Background/Purpose: a high number of antinuclear antibody specificities can be detected in Systemic Lupus Erythematosous (SLE). Some of them are related to a distinct clinical subset of disease, independently from their frequence. Aim of our study was investigate, in a cohort of SLE patients from a single Centre, the prevalence and the clinical relevance of autoantibodies to cellular antigens less frequently found in SLE.

Methods: antinuclear antibodies was detected by indirect immunofluorescence (IIF) on HEp-2 cells while counterimmunoelectrophoresis (CIE) was used to detect anti-ENA antibodies in  532 patients with SLE classified according  to SLICC criteria¹. Clinical and serological features about our cohort of SLE patients were collected from clinical charts. Categorical variables were analyzed with Chi-Squared test or Fisher’s exact test. Multivarite analysis was conducted with a logistical regression model (Statview), p<0.05 was considered as significant.

Results: 311 (58.5%) of 532 sera were positive for anti-ENA antibodies. Anti-SSA/Ro was the most prevalent antibody found in 232 out of the 311 positive sera (74.5%), 50 of whom (16%) also contains anti-SSB/La. Anti-U1RNP were detected in 69 (22%) and anti-Sm in 45 (14.5%) patients. In a multivariate analysis anti-U1UNP and anti-SSA/Ro resulted to be associated with malar rash (p= 0.010 and p=0.029 respectively) while anti-U1RNP was also associated with leukopenia (p=0.0065). Other anti-ENA antibodies were found in 49 out of the 311 anti-ENA positive sera (15.8%).  Anti-Ki/SL antibodies represented the most frequent between these rare antibodies and were detected in 31 sera, anti-Ku in 8 sera, anti-centromere in 4, isolated anti-SSB/La, PCNA and anti-Scl70 in 3 sera each and anti-Jo-1 in 2 sera.  About half of these antibodies (26 out of 49; 53%) were detected as the single anti-ENA specificity in serum. Anti-Ki/SL was significantly associated with male gender (p=0.0054), being detected in 7 males and in 24 females; anti-Ku was significantly associated with African ethnicity (0.00031) being detected in 3 out of 11 patients of African origin. No sign of muscular or pulmonary involvement were found in the anti-Jo-1 positive patients while features of systemic sclerosis were detectable in 2 out of 3 anti-Scl70 and in one of the 4 anti-centromere positive patients.

Conclusion: our study shows that antibodies to cellular antigens more rarely found in SLE are detectable in more than 15% of patients with anti-ENA antibodies. The majority of them are found as a single anti-ENA specificity. Anti-Ki and anti-Ku appears to characterize a subset of disease with a prevalence of male and of patients from African origin respectively. Clinical features of scleroderma and/or myositis was found only in a minority of patients with antibodies to topoisomerase-1, Jo-1 or centromere.

¹ Petri M, Orbai A-M, Alarcon G, et al. Derivation and Validation of the Systemic  Lupus International Collabarating Clinics Classification Criteria fo Systemic Lupus Erithematosous. Arthritis Rheum 2012; 64:2677-86.

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ACR Meeting Abstracts - https://acrabstracts.org/abstract/rare-autoantibodies-to-cellular-antigens-in-systemic-lupus-erythematosous/