Anti-Sm

Anti-Smith Antibodies

Outros

Última revisão: 7 de abril de 2026. Abordagem de fontes: contexto padrão de interpretação laboratorial, material médico de referência e orientações clínicas ou de saúde pública quando relevantes.

O que é Anti-Smith Antibodies?

Anti-Smith (anti-Sm) antibodies are autoantibodies directed against the Smith antigen, a complex of small nuclear ribonucleoproteins (snRNPs) involved in RNA splicing within the cell nucleus. These antibodies are named after Stephanie Smith, the patient in whom they were first identified. Anti-Sm antibodies target specific proteins (B/B', D1, D2, D3, E, F, and G) that form the core of the spliceosomal snRNP complex, a structure essential for processing precursor messenger RNA (pre-mRNA) into mature mRNA.

Anti-Smith antibodies are highly specific for systemic lupus erythematosus (SLE) and are included in the American College of Rheumatology (ACR) and Systemic Lupus International Collaborating Clinics (SLICC) classification criteria for the disease. While they are found in only 20–30% of SLE patients overall (with higher prevalence in African American and Asian populations), their presence is virtually diagnostic—anti-Sm antibodies are rarely if ever found in other autoimmune diseases or healthy individuals. This makes them one of the most specific serological markers for lupus, alongside anti-double-stranded DNA (anti-dsDNA) antibodies.

Por que isso importa

Anti-Smith antibodies are among the most specific markers for systemic lupus erythematosus, with a specificity approaching 99%. While their sensitivity is limited (present in only 20–30% of SLE patients), a positive result essentially confirms the diagnosis of lupus when clinical features are consistent. Unlike anti-dsDNA antibodies, which fluctuate with disease activity, anti-Sm antibodies tend to remain positive regardless of disease activity once they appear, making them useful for diagnosis but less helpful for monitoring flares. Some studies suggest that anti-Sm positivity correlates with renal involvement (lupus nephritis) and central nervous system disease, though this association is debated.

Faixas de referência normais

GrupoFaixaUnidade
Negative<1.0AI (antibody index)
Equivocal1.0–1.5AI
Positive>1.5AI

As faixas de referência podem variar entre laboratórios. Sempre compare seus resultados com as faixas fornecidas pelo seu local de exame.

O que significam níveis altos de Anti-Sm

Causas comuns

  • Systemic lupus erythematosus (SLE)—highly specific
  • Overlap connective tissue disease (rarely)
  • Mixed connective tissue disease (uncommon)

Possíveis sintomas

  • Joint pain and swelling (arthralgia, arthritis)
  • Butterfly rash (malar rash) across cheeks and nose
  • Photosensitivity
  • Fatigue and malaise
  • Oral ulcers
  • Pleurisy or pericarditis
  • Kidney involvement (proteinuria, hematuria)
  • Cytopenias (low blood counts)

O que fazer: A positive anti-Sm result in a patient with compatible symptoms strongly supports SLE diagnosis. Referral to rheumatology is essential. Additional workup should include ANA, anti-dsDNA, complement levels (C3, C4), complete blood count, urinalysis, and renal function tests. Treatment depends on organ involvement and disease severity, ranging from hydroxychloroquine for mild disease to immunosuppressive agents (mycophenolate, cyclophosphamide) and biologics (belimumab) for severe manifestations.

O que significam níveis baixos de Anti-Sm

Causas comuns

  • Normal finding—most healthy people and non-lupus patients are negative
  • SLE without anti-Sm antibodies (70–80% of SLE patients are anti-Sm negative)

Possíveis sintomas

  • No symptoms—a negative result is expected in healthy individuals

O que fazer: A negative anti-Sm result does not rule out SLE, as 70–80% of lupus patients are anti-Sm negative. If SLE is clinically suspected despite negative anti-Sm, evaluate other lupus-specific antibodies (anti-dsDNA, anti-Ro, anti-La, anti-RNP), ANA pattern, and complement levels. Clinical criteria should guide diagnosis.

Quando o exame de Anti-Sm é recomendado?

  • When systemic lupus erythematosus is suspected
  • As part of an autoimmune antibody panel (ANA, anti-dsDNA, ENA panel)
  • When a positive ANA requires further characterization
  • In patients with lupus-like symptoms and negative anti-dsDNA
  • To support SLE classification criteria

Perguntas frequentes

False-positive anti-Sm results are extremely rare. Anti-Smith antibodies have near 99% specificity for SLE, meaning that a positive result almost always indicates lupus. In very rare cases, low-titer positive results may be found in other autoimmune conditions, but these are uncommon enough that a positive anti-Sm should be considered highly suggestive of SLE until proven otherwise. If the result is equivocal, repeating the test or using a different assay method (immunoblot, ELISA) may help clarify.
Unlike anti-dsDNA antibodies, which tend to rise during lupus flares and fall during remission, anti-Sm antibodies generally remain relatively stable over time once they become positive. They do not reliably track with disease activity and should not be used to monitor flare status. For monitoring SLE activity, anti-dsDNA titers, complement levels (C3, C4), and clinical assessment are more useful. Anti-Sm is best used as a diagnostic marker rather than a monitoring tool.
Anti-Smith antibodies are found in approximately 30–40% of African American SLE patients and 30–50% of Asian SLE patients, compared to only 10–20% of Caucasian SLE patients. The reasons for this disparity are not fully understood but likely involve genetic factors affecting immune regulation, HLA haplotype distribution, and differences in lupus phenotype across populations. African American and Asian patients with SLE also tend to have more severe disease overall, including higher rates of lupus nephritis, which has been associated with anti-Sm positivity in some studies.

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Aviso médico: Estas informações são apenas educativas e não substituem orientação, diagnóstico ou tratamento médico profissional. As faixas de referência podem variar entre laboratórios. Sempre converse com seu profissional de saúde sobre a interpretação dos seus resultados específicos.

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