Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma

Neural stem cells (NSCs) are inherently tumor-tropic, which allows them to migrate through normal tissue and selectively localize to invasive tumor sites in the brain. We have engineered a clonal, immortalized allogeneic NSC line (HB1.F3.CD21; CD-NSCs) that maintains its stem-like properties, a norm...

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Autores principales: Gutova, Margarita, Flores, Linda, Adhikarla, Vikram, Tsaturyan, Lusine, Tirughana, Revathiswari, Aramburo, Soraya, Metz, Marianne, Gonzaga, Joanna, Annala, Alexander, Synold, Timothy W., Portnow, Jana, Rockne, Russell C., Aboody, Karen S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2019
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6389659/
https://www.ncbi.nlm.nih.gov/pubmed/30838174
http://dx.doi.org/10.3389/fonc.2019.00068
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author Gutova, Margarita
Flores, Linda
Adhikarla, Vikram
Tsaturyan, Lusine
Tirughana, Revathiswari
Aramburo, Soraya
Metz, Marianne
Gonzaga, Joanna
Annala, Alexander
Synold, Timothy W.
Portnow, Jana
Rockne, Russell C.
Aboody, Karen S.
author_facet Gutova, Margarita
Flores, Linda
Adhikarla, Vikram
Tsaturyan, Lusine
Tirughana, Revathiswari
Aramburo, Soraya
Metz, Marianne
Gonzaga, Joanna
Annala, Alexander
Synold, Timothy W.
Portnow, Jana
Rockne, Russell C.
Aboody, Karen S.
author_sort Gutova, Margarita
collection PubMed
description Neural stem cells (NSCs) are inherently tumor-tropic, which allows them to migrate through normal tissue and selectively localize to invasive tumor sites in the brain. We have engineered a clonal, immortalized allogeneic NSC line (HB1.F3.CD21; CD-NSCs) that maintains its stem-like properties, a normal karyotype and is HLA Class II negative. It is genetically and functionally stable over time and multiple passages, and has demonstrated safety in phase I glioma trials. These properties enable the production of an “off-the-shelf” therapy that can be readily available for patient treatment. There are multiple factors contributing to stem cell tumor-tropism, and much remains to be elucidated. The route of NSC delivery and the distribution of NSCs at tumor sites are key factors in the development of effective cell-based therapies. Stem cells can be engineered to deliver and/or produce many different therapeutic agents, including prodrug activating enzymes (which locally convert systemically administered prodrugs to active chemotherapeutic agents); oncolytic viruses; tumor-targeted antibodies; therapeutic nanoparticles; and extracellular vesicles that contain therapeutic oligonucleotides. By targeting these therapeutics selectively to tumor foci, we aim to minimize toxicity to normal tissues and maximize therapeutic benefits. In this manuscript, we demonstrate that NSCs administered via intracerebral/ventricular (IVEN) routes can migrate efficiently toward single or multiple tumor foci. IVEN delivery will enable repeat administrations for patients through an Ommaya reservoir, potentially resulting in improved therapeutic outcomes. In our preclinical studies using various glioma lines, we have quantified NSC migration and distribution in mouse brains and have found robust migration of our clinically relevant HB1.F3.CD21 NSC line toward invasive tumor foci, irrespective of their origin. These results establish proof-of-concept and demonstrate the potential of developing a multitude of therapeutic options using modified NSCs.
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spelling pubmed-63896592019-03-05 Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma Gutova, Margarita Flores, Linda Adhikarla, Vikram Tsaturyan, Lusine Tirughana, Revathiswari Aramburo, Soraya Metz, Marianne Gonzaga, Joanna Annala, Alexander Synold, Timothy W. Portnow, Jana Rockne, Russell C. Aboody, Karen S. Front Oncol Oncology Neural stem cells (NSCs) are inherently tumor-tropic, which allows them to migrate through normal tissue and selectively localize to invasive tumor sites in the brain. We have engineered a clonal, immortalized allogeneic NSC line (HB1.F3.CD21; CD-NSCs) that maintains its stem-like properties, a normal karyotype and is HLA Class II negative. It is genetically and functionally stable over time and multiple passages, and has demonstrated safety in phase I glioma trials. These properties enable the production of an “off-the-shelf” therapy that can be readily available for patient treatment. There are multiple factors contributing to stem cell tumor-tropism, and much remains to be elucidated. The route of NSC delivery and the distribution of NSCs at tumor sites are key factors in the development of effective cell-based therapies. Stem cells can be engineered to deliver and/or produce many different therapeutic agents, including prodrug activating enzymes (which locally convert systemically administered prodrugs to active chemotherapeutic agents); oncolytic viruses; tumor-targeted antibodies; therapeutic nanoparticles; and extracellular vesicles that contain therapeutic oligonucleotides. By targeting these therapeutics selectively to tumor foci, we aim to minimize toxicity to normal tissues and maximize therapeutic benefits. In this manuscript, we demonstrate that NSCs administered via intracerebral/ventricular (IVEN) routes can migrate efficiently toward single or multiple tumor foci. IVEN delivery will enable repeat administrations for patients through an Ommaya reservoir, potentially resulting in improved therapeutic outcomes. In our preclinical studies using various glioma lines, we have quantified NSC migration and distribution in mouse brains and have found robust migration of our clinically relevant HB1.F3.CD21 NSC line toward invasive tumor foci, irrespective of their origin. These results establish proof-of-concept and demonstrate the potential of developing a multitude of therapeutic options using modified NSCs. Frontiers Media S.A. 2019-02-19 /pmc/articles/PMC6389659/ /pubmed/30838174 http://dx.doi.org/10.3389/fonc.2019.00068 Text en Copyright © 2019 Gutova, Flores, Adhikarla, Tsaturyan, Tirughana, Aramburo, Metz, Gonzaga, Annala, Synold, Portnow, Rockne and Aboody. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Gutova, Margarita
Flores, Linda
Adhikarla, Vikram
Tsaturyan, Lusine
Tirughana, Revathiswari
Aramburo, Soraya
Metz, Marianne
Gonzaga, Joanna
Annala, Alexander
Synold, Timothy W.
Portnow, Jana
Rockne, Russell C.
Aboody, Karen S.
Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma
title Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma
title_full Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma
title_fullStr Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma
title_full_unstemmed Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma
title_short Quantitative Evaluation of Intraventricular Delivery of Therapeutic Neural Stem Cells to Orthotopic Glioma
title_sort quantitative evaluation of intraventricular delivery of therapeutic neural stem cells to orthotopic glioma
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6389659/
https://www.ncbi.nlm.nih.gov/pubmed/30838174
http://dx.doi.org/10.3389/fonc.2019.00068
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