Can the SARS-CoV-2 infection trigger systemic lupus erythematosus? A case-based review.

Systemic lupus erythematosus (SLE) is an autoimmune and multisystemic chronic inflammatory disease that can affect various organs, including skin, joints, kidneys, lungs and the nervous system. Infectious agents have long been implicated in the pathogenesis of SLE. The new viral infection caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has shown that, in genetically predisposed patients could trigger the presentation or exacerbation of the autoimmune disease. We herein report a case of a 45-year-old man who presented respiratory symptoms, bilateral pleural effusion, ascites, splenomegaly, severe thrombocytopenia and renal failure with proteinuria and hematuria. SARS-CoV-2 PCR confirmed the COVID-19 diagnosis. We diagnosed the patient with SLE based on the clinical manifestations and positive immunological markers (2019 European League Against Rheumatism/American College of Rheumatology, score of 18). Glucocorticoid pulses were administered to the patient, which improved renal function. However, thrombocytopenia was also refractory to IV immunoglobulin and rituximab, so the patient underwent splenectomy. Through a systematic search of the medical literature, we retrieved two cases with newly onset SLE and five cases with previous SLE diagnosis that showed activity of the disease due to SARS-CoV-2 infection. We herein present a systemic review of these cases and discuss the clinical manifestations that could help to the diagnosis of this clinical condition.

Introduction

Systemic lupus erythematosus (SLE) is a multisystemic, chronic and potentially fatal autoimmune disease that causes alterations in various steps of the immune cascade, resulting in a remarkable heterogeneity of clinical manifestations, including those at the cutaneous, musculoskeletal, hematological, renal and neurological levels, among others [1, 2]. The natural history of SLE ranges from an insidious slow and progressive disease, with exacerbations and remissions, to an acute and rapidly fatal disease. It is one of the most common autoimmune diseases, especially among Afro-Americans, Hispanic and Asian populations. The highest frequency of SLE is observed in women in the reproductive period with a female:male ratio of up to 9:1 [1]. The leading causes of death in SLE patients include renal disease, severe disease flares with significant organ damage and infections [3]. The most recent 2019 European League Against Rheumatism (EULAR)/American College of Rheumatology (ACR) classification criteria include positive antinuclear antibody (ANA) positive antinuclear antibodies as mandatory criteria followed by criteria grouped into 7 clinical domains (constitutional, hematological, neuropsychiatric, mucocutaneous, serous, musculoskeletal, renal) and 3 immunological domains (antiphospholipid antibodies, complement proteins, SLE-specific antibodies) weighted from 2 to 10. Patients accumulating ≥ 10 points are classified with SLE with a sensitivity of 96.1% and a specificity of 93.4% [4].

The etiology of SLE remains unknown, although both exogenous and endogenous factors have been found to influence its pathogenesis, with infectious agents playing an important role in genetically predisposed individuals [5]. Various pathogens have been implicated in the development of SLE, especially viruses such as human endogenous retroviruses, Epstein-Barr virus, parvovirus B19, cytomegalovirus and human immunodeficiency virus type 1 [6]. These agents can contribute to the pathogenesis of the disease by triggering autoimmunity through various mechanisms including structural or functional molecular mimicry, encoding proteins that induce cross-reactive immune responses to self-antigens or modulate antigen processing, activation, or apoptosis of B and T cells, macrophages or dendritic cells [6-8]. Coronavirus disease 19 (COVID-19), a newly emerged respiratory disease caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), has recently become pandemic. The COVID-19 pathophysiology has shown that in genetically predisposed patients, it could lead to the presentation or exacerbations of autoimmune diseases [9]. Hence, we present the case of a patient who developed SLE probably triggered by a SARS-CoV-2 infection and we also conducted a review of the literature.

Case report

A 45-year-old Hispanic man was admitted in the emergency department with dry cough, malaise, myalgia, arthralgia, fever and swelling of the legs. The patient’s symptoms started 3-weeks before with recurrent episodes of fever, dry cough, myalgia and arthralgia, which had worsened during the last week and adding edema of the legs. A general practitioner prescribed azithromycin, acetylsalicylic acid, paracetamol, and oseltamivir 2 weeks after the onset of symptoms. The patient was previously healthy, without a history of drug abuse or a family history of autoimmune diseases. Initial physical examination revealed a body temperature of 37.1 °C, a blood pressure of 116/70 mmHg, a pulse of 102 beats per minute, and a respiratory rate of 22 breaths per minute. Pulse oximetry showed an oxygen saturation of 92% in room air. His throat was hyperemic. No abnormalities were detected on auscultation of the lungs and heart. No lymphadenopathy or hepatosplenomegaly were found. He had edema of the lower extremities (1 +). Initial laboratory studies showed hyperazotemia (creatinine 2.53 mg/dL [normal range (NR) 0.7–1.2 mg/L], urea 107.96 mg/dL (NR 10–50 mg/dL), hypoalbuminemia (2.5 g/dL, NR 3.4–4.8 g/dL), thrombocytopenia (13.000/μL, NR 150.000–450.000/μL), mild anemia (11.8 g/dL, NR 14.0–18.0 g/dL), prolonged activated partial thromboplastin time (39.2 s, NR 24.0–35 s) and elevated fibrinogen (706 mg/dL, NR 200–400 mg/dL). Chest X-ray showed bilateral reticular pattern with vascular enlargement (Fig. 1). Abdominal ultrasonography revealed small bilateral pleural effusion, peritoneal fluid and splenomegaly. The SARS-CoV-2 polymerase chain reaction (PCR) with nasopharyngeal swab was positive.

Fig. 1

Chest X-ray showed bilateral reticular pattern with vascular enlargement

The patient was admitted to the isolation area for COVID-19 patients of the Department of Internal Medicine; therapy with dexamethasone 6 mg IV/day, ceftriaxone 1 gr IV twice daily, furosemide 20 mg IV twice daily and paracetamol 1 gr PO was started. Further investigation revealed D-dimer of 3437 ng/mL (NR 0.0–222 ng/mL), C-reactive protein (CRP) of 154.09 mg/L (NR 0.0–5.0), ferritin level of 1752.21 ng/mL (NR 17.9–464.0 ng/mL), urinalysis with albuminuria (0.25 g/24 h) and erythrocyturia. Immunologic test showed signs of autoimmune disease, including antinuclear antibodies (ANA) 1:1280 positive antinuclear antibodies with coarse speckled pattern, anti-double-stranded (ds) DNA 23 IU/mL (negative < 20 IU/mL), anti-SSA 83.44 IU/mL (negative < 20 IU/mL), anti-SSB 26.754 IU/mL (negative < 20 IU/mL), complement C3 71.4 mg/dL (NR 90–177 mg/dL) and immunoglobulin IgG 1790 mg/dL (NR 770–1510 mg/dL). Serology tests for human immunodeficiency virus (human T-lymphotropic virus-1 and virus-2), hepatitis B virus and hepatitis C virus were negative. TORCH profile was positive to anti-rubella IgG antibodies and anti-herpes simple IgG antibodies (Table 1). The clinical and laboratory findings led to the diagnosis of SLE (2019 ACR/EULAR score of 18).

Table 1

Laboratory characteristics of the patient

Laboratory values (reference range and units)	Initial values	Peak/nadir values	After treatment
Hemoglobin (14.0–18.0 g/dL)	11.8	10.2	10.6
Platelets (150.000–450.000/μL)	13,000	5000	34,000
Leukocytes (4000–13,500/μL)	7250	10,330	4610
Neutrophils (2000–6900/μL)	4240	8780	3360
Lymphocytes (600–3400/μL)	1890	770	1040
Creatinine (0.7–1.2 mg/dL)	2.53	2.8	0.25
Urea (10–50 mg/dL)	107.96	281.5	45.2
BUN (7.0–18 mg/dL)	58.41	125.42	20.89
Creatinine kinase (38–174 U/L)	32.82	195	28
SGOT (10–50 U/L)	38.12	66.8	16.9
SGTP (10–40 U/L)	20.69	70.9	12.4
Alkaline phosphatase (40–129 U/L)	165	362	120
GGT (8.0–61.0 U/L)	65	352	92
LDH (240–480 U/L)	439.7	444.7	139
Ferritin (17.9–464.0 ng/mL)	1752.21
CRP (0.0–5.0 mg/L)	154.09	167.36	6.19
D-dimer (0.0–22 ng/mL)	3437	3983
Fibrinogen (200–400 mg/dL)	706	604	307
INR (0.73–1.26)	1.2	1.1	0.96
PT (11.8–15.6 s)	13.9	11.8	11.1
aPTT (24.0–35.0 s)	39.2	34.2	26.8
ANA (negative titers < 1:20)	Titers 1:1280, coarse speckled pattern
Anti-double-stranded DNA antibodies (negative < 20 U/mL)	23
Anti-Smith (negative < 20 U/mL)	1.655
Anti-RNP (negative < 20 U/mL)	3.319
Anti-SSA (negative < 20 U/mL)	83.44
Anti-SSB (negative < 20 U/mL)	26.754
Anticardiolopin IgM (negative < 20 U/mL)	< 2.0
Anticardiolipin IgG (negative < 20 U/mL)	< 2.0
Complement C3 (90–177 mg/dL)	71.4
Complement C4 (15–45 mg/dL)	16
Immunoglobulin IgG (770–1510 mg/dL)	1790
Immunoglobulin IgA (134–297 mg/dL)	192.9
Immunoglobulin IgM (67–208 mg/dL)	78.3
Anti-HIV 1/HIV 2 antibodies (negative < 1.0 S/CO)	0.1
HBsAg (negative < 1.0 S/CO)	0.14
HCAc (negative < 1.0 S/CO)	0.07
Anti-toxoplasma gondii IgG antibodies (negative < 1.0 U/mL)	0.13
Anti-toxoplasma gondii IgM antibodies (negative < 0.79 INDEX)	0.21
Anti-rubella IgG antibodies (negative < 10 U/mL)	37.41
Anti-rubella IgM antibodies (negative < 0.80 S/CO)	0.25
Anti-herpes simplex IgG antibodies (negative < 0.9 U/mL)	20.4
Anti-herpes simplex IgM antibodies (negative < 1.0 S/CO)	0.6
Anti-cytomegalovirus IgG antibodies (negative < 0.5 U/mL)	201.5
Anti-cytomegalovirus IgM antibodies (negative < 0.69 INDEX)	0.178
Urine albumin (negative, g/24 H)	0.25
Urine hemoglobin (negative, mg/dL)	250

aTTP activated partical thromboplastin time, ANA antinuclear antibodies, Anti-dsDNA anti-double-stranded deoxyribonucleic acid antibodies, Anti-RNP anti-ribonucleoprotein, BUN blood urea nitrogen, CRP C-reactive protein, GGT gamma-glutamyl transaminase, HBsAg hepatitis B surface antigen, HCAc hepatitis C antibody, HIV human immunodeficiency virus, LDH lactate dehydrogenase, PT prothrombine time, SGOT serum glutamate-oxalate transaminase, SGTP serum glutamate-pyruvate transaminase

With the initial treatment, the patient showed improvement in constitutional and respiratory symptoms. However, his renal function worsened [blood urea nitrogen (BUN) 125.42 mg/dL, urea 281.5 mg/dL] with persistent severe thrombocytopenia (< 10,000/μL) and abnormal liver function tests [serum glutamate-oxalate transaminase (SGOT) 66.8 U/L, serum glutamate-pyruvate transaminase (SGTP) 70.9 U/L, alkaline phosphatase 362 U/L, gamma-glutamyl transaminase (GGT) 352 U/L]. The patient received pulse methylprednisolone therapy (1 g IV for 5 days) and chloroquine 150 mg per day was initiated. After this treatment, kidney and liver functions improved markedly. Due to persistent severe thrombocytopenia, the patient was administered IV immunoglobulin (2 mg/kg/for 4 days) and rituximab 600 mg (3 doses) without a satisfactory response (< 10,000/μL). Finally, the patient underwent splenectomy, raising his platelets to 38,000/μL and without evidence of bleeding. The patient was discharged on prednisone 60 mg daily and chloroquine 150 mg per day.

Search strategy

According to the published guidance on narrative reviews [10], a literature search from December 2019 (when SARS-CoV-2 was first reported) to November 2, 2020 in PubMed and Scopus with MeSH search terms “Lupus Erythematosus Systemic” and “Severe Acute Respiratory Syndrome Coronavirus 2” or “Coronavirus” or “COVID-19” was performed. Case reports of patients with SARS-COV-2 infection and diagnosis of SLE (new onset or previous SLE diagnosis) with activity triggered (defined as a measurable increase in disease activity in one or more organ or systems involving new or worse clinical signs and symptoms and/or laboratory measurements) were included. Publications without restrictions in the language were eligible for inclusion. We extracted the following data from the selected papers: age, sex, SLE duration, clinical symptomatology, laboratory tests (including immunologic profile), antiviral therapy, SLE therapy, complications and outcome.

Discussion

A total of 78 potentially relevant citations were identified. After removing the duplicate citations, title and abstracts of 48 articles were evaluated, and 9 relevant articles were reviewed to detail. Seven case reports were found to be relevant for this research (Fig. 2) [11-17]. With the present report, a total of 8 cases were included for this review. Of the 8 patients (including ours), 6 (75%) were women with a median age of 48 (range 18–85) (Table 2). Five cases (63%) occurred in patients with a previous history of SLE (one case with associated antiphospholipid syndrome and another case with end-stage renal disease secondary to WHO Class IV lupus nephritis) [11, 12, 14, 16, 17]. The nonspecific clinical manifestations reported were fever in 5 cases [12,13,16,17 and the present report], malaise in 3 cases [13,17 and the present report], 1 case with headache [14] and 1 case with myalgia and arthralgia [present report]. Organ-specific manifestations reported were pulmonary (cough in 4 cases [13,14,17 and present report]), shortness of breath in 4 cases [12-14], chest discomfort in 1 case [11] and peripheral cyanosis in 1 case [15]), cardiovascular (2 cases with circulatory collapse [13, 15]), hematological (hemoptysis in 1 case [16], gingival bleeding in 1 case [11] and 1 case with diffuse purpuric rash [14]) and renal (edema in 2 cases [15 and the present report]) features. Laboratory findings included anemia in 3 cases (one with confirmed immune hemolysis) [13,14 and the present report], thrombocytopenia in 6 cases (5 with severe thrombocytopenia [< 50.000/μL]) [11,13–16 and the present report], lymphopenia in 5 cases [11–13, 15, 17], hyperazotemia in 4 cases [13,15,17 and the present report], increased transaminases in 1 case [present report], hyperbilirubinemia in 1 case [14], increased LDH in 4 cases [12, 13, 15, 17], elevated CRP in 6 cases [11,13–15,17 and the present report], hyperferritinemia in 4 cases [13,15,17 and the present report], prolonged prothrombin time in 1 case [14], prolonged activated partial thromboplastin time in 4 cases [11,13,14 and the present report], prolonged international normalized ratio in 2 cases [13, 16], elevated fibrinogen in 2 cases [14 and the present report], elevated D-dimer in 5 cases [12–14,17 and present report], proteinuria in 3 cases [13,15 and the present report] and hematuria in 3 cases [13,15 and the present report]. Immunological tests showed low serum complement in 5 cases [12–14,17 and the present report], high titer of ANA in 4 cases [13,15 and the present report], high titers of anti-dsDNA antibodies in 4 cases [12,13,17 and the present report], anti-Ro/SSA antibodies in 1 case [present report], positive anti-La/SSB antibodies in 1 case [present report], positive lupus anticoagulant in 3 cases [11, 13, 14], positive anticardiolipin antibodies in 2 cases [13, 14], and positive anti-β2-glycoprotein 1 antibodies in 2 cases [13, 14]. Reported SLE activity was hematologic in 6 patients [11,13–16 and the present report], serosal in 3 patients [13,15 and the present report], renal in 3 patients [13,15 and the present report] and pulmonary in two patients [13, 17]. The diagnosis of SARS-CoV-2 infection was made by PCR test in 7 patients [11–14, 16, 17] and by serologic test in 1 patient [15]. Imaging studies found bilateral pleural effusion in 3 cases [13,15 and the present report], patchy ground-glass opacities in 5 cases (one with chronic interstitial lung fibrosis) [12–14, 16, 17], bilateral reticular pattern with vascular enlargement in 1 case [present report], pericardial effusion with tamponade in 1 case [13] and impaired left ventricle ejection fraction in 1 case [13]. The treatment used in patients with a previous diagnosis of SLE included hydroxychloroquine-belimumab-azathioprine-warfarin [16]; hydroxychloroquine-mycophenolic acid [12, 17]; prednisone [11]; and no therapy [14]. Treatment for COVID-19 was administered in 4 patients, remdesivir in 1 case [14], tocilizumab in 1 case [13], lopinavir/ritonavir and ribavirin in 1 case [17] and dexamethasone in 1 case [present report]. On the other hand, SLE activity was treated with glucocorticoids in all cases; IVIg was added in 4/7 patients [11,14,17 and the present report]; antimalarial drugs in 3/7 patients [13,16, and the present report]; rituximab in 2/7 patients [14 and the present report]; plasmapheresis [13] and eltrombopag [16] in one patient each. Our patient underwent splenectomy for refractory thrombocytopenia. Four patients required 3 or more drugs for the management of SLE activity [13,14,16 and the present report]. Five patients required supplemental oxygen [12–15, 17]; 3 patients developed severe acute respiratory distress syndrome and used invasive ventilation [13, 14, 17]. One case presented intraventricular hemorrhage due to severe thrombocytopenia [14]; and one case presented multiple deep venous thrombosis (DVT), with heart failure, and kidney failure that warranted hemodialysis [13]. Death was reported in 2 cases (one case with severe acute respiratory distress syndrome, heart failure, kidney injury and multiple DVT [13] and one case with severe acute respiratory distress syndrome and intraventricular hemorrhage [14]).

Fig. 2

Flow chart of study selection

Table 2

Major clinical manifestations, findings of complementary studies and outcomes in patients with SLE triggered by SARS-CoV-2 infection

First author of study	Age/Sex	Time onset of SLE	Clinical manifestations	Relevant laboratory findings	Immunological test	Imagingfinding	Specific activity of SLE	Treatment to SLE activity	Complications	Outcome
Kondo [11]	58/F	20 yr	Chest discomfort, gingival bleeding	Lymphopenia (650/µL) ↑ CRP (0.5 mg/dL) Thrombocytopenia (5000/µL) ↑ aTTP (41.3 s)	Lupus anticoagulant ( +)	CT: Patchy ground-glass opacities in both lungs	Hematologic	Prednisone (10 mg/day) IVIg (20 g doses × 5 days)	ND	Improved
Kichloo [12]	22/F	Previous diagnosis (unspecified time)	Fever, shortness of breath	Lymphopenia, ↑ D-dimer, ↑ LDH	↑ anti-dsDNA (19 IU/mL), ↓ C3 (84 mg/dL), ↓ C4 (9 mg/dL)	CT: Ground glass opacities with chronic interstitial lung fibrosis	Pulmonary	Methylprednisolone (60 mg 3 times daily × 5 days)	ND	Improved
Mantovani-Cardoso [13]	18/F	New-onset	Productive cough, shortness of breath, fever, malaise, tachycardia, hypotension	↑ SCr (4.6 mg/dL), ↑ BUN (82 mg/dL), anemia (5.4 g/dL), leukocytosis (38,600/µL), lymphopenia (0.300/µL), thrombocytopenia (32,000/µL), ↑ ferritin (2112 µg/L), ↑ LDH (805 U/L), ↑ CPR (3.73 mg/dL), ↑ ESR (38 mm/h), ↑ D-dimer (2443 ng/mL), ↑INR (1.7), ↑ aPTT (54 s), urine hemoglobin ( +), urine protein/Cr ratio 2.84	ANA (+ , >  = 1:2560, homogeneous pattern), Anti-dsDNA (+ , 943 IU/mL), Antihistone ( +), ↓C3 (29 mg/dL), ↓C4 (9 mg/dL), Anticardiolipin IgA (+ , 12.1 U/mL, lupus anticoagulant ( +), beta-2-microglobulin ( +)	Point-of- care US: Pericardial effusion with tamponade Rx: Multifocal airspace consolidation, bilateral pleural effusions ECHO: LVEF 20–25% with left ventricle dilatation	Serosal Hematologic Renal	Pulse steroids, hydroxychloroquine, plasmapheresis, tocilizumab	ARDS (invasive ventilation), multiple deep venous thrombosis, heart failure and kidney failure (with hemodialysis)	Death
Raghavan [14]	62/M	3 wk	Cough, shortness of breath, headache, diffuse purpuric rash	Anemia (9.1 g/dL, immune-mediated hemolysis), thrombocytopenia (2000/µL), indirect hyperbilirubinemia (2.9 mg/dL), ↑ PT (15.4 s), ↑ aPTT (41.8 s), ↑ fibrinogen (561 mg/dL), ↑ D-dimer, ↑ CRP (11.9 mg/dL)	Lupus anticoagulant ( +), anticardiolipin ( +), anti-beta2-glycoprotein ( +)	Rx: Bilateral patchy airspace opacities	Hematologic	Dexamethasone (40 mg daily × 4 days), IVIg (1 mg/kg daily × 5 days)	Intraventricular hemorrhage, ARDS	Death
Bonometti [15]	85/F	New-onset	Severe hypotension, diffuse dyscrasic edemas, peripheral cyanosis	Leukocytosis, lymphopenia, thrombocytopenia, acute kidney injury, ↑ CRP, ↑ ferritin, ↑ LDH, proteinuria, hematuria	ANA (+ , 1:320 homogeneous pattern), ↓ complement	Rx: Pleural effusion	Serosal Hematologic Renal	Steroids	Dried gangrene developed on her three fingertips of left hand	Improved
Hayden [16]	51/F	18 yr	Fever, hemoptysis	Thrombocytopenia (< 10,000/µL), ↑ INR (1.94)	ND	CT: Ground glass opacities in the left lower lobe	Hematologic	Hydroxychloroquine (300 mg daily), IVIg (total of 2 g/kg body weight), prednisone (60 mg daily), eltrombopag (50 mg)	ND	Improved
Altharthy [17]	28/F	Previous diagnosis (unspecified time)	Fever¸ cough, fatigue, dyspnea	Lymphopenia (590/µL), ↑ CRP (354 mg/L), ↑ D-dimer (1.9 mcg/ml), ↑DHL (737 U/L), ↑ferritin (1126 ng/ml)	↑anti-dsDNA (22 U/ml), ↓C3 (64 mg/dl), ↓ C4 (6 mg/dL)	CT: Bilateral ground-glass opacities in both lung	Pulmonary	Pulse methylprednisolone therapy (1 g/day IV  × three days	Shock, ARDS	Improved
Current case	45/M	New-onset	Fever, dry cough, myalgia and arthralgia, edema of the legs	Anemia (10.2 g/dL), thrombocytopenia (5000/µL), ↑ SCr (2.8 mg/dL), ↑ urea (281.5 mg/dL), ↑ SGOT (66.8 U/L), ↑ SGTP (70.9 U/L), ↑ AP (362 U/L), ↑ GGT 352, ↑ ferritin (1752.21 ng/mL), ↑ CRP (167.36 mg/L), ↑ D-dimer (3983 ng/mL), ↑ fibrinogen (706 mg/dL), ↑ aPTT (39.2 s), ↑ urine albumin (0.25 g/24 H), ↑ urine hemoglobin (250 mg/dL)	ANA (+ , 1:1280 coarse speckled pattern), anti-dsDNA (+ , 23/mL), anti-RNP (+ , 3.319 U/mL), anti-SSA (+ , 83.44 U/mL), Anti-SSB (+ , 26.754 U/mL), ↓ C3, ↑ IgG (1790 mg/dL)	Rx: Bilateral reticular pattern with vascular enlargement Abdominal US: Bilateral pleural effusion, ascites, splenomegaly	Serosal Hematologic Renal	Methylprednisolone (1 g × 5 days), chloroquine (150 mg daily), IVIg (2 g/kg/body weight × 4 days), rituximab (600 mg, 3 doses), splenectomy	ND	Improved

aTTP activated partical thromboplastin time, AP alkaline phosphatase, ANA antinuclear antibodies, Anti-dsDNA anti-double-stranded deoxyribonucleic acid antibodies, Anti-RNP anti-ribonucleoprotein, ARDS acute severe respiratory distress syndrome, BUN blood urea nitrogen, CRP C-reactive protein, CT computed tomography, ECHO echocardiography, ERS erythrocyte sedimentation rate, F female, GGT gamma-glutamyl transaminase, IVIg intravenous immunoglobulin, LDH lactate dehydrogenase, LVEF left ventricular ejection fraction, M male, ND not documented, PT prothrombine time, SCr serum creatinine, SGOT serum glutamate-oxalate transaminase, SGTP serum glutamate-pyruvate transaminase, US ultrasound, Rx chest X-ray, wk weeks, yr years

The diagnosis of recent onset or reactivation of SLE can be challenging in patients with SARS-CoV-2 infection because both diseases share some characteristics. The spectrum of presentation of COVID-19 ranges from asymptomatic individuals or mild symptoms to severe-critical illness [18]. According to a recently published systematic review that included 148 articles (24,410 patients), the most prevalent constitutional symptoms in patients with confirmed COVID-19 were fever (78%), fatigue (31%), myalgia (17%) and arthralgia (11%) [19]. In SLE patients, fatigue (80–100%), arthralgia (90%), fever (over 50%) and myalgia are the most prevalent constitutional symptoms [20]. These symptoms are nonspecific, and therefore do not allow any differentiation between these diseases.

Pulmonary manifestations are very common in patients with SLE, with 50–70% of patients affected by some pulmonary complication throughout their disease [21]. However, acute pulmonary pneumonitis is an uncommon (1–2%) manifestation of SLE (although in about half of patients with acute lupus pneumonitis, this is the first manifestation of SLE) [21, 22]. In one case series, the most common presenting symptoms of lupus pneumonitis included fever, cough, dyspnea, hypoxia and lung crepitations [23]. In patients with COVID-19, the main respiratory symptoms reported are cough (57%), dyspnea (23%) and chest pain (7%) [19]. Both diseases showed a ground-glass appearance by CT [21, 24]. Due to these similarities, and given the current pandemic state by SARS-CoV-2, respiratory symptoms should be attributed to COVID-19 unless the patient does not respond to empiric treatment for pneumonia and when extrapulmonary features of SLE are noted (e.g., malar rash, oral ulcers, alopecia, polyserositis, abnormal urine sediment, renal failure, hemocytopenias, thrombophilia, lymphadenopathy, splenomegaly, joint swelling). In the present review, the respiratory manifestations were attributed to SARS-CoV-2 infection (including ARDS in 2 patients), except 2 patients diagnosed with lupus pneumonitis in whom this diagnosis was considered only after a lack of response to initial treatment for COVID-19. On the other hand, pleural effusion is uncommon in COVID-19. In a systematic review that included 55 studies, pleural effusion detected by chest CT scan was observed in only 11% of patients [24]. Pleuritis is the most common pulmonary complication in patients with SLE. Clinically apparent pleural effusion has been reported in up to 50% of patients with SLE and may be found in up to 93% of patients in necropsy studies [25]. In the present review, pleural effusion was reported in 37.5% of cases and its presence was associated to activity of SLE.

The most frequently reported blood count abnormality in patients with SARS-CoV-2 infection is lymphopenia, which occurs in 35% to 83% of cases [26]. However, lymphopenia is present in 75% of SLE patients with active disease [27]. Therefore, this finding is not useful for a differential diagnosis between both diseases. Instead, abnormal platelet count should be looked at with attention. Mild thrombocytopenia (100,000–150,000/μL) has been reported in up to 20–36% of COVID‐19 patients but severe thrombocytopenia (< 50,000/μL) is unusual and it is associated with the severity of the disease [26, 28]. In a case series of patients admitted to an intensive care unit (ICU) in Wuhan, a platelet count of < 100,000/μL was observed in only 5% of patients [29]. Thrombocytopenia < 100,000/μL has been reported in 20–40% of patients with SLE [30]. In the present series, thrombocytopenia was reported in 6 of 7 patients and was considered severe (< 50,000/μL) and refractory to treatment in 5 cases. Possible pathophysiological mechanisms of SARS-CoV-2 infection-induced thrombocytopenia include direct attack to the hematopoietic stem/progenitor cells and damage to the lungs by autoantibodies and immune complexes [31]. We speculate that the immuno-mediated mechanisms against platelets in SARS-CoV-2 infection may be more severe in genetically predisposed patients or patients with a history of SLE, which may lead to more severe thrombocytopenia refractory to treatment.

Renal damage in COVID-19 patients has been reported in > 20% of hospitalized patients and in > 50% in patients admitted to the ICU [32]. The clinical spectrum of renal disease in COVID-19 ranges from the presence of proteinuria and hematuria to acute kidney injury (AKI) requiring renal replacement therapy [33]. Lupus nephritis represents a leading cause of severe organ involvement observed in ~ 50% of patients [34]. The clinical presentation and laboratory findings in LN range from “silent” LN to severe proteinuria and nephrotic syndrome, which can result in AKI. However, patients most commonly present with mild proteinuria and/or hematuria and, in some cases, leukocyturia [35]. Due to these shared characteristics, kidney injury in a patient with suspected SLE activity infected with SARS-CoV-2 can be challenging. In the present series, 3 cases showed kidney disease; in 2 of them the severity of the kidney injury was not consistent with the respiratory disease caused by COVID-19. Therefore, this can be taken into account when making the differential diagnosis.

In the present review, it was found that glucocorticoids were used as the first line of treatment in all patients, regardless of the type and degree of severity, according to the current guidelines [36]. The treatment with glucocorticoids alone was successful in 2 patients and other 4 needed three or more drugs to achieve the control of SLE. Notably, hematological activity was found to be the main manifestation that was refractory to the standard treatment. Rheumatologists should be aware of this situation in order to act promptly in this case.

The possible mechanisms of autoimmunity following SARS-CoV-2 infection include molecular mimicry (cross-reacting epitope between the virus and the host), bystander killing (virus-specific CD8 + T cells migrating to the target tissues and exerting cytotoxicity), epitope spreading, viral persistence (polyclonal activation due to the constant presence of viral antigens driving immune-mediated injury) and formation of neutrophil extracellular traps [37]. In patients hospitalized due to SARS-CoV-2 pneumonia, a prevalence of ANA of 35.6% and lupus anticoagulant of 11.1% has been reported [38]. Other autoantibodies such as anti-Ro/SSA have also been reported [39]. Therefore, this highlights the ability of SARS-CoV-2 to trigger autoimmunity phenomena, which can lead to onset of SLE or a flare of it.

This review has several limitations owing to its retrospective nature, limited size and heterogeneity. In addition, the SARS-CoV-2 infection is still under study and the spectrum of manifestations that it can cause in patients with a previous or new-onset diagnosis of SLE is still unknown. However, this case series can provide meaningful information regarding the clinical profile, diagnosis and management of this complex situation.

In conclusion, the diagnosis of new onset or flare of SLE in a patient with SARS-CoV-2 infection is a challenge. To our knowledge and derived from the present series, the clinical keys that could help with the differential diagnosis are severe thrombocytopenia, serositis and kidney damage that are not related to the severity of the respiratory disease. The presence of such findings should lead to the determination of immunological markers to confirm or rule out the presence of SLE. The goal should be a prompt diagnosis of SLE activity for a timely initiation of specific treatment.