AI Article Synopsis

  • Autoantibodies with enzymatic activities, known as abzymes, may also be present in patients with viral diseases like HIV, specifically targeting viral proteins.
  • A study found that 89.5% of IgGs from HIV-infected patients could specifically hydrolyze the integrase enzyme, signifying a unique characteristic of these antibodies that is not found in healthy individuals.
  • The presence of integrase-hydrolyzing IgGs raises the possibility of a beneficial role in combating HIV, and this enzymatic activity could serve as a valuable tool for diagnosis and assessing immune status in AIDS patients.

Article Abstract

Autoantibodies with enzymic activities (abzymes) are a distinctive feature of autoimmune diseases. It was interesting whether Abs from patients with viral diseases can hydrolyze viral proteins. Electrophoretically and immunologically homogeneous IgGs were isolated from sera of AIDS patients by chromatography on several affinity sorbents. We present evidence showing that 89.5% IgGs purified from the sera of HIV-infected patients using several affinity resins including Sepharose with immobilized integrase specifically hydrolyze only HIV integrase (IN) but not many other tested proteins. Several rigid criteria have been applied to show that the IN-hydrolyzing activity is an intrinsic property of AIDS IgGs but not from healthy donors. Similar to autoimmune proteolytic abzymes, IN-hydrolyzing IgGs from some patients were inhibited by specific inhibitors of serine and metal-dependent proteases but a significant inhibition of the activity by specific inhibitors of acidic- and thiol-like proteases was observed for the first time. Although HIV infection leads to formation of Abs to many viral and human antigens, no possible biological role for most of them is known. Since anti-IN IgG can efficiently hydrolyze IN, a positive role of abzymes in counteracting the infection cannot be excluded. In addition, detection of IN-hydrolyzing activity can be useful for diagnostic purposes and for estimation of the immune status in AIDS patients.

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Source
http://dx.doi.org/10.1016/j.biochi.2009.06.018DOI Listing

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