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Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C

Effective cancer treatment needs both, passive and active targeting approaches, to achieve highly specific drug delivery to the target cells while avoiding cytotoxicity to normal cells. Protein drugs are useful in this context because they can display excellent specificity and potency. However, thei...

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Autores principales: Figueroa, Cindy M., Morales-Cruz, Moraima, Suárez, Bethzaida N., Fernández, Jean C., Molina, Anna M., Quiñones, Carmen M., Griebenow, Kai
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4864004/
https://www.ncbi.nlm.nih.gov/pubmed/27182458
http://dx.doi.org/10.4172/2157-7439.1000316
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author Figueroa, Cindy M.
Morales-Cruz, Moraima
Suárez, Bethzaida N.
Fernández, Jean C.
Molina, Anna M.
Quiñones, Carmen M.
Griebenow, Kai
author_facet Figueroa, Cindy M.
Morales-Cruz, Moraima
Suárez, Bethzaida N.
Fernández, Jean C.
Molina, Anna M.
Quiñones, Carmen M.
Griebenow, Kai
author_sort Figueroa, Cindy M.
collection PubMed
description Effective cancer treatment needs both, passive and active targeting approaches, to achieve highly specific drug delivery to the target cells while avoiding cytotoxicity to normal cells. Protein drugs are useful in this context because they can display excellent specificity and potency. However, their use in therapeutic formulations is limited due to their physical and chemical instability during storage and administration. Polysaccharides have been used to stabilize proteins during formulation and delivery. To accomplish both, stabilization and targeting simultaneously, the apoptosis-inducing protein cytochrome c (Cyt c) was modified with the polysaccharide hyaluronic acid (HA) because its corresponding receptor CD44 is overexpressed in many cancers. Cyt c-HA bioconjugates were formed using low and high molecular weight HA (8 kDa and 1 MDa) with a resultant Cyt c loading percentage of 4%. Circular dichroism and a cell-free caspase assay showed minor structural changes and high bioactivity (more than 80% caspase activation) of Cyt c, respectively, after bioconjugate formation. Two CD44-positive cancer cells lines, HeLa and A549 cells, and two CD44-negative normal cell lines, Huvec and NIH-3T3 cells, were incubated with the samples to assess selectivity and cytotoxicity. After 24 h of incubation with the samples, cancer cell viability was reduced at least 3-fold while CD44-negative control cell lines remained minimally affected. Fluorescence imaging confirmed selective internalization of the Cyt c-HA construct by CD44-positive cancer cell lines. These results demonstrate the development of a drug delivery system that incorporates passive and active targeting which is essential for cancer treatment.
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spelling pubmed-48640042016-05-12 Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C Figueroa, Cindy M. Morales-Cruz, Moraima Suárez, Bethzaida N. Fernández, Jean C. Molina, Anna M. Quiñones, Carmen M. Griebenow, Kai J Nanomed Nanotechnol Article Effective cancer treatment needs both, passive and active targeting approaches, to achieve highly specific drug delivery to the target cells while avoiding cytotoxicity to normal cells. Protein drugs are useful in this context because they can display excellent specificity and potency. However, their use in therapeutic formulations is limited due to their physical and chemical instability during storage and administration. Polysaccharides have been used to stabilize proteins during formulation and delivery. To accomplish both, stabilization and targeting simultaneously, the apoptosis-inducing protein cytochrome c (Cyt c) was modified with the polysaccharide hyaluronic acid (HA) because its corresponding receptor CD44 is overexpressed in many cancers. Cyt c-HA bioconjugates were formed using low and high molecular weight HA (8 kDa and 1 MDa) with a resultant Cyt c loading percentage of 4%. Circular dichroism and a cell-free caspase assay showed minor structural changes and high bioactivity (more than 80% caspase activation) of Cyt c, respectively, after bioconjugate formation. Two CD44-positive cancer cells lines, HeLa and A549 cells, and two CD44-negative normal cell lines, Huvec and NIH-3T3 cells, were incubated with the samples to assess selectivity and cytotoxicity. After 24 h of incubation with the samples, cancer cell viability was reduced at least 3-fold while CD44-negative control cell lines remained minimally affected. Fluorescence imaging confirmed selective internalization of the Cyt c-HA construct by CD44-positive cancer cell lines. These results demonstrate the development of a drug delivery system that incorporates passive and active targeting which is essential for cancer treatment. 2015-10-01 2015-10 /pmc/articles/PMC4864004/ /pubmed/27182458 http://dx.doi.org/10.4172/2157-7439.1000316 Text en http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Article
Figueroa, Cindy M.
Morales-Cruz, Moraima
Suárez, Bethzaida N.
Fernández, Jean C.
Molina, Anna M.
Quiñones, Carmen M.
Griebenow, Kai
Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C
title Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C
title_full Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C
title_fullStr Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C
title_full_unstemmed Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C
title_short Induction of Cancer Cell Death by Hyaluronic Acid-Mediated Uptake of Cytochrome C
title_sort induction of cancer cell death by hyaluronic acid-mediated uptake of cytochrome c
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4864004/
https://www.ncbi.nlm.nih.gov/pubmed/27182458
http://dx.doi.org/10.4172/2157-7439.1000316
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