Chromatin condensation during apoptosis requires ATP

Author:

KASS George E. N.12,ERIKSSON John E.3,WEIS Marianne1,ORRENIUS Sten1,CHOW Sek C.14

Affiliation:

1. Institute of Environmental Medicine, Division of Toxicology, Karolinska Institutet, Box 210, S-171 77 Stockholm, Sweden

2. School of Biological Sciences, University of Surrey, Guildford, Surrey GU2 5XH, U.K.

3. Turku Centre for Biotechnology, PB 123, FIN-20521 Turku, Finland

4. Centre for Mechanisms of Human Toxicity, University of Leicester, Leicester LE1 2HQ, U.K.

Abstract

The processes leading to morphological changes of the chromatin in cells that undergo apoptosis are presently unclear. We have recently shown that chromatin fragmentation and the nuclear morphological changes typically seen in apoptosis were reproduced in an in vitro system comprised of isolated rat thymocyte nuclei incubated in the presence of a lysate from Fas/APO-1-stimulated JURKAT cells [Chow, Weis, Kass, Holmström, Eriksson and Orrenius (1995) FEBS Lett. 364, 134–138]. Using this in vitro system, we now report that the presence of ATP is necessary for chromatin condensation, its movement to the nuclear periphery and apoptotic body formation. In clear contrast, chromatin cleavage into high-molecular-mass and oligonucleosomal-length DNA fragments induced by lysates derived from Fas/APO-1-activated JURKAT cells did not require the presence of ATP. The induction of these morphological changes by ATP could not be substituted by the analogues, adenosine 5´-[β,γ-methylene]triphosphate and adenosine 5´-[α,β-methylene]-triphosphate, AMP, cAMP and UTP. However, adenosine 5´-[γ-thio]triphosphate, and to a lesser degree GTP and ADP, could partially replace ATP in inducing nuclear apoptotic morphological changes. It is concluded that ATP is essential for the morphological changes occurring in nuclei during apoptosis, but not for DNA fragmentation.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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