Microbubbles and ultrasound increase intraventricular polyplex gene transfer to the brain

James Kevin Y. Tan; Binhan Pham; Yujin Zong; Camilo Perez; Don O. Maris; Ashton Hemphill; Carol H. Miao; Thomas J. Matula; Pierre D. Mourad; Hua Wei; Drew L. Sellers; Philip J. Horner; Suzie H. Pun

doi:10.1016/j.jconrel.2016.02.003

Microbubbles and ultrasound increase intraventricular polyplex gene transfer to the brain

James Kevin Y. Tan, Binhan Pham, Yujin Zong, Camilo Perez, Don O. Maris, Ashton Hemphill, Carol H. Miao, Thomas J. Matula, Pierre D. Mourad, Hua Wei, Drew L. Sellers, Philip J. Horner, Suzie H. Pun

Research output: Contribution to journal › Article › peer-review

38 Scopus citations

Abstract

Neurons in the brain can be damaged or lost from neurodegenerative disease, stroke, or traumatic injury. Although neurogenesis occurs in mammalian adult brains, the levels of natural neurogenesis are insufficient to restore function in these cases. Gene therapy has been pursued as a promising strategy to induce differentiation of neural progenitor cells into functional neurons. Non-viral vectors are a preferred method of gene transfer due to potential safety and manufacturing benefits but suffer from lower delivery efficiencies compared to viral vectors. Since the neural stem and progenitor cells reside in the subventricular zone of the brain, intraventricular injection has been used as an administration route for gene transfer to these cells. However, the choroid plexus epithelium remains an obstacle to delivery. Recently, transient disruption of the blood-brain barrier by microbubble-enhanced ultrasound has been used to successfully improve drug delivery to the brain after intravenous injection. In this work, we demonstrate that microbubble-enhanced ultrasound can similarly improve gene transfer to the subventricular zone after intraventricular injection. Microbubbles of different surface charges (neutral, slightly cationic, and cationic) were prepared, characterized by acoustic flow cytometry, and evaluated for their ability to increase the permeability of immortalized choroid plexus epithelium monolayers in vitro. Based on these results, slightly cationic microbubbles were evaluated for microbubble and ultrasound-mediated enhancement of non-viral gene transfer in vivo. When coupled with our previously reported gene delivery vehicles, the slightly cationic microbubbles significantly increased ultrasound-mediated transfection of the murine brain when compared to commercially available Definity® microbubbles. Temporary disruption of the choroid plexus by microbubble-enhanced ultrasound is therefore a viable way of enhancing gene delivery to the brain and merits further research.

Original language	English (US)
Pages (from-to)	86-93
Number of pages	8
Journal	Journal of Controlled Release
Volume	231
DOIs	https://doi.org/10.1016/j.jconrel.2016.02.003
State	Published - Jun 10 2016

Keywords

Choroid plexus epithelium
Gene delivery
In vivo
Microbubble
Polyplex
Ultrasound

ASJC Scopus subject areas

Pharmaceutical Science

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10.1016/j.jconrel.2016.02.003

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@article{40eccc6bf00a4aedb70eec354464932e,

title = "Microbubbles and ultrasound increase intraventricular polyplex gene transfer to the brain",

abstract = "Neurons in the brain can be damaged or lost from neurodegenerative disease, stroke, or traumatic injury. Although neurogenesis occurs in mammalian adult brains, the levels of natural neurogenesis are insufficient to restore function in these cases. Gene therapy has been pursued as a promising strategy to induce differentiation of neural progenitor cells into functional neurons. Non-viral vectors are a preferred method of gene transfer due to potential safety and manufacturing benefits but suffer from lower delivery efficiencies compared to viral vectors. Since the neural stem and progenitor cells reside in the subventricular zone of the brain, intraventricular injection has been used as an administration route for gene transfer to these cells. However, the choroid plexus epithelium remains an obstacle to delivery. Recently, transient disruption of the blood-brain barrier by microbubble-enhanced ultrasound has been used to successfully improve drug delivery to the brain after intravenous injection. In this work, we demonstrate that microbubble-enhanced ultrasound can similarly improve gene transfer to the subventricular zone after intraventricular injection. Microbubbles of different surface charges (neutral, slightly cationic, and cationic) were prepared, characterized by acoustic flow cytometry, and evaluated for their ability to increase the permeability of immortalized choroid plexus epithelium monolayers in vitro. Based on these results, slightly cationic microbubbles were evaluated for microbubble and ultrasound-mediated enhancement of non-viral gene transfer in vivo. When coupled with our previously reported gene delivery vehicles, the slightly cationic microbubbles significantly increased ultrasound-mediated transfection of the murine brain when compared to commercially available Definity{\textregistered} microbubbles. Temporary disruption of the choroid plexus by microbubble-enhanced ultrasound is therefore a viable way of enhancing gene delivery to the brain and merits further research.",

keywords = "Choroid plexus epithelium, Gene delivery, In vivo, Microbubble, Polyplex, Ultrasound",

author = "Tan, {James Kevin Y.} and Binhan Pham and Yujin Zong and Camilo Perez and Maris, {Don O.} and Ashton Hemphill and Miao, {Carol H.} and Matula, {Thomas J.} and Mourad, {Pierre D.} and Hua Wei and Sellers, {Drew L.} and Horner, {Philip J.} and Pun, {Suzie H.}",

note = "Funding Information: This work was supported by NIH 2R01NS064404 and Washington State Life Discovery Fund (3292512). JKYT was supported by NSF GRFP (2011128558). We would like to thank: Dr. Joyce Wong (Boston University) for her consultation on microbubbles, Dr. Wei Zheng (Purdue University) for providing the Z310 choroid plexus cells, Dr. Shaoyi Jiang (University of Washington) for the use of his Zetasizer Nano ZS, Dr. Elaine Raines (University of Washington) for the use of her EVOM instrument, and Chayanon Ngambenjawong and Nathaniel Coulson for their assistance with experiments. Publisher Copyright: {\textcopyright} 2016 Elsevier B.V. All rights reserved.",

year = "2016",

month = jun,

day = "10",

doi = "10.1016/j.jconrel.2016.02.003",

language = "English (US)",

volume = "231",

pages = "86--93",

journal = "Journal of Controlled Release",

issn = "0168-3659",

publisher = "Elsevier",

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T1 - Microbubbles and ultrasound increase intraventricular polyplex gene transfer to the brain

AU - Tan, James Kevin Y.

AU - Pham, Binhan

AU - Zong, Yujin

AU - Perez, Camilo

AU - Maris, Don O.

AU - Hemphill, Ashton

AU - Miao, Carol H.

AU - Matula, Thomas J.

AU - Mourad, Pierre D.

AU - Wei, Hua

AU - Sellers, Drew L.

AU - Horner, Philip J.

AU - Pun, Suzie H.

N1 - Funding Information: This work was supported by NIH 2R01NS064404 and Washington State Life Discovery Fund (3292512). JKYT was supported by NSF GRFP (2011128558). We would like to thank: Dr. Joyce Wong (Boston University) for her consultation on microbubbles, Dr. Wei Zheng (Purdue University) for providing the Z310 choroid plexus cells, Dr. Shaoyi Jiang (University of Washington) for the use of his Zetasizer Nano ZS, Dr. Elaine Raines (University of Washington) for the use of her EVOM instrument, and Chayanon Ngambenjawong and Nathaniel Coulson for their assistance with experiments. Publisher Copyright: © 2016 Elsevier B.V. All rights reserved.

PY - 2016/6/10

Y1 - 2016/6/10

N2 - Neurons in the brain can be damaged or lost from neurodegenerative disease, stroke, or traumatic injury. Although neurogenesis occurs in mammalian adult brains, the levels of natural neurogenesis are insufficient to restore function in these cases. Gene therapy has been pursued as a promising strategy to induce differentiation of neural progenitor cells into functional neurons. Non-viral vectors are a preferred method of gene transfer due to potential safety and manufacturing benefits but suffer from lower delivery efficiencies compared to viral vectors. Since the neural stem and progenitor cells reside in the subventricular zone of the brain, intraventricular injection has been used as an administration route for gene transfer to these cells. However, the choroid plexus epithelium remains an obstacle to delivery. Recently, transient disruption of the blood-brain barrier by microbubble-enhanced ultrasound has been used to successfully improve drug delivery to the brain after intravenous injection. In this work, we demonstrate that microbubble-enhanced ultrasound can similarly improve gene transfer to the subventricular zone after intraventricular injection. Microbubbles of different surface charges (neutral, slightly cationic, and cationic) were prepared, characterized by acoustic flow cytometry, and evaluated for their ability to increase the permeability of immortalized choroid plexus epithelium monolayers in vitro. Based on these results, slightly cationic microbubbles were evaluated for microbubble and ultrasound-mediated enhancement of non-viral gene transfer in vivo. When coupled with our previously reported gene delivery vehicles, the slightly cationic microbubbles significantly increased ultrasound-mediated transfection of the murine brain when compared to commercially available Definity® microbubbles. Temporary disruption of the choroid plexus by microbubble-enhanced ultrasound is therefore a viable way of enhancing gene delivery to the brain and merits further research.

AB - Neurons in the brain can be damaged or lost from neurodegenerative disease, stroke, or traumatic injury. Although neurogenesis occurs in mammalian adult brains, the levels of natural neurogenesis are insufficient to restore function in these cases. Gene therapy has been pursued as a promising strategy to induce differentiation of neural progenitor cells into functional neurons. Non-viral vectors are a preferred method of gene transfer due to potential safety and manufacturing benefits but suffer from lower delivery efficiencies compared to viral vectors. Since the neural stem and progenitor cells reside in the subventricular zone of the brain, intraventricular injection has been used as an administration route for gene transfer to these cells. However, the choroid plexus epithelium remains an obstacle to delivery. Recently, transient disruption of the blood-brain barrier by microbubble-enhanced ultrasound has been used to successfully improve drug delivery to the brain after intravenous injection. In this work, we demonstrate that microbubble-enhanced ultrasound can similarly improve gene transfer to the subventricular zone after intraventricular injection. Microbubbles of different surface charges (neutral, slightly cationic, and cationic) were prepared, characterized by acoustic flow cytometry, and evaluated for their ability to increase the permeability of immortalized choroid plexus epithelium monolayers in vitro. Based on these results, slightly cationic microbubbles were evaluated for microbubble and ultrasound-mediated enhancement of non-viral gene transfer in vivo. When coupled with our previously reported gene delivery vehicles, the slightly cationic microbubbles significantly increased ultrasound-mediated transfection of the murine brain when compared to commercially available Definity® microbubbles. Temporary disruption of the choroid plexus by microbubble-enhanced ultrasound is therefore a viable way of enhancing gene delivery to the brain and merits further research.

KW - Choroid plexus epithelium

KW - Gene delivery

KW - In vivo

KW - Microbubble

KW - Polyplex

KW - Ultrasound

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DO - 10.1016/j.jconrel.2016.02.003

M3 - Article

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SN - 0168-3659

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EP - 93

JO - Journal of Controlled Release

JF - Journal of Controlled Release

ER -

Microbubbles and ultrasound increase intraventricular polyplex gene transfer to the brain

Abstract

Keywords

ASJC Scopus subject areas

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