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Vascular Graft Infection: Do we
need antimicrobial grafts?
Suat Nail Ömeroğlu
Cardiovascular Surgeon / İ.Ü. Cerrahpaşa Faculty of Medicine,
Turkey
Preventing surgical site infections (SSIs) became a high
priority.
SSIs are the third most common type of health care –
associated infection.
SSIs are associated with
longer postoperative hospital stays,
additional surgical procedures,
admission to intensive care units,
additional medical therapy.
Economic impact of SSIs is significant. In the US, the Center for
Disease Control estimates that hospital costs double for each
patient with a SSI, and the overall costs associated with SSIs are
approximately $10 billion
RD Scott. The Direct Medical Costs of Healthcare-Associated Infections in U.S. Hospitals and the Benefits of
Prevention. Division of Healthcare Quality Promotion National Center for Preparedness, Detection, and Control of
Infectious Diseases Coordinating Center for Infectious Diseases Centers for Disease Control and Prevention,
Atlanta (GA) (2009)
Frequency of SSI
• SSI risk (mean SSI rate 2.48%):
– Carotid artery reconstruction (pooled mean SSI rate: 0.14%)
– Abdominal aorta surgery (pooled mean SSI rate: 1.08%)
– Arterial reconstruction of the lower extremities (pooled mean SSI rate:
3.32%)
Vascular Graft Infection
• Incidence of vascular graft infection range from 0.5% to 6%.
• Morbidity and mortality associated with prosthetic graft infection is high.
– For peripheral vascular prostheses, studies have reported morbidity
rates as high as 41%, with most cases resulting in amputation, and an
attributable mortality of 17%.
– For aortic vascular grafts, the reported mortality rates have ranged from
24% to 75%, with a 5-year survival rate <50%.
Seeger JM: Management of patients with prosthetic vascular graft infections. Am Surg 66:166-177, 2000
Oderich GS, Panneton GM: Aortic graft infections: what have we learnt during the last decades? Acta Cir Belg 102:7-13, 2002
Complications of Prosthetic Graft Infection
• Anastomotic disruption with massive hemorrhage
• Pseudoaneurysm formation
• Graft thrombosis
• Limb loss
• High perioperative and late mortality
Prosthetic Graft Infection
Prosthetic graft infection starts with contamination of the graft and formation
of biofilms. Biofilms result from microbial adhesion to surfaces in moist
environment with sufficient provision of water and nutrients. If the attached
organisms are not immediately separated from the surface or inactivated, they
will start colonizing the surface permanently. Once colonization begins, the
biofilm will grow by a combination of cell division and by genesis of a matrix
of excreted extracellular polymeric substance.
Treatment of infected vascular grafts
• Best treatment remains controversial.
• Early and complete removal of the infected graft, with replacement using
an in situ autologous vein or an extra-anatomic prosthetic bypass.
• Conservative treatment is rarely successful and is used only in high-risk
patients and limited infection.
• The most pre-eminent strategy is primary prevention of vascular graft
infection.
Prevention of Graft Infection
– Preoperative precautions: have the patient shower or scrub with an
antibacterial soap.
– Reduce preoperative stay to minimize the development of skin flora
resistant to commonly used antibiotics.
– Consider any patient attending surgery as being at risk of infection.
– Operative guidelines and aseptic conditions during the operation
– Shorten surgery time,
– Graft protection with muscle flap and multiple layer suture.
– Associated local measures capable of protecting the graft and the
surrounding tissue (Rifampicin soaking, etc.).
Prevention of Graft Infection
• Graft infections still occur.
– There is an increasing prevalence of antibiotic- resistant micro-
organisms, such as methicillin-resistant Staphlococcus Aureus (MRSA)
– Greater than 90% of patients have known risk factors for the
development of graft infection
Efficacy of antibiotic prophylaxis
• 10 RCTs on systemic antibiotics versus placebo demonstrated
a consistent benefit in reduction of wound infection in 1297
patients.
– 6 of 10 RCTs included a case-mix of patients with both prosthetic and
vein grafts. The prophylactic effect of antibiotics is not significant for
prosthetic grafts. It is only statistically significant with vein grafts.
– This meta-analysis mainly investigated β-lactam antibiotics.
Antimicrobial Vascular Grafts
• Antimicrobial compounds need to fulfill a number of distinct requirements:
– Toxicologically safe
– No or limited allergic potency
– Low rate of resorption
– Should not induce bacterial resistance
– Antimicrobially active
Antimicrobial Vascular Grafts
Antibiotic-Bonded Grafts Antiseptic-Impregnated/Coated Grafts
- Vancomycin - Octenidine-dihydrochloride
- Levofloxacin - Polihexanide
- Tobramycin - Triclosan
- Minocycline - Povidone-iodine
- Linezolid - Chitosan
- Levofloxacin-rifampicin - Silver
- Daptomycin-rifampicin
Antimicrobial Silver Grafts
• The first silver-acetate-coated graft (InterGard Silver; Intervascular,
Datascope, Inc, La Ciotat, France) was introduced 13 years ago. It was
designed for routine use in vascular bypass procedures.
• In 2006 another silver-coated device, the B. Braun Silver Graft became
available (B. Braun, Inc, Melsungen, Germany).
• The effectiveness of silver-coated grafts has been shown in-
vitro.
• There are good results with this graft in the aorto-iliaco-
femoral position, but in cases of femorodistal grafting the
difference could not be showed.
New Combination of AntisepticAgents
Combination of two topical antiseptic agents: silver acetate and
triclosan
Triclosan
• Toxicologically safe
• Rapid antimicrobial action
• Leaches rapidly from the graft material
• Metabolized in the liver
• Stable, synthetic, polychlorinated, aromatic hydrocarbon with broad
antimicrobial properties
• Lipophilic and active within a broad pH range (optimum pH, 4-8)
• After exposure it is cleared from the bloodstream in app. 3.8 days.
Triclosan
• Other products that triclosan is used:
– Medicated soap
– Skin antiseptics
– Catheters
– Surgical sutures
– Kitchenware
– Dishwashing liquids
– Dog’s drinking bowls
– Antimicrobial underwear
(A) Silver ions penetrate the bacterial cell wall and bind to the phospholipid layer of the
cytoplasmic membrane. (B) Bind with the bacterial DNA disrupting DNA replication. (C) Impair
the ability of ribosomes to transcribe messenger RNA. (D) Bind to the sulfhydryl group of the
cytochrome b.
(1) Triclosan binds to bacterial enoyl-acyl carrier protein reductase enzyme (ENR). This binding
increases the enzyme’s affinity for nicotinamide adenine dinucleotide (NAD). This results in the
formation of a stable ternary complex of ENR-NAD-triclosan, which is unable to participate in
fatty acid synthesis. Fatty acids are necessary for reproducing and building cell membranes.
Humans do not have an ENR enzyme, and thus are not affected.
Silver collagen and silver triclosan grafts were designed for
inhibiting microbial colonization of the graft during the early
postoperative period only by providing a release of antimicrobial
agents up to 30 days. Whether this is sufficient to prevent
vascular graft infections in unknown.
 Unlike many antibiotics, silver and triclosan are not limited to
one target.
 This is why silver acetate and triclosan do not produce bacterial
resistance and, to date, there are no known reported cases in the
vascular surgery literature of silver or triclosan producing
bacterial strain resistance.
Silver acetate and Triclosan
• The bactericidal efficacy against MRSA was shown in vitro
studies.
• The efficacy of this graft against other bacteria and the in vivo
efficacy must be investigated.
Conclusion
• Vascular graft infection is one of the most serious complications of vascular
surgery.
• Conservative treatment of prosthetic graft infections is rarely successful
and is used in very limited number of patients.
• The most pre-eminent strategy against this severe complication is primary
prevention.
• We really need antimicrobial grafts!
• We still don’t know the best antimicrobial agents for this
purpose!

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Vascular graft infection do we need antimicrobial grafts

  • 1. Vascular Graft Infection: Do we need antimicrobial grafts? Suat Nail Ömeroğlu Cardiovascular Surgeon / İ.Ü. Cerrahpaşa Faculty of Medicine, Turkey
  • 2. Preventing surgical site infections (SSIs) became a high priority. SSIs are the third most common type of health care – associated infection. SSIs are associated with longer postoperative hospital stays, additional surgical procedures, admission to intensive care units, additional medical therapy.
  • 3. Economic impact of SSIs is significant. In the US, the Center for Disease Control estimates that hospital costs double for each patient with a SSI, and the overall costs associated with SSIs are approximately $10 billion RD Scott. The Direct Medical Costs of Healthcare-Associated Infections in U.S. Hospitals and the Benefits of Prevention. Division of Healthcare Quality Promotion National Center for Preparedness, Detection, and Control of Infectious Diseases Coordinating Center for Infectious Diseases Centers for Disease Control and Prevention, Atlanta (GA) (2009)
  • 4. Frequency of SSI • SSI risk (mean SSI rate 2.48%): – Carotid artery reconstruction (pooled mean SSI rate: 0.14%) – Abdominal aorta surgery (pooled mean SSI rate: 1.08%) – Arterial reconstruction of the lower extremities (pooled mean SSI rate: 3.32%)
  • 5. Vascular Graft Infection • Incidence of vascular graft infection range from 0.5% to 6%. • Morbidity and mortality associated with prosthetic graft infection is high. – For peripheral vascular prostheses, studies have reported morbidity rates as high as 41%, with most cases resulting in amputation, and an attributable mortality of 17%. – For aortic vascular grafts, the reported mortality rates have ranged from 24% to 75%, with a 5-year survival rate <50%. Seeger JM: Management of patients with prosthetic vascular graft infections. Am Surg 66:166-177, 2000 Oderich GS, Panneton GM: Aortic graft infections: what have we learnt during the last decades? Acta Cir Belg 102:7-13, 2002
  • 6. Complications of Prosthetic Graft Infection • Anastomotic disruption with massive hemorrhage • Pseudoaneurysm formation • Graft thrombosis • Limb loss • High perioperative and late mortality
  • 7. Prosthetic Graft Infection Prosthetic graft infection starts with contamination of the graft and formation of biofilms. Biofilms result from microbial adhesion to surfaces in moist environment with sufficient provision of water and nutrients. If the attached organisms are not immediately separated from the surface or inactivated, they will start colonizing the surface permanently. Once colonization begins, the biofilm will grow by a combination of cell division and by genesis of a matrix of excreted extracellular polymeric substance.
  • 8. Treatment of infected vascular grafts • Best treatment remains controversial. • Early and complete removal of the infected graft, with replacement using an in situ autologous vein or an extra-anatomic prosthetic bypass. • Conservative treatment is rarely successful and is used only in high-risk patients and limited infection. • The most pre-eminent strategy is primary prevention of vascular graft infection.
  • 9. Prevention of Graft Infection – Preoperative precautions: have the patient shower or scrub with an antibacterial soap. – Reduce preoperative stay to minimize the development of skin flora resistant to commonly used antibiotics. – Consider any patient attending surgery as being at risk of infection. – Operative guidelines and aseptic conditions during the operation – Shorten surgery time, – Graft protection with muscle flap and multiple layer suture. – Associated local measures capable of protecting the graft and the surrounding tissue (Rifampicin soaking, etc.).
  • 10. Prevention of Graft Infection • Graft infections still occur. – There is an increasing prevalence of antibiotic- resistant micro- organisms, such as methicillin-resistant Staphlococcus Aureus (MRSA) – Greater than 90% of patients have known risk factors for the development of graft infection
  • 11. Efficacy of antibiotic prophylaxis • 10 RCTs on systemic antibiotics versus placebo demonstrated a consistent benefit in reduction of wound infection in 1297 patients. – 6 of 10 RCTs included a case-mix of patients with both prosthetic and vein grafts. The prophylactic effect of antibiotics is not significant for prosthetic grafts. It is only statistically significant with vein grafts. – This meta-analysis mainly investigated β-lactam antibiotics.
  • 12. Antimicrobial Vascular Grafts • Antimicrobial compounds need to fulfill a number of distinct requirements: – Toxicologically safe – No or limited allergic potency – Low rate of resorption – Should not induce bacterial resistance – Antimicrobially active
  • 13. Antimicrobial Vascular Grafts Antibiotic-Bonded Grafts Antiseptic-Impregnated/Coated Grafts - Vancomycin - Octenidine-dihydrochloride - Levofloxacin - Polihexanide - Tobramycin - Triclosan - Minocycline - Povidone-iodine - Linezolid - Chitosan - Levofloxacin-rifampicin - Silver - Daptomycin-rifampicin
  • 14. Antimicrobial Silver Grafts • The first silver-acetate-coated graft (InterGard Silver; Intervascular, Datascope, Inc, La Ciotat, France) was introduced 13 years ago. It was designed for routine use in vascular bypass procedures. • In 2006 another silver-coated device, the B. Braun Silver Graft became available (B. Braun, Inc, Melsungen, Germany).
  • 15. • The effectiveness of silver-coated grafts has been shown in- vitro. • There are good results with this graft in the aorto-iliaco- femoral position, but in cases of femorodistal grafting the difference could not be showed.
  • 16. New Combination of AntisepticAgents Combination of two topical antiseptic agents: silver acetate and triclosan
  • 17. Triclosan • Toxicologically safe • Rapid antimicrobial action • Leaches rapidly from the graft material • Metabolized in the liver • Stable, synthetic, polychlorinated, aromatic hydrocarbon with broad antimicrobial properties • Lipophilic and active within a broad pH range (optimum pH, 4-8) • After exposure it is cleared from the bloodstream in app. 3.8 days.
  • 18. Triclosan • Other products that triclosan is used: – Medicated soap – Skin antiseptics – Catheters – Surgical sutures – Kitchenware – Dishwashing liquids – Dog’s drinking bowls – Antimicrobial underwear
  • 19. (A) Silver ions penetrate the bacterial cell wall and bind to the phospholipid layer of the cytoplasmic membrane. (B) Bind with the bacterial DNA disrupting DNA replication. (C) Impair the ability of ribosomes to transcribe messenger RNA. (D) Bind to the sulfhydryl group of the cytochrome b. (1) Triclosan binds to bacterial enoyl-acyl carrier protein reductase enzyme (ENR). This binding increases the enzyme’s affinity for nicotinamide adenine dinucleotide (NAD). This results in the formation of a stable ternary complex of ENR-NAD-triclosan, which is unable to participate in fatty acid synthesis. Fatty acids are necessary for reproducing and building cell membranes. Humans do not have an ENR enzyme, and thus are not affected.
  • 20. Silver collagen and silver triclosan grafts were designed for inhibiting microbial colonization of the graft during the early postoperative period only by providing a release of antimicrobial agents up to 30 days. Whether this is sufficient to prevent vascular graft infections in unknown.
  • 21.  Unlike many antibiotics, silver and triclosan are not limited to one target.  This is why silver acetate and triclosan do not produce bacterial resistance and, to date, there are no known reported cases in the vascular surgery literature of silver or triclosan producing bacterial strain resistance.
  • 22.
  • 23. Silver acetate and Triclosan • The bactericidal efficacy against MRSA was shown in vitro studies. • The efficacy of this graft against other bacteria and the in vivo efficacy must be investigated.
  • 24. Conclusion • Vascular graft infection is one of the most serious complications of vascular surgery. • Conservative treatment of prosthetic graft infections is rarely successful and is used in very limited number of patients. • The most pre-eminent strategy against this severe complication is primary prevention.
  • 25. • We really need antimicrobial grafts! • We still don’t know the best antimicrobial agents for this purpose!