Childhood Systemic Lupus Erythematosus (cSLE)
Childhood Systemic Lupus Erythematosus (cSLE) is a chronic heterogeneous autoimmune disease associated with considerable morbidity and significant mortality. It is characterized by multisystem sequential or simultaneous organ involvement (predominant musculoskeletal, cutaneous, renal, hematologic, and neuropsychiatric manifestations) and the presence of antinuclear and other antibodies.
Standard Treatment Guidelines 2022
The Indian Academy of Pediatrics (IAP) has released Standard Treatment Guidelines 2022 for Childhood Systemic Lupus Erythematosus. The lead author for these guidelines is Dr. Nutan Kamath along with co-author Dr. Amit Rawat and Dr. Aaradhana Singh. The guidelines come under the auspices of the IAP Action Plan 2022, and the members of the IAP Standard Treatment Guidelines Committee include:
- Chairperson: Remesh Kumar R
- IAP Coordinator: Vineet Saxena
- National Coordinators: SS Kamath, Vinod H Ratageri
- Member Secretaries: Krishna Mohan R, Vishnu Mohan PT
- Members: Santanu Deb, Surender Singh Bisht, Prashant Kariya, Narmada Ashok, Pawan Kalyan
Major Recommendations of Guidelines
Clinical Manifestations and Classification Criteria for SLE
Source: Indian Academy of Pediatric Guidelines
The Severity of Illness
Source: Indian Academy of Pediatric Guidelines
Investigations
Laboratory investigations form an integral part of the diagnosis and management of patients with SLE.
General Laboratory Investigations
- Erythrocyte sedimentation rate (ESR): An increase in ESR is in proportion to disease activity. May be falsely elevated in hypergammaglobulinemia.
- C-reactive protein: Usually normal even with active disease. Increased in patients with concomitant infection, serositis, or arthritis.
- Ferritin: Increased, albeit not as much as in macrophage activation syndrome.
Specific Immunological Investigations
| Method of Detection | Comments |
|---|---|
| Antinuclear antibodies (ANA) | Indirect immunofluorescence on HEp2 cells remains the gold standard for detection. Present in more than 90% of children with lupus. Patterns of staining may reflect the antigenic specificity of the antibody. |
| Anti-double stranded antibodies (anti-dsDNA) | Enzyme immunoassay or immunofluorescence. High specificity for SLE. Marker for the active disease especially lupus nephritis. |
| Complement estimation | Nephelometry or enzyme immunoassay. Complement C3 and C4 are commonly measured. Low levels detected in active disease. |
| Extractable nuclear antigens | Can be detected by immunoblotting or by counterimmunoelectrophoresis. Provide useful information on antigenic specificity of ANA. |
| Antiphospholipid (aPL) antibodies | ELISA for anticardiolipin and anti-b2-glycoprotein I antibodies. Lupus anticoagulant assay by activated partial thromboplastin time (aPTT) and dilute Russell's viper venom time (dRVVT). Positive in a significant proportion of pediatric SLE patients. Anticoagulants (heparin and oral anticoagulants) may interfere with the detection of lupus anticoagulant. |
Treatment
Childhood systemic lupus erythematosus ranges in severity from mild disease with arthritis and rash to devastating nephritis with renal failure or profound neurological disturbances. The approach to therapy is individualized for each patient and based on the clinical features. Nevertheless, treatment is unified based on a few guiding principles.
Ten Principles of Treatment
- Treatment by a multidisciplinary team with the pediatric rheumatologist as the Lead
- Assess organ involvement
- Assess disease activity and damage index
- Direct therapy to specific disease manifestations that are active
- Achieve remission with adequate immunosuppression
- Therapy for the shortest period and at the lowest possible doses
- Maintain remission with minimal toxicity of drugs
- Prompt recognition and aggressive treatment of 'flares' and infection
- Counsel and educate parents and children
- Transition to adult care in late adolescence
General Treatment
Source: Indian Academy of Pediatric Guidelines
Organ-Specific Treatment
Source: Indian Academy of Pediatric Guidelines
Assess Disease Activity and Damage Index
Assessment of disease activity and damage is best done by pediatric rheumatologist using the SLE Disease Activity Index (SLEDAI)/British Isles Lupus Assessment Group (BILAG) index and pediatric version of American College of Rheumatology/Systemic Lupus International Collaborating Clinics (ACR/SLICC) damage score index.
Counseling and Education
- About chronic nature of illness with flares and remissions
- Regular follow-up
- Monitoring for side effects of drugs
- Need for prolonged therapy
- Access to patient information material
- Need for shared care with a multidisciplinary team
- Career choices
- Transition to medical care in late adolescence
- Coping strategies for parents and child
Drugs Used in the Management of SLE
| Name | Dosage | Indications | Important Side Effects | Monitoring |
|---|---|---|---|---|
| Prednisolone | Initiation of therapy (4–6 weeks): 0.5–2 mg/kg/day (max 60 mg/day) in at least two divided doses based on type and severity of organ involved. Tapering dose: Reduce by 2.5–5 mg/week till a daily dose of 20 mg. Further reduction by 1–2.5 mg every 2–4 weeks till a daily dose of 10 mg. After a daily dose of 10 mg is reached, reduce it by 0.5–1 mg every 2–4 weeks. | Mainstay of treatment to induce and maintain remission | Obesity, glaucoma, cataract, hypertension, growth suppression, diabetes, osteoporosis, avascular necrosis of bone, infections | Regular blood pressure and random blood sugar monitoring, calcium and vitamin D supplement, bone density monitoring |
| Intravenous pulse methylprednisolone | 10–30 mg/kg to a maximum of 1 g/day for 1–5 consecutive days followed by oral prednisolone as above | Severe cytopenias, proliferative nephritis, major CNS disease, vasculitis, "lupus crisis" | Hypertension, hyperglycemia. Rest of the side effects similar to prednisolone | Monitoring of vitals especially blood pressure before starting and during infusion |
| Hydroxychloroquine | 4–6 mg/kg/day at bedtime (maximum dose 400 mg/day) | Cutaneous disease and adjunct to steroids for systemic disease | Nausea, pruritis, rarely maculopathy | Eye check at starting the drug and biannually for visual acuity, color vision testing, visual field testing, and retinoscopy |
| Methotrexate | 10–15 mg/m2 subcutaneously weekly once | Arthritis, Resistant skin disease | GI intolerance, mouth ulcers, alopecia, bone marrow suppression, hepatotoxicity | AST/ALT, serum albumin, CBC at baseline and then at 8–12 weeks intervals |
| Nonsteroidal anti-inflammatory drugs (NSAIDs) | GI intolerance/bleed, renal impairment, hypersensitivity | AST/ALT, serum creatinine at baseline and 6-month intervals | ||
| Naproxen | 15–20 mg/kg/day in two divided doses (maximum dose 1 g) | Myalgia, arthralgia, arthritis | Pseudoporphyria-pruritis, urticarial, morbilliform rash, erythema multiforme | |
| Ibuprofen | 30–40 mg/kg/day in three divided doses (maximum dose 2.4 g) | Positive aPL antibodies | ||
| Aspirin | 3–5 mg/kg/day | |||
| Cyclophosphamide | 1–2 mg/kg/day (PO) or 500–1000 mg/m2/month (IV) in severe disease | Severe cytopenias, proliferative nephritis, major CNS disease, vasculitis | Nausea, vomiting, cytopenias, infections, hemorrhagic cystitis | Ensure adequate fluid intake. CBC on days 7 and 14 if on pulse therapy |
| Azathioprine | 0.5–2.5 mg/kg/day (PO) (Maximum 150 mg/day) | Mild SLE unresponsive to glucocorticoids and HCQS or develop unacceptable drug toxicity | Cytopenias, pancreatitis, Opportunistic infections | CBC monthly and after dose increments, hepatic enzymes, BUN, creatinine amylase, and lipase at the onset of treatment and every 3 months |
| Mycophenolate Mofetil | 1200–1800 mg/m2/day twice daily (PO) (Maximum 3000 mg/day) | Induction and maintenance of severe cytopenias, vasculitis, proliferative and membranous nephritis, steroid sparing in moderate to severe illness | GI intolerance, Pancytopenia, Opportunistic infections | CBC every 8–12 weeks |
| Cyclosporine A | 2.5–5 mg/kg/day | Membranous nephropathy | Nephrotoxic | Blood urea nitrogen, creatinine, urine analysis, hepatic enzymes, CBC at start of therapy and monthly |
| IV Immunoglobulin | Up to 2 g/kg | Severe thrombocytopenia, catastrophic antiphospholipid syndrome | Anaphylaxis, Aseptic meningitis (Headache, vomiting 18–36 hours after the infusion) | Monitor blood pressure and pulse rate every 15 minutes for the first hour, every 30 minutes for the second hour, and every hour thereafter |
| Rituximab | 375 mg/m2/week intravenously (four doses at intervals of 7 days) OR 750 mg/m2 (two doses at intervals of 14 days) | Severe and refractory disease | Infection, Hypogammaglobulinemia, Infusion reaction | Monitor CBC at the start of therapy |
| Belimumab (approved for children > 5 years) | 10 mg/kg every 4 weeks | Clinically active disease without severe nephritis or neuropsychiatric lupus | Infection | Monitor CBC at the start of therapy and monthly |
(CBC: complete blood count; ALT: alanine transaminase; AST: aspartate aminotransferase)
Complications
Source: Indian Academy of Pediatric Guidelines
Role of General Pediatrician (GP)
Source: Indian Academy of Pediatric Guidelines
Prognosis
Early diagnosis and appropriate therapy ensure a good prognosis. Intercurrent infections, flares, renal and cardiovascular disease, neurologic manifestations, and poor adherence to treatment affect the outcome. The morbidity of the disease and adverse effects of the medications must be minimized to achieve a satisfactory long-term outcome.
Neonatal Lupus
Source: Indian Academy of Pediatric Guidelines
Drug-induced Lupus
Source: Indian Academy of Pediatric Guidelines
Lupus Mimics
- Infections
- Viral: Epstein-Barr virus, Cytomegalovirus, Parvovirus B19, Human Herpes Virus 6
- Bacterial: Brucellosis, Leptospirosis, Q fever, Mycoplasma
- Spirochetal: Lyme disease
- Protozoal: Toxoplasmosis
- Malignancy
- Leukemia, Lymphoma
- Other autoimmune diseases
- Mixed connective tissue disease, systemic vasculitis, antiphospholipid syndrome, juvenile dermatomyositis
Summary
Diagnosis and management of cSLE is a challenge due to its myriad clinical presentations. Shared care pathways between specialists from different disciplines and different levels of care (primary, secondary, and tertiary) are of paramount importance in the management of cSLE.
Reference
- Aringer M, Costenbader K, Daikh D, et al. 2019 European League Against Rheumatism/American College of Rheumatology classification criteria for systemic lupus erythematosus. Arthritis Rheumatol. 2019;71(9):1400-12.
- Gergianaki I, Bertsias G. Systemic lupus erythematosus in primary care: an update and practical messages for the general practitioner. Front Med (Lausanne). 2018;5:161.
- Groot N, de Graeff N, Marks SD, Brogan P, Avcin T, Bader-Meunier B, et al. European evidence-based recommendations for the diagnosis and treatment of childhood-onset lupus nephritis: the SHARE initiative. Ann Rheum Dis. 2017;76(12):1965-73.
- Massias JS, Smith EMD, Al-Abadi E, et al. Clinical and laboratory characteristics in juvenile-onset systemic lupus erythematosus across age groups. Lupus. 2020;29(5):474-81.
- Trindade VC, Carneiro-Sampaio M, Bonfa E, Silva CA. An update on the management of childhood-onset systemic lupus erythematosus. Paediatr Drugs. 2021;23(4):331-47.
The guidelines can be accessed on the official site of IAP: https://iapindia.org/standard-treatment-guidelines/
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