Collagenous Alzheimer amyloid plaque component assembles amyloid fibrils into protease resistant aggregates

Abstract

Recently, a novel plaque-associated protein, collagenous Alzheimer amyloid plaque component (CLAC), was identified in brains from patients with Alzheimer's disease. CLAC is derived from a type II transmembrane collagen precursor protein, termed CLAC-P (collagen XXV). The biological function and the contribution of CLAC to the pathogenesis of Alzheimer's disease and plaque formation are unknown. In vitro studies indicate that CLAC binds to fibrillar, but not to monomeric, amyloid β-peptide (Aβ). Here, we examined the effects of CLAC on Aβ fibrils using assays based on turbidity, thioflavin T binding, sedimentation analysis, and electron microscopy. The incubation of CLAC with preformed Aβ fibrils led to increased turbidity, indicating that larger aggregates were formed. In support of this contention, more Aβ was sedimented in the presence of CLAC, as determined by gel electrophoresis. Moreover, electron microscopy revealed an increased amount of Aβ fibril bundles in samples incubated with CLAC. Importantly, the frequently used thioflavin T-binding assay failed to reveal these effects of CLAC. Digestion with proteinase K or trypsin showed that Aβ fibrils, incubated together with CLAC, were more resistant to proteolytic degradation. Therefore, CLAC assembles Aβ fibrils into fibril bundles that have an increased resistance to proteases. We suggest that CLAC may act in a similar way in vivo. © 2005 FEBS.