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Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C

Menadione (Vitamin K3) has anti-tumoral effects against a wide range of cancer cells. Its potential toxicity to normal cells and narrow therapeutic range limit its use as single agent but in combination with radiation or other anti-neoplastic agents can be of therapeutic use. In this paper, we first...

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Autores principales: Vita, Marina F., Nagachar, Nivedita, Avramidis, Dimitrios, Delwar, Zahid M., Cruz, Mabel H., Siden, Åke, Paulsson, Kajsa M., Yakisich, Juan Sebastian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer US 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3171656/
https://www.ncbi.nlm.nih.gov/pubmed/20625795
http://dx.doi.org/10.1007/s10637-010-9489-0
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author Vita, Marina F.
Nagachar, Nivedita
Avramidis, Dimitrios
Delwar, Zahid M.
Cruz, Mabel H.
Siden, Åke
Paulsson, Kajsa M.
Yakisich, Juan Sebastian
author_facet Vita, Marina F.
Nagachar, Nivedita
Avramidis, Dimitrios
Delwar, Zahid M.
Cruz, Mabel H.
Siden, Åke
Paulsson, Kajsa M.
Yakisich, Juan Sebastian
author_sort Vita, Marina F.
collection PubMed
description Menadione (Vitamin K3) has anti-tumoral effects against a wide range of cancer cells. Its potential toxicity to normal cells and narrow therapeutic range limit its use as single agent but in combination with radiation or other anti-neoplastic agents can be of therapeutic use. In this paper, we first evaluated the early (within 3 h) effect of menadione on ongoing DNA replication. In normal rat cerebral cortex mini-units menadione showed an age dependent anti-proliferative effect. In tissue mini-units prepared from newborn rats, menadione inhibited ongoing DNA replication with an IC (50) of approximately 10 μM but 50 μM had no effect on mini-units from prepared adult rat tissue. The effect of short (72 h) and prolonged exposure (1–2 weeks) to menadione alone in the DBTRG.05MG human glioma cells line and in combination with vitamin C was studied. After short period of exposure data show that menadione alone or in combination with vitamin C provided similar concentration-response curves (and IC(50) values). Prolonged exposure to these drugs was evaluated by their ability to kill 100% of glioma cells and prevent regrowth when cells are re-incubated in drug-free media. In this long-term assay, menadione:vitamin C at a ratio 1:100 showed higher anti-proliferative activity when compared to each drug alone and allowed to reduce each drug concentration between 2.5 to 5-fold. Similar anti-proliferative effect was demonstrated in 8 patient derived glioblastoma cell cultures. Our data should be able to encourage further advanced studies on animal models to evaluate the potential use of this combination therapy for glioma treatment.
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spelling pubmed-31716562011-09-26 Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C Vita, Marina F. Nagachar, Nivedita Avramidis, Dimitrios Delwar, Zahid M. Cruz, Mabel H. Siden, Åke Paulsson, Kajsa M. Yakisich, Juan Sebastian Invest New Drugs Preclinical Studies Menadione (Vitamin K3) has anti-tumoral effects against a wide range of cancer cells. Its potential toxicity to normal cells and narrow therapeutic range limit its use as single agent but in combination with radiation or other anti-neoplastic agents can be of therapeutic use. In this paper, we first evaluated the early (within 3 h) effect of menadione on ongoing DNA replication. In normal rat cerebral cortex mini-units menadione showed an age dependent anti-proliferative effect. In tissue mini-units prepared from newborn rats, menadione inhibited ongoing DNA replication with an IC (50) of approximately 10 μM but 50 μM had no effect on mini-units from prepared adult rat tissue. The effect of short (72 h) and prolonged exposure (1–2 weeks) to menadione alone in the DBTRG.05MG human glioma cells line and in combination with vitamin C was studied. After short period of exposure data show that menadione alone or in combination with vitamin C provided similar concentration-response curves (and IC(50) values). Prolonged exposure to these drugs was evaluated by their ability to kill 100% of glioma cells and prevent regrowth when cells are re-incubated in drug-free media. In this long-term assay, menadione:vitamin C at a ratio 1:100 showed higher anti-proliferative activity when compared to each drug alone and allowed to reduce each drug concentration between 2.5 to 5-fold. Similar anti-proliferative effect was demonstrated in 8 patient derived glioblastoma cell cultures. Our data should be able to encourage further advanced studies on animal models to evaluate the potential use of this combination therapy for glioma treatment. Springer US 2010-07-13 2011 /pmc/articles/PMC3171656/ /pubmed/20625795 http://dx.doi.org/10.1007/s10637-010-9489-0 Text en © The Author(s) 2010 https://creativecommons.org/licenses/by-nc/4.0/ This article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
spellingShingle Preclinical Studies
Vita, Marina F.
Nagachar, Nivedita
Avramidis, Dimitrios
Delwar, Zahid M.
Cruz, Mabel H.
Siden, Åke
Paulsson, Kajsa M.
Yakisich, Juan Sebastian
Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C
title Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C
title_full Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C
title_fullStr Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C
title_full_unstemmed Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C
title_short Pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin C
title_sort pankiller effect of prolonged exposure to menadione on glioma cells: potentiation by vitamin c
topic Preclinical Studies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3171656/
https://www.ncbi.nlm.nih.gov/pubmed/20625795
http://dx.doi.org/10.1007/s10637-010-9489-0
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