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A new erythrocyte-based biochemical approach to predict the antiproliferative effects of heterocyclic scaffolds: The case of indolone
Authors:Angela Scala  Silvana Ficarra  Annamaria Russo  Davide Barreca  Elena Giunta  Antonio Galtieri  Giovanni Grassi  Ester Tellone
Affiliation:1. Department of Chemical Sciences, University of Messina, V.le F. Stagno d''Alcontres 31, 98166 Messina, Italy;2. Virology and Microbiology AOOR Papardo–Piemonte, V.le F. Stagno d''Alcontres, 98166 Messina, Italy
Abstract:

Background

The indole core is a key structural feature of many natural products and biomolecules with broad spectrum chemotherapeutic properties. Some of us have recently synthesized a library of biologically promising indolone-based compounds. The present study focuses on the effects of one of them, namely DPIT, on human erythrocytes.

Methods

We have examined the influence of DPIT on band 3 protein, intracellular ATP concentration and transport, caspase 3 activation, metabolic adaptation and membrane stability.

Results

Our study elucidates that DPIT, intercalated into the phospholipid bilayer, decreases the anion transport, the intracellular ATP concentration and the cytosolic pH, inducing a direct activation of caspase 3.

Conclusions

Starting from the metabolic similarity between erythrocytes and cancer cells, we investigate how the metabolic derangements and membrane alterations induced by selected heterocycles could be related to the antiproliferative effects.

General significance

Our work aims to propose a new model of study to predict the antiproliferative effects of heterocyclic scaffolds, pointing out that only one of the listed conditions would be unfavorable to the life cycle of neoplastic cells.
Keywords:Heterocycle   Red blood cell   Anion transport   Caspase 3   ATP transport   Antiproliferation
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