COVID-19 Presenting as Lupus Erythematosus-Like Syndrome

The 2019 coronavirus disease (COVID-19) infection had newly emerged with predominant respiratory complications. Other extrapulmonary features had been recently described. Here, we describe a COVID-19 patient presenting with multiorgan involvement mimicking systemic lupus erythematosus. He was successfully treated with glucocorticoids and tocilizumab.

C oronavirus disease (COVID-19) uses angiotensin converting enzyme 2 as its functional receptor to infect endothelial target cells in lung, kidney, liver, heart, and the gastrointestinal tract. Therefore, in addition to respiratory symptoms that usually dominate the clinical presentation, there is recent increasing data showing that this novel coronavirus has potential extrapulmonary complications. Here, we report the case of the COVID-19 infection with multiorgan dysfunction, simulating systemic lupus erythematosus (SLE) presentation.
A 62-year-old man with no medical history was referred by his primary care physician to our Department of Internal Medicine on April 4, 2020, for shortness of breath associated with a kidney injury. He suffered from fever, cough, and myalgia 17 days before. On examination, the temperature was 39°C, the blood pressure 105/85 mm Hg, and the heart rate 97 beats per minute. His oxygen saturation was 94% on room air. He had bibasilar rales. A neuropsychiatric examination showed acute confusion, disorientation in time and space, and behavioral disorders. He had dysexecutive syndrome consisting of slowed thinking, information processing impairment, memory loss, inattention, and poorly and slowed organized movements in response to command. Laboratory tests showed the white blood cell count at 10 900/mm 3 , lymphopenia at 800/mm 3 , 0 eosinophils per mm 3 , mildly increased liver enzymes, elevated C-reactive protein (CRP) concentration and procalcitonin at 208 mg/l and 2.41 ng/ml, respectively. Protein electrophoresis showed hypoalbuminemia at 19.7 g/l and elevated α 2 globulin at 11.8 g/l. He had a blood urea nitrogen at 7 μmol/L, blood creatinine at 204 μmol/L with an estimated glomerular filtration rate (EGFR) at 38 mL/min/1.73 m 2 . His baseline creatinine level was unknown. A urinalysis showed the protein-to-creatinine ratio at 233 mg/mmol with no evidence of hematuria, sodium 9 mmol/L, and potassium 36 mmol/L. Blood and urine cultures were negative. The laboratory results are shown in Table 1.
Investigations for mycoplasma pneumoniae, human immunodeficiency virus, influenza A and B, hepatitis A, B, and C, and antineutrophil cytoplasmic antibodies were negative. Serum Complement 3 and 4 levels were normal. Antinuclear antibodies (ANA) were positive at 1/160. Anti-double stranded (ds) DNA and anti-extractable nuclear antigen antibodies were negative. A cerebrospinal fluid (CSF) examination and brain magnetic resonance imaging were normal. A lung computed tomography (CT) imaging revealed extensive lesions with ground-glass opacities, consolidations, and a crazy paving pattern with the extent of the lesions at 25% ( Figure 1A). A CT scan of the abdomen and pelvis showed normal-sized kidneys with permeable arteries and urinary tract. In view of the pandemic context, reverse-transcriptasepolymerase-chain-reaction (RT-PCR) test for the virus responsible for COVID-19, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), was performed. It was positive in the nasopharyngeal swab, nevertheless, and it was negative in CSF.
The patient was started on empiric antibiotics (Rovamycine and ceftriaxone) and prophylactic anticoagulation. Three days after, the oxygen flow rate was progressively increased to 6 L/min. He had tachycardia at 120/min. His renal function worsened with his respiratory distress. Blood creatinine continued to rise to 325 μmol/L. His urine output remained between 1500 and 1800 ml/day. He was given curative anticoagulation due to pulmonary embolism suspicion. Angio CT of the thorax was not performed due to his renal function deterioration. He received progressive intravenous hydration with little improvement of his creatinine level that subsequently stabilized at 260 μmol/L.
On Day 10, the patient's hypoxemia progressed requiring an oxygen flow at 12 L/min. He remained febrile at 39°C. A clinical examination showed cognitive and motor disorders worsening. Repeat kidney laboratory tests were notable for acute organic kidney injury (EGFR 28 ml/min/1.73 m 2 , urine sodium: 40 mmol/l, urine potassium: 29 mmol/l) with a protein-to-creatinine ratio at 200 mg/mmol, hematuria at 200/mm 3 , and leukocyturia at 100/mm 3 . Urine culture remained negative. An angio CT of the thorax, abdomen, and pelvis showed significant worsening of pulmonary lesions extent between 50 and 75% (see Figure 1B) with no evidence of embolism and splenomegaly. With a persistent fever, simultaneous declining of pulmonary, renal, and neurological status and biological inflammatory parameters rising, the treatment had been started with 120 mg of intravenous methylprednisolone for 2 repeated doses, tocilizumab (TCZ) at 600 mg, and

COVID-19 Mimicking Lupus Erythematosus
Tazocilline. Two days later, corticoids were decreased to 80 mg for 2 days then 40 mg for 2 more days.
On Day 14, the oxygen requirement was progressively decreased, the neurological status was gradually improved, serum creatinine level decreased to 115 μmol/L, and inflammatory parameters regressed. After 22 days in the hospital, the patient was weaned from oxygen and transferred to a rehabilitation facility.
One month later, the patient had a normal neurological status. His serum creatinine level was stable at 120 μmol/L with EGFR at 62 ml/min/1.73 m 2 . His urinalysis showed the proteinto-creatinine ratio at 57 mg/mmol with neither hematuria nor leukocyturia. A lung CT scan revealed a significant improvement of his pulmonary lesions (see Figure 1C).
Lupus-like syndrome is usually induced by drugs, more rarely by infections activating autoimmune response by transient positive autoantibodies, which can be associated with lupus-like symptoms such as malar rash, arthralgia, nephritis, and acute hepatitis. 1 Our patient's clinical presentation, including glomerular syndrome with significant proteinuria and hematuria, neuropsychiatric symptoms, lymphopenia, and positive ANA, fulfilled the 2012 Systemic Lupus International Collaborating Clinics revised classification criteria. Hepatitis and interstitial pneumonia could be considered as supporting criteria for this diagnosis. Nevertheless, an anti-Sm (Smith antibody) and anti-dsDNA antibody test are more specific than ANA for lupus nephritis, which is usually associated with complement consumption. Therefore, the age and male gender of our patient, elevated CRP and procalcitonin, low ANA titer, negative anti-dsDNA and anti Sm, and normal serum complement level called into doubt the diagnosis of SLE. The diagnosis of COVID-19 with multiorgan damages was more probable.
Recently, some publications have illustrated the renal invasive potential of COVID-19. Notably, acute kidney injury (AKI) is noted in 9.2% of population in South Korea. 2 In Cheng et al.'s large prospective cohort study including 701 patients with COVID-19, 3 the prevalence of proteinuria, hematuria, EGFR under 60 ml/min/1.73m 2 , and AKI occurring during the study period was 43.9%, 26.7%, 13.1%, and 5.1%, respectively. A Chinese report on a renal histopathological analysis of 26 autopsies of patients with COVID-19 revealed acute proximal tubular injury, vacuolar degeneration, erythrocyte aggregation in peritubular and glomerular capillaries, glomerular fibrin thrombi, ischemic changes, and severe endothelial injury. 4 COVID-19 particles were identified in the cytoplasm of renal proximal tubular epithelium, as well as in the podocytes with positive COVID-19 nucleoprotein in tubules by an indirect fluorescence method. Interestingly, rare cases of glomerulonephritis in patients with COVID-19 have been described. 5 In addition to direct virus mediated injury, kidney involvement with a COVID-19 infection could be due to systemic hypoxia, hypercoagulability, microangiopathy, rhabdomyolysis, sepsis, cytokine storm, and angiotensin II pathway activation. 6 Our patient had no cardiovascular factors risk. His volume contraction due to decreased oral input and insensible fluid loss associated with fever contributed to AKI, which explained little improvement of his renal function after fluid resuscitation. His urine dipstick test was compatible with glomerular syndrome and probable tubular disorders. Unfortunately, he did not have a renal biopsy because of safety concerns.
There is also an increasing evidence of central neurological complications of COVID-19, including headaches, acute stroke, 7  Kidney and neurological complications were described in critically ill patients with COVID-19. 3,7 Renal involvement is considered a new predictor of patient deterioration. It correlates with a poor prognosis and is associated with a higher risk of mortality. 3 In recent reports, TCZ has been used in patients with COVID-19 and severe pulmonary involvement showing encouraging results with reduced ventilatory support requirements, especially in those with cytokine storm and higher IL-6 levels. 9,10 The most used medications in COVID-19 patients with renal complications are diuretics, glucocorticoids, antivirus, and renal replacement therapy. 3 To our knowledge, preliminary data on TCZ use in kidney complications are very limited. Interestingly, our patient was successfully treated with glucocorticoids and TCZ, preventing admission in ICU with significant improvement of kidney, respiratory, neurological, and liver damages.
COVID-19 can induce kidney, neurological, liver, and vascular damage with possible positive ANA simulating multisystem inflammatory disease. Renal dysfunction is rare during this infection and usually associated with a fatal clinical course. Fortunately, our patient was discharged from the hospital with favorable outcome after glucocorticoids and TCZ treatment. Therefore, regulatory monitoring of inflammatory parameters, creatinine, and urine sample analysis allows an early disease worsening prediction leading to appropriate therapeutic options onset in critically ill patients.

COVID-19 Mimicking Lupus Erythematosus
Disaster Medicine and Public Health Preparedness