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Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response

Resistance of hypoxic solid tumor niches to chemotherapy and radiotherapy remains a major scientific challenge that calls for conceptually new approaches. Here we exploit a hitherto unrecognized ability of sickled erythrocytes (SSRBCs) but not normal RBCs (NLRBCs) to selectively target hypoxic tumor...

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Autores principales: Terman, David S., Viglianti, Benjamin L., Zennadi, Rahima, Fels, Diane, Boruta, Richard J., Yuan, Hong, Dreher, Mathew R., Grant, Gerald, Rabbani, Zahid N., Moon, Ejung, Lan, Lan, Eble, Joseph, Cao, Yiting, Sorg, Brian, Ashcraft, Kathleen, Palmer, Greg, Telen, Marilyn J., Dewhirst, Mark W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3541382/
https://www.ncbi.nlm.nih.gov/pubmed/23326340
http://dx.doi.org/10.1371/journal.pone.0052543
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author Terman, David S.
Viglianti, Benjamin L.
Zennadi, Rahima
Fels, Diane
Boruta, Richard J.
Yuan, Hong
Dreher, Mathew R.
Grant, Gerald
Rabbani, Zahid N.
Moon, Ejung
Lan, Lan
Eble, Joseph
Cao, Yiting
Sorg, Brian
Ashcraft, Kathleen
Palmer, Greg
Telen, Marilyn J.
Dewhirst, Mark W.
author_facet Terman, David S.
Viglianti, Benjamin L.
Zennadi, Rahima
Fels, Diane
Boruta, Richard J.
Yuan, Hong
Dreher, Mathew R.
Grant, Gerald
Rabbani, Zahid N.
Moon, Ejung
Lan, Lan
Eble, Joseph
Cao, Yiting
Sorg, Brian
Ashcraft, Kathleen
Palmer, Greg
Telen, Marilyn J.
Dewhirst, Mark W.
author_sort Terman, David S.
collection PubMed
description Resistance of hypoxic solid tumor niches to chemotherapy and radiotherapy remains a major scientific challenge that calls for conceptually new approaches. Here we exploit a hitherto unrecognized ability of sickled erythrocytes (SSRBCs) but not normal RBCs (NLRBCs) to selectively target hypoxic tumor vascular microenviroment and induce diffuse vaso-occlusion. Within minutes after injection SSRBCs, but not NLRBCs, home and adhere to hypoxic 4T1 tumor vasculature with hemoglobin saturation levels at or below 10% that are distributed over 70% of the tumor space. The bound SSRBCs thereupon form microaggregates that obstruct/occlude up to 88% of tumor microvessels. Importantly, SSRBCs, but not normal RBCs, combined with exogenous prooxidant zinc protoporphyrin (ZnPP) induce a potent tumoricidal response via a mutual potentiating mechanism. In a clonogenic tumor cell survival assay, SSRBC surrogate hemin, along with H(2)O(2) and ZnPP demonstrate a similar mutual potentiation and tumoricidal effect. In contrast to existing treatments directed only to the hypoxic tumor cell, the present approach targets the hypoxic tumor vascular environment and induces injury to both tumor microvessels and tumor cells using intrinsic SSRBC-derived oxidants and locally generated ROS. Thus, the SSRBC appears to be a potent new tool for treatment of hypoxic solid tumors, which are notable for their resistance to existing cancer treatments.
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spelling pubmed-35413822013-01-16 Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response Terman, David S. Viglianti, Benjamin L. Zennadi, Rahima Fels, Diane Boruta, Richard J. Yuan, Hong Dreher, Mathew R. Grant, Gerald Rabbani, Zahid N. Moon, Ejung Lan, Lan Eble, Joseph Cao, Yiting Sorg, Brian Ashcraft, Kathleen Palmer, Greg Telen, Marilyn J. Dewhirst, Mark W. PLoS One Research Article Resistance of hypoxic solid tumor niches to chemotherapy and radiotherapy remains a major scientific challenge that calls for conceptually new approaches. Here we exploit a hitherto unrecognized ability of sickled erythrocytes (SSRBCs) but not normal RBCs (NLRBCs) to selectively target hypoxic tumor vascular microenviroment and induce diffuse vaso-occlusion. Within minutes after injection SSRBCs, but not NLRBCs, home and adhere to hypoxic 4T1 tumor vasculature with hemoglobin saturation levels at or below 10% that are distributed over 70% of the tumor space. The bound SSRBCs thereupon form microaggregates that obstruct/occlude up to 88% of tumor microvessels. Importantly, SSRBCs, but not normal RBCs, combined with exogenous prooxidant zinc protoporphyrin (ZnPP) induce a potent tumoricidal response via a mutual potentiating mechanism. In a clonogenic tumor cell survival assay, SSRBC surrogate hemin, along with H(2)O(2) and ZnPP demonstrate a similar mutual potentiation and tumoricidal effect. In contrast to existing treatments directed only to the hypoxic tumor cell, the present approach targets the hypoxic tumor vascular environment and induces injury to both tumor microvessels and tumor cells using intrinsic SSRBC-derived oxidants and locally generated ROS. Thus, the SSRBC appears to be a potent new tool for treatment of hypoxic solid tumors, which are notable for their resistance to existing cancer treatments. Public Library of Science 2013-01-09 /pmc/articles/PMC3541382/ /pubmed/23326340 http://dx.doi.org/10.1371/journal.pone.0052543 Text en © 2013 Terman et al 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 properly credited.
spellingShingle Research Article
Terman, David S.
Viglianti, Benjamin L.
Zennadi, Rahima
Fels, Diane
Boruta, Richard J.
Yuan, Hong
Dreher, Mathew R.
Grant, Gerald
Rabbani, Zahid N.
Moon, Ejung
Lan, Lan
Eble, Joseph
Cao, Yiting
Sorg, Brian
Ashcraft, Kathleen
Palmer, Greg
Telen, Marilyn J.
Dewhirst, Mark W.
Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response
title Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response
title_full Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response
title_fullStr Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response
title_full_unstemmed Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response
title_short Sickle Erythrocytes Target Cytotoxics to Hypoxic Tumor Microvessels and Potentiate a Tumoricidal Response
title_sort sickle erythrocytes target cytotoxics to hypoxic tumor microvessels and potentiate a tumoricidal response
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3541382/
https://www.ncbi.nlm.nih.gov/pubmed/23326340
http://dx.doi.org/10.1371/journal.pone.0052543
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