Next Article in Journal
A New Approach for Phage Cocktail Design in the Example of Anti-Mastitis Solution
Previous Article in Journal
From Global to Nano: A Geographical Perspective of Aggregatibacter actinomycetemcomitans
Previous Article in Special Issue
Genetic Diversity, Virulence, and Antibiotic Resistance Determinants of Campylobacter jejuni Isolates in Romania
 
 
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Case Report

Campylobacter coli Prosthetic Joint Infection: Case Report and a Review of the Literature

by
Stijn Jonckheere
1,
Celestin Mairesse
2,
Patricia Vandecandelaere
1,
Jens Vanbiervliet
3,
Wim Terryn
4,
Jan Somers
3,
Benoit Prevost
2 and
Delphine Martiny
2,5,*
1
Department of Laboratory Medicine, Jan Yperman Hospital, 8900 Ypres, Belgium
2
Department of Microbiology, Laboratoire Hospitalier Universitaire de Bruxelles-Universitair Laboratorium Brussel (LHUB-ULB), Université Libre de Bruxelles (ULB), 1000 Brussels, Belgium
3
Department of Orthopaedic Surgery, Jan Yperman Hospital, 8900 Ypres, Belgium
4
General Internal Medicine and Nephrology, Jan Yperman Hospital, 8900 Ypres, Belgium
5
Faculty of Medicine and Pharmacy, University of Mons (UMONS), 7000 Mons, Belgium
*
Author to whom correspondence should be addressed.
Pathogens 2024, 13(10), 838; https://doi.org/10.3390/pathogens13100838
Submission received: 5 September 2024 / Revised: 17 September 2024 / Accepted: 23 September 2024 / Published: 27 September 2024
(This article belongs to the Collection Campylobacter Infections Collection)

Abstract

:
Prosthetic joint infections caused by Campylobacter are uncommon, with the majority of cases being attributed to C. fetus. This case report represents the third instance of a prosthetic hip infection caused by C. coli following an episode of gastroenteritis and, notably, in an immunocompetent patient. The infection was successfully managed by surgical debridement and lavage with retention of the prosthesis and 12 weeks of antibiotics. Furthermore, we present the first whole-genome sequence of a Campylobacter strain responsible for prosthetic joint infection and offer a comprehensive review of the literature on such infections.

1. Introduction

Campylobacteriosis is the leading bacterial cause of human gastroenteritis worldwide, and it represents a significant global public health problem. In 2022, there were 137,107 confirmed cases of human campylobacteriosis in the European Union, corresponding to a reporting rate of 43.1 cases per a population of 100,000 [1]. In the same year, the Foodborne Diseases Active Surveillance Network in the United States reported a campylobacter infection incidence of 19.2 cases per a population of 100,000 [2]. The exact burden of disease in low-resource settings, such as countries in Sub-Saharan Africa, is unknown due to limited surveillance, and the estimated prevalence of human infection in this region ranges from 8.5% to 14.1%, with prevalence rates reaching approximately 50% in children under 5 years of age and HIV patients [3].
As with other zoonoses, a significant decrease in the number of reported cases was observed in the 27 EU Member States during the pandemic, probably due to both underreporting and a real decrease in infections due to a reduction in international travel [2]. However, Kuhn et al. expect a significant increase in campylobacteriosis in the future due to global warming [4].
Poultry meat has been identified as a significant contributor to Campylobacter infections globally. However, other potential sources have been identified, such as other meats, raw milk, contaminated water supplies, or contact with pets [2,3]. Campylobacter infections can be prevented by practicing proper hand and cooking hygiene, consuming pasteurized milk or treated water, and taking precautions with animals, including pets.
The genus Campylobacter currently comprises 45 species and 13 subspecies, of which more than 10 are definitively associated with human infections. The filtration culture, which allows the isolation of non-thermophilic campylobacters, is currently limited to a few reference laboratories [5]. As a result, thermophilic C. jejuni/coli is considered the first bacterial cause of gastroenteritis worldwide and the most common zoonosis in Europe. There are significantly more C. jejuni than C. coli, and other Campylobacter species are probably greatly underestimated [5].
While gastroenteritis is a common manifestation of Camplobacter infection, focal extraintestinal infections occur uncommonly. To date, fewer than thirty cases of Campylobacter prosthetic joint infections have been reported worldwide, and they are predominantly caused by C. fetus in immunocompromised patients. This case study presents a case of C. coli prosthetic hip infection with bacteriemia following a gastroenteritis in an immunocompetent patient, the only relevant medical history of which was an uncomplicated gastric bypass. In addition, we provide a complete analysis of the strain’s whole-genome sequence and a comprehensive literature review, both of which should improve patient care in the future.

2. Case Description

A 61-year-old woman presented to the emergency department of Jan Yperman hospital (Ypres, Belgium) with atraumatic right hip pain, fever, and chills that had been ongoing for two days. She had a history of total hip prothesis 7 years prior and bariatric surgery (laparoscopic gastric bypass) 5 years prior. There was no nicotine abuse and only occasional alcohol consumption. Several weeks before her current onset of hip pain, she experienced anorexia and nausea. She had no direct contact with animals, had no recent travel, did not recall consuming undercooked meats, and had no ill contacts. The C-reactive protein (CRP) level was 177 mg/L, and she had a normal leukocyte count (5900/µL with 69.8% neutrophiles).
Based on the anamnestic and clinical findings, a prosthetic joint infection (PJI) was suspected, and a surgical debridement and lavage with synovectomy was performed on Day 2 of admission. During this procedure, a synovial punction and five tissue biopsies were taken. Besides antibiotic prophylaxis, no antibiotics were given before surgery, and vancomycin was intravenously initiated after surgery. The arthrocentesis of the right hip yielded 10 mL of bloody fluid, with 335,000 red blood cells/µL, only 11 leukocytes/µL, and an absence of crystals.
On Day 3 of admission, the aerobic blood culture bottles (BD BACTEC, BD Diagnostics, Sparks, MD, USA) taken on admission were flagged positive after 1 day, and 18 h of incubation and microscopic Gram-staining revealed Gram-negative rods. After culturing on blood agar, these were identified as Campylobacter coli via Matrix-Assisted Laser Desorption/Ionization-Time-of-Flight Mass Spectrometry (MALDI-TOF MS) using VITEK MS PRIME (bioMerieux, Marcy-l’Etoile, France) with knowledge base version 8.5.0-3. After two days of incubation, the hip punction and per-operative tissue samples all grew C. coli. Additionally, a feces sample that was taken on Day 3 of admission tested positive for PCR Campylobacter spp. using the Allplex GI-EB Screening Assay (Seegene, Seoul, Republic of Korea). Other targets were negative. The feces culture on Campylosel agar (bioMérieux SA, Marcy-l’Étoile, France) also revealed C. coli. Despite our best efforts, we were unable to identify any potential sources of the C. coli gastroenteritis. We also conducted a thorough review of the potential exposure to cattle or poultry but none were identified.
The antimicrobial susceptibility testing (AST) was conducted at the local laboratory and subsequently validated by the National Reference Center (NRC) through the utilization of gradient strips (Etest®, bioMérieux, Marcy l’Etoile, France) and the disk diffusion method, which was based on the EUCAST version 13.1 guidelines. The inoculum was applied to Mueller–Hinton agar supplemented with 5% defibrinated horse blood and 20 mg/L of β-NAD (MH-F), which was then incubated in a micro-aerobic environment at 41 ± 1 °C for 24 ± 1 h. When EUCAST breakpoints were not available, CA-SFM breakpoints 2023 v1.0 were used. An identical susceptibility profile was found for both the C. coli strains isolated from arthrocentesis and the feces culture. Based on the susceptibility results, antibiotic treatment was switched to levofloxacine 500 mg twice a day, which continued for 12 weeks.
Three days after the first debridement and lavage, a second extensive lavage was performed. The infected hip prothesis was retained. The patient made a good clinical and biochemical recovery with a favorable wound healing, and, after 10 days of admission, the patient was discharged from hospital with a CRP value of 15.1 mg/L. A full recovery was made with a pain-free hip joint and a CRP value of 3.2 mg/L one month after the discontinuation of antibiotics. Follow-up at 1 year showed no recurrence of infection.
Both strains were submitted to the NRC, which confirmed the phenotypic results (identification and AST) obtained by the local laboratory, and they were then submitted to whole-genome sequencing (WGS). DNA extraction was performed using an EZ1&2 Virus Mini Kit v2.0 on an EZ2® Connect MDx instrument (Qiagen, Hilden, Germany). DNA was enzymatically fragmented according to the manufacturer’s instructions and modified to generate an Illumina-compatible DNA library using NEBNext® Ultra™ II FS DNA Library Prep Kit for Illumina. The final libraries were qualified using an AATI Fragment Analyser (Agilent Technologies Inc., Santa Clara, CA, USA) with a DNF-474 High-Sensitivity NGS Fragment Analysis Kit, and they were then quantified using a Qubit 2.0 with a Qubit dsDNA HS Assay Kit (Life Technologies, Carlsbad, CA, USA). After equimolar pooling, the libraries were sequenced using a NovaSeq 6000 machine (Illumina Inc., San Diego, CA, USA) with a NovaSeq 6000 SP Reagent Kit v1.5 (300 cycles) in 2 × 150 bp paired mode. An average coverage of 100× was targeted.
FASTQ files from both sequenced genomes were processed using a Bionumerics v8.1 calculation engine (bioMérieux, Marcy l’Etoile, France). The de novo assembly was performed using the SPAdes genome assembler, and the quality of the assembly was assessed (Supplementary Materials, Table S1).
Multi Locus Sequence Typing (MLST) analysis classified both isolates as belonging to a new sequence type (ST-14004) (Supplementary Materials, Table S1).
Detection of the acquired resistance gene and point mutation was performed using Resfinder-4.5.0 for C. coli, with gene lengths of ≥80% and identities of ≥70%. Detection of virulence-associated genes was performed using the Custom Genotyping plug-in in BioNumerics v.8.1 based on the Basic Local Alignment Search Tool (BLAST, National Center for Biotechnology Information, US National Library of Medecine, Rockville Pike Bethesda, USA). The minimum sequence coverage and identity was set at 75%.
Table 1 provides a summary of the genes and point mutations observed in both strains, as well as those that were not identified but which were frequently considered to be reliable indicators of antimicrobial resistance [6]. Despite the absence of point mutations, seven resistant determinants were identified. The blaOXA-460 gene, which is associated with resistance to beta-lactam antibiotics, was identified with 92.9% identity and 100% coverage. The cmeB, cmeC, cmeD, cmeE, and cmeF genes were identified with 100% coverage and 85%, 84%, 84%, 83%, and 85% identity, respectively. Additionally, aadE-Cc was identified with a coverage of 80% and an identity of 85%.
A total of 133 virulence genes associated with adhesion, immune modulation, motility, cytotoxicity, and invasion were screened, and 63 genes were identified in both isolates (Supplementary Materials, Table S1). Among these genes, 44 (70%) are known to be associated with bacterial motility, 16 (25%) with immune modulation, 2 (3%) with invasion into host cells, and 1 (1%) with adhesion (Supplementary Materials, Table S2).

3. Discussion and Review of the Literature

In this study, we reviewed the literature pertaining to Campylobacter-associated PJI. The review was restricted to articles published in English and referenced within the PubMed database. Twenty-six cases (including our case) have been reported [7,8,9,10,11,12,13,14,15,16,17,18,19,20,21,22,23,24] (Table 2). Most of these Campylobacter PJI were caused by C. fetus (n = 16), with only a few published cases of C. jejuni (n = 5), C. coli (n = 3), C. lari (n = 1), and C. upsaliensis (n = 1). There is no clear gender preponderance (58% being male) for Campylobacter PJI, with patients having a median age of 73 years (range: 24 to 88 years), and cases are equally distributed between the hip (n = 14) and knee (n = 12) PJI. There are no reports of Campylobacter PJI of the shoulder joint. Most published cases have been of immunocompromised patients (15 of 26 documented cases according to our interpretation); however, the patient in our case was not considered immunosuppressed as an uncomplicated gastric bypass was the only relevant medical history and there was no history of recurrent infections in the past.
Identical to the two previous case reports of C. coli PJI, our patient had a gastro-enteritis before the onset of the PJI, with a positive PCR and culture on stool. At the time of PJI diagnosis, blood cultures were also positive for C. coli, supporting the hematogenous seeding of the site of a prosthetic joint after a gastrointestinal illness. When considering the 26 published cases, 12 (46%) and 6 (23%) of them produced positive blood and stool cultures, respectively, although the results of these cultures were not obtained and/or not reported in all cases. Current treatment recommendations for Campylobacter gastro-enteritis is to limit treatment to those with severe disease or risk of severe disease. Patients with severe disease include individuals with bloody stools, high fever, extra-intestinal infection, worsening or relapsing symptoms, or symptoms lasting longer than one week [25]. Those at risk for severe disease include patients who are older, pregnant, or immunocompromised [26]. Based on the findings reported here and those found in our literature review, treatment might also be considered for those with prosthetic joints because patients with prosthetic joints may have a predilection to developing PJI after what may initially seem like an innocuous gastrointestinal illness. However, the impact on antimicrobial resistance and the potential side-effects of more widespread antibiotic use should be considered in relation to the potential prevention of a Campylobacter PJI, which is still a very rare occurrence.
A variety of surgical and antimicrobial regiments have been described for the management of Campylobacter PJI. Five cases have been managed without surgery; eleven with debridement, antibiotics, and implant retention (DAIR); and nine with one- or two-stage reimplantation arthroplasty. Various antimicrobial classes have been used, mostly in combination therapy and starting with an intravenous therapy followed by an oral phase, including ẞ-lactams (including ẞ-lactams + ẞ-lactamase inhibitors and carbapenems) in 60%, aminoglycosides in 44%, fluoroquinolones in 36%, macrolides in 32%, clindamycin in 20%, and tetracyclines in 8% of documented cases. The total duration of antibiotic treatment (for documented cases where the patient survived) ranged from 6 weeks to indefinite suppression therapy. Despite heterogeneous treatment, most cases have had a successful outcome even without surgical intervention. While these numbers are too small to draw conclusions, it seems that Campylobacter PJI’s have a favorable outcome without the need for an aggressive surgical approach or long-term antibiotic therapy. We successfully treated our patient as an acute Gram-negative PJI according to the recommendations of the PRO-IMPLANT foundation [27] with debridement and retention of the prosthesis, as well as 12 weeks of high dose fluoroquinolone after susceptibility was confirmed.
The WGS analysis enabled us to genetically characterize the two C. coli strains isolated from both the hip punction and fecal samples. The two strains showed an identical MLST allelic signature, identical resistance determinants, and identical virulence-associated genes (Supplementary Materials, Table S1).
No resistance genes known to be associated with macrolide and tetracycline resistance were identified, which is consistent with the susceptible phenotype (Table 1).
The blaOXA-460 gene, a variant of blaOXA-61, was identified in both strains. These genes are associated with resistance to beta-lactams [28,29]. The identification of blaOXA-460 was not found to be correlated with the phenotype (Table 1). The genotype–phenotype concordance of blaOXA genes was moderate, with a concordance of 67.4 observed for the blaOXA-61 in the study by Wysok and colleagues [30].
The cmeDEF operon, which was also identified in both strains, has been described in C. jejuni as an efflux system with ampicillin as a substrate [31]. Nevertheless, we did not identify the cmeDEF operon in correlation with ampicillin resistance. The cmeABC operon codes for an active efflux pump has been associated with resistance to fluoroquinolone [32]. Absence of the cmeA gene in both strains suggested that the efflux pump complex might not form, and this would be consistent with the observed fluoroquinolone-susceptible phenotype (Table 1). Moreover, no point mutations associated with fluoroquinolone resistance were identified.
The aadE-sat4-aphA3 gene cluster is associated with resistance to multiple aminoglycosides [33]. Both strains exhibited only part of this cluster, solely harboring the aadE-Cc gene. The lack of aminoglycoside resistance in these strains may be attributed to a truncated cluster, suggesting incomplete functionality.
Seventy percent of the genes identified in the virulence gene screening were genes encoding proteins that are responsible for bacterial motility associated with flagellar machinery (Supplementary Materials, Table S2) [34,35,36,37,38,39,40,41]. The flagellar machinery allows the bacterium to rotate and could be linked to adhesion and biofilm formation [42]. The flagellum in Campylobacter spp. plays a role in motility and is involved in several other biological processes, including secretion, colonization factors, cell division, and the regulation of these processes [42]. Screening for virulence factors identified 5 kps genes (kpsD, E, M, S, and T) associated with capsule biosynthesis and transport [43,44]. The deletion of the kpsS-C-M-gene in C. jejuni mutant strains has resulted in a notable reduction in their capacity to induce bacteremia in a murine model, suggesting a decreased infectivity for this bacterium [43,45,46,47]. Additionally, both CiaB and CiaC genes were identified. This evidence suggests that the bacteria possess the ability to secrete Campylobacter invasion antigens (Cia). The proteins in question may be transported by the flagellum and subsequently released into the cytosol of the host, where they may play a role in the organism’s virulence [48,49].
Our study will undoubtedly contribute to improving the diagnosis and management of patients suffering from PJI in the future. The literature review clearly demonstrated that Campylobacter, particularly C. fetus, is a potential cause of PJI. It should, therefore, form part of the diagnostic workup in clinical laboratories. This is crucial, given the specific growth conditions of the Campylobacter species (microaerobic atmosphere). Secondly, our literature review and case study definitively supports the optimal surgical and antibiotic approach for treating Campylobacter PJIs. Finally, the WGS analysis, when combined with more WGS data of invasive and non-invasive strains, will undoubtedly contribute to a better understanding of the pathogenesis of invasive infections in the future.
The primary limitation of our study is that only two strains from a single patient have been sequenced. Naturally, it is essential to sequence a substantial number of both invasive and non-invasive strains to obtain reliable conclusions.

4. Conclusions

Campylobacter prosthetic joint infections are a rare occurrence, they are predominantly caused by C. fetus, and they affect patients with immunocompromising conditions. Here, we reported a C. coli PJI in an immunocompetent patient.
Extensive surgical debridement with retention of the prosthesis in combination with antibiotics has been found, with an overall favorable prognosis, to be an efficacious treatment for such infections.
To date, no strain of Campylobacter responsible for prosthetic joint infections has been subjected to WGS as far as we are aware from an examination of the relevant literature. Our virulome analysis of this invasive Campylobacter strain identified several virulence factors. Further characterization of other invasive strains could reveal novel insight into the underlying mechanisms of the pathogenesis in Campylobacter strains involved in PJI and other invasive infections.
Consequently, it underscores the importance of systematically assigning invasive strains to the NRC.

Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/pathogens13100838/s1, Table S1: The origin, host, source, isolation dates, MLST characteristics, genome metrics, antibioresistance, and the virulence gene detected in the two strains of Campylobacter coli; Table S2: The virulence-associated genes in both C. coli strains.

Author Contributions

Conceptualization, S.J. and D.M.; investigation, S.J., P.V., J.V., J.S., B.P. and C.M.; writing—original draft preparation, S.J., D.M. and C.M.; writing—review and editing, S.J., C.M., P.V., J.V., J.S., B.P., D.M. and W.T.; visualization, S.J. and D.M.; supervision, S.J. and D.M.; project administration, S.J. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

This study was conducted in accordance with the guidelines detailed in the Declaration of Helsinki, and it was approved by the Medical Ethics Committee of Jan Yperman Hospital (protocol code: JYS202404, 26 April 2024).

Informed Consent Statement

Written informed consent was obtained from the patient(s) to publish this paper (22 May 2024).

Data Availability Statement

The original contributions presented in the study are included in the article/supplementary materials, further inquiries can be directed to the corresponding author.

Conflicts of Interest

The authors declare no conflicts of interest.

References

  1. European Food Safety Authority (EFSA); European Centre for Disease Prevention and Control (ECDC). The European Union One Health 2022 Zoonoses Report. J. Eur. Food Saf. Auth. 2023, 21, e8442. [Google Scholar] [CrossRef]
  2. Delahoy, M.J.; Shah, H.J.; Weller, D.L.; Ray, L.C.; Smith, K.; McGuire, S.; Trevejo, R.T.; Scallan Walter, E.; Wymore, K.; Rissman, T.; et al. Preliminary Incidence and Trends of Infections Caused by Pathogens Transmitted Commonly through Food—Foodborne Diseases Active Surveillance Network, 10 U.S. Sites, 2022. Morb. Mortal. Wkly. Rep. 2023, 72, 701–706. [Google Scholar] [CrossRef] [PubMed]
  3. Paintsil, E.K.; Masanta, W.O.; Dreyer, A.; Ushanov, L.; Smith, S.I.; Frickmann, H.; Zautner, A.E. Campylobacter in Africa—A specific viewpoint. Eur. J. Microbiol. Immunol. 2023, 13, 107–124. [Google Scholar] [CrossRef]
  4. Kuhn, K.G.; Nygård, K.M.; Guzman-Herrador, B.; Sunde, L.S.; Rimhanen-Finne, R.; Trönnberg, L.; Jepsen, M.R.; Ruuhela, R.; Wong, W.K.; Ethelberg, S. Campylobacter infections expected to increase due to climate change in Northern Europe. Sci. Rep. 2020, 10, 13874. [Google Scholar] [CrossRef]
  5. Giraudon, E.; Miendje Deyi, V.Y.; Martiny, D. Assessing the Prevalence and Dynamics of Emerging Campylobacterales in Human Stool Samples in Brussels by Filtration Culture. Pathogens 2024, 13, 475. [Google Scholar] [CrossRef]
  6. Proposed Protocol for Whole Genome Sequencing Based Analysis for Detection and Tracing of Epidemic Clones of Antimicrobial Resistant Salmonella and Campylobacter to Be Used for National Surveillance and Integrated Outbreak Investigations by NRLs for Public Health. FWD AMR-RefLabCap. 2022. Available online: https://www.fwdamr-reflabcap.eu/resources/reflabcap-protocols-and-guidelines (accessed on 12 August 2024).
  7. Yao, J.D.; Ng, H.M.; Campbell, I. Prosthetic hip joint infection due to Campylobacter fetus. J. Clin. Microbiol. 1993, 31, 3323–3324. [Google Scholar] [CrossRef] [PubMed]
  8. Bates, C.J.; Clarke, T.C.; Spencer, R.C. Prosthetic hip joint infection due to Campylobacter fetus. J. Clin. Microbiol. 1994, 32, 2037. [Google Scholar] [CrossRef]
  9. Cone, L.A.; Dreisbach, P.B.; Hirschberg, J.; Shekar, C.; Dreisbach, L.P.; Salatich, W. Cellulitis and septic arthritis caused by Campylobacter fetus and Campylobacter jejuni: Report of 2 cases and review of the literature. J. Clin. Rheumatol. Pract. Rep. Rheum. Musculoskelet. Dis. 2003, 9, 362–369. [Google Scholar] [CrossRef]
  10. David, J.; Nasser, R.M.; Goldberg, J.W.; Reed, K.D.; Earll, M.D. Bilateral prosthetic knee infection by Campylobacter fetus. J. Arthroplast. 2005, 20, 401–405. [Google Scholar] [CrossRef]
  11. Chambers, S.T.; Morpeth, S.C.; Laird, H.M. Campylobacter fetus prosthetic hip joint infection: Successful management with device retention and review. J. Infect. 2005, 50, 258–261. [Google Scholar] [CrossRef]
  12. Meyer, A.; Theulin, A.; Chatelus, E.; Argemi, X.; Sordet, C.; Javier, R.M.; Hansmann, Y.; Sibilia, J.; Gottenberg, J.E. Campylobacter fetus infection in three rheumatoid arthritis patients treated with rituximab. Ann. Rheum. Dis. 2012, 71, 1094–1095. [Google Scholar] [CrossRef] [PubMed]
  13. Prendki, V.; Marmor, S.; Zeller, V.; Lhotellier, L.; Mégraud, F.; Desplaces, N. Campylobacter infection after prosthetic joint surgery. Scand. J. Infect. Dis. 2013, 45, 706–710. [Google Scholar] [CrossRef]
  14. Yahia, S.A.; Zeller, V.; Desplaces, N.; Chazerain, P.; Lhotellier, L.; Marmor, S.; Ziza, J.M. Crystal-induced arthritis after arthroplasty: 7 cases. Jt. Bone Spine 2016, 83, 559–562. [Google Scholar] [CrossRef] [PubMed]
  15. Dumic, I.; Sengodan, M.; Franson, J.J.; Zea, D.; Ramanan, P. Early Onset Prosthetic Joint Infection and Bacteremia due to Campylobacter fetus Subspecies fetus. Case Rep. Infect. Dis. 2017, 2017, 5892846. [Google Scholar] [CrossRef]
  16. Zamora-López, M.J.; Álvarez-García, P.; García-Campello, M. Prosthetic hip joint infection caused by Campylobacter fetus: A case report and literature review. Rev. Esp. Quimioter. Publ. Off. Soc. Esp. Quimioter. 2018, 31, 53–57. [Google Scholar]
  17. Peterson, M.C.; Farr, R.W.; Castiglia, M. Prosthetic hip infection and bacteremia due to Campylobacter jejuni in a patient with AIDS. Clin. Infect. Dis. Off. Publ. Infect. Dis. Soc. Am. 1993, 16, 439–440. [Google Scholar] [CrossRef] [PubMed]
  18. Vasoo, S.; Schwab, J.J.; Cunningham, S.A.; Robinson, T.J.; Cass, J.R.; Berbari, E.F.; Walker, R.C.; Osmon, D.R.; Patel, R. Campylobacter prosthetic joint infection. J. Clin. Microbiol. 2014, 52, 1771–1774. [Google Scholar] [CrossRef] [PubMed]
  19. Ali, S.; Siddiqui, B.; Lawal, F. Campylobacter jejuni prosthetic joint infection in an ulcerative colitis patient in the absence of gastrointestinal symptoms. IDCases 2020, 22, e00920. [Google Scholar] [CrossRef]
  20. Simms, A.J.; Kobayashi, T.; Schwartzhoff, P.V.; Sekar, P. Prosthetic hip infection due to Campylobacter jejuni. BMJ Case Rep. 2022, 15, e248240. [Google Scholar] [CrossRef]
  21. Sharp, S.E. Campylobacter coli prosthetic hip infection associated with ingestion of contaminated oysters. J. Clin. Microbiol. 2009, 47, 3370–3371. [Google Scholar] [CrossRef]
  22. Suarez, A.; Parsons, C.; Parsons, E.; Gowe, I.; Vickery, S. Diarrheal illness and prosthetic joint infection caused by Campylobacter coli following consumption of undercooked chicken wings. IDCases 2019, 18, e00644. [Google Scholar] [CrossRef] [PubMed]
  23. Werno, A.M.; Klena, J.D.; Shaw, G.M.; Murdoch, D.R. Fatal case of Campylobacter lari prosthetic joint infection and bacteremia in an immunocompetent patient. J. Clin. Microbiol. 2002, 40, 1053–1055. [Google Scholar] [CrossRef] [PubMed]
  24. Issartel, B.; Pariset, C.; Roure, C.; Boibieux, A.; Peyramond, D. Successful treatment of prosthetic knee infection due to Campylobacter upsaliensis. Eur. J. Clin. Microbiol. Infect. Dis. Off. Publ. Eur. Soc. Clin. Microbiol. 2002, 21, 234–235. [Google Scholar] [CrossRef]
  25. Ruiz-Palacios, G.M. The health burden of Campylobacter infection and the impact of antimicrobial resistance: Playing chicken. Clin. Infect. Dis. Off. Publ. Infect. Dis. Soc. Am. 2007, 44, 701–703. [Google Scholar] [CrossRef]
  26. White, A.E.; Ciampa, N.; Chen, Y.; Kirk, M.; Nesbitt, A.; Bruce, B.B.; Walter, E.S. Characteristics of Campylobacter and Salmonella Infections and Acute Gastroenteritis in Older Adults in Australia, Canada, and the United States. Clin. Infect. Dis. Off. Publ. Infect. Dis. Soc. Am. 2019, 69, 1545–1552. [Google Scholar] [CrossRef]
  27. Izakovicova, P.; Borens, O.; Trampuz, A. Periprosthetic joint infection: Current concepts and outlook. EFORT Open Rev. 2019, 4, 482–494. [Google Scholar] [CrossRef]
  28. Tang, Y.; Fang, L.; Xu, C.; Zhang, Q. Antibiotic resistance trends and mechanisms in the foodborne pathogen, Campylobacter. Anim. Health Res. Rev. 2017, 18, 87–98. [Google Scholar] [CrossRef]
  29. Harrison, L.; Mukherjee, S.; Hsu, C.H.; Young, S.; Strain, E.; Zhang, Q.; Tillman, G.E.; Morales, C.; Haro, J.; Zhao, S. Core Genome MLST for Source Attribution of Campylobacter coli. Front. Microbiol. 2021, 12, 703890. [Google Scholar] [CrossRef]
  30. Wysok, B.; Wojtacka, J.; Hänninen, M.L.; Kivistö, R. Antimicrobial Resistance and Virulence-Associated Markers in Campylobacter Strains From Diarrheic and Non-diarrheic Humans in Poland. Front. Microbiol. 2020, 11, 1799. [Google Scholar] [CrossRef]
  31. Pumbwe, L.; Randall, L.P.; Woodward, M.J.; Piddock, L.J. Evidence for multiple-antibiotic resistance in Campylobacter jejuni not mediated by CmeB or CmeF. Antimicrob. Agents Chemother. 2005, 49, 1289–1293. [Google Scholar] [CrossRef]
  32. Lin, J.; Michel, L.O.; Zhang, Q. CmeABC functions as a multidrug efflux system in Campylobacter jejuni. Antimicrob. Agents Chemother. 2002, 46, 2124–2131. [Google Scholar] [CrossRef] [PubMed]
  33. Qin, S.; Wang, Y.; Zhang, Q.; Chen, X.; Shen, Z.; Deng, F.; Wu, C.; Shen, J. Identification of a novel genomic island conferring resistance to multiple aminoglycoside antibiotics in Campylobacter coli. Antimicrob. Agents Chemother. 2012, 56, 5332–5339. [Google Scholar] [CrossRef] [PubMed]
  34. Carrillo, C.D.; Taboada, E.; Nash, J.H.; Lanthier, P.; Kelly, J.; Lau, P.C.; Verhulp, R.; Mykytczuk, O.; Sy, J.; Findlay, W.A.; et al. Genome-wide expression analyses of Campylobacter jejuni NCTC11168 reveals coordinate regulation of motility and virulence by flhA. J. Biol. Chem. 2004, 279, 20327–20338. [Google Scholar] [CrossRef] [PubMed]
  35. Radomska, K.A.; Wösten, M.M.S.M.; Ordoñez, S.R.; Wagenaar, J.A.; van Putten, J.P.M. Importance of Campylobacter jejuni FliS and FliW in Flagella Biogenesis and Flagellin Secretion. Front. Microbiol. 2017, 8, 1060. [Google Scholar] [CrossRef]
  36. Cohen, E.J.; Nakane, D.; Kabata, Y.; Hendrixson, D.R.; Nishizaka, T.; Beeby, M. Campylobacter jejuni motility integrates specialized cell shape, flagellar filament, and motor, to coordinate action of its opposed flagella. PLoS Pathog. 2020, 16, e1008620. [Google Scholar] [CrossRef]
  37. Sommerlad, S.M.; Hendrixson, D.R. Analysis of the roles of FlgP and FlgQ in flagellar motility of Campylobacter jejuni. J. Bacteriol. 2007, 189, 179–186. [Google Scholar] [CrossRef]
  38. Lertsethtakarn, P.; Ottemann, K.M.; Hendrixson, D.R. Motility and chemotaxis in Campylobacter and Helicobacter. Annu. Rev. Microbiol. 2011, 65, 389–410. [Google Scholar] [CrossRef]
  39. Nachamkin, I.; Yang, X.H.; Stern, N.J. Role of Campylobacter jejuni flagella as colonization factors for three-day-old chicks: Analysis with flagellar mutants. Appl. Environ. Microbiol. 1993, 59, 1269–1273. [Google Scholar] [CrossRef]
  40. Wassenaar, T.M.; van der Zeijst, B.A.; Ayling, R.; Newell, D.G. Colonization of chicks by motility mutants of Campylobacter jejuni demonstrates the importance of flagellin A expression. J. Gen. Microbiol. 1993, 139 Pt 6, 1171–1175. [Google Scholar] [CrossRef]
  41. Chen, S.; Beeby, M.; Murphy, G.E.; Leadbetter, J.R.; Hendrixson, D.R.; Briegel, A.; Li, Z.; Shi, J.; Tocheva, E.I.; Müller, A.; et al. Structural diversity of bacterial flagellar motors. EMBO J. 2011, 30, 2972–2981. [Google Scholar] [CrossRef]
  42. Burnham, P.M.; Hendrixson, D.R. Campylobacter jejuni: Collective components promoting a successful enteric lifestyle. Nat. Reviews. Microbiol. 2018, 16, 551–565. [Google Scholar] [CrossRef] [PubMed]
  43. Stahl, M.; Ries, J.; Vermeulen, J.; Yang, H.; Sham, H.P.; Crowley, S.M.; Badayeva, Y.; Turvey, S.E.; Gaynor, E.C.; Li, X.; et al. A novel mouse model of Campylobacter jejuni gastroenteritis reveals key pro-inflammatory and tissue protective roles for Toll-like receptor signaling during infection. PLoS Pathog. 2014, 10, e1004264. [Google Scholar] [CrossRef]
  44. Christie, P.J. Type IV secretion: Intercellular transfer of macromolecules by systems ancestrally related to conjugation machines. Mol. Microbiol. 2001, 40, 294–305. [Google Scholar] [CrossRef] [PubMed]
  45. Bacon, D.J.; Szymanski, C.M.; Burr, D.H.; Silver, R.P.; Alm, R.A.; Guerry, P. A phase-variable capsule is involved in virulence of Campylobacter jejuni 81-176. Mol. Microbiol. 2001, 40, 769–777. [Google Scholar] [CrossRef]
  46. Bachtiar, B.M.; Coloe, P.J.; Fry, B.N. Knockout mutagenesis of the kpsE gene of Campylobacter jejuni 81116 and its involvement in bacterium-host interactions. FEMS Immunol. Med. Microbiol. 2007, 49, 149–154. [Google Scholar] [CrossRef] [PubMed]
  47. Corcionivoschi, N.; Clyne, M.; Lyons, A.; Elmi, A.; Gundogdu, O.; Wren, B.W.; Dorrell, N.; Karlyshev, A.V.; Bourke, B. Campylobacter jejuni cocultured with epithelial cells reduces surface capsular polysaccharide expression. Infect. Immun. 2009, 77, 1959–1967. [Google Scholar] [CrossRef] [PubMed]
  48. Neal-McKinney, J.M.; Konkel, M.E. The Campylobacter jejuni CiaC virulence protein is secreted from the flagellum and delivered to the cytosol of host cells. Front. Cell. Infect. Microbiol. 2012, 2, 31. [Google Scholar] [CrossRef]
  49. Konkel, M.E.; Klena, J.D.; Rivera-Amill, V.; Monteville, M.R.; Biswas, D.; Raphael, B.; Mickelson, J. Secretion of virulence proteins from Campylobacter jejuni is dependent on a functional flagellar export apparatus. J. Bacteriol. 2004, 186, 3296–3303. [Google Scholar] [CrossRef]
Table 1. Antimicrobial susceptibility testing and the genotypic antimicrobial resistance profile.
Table 1. Antimicrobial susceptibility testing and the genotypic antimicrobial resistance profile.
Antibiotic ClassDrug TestedDisc Diffusion (mm)Etest (mg/L)S/I/RAssociated
Resistance Gene(s) Found
Associated Resistance Gene(s) or Point Mutation(s) Not Found
Beta-lactamsAMP301SblaOXA-460
cmeDEF
blaOXA-61 and blaOXAderivate a
AMC380.125S
QuinolonesCIP360.064IcmeB, C, D, E, FSingle- or multiple-point mutations (PM) in gyrA.
cmeABC b
MacrolidesERY241SNoneerm(B), erm(N), PM in 23S_A2075G, 50S_L22_G86E
TetracyclinesTET350.25SNonetet(O)
AminoglycosidesGEN241SaadE-Ccant(6)-Ia, aph(2″)-If, aph(2″)-Ig, aph(2″)-Ih, aph(2″)-IIIa, aph(3′), aph(3′)-IIIa, aph(3′)-VIIa, aadE, aad9, sat4.
PM in rpsL_K43R, rpsL_K88R.
aadE-sat4-aphA-3 Gene Cluster
a blaOXA-61, blaOXA-184, blaOXA-193, blaOXA-447, blaOXA-449, blaOXA-461, blaOXA-466, blaOXA-489, blaOXA-493, blaOXA-577, blaOXA-578, blaOXA-580, blaOXA-594, blaOXA-595, and blaOXA-603, blaOXA-623. b Operon cmeABC code for a multidrug efflux protein that contributes to resistance to different antimicrobial drugs. Abbreviations: AMP: ampicillin; AMC: amoxicillin–clavulanic acid; CIP: ciprofloxacin; ERY: erythromycin; TET: tetracyclin; and GEN: gentamycin.
Table 2. The Campylobacter prosthetic joint infections reported in the literature.
Table 2. The Campylobacter prosthetic joint infections reported in the literature.
YearSpeciesAge/SexJointUnderlying Disease or Relevant ExposureGIBCStoolJoint Fluid/Periprosthetic SpecimenSurgeryAntibiotic TreatmentRecoveryDuration of
Follow-Up
Ref.
1993C. fetus75/MHipChronic lymphocytic leukemia, prednisoneNoNDND
(inhibited a)
DAIRIMI + GEN (7 d)
AMO (LTAS)
Y2 m[7]
1994C. fetus68/FHiprheumatoid arthritis, prednisoneNoNDND+DAIRGEN + AZI (3 d)
CHL (4 w)
DFUE2 m[8]
2003C. fetus76/MKneeNoneNo+ND+No surgeryCTR (6 w)
CURa (9 m)
Y10 m[9]
2005C. fetus72/MKneeCattle farmerNoNDND+2SRGEN + CIP + RIF (3 w)
CIP (5 w)
Y6 m[10]
2005C. fetus72/MHipAlcohol abuse, chronic granulocytic leukemia,
hypertension
No+++DAIRCTR (3 w)
ROX (3 m)
Y
DFUE
2,5 y[11]
2012C. fetus71/FKneerheumatoid arthritis (corticosteroids + MTX),
diabetes mellitus, cardiomyopathy
NDNDNDNDNDCL +DOX (3 m)YND[12]
2013C. fetus70/FKneeliver cirrhosis, alcohol abuseND+ND+1SRAMC (6 w)
CIP + CL (6 w)
DFUEND[13]
2013C. fetus78/FHipNoneNDND+DAIRCL (8 w) + GEN (2 w)
AMO (LTAS)
Y5 y[13]
2013C. fetus88/MHipLung cancerND++No surgeryCL (4 w) + GEN (1 w)
CL (LTAS)
Y2 y[13]
2013C. fetus85/FHipLiver cirrhosis, alcohol abuseND++No surgeryAMO (4 w) + GEN (1 w)
AMO (LTAS)
Y3 y[13]
2013C. fetus52/FKneeNoneND++1SRAMC (6 w) + CL (1 w)
CL (6 w)
Y2 y[13]
2013C. fetus76/FKneeNoneND++DAIRCLR (4 w) + GEN (1 w)
CLR (8 w)
Y2 y[13]
2013C. fetus75/MHipRenal transplantND+++1SRCLR (4 w) + GEN (1 w)
CLR (8 w)
Y2 y[13]
2016C. fetus77/FKneeNDNDNDND+DAIRnot specified (3 m)YND[14]
2017C. fetus75/FKneeDiabetes mellitus, vascular diseaseYes++DAIRMER (6 w)
DOX (LTAS)
Y4 m[15]
2018C. fetus60/MHipDiabetes mellitus, immunosuppressive disease,
vascular disease
No+ND+2SRIMI + AZI (6 w)YND[16]
1993C. jejuni60/MHipAIDS, B cell lymphoma, hemophilia A,
liver cirrhosis
Yes+
(inhibited)
+No surgeryGEN + CIP (17 d)
ERY + CIP (8 w)
Y2 m[17]
2013C. jejuni77/MKneeimmunosuppressive diseaseNDND91SRAMC (6 w) + GEN (1 w)
CIP (16 w)
Y8 y[13]
2013C. jejuni75/MKneeThyroid cancer, hypertensionYes+ +
(PCR)
2SR1/MER + AZI (6 w)-> AZI (7 w)
2/MER (2 w)->AZI (LTAS)
Y3 m[18]
2020C. jejuni73/MKneeUlcerative colitisNo+ND2SR bETP (6 w)
MOX + AMC (8 w)
Y3 m[19]
2022C. jejuni60 *FHipScleroderma (no immunosuppressive therapy),
Raynaud’s phenomenon, chronic diarrhea
NoNDND+1SRLEV
(15/12 w before/after surgery)
Y21 m[20]
2009C. coli60/MHipobesity, hypertension
Ingestion of contaminated raw oysters
YesND+DAIRTIL (6 w)
CIP (3 w)
YND[21]
2019C. coli63/MHipNot immunocompromised
Ingestion of undercooked chicken
YesND+DAIRCIP (6 m)Y6 m[22]
2024C. coli61/FHipBariatric surgeryYes+++DAIRLEV (12 w)Y1 y
2002C. lari81/MHipCardiovascular disease
not immunocompromised
No+ND+DAIRPEN + FLU + GEN (2 d)Death < sepsis at D2ND[23]
2002C. upsaliensis24/MKneeOsteoblastic osteosarcomaYes
(inhibited)
+No surgeryCTR + MET (2 w)
CTR + ROX (4 w)
AMO + ROX (6 m)
Y34 m[24]
a Culture potentially inhibited by systemic antibiotics at the time of sampling. b Only one stage performed with retention of spacer. Abbreviations: GI: gastro-intestinal illness; BC: blood cultures; ND: not determined; DAIR: debridement, antibiotics and implant retention; LTAS: long-term suppression therapy; 1SR: one-stage reimplantation arthroplasty; 2SR: two-stage reimplantation arthroplasty; MTX: methotrexate; DFUE: death from unrelated event; AMO: antibiotics; AMC: amoxicillin, amoxicillin–clavulanic acid; AZI: azithromycin; CURa: cefuroxime axetil; CHL: chloramphenicol; CIP: ciprofloxacin; CTR: ceftriaxone; DOX: doxycycline; FLU: flucloxacillin; GEN: gentamycin; IMI: imipenem; LEV: levofloxacin; MER: meropenem; MET: metronidazole; MOX: moxifloxacin; PEN: penicillin; RIF: rifampin; ROX: roxithromycin; and TIL: ticarcillin–clavulanic acid. * a woman “in her sixties”.
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Jonckheere, S.; Mairesse, C.; Vandecandelaere, P.; Vanbiervliet, J.; Terryn, W.; Somers, J.; Prevost, B.; Martiny, D. Campylobacter coli Prosthetic Joint Infection: Case Report and a Review of the Literature. Pathogens 2024, 13, 838. https://doi.org/10.3390/pathogens13100838

AMA Style

Jonckheere S, Mairesse C, Vandecandelaere P, Vanbiervliet J, Terryn W, Somers J, Prevost B, Martiny D. Campylobacter coli Prosthetic Joint Infection: Case Report and a Review of the Literature. Pathogens. 2024; 13(10):838. https://doi.org/10.3390/pathogens13100838

Chicago/Turabian Style

Jonckheere, Stijn, Celestin Mairesse, Patricia Vandecandelaere, Jens Vanbiervliet, Wim Terryn, Jan Somers, Benoit Prevost, and Delphine Martiny. 2024. "Campylobacter coli Prosthetic Joint Infection: Case Report and a Review of the Literature" Pathogens 13, no. 10: 838. https://doi.org/10.3390/pathogens13100838

APA Style

Jonckheere, S., Mairesse, C., Vandecandelaere, P., Vanbiervliet, J., Terryn, W., Somers, J., Prevost, B., & Martiny, D. (2024). Campylobacter coli Prosthetic Joint Infection: Case Report and a Review of the Literature. Pathogens, 13(10), 838. https://doi.org/10.3390/pathogens13100838

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop