4.3 Article

Could antibodies against Serum Amyloid A function as physiological regulators in humans?

Journal

AUTOIMMUNITY
Volume 44, Issue 2, Pages 149-158

Publisher

TAYLOR & FRANCIS LTD
DOI: 10.3109/08916934.2010.487504

Keywords

Natural autoantibodies; serum amyloid A; acute phase; anti-SAA antibodies; homeostasis

Categories

Funding

  1. Ministry of Higher Education, Science and Technology, Slovenia [P3-0314]
  2. Austrian Ministry of Science and Research
  3. European Commission [28414, 028414]
  4. Ministry of High Education, Science, and Technology of Slovenia [P3 0314]

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The natural structuring of the immune system is responsible for the functional physiological state of the body. The development of natural autoantibodies involved in homeostasis relics on the ability to distinguish between exposed/masked and altered/non-altered self antigens. The objectives of this article were to address the relationships between antigen and autoantibodies against scrum amyloid A (SAA), define SAA protein concentrations in 219 blood donor (BD) sera and determine their autoantibody levels and search for possible clinical associations with autoimmune and thrombotic diseases. Just recently, an increasing number of reports have indicated significantly decreased levels of autoantibodies against pro-inflammatory molecules, such as anti-TNF-alpha, anti-IL-6, or anti-CRP found in diseased conditions, as compared to healthy donors, or even to less severe disease conditions. In accord with this line of thought, our data indicate a predominant presence of anti-SAA autoantibodies in healthy BDs (above 95% as tested by the immunoblot analysis, n = 41). Using ELISA, high levels of anti-SAA antibodies were confirmed with a median OD = 0.996 for the BD group (n = 219). This suggests that anti-SAA antibodies might have a physiological role in homeostasis and/or the innate immune system and could actually be a part of the natural antibody repertoire. Significantly, lower median levels were found in patients with arterial thrombosis. Based on 219 BD sera, we could establish a new median value of 20 mu g/ml for SAA antigen and a cut-off value of 114.7 mu g/ml (97.5th percentile). Significantly, higher concentrations of SAA were observed for antiphospholipid syndrome, rheumatoid arthritic, and SLE patients.

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