Effect of prolonging Clostridium difficile (CD) treatment on recurrence rate in patients receiving concomitant systemic antibiotic therapy 5-yr retrospective single-centre study in 301 patients with first episode of Clostridium difficile infection (CDI) (period ) Bivariate analysis of 65 patients with concomitant systemic antibiotic therapy* and follow-up of ≥12 wk: –23 patients with standard CD treatment duration (35%) –42 patients with prolonged CD treatment duration (defined as ≥15 days; 65%) Highest CDI recurrence rate in patients receiving oral vancomycin: –36% for vancomycin alone –50% for vancomycin and metronidazole –20% for metronidazole alone Ponce-Terashima R. IDSA 2012 abs of 2

Effect of prolonging Clostridium difficile (CD) treatment on recurrence rate in patients receiving concomitant systemic antibiotic therapy Prolonging CD treatment in patients on concomitant antibiotics may not reduce the CDI recurrence rate Ponce-Terashima R. IDSA 2012 abs of 2

Colonoscopic vs nasogastric faecal transplantation for treatment of Clostridium difficile infection (CDI) Pooled analysis of study data (published until December 2011) on faecal transplantation for recurrent CDI 12 studies with 182 patients Postigo R. IDSA 2012 abs of 2

Colonoscopic vs nasogastric faecal transplantation for treatment of Clostridium difficile infection (CDI) No significant AEs were noted Faecal transplantation for recurrent CDI via colonoscopy or nasogastric tube appears highly and equally effective, and safe Postigo R. IDSA 2012 abs of 2

Impact of probiotics on occurrence of Clostridium difficile infection (CDI) in patients receiving high-risk antibiotics Retrospective cohort study in adult inpatients who received antibiotics (with high risk of acquiring CDI) during ≥5 days in the period July-Dec 2010 –Selected high-risk antibiotics: clindamycin, ceftriaxone, ciprofloxacin, levofloxacin –Patient demographics, comorbidities, probiotics use (Lactobacillus GG and Saccharomyces boulardii), concomitant proton pump inhibitor (PPI) use 20 of 389 (5.1%) had CDI within 90 days of antibiotic use: Dickson J. IDSA 2012 abs of 2

Impact of probiotics on occurrence of Clostridium difficile infection (CDI) in patients receiving high-risk antibiotics 65% of patients who developed CDI used levofloxacin but even after adjusting for levofloxacin use, risk remains 2.6-fold higher for probiotics users compared with non-users (P<0.05) Effect of concomitant PPI use on occurrence of CDI: The use of probiotics seems to increase the risk of CDI in patients on high-risk antibiotics; concomitant PPI use may even further increase this risk Dickson J. IDSA 2012 abs of 2

Differential risk of antibiotics on community-associated Clostridium difficile infection (CDI) Meta-analysis of 4 observational studies comparing antibiotic vs non-antibiotic use in non-hospitalised patients (retrieved from 465 publications from 2 databases by 2 independent reviewers) In the community setting, there seems to be substantial variation between different antibiotic classes for the risk of CDI Brown K. IDSA 2012 abs.723

Risk factors associated with systemic absorption of oral vancomycin in the treatment of Clostridium difficile colitis (CDC) Retrospective single-centre study in 85 adult (≥18 yr) patients with CDC receiving oral vancomycin during ≥5 days without concomitant iv vancomycin Vancomycin serum levels during therapy assessed on day 5, 10 and weekly thereafter Multivariate logistic regression analysis to assess risk factors for systemic absorption of vancomycin with P value of ≤0.20 on Chi-square analysis Carver PL. IDSA 2012 abs of 2

Risk factors associated with systemic absorption of oral vancomycin in the treatment of Clostridium difficile colitis (CDC) 60 patients (71%) had ≥1 detectable vancomycin plasma level (range µg/ml) of which 15 patients ≥1 level >2.5 µg/ml CDC severity, oral vancomycin dose, ICU admission and gastrointestinal pathology seem risk factors for systemic absorption Carver PL. IDSA 2012 abs of 2

Outcome of intestinal microbiota transplantation on death/colectomy in patients with severe/fulminant Clostridium difficile infection (CDI) Single-centre retrospective study (period May 2010-Dec 2011) in 28 patients with severe/fulminant colitis due to CDI (median age 60 yr) unresponsive to conventional CDI therapy Donors for intestinal microbiota transplantation: screened for negative serology for HIV, hepatitis A/B/C and syphilis, stool tested by PCR for negative C. difficile DNA Outcome: –Primary: clinical improvement (resolution of diarrhoea) –Secondary: CDI recurrence within 100 days Hassan M. IDSA 2012 abs of 2

Outcome of intestinal microbiota transplantation on death/colectomy in patients with severe/fulminant Clostridium difficile infection (CDI) 28/28 (100%) tolerated the procedure well, no AEs 28/28 (100%) recovered dramatically within 1-4 days post transplant 28/28 (100%) had no recurrence within 100 days post transplant Intestinal microbiota transplantation for refractory severe/fulminant colitis due to CDI appears life-saving and safe Hassan M. IDSA 2012 abs of 2

Removal of catheter and therapy duration in cancer patients with Staphylococcus aureus central line- associated bloodstream infection (BSI) Single-centre, retrospective study in cancer patients with suspected Staphylococcus aureus central line-associated BSI (SA-CLBSI; period ) Of 762 patients, 299 patients (304 episodes) fulfilled the CDC definition of SA-CLBSI Patient characteristics*: –52% with haematological malignancy –23% with neutropenia –69% had fever –76% had sepsis –28% had signs of inflammation at the catheter site –64% developed complications El Zakhem A. IDSA 2012 abs of 2

Removal of catheter and therapy duration in cancer patients with Staphylococcus aureus central line- associated bloodstream infection (BSI) Staphylococcus aureus isolates*: –51% had MIC of 2 to vancomycin –47% were methicillin resistant (MRSA) Catheter: –64% removed/exchanged within 3 days (80% within 7 days) –Removal within 3 days associated with lower relapse compared with no/late removal after 7 days (P=0.009) BSI episodes: –109/304 (36%) was uncomplicated at time of presentation –29/109 (27%) became late complications –No association between therapy duration (14 days as cut-off) and late complications, relapse/recurrence, all-cause mortality in uncomplicated group Catheter removal within 3 days of SA-CLABSI onset seems associated with a lower relapse rate in cancer patiens; for uncomplicated infections, therapy duration beyond 14 days may not be necessary El Zakhem A. IDSA 2012 abs of 2

Comparison of nasal mupirocin ointment with povidone- iodine solution for preventing Staphylococcus aureus (SA) surgical site infection (SSI) Investigator-driven, open-label randomised trial: 1 application nasal povidone-iodine (PI) solution vs 5-days nasal mupirocin ointment prior to surgery on SA SSI outcome in patients after arthroplasty or spine fusion surgery Standard in both groups: 2 applications of topical chlorhexidine gluconate (CHG) Endpoints: –Primary: deep SA SSI at 3-mo follow-up (CDC/NHSN case definition, determined by blinded investigators) –Secondary: superficial SA SSI, deep SSI due to any pathogen, drug-related AEs, risk factors for infection assessed by uni/multivariate analysis Preoperative SA colonisation associated with deep SA SSI (P=0.002) ITT analysis: –1 vs 0 superficial SA SSI for PI vs mupirocin group –6/887 (0.68%) vs 14/879 (1.59%) deep SSI due to any pathogen for PI vs mupirocin group (P=0.07) Phillips MS. IDSA 2012 late breaking abs.3 1 of 2

Comparison of nasal mupirocin ointment with povidone- iodine solution for preventing Staphylococcus aureus (SA) surgical site infection (SSI) AE due to study drug or CHG: 3% for PI group vs 10% for mupirocin group (P<0.001) Given the lower rate of deep SSI due to SA, PI could be an effective and safe preoperative alternative to mupirocin Phillips MS. IDSA 2012 late breaking abs.3 2 of 2

Penicillin-susceptible Staphylococcus aureus (SA) infection in an era of multidrug resistance Retrospective chart review of patients with SA in blood cultures in lab database (period July-Dec 2011) : adults only, no repeat episodes Study background : –5% of methicillin-sensitive SA isolates are sensitive to penicillin –Aimed to characterise frequency of serious infections due to penicillin-sensitive SA (PSSA) and how these patients are managed Of 445 patients with SA: 280 had MSSA Of 280 patients with MSSA: 58 (21%) had PSSA Mortality in PSSA group during index hospitalisation: 14% 2 excluded (no adults), 8 received broad spectrum antibiotics or died  48 patients with PSSA were analysed for treatment choice Goodman J. IDSA 2012 abs of 2

Penicillin-susceptible Staphylococcus aureus (SA) infection in an era of multidrug resistance Labs should (continue to) report penicillin sensitivity for SA infection because large part of MSSA is PSSA; many patients with PSSA receive inappropriate therapy Goodman J. IDSA 2012 abs of 2

Clinical outcome of linezolid vs vancomycin treatment in patients with ventilator-associated pneumonia (VAP) due to methicillin-resistant Staphylococcus aureus (MRSA) Multi-centre, retrospective observational IMPACT-HAP study in 144 ICU patients with VAP due to MRSA treated with linezolid vs vancomycin in the US VAP due to MRSA defined according to CDC/NHSN surveillance and if MRSA isolated from tracheal aspirate or bronchoalveolar lavage Exclusion: patients with do-not-resuscitate or do-not-intubate order Clinical success defined as symptom improvement or resolution by day 14 or at earlier hospital discharge Peyrani P. IDSA 2012 abs of 2

Clinical outcome of linezolid vs vancomycin treatment in patients with ventilator-associated pneumonia (VAP) due to methicillin-resistant Staphylococcus aureus (MRSA) Propensity-adjusted logistic regression model: lowering clinical success rate with increasing APACHE II score for both treatment groups but significantly higher rates at each APACHE II score for linezolid compared with vancomycin (P<0.001) Patients with VAP due to MRSA treated with linezolid seem more likely to respond favourably compared with patients treated with vancomycin Peyrani P. IDSA 2012 abs of 2

Prevalence and risk factors of carriers of extended spectrum β-lactamase (ESBL)-producing Enterobacteriaceae Prospective single-centre study in 525 patients admitted to hospital (over 1 week) and screened for ESBL Excluding paediatric and obstetric departments, rectal swabs collected 56/525 (10.6%) were positive for ESBL: –41/56 (73.2%) with E. Coli –76.8% without positive clinical cultures or not previously known as ESBL carrier Multivariate analysis to identify independent risk factors for ESBL carriage Shitrit P. IDSA 2012 abs of 2

Prevalence and risk factors of carriers of extended spectrum β-lactamase (ESBL)-producing Enterobacteriaceae Of screened patients with ≥1 risk factor (N=273), 49 (18%) was positive compared with 7/252 (3%) of screened patients without risk factors Screening of population at risk would discover 88% of positive pts 11% prevalence of ESBL carriers among new hospital admissions and the identification of risk factors warrant targeted screening Shitrit P. IDSA 2012 abs of 2

Role of procalcitonin (PCT) in guiding antibiotic therapy Descriptive review of RCTs using PCT to guide antibiotic therapy –2 RCTs in outpatient primary care setting: About 1,000 patients with upper/lower respiratory tract infections Antibiotic use: PCT cut-off value of 0.25 µg/l was used –5 RCTs in emergency room and inpatient medical floor setting: Patients with COPD exacerbation, bronchitis and community-acquired pneumonia Antibiotic use: control group according to standard of care vs PCT group according to algorithm (start if PCT level >0.25 µg/l, stop if PCT level <0.25 µg/l) –Several RCTs in ICU setting: Antibiotic use: started in control and PCT group but stopped according to PCT-based algorithm Maskey M. IDSA 2012 abs of 2

Role of procalcitonin (PCT) in guiding antibiotic therapy Significant reduction in antibiotic use –In outpatient setting –In PCT-guided group compared with control group in emergency/inpatient setting Shorter duration of antibiotic treatment in ICU setting in PCT vs control group Similar clinical outcome in PCT group compared with control group No adverse clinical outcome in PCT group in neither of studies PCT seems a promising biomarker for bacterial infection and may give guidance in antibiotic therapy Maskey M. IDSA 2012 abs of 2

Antibiotic combination therapy vs monotherapy for Pseudomonas aeruginosa bloodstream infections 2-centre retrospective review of adult patients with bloodstream infections due to Pseudomonas aeruginosa (period ) who started on antibiotic combination therapy Comparison between patients who continued to those who changed to monotherapy after report of antimicrobial susceptibility testing (AST) Of 239 patients, 148 (62%) started on combination therapy, and after AST: Viehman JA. IDSA 2012 abs of 2

Antibiotic combination therapy vs monotherapy for Pseudomonas aeruginosa bloodstream infection No difference between groups in age, gender, presence of diabetes, neutropenia, septic shock, history of organ transplant mechanical ventilation, Charlson comorbidity index, rate of C. difficile colitis (±10%) and acute renal failure after antibiotics (±17%) Multivariable logistic regression analysis: no difference for adjusted in-hospital mortality between combi and monotherapy (39% vs 32%, P=0.19) Continuing double coverage in pts with Pseudomonas bloodstream infection once AST data are available seems not beneficial Viehman JA. IDSA 2012 abs of 2

Efficacy and safety of moxifloxacin in patients with secondary peritonitis Post-hoc pooled analysis of 4 prospective multi-centre phase III RCTs in adult patients with complicated abdominal infections: –Secondary peritonitis with APACHE score of 7.0±5.0 and community- acquired origin –Moxifloxacin 400 mg iv/PO or iv od vs comparators: ertapenem (1.0 g iv od) piperacillin/tazobactam (3.0 g/0.375 g iv qid) ceftriaxone 2.0 g od iv/metronidazole (500 mg iv bid or tid) amoxicillin/clavulanic acid (800 mg/114 mg PO bid or 500 mg/125 mg PO tid) Primary efficacy endpoint: clinical success* at the test-of-cure visit at days after the end of therapy in PP population De Waele J. IDSA 2012 abs of 2

Efficacy and safety of moxifloxacin in patients with secondary peritonitis Overall clinical success rate: similar between groups for different infection sites Safety analysis: Compared with other antibiotics, moxifloxacin appears to be an effective and safe option for the treatment of secondary peritonitis De Waele J. IDSA 2012 abs of 2

Clinical and economical outcomes of meropenem and piperacillin-tazobactam treatment using extended compared with intermittent infusions in critically ill patients Single-centre retrospective chart review of patients –Receiving ≥48h meropenem (500 mg Q6h) or piperacillin-tazobactam (PT; g Q8h) –Both treatments using intermittent infusions (period Jan-Dec 2010) and extended* infusions (period Nov 2011-April 2012) Outcomes: –Primary: in-hospital all-cause mortality –Secondary: length of hospital stay, length of ICU stay, time to normalisation of white blood cell count and temperature Baseline characteristics: –Between meropenem groups (N=100): difference in continuous renal replacement therapy and solid organ transplant –Between PT groups (N=148): no difference Ternes L. IDSA 2012 abs of 2

Extended infusion in PT group: 13.2% reduction in average cost/patient/day Clinical and economical outcomes of meropenem and piperacillin-tazobactam treatment using extended compared with intermittent infusions in critically ill patients Extended compared with intermittent infusion seems to result in faster progression to death (significant for meropenem and likely for PT) Ternes L. IDSA 2012 abs of 2

Impact of gentamicin-collagen sponge on the risk of surgical site infection (SSI) Meta-analysis of 14 publications/13 study populations on prophylactic use of gentamicin-collagen sponges for SSI: –Cardiac surgery (N=4)- Colorectal surgery (N=5) –Gastrointestinal surgery (N=2)- Hernia surgery (N=2) Retrieved from PubMed/Cinahl database (period ): data extraction independently by 2 persons, summary estimates using random-effects model The use of gentamicin-collagen sponges appears associated with a reduced risk of SSI following cardiac (but not colorectal) procedures Formanek M. IDSA 2012 abs.1294

Evaluation of serotonin toxicity associated with linezolid or vancomycin treatment Observational matched cohort study in 502 hospitalised patients treated with linezolid or vancomycin (1:1) at the Upstate New York Veterans’ Affairs Healthcare Network (period ) Matching for: –Hospital –Hospital ward (ICU vs non-ICU) –Hospital length of stay prior to treatment start with linezolid/vancomycin –Age ( 75 yr) –Baseline platelets ( 100,000 cells/mm 3 ) Toxicity evaluation using intensive natural word search algorithm: –Symptoms consistent with serotonin toxicity –Hunter serotonin toxicity criteria (HSTC) Lodise T. IDSA 2012 abs of 2

Evaluation of serotonin toxicity associated with linezolid or vancomycin treatment Baseline patient characteristics similar for linezolid and vancomycin groups Low rates of serotonin toxicity are found in hospitalised patients treated with linezolid (slightly more with vancomycin) Lodise T. IDSA 2012 abs of 2

Treatment duration and outcomes for male urinary tract infection (UTI) Retrospective review of 33,336 patients with index UTI from Veterans Affairs database (fiscal yr 2009) Association between patient/treatment characteristics and outcome (UTI recurrence and Clostridium difficile infection (CDI) over 12 mo) for index cases in uni/multivariate analysis Antibiotics with highest use: –Ciprofloxacin 62.7% –Trimethoprim/sulfamethoxazole 26.8% Drekonja DM. IDSA 2012 abs of 2

Treatment duration and outcomes for male urinary tract infection (UTI) CDI risk was higher with longer than shorter treatment duration: 0.5% vs 0.3%, P=0.02; OR 1.40; 95% CI Longer antibiotic treatment duration of ≥7 days may be associated with increased late recurrence of UTI and subsequent CDI Drekonja DM. IDSA 2012 abs of 2

Relevance of empiric antibiotics for urinary tract infection (UTI) in non-critically ill patients Retrospective review of 447 non-critically ill patients with UTI (period June ) Exclusion: requirement of ICU or inotropes, concurrent other infections Grouping according to susceptibility of urine cultures to empiric antibiotics used: comparison for clinical response to antibiotics at day 3-5, in-hospital mortality, length of stay Lee SY. IDSA 2012 abs of 2

Relevance of empirical antibiotics for urinary tract infection (UTI) in non-critically ill patients Since no adverse clinical outcomes are found, choice of antibiotics in non-critically ill patients could be deferred to after culturing results Lee SY. IDSA 2012 abs of 2

Mortality outcomes and associated risk factors of Stenotrophomonas maltophilia bloodstream infections (BSI) Retrospective single-centre study of 116 patiens with Stenotrophomonas maltophilia BSI (period ) Exclusion: patients with polymicrobial blood cultures Patient characteristics: –89% received previous antibiotics –91% had central venous catheter –44% were in ICU –55% had comorbid malignancy –79% was line-related, 17% secondary, 4% undetermined –Of isolates tested (N=73): 90% sensitive to sulfamethoxazole-trimethoprim (SMX-TMP) and 16% to ticarcillin/clavulanate –65% were treated with appropriate antibiotics (88% of these with SMX-TMP) –Alternative regimens were ticarcillin/clavulanate (N=5), tigecycline (N=13), moxifloxacin (N=2) Hunter AS. IDSA 2012 abs of 2

Mortality outcomes and associated risk factors of Stenotrophomonas maltophilia bloodstream infections (BSI) All-cause 14-day mortality outcome: overall 18% –Similar between patients treated with SMX-TMP and alternatives –Survivors: trend towards longer median time before appropriate therapy –30% when treated with tigecycline (N=13) and 0% when treated with moxifloxacin (N=2); 29% when having SMX-TMP-resistant isolates All-cause 14-day mortality seems comparable between SMX-TMP and alternative regimens in the treatment of S. Maltophilia BSI; independent risk factors could be dissociated Hunter AS. IDSA 2012 abs of 2

Dilated fundoscopic examination (DFE) for ocular candidiasis and echocardiography for infective endocarditis (IE) in patients with Candida bloodstream infection (BSI) Retrospective review of lab surveillance data from active residents in metropolitan Atlanta and Baltimore city and county (period March 2008-May 2010) For adults (≥20 yr) and children with Candida positive blood culture: review of screening DFE and echocardiography documentation (≤14 days after positive blood culture), demographic and clinical data Doshi SS. IDSA 2012 abs.128; Doshi SS. IDSA 2012 abs of 3

Dilated fundoscopic examination (DFE) for ocular candidiasis and echocardiography for infective endocarditis (IE) in patients with Candida bloodstream infection (BSI) Adults with ocular candidiasis (N=8; 5 albicans, 2 glabrata, 1 tropicalis): median age 54 yr, 5 black, 4 male, 6 with >1 positive Candida blood culture day, all required ICU admission Doshi SS. IDSA 2012 abs.128; Doshi SS. IDSA 2012 abs of 3

Dilated fundoscopic examination (DFE) for ocular candidiasis and echocardiography for infective endocarditis (IE) in patients with Candida bloodstream infection (BSI) Adults with IE (N=30; 11 with albicans): median age 63 yr, 18 had prior antibacterials, 3 had non-healthcare-associated onset of Candida BSI, 7 died ≤30 days after initial positive blood culture, 13 (43%) had >1 positive Candida culture day Children with IE (N=4; 3 with albicans): 1 positive Candida culture day Although ocular candidiasis and IE may occur, few patients with Candida BSI are screened with DFE and echocardiography Doshi SS. IDSA 2012 abs.128; Doshi SS. IDSA 2012 abs of 3

Liver safety of posaconazole in early salvage therapy for invasive fungal infection (IFI) caused by molds and yeasts Prospective multi-centre cohort phase II study with posaconazole treatment (oral 400 mg bid) in 40 patients with IFI who failed or were intolerant to prior antifungal treatment (Canada, period ) Patient characteristics: –53% had ≥1 elevated liver enzyme at entry –Conditions: leukemia (33%) > stem cell transplant (30%) > lung and renal transplant (23%) > others (15%) –Prior therapies: voriconazole (53%) > amphotericin B (23%) > fluconazole (13%) > caspofungin (5%) Efficacy analysis (according to EORTC criteria) Haider S. IDSA 2012 abs of 2

Liver safety of posaconazole in early salvage therapy for invasive fungal infections caused by molds and yeasts Safety Given its favourable efficacy/safety profile, posaconazole may be used in immunocompromised pts refractory or intolerant to other antifungals Haider S. IDSA 2012 abs of 2

Voriconazole therapeutic drug monitoring in haematologic and ICU patients with invasive aspergillosis (IA) HPLC study of 81 voriconazole plasma concentrations (VPC) in 18 patients: –13 ICU patients; 5 haematologic patients –8 with probable IA, 8 with possible IA, 2 with voriconazole prophylaxis With target range on mg/l: Hoenigl M. IDSA 2012 abs of 2

Voriconazole therapeutic drug monitoring in haematologic and ICU patients with invasive aspergillosis (IA) Continuously low VPC in 3 patients (despite dosage increase to 12 mg/kg)  discontinuation of voriconazole  change to alternative therapy: 2 on oral posaconazole, 1 on liposomal amphotericin B Toxicity: 3 patients with cholestatic hepatopathy –VPC 6.0 mg/l –VPC 4.2 mg/l –VPC 1.4 mg/l despite voriconazole 12 mg/kg Given that VPCs below target range are frequently found in haematologic and ICU patients, therapeutic drug monitoring of voriconazole may be useful Hoenigl M. IDSA 2012 abs of 2

Longitudinal analysis of leukocyte differentials in peripheral blood of patients with acute influenza infection Retrospective study of experimental human challenge tests with influenza A/Wisconsin/67/2005 (H3N2) to assess temporal development and time-dependent utility of leukocyte differential Of 17 inoculated volunteers, 9 (53%) developed symptomatic infection Peripheral blood: daily measurement of differentials from immediately prior to inoculation to resolution of disease McClain M. IDSA 2012 abs.93 1 of 2

Longitudinal analysis of leukocyte differentials in peripheral blood of patients with acute influenza infection Lymphocyte:monocyte ratio of <2 at the time of maximal symptoms correctly classified 100% of the volunteers according to symptom status Despite usefulness of leukocyte differentials to determine infected status, its utility is heavily time dependent McClain M. IDSA 2012 abs.93 2 of 2

Emergence of oseltamivir resistance in patients with influenza A infections Global observational trial IRIS: Influenza Resistance Information Study (NCT ) Patients with influenza-like illness and/or positive rapid test for influenza: –Throat/nose swabs on day 1, 3, 6, 10 for real-time RT-PCR analysis of influenza type/subtype, resistance to neuraminidase inhibitor oseltamivir –Severity scoring (0-3) of 7 symptoms for day 1-12 Of 1,855 RT-PCR positives with single influenza infection in first 3 yr: 1,310 patients had influenza A 700/1,310 (53%) received oseltamivir monotherapy within 2 days after symptom onset: N=9 with seasonal H1, N=222 with H3N2, N=469 with H1N Schutten M. IDSA 2012 abs.94 1 of 2

Emergence of oseltamivir resistance in patients with influenza A infections Post day 1 emergent resistance to oseltamivir in influenza A patients: 19 out of 700 patients (2.7%): Emergent resistance of influenza A to oseltamivir seems to occur mostly in 1-5 yr old children, without effect on symptom resolution Schutten M. IDSA 2012 abs.94 2 of 2

Use of sonication for diagnosis of orthopaedic hardware infection Single-centre retrospective cohort study (period ) of 48 adult patients with removal of infected orthopaedic hardware (plates, screws, nails, K wires; no prosthetic joints) Measurement of agreement (kappa statistics) between results of bacterial culture of tissue with culture of sonicate fluids from orthopaedic hardware Sonicate fluid was incubated on blood, McConkey and chocolate agar, broth media and inoculated into aerobic and anaerobic blood culture bottles Patient demographics: median age 55 yr, 30 (63%) male, 8 (17%) diabetic, 12 (25%) on antibiotics 14 days prior to culture Khumri S. IDSA 2012 abs of 2

Use of sonication for diagnosis of orthopaedic hardware infection Sonication fluid culturing appears complimentary to tissue culturing for the diagnosis of orthopaedic hardware-associated infection but requires optimisation Khumri S. IDSA 2012 abs of 2

Application of whole genome sequencing (WGS) in understanding the role of patients in nosocomial transmission of Staphylococcus aureus (SA) Prospective single-centre study in 1,093 patients admitted to ICU (period ) to assess acquisition* of SA and patient-to- patient transmission # Weekly serial swabs: isolates were spa-typed and underwent WGS to assess relatedness by comparing single nucleotide variants (SNVs) 15.6% of screened patients had SA (4.2% methicillin-resistant SA) 39/676 patients (5.8%) with >1 swab acquired SA Price J. IDSA 2012 abs of 2

Application of whole genome sequencing (WGS) in understanding the role of patients in nosocomial transmission of Staphylococcus aureus (SA) 4/39 patients had patient-to-patient transmission –3 of 4 appeared MRSA spa type t032 outbreak-related BUT –2 of 4: true transmissions according to WGS (>40 SNVs) 10/35 acquisitions: –No epidemiological or spa type evidence for transmission BUT –WGS revealed clusters of highly related isolates (15-38 SNVs) suggesting pre-ICU transmission events In this study, minority of apparent SA acquisitions in ICU seem to be attributable to direct patient-to-patient transmission Price J. IDSA 2012 abs of 2

Aetiology of community-acquired pneumonia in hospitalised adults in the US CDC EPIC (Etiology of Pneumonia in the Community) study: prospective multi-centre design enrolling US patients with community-acquired pneumonia* Blood: culturing and lytA/spy Streptococcus PCR Sputum: culture and Legionella PCR Urine: Pneumococcus and Legionella antigen testing Naso/oropharyngeal swabs: PCR for respiratory viruses/atypical bacteria Preliminary data from Jan 2010-July 2011: 1,608 patients with community-acquired pneumonia –Admission to ICU / mortality: 21% / 3% –1st culture / PCR before inpatient antibiotics: 81% / 59% Jain S. IDSA 2012 abs of 2

Aetiology of community-acquired pneumonia in hospitalised adults in the US Viral or bacterial pathogen detected in 26% and 11% respectively Viruses seem more commonly detected than other pathogens in adults with community-acquired pneumonia Jain S. IDSA 2012 abs of 2

Utility of pneumococcal urinary antigen test (UAT) for antibiotic therapy or stewardship Retrospective single-centre study in 642 inpatients with pneumococcal UAT performed (period Aug 2011-March 2012) 38 patients (5.9%) were positive for pneumococcal UAT Indications (N=38): –58% with community-acquired pneumonia (N=22; CAP) –29% with healthcare-acquired pneumonia (N=11; HCAP) –13% other (N=5) –84% had an indication for pneumococcal UAT De-escalation of antibiotic therapy could have occurred in 9 patients –6 also had positive blood/sputum culture for Pneumococcus as basis for de-escalation, resulting in role for UAT in only 3 of 642 patients (0.5%) –1/3rd of CAP patients were de-escalated (N=7) Because UAT seems to have little effect on antibiotic therapy course and is expensive, the utility of pneumococcal UAT is questionnable Radigan E. IDSA 2012 abs.733

Feedback intervention on infectious disease (ID) physicians in antibiotic stewardship programme Prospective single-centre study in 8 ID physicians Restricted antibiotic prescriptions: –Daptomycin, carbapenem, linezolid, micafungin, tigecycline, voriconazole, posaconazole –Reviewed by an ID Pharm D –Intervention: feedback on weekly ratio to individual ID physician in relation to anonymous colleagues Decreased in number of restricted prescriptions for each ID physician Feedback intervention seems to influence ID physicians’ prescribing habits and may reduce variability Landon E. IDSA 2012 abs.741