Aerosolized BC-819 inhibits primary but not secondary lung cancer growth.
Despite numerous efforts, drug based treatments for patients suffering from lung cancer remains poor. As a promising alternative, we investigated the therapeutic potential of BC-819 for the treatment of lung cancer in mouse tumor models. BC-819 is a novel plasmid DNA which encodes for the A-fragment...
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doaj-d51f6abb298e45139f8015dff7af4bf32020-11-25T02:00:17ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-0166e2076010.1371/journal.pone.0020760Aerosolized BC-819 inhibits primary but not secondary lung cancer growth.Günther HasenpuschCorinna PfeiferManish Kumar AnejaKai WagnerDietrich ReinhardtMichal GilonPatricia OhanaAvraham HochbergCarsten RudolphDespite numerous efforts, drug based treatments for patients suffering from lung cancer remains poor. As a promising alternative, we investigated the therapeutic potential of BC-819 for the treatment of lung cancer in mouse tumor models. BC-819 is a novel plasmid DNA which encodes for the A-fragment of Diphtheria toxin and has previously been shown to successfully inhibit tumor growth in human clinical study of bladder carcinoma. In a first set of experiments, we examined in vitro efficacy of BC-819 in human lung cancer cell-lines NCI-H460, NCI-H358 and A549, which revealed >90% reduction of cell growth. In vivo efficacy was examined in an orthotopic mouse xenograft lung cancer model and in a lung metastasis model using luminescent A549-C8-luc adenocarcinoma cells. These cells resulted in peri- and intra-bronchiolar tumors upon intrabronchial application and parenchymal tumors upon intravenous injection, respectively. Mice suffering from these lung tumors were treated with BC-819, complexed to branched polyethylenimine (PEI) and aerosolized to the mice once per week for a period of 10 weeks. Using this regimen, growth of intrabronchially induced lung tumors was significantly inhibited (p = 0.01), whereas no effect could be observed in mice suffering from lung metastasis. In summary, we suggest that aerosolized PEI/BC-819 is capable of reducing growth only in tumors arising from the luminal part of the airways and are therefore directly accessible for inhaled BC-819.http://europepmc.org/articles/PMC3110766?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Günther Hasenpusch Corinna Pfeifer Manish Kumar Aneja Kai Wagner Dietrich Reinhardt Michal Gilon Patricia Ohana Avraham Hochberg Carsten Rudolph |
spellingShingle |
Günther Hasenpusch Corinna Pfeifer Manish Kumar Aneja Kai Wagner Dietrich Reinhardt Michal Gilon Patricia Ohana Avraham Hochberg Carsten Rudolph Aerosolized BC-819 inhibits primary but not secondary lung cancer growth. PLoS ONE |
author_facet |
Günther Hasenpusch Corinna Pfeifer Manish Kumar Aneja Kai Wagner Dietrich Reinhardt Michal Gilon Patricia Ohana Avraham Hochberg Carsten Rudolph |
author_sort |
Günther Hasenpusch |
title |
Aerosolized BC-819 inhibits primary but not secondary lung cancer growth. |
title_short |
Aerosolized BC-819 inhibits primary but not secondary lung cancer growth. |
title_full |
Aerosolized BC-819 inhibits primary but not secondary lung cancer growth. |
title_fullStr |
Aerosolized BC-819 inhibits primary but not secondary lung cancer growth. |
title_full_unstemmed |
Aerosolized BC-819 inhibits primary but not secondary lung cancer growth. |
title_sort |
aerosolized bc-819 inhibits primary but not secondary lung cancer growth. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2011-01-01 |
description |
Despite numerous efforts, drug based treatments for patients suffering from lung cancer remains poor. As a promising alternative, we investigated the therapeutic potential of BC-819 for the treatment of lung cancer in mouse tumor models. BC-819 is a novel plasmid DNA which encodes for the A-fragment of Diphtheria toxin and has previously been shown to successfully inhibit tumor growth in human clinical study of bladder carcinoma. In a first set of experiments, we examined in vitro efficacy of BC-819 in human lung cancer cell-lines NCI-H460, NCI-H358 and A549, which revealed >90% reduction of cell growth. In vivo efficacy was examined in an orthotopic mouse xenograft lung cancer model and in a lung metastasis model using luminescent A549-C8-luc adenocarcinoma cells. These cells resulted in peri- and intra-bronchiolar tumors upon intrabronchial application and parenchymal tumors upon intravenous injection, respectively. Mice suffering from these lung tumors were treated with BC-819, complexed to branched polyethylenimine (PEI) and aerosolized to the mice once per week for a period of 10 weeks. Using this regimen, growth of intrabronchially induced lung tumors was significantly inhibited (p = 0.01), whereas no effect could be observed in mice suffering from lung metastasis. In summary, we suggest that aerosolized PEI/BC-819 is capable of reducing growth only in tumors arising from the luminal part of the airways and are therefore directly accessible for inhaled BC-819. |
url |
http://europepmc.org/articles/PMC3110766?pdf=render |
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