Gulzeb Aziz scite author profile

Procaspase-activating compound 1, PAC-1, has been introduced as a direct activator of procaspase-3 and has been suggested as a therapeutic agent against cancer. Its activation of procaspase-3 is dependent on the chelation of zinc. We have tested PAC-1 and an analogue of PAC-1 as zinc chelators in vitro as well as their ability to activate caspase-3 and induce cell death in chicken cerebellar granule neuron cultures. These neurons are non-dividing, primary cells with normal caspase-3. The results reported herein show that PAC-1 chelates zinc, activates procaspase-3, and leads to caspase-3-dependent cell death in neurons, as the specific caspase-3-inhibitor Ac-DEVD-cmk inhibited both the caspase-3 activity and cell death. Thus, chicken cerebellar granule neurons is a suitable model to study mechanisms of interference with apoptosis of PAC-1 and similar compounds. Furthermore, the present study also raises concern about potential neurotoxicity of PAC-1 if used in cancer therapy.

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Combretastatin A-4 and structurally related triazole analogues induce caspase-3 and reactive oxygen species-dependent cell death in PC12 cells

Aziz

Odlo

Hansen

et al. 2013

European Journal of Pharmacology

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Cell death induced by novel procaspase-3 activators can be reduced by growth factors

Debernard

Aziz

Gjesvik

et al. 2011

Biochemical and Biophysical Research Communications

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Pharmacokinetic Studies of Ranitidine Tablets on Healthy Human Subjects Using Two Binders

Akhtar

Ahmad

Aziz

et al. 2006

Bulletin of Pharmaceutical Sciences. Assiut

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Gulzeb Aziz

Synthesis and initial in vitro biological evaluation of two new zinc-chelating compounds: Comparison with TPEN and PAC-1

Procaspase-activating compound 1 induces a caspase-3-dependent cell death in cerebellar granule neurons

Combretastatin A-4 and structurally related triazole analogues induce caspase-3 and reactive oxygen species-dependent cell death in PC12 cells

Cell death induced by novel procaspase-3 activators can be reduced by growth factors

Pharmacokinetic Studies of Ranitidine Tablets on Healthy Human Subjects Using Two Binders

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