Submitted:
25 April 2025
Posted:
25 April 2025
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Abstract
Coxitis is an inflammation of the hip joint, often resulting in pain and functional decline. It can be caused by various factors, including avascular necrosis, trauma, and infection. We report a case of coxitis caused by MRSA in a patient with severe comorbidities, which posed significant diagnostic and therapeutic challenges, but ultimately resulted in a successful outcome, along with a brief literature review. To the best of our knowledge, there is limited literature on MRSA-induced purulent coxitis specifically in patients with HIV and tetraplegia, making this case particularly valuable for expanding the understanding of this rare and complicated condition.
Keywords:
coxitis
; MRSA
; HIV
; tetraplegia
; Girdlestone procedure
1. Introduction
Coxitis, or inflammation of the hip joint, most commonly affects the epiphyseal region and can lead to significant morbidity if left untreated. Clinically, it typically presents as pain localized to the groin or lower buttock, with possible radiation toward the knee. This pain is usually aggravated by physical activity and relieved with rest. The onset can be insidious, evolving gradually over months or even years, which often delays diagnosis and treatment. As the disease progresses, it can result in a marked decline in hip function and overall mobility.
The etiology of hip arthritis is diverse. It may stem from mechanical, inflammatory, metabolic, or infectious origins. Common causes include avascular necrosis, trauma, septic arthritis, and systemic conditions such as rheumatoid arthritis. Less commonly, metabolic bone disorders like Paget’s disease can contribute to degenerative changes. Certain anatomical abnormalities — such as developmental dysplasia of the hip and slipped capital femoral epiphysis — also predispose patients to early osteoarthritis due to abnormal joint mechanics.
Infectious coxitis, though relatively rare, represents a serious diagnostic and therapeutic challenge. Among bacterial causes, Staphylococcus aureus is the most frequently implicated pathogen, with methicillin-resistant Staphylococcus aureus (MRSA) posing particular concern due to its resistance profile and potential for aggressive joint destruction. Reports of MRSA-induced purulent coxitis are limited, and the condition is especially rare in patients with complex comorbidities [1,2].
This case is clinically significant because, in addition to the rarity of MRSA coxitis and sepsis, the patient presented with severe comorbidities — namely HIV infection and post-traumatic tetraplegia following a gunshot injury. Notably, the typical symptoms of coxitis, such as localized hip pain and limited range of motion, were absent in this case due to the patient’s neurological deficits. The lack of classical symptomatology significantly complicated the identification of the infection source and delayed diagnosis, underlining the importance of clinical vigilance in atypical presentations.
The aim of this publication is to report this unusual and diagnostically challenging case, accompanied by a brief review of the literature, in order to contribute to the limited understanding of MRSA-related coxitis in immunocompromised and neurologically impaired patients.
2. Case Report
A 38-year-old male presented with fever up to 39 °C accompanied by chills, general weakness, profuse sweating and a wound in the region of the left elbow joint. According to the patient, symptoms began approximately three weeks prior (around November 20), when he developed febrile fever with chills reaching 39.9 °C. He self-medicated with oral non-steroidal anti-inflammatory drugs and consulted a general practitioner, where a urinary tract infection was suspected and empiric antibacterial therapy was prescribed, though the specific regimen is unknown. Despite treatment, the condition did not improve, and febrile episodes persisted. The patient continued taking antipyretics, but without significant relief. Around the same time, a wound developed near the left elbow joint, which he managed with once-daily dressings using povidone-iodine solution. As his condition failed to improve, he contacted emergency medical services and was transported to the Emergency Department.
Upon initial examination, the patient experienced chills and profuse sweating. He was conscious, communicative, and oriented, responding to questions appropriately. The skin and visible mucous membranes appeared pale. The tongue was dry and coated. The pharynx, and tonsils appeared normal. Hemodynamics were stable, with regular heart rhythm and tachycardia with a heart rate of 106 beats per minute. Vesicular breath sounds were heard in the lungs without rales, and oxygen saturation was 99% on room air. The abdomen was soft on palpation, with no tenderness and normal bowel sounds. No peripheral edema was present. There were signs of tetraplegia. Importantly, the patient also had a purulent wound at the left elbow joint, because it moves by relying on its elbows, raising concerns about a potential source of systemic infection. In the area of the left elbow joint, a deep purulent wound measuring 3×4 cm in diameter was observed, with reddened wound edges. On the right elbow, there was a superficial abrasion. No wounds were found on the feet, although the skin was dry and scaly.
Initial laboratory results revealed leukocytes 7.94 ×10⁹/L, neutrophils 75.3%, hemoglobin 99 g/L, erythrocytes 3.34 ×10¹²/L, and platelets 439 ×10⁹/L. Biochemical analysis showed CRP 242.15 mg/L, creatinine 43 μmol/L, glucose 6.95 mmol/L, potassium 4.4 mmol/L, and sodium 128 mmol/L. Urinalysis showed leukocytes 25 per field and negative nitrites. Chest X-ray revealed no signs of pulmonary infiltrates. Due to persistent fever of unclear origin, the patient was transferred to the Department of Infectious Diseases for further diagnostic evaluation and treatment.
Notably, the patient has a complex medical history. In 2013, he sustained a gunshot wound to the neck resulting in a thoracic vertebra (Th5) injury and subsequent tetraplegia. He is also diagnosed with HIV and is on regular antiretroviral therapy, specifically Efavirenz 600 mg once daily and Abacavir/Lamivudine 600/300 mg once daily, with reported full adherence. The latest available outpatient laboratory results from November, 2018 showed a CD4+ count of approximately 290 cells/μL, HIV RNA load was undetectable. In addition, from October 17 to November 18, 2018, the patient was hospitalized for unclassified enteritis, during which he developed symptoms of constipation requiring enemas. He also reports an allergy to co-trimoxazole.
A thorough diagnostic evaluation was undertaken to identify the etiology and extent of the infection. Laboratory tests revealed markedly elevated C-reactive protein (CRP) levels ranging from 201 to 242.15 mg/L, consistent with a significant inflammatory response (Table 1). Creatinine levels were noted to fluctuate between 43 and 295.4 μmol/L, raising concerns about potential renal impairment secondary to sepsis. Hemoglobin levels were found to be decreased (74 to 99 g/L), indicative of anemia, often associated with chronic disease and severe infection. Leukocyte counts were from 7.9 x109/L to 3.8 x109/L over the course of hospitalization. Platelet counts ranged from 83 to 452 x109/L. Urinalysis showed the presence of leukocytes, erythrocytes, protein, and glucose, suggesting concurrent urinary tract infection or sepsis-related renal involvement.
Blood cultures returned positive for Methicillin-resistant Staphylococcus aureus (MRSA), confirming the presence of a systemic bacterial infection (Table 2). Culture of the wound at the left elbow also yielded MRSA, indicating a common pathogen responsible for both the systemic and localized infections.
In the urine culture, 107 CFU/ml of Klebsiella pneumoniae was isolated, which was moderately susceptible to amikacin, but susceptible to imipenem, meropenem, and resistant to ciprofloxacin, gentamicin, ampicillin, piperacillin/tazobactam, cefuroxime, cefotaxime, nitrofurantoin, trimethoprim/sulfamethoxazole, and trimethoprim. Additionally, Acinetobacter spp. was susceptible to gentamicin, amikacin, ampicillin/sulbactam, imipenem, and meropenem, but resistant to ciprofloxacin and trimethoprim/sulfamethoxazole. The culture from the tongue revealed a high amount of Candida albicans.
The patient was empirically treated with ceftriaxone for 1 day and piperacillin/tazobactam for 2 days. The treatment was adjusted based on the culture results. Patient was treated with vancomycin, meropenem (for suspected Klebsiella and Acinetobacter urinary tract infection) and fluconazole. Vancomycin serum concentration ranged between 14.3 µmol/L and 17.3 μg/mL. However, despite the treatment, the fever persisted, and the source of the infection was being investigated. Since the patient had undergone neck surgery after a gunshot injury and it was not clear whether there was an implant, additional tests were conducted to investigate a possible implant-related infection. Imaging studies, including X-ray and MRI of the neck were normal. Echocardiography was performed, with no evidence of endocarditis. X-ray and ultrasound examination of the left elbow were performed, with no fluid or destruction detected.
During a detailed repeat physical examination, crepitus was noted in the right hip area. Since the patient was tetraplegic, he did not feel any pain. X-ray of the hip demonstrated joint effusion and significant soft tissue swelling, strongly suggestive of a purulent process within the hip joint. These findings supported the clinical suspicion of purulent coxitis differentiating from avascular necrosis. A CT scan of the pelvis was performed, describing 6 fluid accumulations in the right hip joint and surrounding muscles. An orthopedic surgeon consultation was conducted, and the right hip joint was aspirated, yielding hemorrhagic (non-purulent) synovial fluid. No bacterial growth was observed in the synovial fluid, possibly due to prior antimicrobial treatment, and cytology showed numerous neutrophilic granulocytes (inflammatory changes) in the joint aspirate.
The patient was diagnosed with purulent coxitis secondary to MRSA infection. Given the severity of his presentation, the patient underwent surgery. Resection of the femoral neck (Girdlestone procedure) end removal of necrotic tissues and sequestra, debridement and irrigation with antiseptic solutions was performed during surgery. Combined antibacterial therapy with vancomycin and rifampicin was prescribed for treatment. The possibility of remaining chronic osteomyelitis cannot be ruled out. Subsequently, the treatment was changed to rifampicin 450 mg twice daily and tetracycline 100 mg twice daily (30 days) as a combination therapy.
Despite the severe nature of his infection, the patient responded well to the antibiotic therapy and surgery. His fever subsided, allowing for a reduction in inflammatory markers such as CRP. Renal function stabilized with supportive care, and hemoglobin levels began to recover with blood transfusion before and after the surgery. Upon repeating the blood cultures, no growth was observed. The purulent wound at the left elbow also showed signs of improvement with local wound care and systemic antibacterial therapy.
3. Discussion
Coxitis in immunocompromised patients is an understudied disease. Only a few articles study prevalence, etiological diagnosis, and treatment. Medical management of infection should be focused on adequate and timely drainage of the infected synovial fluid; administration of appropriate antibiotic(s); and debridement of any associated osteomyelitis or soft tissue infection with immobilization of the joint to control pain [3].
Coxitis starts with restrictive pain in the hip joint which radiates to the knee. The pain is expressed more in the external and internal rotation, and those movements are hard to execute. Anteflexion and retroflection among those patients are limited, and therefore their steps are short and slow. Movement restrictions are also found in adduction and abduction. The physical examination of patients with septic arthritis almost always reveals a severely painful joint with motion, often including an obvious effusion. The presentation is typically more subtle in those with periprosthetic joint infections, small joint infections, atypical infections (e.g., fungal, Lyme disease, tuberculosis), or immunosuppression, paralysis. An overlying skin infection can be the source of the entry point of the intra-articular infection. Septic arthritis should be considered in adults presenting with acute monoarticular arthritis. A delay in diagnosis and treatment of septic arthritis can lead to permanent morbidity and mortality. Subcartilaginous bone loss, cartilage destruction, and permanent joint dysfunction can occur if appropriate antibiotic therapy is not initiated within 24 to 48 hours of onset. The reported incidence of septic arthritis is four to 29 cases per 100,000 person-years, and risk increases with age, use of immunosuppressive medications, and lower socioeconomic status [1].
For this patient, the clinical diagnosis was initially complicated by tetraplegia and the absence of pain sensation. Differentiating avascular necrosis from septic arthritis involves a thorough clinical evaluation and imaging studies. Avascular necrosis typically presents with gradual onset of pain and limited range of motion in the affected joint, often following risk factors such as corticosteroid use or trauma. In contrast, septic arthritis usually manifests with acute onset of severe pain, swelling, and fever, indicating an infectious process. Laboratory tests, such as joint aspiration and culture, are crucial in identifying the presence of infection in septic arthritis, while MRI or X-rays may reveal changes indicative of avascular necrosis [4,5,6].
Pathogenesis of septic arthritis involves bacterial invasion of the synovial membrane which leads to inflammatory process producing the characteristic purulent synovial fluid observed with arthrocentesis. Septic arthritis most commonly occurs due to hematogenous seeding secondary to bacteremia, other causes include penetrating trauma and corticosteroids joint injections.
The diagnosis of septic arthritis is established with arthrocentesis of the effected joint. Cytosis (WBC of >50,000/μL) and polymorphonuclear cells of greater than 90% increase the likelihood of septic arthritis. Diagnosis and etiology are confirmed with gram stain and culture of the joint fluid. Risk factors for septic arthritis include age older than 60 years, recent bacteremia, degenerative arthritis, rheumatoid arthritis, metabolic syndrome, immunocompromised state, joint endoprostheses, skin infection and history of sexually transmitted diseases.
Antibiotics should initially cover gram-positive cocci because they are most common (in particular Staphylococcus). Gram-negative coverage should be considered for patients with other risk factors, such as older age, immunosuppression, or bacteremia from a urinary or gastrointestinal source. Treatment should be individualized according to clinical response and microbiology results. Septic arthritis caused by methicillin-resistant S. aureus requires drainage or debridement and three to four weeks of antibiotics. Parenteral options include intravenous vancomycin and daptomycin. Oral options include trimethoprim/sulfamethoxazole with rifampin, linezolid, and clindamycin, but there is no specific guidance regarding the duration of intravenous therapy before initiation of oral therapy [3,5].
Rifampicin has been recognized as an effective treatment option for native joint infections, particularly when caused by Staphylococcus aureus, including MRSA. Studies have shown that rifampicin, when used in combination with other antibiotics, can enhance bioavailability and penetrate into biofilms, thereby improving therapeutic outcomes in septic arthritis. Furthermore, its unique mechanism of action, which inhibits bacterial RNA synthesis, makes rifampicin particularly valuable in treating chronic infections associated with prosthetic devices. However, the emergence of resistance and potential drug interactions necessitate careful monitoring and consideration of the patient’s overall antibiotic regimen. Additionally, the role of rifampicin in the management of native joint infections should be weighed against its pharmacokinetic properties and the necessity of combination therapy to optimize clinical outcomes and minimize the risk of relapse [7,8].
The literature review indicates that individuals with HIV have an increased risk of MRSA infections, though most of these infections are related to skin and soft tissue [9].While there is a reported case of a paraplegic patient developing MRSA-induced necrotizing fasciitis, there are no specific reports in the literature regarding MRSA-induced coxitis in patients with HIV and tetraplegia [10].
Due to the rarity of MRSA-induced coxitis in immunocompromised patients, especially those with neurological impairments, further clinical observations and reports are needed. Sharing similar cases could help raise awareness, improve recognition of atypical presentations, and support more timely diagnosis and treatment in the future.
4. Conclusions
This case highlights the interplay between systemic infection, immunocompromised status, and joint infection, emphasizing the need for vigilant monitoring and prompt treatment in similar clinical scenarios. Multidisciplinary collaboration is essential to optimize outcomes for patients with purulent coxitis, especially when underlying conditions complicate the clinical picture. Purulent coxitis, a rare but severe infection of the hip joint, presents significant challenges in immunocompromised patients, such as those with HIV. In this case, the patient’s immunocompromised status and MRSA infection contributed to the development of purulent coxitis. Early recognition and aggressive management are crucial to prevent joint destruction and systemic complications. This case underscores the importance of comprehensive care, including antibiotic therapy and surgical intervention, in managing such complex infections.
Author Contributions
EB participated in the design of the study, in the interpretation of data, and drafted the manuscript. JL participated in the design of the study, in the interpretation of data, and drafted the manuscript. DS participated in acquisition of data, revised critically the manuscript. MR participated in acquisition of data, revised critically the manuscript. DV participated in the design and coordination of the study and helped to draft the manuscript. All authors read and approved the final manuscript.
Funding
This research received no external funding. Publication costs – Lithuanian University of Health Sciences.
Informed Consent Statement
The patient provided written consent. This report does not include elements that require approval from the local institutional review board.
Acknowledgments
We acknowledge all healthcare professionals for their outstanding efforts and dedication to the care of the patient.
Conflicts of Interest
The authors declare no conflicts of interest.
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Table 1.
Blood results.
| Dec 14, 2018 | Dec 20, 2018 | Dec 27, 2018 | Jan 7, 2019 | Jan 10, 2019 | Jan 10, 2019 | Jan 15, 2019 | Jan 18, 2019 | Jan 24, 2019 | Jan 25, 2019 | |
| Leucocytes (x109/L) | 7.94 | 7.9 | 5.5 | 3.8 | 6.7 | 5.3 | 4.9 | |||
| Hemoglobin(g/L) | 99 | 97 | 86 | 79 | 82 | 74 | 85 | |||
| Platelets (x109/L) | 439 | 413 | 452 | 163 | 331 | 83 | 167 | |||
| Neutrophils (%) | 75.3 | 70 | 58.3 | 59.7 | 77.6 | 67.4 | 65.9 | |||
| Potassium (mmol/L) | 4.4 | 4.1 | 3.9 | 4 | 3.77 | 3.88 | 2.8 | 3.4 | ||
| Sodium (mmol/L) | 128 | |||||||||
| Creatinine (µmol/L) | 43 | 41 | 47 | 44.3 | 295.14 | 201 | 111 | |||
| AST (U/L) | 79 | 25 | 19 | |||||||
| ALT (U/L) | 89 | 17 | 12 | |||||||
| SPA (%) | 68 | 65 | ||||||||
| INR | 1.2 | 1.2 | ||||||||
| CRP (mg/L) | 242.15 | 91 | 147 | 201 | 110 | 80.3 | 44.1 | |||
| ESR (mm/h) | >170 | 168 |
Table 2.
Blood and wound cultures results.
| Antibacterial agents | Staphylococcus aureus |
|---|---|
| Penicillin | R |
| Oxacillin | R |
| Gentamicin | S |
| Tetracycline | S |
| Fusidic acid | S |
| Erythromycin | R |
| Clindamycin | R |
| Vancomycin | S |
| Trimethoprim/sulfamethoxazole | S |
| Rifampicin | S |
| Linezolid | S |
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