Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis

BACKGROUND: Miriplatin (formerly SM-11355), a novel lipophilic platinum complex developed to treat hepatocellular carcinoma, is administered into the hepatic artery using an oily lymphographic agent (Lipiodol Ultra-Fluide(®)) as a carrier. We clarified the usefulness of miriplatin as an agent for tr...

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Autores principales: Hanada, Mitsuharu, Baba, Akemi, Tsutsumishita, Yasuyuki, Noguchi, Toshihiro, Yamaoka, Takashi, Chiba, Nobuyoshi, Nishikaku, Fumio
Formato: Texto
Lenguaje:English
Publicado: Springer-Verlag 2008
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2691803/
https://www.ncbi.nlm.nih.gov/pubmed/19104812
http://dx.doi.org/10.1007/s00280-008-0895-3
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author Hanada, Mitsuharu
Baba, Akemi
Tsutsumishita, Yasuyuki
Noguchi, Toshihiro
Yamaoka, Takashi
Chiba, Nobuyoshi
Nishikaku, Fumio
author_facet Hanada, Mitsuharu
Baba, Akemi
Tsutsumishita, Yasuyuki
Noguchi, Toshihiro
Yamaoka, Takashi
Chiba, Nobuyoshi
Nishikaku, Fumio
author_sort Hanada, Mitsuharu
collection PubMed
description BACKGROUND: Miriplatin (formerly SM-11355), a novel lipophilic platinum complex developed to treat hepatocellular carcinoma, is administered into the hepatic artery using an oily lymphographic agent (Lipiodol Ultra-Fluide(®)) as a carrier. We clarified the usefulness of miriplatin as an agent for transarterial chemoembolization. METHODS: Platinum compounds released from miriplatin into serum, medium and Earle’s balanced salt solution were examined. Then, miriplatin and cisplatin were administered to rats bearing hepatoma AH109A tumors in livers. Platinum concentrations in tissues and DNA were assessed. RESULTS: Miriplatin showed a more sustained release than cisplatin. Dichloro[(1R, 2R)-1, 2-cyclohexane diamine-N, N′]platinum, the most abundant platinum compound released from miriplatin, was as effective as cisplatin in inhibiting the growth of cells. Miriplatin was selectively disposed of in tumors, maintained in tumors longer than cisplatin and caused apparent tumor regression inducing platinum-DNA adducts to form and massive apoptosis. CONCLUSION: Miriplatin appears to be a suitable chemotherapeutic agent for transarterial chemoembolization.
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spelling pubmed-26918032009-06-08 Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis Hanada, Mitsuharu Baba, Akemi Tsutsumishita, Yasuyuki Noguchi, Toshihiro Yamaoka, Takashi Chiba, Nobuyoshi Nishikaku, Fumio Cancer Chemother Pharmacol Original Article BACKGROUND: Miriplatin (formerly SM-11355), a novel lipophilic platinum complex developed to treat hepatocellular carcinoma, is administered into the hepatic artery using an oily lymphographic agent (Lipiodol Ultra-Fluide(®)) as a carrier. We clarified the usefulness of miriplatin as an agent for transarterial chemoembolization. METHODS: Platinum compounds released from miriplatin into serum, medium and Earle’s balanced salt solution were examined. Then, miriplatin and cisplatin were administered to rats bearing hepatoma AH109A tumors in livers. Platinum concentrations in tissues and DNA were assessed. RESULTS: Miriplatin showed a more sustained release than cisplatin. Dichloro[(1R, 2R)-1, 2-cyclohexane diamine-N, N′]platinum, the most abundant platinum compound released from miriplatin, was as effective as cisplatin in inhibiting the growth of cells. Miriplatin was selectively disposed of in tumors, maintained in tumors longer than cisplatin and caused apparent tumor regression inducing platinum-DNA adducts to form and massive apoptosis. CONCLUSION: Miriplatin appears to be a suitable chemotherapeutic agent for transarterial chemoembolization. Springer-Verlag 2008-12-24 2009-07 /pmc/articles/PMC2691803/ /pubmed/19104812 http://dx.doi.org/10.1007/s00280-008-0895-3 Text en © The Author(s) 2008
spellingShingle Original Article
Hanada, Mitsuharu
Baba, Akemi
Tsutsumishita, Yasuyuki
Noguchi, Toshihiro
Yamaoka, Takashi
Chiba, Nobuyoshi
Nishikaku, Fumio
Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis
title Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis
title_full Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis
title_fullStr Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis
title_full_unstemmed Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis
title_short Intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-DNA adducts to form and massive apoptosis
title_sort intra-hepatic arterial administration with miriplatin suspended in an oily lymphographic agent inhibits the growth of tumors implanted in rat livers by inducing platinum-dna adducts to form and massive apoptosis
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2691803/
https://www.ncbi.nlm.nih.gov/pubmed/19104812
http://dx.doi.org/10.1007/s00280-008-0895-3
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