Full Title of Guideline. Author: Contact Name and Job Title. Division & Speciality. Review date December 2020

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Full Title of Guideline Author: Contact Name and Job Title Division & Speciality Guideline for the treatment of prosthetic joint infections in adults Mr Peter James - Consultant Orthopaedic Surgeon Dr Susan Snape - Consultant Microbiologist Surgery - orthopaedics Review date December 2020 Explicit definition of patient group to which it applies (e.g. inclusion and exclusion criteria, diagnosis) Immunocompetent adult patients with prosthetic joint infections Changes from previous guideline Shorter courses of treatment in line with current practice Ciprofloxacin and meropenem dosing updated Summary of evidence base this guideline has been created from 1) Local microbiological sensitivity surveillance 2) Recommended best practice based on clinical experience of guideline developers 3) W Zimmerli, A Trampuz, and PE Ochsner. Prosthetic-Joint Infections NEJM (2004) 351 p1645-54 (1) 4) BL Atkins, N Athanasou, JJ Deeks et al. Prospective Evaluation of Criteria for Microbiological Diagnosis of Prosthetic-Joint Infection at Revision Arthroplasty Journal of Clinical Microbiology (1998) 36 (10) p2932-2939 (2) 5) E Moran, I Byren and BL Atkins. The diagnosis and management of prosthetic joint infection. JAC (2010) 65 Suppl 3: iii45-54 (3) 6) I Byren, P Bejon, BL Atkins et al. One hundred and twelve infected arthroplasties treated with DAIR (debridement, antibiotics and implant retention): antibiotic duration and outcome. JAC (2009) 63 p1264-71 (4) 7) P Bejon, A Berendt, BL Atkins et al Two-stage revision for prosthetic joint infection: predictors of outcome and the role of reimplantation microbiology. JAC (2010) 65: 569-575 (5) 8) DR Osmon, EF Berbari, AR Berendt et al Diagnosis and Management of Prosthetic Joint Infection: Clinical Practice Guidelines by the Infecitous Diseases Society of America. CID (2013): 54(1):e1-25 9) AP Puhto, T Puhto and H Syrjala Short-course antibiotcs for prosthetic joint infection treatment with prosthesis retention. Clin Microbiol and Infection (2012): 18:1143-1148 This guideline has been registered with the trust. However, clinical guidelines are guidelines only. The interpretation and application of clinical guidelines will remain the responsibility of the individual clinician. If in doubt contact a senior colleague or expert. Caution is advised when using guidelines after the review date. Nottingham Antimicrobial Guidelines Committee Page 1 of 9 Written: Mr Peter James & Dr Sue Snape

Guideline for the treatment of prosthetic joint infections Presentation: Patients present in different ways with prosthetic joint infections but can be divided into 3 groups depending on their route of acquisition and timing of presentation in relation to surgery (1): 1. Acquired at implantation a. Early presentation within 3 months (~30%) - Acute onset of joint pain, effusion, implant site erythema and warmth, oedema and induration at implant site, fever. May have cellulitis, sinus tract formation, purulent discharge. Virulent organisms involved eg Staphylococcus aureus, Gram negative bacilli b. Delayed presentation from 3 months to 1 year (~40%) - Subtle signs and symptoms including implant loosening, persistent joint pain independent of movement or both. There is fever in <50% cases and a raised WCC 10% cases. Less virulent organisms are involved eg Coagulase negative Staphylococcus, Propionibacterium acnes 2. Haematogenous spread at greater than 1 year (~30%) Frequently from sources of bacteraemia include skin, respiratory tract, dental and urinary tract infections. Patients present acutely with symptoms of joint infection in a previously well-functioning joint (similar to early). The pathogens are usually Staphylococcus aureus, Coagulase negative Staphylococcus, Gram negative bacilli or Streptococci Diagnosis: Diagnosis can be made using the history, examination and the following investigations: Bloods FBC looking especially at the WCC and CRP Blood Cultures (looking for associated bacteraemia) Radiology Plain films are often unhelpful in the acute setting but may show loosening in the delayed presentations. Ultrasound may demonstrate effusions or synovial thickening. Joint aspiration and synovial biopsy send to microbiology for urgent MC&S and synovial biopsy for histology if the patient is already on antibiotics Theatre specimens: Microbiology - 6 samples taken using different forceps and scalpels into different universal tubes and sent to microbiology (2). These samples should be sent as URGENT no matter what time of day they are taken. (Tissues and fluid Nottingham Antimicrobial Guidelines Committee Page 2 of 9 Written: Mr Peter James & Dr Sue Snape

from the joint are much more sensitive samples than swabs with a much higher yield of pathogens cultured compared with swabs.) Histology samples should be taken routinely and are especially helpful if the patient had been on antibiotics prior to surgery as pathogens may not be cultured but antibiotics may still be appropriate Diagnosis of a prosthetic joint infection is confirmed if: Discharging sinus or exposed prosthesis OR Indistinguishable organism in 2 or more deep samples OR Positive histology + negative microbiology & clinical suspicion of infection. Management (see appendix 1 for flow chart) (3): All management must be tailored to the individual patient. Certain frail patients with poor mobility for other reasons may gain little from a new prosthesis and conservative (nonsurgical) management or an excision arthroplasty may be all that is appropriate. In an acute presentation: Implant retention Take blood cultures and aspirate the joint. Give antibiotics only if the patient is haemodynamically unstable. Review in light of the guidelines for the management of severe sepsis: http://nuhnet/diagnostics_clinical_support/antibiotics/pages/septicaemia/septicaemia.asp x Urgent (within 24hrs) open debridement with implant retention is the surgery of choice (DAIR). A washout alone is not enough as outcomes are much poorer than with appropriate debridement (4). If the patient fails to settle then extensive debridement with exchange of modular components is essential. If appropriate debridement is undertaken at this stage other centres report implant retention rates of 80% (4) Take 6 intra-operative samples for microbiology. Once the operative microbiology samples are taken give: Vancomycin IV, refer to antibiotic website for dosing, pre-dose level monitoring advice and the vancomycin dosing calculator. and Meropenem 500mg QDS IV (Do not use meropenem in severe penicillin allergy eg anaphylaxis, immediate onset urticaria or angioedema) until further microbiology is known If the patient has a severe penicillin allergy then give: Nottingham Antimicrobial Guidelines Committee Page 3 of 9 Written: Mr Peter James & Dr Sue Snape

Vancomycin IV, refer to antibiotic website for dosing, pre-dose level monitoring advice and the vancomycin dosing calculator. and Ciprofloxacin 750mg BD PO. Under the guidance of the microbiology team antimicrobials should aim to be given for 6 weeks intravenously then 6 weeks orally. The antimicrobials should be tailored to the bacteria/fungi cultured from the specimens. A PICC line should be inserted in these patients if intravenous antibiotics are possible. Assess whether the patient would be suitable for the Outpatient Parenteral Antibiotic Therapy (OPAT) programme. Contact the OPAT team as soon as possible if a patient is considered eligible so that early assessment and patient education can be started. Please fill in an OPAT referral form available via the intranet type OPAT into the search facility. If you have urgent queries please contact the OPAT coordinator on 07713093409 or email OPAT@nuh.nhs.uk. If a prosthesis is found to be unexpectedly loose it may be necessary to change to a one- or two-stage revision intra-operatively and patients should be consented appropriately. If the patient fails to settle clinically (wound/joint) then repeat the debridement. In a chronic presentation: Implant retention striving for cure (DAIR) If the implant is well fixed and ideally if the microbiology is known then implant retention can be the aim follow the protocol above. Of note this is much less likely to be successful than if the infection is acute and has been present for LESS than 3 weeks. Implant retention striving for suppression / Excision arthroplasty/ Amputation If the implant is loose but the patient is not fit for implant replacement surgery then one of the above may be appropriate. Nottingham Antimicrobial Guidelines Committee Page 4 of 9 Written: Mr Peter James & Dr Sue Snape

Revision Surgery If the implant is loose and hence amenable to revision surgery then whether a 1 stage or a 2 stage procedure will be performed is governed by the following questions: Is the patient high risk? Is there an easy to treat organism involved? Is the patient unsuitable for a 2 stage procedure? If yes - consider a 1 stage procedure. If no - consider a 2 stage procedure. For all revision surgery: Consider pre-op aspirate to define microbiology & antibiotic in cement options. Take 6 intra-operative samples (taken with separate instruments) for microbiology & consider histology if the patient has had previous antibiotics. Consider an intra-operative frozen section if infection uncertain & decision to reimplant may be amended. Resect ALL foreign material & abnormal tissues and consider muscle flap if soft tissues compromised. Empirical broad spectrum antibiotic therapy once all microbiology samples taken: Vancomycin IV, refer to antibiotic website for dosing, pre-dose level monitoring advice and the vancomycin dosing calculator. and Meropenem 500mg QDS IV (do not use meropenem in severe penicillin allergy e.g. anaphylaxis, immediate onset urticaria or angioedema) until further microbiology is known (do not use meropenem in severe penicillin allergy e.g. anaphylaxis, immediate onset urticaria or angioedema). If the patient has a severe penicillin allergy then give: Vancomycin IV, refer to antibiotic website for dosing, pre-dose level monitoring advice and the vancomycin dosing calculator. and Ciprofloxacin 750mg BD PO. Nottingham Antimicrobial Guidelines Committee Page 5 of 9 Written: Mr Peter James & Dr Sue Snape

In a 1 stage revision: Allow antibiotic infusion prior to starting the reimplantation stage. Rescrub, redrape and reimplant. Under the guidance of the microbiology team, for a 1 stage revision antimicrobials should be given for 6 weeks intravenously then 6 weeks orally. The antimicrobials should be tailored to the bacteria/fungi cultured from the specimens. A PICC line should be inserted in these patients if intravenous antibiotics are possible. Assess whether the patient would be suitable for the Outpatient Parenteral Antibiotic Therapy (OPAT) programme. Contact the OPAT team as soon as possible if a patient is considered eligible so that early assessment and patient education can be started. Please fill in an OPAT referral form available via the intranet type OPAT into the search facility. If you have urgent queries please contact the OPAT coordinator on 07713093409 or email OPAT@nuh.nhs.uk. If the patient fails to settle clinically (wound/joint) then may need further revision or resection arthroplasty. In a 2 stage revision: Consider an antibiotic impregnated cement spacer at the 1 st stage. Between the operations antimicrobials should be given for 6 weeks intravenously then if clinically settled stop antibiotics and reimplant the 2 nd stage. An antibiotic free period between stages is not essential (5). Under the guidance of the microbiology team, the antimicrobials should be tailored to the bacteria/fungi cultured from the specimens. A PICC line should be inserted in these patients if intravenous antibiotics are possible. Assess whether the patient would be suitable for the Outpatient Parenteral Antibiotic Therapy (OPAT) programme. Contact the OPAT team as soon as possible if a patient is considered eligible so that early assessment and patient education can be started. Please fill in an OPAT referral form available via the intranet type OPAT into the search facility. If you have urgent queries please contact the OPAT coordinator on 07713093409 or email OPAT@nuh.nhs.uk. If all appears settled at the second stage, microbiology samples should be sent, routine prophylaxis should be given and no further antibiotics should be given. If on reexamination of the soft tissues the site still looks infected then re-debride, send further Nottingham Antimicrobial Guidelines Committee Page 6 of 9 Written: Mr Peter James & Dr Sue Snape

samples to microbiology, restart antibiotics and do not re-implant until the site has settled. Appendix 1 Flow chart (3) Oral antibiotics for 6 weeks (based on culture results under the guidance of microbiology if no growth oral antibiotics are not required) Flow chart summarizing the selection of an appropriate management strategy for an infected prosthetic joint. (*) 1 A negative aspiration does not rule out infection. 2 Consider endocarditis and metastatic osteomyelitis particularly if S. aureus is isolated. 3 DAIR, debridement, antibiotics, implant retention. 4 Empirical antibiotics should be selected on the basis of local susceptibility data. 5 Excision arthroplasty alone may be appropriate in certain patients for either social or technical reasons Nottingham Antimicrobial Guidelines Committee Page 7 of 9 Written: Mr Peter James & Dr Sue Snape

Appendix 2: Monitoring with frequently used antibiotics Rifampicin - Daptomycin Vancomycin Teicoplanin weekly LFTs watch for interactions with other drugs warn patient about orange red urine/ tears/ contact lenses weekly CK don t prescribe with a statin stop the statin and restart after ABx finished use the Trust dosing calculator monitor levels as per the Trust guidelines check U&Es monitor urine output Refer to the antibiotic website monitor levels as per the Trust guidelines check U&Es and FBC Nottingham Antimicrobial Guidelines Committee Page 8 of 9 Written: Mr Peter James & Dr Sue Snape

Audit form for Prosthetic joint infections When the diagnosis was made were the following things recorded in the medical notes: Date of original and subsequent implants Date of onset of symptoms Clinical signs of sepsis Clinical signs of joint infection FBC CRP Blood cultures Joint aspiration and synovial biopsy sent to micro Theatre specimens - 6 samples taken using different forceps and scalpels into different universal tubes and sent to microbiology Theatre specimens histology if on ABx pre surgery Yes No In an acute presentation: Were there clinical signs of severs sepsis Was a washout performed If the aim was implant retention was extensive debridement and change of modular components performed Were empirical antibiotics started in line with guideline once samples taken (or before if septic) Were antibiotics tailored to microbiology advice Was the duration of antibiotics given in line with microbiology advice Was a PICC line inserted Was the patient assessed for OPAT In a chronic presentation: Were there clinical signs of severs sepsis Was a washout performed Was implant retention planned striving for cure Was implant retention planned striving for suppression/excision arthroplasty/amputation Was a 1 stage procedure planned Was a 2 stage procedure planned Were empirical antibiotics started in line with guideline once samples taken (or before if septic) Were antibiotics tailored to microbiology advice Was the duration of antibiotics given in line with microbiology advice Was a PICC line inserted Was the patient assessed for OPAT Yes Yes No No Nottingham Antimicrobial Guidelines Committee Page 9 of 9 Written: Mr Peter James & Dr Sue Snape