Abstract

Purpose : To investigate the mechanisms and pathways of X-ray apoptosis in Molt-4 cells, focusing on mitochondrial and cytosolic Ca2+ ([Ca2+]i) regulation. Materials and methods : X-irradiated Molt-4 cells and cell extract (CE) were used to analyse: (1) induced apoptosis (Giemsa stain), (2) p53, Bcl-2 and Bax expressions (immunoblot), (3) mitochondrial potential Deltapsi and (4) [Ca2+]i (flow cytometry), (5) caspasem 3 activity, and (6) roles of [Ca2+]- and caspase-3-mediated pathways by inhibiting either or both pathways for induced apoptosis. Results : Molt-4 cells were sensitive to apoptosis since 5Gy induced 57 and 94% apoptosis at 6 and 24h. After 5Gy, p53 was accumulated that upregulated Bax but which repressed Bcl-2 with time, resulting in a 7-fold increase in Bax/Bxl-2 at 6h. Predominant Bax reduced Deltapsi m, and low- Deltapsi m cells increased 45 min earlier than apoptosis after 5Gy. Caspase-3 was activated in apoptotic CE. The caspase-3 inhibitor Ac-DEVD-CHO inhibited apoptosis and DNA-ladder formation by ~50%, suggesting a ~50% role of caspase-3-activated DNase (CAD). [Ca2+]i was increased after 5Gy. [Ca2+]i-chelating BAPTA-AM (5mum) and/or DNase gamma -inhibiting Zn2+ (0.5mm) inhibited ~50% of induced apoptosis and DNA-laddering, indicating a 50% participation of Ca2+ /Mg2-dependent DNase gamma . Conclusions : The p53-Bax-mitochondria-caspase-3-CAD pathway and the [Ca2+]i-mediated DNase gamma pathway were involved in the regulation of X i-ray apoptosis in sensitive Molt-4 cells.

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