Antimicrobial Resistance

Antimicrobial Resistance - Current Threats Camilla Wiuff November 2010

Antimicrobial resistance - a threat to public health and patient safety • Infections with resistant organisms are associated with increased morbidity and mortality • Extended stays in hospitals • Reduced treatment options • Untreatable infections • Increased healthcare costs

Evolution of antibiotic resistance is a consequence of selective pressure

Selection for resistance Antibiotic not effective antibiotic

Antibiotic Use Overview of Antimicrobial Usage and Bacterial Resistance in Selected Human and Animal Pathogens in the UK: 2007 – Joint Report ~ 80% of antimicrobial use in humans was for patients in the community

Use of antibiotics in Scotland 1994-2009 in primary care SAPG – Report on Antimicrobial Use and Resistance – draft (publication January 2011)

Qualitative measures of antimicrobial prescribing in hospitals – ESAC Point Prevalence Survey 2009 SAPG – Report on Antimicrobial Use and Resistance – draft (publication January 2011)

The association between antimicrobial use and resistance is complex and difficult to measure • Time delay (>1-2 years) between use and the development of resistance • Co-selection by other antibiotics (due to linked resistance genes) • Co-selection by metal-ions, disinfectants, other agents/chemicals • Selection of non-specific resistance mechanisms (e.g. efflux pumps, outer membrane porins) • Spread of highly resistant (and fit) clones and plasmids

Association between use and resistance at country level (ESAC and EARSS data) Penicillin non-susceptible S. pneumoniae Fluoroquinolone resistant E. coli Sande-Bruinsma, EID, 14, Nov, 2008

Gram-negatives • Penicillinase indentified in the laboratory, 1940 Penicillin entered clinical use • Penicillinase quickly spread in clinical isolates Broad-spectrum antibiotics became available in 1950-60’s • Beta-lactamases with increasing spectrum 1950-1970 Cephalosporins became available in the 1970’s • Extended spectrum beta-lactamases, ESBLs, 1980-1990 (TEM, SHV, CTX-M, OXA, AmpC) Carbapenems became available 1985 • 1996 (2003 EU) carbapenemases (KPC, VIM, OXA, NDM-1) • 2009- carbapenem-non-susceptible Enterobacteriaceae (CSNEs) – “UNTREATABLE”!

Emerging carbapenem resistance in Gram-negatives • Significantly limits treatment options for life-threatening infections • No new drugs are under development for gram-negative infections • Resistance mechanisms (carbapenemases) are mobile (spread readily via plasmids) • Co-resistance to other agents is common • Surveillance, prudent antimicrobial prescribing and infection control are necessary to limit the spread of carbapenemases

Surveillance of Gram-negatives in Scotland • The national surveillance is focussed on bacteraemia • Clinically important infection (high morbidity and mortality) • All symptomatic patients are sampled and tested • Resistance data are comparable with European EARS-Net data from 27 countries • Resistance in bacteraemia isolates is likely to reflect earlier resistance problems in other infections (UTI, GTI, RTI)

Cases of bacteraemia and ESBLs in Scotland

E.coli bacteraemia – Scotland 2009 SAPG annual AMR report, due Jan 2011

Gram-negative bacteraemia – Trends Scotland • Large increase in reporting of bacteraemia to HPS (2008-2009) • Resistance to all clinically important antibiotics (aminopenicillins, cephalosporins, fluoroquinolones, aminoglycosides) • No change in %ESBL (~7-8 %) • Stabilisation in resistance proportions in 2009 • Significant decrease in (%) resistance to 3rd gen. cephalosporins in E. coli • No carbapenem resistant bacteraemia reported in 2009 (but 10 isolates of other types) • Are we starting to see an effect of antimicrobial stewardship programmes?

Multi-drug resistance MDR: resistant to at least 1 antibiotic in 3 antimicrobial categories XDR: resistant to all but 2 antimicrobial categories PDR: resistant to all antimicrobial categories Magiorakos et al., ECDC, draft definitions, 2010

ESBL production among cephalosporin resistant bacteraemia isolates • E. coli 7.5% of all E. coli bacteraemia 50% of isolates resistant to cefuroxime (2. gen) 70% of isolates resistant to ceftriaxone/cefotaxime/ceftazidime (3. gen) • K. pneumoniae 8.8% of all K. pneumoniae bacteraemia 45% of isolates resistant to cefuroxime (2. gen) 65% of isolates resistant to ceftriaxone/cefotaxime/ceftazidime (3. gen)

Carbapenemases in Scotland in 2009 Isolates characterised by ARMRL, Colindale: • 4 isolates of Pseudomonas aeruginosa (VIM) • 2 Klebsiella pneumoniae (KPC) • 3 Enterobacter (VIM, KPC) • 1 Citrobacter freundii (NDM) • 4.7% (9/192) of Pseudomonas aeruginosa bacteraemia isolates were resistant to meropenem

Epidemiology of KPC carbapenemases • Klebsiella pneumoniae clones of KPC carbapenemases circulating in USA, Israel and Greece • Sporadic isolations of KPC in South America, Europe, UK • Further spread in China, Colombia, Puerto Rico • KPC have been reported in E. coli, Salmonella cubana, Enterobacter, Proteus mirabilis, Citrobacter freundii, Serratia marcescens, P. aeruginosa, Acinetobacter baumannii

NDM-1 carbapenemases in the UK • Carbapenemase-producers were sporadic in the UK in 2003-2007 • Isolations of carbapenemase-producers increased in the UK 2008-2009 • First NDM-1 isolated in 2008 in the UK • In 2009, NDM-1 became the predominant carbapenemase in Enterobacteriaceae (44%) in the UK • 37 isolates of NDM-1 were referred from 25 UK laboratories in 2008-2009 (urines (15), blood (3), burns/wound (4), sputum (2). CL (1), throat (1), unknown (3)) • Average age of UK patients: 60 years (range 1-87) (India: 36 years) • 17 out of 29 patients with NDM-1 had been in India/Pakistan within the past year (14 had been in hospitals during their travels) • Most UK carbapenemase-producers concurrently carry additional beta-lactamases (CTXM-15, CMY-4), fluoroquinolone and gentamicin resistance mechanisms

Carbapenemases - Is there a link to medical tourism? Kumarasamy, Lancet Infection, Aug 2010 Clones and plasmids are transported between continents in the human gut flora – most dissemination is undetected!

Carbapenemases – UK and India • UK: Non-clonal isolates (NDM-1 on chromosome, variable plasmids, conjugates easily) • Chennai (South India) : Non-clonal isolates (NDM-1 on plasmids, variation of plasmids, conjugates easily) • Haryana (North India): Clonal isolates – outbreak? • There were no genetic links between isolates from India and the UK (possibly due to too few isolates investigated) • UK is the first Western country to report widespread occurrence of NDM-1 • Most patients in Haryana and Chennai were from community-acquired infections in younger people (mean=36 yrs) • Non-prescription use of carbapenems in India is of major concern

Surveillance of carbapenemases in Scotland • Susceptibility testing in diagnostic laboratories • Sensitive, reliable and standardised testing methodology is key – automated VITEK systems are part of the Scottish strategy for obtaining high quality data on emerging carbapenem resistance • Further investigations by ARMRL, Colindale to determine resistance mechanism and subtype • HPS AMR-alert system that prompts laboratories to unusual susceptibility results (in specific drug-bug combinations) – weekly • Annual report on resistance in bacteraemia isolates • Development of national surveillance of resistance in UTI (proportional system)

Resistance in Gram-positives • Less of a concern in Scotland at the moment • Newer antibiotics with activity against Gram-positives are available (linezolid, daptomycin, tigecycline) • Except for MRSA, resistance rates are generally low among Gram-positive in Scotland • Gram-positive exhibit a remarkable ability to develop antibiotic resistance through a range of mutational events and gene transfers, followed by spread of successful resistant clones

Glycopeptide resistance • Glycopeptides: vancomycin and teicoplanin • Used for life-threatening Gram-positive infections – last resort drugs • Vancomycin Resistant Enterococci (VRE) reported in 1987-1988 in UK (high-level resistance, later low-level resistance reported) • Vancomycin resistance in Enterococcus faecium (VRE)in Scotland- 17% in 2008, 28% in 2009 • In 2008, Ireland, Greece and the UK reported >25% VRE (and increasing trends) • Enterococci are a common cause of bacteraemia • Glycopeptide resistance transfer via plasmids to more pathogenic bacteria such as MRSA – is a concern

Mupirocin • Mupirocin (pseudomonic acid A) is a topical antibiotic • Used to treat skin and soft tissue infections • Used to eradicate staphylococcal nasal carriage in patients pre-operatively • Used to eradicate MRSA in healthcare facilities • High-level resistance leads to treatment failure • It is a concern that the implementation of the national MRSA screening programme will lead to increased mupirocin resistance

Summary • Evolution and spread of antibiotic resistance is a consequence of how antibiotics are used and mis-used in humans, animals and the environment. • Large efforts are going into improving the quality of antimicrobial prescribing and limiting the spread of resistance in NHS Scotland – activities are coordinated by SAPG • A reduced number of prescriptions was seen in primary care in Scotland in 2009 compared to 2008 (co-amoxiclav, cephalosporins and fluoroquinolones) • Resistance rates in Gram-negative bacteraemia stabilised in 2009, and cephalosporin resistance decreased. • Carbapenem (and multidrug) resistance in Gram-negatives (in particular Enterobacteriaceae) is a worldwide threat to public health • Increasing glycopeptide resistance in Enterococci (e.g. VRE) and increasing mupirocin resistance in S. aureus is causing concern • Improved quality of antimicrobial prescribing and standardised susceptibility testing are key to monitoring and limiting emerging resistance problems

The HPS-ISD AMR Team • Anne Eastaway • Camilla Wiuff • William Malcolm • Julie Wilson • Tracey Cromwell • Marion Bennie • A-Lan Banks • David Henderson • Ernest Amaziro • HPS, ISD, NSS IM&T departments

"Don't forget to take a handful of our complimentary antibiotics on your way out“ New Yorker Jan 12, 98

Antimicrobial Resistance - Current Threats