκυκλίνη, αντίστοιχα. Όπως αναμενόταν η λήψη των συγκεκριμένων αντιβιοτικών συνέβαλε στον αποικισμό, όμως ο σημαντικότερος παράγοντας για αποικισμό ήταν η παρουσία αποικισμένου ασθενή στις διπλανές κλίνες υποδηλώνοντας τη σημασία της διασποράς των στελεχών και όχι της de novo ανάπτυξη αντοχής. Η σύγκριση των δύο ΜΕΘ, ανέδειξε ότι μεγαλύτερο ποσοστό των ασθενών της ΜΕΘ Α αποικίζονται κατά τη διάρκεια νοσηλείας σε σχέση με τη ΜΕΘ Β (61.8% vs 34.1%) και σε συντομότερο χρονικό διάστημα (10.6 vs 19.9 ημέρες). Τα στοιχεία αυτά μπορούν να ερμηνευτούν από το υψηλότερο ποσοστό εισαγωγών αποικισμένων ασθενών (11.4% vs 1.8%), τη μικρότερη αναλογία νοσηλευτών/ασθενών καθώς και την αυξημένη κατανάλωση καρβαπενεμών στη ΜΕΘ Α. Συνολικά, 305 και 100 στελέχη K. pneumoniae που απομονώθηκαν από τη ΜΕΘ Α και Β, αντίστοιχα, ήταν θετικά για την παρουσία του γονιδίου blaKPC ενώ πέντε στελέχη της ΜΕΘ Α ήταν θετικά και για το γονίδιο blaVIM. Και στις δύο ΜΕΘ τα στελέχη ήταν ανθεκτικά σε πενικιλλίνες, στις κεφαλοσπορίνες, στην αζτρεονάμη, στην τριμεθοπρίμη-σουλφαμεθοξαζόλη (30% των στελεχών της ΜΕΘ Β ήταν ευαίσθητα), στην αμικασίνη, στην τομπραμυκίνη και στις κινολόνες. Η αντοχή στις καρβαπενέμες (67.9% vs 60%), στην κολιστίνη (35.1% vs 18%), στη γενταμικίνη (50.8% vs 24%) και στην τιγεκυκλίνη (17% vs 18%) στα στελέχη των δύο ΜΕΘ κυμαινόταν στα ίδια επίπεδα. Πενήντα επτά και 20 στελέχη της ΜΕΘ Α και Β, αντίστοιχα, ταυτοποιήθηκαν με PFGE, η οποία ανέδειξε την παρουσία δύο τύπων στη ΜΕΘ Α, με τον τύπο Α να απαρτίζεται από το 65.5% των στελεχών, ενώ στη ΜΕΘ Β όλα τα στελέχη ανήκαν στον τύπο Α. Τα ποσοστά αποικισμού από VRE στις δύο ΜΕΘ είναι χαμηλότερα σε σχέση με αυτά της KPC-Kp. Αποικισμός κατά την εισαγωγή στη ΜΕΘ παρατηρήθηκε σε 14.3% (71 από 497 ασθενείς), ενώ κατά τη διάρκεια νοσηλείας ήταν 14.4% (36 από 250 ασθενείς). Ο σημαντικότερος παράγοντας για αποικισμό από VRE κατά τη διάρκεια νοσηλείας είναι η νοσηλεία αποικισμένων ασθενών σε διπλανές κλίνες υποδεικνύοντας ότι η μη τήρηση των μέτρων υγιεινής των χεριών ίσως διαδραματίζει το σημαντικότερο ρόλο στη διασπορά του VRE. Συνολικά 107 στελέχη VRE απομονώθηκαν (100 E. faecium και 7 E. faecalis). Ογδόντα τέσσερα στελέχη έφεραν το γονίδιο vanA και ήταν ανθεκτικά στη βανκομυκίνη και στην τεϊκοπλανίνη, ενώ τα υπόλοιπα 23 έφεραν το γονίδιο vanB και χαρακτηρίζονταν από χαμηλού επιπέδου αντοχή στη βανκομυκίνη (12 στελέχη ήταν ευαίσθητα) και ευαίσθητα στην τεϊκοπλανίνη. Όλα τα στελέχη ήταν ευαίσθητα στη λινεζολίδη, στη δαπτομυκίνη και στην τιγεκυκλίνη. Η MLST αποκάλυψε ότι τα στελέχη E. faecium ανήκουν σε έξι διαφορετικούς κλώνους (STs: ST117, ST17, ST203, ST226, ST786, ST125) με το 90% των E. faecium, ανήκουν στο Κλωνικό Σύμπλεγμα 17 (Clonal Complex CC17). Τα στελέχη E. faecalis ταξινομήθηκαν σε τέσσερις κλώνους (STs: ST6, ST41, ST19, ST28). Τα ποσοστά αποικισμού από MRSA κατά την εισαγωγή και κατά τη διάρκεια νοσηλείας είναι χαμηλά (5.3% και 3.7%, αντίστοιχα) με το σημαντικότερο παράγοντα που σχετίζεται με τον αποικισμό να είναι ο εντερικός αποικισμός με vanA-θετικό στέλεχος Enterococcus. Ο έλεγχος φορείας για MRSA ανέδειξε 28 mecA-θετικά στελέχη S. aureus, με την πλειονότητα (ν=19) να είναι PVL-θετικά, να ανήκουν στον κλώνο ST80 και να είναι ανθεκτικά σε καναμυκίνη, τετρακυκλίνη και φουσιδικό, ενώ τα υπόλοιπα ταξινομήθηκαν σε τέσσερις κλώνους με MLST (6 στον ST239 και από ένα σε ST225, ST72 και ST30). Το στέλεχος που ανήκε στον ST30 ήταν tst-θετικό. Η σύγκριση των στελεχών φορείας S. aureus που απομονώθηκαν από αθενείς (ν=67) και προσωπικό (ν=23) των ΜΕΘ (Ομάδα Α) με τα στελέχη φορείας (ν=53) και βακτηριαιμιών (ν=75) μη νοσηλευόμενων σε ΜΕΘ (Ομάδα Β), ανέδειξε υψηλότερο ποσοστό MRSA (46.9% vs 31.1%) και PVL-θετικών στελεχών (39.8% vs 25.6%) στην Ομάδα Β, ενώ η Ομάδα Α χαρακτηρίζεται από υψηλότερο ποσοστό tst-θετικών στελεχών (21.1% vs 2.3%) υποδεικνύοντας τη σιωπηρή τους διασπορά στους ασθενείς και στο προσωπικό των ΜΕΘ. Προϊόν της παρούσας ερευνητικής εργασίας ήταν η ανεύρεση των παραγόντων κινδύνου για αποικισμό ή λοίμωξη από KPC-Kp, VRE και MRSA με στόχο την καθοδήγηση των μελλοντικών προσπαθειών περιορισμού της διασποράς τους στις δύο ΜΕΘ καθώς και στα ελληνικά νοσοκομεία, τα οποία στο σύνολο τους μαστίζονται από τα συγκεκριμένα παθογόνα. / The purpose of this study was to investigate the colonization and infections caused by KPC-producing Klebsiella pneumoniae (KPC-Kp), vancomycin-resistant Enterococcus (VRE) and methicillin-resistant Staphylococcus aureus in patients hospitalized in the Intensive Care Units of the University Hospital of Patras (ICU A) and the General Hospital “Saint Andrew” during October 2009 and February 2012. The dissemination of KPC-Kp constitutes the most important issue in Greek ICUs, with its percentage rising in medical and surgical wards. During the duration of this study, 12.8% of patients admitted in the ICU A (52 from 405 patients) were colonized upon admission and previous ICU stay, chronic obstructive pulmonary disease, duration of previous hospitalization and previous usage of carbapenem or combination of beta-lactamic/lactamase were found to influence colonization. A gradual increase of the percentage of colonized patients admitted at the ICU from 3.9% (4 from 102 patients) during the first 6 months to 15.8% (48 from 300 patients) the next 16 months that reflects the dissemination of KPC-Kp in non-ICU wards. Among the 226 non-colonized upon ICU A admission patients, 164 (72.6%) became colonized during their stay with the presence of colonized patients in nearby beds and the previous colonized occupant in the same bed were associated with colonization, which did not influence mortality. The high percentage of colonization in combination with the aforementioned factors indicates the importance of the dissemination of KPC-Kp among patients via the personnel and signifies the value of a strict implementation of infection control protocols. In total, 53 patients developed KPC-Kp bloodstream infection during ICU A stay with 43.4% mortality. The most important factors that influence mortality were the resistance of the strain to gentamicin/colistin/tigecycline and septic shock, while the treatment with two active antibiotics was associated with better survival confirming the results of previous studies favoring combination therapy for the treatment of KPC-Kp infection. The development of resistance against colistin or tigecycline, which are considered the last frontier in the treatment of KPC-Kp infections, is an alarming phenomenon. In total, 24.4% and 17.9% of ICU A patients became colonized by KPC-Kp resistant to colictin or tigecycline, respectively. As expected, the administration of colistin or tigecycline influenced colonization, while the most important factor favoring colonization was the presence of colonized patients in nearby patients, indicating the importance of dissemination of these strains against de novo resistance development. The comparison of the two ICUs, found a higher percentage of patients colonized during ICU A stay (61.8% vs 34.1%) and in a shorter period (10.6 vs 19.9 days). These results may be explained by the higher percentage of patients colonized upon admission (11.4% vs 1.8%), the lower nurse/patient ration and the higher carbapenem administration. In total, 305 and 100 strains of K. pneumoniae isolated from patients hospitalized in ICU A and B, respectively, were positive for the presence of blaKPC gene while five strains in ICU A were positive for the blaVIM gene also. All strains were resistant to penicillins, cephalosporins, aztreonam, trimethoprim sulfamethoxazole (30% of ICU B strains were sensitive), amikacin, tombramycin and quinolones. The resistance rates to carbapenems (67.9% vs 60%), colisitn (35.1% vs 18%), gentamicin (50.8% vs 24%) and tigecycline (17% vs 18%) among the ICUs strains were comparable. PFGE of 57 and 20 isolates from ICU A and B, respectively, revealed that ICU A strains belonged in two types, with type A comprising 65.5% of the isolates, while all ICU B isolates belonged in type A. The percentage of VRE colonization in both ICUs were lower in comparison with those of KPC-Kp. During ICU admission 14.3% (71 from 497 patients) was already colonized, while 14.4% (36 from 250 patients) became colonized during stay. The most important factor influencing colonization was the presence of colonized patients in nearby beds, indicating that non adherence with hand hygiene may play a predominate role in VRE dissemination. In total 107 VRE strains were isolated (100 E. faecium and 7 E. faecalis). Eighty four were positive for the vanA gene and resistant to vancomycin and teicoplanin, while the rest were vanB positive and were characterized by low level resistance to vancomycin (12 were in susceptibility range) and susceptible to teicoplanin. All strains were susceptible to linezolid, daptomycin and tigecycline. As MLST revealed, E. faecium strains belonged in six different Sequencing Types (ST117, ST17, ST203, ST226, ST786, ST125) with 90% among them belonging to the Clonal Complex CC17. E. faecalis strains were categorized in four STs (ST6, ST41, ST19, ST28). The proportion of colonized patients by MRSA upon admission and during ICU stay was very low (5.3% and 3.7%, respectively). The most important factor associated with colonization was enteric carriage of vanA-positive Enterococcus. Surveillance cultures revealed 28 mecA-positive S. aureus strains, with the majority (n=19) being PVL-positive, belonging to ST80 and resistant only to kanamycin, tetracycline and fucidic acid, while the remaining were categorized in four STs (6 strains in ST239 and one at ST225, ST72 and ST30). The ST30 strain was tst-positive. The comparison of colonization strains from patients (n=67) and personnel (n=23) of the ICUs (Group A) with the strains of colonization (n=53) and bloodstream infections (n=75) isolated from non-ICU patients (Group B), revealed a higher percentage of MRSA and PVL-positive strains in Group B, while Group A was characterized by higher percentage of tst-positive strains indicating their silent dissemination between ICU patients and personnel. The present study has identified the risk factors for colonization of infection by KPC-Kp, VRE and MRSA, in order to guide the future efforts towards containing their dissemination in the two ICUs, as well as, to the Greek hospitals, which in total are plagued by the aforementioned pathogens.

Λοίμωξη

Αποικισμός

614.57

Vancomycin resistant Enterococcus

Intensive Care Unit

Infections

Colonization

Surveillance cultures

KPC producing Klebsiella pneumoniae

Sensibilidade in vitro de isolados de Clostridium difficile: comparação de duas metodologias (disco-difusão e ágar-diluição) / Susceptibility in vitro of isolates of Clostridium difficile: comparison of two methodologies (disk-diffusion and agar-dilution)

Fraga, Edmir Geraldo de Siqueira

16 July 2015

Introdução: O Clostridium difficile é um bacilo Gram-positivo, anaeróbio estrito, formador de esporos, que produz toxinas que podem causar diarreia, colite pseudomembranosa, dilatação do cólon, sepse e até morte. Nos últimos anos o quadro clínico e epidemiológico das infecções por Clostridium difficile tem se modificado e as limitações das opções terapêuticas tornaram-se mais evidentes. Objetivo Primário: Comparar as metodologias de disco-difusão e ágar-diluição na detecção de sensibilidade/resistência de isolados de Clostridium difficile. Objetivos Secundários: Avaliar prospectivamente o perfil de sensibilidade/resistência de isolados clínicos hospitalares de Clostridium difficile provenientes de seis hospitais terciários da cidade de São Paulo e fornecer evidências para fundamentar o diagnóstico e o tratamento empírico das diarreias causadas por Clostridium difficile. Métodos: utilizamos os métodos de disco-difusão e ágar-diluição, de acordo com os critérios estabelecidos pelo CLSI e EUCAST. Resultados: Os coeficientes de correlação observados entre os diâmetros dos halos de inibição e Concentração Inibitória Mínima foram abaixo do esperado tornando inviável o método de disco-difusão para determinação de sensibilidade aos antimicrobianos nitazoxanida, teicoplanina e tigeciclina. Todas as 50 cepas deste estudo foram sensíveis ao metronidazol (MIC50 foi de 1 ?g/mL a MIC90 foi de 2 ug/mL). Para o método de disco-difusão, sugerimos que halos de inibição >= 33mm possam ser interpretados como sensíveis. Devido à moderada correlação, significância estatística e distribuição de halos de inibição das amostras próximos aos valores encontrados utilizando a cepa ATTC, sugere-se a utilização do método de disco-difusão para vancomicina, onde halos com diâmetro >= 22mm possam ser considerados como sensíveis pelo método. Para o moxifloxacino houve uma boa correlação entre as duas metodologias: discodifusão e de ágar-diluição (O coeficiente de Pearson foi de -0,84, e o valor de p foi menor que 0,00001), sugerindo que halos de inibição >= 18mm possam ser interpretados como sensíveis pela metodologia de disco-difusão. A nitazoxanida foi à droga que mostrou melhor atividade in vitro (MIC50 foi 0,06 ?g/mL e a MIC90 de 0,12 ug/mL). Por se mostrar uma droga com potente atividade in vitro (MIC50 e a MIC90 foi de 0,12 ug/mL), a tigeciclina poderia ser mais uma opção terapêutica em infecções por Clostridium difficile, dependendo de mais estudos para avaliar sua real eficácia clínica e segurança. Conclusão: Os resultados verificados neste estudo indicam a necessidade de mais estudos in vitro e clínicos para definir os limites de sensibilidade/resistência para a teicoplanina e a nitazoxanida, pois faltam critérios de interpretação tanto para disco-difusão quanto para ágar-diluição. Os resultados deste trabalho in vitro confirmaram a utilidade do metronidazol como uma droga eficaz no tratamento de infecção por Clostridium difficile. A nitazoxanida foi à droga que mostrou melhor atividade in vitro por método dilucional. Sugerimos a utilização do método de disco-difusão para: metronidazol, vancomicina e moxifloxacino. Os resultados desse trabalho sugerem que halos de inibição para metronidazol ( >= 33mm), moxifloxacino ( >= 18mm) e vancomicina ( >= 22mm) poderiam ser considerados como sensíveis pelo método de disco-difusão. O método de ágardiluição é um método de boa acurácia, porém trabalhoso para ser executado na rotina laboratorial / Introduction: Clostridium difficile is a Gram-positive bacillus, strictly anaerobic, spore-forming, which produces toxins that can cause diarrhea, colitis pseudomembranous, colon expansion, sepsis and even death. In recent years the clinical and epidemiological picture of infection by Clostridium difficile has been modified and limitations of therapeutic options have become more evident. Primary Objective: Comparing the methods of disk diffusion and agar dilution in the detection sensitivity/resistance isolates of Clostridium difficile. Secondary Objectives: Prospectively evaluate the profile of sensitivity/resistance of hospital clinical isolates of Clostridium difficile from six tertiary hospitals in São Paulo city and provide evidence to support the diagnosis and empirical treatment of diarrhea caused by Clostridium difficile. Methods: We use the disk diffusion method and agar dilution method, according to the established criteria by CLSI and EUCAST. Results: The observed correlation coefficients between the inhibitions diameter zone of the and Minimum Inhibitory Concentration were under expectations impeding the disk diffusion method for determining sensitivity to nitazoxanide antimicrobial, teicoplanin and tigecycline. All 50 strains of this study were sensitive to metronidazole (MIC50 was 1 Ug/ml to MIC90 was 2 ug/ml). For the method disk diffusion, we suggest that inhibition zones >= 33mm can be interpreted as sensitive. Due to the moderate correlation, statistical significance and distribution of zones of inhibition on samples of the next found values using the strain ATTC, we suggest using the disk diffusion method for vancomycin where halos diameter >= 22mm can be considered as sensitive by the method. There was a good correlation to moxifloxacin between the two methodologies: disk diffusion and agar dilution (Pearson\'s coefficient was -0.84 , and the \"p\" value was less than 0.00001), suggesting that inhibition zones >= 18mm can be interpreted as sensitive by disk diffusion method. Nitazoxanide was the drug that showed a better performance in vitro activity (MIC50 was 0.06 ?g/ml and MIC90 0.12 ug/ml). For a drug that shows potent activity in vitro (MIC50 and MIC90 was 0.12 ug/ml), the tigecycline could be a therapeutic option in infection by Clostridium difficile, depending on further studies to evaluate their real clinical efficacy and security. Conclusion: Obtained results in this study indicate the need for further studies in vitro and clinicians to define the limits of sensitivity/resistance to teicoplanin and nitazoxanide, so there is no interpretation criteria for both disk diffusion and for agar dilution. Results of this work in vitro study confirmed the utility of metronidazole as an effective drug in the treatment of infection by Clostridium difficile. Nitazoxanide was the drug that showed better performance in vitro by dilutional method. We suggest the use of disk diffusion method: metronidazole, vancomycin and moxifloxacin. This work suggest that inhibition zones for metronidazole ( >= 33mm), moxifloxacin ( >= 18mm) and vancomycin ( >= 22mm) could be considered as sensitive by disk diffusion method. The agar dilution method is a method to be accurate, but laborious to run in the laboratory routine

Bacilos gram-positivos

Clostridium difficile

Clostridium difficile

Diarreia

Diarrhea

Disk diffusion antimicrobial tests

Drug resistance, Gram-positive rods

Gastroenteropatias

Gastrointestinal diseases

Metronidazol

Metronidazole

Microbial sensitivity tests

Moxifloxacino

Nitazoxanida

Nitazoxanide

Resistência a medicamentos

Teicoplanin

Teicoplanina

Testes de sensibilidade microbiana

Tigeciclina

Tigecycline

Vancomicina

Vancomycin, Moxifloxacin

"Estudo comparativo do tratamento das artroplastias infectadas do quadril sem e com o uso do espaçador de cimento com antibiótico" / Prospective study of the treatment of chronically infected hip replacements with and without the use of an antibiotic-loaded acrylic cement spacer

Cabrita, Henrique Antonio Berwanger de Amorim

12 April 2004

Em um estudo prospectivo sobre o tratamento das artroplastias de quadril infectadas, com perdas ósseas e fístulas ativas, 25 pacientes foram tratados em dois tempos e 36 pacientes foram tratados em dois tempos com espaçador de cimento impregnado com vancomicina. O acompanhamento médio foi de dois anos e onze meses. A taxa de recidiva infecciosa foi de 29,2% nos tratados em dois tempos e de 8,8% nos tratados com espaçador. O Escore de Harris para Quadril médio passou de 19,3 para 69,0 pontos nos casos tratados em dois tempos e de 19,7 para 72,2 pontos nos pacientes tratados com espaçador. Ao final do estudo, 86,1% dos tratados com espaçador e em 33,3% dos tratados em dois tempos tinham próteses em bom funcionamento e sem infecção. O espaçador de cimento com antibiótico é o tratamento de escolha nas próteses infectadas de quadril / We report a prospective study of 61 patients with chronically deep infected hip replacements with actively discharging sinuses, treated with a two-stage revision protocol, with and without a cement spacer impregnated with vancomycin. The average follow-up was two years and eleven months. Twenty-five patients were treated without a spacer and seven had recurrence of infection. Thirty-three patients were treated with a spacer and three had recurrence of infection. The average Harris Hip score increased from 19,3 to 69,0 on the non-spacer patients and from 19,7 to 75,2 on the spacer group. At the end of the study, the success rate was 86,1% for the spacer group and 33,3% for the non-spacer group. The use of the spacer increased the results of the two-stage chronic infected hip replacements

ARTHROPLASTY REPLACEMENT HIP/methods

ARTROPLASTIA DE QUADRIL/métodos

BONE CEMENTS/therapeutic use

CIMENTO PARA OSSOS/uso terapêutico

COMPARATIVE STUDY

CONTROL GROUPS

ESTUDO COMPARATIVO

ESTUDOS PROSPECTIVOS

GRUPOS CONTROLE

PROSPECTIVE STUDIES

PROSTHESIS-RELATED INFECTIONS/surgery

VANCOMICINA/uso terapêutico

VANCOMYCIN/therapeutic use

Epidemiologia das infecções causadas por Staphylococcus aureus resistente a meticilina com perfil comunitário (CA-MRSA) em pacientes atendidos em um hospital terciário no Rio de Janeiro / Epidemology of infections due to community-acquired methicillin-resistant staphylococcus aureos (CA-MRSA) in patients hospitalized in tertiary hospital in Rio de Janeiro

Julio Cesar Delgado Correal

02 December 2011

Fundação de Amparo à Pesquisa do Estado do Rio de Janeiro / O Staphylococcus aureus resistente a meticilina (MRSA) foi inicialmente descrito como um patógeno associado a infecções relacionadas à assistência em saúde; porém, um clone de MRSA, o CA-MRSA emergiu na comunidade e está atualmente incrementando nos hospitais. O objetivo desta tese foi descrever aspectos relacionados com a epidemiologia das infecções por cepas CA-MRSA no Hospital Universitário Pedro Ernesto da Universidade do Estado do Rio de Janeiro (HUPE/UERJ), avaliando especificamente fatores de risco relacionado com as infecções por CA-MRSA. Usando informações das bases de dados do laboratório de microbiologia, da farmácia e da Comissão para Controle da Infecção Hospitalar do HUPE/UERJ foi realizado um estudo retrospectivo de infecções/colonizações por cepas de S. aureus (fevereiro 2005 a Julho 2011). Foi realizado um estudo caso e controle, utilizando como casos os pacientes com infecções por cepas CA-MRSA. Na avaliação da susceptibilidade aos antimicrobianos usados em infecções graves por MRSA (vancomicina, teicoplanina, daptomicina e linezolida), foram determinadas as concentrações inibitórias mínimas (CIM) das amostras por diferentes metodologias (testes de difusão em agar, microdiluição em caldo e E-test). Nas analises das tendências temporais da apresentação dos subtipos de MRSA, usando um critério fenotípico para classificação das cepas MRSA, foi observada uma diminuição do número de cepas de MRSA multirresistente (HA-MRSA) (p<0.05). Também foi observada uma tendência ao aumento de cepas não-multirresistentes (CA-MRSA), mas sem alcançar a significância estatística (p = 0.06) igual que os S. aureus sensíveis a meticilina (MSSA) (p = 0.48). Não houve associação entre o subtipo de MRSA e a mortalidade devida à infecção por cepas MRSA. Uma idade acima de 70 anos (OR: 2.46, IC95%: 0.99 - 6.11), a presença de pneumonia adquirida no hospital (OR: 4.94, IC95%: 1.65 -14.8), a doença pulmonar obstrutiva crônica (OR: 6.09, IC95% 1.16 31.98) e a leucemia (OR: 8.2, IC95%: 1.25 54.7) foram fatores de risco associadas à mortalidade nas infecções por cepas de S. aureus. Usando curvas de Kaplan-Meier, foi observada uma tendência ao aumento da mortalidade em infecções causadas por MSSA na primeira semana, porém sem alcançar significância estatística (p = 0.07). Não foram observadas amostras MRSA com susceptibilidade intermediaria a vancomicina, linezolida, daptomicina ou teicoplanina. A dinâmica das infecções por S. aureus no HUPE/UERJ mudou durante o período de estudo, com menor número de episódios infecciosos causados por cepas de MRSA multirresistentes. Existe uma tendência ao aumento das cepas não-multirresistentes de MRSA entanto que a taxa de infecções por MSSA permaneceu estável no período do estudo. O perfil de resistência dos estafilococos não teve associação com a mortalidade / The methicillin-resistant Staphylococcus aureus (MRSA) was described initially like a health-care associated pathogen. However, an MRSA clone called community-adquired S. aureus emerged with success in the community and now has a worring increasing frequency in hospital settings. The aim of this study was to descript issues related to the epidemiology of infections due tu CA-MRSA isolates at the Pedro Ernesto Universitary Hospital (HUPE/UERJ) in Rio de Janeiro, Brazil from february 2005 to june 2011, analyzing risk factors related to these infections. Thus, using databases of the microbiology laboratory, pharmacia department and the infection control committee of the HUPE-UERJ, was realized an restrospective study of S. aureus isolates obtained from infected/colonizated patients hospitalized from February 2005 to July 2011. To evaluate risk factors related to CA-MRSA infections was conduced a case-control study, using patients with true infections due to MRSA like cases and patients with methicillin susceptible S. aureus (MSSA) like controls. To test the antimicrobial susceptibility of the antibiotics used in MRSA severe infections (Vancomycin, teicoplanin, daptomycin and linezolid), were determinated the minimal inhibitory concentration (MIC) of MRSA isolates using differents methods (disk-difusion test, microdilution in broth and E-test strips). The trend analyses of the MRSA types, using a phenotypic criteria to classificate the MRSA isolates, found a decrease in the infections due to multi-resistant MRSA isolates (HA-MRSA) in our hospital (p<0.05). Also was observed and increase in non-multi-resistant MRSA strains (CA-MRSA), but without reach statistic significancy (p = 0.06), similar to MSSA (p = 0.48). There is not association between the MRSA phenotype and the mortality due to S. aureus infection. In the multivariate analysis, were observed that an older age than 70 years (OR: 2.46, IC95%: 0.99 - 6.11), health-care pneumonia (OR: 4.94, IC95%: 1.65 -14.8), chronic obstructive pulmonary disease (OR: 6.09, IC95% 1.16 31.98) and leucaemia (OR: 8.2, IC95%: 1.25 54.7) were risk factors associated with mortality due to S. aureus infections. The Kaplan-Meier analysis, found a trend to high mortality due to MSSA infections in the first week, but without get statistic significancy (p = 0.07). We dont found any MRSA isolated with resistance or intermediary resistance to vancomycin, linezolid, daptomycin or teicoplanin. There is good correlation between both MICs determinations, with broth microdiluiton and E-Test strips metodhology. Its were concluded that the dynamic of the S. aureus infections at the HUPE/UERJ is changing, with less number of infectious episodes due to multi-resistant MRSA isolates. Moreover, there are an increasing number of infections due to non-multi-resistant MRSA isolate. The prevalence of infections due to MSSA dont have change in the time of period study. The kind of the S. aureus phenotype dont has association with all-causes-mortality

fatores de risco

bacteremia

CA-MRSA

HA-MRSA

daptomicina

vancomicina

linezolida

teicoplanina

estafilococos áureos

infecção hospitalar

staphylococcus aureus

health-care infections

risk factors

bloodstream infection

CA-MRSA

HA-MRSA

daptomycin

vancomycin

linezolid

teicoplanin

MICROBIOLOGIA MEDICA

Sensibilidade in vitro de isolados de Clostridium difficile: comparação de duas metodologias (disco-difusão e ágar-diluição) / Susceptibility in vitro of isolates of Clostridium difficile: comparison of two methodologies (disk-diffusion and agar-dilution)

Edmir Geraldo de Siqueira Fraga

16 July 2015

Introdução: O Clostridium difficile é um bacilo Gram-positivo, anaeróbio estrito, formador de esporos, que produz toxinas que podem causar diarreia, colite pseudomembranosa, dilatação do cólon, sepse e até morte. Nos últimos anos o quadro clínico e epidemiológico das infecções por Clostridium difficile tem se modificado e as limitações das opções terapêuticas tornaram-se mais evidentes. Objetivo Primário: Comparar as metodologias de disco-difusão e ágar-diluição na detecção de sensibilidade/resistência de isolados de Clostridium difficile. Objetivos Secundários: Avaliar prospectivamente o perfil de sensibilidade/resistência de isolados clínicos hospitalares de Clostridium difficile provenientes de seis hospitais terciários da cidade de São Paulo e fornecer evidências para fundamentar o diagnóstico e o tratamento empírico das diarreias causadas por Clostridium difficile. Métodos: utilizamos os métodos de disco-difusão e ágar-diluição, de acordo com os critérios estabelecidos pelo CLSI e EUCAST. Resultados: Os coeficientes de correlação observados entre os diâmetros dos halos de inibição e Concentração Inibitória Mínima foram abaixo do esperado tornando inviável o método de disco-difusão para determinação de sensibilidade aos antimicrobianos nitazoxanida, teicoplanina e tigeciclina. Todas as 50 cepas deste estudo foram sensíveis ao metronidazol (MIC50 foi de 1 ?g/mL a MIC90 foi de 2 ug/mL). Para o método de disco-difusão, sugerimos que halos de inibição >= 33mm possam ser interpretados como sensíveis. Devido à moderada correlação, significância estatística e distribuição de halos de inibição das amostras próximos aos valores encontrados utilizando a cepa ATTC, sugere-se a utilização do método de disco-difusão para vancomicina, onde halos com diâmetro >= 22mm possam ser considerados como sensíveis pelo método. Para o moxifloxacino houve uma boa correlação entre as duas metodologias: discodifusão e de ágar-diluição (O coeficiente de Pearson foi de -0,84, e o valor de p foi menor que 0,00001), sugerindo que halos de inibição >= 18mm possam ser interpretados como sensíveis pela metodologia de disco-difusão. A nitazoxanida foi à droga que mostrou melhor atividade in vitro (MIC50 foi 0,06 ?g/mL e a MIC90 de 0,12 ug/mL). Por se mostrar uma droga com potente atividade in vitro (MIC50 e a MIC90 foi de 0,12 ug/mL), a tigeciclina poderia ser mais uma opção terapêutica em infecções por Clostridium difficile, dependendo de mais estudos para avaliar sua real eficácia clínica e segurança. Conclusão: Os resultados verificados neste estudo indicam a necessidade de mais estudos in vitro e clínicos para definir os limites de sensibilidade/resistência para a teicoplanina e a nitazoxanida, pois faltam critérios de interpretação tanto para disco-difusão quanto para ágar-diluição. Os resultados deste trabalho in vitro confirmaram a utilidade do metronidazol como uma droga eficaz no tratamento de infecção por Clostridium difficile. A nitazoxanida foi à droga que mostrou melhor atividade in vitro por método dilucional. Sugerimos a utilização do método de disco-difusão para: metronidazol, vancomicina e moxifloxacino. Os resultados desse trabalho sugerem que halos de inibição para metronidazol ( >= 33mm), moxifloxacino ( >= 18mm) e vancomicina ( >= 22mm) poderiam ser considerados como sensíveis pelo método de disco-difusão. O método de ágardiluição é um método de boa acurácia, porém trabalhoso para ser executado na rotina laboratorial / Introduction: Clostridium difficile is a Gram-positive bacillus, strictly anaerobic, spore-forming, which produces toxins that can cause diarrhea, colitis pseudomembranous, colon expansion, sepsis and even death. In recent years the clinical and epidemiological picture of infection by Clostridium difficile has been modified and limitations of therapeutic options have become more evident. Primary Objective: Comparing the methods of disk diffusion and agar dilution in the detection sensitivity/resistance isolates of Clostridium difficile. Secondary Objectives: Prospectively evaluate the profile of sensitivity/resistance of hospital clinical isolates of Clostridium difficile from six tertiary hospitals in São Paulo city and provide evidence to support the diagnosis and empirical treatment of diarrhea caused by Clostridium difficile. Methods: We use the disk diffusion method and agar dilution method, according to the established criteria by CLSI and EUCAST. Results: The observed correlation coefficients between the inhibitions diameter zone of the and Minimum Inhibitory Concentration were under expectations impeding the disk diffusion method for determining sensitivity to nitazoxanide antimicrobial, teicoplanin and tigecycline. All 50 strains of this study were sensitive to metronidazole (MIC50 was 1 Ug/ml to MIC90 was 2 ug/ml). For the method disk diffusion, we suggest that inhibition zones >= 33mm can be interpreted as sensitive. Due to the moderate correlation, statistical significance and distribution of zones of inhibition on samples of the next found values using the strain ATTC, we suggest using the disk diffusion method for vancomycin where halos diameter >= 22mm can be considered as sensitive by the method. There was a good correlation to moxifloxacin between the two methodologies: disk diffusion and agar dilution (Pearson\'s coefficient was -0.84 , and the \"p\" value was less than 0.00001), suggesting that inhibition zones >= 18mm can be interpreted as sensitive by disk diffusion method. Nitazoxanide was the drug that showed a better performance in vitro activity (MIC50 was 0.06 ?g/ml and MIC90 0.12 ug/ml). For a drug that shows potent activity in vitro (MIC50 and MIC90 was 0.12 ug/ml), the tigecycline could be a therapeutic option in infection by Clostridium difficile, depending on further studies to evaluate their real clinical efficacy and security. Conclusion: Obtained results in this study indicate the need for further studies in vitro and clinicians to define the limits of sensitivity/resistance to teicoplanin and nitazoxanide, so there is no interpretation criteria for both disk diffusion and for agar dilution. Results of this work in vitro study confirmed the utility of metronidazole as an effective drug in the treatment of infection by Clostridium difficile. Nitazoxanide was the drug that showed better performance in vitro by dilutional method. We suggest the use of disk diffusion method: metronidazole, vancomycin and moxifloxacin. This work suggest that inhibition zones for metronidazole ( >= 33mm), moxifloxacin ( >= 18mm) and vancomycin ( >= 22mm) could be considered as sensitive by disk diffusion method. The agar dilution method is a method to be accurate, but laborious to run in the laboratory routine

Bacilos gram-positivos

Clostridium difficile

Diarreia

Gastroenteropatias

Metronidazol

Moxifloxacino

Nitazoxanida

Resistência a medicamentos

Teicoplanina

Testes de sensibilidade microbiana

Tigeciclina

Vancomicina

Clostridium difficile

Diarrhea

Disk diffusion antimicrobial tests

Drug resistance, Gram-positive rods

Gastrointestinal diseases

Metronidazole

Microbial sensitivity tests

Nitazoxanide

Teicoplanin

Tigecycline

Vancomycin, Moxifloxacin

Epidemiologia das infecções causadas por Staphylococcus aureus resistente a meticilina com perfil comunitário (CA-MRSA) em pacientes atendidos em um hospital terciário no Rio de Janeiro / Epidemology of infections due to community-acquired methicillin-resistant staphylococcus aureos (CA-MRSA) in patients hospitalized in tertiary hospital in Rio de Janeiro

Julio Cesar Delgado Correal

02 December 2011

Fundação de Amparo à Pesquisa do Estado do Rio de Janeiro / O Staphylococcus aureus resistente a meticilina (MRSA) foi inicialmente descrito como um patógeno associado a infecções relacionadas à assistência em saúde; porém, um clone de MRSA, o CA-MRSA emergiu na comunidade e está atualmente incrementando nos hospitais. O objetivo desta tese foi descrever aspectos relacionados com a epidemiologia das infecções por cepas CA-MRSA no Hospital Universitário Pedro Ernesto da Universidade do Estado do Rio de Janeiro (HUPE/UERJ), avaliando especificamente fatores de risco relacionado com as infecções por CA-MRSA. Usando informações das bases de dados do laboratório de microbiologia, da farmácia e da Comissão para Controle da Infecção Hospitalar do HUPE/UERJ foi realizado um estudo retrospectivo de infecções/colonizações por cepas de S. aureus (fevereiro 2005 a Julho 2011). Foi realizado um estudo caso e controle, utilizando como casos os pacientes com infecções por cepas CA-MRSA. Na avaliação da susceptibilidade aos antimicrobianos usados em infecções graves por MRSA (vancomicina, teicoplanina, daptomicina e linezolida), foram determinadas as concentrações inibitórias mínimas (CIM) das amostras por diferentes metodologias (testes de difusão em agar, microdiluição em caldo e E-test). Nas analises das tendências temporais da apresentação dos subtipos de MRSA, usando um critério fenotípico para classificação das cepas MRSA, foi observada uma diminuição do número de cepas de MRSA multirresistente (HA-MRSA) (p<0.05). Também foi observada uma tendência ao aumento de cepas não-multirresistentes (CA-MRSA), mas sem alcançar a significância estatística (p = 0.06) igual que os S. aureus sensíveis a meticilina (MSSA) (p = 0.48). Não houve associação entre o subtipo de MRSA e a mortalidade devida à infecção por cepas MRSA. Uma idade acima de 70 anos (OR: 2.46, IC95%: 0.99 - 6.11), a presença de pneumonia adquirida no hospital (OR: 4.94, IC95%: 1.65 -14.8), a doença pulmonar obstrutiva crônica (OR: 6.09, IC95% 1.16 31.98) e a leucemia (OR: 8.2, IC95%: 1.25 54.7) foram fatores de risco associadas à mortalidade nas infecções por cepas de S. aureus. Usando curvas de Kaplan-Meier, foi observada uma tendência ao aumento da mortalidade em infecções causadas por MSSA na primeira semana, porém sem alcançar significância estatística (p = 0.07). Não foram observadas amostras MRSA com susceptibilidade intermediaria a vancomicina, linezolida, daptomicina ou teicoplanina. A dinâmica das infecções por S. aureus no HUPE/UERJ mudou durante o período de estudo, com menor número de episódios infecciosos causados por cepas de MRSA multirresistentes. Existe uma tendência ao aumento das cepas não-multirresistentes de MRSA entanto que a taxa de infecções por MSSA permaneceu estável no período do estudo. O perfil de resistência dos estafilococos não teve associação com a mortalidade / The methicillin-resistant Staphylococcus aureus (MRSA) was described initially like a health-care associated pathogen. However, an MRSA clone called community-adquired S. aureus emerged with success in the community and now has a worring increasing frequency in hospital settings. The aim of this study was to descript issues related to the epidemiology of infections due tu CA-MRSA isolates at the Pedro Ernesto Universitary Hospital (HUPE/UERJ) in Rio de Janeiro, Brazil from february 2005 to june 2011, analyzing risk factors related to these infections. Thus, using databases of the microbiology laboratory, pharmacia department and the infection control committee of the HUPE-UERJ, was realized an restrospective study of S. aureus isolates obtained from infected/colonizated patients hospitalized from February 2005 to July 2011. To evaluate risk factors related to CA-MRSA infections was conduced a case-control study, using patients with true infections due to MRSA like cases and patients with methicillin susceptible S. aureus (MSSA) like controls. To test the antimicrobial susceptibility of the antibiotics used in MRSA severe infections (Vancomycin, teicoplanin, daptomycin and linezolid), were determinated the minimal inhibitory concentration (MIC) of MRSA isolates using differents methods (disk-difusion test, microdilution in broth and E-test strips). The trend analyses of the MRSA types, using a phenotypic criteria to classificate the MRSA isolates, found a decrease in the infections due to multi-resistant MRSA isolates (HA-MRSA) in our hospital (p<0.05). Also was observed and increase in non-multi-resistant MRSA strains (CA-MRSA), but without reach statistic significancy (p = 0.06), similar to MSSA (p = 0.48). There is not association between the MRSA phenotype and the mortality due to S. aureus infection. In the multivariate analysis, were observed that an older age than 70 years (OR: 2.46, IC95%: 0.99 - 6.11), health-care pneumonia (OR: 4.94, IC95%: 1.65 -14.8), chronic obstructive pulmonary disease (OR: 6.09, IC95% 1.16 31.98) and leucaemia (OR: 8.2, IC95%: 1.25 54.7) were risk factors associated with mortality due to S. aureus infections. The Kaplan-Meier analysis, found a trend to high mortality due to MSSA infections in the first week, but without get statistic significancy (p = 0.07). We dont found any MRSA isolated with resistance or intermediary resistance to vancomycin, linezolid, daptomycin or teicoplanin. There is good correlation between both MICs determinations, with broth microdiluiton and E-Test strips metodhology. Its were concluded that the dynamic of the S. aureus infections at the HUPE/UERJ is changing, with less number of infectious episodes due to multi-resistant MRSA isolates. Moreover, there are an increasing number of infections due to non-multi-resistant MRSA isolate. The prevalence of infections due to MSSA dont have change in the time of period study. The kind of the S. aureus phenotype dont has association with all-causes-mortality

fatores de risco

bacteremia

CA-MRSA

HA-MRSA

daptomicina

vancomicina

linezolida

teicoplanina

estafilococos áureos

infecção hospitalar

staphylococcus aureus

health-care infections

risk factors

bloodstream infection

CA-MRSA

HA-MRSA

daptomycin

vancomycin

linezolid

teicoplanin

MICROBIOLOGIA MEDICA

"Estudo comparativo do tratamento das artroplastias infectadas do quadril sem e com o uso do espaçador de cimento com antibiótico" / Prospective study of the treatment of chronically infected hip replacements with and without the use of an antibiotic-loaded acrylic cement spacer

Henrique Antonio Berwanger de Amorim Cabrita

12 April 2004

Em um estudo prospectivo sobre o tratamento das artroplastias de quadril infectadas, com perdas ósseas e fístulas ativas, 25 pacientes foram tratados em dois tempos e 36 pacientes foram tratados em dois tempos com espaçador de cimento impregnado com vancomicina. O acompanhamento médio foi de dois anos e onze meses. A taxa de recidiva infecciosa foi de 29,2% nos tratados em dois tempos e de 8,8% nos tratados com espaçador. O Escore de Harris para Quadril médio passou de 19,3 para 69,0 pontos nos casos tratados em dois tempos e de 19,7 para 72,2 pontos nos pacientes tratados com espaçador. Ao final do estudo, 86,1% dos tratados com espaçador e em 33,3% dos tratados em dois tempos tinham próteses em bom funcionamento e sem infecção. O espaçador de cimento com antibiótico é o tratamento de escolha nas próteses infectadas de quadril / We report a prospective study of 61 patients with chronically deep infected hip replacements with actively discharging sinuses, treated with a two-stage revision protocol, with and without a cement spacer impregnated with vancomycin. The average follow-up was two years and eleven months. Twenty-five patients were treated without a spacer and seven had recurrence of infection. Thirty-three patients were treated with a spacer and three had recurrence of infection. The average Harris Hip score increased from 19,3 to 69,0 on the non-spacer patients and from 19,7 to 75,2 on the spacer group. At the end of the study, the success rate was 86,1% for the spacer group and 33,3% for the non-spacer group. The use of the spacer increased the results of the two-stage chronic infected hip replacements

ARTROPLASTIA DE QUADRIL/métodos

CIMENTO PARA OSSOS/uso terapêutico

ESTUDO COMPARATIVO

ESTUDOS PROSPECTIVOS

GRUPOS CONTROLE

VANCOMICINA/uso terapêutico

ARTHROPLASTY REPLACEMENT HIP/methods

BONE CEMENTS/therapeutic use

COMPARATIVE STUDY

CONTROL GROUPS

PROSPECTIVE STUDIES

PROSTHESIS-RELATED INFECTIONS/surgery

VANCOMYCIN/therapeutic use