Abstract
Background
Surgical site infection (SSI) is a common type of healthcare-associated infection in gastrointestinal (GI) surgical procedures, which often has major consequences for patient recovery and increased healthcare costs due to prolonged hospital stay. This article provides an overview of the efficacy and safety of prophylactic application of resorbable gentamicin-containing collagen implants (GCI) in the prevention of SSI following high-risk GI surgical procedures.
Method
Nine publications were identified using the PubMed online database and search terms ‘gentamicin collagen implant’ plus ‘surgical site infection’, ‘wound infection’ and ‘gastrointestinal surgery’.
Results
Data from 483 patients treated prophylactically have demonstrated that GCI can reduce the wound infection rate in high-risk GI surgical procedures and improve wound healing after pilonidal sinus excision. In a study of 221 patients who underwent colorectal surgery, the wound infection rate was reduced to 5.6% in the GCI group compared to 18.4% in the control group (P < 0.01). GCI also positively influences the post-operative course for patients undergoing particularly risky procedures e.g. abdominoperineal resection (APR) combined with neoadjuvant radiotherapy. In one such patient series, GCI reduced the wound infection rate by over 70% and the length of hospital stay by 40%. Few side effects of GCI were noted in the 9 clinical studies.
Conclusions
This review demonstrates that GCI can have a positive effect on wound infection rates in high-risk GI surgery and can also improve wound healing after pilonidal sinus excision.
Keywords: Collagen, Collagen implant, Gentamicin, Rectal surgery, Surgical site infection, Wound infection
Introduction
Surgical site infection (SSI) is a common type of healthcare-associated infection, which often has major consequences for patient recovery and increased healthcare costs due to prolonged hospital stay.
The risk of a patient developing an SSI is related to comorbidities, type of procedure and other factors such as length of surgery and use of prosthetic implants [1–3]. Data from national and regional surveys and single studies have highlighted high SSI rates in gastrointestinal (GI) surgical procedures (e.g. elective colorectal resection) [4–6]. Some of the higher rates of SSI in GI surgery are associated with newer techniques aimed at improving local control and resectability of the tumour, e.g. pre-operative radiotherapy followed by abdominoperineal resection (APR) [7, 8]. Therefore, there is a need for better prevention of SSIs following GI surgery in order to improve patient morbidity and decrease healthcare costs.
The mainstay of SSI prevention in addition to strict aseptic surgical technique is the use of antibiotic prophylaxis administered systemically both pre- and post-operatively.
Results from 4 individual studies contained within a systematic review showed consistently that the wound infection rate was much lower in the antibiotic groups than that in the control groups (13% versus 40%; OR 4.08, 95% CI (c.i) 2.33–7.13) [9]. However, following GI surgery there is a tendency to administer systemic antibiotics for longer time periods, despite the fact that this may not necessarily lower the risk of SSI and this may in turn lead to a greater risk of antibiotic resistance [9–12].
The emergence of technologies such as resorbable gentamicin-containing collagen implants (GCI), which deliver high local concentrations of gentamicin with correspondingly low serum levels offer a means of reducing SSI rates following GI surgery, lowering the risk of antibiotic resistance by reducing the need for long-term administration of systemic antibiotics, avoiding toxicity associated with systemic antibiotics, and avoiding the need for reoperation as the implant is fully resorbable. The use of collagen as a carrier also has positive effects on wound healing.
GCI seems to limit the risk of SSI in several ways. Collagen causes faster coagulation to stop bleeding [13] and reduces the risk of seroma and haematoma formation that can in turn accelerate bacterial proliferation [14, 15]. The breakdown of the GCI by macrophage collagenases increases the number of collagen fibres released, which attracts fibroblasts and stimulates the fibroblasts to proliferate and lay down new collagen in the healing process [13].
Immune responses against collagen implants are uncommon [13, 16, 17], whereas collagen implants act as effective drug carriers [18, 19]. Drugs are released from the collagen matrix by a combination of diffusion and natural enzymatic breakdown of the collagen matrix providing rapid (diffusion) and prolonged (breakdown of the matrix) drug release [19].
The antimicrobial profile of gentamicin seems to be appropriate for use with GCI. Gentamicin allows sterilisation of the implants by gamma rays and does not seem to affect the collagen clotting features, as discussed above [16, 20]. The local use of gentamicin delivers a bactericidal concentration that is much higher than that allowed by systemic injection, so antibiotic blood concentrations remain low and reduce the chance of adverse effects (e.g. nephrotoxicity), while the local drug concentrations are kept high for at least 48 h [21, 22]. In this way, resistance to antibiotics caused by low drug dosage is avoided [23], and gentamicin behaves like a broad spectrum antibiotic [21, 23].
A number of resorbable GCI are available worldwide. The objective of this article is to review all published clinical data regarding prophylactic application of resorbable GCI following GI surgery in order to provide an overview of the efficacy and safety of GCI for specific indications with particular focus on high-risk procedures.
Method
The candidate publications were identified using the National Library of Medicine’s PubMed online search utility and the search term ‘gentamicin collagen implant’ plus ‘surgical site infection’, ‘wound infection’ and ‘gastrointestinal surgery’. This search identified 28 potential publications. Nine publications focusing specifically on GI surgery and related areas (e.g. pilonidal sinus resection) were selected. These studies concerned the use of two GCI i.e. Collatamp® (EUSA Pharma [Europe], Oxford, United Kingdom) and Septocoll® (Biomet Deutschland GmbH, Berlin, Germany). Collatamp contains 2 mg/cm2 gentamicin sulphate. The collagen in Collatamp, present at 2.8 mg/cm2, is type I collagen from a renatured bovine or equine source. Septocoll contains gentamicin sulphate (70 mg gentamicin from 116 mg gentamicin sulphate base in a 10 cm × 8 cm implant) and gentamicin crobefate (70 mg gentamicin from 350 mg gentamicin crobefate in a 10 cm × 8 cm implant). Septocoll contains type I collagen from a renatured equine source.
The outcome measures of primary interest were SSI rate (superficial and deep), primary and secondary healing rate together with post-operative and surgical complication rate. Other outcome measures include time to complete wound healing; operating time; length of hospital stay; tumour recurrence (local and distant); survival time; pain score; analgesic use and cost. The level of evidence for each study was graded according to the criteria developed by Carruthers et al. [24] (see Table 1).
Table 1.
Level | Definition of evidence |
---|---|
1 | Randomised, controlled trial (RCT) that demonstrated a statistically significant difference in at least one important outcome |
OR | |
If the difference is not statistically significant, an RCT of adequate sample size to exclude a 25% difference in relative risk with 80% power, given the observed results | |
2 | RCT that does not meet level 1 criteria |
3 | Non-randomized trial with contemporaneous controls selected by some systematic method (i.e. not selected by perceived suitability for one of the treatment options for individual patients) |
OR | |
Subgroup analysis of a randomised trial | |
4 | Before-after study or case series (of ≥10 patients) with historical controls or controls drawn from other studies |
5 | Case series (of ≥10 patients) without controls |
6 | Case reports (of <10 patients) |
Clinical experience
To date, there have been 9 clinical studies which have focused on the local application of GCI in the prophylaxis of SSI following gastrointestinal surgery (Table 2). Six studies were of what would be considered procedures at high-risk of SSI and three of procedures at medium-risk. Eight of the studies were of randomised, controlled design, and one included a consecutive patient series with contemporaneous controls. Seven of the studies were graded as level 1 (see Table 2). Taken together these studies represent experience with 483 patients treated prophylactically with GCI (n = 383 with Collatamp and n = 100 with Septocoll) following GI surgery.
Table 2.
Author and evidence grading | Product | Population | Number of subjects and treatment groups | Results |
---|---|---|---|---|
Rutten (1997)[25] Level 1 |
Collatamp®* Implant cut into three longitudinal strips. The fascia was closed and the implant placed directly upon the closed fascia directly adjacent to the surgical wound. The skin was closed with a double layer of resorbable sutures |
Patients stratified by type of procedure Colonic resection Reversal of Hartmann procedure Abdominoperineal resection (APR) Subtotal colectomy Low anterior resection |
n = 221 total patients n = 107 gentamicin collagen implant plus ceftriaxone + metronidazole IV or gentamicin + metronidazole IV (Group I) n = 114 ceftriaxone + metronidazole IV or gentamicin + metronidazole IV (Group II) |
Wound infections: Group I: 5.6% (6/107) vs. Group II: 18.4% (21/114) (P < 0.01) LOS: Group I: 13.8 days vs. Group II: 16.3 days (P = 0.015) Microbiology: Bacterial species were cultured from n = 3/107 in group I and n = 8/114 in group II |
Grüssner (2001) [27] Level 1 |
Septocoll® Three implants 5 × 8 cm evenly inserted into the sacral cavity at one level with the remnants of the levator ani muscle |
Patients undergoing abdominoperineal resection (APR) for low rectal carcinoma |
n = 97 total patients n = 49 gentamicin collagen implant plus cefazoline + metronidazole plus sacral drainage (Group I) n = 48 cefazoline + metronidazole plus sacral drainage (Group II) |
Wound infections: Group I: 6.1% (3/49) vs. Group II: 20.83% (10/48) (P < 0.05) Wound healing: Primary perineal wound healing—Group I: 88% (43/49) vs. Group II: 75% (36/48) (P = 0.12) Secondary perineal wound healing with infection—Group I: 6% (3/49) vs. Group II : 21% (10/48) (P < 0.05) Microbiology: Bacteriologic efficacy in Group I: 83.7% (41/49) vs. Group II: 60.4% (29/48) (P = 0.013) |
Nowacki (2005) [26] Level 1 |
Collatamp® One 10 × 10 cm implant placed in the presacral area below the peritoneal reflection. When anterior resection was performed, the implant was wrapped around the anastomosis |
Patients undergoing Anterior resection Low anterior resection Abdominoperineal resection (APR) Hartmann procedure |
n = 229 randomised n = 113 gentamicin collagen implant plus metronidazole + cefuroxamine IV (Group I) n = 116 metronidazole + cefuroxamine IV (Group II) |
Early post-operative complications (30 days): Total complications—Group I: 20.7% (22/106) vs. Group II: 37.5% (42/112) (P = 0.0441) Surgery > 3 h—Group I: 19.2% (15/78) vs. Group II: 40.8% (31/76) (P = 0.0314) Intraoperative bowel perforation/contamination of peritoneal cavity—Group I: 20% (3/15) vs. Group II: 57.9% (11/19) (P = 0.01) Cancer recurrence: Local recurrence/or metastasis at 36 months—Group I: 14.4% vs. Group II: 32.3% (P = 0.03) Rate of local recurrence similar in both groups Distant metastasis—Group I: 10.3% vs Group II: 28.1% (P = 0.0095) Survival: 3-year survival—Group I: 88.66% vs. Group II: 73.96% |
de Bruin (2008) [28] Level 3 |
Collatamp® Three implants inserted into the sacral wound cavity at one level with the remnants of the levator ani muscle |
Consecutive series of patients undergoing abdominoperineal resection (APR) for rectal cancer after short-course radiotherapy |
n = 40 total n = 19 gentamicin collagen implant plus amoxicillin + clavulanate IV plus sacral drainage (Group I) n = 21 amoxicillin + clavulanate IV plus sacral drainage (Group II) |
Wound infections: Total wound infection (deep & superficial)—Group I: 16% (3/19) vs. Group II: 57% (12/21) (P = 0.01) Deep wound infection—Group I: 5% (1/19) vs Group II: 29% (6/21) (P = 0.05) Superficial wound infection—Group I: 11% (2/19) vs. Group II: 29% (6/21) (n.s) Wound healing: Primary wound healing—Group I: 84% (16/19) vs. Group II: 43% (9/21) (P < 0.01) LOS: Group I: 15 days vs. Group II: 25 days (P = 0.04) |
Gomez (1999) [29] Level 1 |
Collatamp® One 10 × 10 cm implant placed in the wound above the aponeurosis and wound sutured |
Patients with ‘dirty’ abdominal wounds derived from lower GI tract surgery e.g. colon perforation, acute appendicitis or gallbladder perforation |
n = 66 total patients n = 34 gentamicin collagen implant plus metronidazole IV for 7 days plus primary closure (Group I) n = 32 open wound cleaned daily with povidone solution plus metronidazole + gentamicin IV for 7 days. The wound was closed after 3 days if no infection (Group II) |
Wound infections: Group I: 8.82% (3/34) vs. Group II: 43.75% (14/32) (P < 0.001) Wound healing: Group I: 10.31 days vs. Group II: 15.20 days (P < 0.001) LOS: Group I: 5.45 days vs. Group II: 7 days Microbiology: Group I had monomicrobial wound infections whereas Group II had multimicrobial wound infections |
Haase (2005) [30] Level 2 |
Collatamp® One implant placed subcutaneously and wound sutured |
Patients undergoing loop-ileostomy closure |
n = 80 total patients n = 40 gentamicin collagen implant (Group I) n = 40 collagen implant without gentamicin (placebo) (Group II) |
Wound infections: There was no statistical difference in the rate of wound infections between the two groups The infection rate in both groups was much lower than previously reported with this type of procedure Surgical complications: There was no statistical difference in the rate of surgical complications between the two groups |
Vogel (1992) [34] Level 1 |
Collatamp® Wound covered with 1–4 implants according to the size of the excision and the wound closed with 1–2 layers of sutures |
Patients undergoing surgical excision for pilonidal sinus |
n = 80 total patients n = 40 gentamicin collagen implant plus extensive excision of pilonidal sinus (Group I) n = 40 extensive excision of pilonidal sinus (Group II) |
Wound healing: Primary healing rate—Group I: 87.5% vs. Group II: 35% (P < 0.001) Secondary wound healing—Group I: 12.5% vs. Group II: 62.5% (P < 0.001) Abscesses led to secondary wound healing in 7.5% (3/40) in Group I vs. 50% (20/40) in Group II (P < 0.001) On follow-up examination at 1 year, no recurrence had occurred in either group |
Holzer (2003) [35] Level 1 |
Septocoll® One 5 × 8 cm implant implanted in the wound cavity. The wound was closed with 1–2 layers of sutures after placement of a drain |
Patients undergoing surgical excision for pilonidal sinus |
n = 103 total patients n = 51 gentamicin collagen implant plus primary closure (Group I) n = 52 open treatment (Group II) |
Wound healing: Time to complete wound healing—Group I: 17 days vs Group II: 68 days (P = 0.0001) LOS: Group I: 9 (1–24) days vs Group II: 10 (1–13) days One recurrent pilonidal sinus was seen in group I and none in group II in the 26-week follow-up period |
Rao (2009) [36] Level 1 |
Collatamp® One to two implants were inserted depending on size of cavity. The wound was closed with two layers of sutures |
Patients undergoing surgical excision for pilonidal sinus |
n = 60 total patients n = 30 gentamicin collagen implant plus primary closure (Group I) n = 30 open treatment (Group II) |
Wound healing: Percentage of patients healed after 4 weeks—Group I: 90% vs. Group II: 13% (P < 0.001) Mean time to wound healing—Group I: 10 days vs. Group II: 50 days (P < 0.001). LOS: There was no difference seen between the two groups in length of hospital stay |
* Also known as Cronocol®, Duracoll®, Garacol®, Garacoll®, Garamycin® Schwamm, Gentalyn®, Gentimplant®, Sulmycin® Implan
Rectal surgery
There is a growing body of data to support the use of GCI following high-risk GI surgical procedures to reduce wound infection rates, wound healing time and length of hospital stay. Three randomised trials have assessed the effect of GCI in rectal tumour resection. Rutten and colleagues undertook a randomised study in which 221 patients undergoing a range of colorectal surgical procedures were randomised to the application of GCI plus systemic antibiotics (Group I) or systemic antibiotics alone (Group II) (Table 2) [25]. There was a significantly lower rate of post-operative wound infection in Group I (P < 0.01). The difference between the 2 groups was maintained even when patients with multiple complications were excluded (P < 0.05). The patients in Group I also had a significantly shorter hospital stay when compared to those in Group II (P = 0.015). However, after exclusion of the patients with complications unrelated to wound infection, the difference between the two groups diminished, with the median stay in Group I being one day shorter than Group II (13 vs. 14 days, respectively).
A second randomised, single centre study, in a similar group of patients (n = 229) treated with application of GCI plus systemic antibiotics (Group I), or systemic antibiotics alone (Group II) [26] (Table 2), reported a significantly lower post-operative complication rate (including wound infection) at 30 days in Group I (P = 0.0441). Sub-group analysis also revealed that this difference was maintained in patients at even higher risk of post-operative complications i.e. in those whose surgery exceeded 3 h (P = 0.0314) and those who experienced intraoperative bowel perforation (P = 0.01). The patients in Group I also had significantly lower rates of cancer recurrence (local or metastasic) (P = 0.03) and increased overall and disease-free survival (at 3 years). However, the reasons for this are unclear, and further studies are required to confirm these results and clarify the mechanisms involved.
A third randomised, single blind, multicentre study by Grüssner and colleagues focused specifically on 97 patients undergoing abdominoperineal resection (APR) of the anorectum, which is associated with a particularly high risk of infection and other post-operative complications as already discussed [27]. Patients were randomised to treatment with application of GCI; systemic antibiotics plus sacral drainage (Group I) or systemic antibiotics plus sacral drainage (Group II). The patients in Group I had a significantly lower rate of perineal wound infections (P < 0.05) and secondary complications with infection (P < 0.05) compared to those in Group II. In addition, patients in Group I had a much greater reduction in the number of pathogens in the post-operatively obtained wound secretion samples compared to Group II (P = 0.013).
In a recent publication, we studied for the first time the effect of GCI in patients undergoing APR following short-term, neoadjuvant radiotherapy. This study consisted of a consecutive series of 40 subjects. All patients received pre-operative radiation (5 Gy daily for 5 days) followed by a typical APR using the total mesorectal excision technique. Patients were then treated with application of GCI, systemic antibiotics plus sacral drainage (Group I) or systemic antibiotics plus sacral drainage (Group II) [28] (Table 2). This study demonstrated significantly lower rates of wound infection (P = 0.05) and significantly higher rates of primary wound healing (P < 0.01) in Group I. The patients in Group I also had significantly shorter mean hospital stays compared to those in Group II (P = 0.04).
Abdominal surgery
Two randomised studies have assessed the effect of the prophylactic application of GCI in various types of abdominal surgery. Gomez and colleagues randomised 73 patients to the application of GCI plus systemic antibiotics (Group I) and primary wound closure or systemic antibiotics and an open wound technique for the prophylaxis of infection in abdominal wounds that were ‘dirty’(e.g. due to colon perforation) (Group II) [29] (Table 2). Patients in Group I had a statistically significant lower wound infection rate (P < 0.001). The difference between the two groups showed that the application of GCI made prophylaxis four times more effective. Similarly, good results were also evident in Group I for time to wound healing; in Group I, patients took an average of 10.31 days to heal compared to 15.20 days in Group II (P < 0.001). Given the lower rate of wound infection and the quicker time to healing, patients in Group I spent an average of 1.55 days less in hospital compared to those in Group II.
A second, randomised study focused specifically on the effect of GCI on the incidence of wound infection following loop-ileostomy closure [30] (Table 2). Eighty patients were randomised to the application of GCI or identical collagen implants without gentamicin. There was no statistical difference in the rate of wound infections or surgical complications between the two groups. The infection rate in both groups was much lower than previously reported with this type of procedure [31–33].
Pilonidal sinus excision
Three randomised studies have assessed the effectiveness of GCI in patients undergoing pilonidal sinus excision with primary wound closure [34–36]. Vogel and colleagues randomised 80 patients to the application of GCI with primary wound closure (Group I) or primary closure alone (Group II) [34]. The wound in both groups was closed with 1–2 layers of subcutaneous sutures (carefully avoiding any cavity formation) plus skin sutures. The primary healing rate was significantly higher in Group I with over twice the number of patients with wounds that healed post-operatively compared to Group II (P < 0.001). The patients in Group I also had a significantly lower secondary healing rate overall (P < 0.001). With this procedure, less than 10% of the patients had post-operative abscess formation in Group I, in contrast with over half of the patients in Group II (P < 0.001). At 1-year follow-up, no recurrence had occurred in either group.
The second randomised study of pilonidal sinus excision randomised 103 patients to GCI plus primary closure (Group I) or open treatment (Group II), in order to compare surgical techniques for this indication [35]. In Group I, 14 (27%) patients failed to achieve primary healing. Five of these required conversion to open treatment and 9 experienced spontaneous wound dehiscence. Thus overall 37 (73%) patients experienced primary healing at 2 weeks. Wound breakdown was caused either by seroma formation or spontaneous dehiscence; however, complete healing of the failures by secondary intention occurred in almost all patients at 6 and 26 weeks.
Despite a failure rate of 27%, the median time to complete wound healing was significantly shorter in Group I. Patients in Group II took almost four times as long to heal compared to patients in Group I (P = 0.0001). Despite the longer healing time in Group II, there was no significant difference between the two groups in mean length of hospital stay. One recurrent pilonidal sinus was seen in Group I and none in Group II in the 26-week follow-up period.
The third study of this indication for GCI use randomised 60 patients to GCI plus primary closure (Group I) or open treatment (Group II) and followed patients to assess recurrence rates at 5 years [36]. The excision with primary sutures utilised in Group I took a significantly longer time (mean: 23 min) than the open method used in Group II (mean: 14 min) (P < 0.0001).
Significantly more wounds in Group I had healed completely compared to Group II at 4 weeks (P < 0.001). Furthermore, the wounds in Group I healed in a significantly shorter time compared to those in Group II (P < 0.001). There was no difference seen between the two groups in length of hospital stay.
The closed wounds in Group I required fewer dressings (mean 2) when compared to open wounds in Group II (mean 25) (P < 0.001). The patients in Group I also experienced significantly less pain on post-operative days 2, 4 and 7 (as reflected by their linear analogue pain scores) compared to the patients in Group II (P < 0.02). This resulted in less oral analgesic use in Group I. However, the difference between the two groups did not reach statistical significance at any time point.
Despite the lack of difference seen in length of hospital stay between the two groups, the overall cost per patient (calculated as hospital stay, cost of materials e.g. dressings and district nursing costs) was significantly lower for patients in Group I (mean of £149) compared to those in the open Group II (mean of £660) (P < 0.001). Recurrence rates were similar at 5-year follow-up.
Discussion
SSI is a common but potentially avoidable complication following GI surgery [37]. SSIs have significant impact on patient morbidity, mortality, QOL and resource utilisation and therefore, there is a need for more effective prevention in high-risk patients and procedures. There is a lack of evidence that prolonged prophylactic antibiotics reduce SSI rates and this approach may lead to antibiotic resistance. However, as early as 1997, Rutten and colleagues demonstrated the efficacy of locally applied gentamicin (with systemic antibiotics) in lowering the risk of antibiotic resistance.
This review has demonstrated that GCI can reduce the wound infection rate in high-risk GI surgery and improve wound healing after pilonidal sinus excision. GCI can also positively influence the post-operative course of patients undergoing particularly risky procedures e.g. APR combined with neoadjuvant radiotherapy. De Bruin and colleagues demonstrated that GCI reduced the wound infection rate by over 70% and the length of hospital stay by 40% in a series of patients who underwent pre-operative radiotherapy followed by APR [28].
Of the nine studies reviewed, one did not show any significant benefit of local application of GCI compared to systemic antibiotics alone. Haase et al. showed no additional benefit of GCI following loop-ileostomy closure. However, the study did have an extremely low SSI rate in the control group (10%) in contrast to that found in the literature (up to 41% of patients) [32–34, 38, 39]. The lack of effect seen with GCI may therefore be related to the use of a collagen-only implant in the ‘control’ group which, as discussed before, may not be a true ‘control’ as collagen on its own has also been shown to positively impact wound healing.
Few adverse side effects were reported in these studies [26–31, 35, 36]. However, in our experience, the dissolution of the GCI may result in an increase in wound secretion but this does not seem to have further consequences for wound healing. Gentamicin is an aminoglycoside antibiotic that has the potential to induce severe nephrotoxicity and acute renal failure when used at high concentrations [40]. However, systemic concentrations of gentamicin with implantation of 1–5 GCI remain well below the established toxicity thresholds of 10–12 μg/ml for peak values and eventually fall below 2 μg/ml by 24 h [22]. In a multicentre trial of GCI in sternal wound infections, no difference in post-operative renal function was noted [41]. The effects of GCI in patients with chronic renal failure are still unknown and caution is warranted [42].
This review on the efficacy of GCI has brought up several topics which warrant further investigation. Binnebösel and colleagues have discovered that intra-abdominal applied gentamicin can enhance the healing of anastomosis and increase the collagen type I/type III in a rat model [43]. This may have positive implications for patients undergoing pilonidal sinus excision as the same group showed a decrease of extracellular matrix (ECM) and collagen in patients who with delayed wound healing [44]. Junge et al. also demonstrated that the quality of collagen formation was significantly increased when gentamicin was used to supplement a polyvinylidenflouride mesh material used in order to improve scar quality and mesh integration in hernia repair [45, 46]. Although this and other data suggest a positive effect of local gentamicin on collagen content and metabolism, there is conflicting data regarding this subject. Vaneerdeweg et al. studied the influence of GCI on the healing of colonic anastomoses in a rat model of peritonitis [47]. The rats where divided into four groups: control; collagen implant, intravenous (IV) gentamicin and GCI. No significant difference in bursting pressure was seen between the control, IV gentamicin and GCI groups. Almost all rats in the collagen group had anastomotic leakage, suggesting that collagen alone may be a focus for infection and anastomotic breakdown. The Vaneerdeweg data conflicts with that of Haase et al. who demonstrated that collagen had a beneficial effect in their ‘collagen alone’ group compared to the wound infection rate in the literature following loop-ileostomy closure. Therefore, further work is required to elicit the mechanism involved and the implications for GCI use.
Additional study is also required to evaluate the health economic benefit of GCI. The clinical data reviewed here has demonstrated a positive effect on the length of hospital stay with GCI after rectal tumour resection. In our recently published study, the difference in the length of hospital stay between the two groups was 10 days and this may indicate a potentially large saving in hospital costs per patient treated prophylactically with GCI following APR. In addition, overall costs were shown to be significantly reduced with GCI following pilonidal sinus excision in a small series of patients.
Utilising data from Rutten et al., and length of stay information from a UK-based survey on the adverse effects of SSI [48] the cost-benefit of GCI can be estimated. Based on 100 patients undergoing bowel surgery, the total cost saving due to reduction in length of hospital stay with GCI would be approximately £16,000. However, there has been no study to date which has utilised health economic endpoints in order to prospectively analyse the potential direct and indirect costs savings with GCI in high-risk GI surgical procedures.
Conclusions
Prophylactic use of gentamicin-containing collagen implants seems to be safe and simple to use, but does it work? This review demonstrates that GCI can have a positive effect on wound infection rates in high-risk GI surgery and can also improve wound healing after pilonidal sinus excision.
No serious side effects were noted in this review suggesting the prophylactic use of GCI in GI surgery is safe.
Due to the different patient populations, types of study and inclusion/exclusion criteria, a meta-analysis would be challenging to perform. Therefore, randomised trials with well-described patient categories, end points and follow-up could help to confirm the positive effect of GCI on wound healing, and at the same time evaluate their health economic benefit and investigate their potential effect on collagen metabolism.
Acknowledgments
Conflict of interest
There is no financial relationship with the organisation that sponsored the research. We had full control of all primary data, and we agree to allow the journal to review our data if requested.
Open Access
This article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
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