Biochemical and Biophysical Research Communications, Vol.377, No.3, 757-762, 2008
Human caspase-3 inhibition by Z-tLeu-Asp-H: tLeu(P-2) counterbalances Asp(P-4) and Glu(P-3) specific inhibitor truncation
Caspase-3 is responsible for the cleavage of several proteins including the nuclear enzyme poly(ADPribose) polymerase (PARP). Designed on the cleavage site of PARR Ac-Asp-Glu-Val-Asp-H has been reported as a highly specific inhibitor. To overcome the susceptibility to proteolysis, the intrinsic instability, and the scarce membrane permeability of tetra-peptidyl aldehydes, di- and tri-peptidyl caspase-3 inhibitors have been synthesized. Here, the synthesis and the inhibition properties of peptidyl aldehydes Z-tLeu-Asp-H, Z-tLeu-Val-Asp-H, and Z-Val-tLeu-Asp-H are reported. Z-tLeu-Asp-H, Z-tLeu-Val-Asp-H, and Z-Val-tLeu-Asp-H inhibit competitively human caspase-3 activity in vitro with K-i(0) = 3.6 nM, 18.2 nM, and 109 nM, respectively (pH 7.4 and 25 degrees C). Moreover, Z-tLeu-Asp-H impairs apoptosis in human DLD-1 colon adenocarcinoma cells without affecting caspase-8. Therefore, Ac-Asp-Glu-Val-Asp-H can be truncated to Z-tLeu-Asp-H retaining nanomolar inhibitory activity in vitro and displaying action in whole cells, these properties reflect the unprecedented introduction of the bulky and lipophilic tLeu residue at the P-2 position. (C) 2008 Elsevier Inc. All rights reserved.
Keywords:Caspase-3;Peptidyl aldehyde inhibitor;Enzyme competitive inhibition;tert-Leucine;Human DLD-1 colon adenocarcinoma cells;Apoptosis