Editorial
Reducing Catheter-Related Infections in Hemodialysis Patients Daniel Landry and Gregory Braden
Clin J Am Soc Nephrol 9: 1156–1159, 2014. doi: 10.2215/CJN.04700514
Not all hemodialysis accesses are created equal: Compared with patients with ESRD who have an arteriovenous fistula, those with a tunneled central venous catheter have a 15-fold increased risk of catheterrelated bloodstream infection (CRBSI) and an all-cause mortality rate ranging from 12% to 25% (1,2). Ten percent to 20% of CRBSIs are associated with metastatic complications, such as endocarditis, septic arthritis, and epidural abscess, and they cause considerable financial and physical burdens from catheter loss, repeated access procedures, and hospital admissions (2). A single-center study found that a CRBSI resulted in an average hospital stay of 11 days and cost approximately $23,000 (3); several other studies support these data (4,5). Despite the Fistula First Initiative, nearly 80% of patients initiate hemodialysis with a central venous catheter (6). Efforts to reduce CRBSI have focused on comprehensive catheter management protocols and the use of antimicrobial catheter lock solutions. In 2011, the Centers for Disease Control and Prevention (CDC) published a list of core interventions aimed at decreasing the incidence of CRBSI (7). These measures include the use of chlorhexidine skin antisepsis at the catheter exit site, catheter hub disinfection, and the application of triple antibiotic (or povidone iodine) ointment to catheter exit sites during dressing changes. Similar “bundled” care efforts in intensive care units have shown dramatic decreases in nondialysis CRBSI rates (8,9). The CDC Dialysis Collaborative used a comprehensive dialysis catheter management protocol in 17 outpatient dialysis units and found a 54% reduction (P,0.001) in CRBSI during the 15-month intervention period (10). More than 15 years of experience with antimicrobial lock solutions has still not led to a consensus regarding their use for CRBSI prevention. Boyce recently reviewed all antimicrobial lock studies (antibiotic- and non–antibiotic-based) performed from 1999 to 2012 and concluded that antimicrobial locks should be used for CRBSI prevention in all hemodialysis units (11). In addition, five meta-analyses or systematic reviews (12–16) published during this time period indicate significant reductions in CRBSI; in particular, two meta-analyses reported a number needed to treat to prevent one CRBSI of 3 to 4 (12,13). Most of the included studies compared an antimicrobial lock with heparin as the 1156
Copyright © 2014 by the American Society of Nephrology
control and used different protocols for general catheter care, such that infection rates in the control groups were approximately 3 per 1000 catheter-days. Because more recent studies using bundled care without antimicrobial locks have achieved CRBSI rates of #1 per 1000 catheter-days, can the use of antimicrobial locks further reduce CRBSI? Abbas et al. performed an observational study of gentamicin-heparin versus heparin catheter locks, while Maki and Moran and their colleagues performed randomized controlled trials with gentamicin-trisodium citrate (citrate) and citrate– methylene blue–methylparaben–propylparaben, respectively (17–19). All three studies achieved CRBSI rates of ,1 per 1000 catheter-days in their control groups and yet still showed a significant decrease in infection rates with their interventions (Abbas, Moran, and Maki et al. reported rates of 0.62, 0.28, and 0.24 events per 1000 catheter-days, respectively). However, two major unanswered questions remain: (1) Does the routine use of antimicrobial locks in dialysis patients with tunneled central venous catheters lead to a mortality benefit, and (2) is there risk of antibiotic resistance in patients using antibiotic-based lock solutions? In this issue of CJASN, Moore et al. try to answer these questions (20). The authors conducted a prospective, multicenter, observational cohort study in a metropolitan area to compare the effectiveness of a gentamicin-citrate lock versus heparin in 555 hemodialysis patients undergoing dialysis with a tunneled central venous catheter between 2008 and 2011. During the study period, three of the outpatient dialysis units crossed over from heparin to gentamicincitrate lock at different times. Historical controls were compared with antimicrobial lock data. The comprehensive catheter management protocol used in both the historical and the antimicrobial lock time periods was similar to the 2011 CDC list of core interventions. This included the use of a triple antibiotic ointment (bacitracin, neomycin, and polymyxin B) on the exit site in all patients during the entire study period. The dose of gentamicin (0.32 mg/ml) used with 4% citrate was considered low compared with the dose used in many other trials (4 mg/ml). The authors report a reduced rate of CRBSI in the antibiotic lock period of 0.45 per 1000 catheter-days compared with 1.68 events during the heparin period (P50.001), which was maintained after multivariate adjustment (adjusted relative
Renal Division, Tufts University School of Medicine, Baystate Medical Center, Springfield, Massachusetts Correspondence: Dr. Gregory Braden, Renal Division, Tufts University School of Medicine, Baystate Medical Center, 759 Chestnut Street, Springfield, MA 01199. Email Gregory. Braden@ baystatehealth.org
www.cjasn.org Vol 9 July, 2014
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Editorial: Reducing Catheter-Related Infections in Hemodialysis Patients, Landry and Braden
risk, 0.23; 95% confidence interval, 0.13 to 0.38). The use of gentamicin-citrate lock was also associated with a significant reduction in all-cause mortality (0.32; 95% confidence interval, 0.14 to 0.75 after multivariate adjustment). Moore’s group also addressed the issue of antibiotic resistance by conducting in vitro gentamicin susceptibility testing on each blood bacterial isolate in one central microbiology laboratory. Gentamicin resistance rates decreased from 0.40 per 1000 person-years in the heparin period to 0.22 per 1000 person-years in the antimicrobial lock period (P50.01). The authors do not report the outcomes of the patients with gentamicin-resistant CRBSI, but their comparison of gentamicin resistance to a nonantimicrobial lock period certainly is a strength of their study. Unfortunately, the duration of follow-up after the initiation of the gentamicincitrate lock was only 7–8 months in two of their three centers. The authors suggest that either the low dose of gentamicin used in their study or the avoidance of heparin— which is known to increase the production of biofilm—may have played a role in the decrease in gentamicin resistance. Moreover, another prospective, randomized controlled study of low-dose gentamicin (0.32 mg/ml) and citrate lock likewise found no significant change in gentamicin resistance during a 5-year period or in the ensuing 3 years when the lock solution was universally implemented (19). In contrast, our own published data were the first to raise the important question of antibiotic resistance with gentamicin lock. Our observational study of .1400 patients followed for .4 years used heparin with a high-dose gentamicin locking solution (4 mg/ml) but did not have comparison resistance data from a historical control period (21). We used povidone-iodine rather than chlorhexidine as the skin antiseptic and covered the exit site with mupirocin, which has been associated with bacterial resistance (22). Another group found gentamicin resistance in their uncontrolled, observational study of 320 patients using 1 mg/ml gentamicin with heparin during a 3-year period (23), while Venditto et al. reported increased gentamicin resistance to Enterobacteriaceae (but none to Staphylococcus aureus) isolates during their study of 6-month sequential antimicrobial locks consisting of heparin, 47% citrate, and then gentamicin (2 mg/ml) with heparin (24). Alternatives to antibiotic-based lock solutions have been studied for the purpose of eliminating the risk of antibiotic resistance. Several authors have evaluated citrate, but in some studies higher doses (47%) have failed to outperform heparin and have also raised concerns about the possibility of fatal arrhythmias induced by hypocalcemia or systemic emboli from catheter leakage (25,26). However, a recent meta-analysis by Zhao et al. indicated that low-to-moderate concentrations of citrate (1.04%–7%) appear to be of benefit in decreasing the risk for CRBSI (27). The combination of citrate with other novel antimicrobials, such as taurolidine (28–31) and methylene blue–methylparaben–propylparaben, has shown efficacy in reducing CRBSI, but issues with catheter thrombosis have limited their use (18). Hemmelgarn et al. reported successful reduction in CRBSI with the use of once-weekly tissue plasminogen activator, but the longterm cost of this strategy is prohibitive (32). Ethanol locking solutions are effective sterilizing agents for CRBSI prophylaxis, as well as for salvage in silicone-based central venous catheters of oncology patients and pediatric patients
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receiving parenteral nutrition (33). However, safety of ethanol in polyurethane-based hemodialysis catheters has been an ongoing concern. We have shown that carbothane and silicone-based hemodialysis catheters can be exposed to 70% ethanol lock in vitro for at least 6 months without any evidence of damage to catheter integrity (data not shown). This has been supported by the work of Crnich et al. (34), who studied the in vitro mechanical properties of silicone and polyurethane peripherally inserted central catheters exposed to 70% ethanol during a 10-week period. The HEALTHYCATH trial was the first prospective, open-label, randomized, controlled trial in hemodialysis patients using once-weekly 70% ethanol lock (with two heparin locks between other dialysis sessions) versus thrice-per-week heparin lock for the control. This proof of concept study showed no significant difference in CRBSI (0.85 versus 0.28 events/1000 catheter-days in heparin versus ethanol groups; P50.12), but the study was underpowered because of low recruitment. The authors did not report catheter integrity issues but also did not mention the type of dialysis catheters used (35). Should antimicrobial locks be used to reduce CRBSI? Moore and colleagues have made a significant contribution showing evidence of a mortality benefit—without the development of gentamicin resistance—with use of gentamicincitrate lock. The issue of developing gentamicin resistance may not be completely answered, but the preponderance of data would now suggest that low-dose gentamicin used with 4% citrate is safe. The CDC and the Infectious Diseases Society of America do not recommend the routine use of antimicrobial lock in hemodialysis patients dialyzed with a central venous catheter. They suggest reserving this treatment for patients with a history of multiple CRBSIs, citing concerns for the potential emergence of antibiotic resistance (36). In contrast, the European Best Practices Report has concluded that the effectiveness of antimicrobial lock to reduce CRBSI outweighs any potential risk and recommends prophylactic antimicrobial lock use in all patients with ESRD who have tunneled central venous catheters (37). If the “typical” CRBSI is associated with a 12%–25% risk of mortality and considerable cost to the health care system, the real question in 2014 is which locking solution we should use to prevent CRBSI, rather than whether to use a locking solution at all. Prospective, randomized controlled trials are needed comparing the newest antimicrobial locks in order to determine the one best suited to prevent CRBSI with the least propensity for the development of bacterial resistance. For now, we prefer to use low-dose gentamicin-citrate locks for CRBSI prevention in all patients with ESRD who have a tunneled central venous catheter. Disclosures None. References 1. Ravani P, Palmer SC, Oliver MJ, Quinn RR, MacRae JM, Tai DJ, Pannu NI, Thomas C, Hemmelgarn BR, Craig JC, Manns B, Tonelli M, Strippoli GF, James MT: Associations between hemodialysis access type and clinical outcomes: A systematic review. J Am Soc Nephrol 24: 465–473, 2013 2. Allon M: Dialysis catheter-related bacteremia: Treatment and prophylaxis. Am J Kidney Dis 44: 779–791, 2004 3. O’Grady NP, Alexander M, Dellinger EP, Gerberding JL, Heard SO, Maki DG, Masur H, McCormick RD, Mermel LA, Pearson
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ML, Raad II, Randolph A, Weinstein RA; Centers for Disease Control and Prevention: Guidelines for the prevention of intravascular catheter-related infections. MMWR Recomm Rep 51 [RR-10]: 1–29, 2002 Inrig JK, Reed SD, Szczech LA, Engemann JJ, Friedman JY, Corey GR, Schulman KA, Reller LB, Fowler VG Jr: Relationship between clinical outcomes and vascular access type among hemodialysis patients with Staphylococcus aureus bacteremia. Clin J Am Soc Nephrol 1: 518–524, 2006 Engemann JJ, Friedman JY, Reed SD, Griffiths RI, Szczech LA, Kaye KS, Stryjewski ME, Reller LB, Schulman KA, Corey GR, Fowler VG Jr: Clinical outcomes and costs due to Staphylococcus aureus bacteremia among patients receiving long-term hemodialysis. Infect Control Hosp Epidemiol 26: 534–539, 2005 Xue H, Ix JH, Wang W, Brunelli SM, Lazarus M, Hakim R, Lacson E Jr: Hemodialysis access usage patterns in the incident dialysis year and associated catheter-related complications. Am J Kidney Dis 61: 123–130, 2013 Centers for Disease Control and Prevention: CDC Approach to BSI Prevention in Dialysis Facilities (i.e., the Core Interventions for Dialysis Bloodstream Infection (BSI) Prevention). May 13, 2013. Available at: http://www.cdc.gov/dialysis/preventiontools/core-interventions.html. Accessed May 5, 2014 Pronovost P, Needham D, Berenholtz S, Sinopoli D, Chu H, Cosgrove S, Sexton B, Hyzy R, Welsh R, Roth G, Bander J, Kepros J, Goeschel C: An intervention to decrease catheter-related bloodstream infections in the ICU. N Engl J Med 355: 2725–2732, 2006 Patel PR, Yi SH, Booth S, Bren V, Downham G, Hess S, Kelley K, Lincoln M, Morrissette K, Lindberg C, Jernigan JA, Kallen AJ: Bloodstream infection rates in outpatient hemodialysis facilities participating in a collaborative prevention effort: A quality improvement report. Am J Kidney Dis 62: 322–330, 2013 Berenholtz SM, Pronovost PJ, Lipsett PA, Hobson D, Earsing K, Farley JE, Milanovich S, Garrett-Mayer E, Winters BD, Rubin HR, Dorman T, Perl TM: Eliminating catheter-related bloodstream infections in the intensive care unit. Crit Care Med 32: 2014–2020, 2004 Boyce JM: Prevention of central line-associated bloodstream infections in hemodialysis patients. Infect Control Hosp Epidemiol 33: 936–944, 2012 Yahav D, Rozen-Zvi B, Gafter-Gvili A, Leibovici L, Gafter U, Paul M: Antimicrobial lock solutions for the prevention of infections associated with intravascular catheters in patients undergoing hemodialysis: Systematic review and metaanalysis of randomized, controlled trials. Clin Infect Dis 47: 83–93, 2008 Snaterse M, Ruger W: Scholte op Reimer WJM, Lucas C: Antibiotic-based catheter lock solutions for prevention of catheter-related bloodstream infection: A systematic review of randomized controlled trials. J Hosp Infect 75: 1–11, 2010 Labriola L, Crott R, Jadoul M: Preventing haemodialysis catheterrelated bacteraemia with an antimicrobial lock solution: A meta-analysis of prospective randomized trials. Nephrol Dial Transplant 23: 1666–1672, 2008 Jaffer Y, Selby NM, Taal MW, Fluck RJ, McIntyre CW: A metaanalysis of hemodialysis catheter locking solutions in the prevention of catheter-related infection. Am J Kidney Dis 51: 233–241, 2008 James MT, Conley J, Tonelli M, Manns BJ, MacRae J, Hemmelgarn BR; Alberta Kidney Disease Network: Meta-analysis: Antibiotics for prophylaxis against hemodialysis catheter-related infections. Ann Intern Med 148: 596–605, 2008 Abbas SA, Haloob IA, Taylor SL, Curry EM, King BB, Van der Merwe WM, Marshall MR: Effect of antimicrobial locks for tunneled hemodialysis catheters on bloodstream infection and bacterial resistance: A quality improvement report. Am J Kidney Dis 53: 492–502, 2009 Maki DG, Ash SR, Winger RK, Lavin P; AZEPTIC Trial Investigators: A novel antimicrobial and antithrombotic lock solution for hemodialysis catheters: A multi-center, controlled, randomized trial. Crit Care Med 39: 613–620, 2011
19. Moran J, Sun S, Khababa I, Pedan A, Doss S, Schiller B: A randomized trial comparing gentamicin/citrate and heparin locks for central venous catheters in maintenance hemodialysis patients. Am J Kidney Dis 59: 102–107, 2012 20. Moore CL, Besarab A, Ajluni M, Soi V, Peterson EL, Johnson LE, Zervos MJ, Adams E, Yee J: Comparative effectiveness of two catheter locking solutions to reduce catheter related bloodstream infection in hemodialysis patients. Clin J Am Soc Nephrol 9: 1232–1239, 2014 21. Landry DL, Braden GL, Gobeille SL, Haessler SD, Vaidya CK, Sweet SJ: Emergence of gentamicin-resistant bacteremia in hemodialysis patients receiving gentamicin lock catheter prophylaxis. Clin J Am Soc Nephrol 5: 1799–1804, 2010 22. Johnson DW, van Eps C, Mudge DW, Wiggins KJ, Armstrong K, Hawley CM, Campbell SB, Isbel NM, Nimmo GR, Gibbs H: Randomized, controlled trial of topical exit-site application of honey (Medihoney) versus mupirocin for the prevention of catheter-associated infections in hemodialysis patients. J Am Soc Nephrol 16: 1456–1462, 2005 23. Ferna´ndez-Gallego J, Martı´n M, Gutie´rrez E, Cobelo C, Frı´as P, Jironda C, Hidalgo P, Jime´nez T: Prophylaxis with gentamicin locking of chronic tunnelled central venous catheters does not cause bacterial resistance. Nefrologia 31: 308–312, 2011 24. Venditto M, du Montcel ST, Robert J, Trystam D, Dighiero J, Hue D, Bessette C, Deray G, Mercadal L: Effect of catheter-lock solutions on catheter-related infection and inflammatory syndrome in hemodialysis patients: Heparin versus citrate 46% versus heparin/gentamicin. Blood Purif 29: 268–273, 2010 25. FDA issues warning on triCitrasol dialysis catheter anticoagulant. FDA Talk Paper T00–16, Rockville, MD, US Food and Drug Administration, 2000 26. Willicombe MK, Vernon K, Davenport A: Embolic complications from central venous hemodialysis catheters used with hypertonic citrate locking solution. Am J Kidney Dis 55: 348–351, 2010 27. Zhao Y, Li Z, Zhang L, Yang J, Yang Y, Tang Y, Fu P: Citrate versus heparin lock for hemodialysis catheters: A systematic review and meta-analysis of randomized controlled trials. Am J Kidney Dis 63: 479–490, 2014 28. Solomon LR, Cheesbrough JS, Ebah L, Al-Sayed T, Heap M, Millband N, Waterhouse D, Mitra S, Curry A, Saxena R, Bhat R, Schulz M, Diggle P: A randomized double-blind controlled trial of taurolidine-citrate catheter locks for the prevention of bacteremia in patients treated with hemodialysis. Am J Kidney Dis 55: 1060–1068, 2010 29. Allon M: Prophylaxis against dialysis catheter-related bacteremia with a novel antimicrobial lock solution. Clin Infect Dis 36: 1539–1544, 2003 30. Betjes MG, van Agteren M: Prevention of dialysis catheter-related sepsis with a citrate-taurolidine-containing lock solution. Nephrol Dial Transplant 19: 1546–1551, 2004 31. Geron R, Tanchilevski O, Kristal B: [Catheter lock solution— taurolock for prevention of catheter-related bacteremia in hemodialysis patients]. Harefuah 145: 881–884, 943, 2006 32. Hemmelgarn BR, Moist LM, Lok CE, Tonelli M, Manns BJ, Holden RM, LeBlanc M, Faris P, Barre P, Zhang J, Scott-Douglas N, ScottDouglas N; Prevention of Dialysis Catheter Lumen Occlusion with rt-PA versus Heparin Study Group: Prevention of dialysis catheter malfunction with recombinant tissue plasminogen activator. N Engl J Med 364: 303–312, 2011 33. Maiefski M, Rupp ME, Hermsen ED: Ethanol lock technique: Review of the literature. Infect Control Hosp Epidemiol 30: 1096–1108, 2009 34. Crnich CJ, Halfmann JA, Crone WC, Maki DG: The effects of prolonged ethanol exposure on the mechanical properties of polyurethane and silicone catheters used for intravascular access. Infect Control Hosp Epidemiol 26: 708–714, 2005 35. Broom JK, Krishnasamy R, Hawley CM, Playford EG, Johnson DW: A randomised controlled trial of Heparin versus EthAnol Lock THerapY for the prevention of Catheter Associated
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infecTion in Haemodialysis patients—the HEALTHY-CATH trial. BMC Nephrol 13: 146, 2012 36. O’Grady NP, Alexander M, Burns LA, Dellinger EP, Garland J, Heard SO, Lipsett PA, Masur H, Mermel LA, Pearson ML, Raad II, Randolph AG, Rupp ME, Saint S; Healthcare Infection Control Practices Advisory Committee (HICPAC): Guidelines for the prevention of intravascular catheterrelated infections. Clin Infect Dis 52: e162–e193, 2011 37. Vanholder R, Canaud B, Fluck R, Jadoul M, Labriola L, Marti-Monros A, Tordoir J, Van Biesen W: Diagnosis, prevention and treatment of
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haemodialysis catheter-related bloodstream infections (CRBSI): A position statement of European Renal Best Practice (ERBP). NDT Plus 3: 234–246, 2010 Published online ahead of print. Publication date available at www. cjasn.org. See related article, “Comparative Effectiveness of Two Catheter Locking Solutions to Reduce Catheter-Related Bloodstream Infection in Hemodialysis Patients,” on pages 1232–1239.
Reducing Catheter-Related Infections in Hemodialysis Patients Daniel Landry and Gregory Braden
Clin J Am Soc Nephrol 9: 1156–1159, 2014. doi: 10.2215/CJN.04700514
Not all hemodialysis accesses are created equal: Compared with patients with ESRD who have an arteriovenous fistula, those with a tunneled central venous catheter have a 15-fold increased risk of catheterrelated bloodstream infection (CRBSI) and an all-cause mortality rate ranging from 12% to 25% (1,2). Ten percent to 20% of CRBSIs are associated with metastatic complications, such as endocarditis, septic arthritis, and epidural abscess, and they cause considerable financial and physical burdens from catheter loss, repeated access procedures, and hospital admissions (2). A single-center study found that a CRBSI resulted in an average hospital stay of 11 days and cost approximately $23,000 (3); several other studies support these data (4,5). Despite the Fistula First Initiative, nearly 80% of patients initiate hemodialysis with a central venous catheter (6). Efforts to reduce CRBSI have focused on comprehensive catheter management protocols and the use of antimicrobial catheter lock solutions. In 2011, the Centers for Disease Control and Prevention (CDC) published a list of core interventions aimed at decreasing the incidence of CRBSI (7). These measures include the use of chlorhexidine skin antisepsis at the catheter exit site, catheter hub disinfection, and the application of triple antibiotic (or povidone iodine) ointment to catheter exit sites during dressing changes. Similar “bundled” care efforts in intensive care units have shown dramatic decreases in nondialysis CRBSI rates (8,9). The CDC Dialysis Collaborative used a comprehensive dialysis catheter management protocol in 17 outpatient dialysis units and found a 54% reduction (P,0.001) in CRBSI during the 15-month intervention period (10). More than 15 years of experience with antimicrobial lock solutions has still not led to a consensus regarding their use for CRBSI prevention. Boyce recently reviewed all antimicrobial lock studies (antibiotic- and non–antibiotic-based) performed from 1999 to 2012 and concluded that antimicrobial locks should be used for CRBSI prevention in all hemodialysis units (11). In addition, five meta-analyses or systematic reviews (12–16) published during this time period indicate significant reductions in CRBSI; in particular, two meta-analyses reported a number needed to treat to prevent one CRBSI of 3 to 4 (12,13). Most of the included studies compared an antimicrobial lock with heparin as the 1156
Copyright © 2014 by the American Society of Nephrology
control and used different protocols for general catheter care, such that infection rates in the control groups were approximately 3 per 1000 catheter-days. Because more recent studies using bundled care without antimicrobial locks have achieved CRBSI rates of #1 per 1000 catheter-days, can the use of antimicrobial locks further reduce CRBSI? Abbas et al. performed an observational study of gentamicin-heparin versus heparin catheter locks, while Maki and Moran and their colleagues performed randomized controlled trials with gentamicin-trisodium citrate (citrate) and citrate– methylene blue–methylparaben–propylparaben, respectively (17–19). All three studies achieved CRBSI rates of ,1 per 1000 catheter-days in their control groups and yet still showed a significant decrease in infection rates with their interventions (Abbas, Moran, and Maki et al. reported rates of 0.62, 0.28, and 0.24 events per 1000 catheter-days, respectively). However, two major unanswered questions remain: (1) Does the routine use of antimicrobial locks in dialysis patients with tunneled central venous catheters lead to a mortality benefit, and (2) is there risk of antibiotic resistance in patients using antibiotic-based lock solutions? In this issue of CJASN, Moore et al. try to answer these questions (20). The authors conducted a prospective, multicenter, observational cohort study in a metropolitan area to compare the effectiveness of a gentamicin-citrate lock versus heparin in 555 hemodialysis patients undergoing dialysis with a tunneled central venous catheter between 2008 and 2011. During the study period, three of the outpatient dialysis units crossed over from heparin to gentamicincitrate lock at different times. Historical controls were compared with antimicrobial lock data. The comprehensive catheter management protocol used in both the historical and the antimicrobial lock time periods was similar to the 2011 CDC list of core interventions. This included the use of a triple antibiotic ointment (bacitracin, neomycin, and polymyxin B) on the exit site in all patients during the entire study period. The dose of gentamicin (0.32 mg/ml) used with 4% citrate was considered low compared with the dose used in many other trials (4 mg/ml). The authors report a reduced rate of CRBSI in the antibiotic lock period of 0.45 per 1000 catheter-days compared with 1.68 events during the heparin period (P50.001), which was maintained after multivariate adjustment (adjusted relative
Renal Division, Tufts University School of Medicine, Baystate Medical Center, Springfield, Massachusetts Correspondence: Dr. Gregory Braden, Renal Division, Tufts University School of Medicine, Baystate Medical Center, 759 Chestnut Street, Springfield, MA 01199. Email Gregory. Braden@ baystatehealth.org
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Editorial: Reducing Catheter-Related Infections in Hemodialysis Patients, Landry and Braden
risk, 0.23; 95% confidence interval, 0.13 to 0.38). The use of gentamicin-citrate lock was also associated with a significant reduction in all-cause mortality (0.32; 95% confidence interval, 0.14 to 0.75 after multivariate adjustment). Moore’s group also addressed the issue of antibiotic resistance by conducting in vitro gentamicin susceptibility testing on each blood bacterial isolate in one central microbiology laboratory. Gentamicin resistance rates decreased from 0.40 per 1000 person-years in the heparin period to 0.22 per 1000 person-years in the antimicrobial lock period (P50.01). The authors do not report the outcomes of the patients with gentamicin-resistant CRBSI, but their comparison of gentamicin resistance to a nonantimicrobial lock period certainly is a strength of their study. Unfortunately, the duration of follow-up after the initiation of the gentamicincitrate lock was only 7–8 months in two of their three centers. The authors suggest that either the low dose of gentamicin used in their study or the avoidance of heparin— which is known to increase the production of biofilm—may have played a role in the decrease in gentamicin resistance. Moreover, another prospective, randomized controlled study of low-dose gentamicin (0.32 mg/ml) and citrate lock likewise found no significant change in gentamicin resistance during a 5-year period or in the ensuing 3 years when the lock solution was universally implemented (19). In contrast, our own published data were the first to raise the important question of antibiotic resistance with gentamicin lock. Our observational study of .1400 patients followed for .4 years used heparin with a high-dose gentamicin locking solution (4 mg/ml) but did not have comparison resistance data from a historical control period (21). We used povidone-iodine rather than chlorhexidine as the skin antiseptic and covered the exit site with mupirocin, which has been associated with bacterial resistance (22). Another group found gentamicin resistance in their uncontrolled, observational study of 320 patients using 1 mg/ml gentamicin with heparin during a 3-year period (23), while Venditto et al. reported increased gentamicin resistance to Enterobacteriaceae (but none to Staphylococcus aureus) isolates during their study of 6-month sequential antimicrobial locks consisting of heparin, 47% citrate, and then gentamicin (2 mg/ml) with heparin (24). Alternatives to antibiotic-based lock solutions have been studied for the purpose of eliminating the risk of antibiotic resistance. Several authors have evaluated citrate, but in some studies higher doses (47%) have failed to outperform heparin and have also raised concerns about the possibility of fatal arrhythmias induced by hypocalcemia or systemic emboli from catheter leakage (25,26). However, a recent meta-analysis by Zhao et al. indicated that low-to-moderate concentrations of citrate (1.04%–7%) appear to be of benefit in decreasing the risk for CRBSI (27). The combination of citrate with other novel antimicrobials, such as taurolidine (28–31) and methylene blue–methylparaben–propylparaben, has shown efficacy in reducing CRBSI, but issues with catheter thrombosis have limited their use (18). Hemmelgarn et al. reported successful reduction in CRBSI with the use of once-weekly tissue plasminogen activator, but the longterm cost of this strategy is prohibitive (32). Ethanol locking solutions are effective sterilizing agents for CRBSI prophylaxis, as well as for salvage in silicone-based central venous catheters of oncology patients and pediatric patients
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receiving parenteral nutrition (33). However, safety of ethanol in polyurethane-based hemodialysis catheters has been an ongoing concern. We have shown that carbothane and silicone-based hemodialysis catheters can be exposed to 70% ethanol lock in vitro for at least 6 months without any evidence of damage to catheter integrity (data not shown). This has been supported by the work of Crnich et al. (34), who studied the in vitro mechanical properties of silicone and polyurethane peripherally inserted central catheters exposed to 70% ethanol during a 10-week period. The HEALTHYCATH trial was the first prospective, open-label, randomized, controlled trial in hemodialysis patients using once-weekly 70% ethanol lock (with two heparin locks between other dialysis sessions) versus thrice-per-week heparin lock for the control. This proof of concept study showed no significant difference in CRBSI (0.85 versus 0.28 events/1000 catheter-days in heparin versus ethanol groups; P50.12), but the study was underpowered because of low recruitment. The authors did not report catheter integrity issues but also did not mention the type of dialysis catheters used (35). Should antimicrobial locks be used to reduce CRBSI? Moore and colleagues have made a significant contribution showing evidence of a mortality benefit—without the development of gentamicin resistance—with use of gentamicincitrate lock. The issue of developing gentamicin resistance may not be completely answered, but the preponderance of data would now suggest that low-dose gentamicin used with 4% citrate is safe. The CDC and the Infectious Diseases Society of America do not recommend the routine use of antimicrobial lock in hemodialysis patients dialyzed with a central venous catheter. They suggest reserving this treatment for patients with a history of multiple CRBSIs, citing concerns for the potential emergence of antibiotic resistance (36). In contrast, the European Best Practices Report has concluded that the effectiveness of antimicrobial lock to reduce CRBSI outweighs any potential risk and recommends prophylactic antimicrobial lock use in all patients with ESRD who have tunneled central venous catheters (37). If the “typical” CRBSI is associated with a 12%–25% risk of mortality and considerable cost to the health care system, the real question in 2014 is which locking solution we should use to prevent CRBSI, rather than whether to use a locking solution at all. Prospective, randomized controlled trials are needed comparing the newest antimicrobial locks in order to determine the one best suited to prevent CRBSI with the least propensity for the development of bacterial resistance. For now, we prefer to use low-dose gentamicin-citrate locks for CRBSI prevention in all patients with ESRD who have a tunneled central venous catheter. Disclosures None. References 1. Ravani P, Palmer SC, Oliver MJ, Quinn RR, MacRae JM, Tai DJ, Pannu NI, Thomas C, Hemmelgarn BR, Craig JC, Manns B, Tonelli M, Strippoli GF, James MT: Associations between hemodialysis access type and clinical outcomes: A systematic review. J Am Soc Nephrol 24: 465–473, 2013 2. Allon M: Dialysis catheter-related bacteremia: Treatment and prophylaxis. Am J Kidney Dis 44: 779–791, 2004 3. O’Grady NP, Alexander M, Dellinger EP, Gerberding JL, Heard SO, Maki DG, Masur H, McCormick RD, Mermel LA, Pearson
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haemodialysis catheter-related bloodstream infections (CRBSI): A position statement of European Renal Best Practice (ERBP). NDT Plus 3: 234–246, 2010 Published online ahead of print. Publication date available at www. cjasn.org. See related article, “Comparative Effectiveness of Two Catheter Locking Solutions to Reduce Catheter-Related Bloodstream Infection in Hemodialysis Patients,” on pages 1232–1239.
