Apoptosis on Hepatoma Cells but Not on Primary Hepatocytes by Histone Deacetylase Inhibitors Valproate and ITF2357

Overview

Journal J Hepatol

Publisher Elsevier

Specialty Gastroenterology

Date 2005 Jan 25

PMID 15664246

Citations 37

Authors

Sorin Armeanu

Anita Pathil

Sascha Venturelli

Paolo Mascagni

Thomas S Weiss

Martin Gottlicher

Michael Gregor

Ulrich M Lauer

Michael Bitzer

Affiliations

Soon will be listed here.

Abstract

Background/aims: Due to a particular resistance against conventional chemotherapeutics, palliative treatment of hepatocellular carcinomas (HCC) is highly ineffective. Recent demonstration of both proliferation-inhibition and apoptosis of hepatoma cells by a histone deacetylase inhibitor (HDAC-I) treatment opens up a promising new approach. However, little is known about tumor cell death mechanisms and HDAC-I influences on healthy hepatocytes.

Methods: HDAC-I substances with favourable in vivo profiles, valproate (VPA) and ITF2357, were investigated on HCC cell lines and primary human hepatocytes (PHH). Histone acetylation and apoptosis-modulating proteins were investigated by western-blotting, proliferation by sulforhodamin B binding, toxicity by enzyme release, apoptosis by FACS analysis.

Results: VPA and ITF2357 inhibited proliferation in HCC cell lines. Both substances induced considerable cellular damage in HCC-derived cells, but PHH tolerated these substances well. A downregulation of anti- and upregulation of proapoptotic factors was found. Moreover, Bcl-X(L) transfection into HCC cells abrogated apoptosis induced by both substances, indicating that modulation of intracellular pro- and anti-apoptotic proteins is a key event in VPA or ITF2357 induced tumor-cell death.

Conclusions: Preferential induction of cell death in HCC-derived cell lines, without toxicity in PHH, demonstrates the potential of VPA and ITF2357 to become promising new tools in the fight against HCC.

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