Noninfectious Skin Fistulization as a Delayed Complication of Lumbar Interlaminar Device Implantation: A Report of Two Cases

Peer Reviewed

Case Report

Noninfectious Skin Fistulization as a Delayed Complication of Lumbar Interlaminar Device Implantation: A Report of Two Cases

Keyvan Mostofi

Morad Peyravi

Keywords

delayed noninfectious fistulization

March 2023

ISSN 1943-2704

Index Wounds. 2023;35(3):E116-E119. doi:10.25270/wnds/21106

Abstract

Introduction. Delayed wound healing is one reason for readmission after spine surgery. The main cause of delayed wound healing is infection. Infection rates after initial instrumented spine surgery reportedly range from 0.7% to 11.9%. However, there are noninfectious reasons for wound problems as well. Materials and Methods. This report presents 2 cases of noninfectious fistulization, 1 which occurred 11 months and 1 which occurred 2 years after surgery for implantation of a lumbar interlaminar device. Results. Although no sign of infection was found in either patient, in both cases it was necessary to remove the interlaminar device. Conclusions. These 2 cases of delayed noninfectious fistulization following instrumented spine surgery are the first seen by the authors of the current report, and as of the time of this writing, no such cases have been documented in the medical literature.

Abbreviations

CRP, C-reactive protein; IgG, immunoglobulin G; MRI, magnetic resonance imaging; NIF, noninfectious skin fistulization; WBC, white blood cell.

Introduction

The main cause of delayed wound healing is infection. Infection rates after initial instrumented spine surgery reportedly range from 0.7% to 11.9%.^1-4 Delayed infectious skin fistulization after spinal instrumentation has been rarely reported. As of this writing, and to the knowledge of the authors of the current case reports, NIF after spinal instrumentation has never been reported.

This report presents 2 patients with NIF, with 1 case occurring 11 months and the other occurring 2 years after implantation of a lumbar interlaminar device (IntraSPINE [Cousin Surgery]). In 1 patient, the device was implanted at 3 levels via a posterior approach for the management of kissing spine disease, and in the other patient the device was implanted for the management of recurrence of single-level lumbar disc herniation. The lumbar interlaminar device is used in the management of several conditions, including kissing spine syndrome, lumbar spinal canal stenosis, lumbar disc herniation, lumbar facet syndrome, and topping off fusion of the lumbar spine.^1,5-7 This device is made of soft silicone covered with a layer of polyester.

The 2 cases of NIF reported herein presented with a cutaneous lesion. Infection and granuloma were considered in the differential diagnosis. This report documents the management of this delayed, unusual complication of lumbar interlaminar device implantation.

Materials and Methods

Two patients were readmitted owing to the presence of a cutaneous lesion near a surgical incision scar. One patient (case 1) had undergone surgery 11 months before readmission, and the other patient (case 2) had undergone surgery 2 years before readmission. Contrast-enhanced MRI; measurement of serum procalcitonin CRP, erythrocyte sedimentation rate, and WBC counts; and microbiological sampling of the skin were performed for both patients. Both patients underwent surgery to manage the fistulization. Written informed consent was obtained from both patients.

Results

Case 1

A 59-year-old female was readmitted to the neurosurgery department at Centre Clinical de Soyaux with a granuloma-like skin lesion at the lower part of the incision scar from previous spine surgery. Eleven months before readmission, she underwent implantation of lumbar interlaminar devices at the L2-3, L3-4, and L4-5 levels for the management of Baastrup syndrome (ie, kissing spine disease). The result of the initial surgery was satisfactory, with no complications. The patient returned home on the second postoperative day and returned to normal activity 1 month postoperatively. Postoperative wound healing occurred by primary intention, and the incision cicatrix appeared normal. The stitches were removed 14 days postoperatively. At follow-up examination 1.5 months and 3 months postoperatively, the scar was clean and dry, and the patient had no pain or other signs or symptoms.

On readmission 11 months after the initial surgery, the patient presented with a non-oozing, granuloma-like skin lesion that had appeared 2 weeks earlier at the lower part of the scar. The referring physician had advised the patient to apply silver nitrate solution to the skin, but doing so resulted in no improvement. The patient had no signs or symptoms. Contamination-free removal of the skin lesion was performed at the readmission visit. The result of microbiological culture was negative. The CRP level was 3 mg/L, procalcitonin level was less than 0.2 ng/L, and WBC count was 6.400/µL. Contrast-enhanced lumbar spine MRI demonstrated enhancement around the posterior spinous processes of L3, L4, and L5 lumbar vertebrae and around 3 interlaminar devices, particularly the device at the level of L4-5, as well as a fistulization of the device from the L5-S1 space to the skin (Figure).

After informed consent was obtained from the patient, debridement and rinsing of the subcutaneous aspect of the wound was performed. No purulent tissue was found. Macroscopically, the tissue had a consistency that was soft, non-exuding, and tearing, but it was neither liquid nor bloody. Anatomopathological analysis was positive for the presence of interstitial fluid. Several samples were obtained, and all bacterial cultures (aerobes, anaerobes) remained sterile. Subcutaneous tissues and skin were hermetically closed.

The patient returned to the neurosurgery department 3 weeks later. The lesion had reappeared exactly as before. Revision surgery was performed to remove the interlaminar devices. Several bacteriological samples were obtained intraoperatively, all of which were sterile. As of the time of this writing, the lesion had not recurred after 2-year follow-up.

Case 2

A 62-year-old female was readmitted to the neurosurgery department with a granuloma-like skin lesion at the lower part of the incision scar from previous spine surgery. The lesion had appeared 1 month earlier. Two years before this readmission, the patient underwent diskectomy and implantation of the interlaminar device at the L4-5 level for disc herniation at the same institution. The result of the initial surgery was satisfactory, with no complications and with a return to home on the first postoperative day and a return to normal activity 1 month postoperatively. Wound healing was by primary intention, and the incision cicatrix looked normal. The stitches were removed 12 days postoperatively. At follow-up examinations performed 1.5 months and 3 months postoperatively, the scar was clean and dry, and the patient had no pain or other symptoms or signs.

The referring physician performed microbiological samplings of the granuloma-like lesion, all of which were sterile. The CRP level was 2 mg/L, and the procalcitonin value was less than 0.2 ng/L. Contrast-enhanced lumbar spine MRI demonstrated enhancement around the posterior spinous process at the L5-S1 level as well as a fistulization of the device from the L5-S1 space to skin. However, the patient had no signs or symptoms. At the cutaneous level, the tissue had a consistency that was soft, non-exuding, and tearing, but it was neither liquid nor bloody.

Given the experience with case 1, the authors of this report proceeded to device removal. No suspicious purulent collection or inflammatory tissue was found intraoperatively. Several bacteriological samples (aerobes, anaerobes) were obtained. As in case 1, all samples remained sterile. Anatomopathological tests were not conducted. As of the time of this writing, the lesion had not recurred after 2-year follow-up.

Discussion

Cutaneous opening of scar tissue after spine surgery is always concerning. It suggests first and foremost a postoperative surgical site infection, which, as a complication of spine surgery, is the primary cause of unplanned early readmission and sometimes requires revision implant procedures.^2-4,8-11 The incidence of infection after spine surgery is reportedly between 0% and 18%.^12,13 Most risk factors are well established, such as diabetes, obesity, smoking, malnutrition, and timing and duration of surgery.^14-24 Surgical site infection manifests with wound redness, swelling, pain, tenderness, purulent drainage, fever, headache, chills, and palpitation. CRP and procalcitonin levels are high.

MRI with gadolinium contrast is the best method for detecting postoperative spine infection. MRI findings associated with infection include fluid collections with rim enhancement and ascending epidural collections.^24,25 The 2 cases discussed in the current report exhibited no clinical or paraclinical findings of infection. Fistulization between the skin and device was clearly shown on MRI. The granuloma-like skin lesions in these 2 cases were suggestive of fistulization such as can occur after abdominal surgery.

Fistulization is a rare complication of visceral or obstetric and gynecologic surgery and is defined by abnormal communication between the digestive tract or genital organs and the skin. This communication gives rise to externalization of digestive or genital fluid by the newly formed fistular pathway.^25-27 In the vast majority of cases, surgery is performed.²⁸ The authors of the current report have not seen such a case following spine surgery, and to date, no cases have been documented in the medical literature. Only 1 article reported a case of delayed fistulization formation after elective spinal instrumentation,²⁹ but that case involved infectious fistulization formation rather than NIF. Some cases of postoperative skin lesions associated with device-related allergies have been reported, however.^30,31 These cases were associated with increased concentration of IgG protein. In addition, they were accompanied by other signs of allergy, such as pain, itching, and hives.

Limitations

The primary limitation of this report is that it consists of only 2 cases. A lack of sufficient cases and insufficient data do not permit the authors to pinpoint causes and consequences of this fistulization.

Conclusions

To the knowledge of the authors of the current report, the 2 cases presented herein are the first documented cases of noninfectious fistulization formation after lumbar device implantation. Despite the rarity of their presentation, these cases serve as a possible complication for surgeons to consider when investigating the cause of delayed wound healing after spinal surgery.

Acknowledgments

Authors: Keyvan Mostofi, MD, PhD¹; and Morad Peyravi, MD²

Contributions: Dr. Mostofi collected the data and wrote the paper; Dr. Peyravi edited the paper.

Affiliations: ¹Centre Clinical de Soyaux, Department of Neurosurgery, Soyaux, France; ²Hospital Carl-Thiem-Klinikum Cottbus, Cottbus, Germany

Disclosure: The authors disclose no financial or other conflicts of interest.

Correspondence: Keyvan Mostofi, MD, PhD; Centre Clinical de Soyaux, 2 Chemin de Fregeneuil Soyaux, Charente 16800, France; keyvan.mostofi@yahoo.fr

How Do I Cite This?

Mostofi K, Peyravi M. Noninfectious skin fistulization as a delayed complication of lumbar interlaminar device implantation: a report of two cases. Wounds. 2023;35(3):E116-E119. doi:10.25270/wnds/21106

References

1. Guizzardi G, Morichi R. Postoperative infections after IntraSPINE^® implantation surgery. J Neurosurg Sci. 2018;62(1):99-100. doi:10.23736/S0390-5616.16.03488-3

2. Adogwa O, Elsamadicy AA, Han JL, Karikari IO, Cheng J, Bagley CA. 30-day readmission after spine surgery: an analysis of 1400 consecutive spine surgery patients. Spine (Phila Pa 1976). 2017;42(7):520-524. doi:10.1097/BRS.0000000000001779

3. Bernatz JT, Anderson PA. Thirty-day readmission rates in spine surgery: systematic review and meta-analysis. Neurosurg Focus. 2015;39(4):E7. doi:10.3171/2015.7.FOCUS1534

4. McCormack RA, Hunter T, Ramos N, Michels R, Hutzler L, Bosco JA. An analysis of causes of readmission after spine surgery. Spine (Phila Pa 1976). 2012;37(14):1260-1266. doi:10.1097/BRS.0b013e318245f561

5. Herren C, Simons RM, Bredow J, et al. Posterior lumbar interbody fusion versus dynamic hybrid instrumentation: a prospective randomized clinical trial. World Neurosurg. 2018;117:e228-e237. doi:10.1016/j.wneu.2018.06.005

6. Mostofi K, Moghadam BG, Peyravi M. Interlaminar lumbar device implantation in treatment of Baastrup disease (kissing spine). J Craniovertebr Junction Spine. 2018;9(2):83-86. doi:10.4103/jcvjs.JCVJS_139_17

7. Mostofi K, Khouzani RK. Surgical treatment of bilateral nondisplaced isthmic lysis by interlaminar fixation device. J Craniovertebr Junction Spine. 2017;8(3):239-242. doi:10.4103/jcvjs.JCVJS_78_17

8. Avinash M, Renjith KR, Shetty AP, Sharma V, Kanna RM, Rajasekaran S. Unplanned readmissions after spine surgery: a single-center prospective analysis of a 90-day model in 2,860 cases. Asian Spine J. 2020;14(1):43-50. doi:10.31616/asj.2019.0088

9. Martin JR, Wang TY, Loriaux D, et al. Race as a predictor of postoperative hospital readmission after spine surgery. J Clin Neurosci. 2017;46:21-25. doi:10.1016/j.jocn.2017.08.015

10. Kobayashi K, Ando K, Kato F, et al. Predictors of prolonged length of stay after lumbar interbody fusion: a multicenter study. Global Spine J. 2019;9(5):466-472. doi:10.1177/2192568218800054

11. Chaudhary SB, Vives MJ, Basra SK, Reiter MF. Postoperative spinal wound infections and postprocedural diskitis. J Spinal Cord Med. 2007;30(5):441-451. doi:10.1080/10790268.2007.11753476

12. Sharif S, Gulzar F. Postoperative infections of the spine. World Spinal Column J. 2015;1(1):19–26.

13. Yao R, Zhou H, Choma TJ, Kwon BK, Street J. Surgical site infection in spine surgery: who is at risk? Global Spine J. 2018;8(4 Suppl):5S-30S. doi:10.1177/2192568218799056

14. Spina NT, Aleem IS, Nassr A, Lawrence BD. Surgical site infections in spine surgery: preoperative prevention strategies to minimize risk. Global Spine J. 2018;8(4 Suppl):31S-36S. doi:10.1177/2192568217752130

15. Pull ter Gunne AF, Cohen DB. Incidence, prevalence, and analysis of risk factors for surgical site infection following adult spinal surgery. Spine (Phila Pa 1976). 2009;34(13):1422-1428. doi:10.1097/BRS.0b013e3181a03013

16. Cizik AM, Lee MJ, Martin BI, et al. Using the spine surgical invasiveness index to identify risk of surgical site infection: a multivariate analysis. J Bone Joint Surg Am. 2012;94(4):335-342. doi:10.2106/JBJS.J.01084

17. Barnes M, Liew S. The incidence of infection after posterior cervical spine surgery: a 10 year review. Global Spine J. 2012;2(1):3-6. doi:10.1055/s-0032-1307252

18. Bohl DD, Shen MR, Mayo BC, et al. Malnutrition predicts infectious and wound complications following posterior lumbar spinal fusion. Spine (Phila Pa 1976). 2016;41(21):1693-1699. doi:10.1097/BRS.0000000000001591

19. De la Garza-Ramos R, Abt NB, Kerezoudis P, et al. Deep-wound and organ-space infection after surgery for degenerative spine disease: an analysis from 2006 to 2012. Neurol Res. 2016;38(2):117-123. doi:10.1080/01616412.2016.1138669

20. Glassman S, Carreon LY, Andersen M, et al. Predictors of hospital readmission and surgical site infection in the United States, Denmark, and Japan: is risk stratification a universal language? Spine (Phila Pa 1976). 2017;42(17):1311-1315. doi:10.1097/BRS.0000000000002082

21. Kurtz SM, Lau E, Ong KL, et al. Infection risk for primary and revision instrumented lumbar spine fusion in the Medicare population. J Neurosurg Spine. 2012;17(4):342-347. doi:10.3171/2012.7.SPINE12203

22. Marquez-Lara A, Nandyala SV, Sankaranarayanan S, Noureldin M, Singh K. Body mass index as a predictor of complications and mortality after lumbar spine surgery. Spine (Phila Pa 1976). 2014;39(10):798-804. doi:10.1097/BRS.0000000000000232

23. Berwick BW, Luo TD, Sun KW, Sharp RA, Birkedal JP, O’Gara TJ. Epidural abscess in the lumbar spine: a single institution’s experience with nonsurgical and surgical management. J Surg Orthop Adv. 2019;28(3):224-231.

24. Dowdell J, Brochin R, Kim J, et al. Postoperative spine infection: diagnosis and management. Global Spine J. 2018;8(4 Suppl):37S-43S. doi:10.1177/2192568217745512

25. Lloyd DA, Gabe SM, Windsor AC. Nutrition and management of enterocutaneous fistula. Br J Surg. 2006;93(9):1045-1055. doi:10.1002/bjs.5396

26. Parc Y, Frileux P, Vaillant JC, Ollivier JM, Parc R. Postoperative peritonitis originating from the duodenum: operative management by intubation and continuous intraluminal irrigation. Br J Surg. 1999;86(9):1207-1212. doi:10.1046/j.1365-2168.1999.01205.x

27. Lefèvre JH, Parc Y. Péritonites postopératoires. EMC – Chirurgie. 2009;9:1-8. doi: 10.1016/S1155-1968(16)77944-2

28. Girard E, Messager M, Sauvanet A, et al. Anastomotic leakage after gastrointestinal surgery: diagnosis and management. J Visc Surg. 2014;151(6):441-450. doi:10.1016/j.jviscsurg.2014.10.004

29. Etemadrezaei H, Zabihyan S, Shakeri A, Ganjeifar B. 17-year-delayed fistula formation after elective spinal instrumentation: a case report. Iran Red Crescent Med J. 2015;17(5):e28090. doi:10.5812/ircmj.17(5)2015.28090

30. Golish SR, Anderson PA. Bearing surfaces for total disc arthroplasty: metal-on-metal versus metal-on-polyethylene and other biomaterials. Spine J. 2012;12(8):693-701. doi:10.1016/j.spinee.2011.05.008

31. Lee H, Phillips JB, Hall RM, Tipper JL. Neural cell responses to wear debris from metal-on-metal total disc replacements. Eur Spine J. 2020;29(11):2701-2712. doi:10.1007/s00586-019-06177-w