• Title of article

    Kinetic studies of protein L aggregation and disaggregation Original Research Article

  • Author/Authors

    Troy Cellmer، نويسنده , , Rutger Douma، نويسنده , , Ansgar Huebner، نويسنده , , John Prausnitz، نويسنده , , Harvey Blanch، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2007
  • Pages
    10
  • From page
    350
  • To page
    359
  • Abstract
    We have investigated the aggregation of protein L in 25% (vol/vol) TFE and 10 mM HCl. Under both conditions, aggregates adopt a fibrillar structure and bind dyes Congo Red and Thioflavin T consistent with the presence of amyloid fibrils. The kinetics of aggregation in 25% TFE suggest a linear-elongation mechanism with critical nucleus size of either two or three monomers. Aggregation kinetics in 10 mM HCl show a prolonged lag phase prior to a rapid increase in aggregation. The lag phase is time-dependent, but the time dependence can be eliminated by the addition of pre-formed seeds. Disaggregation studies show that for aggregates formed in TFE, aggregate stability is a strong function of aggregate age. For example, after 200 min of aggregation, 40% of the aggregation reaction is irreversible, while after 3 days over 60% is irreversible. When the final concentration of the denaturant, TFE, is reduced from 5% to 0, the amount of reversible aggregation doubles. Disaggregation studies of aggregates formed in TFE and 10 mM HCl reveal a complicated effect of pH on aggregate stability.
  • Keywords
    fibrils , protein aggregation , Aggregation kinetics , amyloid
  • Journal title
    Biophysical Chemistry
  • Serial Year
    2007
  • Journal title
    Biophysical Chemistry
  • Record number

    1119797