The same γ‐secretase accounts for the multiple intramembrane cleavages of APP

Abstract

It has been hypothesized that different C-terminus of β-amyloid peptide (Aβ) may be generated by different γ-secretase activities. Recently, we have identified a new ζ-cleavage site at Aβ46, leading to an important finding that the C-terminus of Aβ is produced by a series of sequential cleavages. This finding prompted us to examine the effects of the known γ-secretase inhibitors on different steps of the γ-secretase-mediated sequential cleavages and specifically their effects on the formation and turnover of the intermediate Aβ₄₆. Our results demonstrate that some of the known inhibitors, such as L-685,458 and III-31C as well as inhibitors IV and V, inhibit the formation of secreted Aβ_40/42 by inhibiting the formation of the intermediate Aβ₄₆. However, most of the other inhibitors show no inhibitory effect on the formation of the intermediate Aβ₄₆, but rather inhibit the turnover of Aβ₄₆, resulting in its accumulation. In addition, the non-steroidal anti-inflammatory drugs (NSAIDs) ibuprofen and sulindac sulfide have no effect on the formation and turnover of Aβ₄₆, but rather modulate the ratio of secreted Aβ at a step after the formation of Aβ₄₀ and Aβ₄₂. Thus, our data strongly suggest that the multi-sequential intramembrane cleavages of amyloid precursor protein C (APP) are likely catalyzed by the same γ-secretase.