Cefepime induced acute interstitial nephritis – a case report

A 62 year old Caucasian female patient (height - 1.60 m, weight 72 kg, BMI 28.1) was admitted to hospital with AKI (patient’s baseline serum creatinine was 85 μmol/L and eGFR was 63 ml/min/1.73 m² by MDRD equation) whilst on treatment for mastoiditis. Her background medical history included hypertension, and type 2 diabetes for which she was on regular sitagliptin-metformin 50/1000 mg half tablet twice a day, metoprolol 25 mg twice daily, lisinopril 10 mg daily and simvastatin 40 mg daily. She had a long medical history of recurrent otitis media for which she required grommet insertion. She was managed as outpatient with topical and oral ciprofloxacin by her otolaryngologist. Trial of oral trimethoprim-sulphamethaxazole (Bactrim DS) was prescribed without much clinical improvement. Eight weeks prior to this admission, she had symptoms of earache, localised post auricular swelling and fever. A CT scan showed mastoiditis and a contiguous subperiosteal abscess. A brain Magnetic Resonance Imaging (MRI) scan and Technetium 99 m labelled bone scan which revealed osteomyelitis (OM) of the petrous temporal bone (Figure 1). She underwent an emergency cortical mastoidectomy with drainage of the abscess and insertion of a new right ear grommet. Empirical therapy with ticarcillin-clavulanate (12.4 grams/day) was commenced.

She made good progress and was discharged with a plan of continuing cefepime for 6 weeks as treatment of OM on ambulatory care basis. After 2 weeks of therapy, she developed malaise and dysgeusia. At 4 weeks, she developed renal impairment (serum creatinine-140 μmol/L) and the cefepime dose was reduced to 4 grams/day. Her blood pressure at time was 130/82 mmHg. There was no fever, rash or peripheral oedema. Urine analysis done by automated iQ200 (Iris Diagnostics, Chatsworth, CA) machine and manual phase contrast microscopy showed WBC of <10 × 10⁶ /L, no RBC and no presence of either WBC/RBC casts. 24 hour urine collection (of 2.47 L) had proteinuria of 0.77 g/day (normal range-0.08-0.15 g/day). C reactive protein was 3 mg/L (normal < 5 mg/L). At week 5 into therapy, she was noted to have worsening AKI (serum creatinine 225 μmol/L) and was admitted for further investigation (Figure 2). She suffered the ‘injury stage’ of AKI according to Risk Injury Failure Loss of kidney function and End stage renal failure (RIFLE) criteria and stage 3 of Acute Kidney Injury Network (AKIN) classification at admission [7]. At this stage she was also noted to have serum potassium of 6.1 mmol/L (range 3.5-5 mmol/L) ,serum sodium of 148 mmol/L (range 135-145 mmol/L), serum chloride was 90 mmol/L (range 97-107 mmol/L) and blood urea of 15 mmol/L (range 2.5-7.5 mmol/L). There were no new medications including non-steroidal anti-inflammatory drugs (NSAIDs), chinese herbal supplements or any other form of naturotherapy that were taken by her.

During her inpatient stay all medications except metoprolol were ceased. Though she was clinically euvolaemic and suffered from non-oliguric renal failure, 36 hours trial of intravenous hydration with normal saline (0.9% w/v) at 80 ml/hour was administered with minimal effect on serum creatinine, blood urea and serum electrolytes. Marginal increase of urine output was noted which was commensurate with the intravenous fluid administered. Laboratory investigations of aetiology of AKI were negative or not detected. This included: Double stranded DNAs, ANCA, extractable nuclear antigens, rheumatoid factor, serum and urine protein electrophoresis, complement levels, immunoglobulin subclasses, streptococcal serology and hepatitis B and C serology. An ANA titre of 1:1280 (homogenous pattern) was noted and was thought to be related as a reaction due to cefepime therapy. Renal ultrasound revealed normal renal size, parenchyma and no obstructive uropathy. A renal biopsy showed moderate tubular atrophy with many intra-tubular casts in the medullary area. A few tubules were distended with cellular debris and acute inflammatory exudate (acute tubulitis). Moderate interstitial fibrosis was present with patchy areas of inflammatory infiltrates comprising predominantly lymphocytes, plasma cells and neutrophils. Eosinophils were not detected in the renal biopsy. Periodic acid Schiff stain and Gomori -silver stain were negative on the biopsy. Immunofluorescence staining was negative for IgA, IgG, IgM, kappa and lambda light chains, C1q, C3, amyloid and fibrinogen. Electron microscopy did not reveal any glomerular abnormality. (Figure 3)

It was concluded that this patient had drug-induced AIN, most likely related to cefepime. Cessation of the antibiotic led to a rapid improvement in her renal function over a week and therefore it was decided to treat her conservatively. The serum creatinine dropped from 295 μmol/L to 170 μmol/L within a week and then continued to trend downwards reaching up to 150 μmol/L on her 2 weekly follow-up post discharge. Her symptoms of malaise and dysgeusia had also abated at this visit. All the electrolytes (sodium, potassium and chloride) including blood urea were within normal ranges at this stage. Corticosteroid was not administered due to partially treated infection, diabetes and rapid improvement in renal function after cessation of antibiotics.

For completion of therapy (another 2 weeks) oral ciprofloxacin 500 mg twice daily was commenced, mindful of the fact that the isolate was resistant to ciprofloxacin with a minimal inhibitory concentration of 4 mg/L. Following discharge from hospital, she remained asymptomatic and continued to improve from her infection perspective. Sitagliptin-metformin, lisinopril and simvastatin were slowly reintroduced over the next 3 months after discharge while her renal function continued to improve.

Table 1 shows the temporal trend in the biochemical parameters including serum creatinine and eGFR. Although serum creatinine has plateaued, mild renal impairment still exists at 8 months of follow-up (serum creatinine of 130 μmol/L and eGFR of 56 ml/min/1.73 m²).

This adverse drug reaction has been recorded permanently in her electronic medical records and also has been reported to Australian Therapeutic goods administration (TGA).

Written consent was obtained from the patient for this publication. A copy of written consent is available for review by the editor of this journal.