Non-invasive molecularly-specific millimeter-resolution manipulation of brain circuits by ultrasound-mediated aggregation and uncaging of drug carriers

Mehmet S. Ozdas; Aagam S. Shah; Paul M. Johnson; Nisheet Patel; Markus Marks; Tansel Baran Yasar; Urs Stalder; Laurent Bigler; Wolfger von der Behrens; Shashank R. Sirsi; Mehmet Fatih Yanik

doi:10.1038/s41467-020-18059-7

Non-invasive molecularly-specific millimeter-resolution manipulation of brain circuits by ultrasound-mediated aggregation and uncaging of drug carriers

Mehmet S. Ozdas, Aagam S. Shah, Paul M. Johnson, Nisheet Patel, Markus Marks, Tansel Baran Yasar, Urs Stalder, Laurent Bigler, Wolfger von der Behrens, Shashank R. Sirsi, Mehmet Fatih Yanik

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

26 Scopus citations

Abstract

Non-invasive, molecularly-specific, focal modulation of brain circuits with low off-target effects can lead to breakthroughs in treatments of brain disorders. We systemically inject engineered ultrasound-controllable drug carriers and subsequently apply a novel two-component Aggregation and Uncaging Focused Ultrasound Sequence (AU-FUS) at the desired targets inside the brain. The first sequence aggregates drug carriers with millimeter-precision by orders of magnitude. The second sequence uncages the carrier’s cargo locally to achieve high target specificity without compromising the blood-brain barrier (BBB). Upon release from the carriers, drugs locally cross the intact BBB. We show circuit-specific manipulation of sensory signaling in motor cortex in rats by locally concentrating and releasing a GABA_A receptor agonist from ultrasound-controlled carriers. Our approach uses orders of magnitude (1300x) less drug than is otherwise required by systemic injection and requires very low ultrasound pressures (20-fold below FDA safety limits for diagnostic imaging). We show that the BBB remains intact using passive cavitation detection (PCD), MRI-contrast agents and, importantly, also by sensitive fluorescent dye extravasation and immunohistochemistry.

Original language	English (US)
Article number	4929
Journal	Nature communications
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41467-020-18059-7
State	Published - Dec 1 2020

ASJC Scopus subject areas

Chemistry(all)
Biochemistry, Genetics and Molecular Biology(all)
Physics and Astronomy(all)

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Ozdas, M. S., Shah, A. S., Johnson, P. M., Patel, N., Marks, M., Yasar, T. B., Stalder, U., Bigler, L., von der Behrens, W., Sirsi, S. R., & Yanik, M. F. (2020). Non-invasive molecularly-specific millimeter-resolution manipulation of brain circuits by ultrasound-mediated aggregation and uncaging of drug carriers. Nature communications, 11(1), Article 4929. https://doi.org/10.1038/s41467-020-18059-7

Ozdas, MS, Shah, AS, Johnson, PM, Patel, N, Marks, M, Yasar, TB, Stalder, U, Bigler, L, von der Behrens, W, Sirsi, SR & Yanik, MF 2020, 'Non-invasive molecularly-specific millimeter-resolution manipulation of brain circuits by ultrasound-mediated aggregation and uncaging of drug carriers', Nature communications, vol. 11, no. 1, 4929. https://doi.org/10.1038/s41467-020-18059-7

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title = "Non-invasive molecularly-specific millimeter-resolution manipulation of brain circuits by ultrasound-mediated aggregation and uncaging of drug carriers",

abstract = "Non-invasive, molecularly-specific, focal modulation of brain circuits with low off-target effects can lead to breakthroughs in treatments of brain disorders. We systemically inject engineered ultrasound-controllable drug carriers and subsequently apply a novel two-component Aggregation and Uncaging Focused Ultrasound Sequence (AU-FUS) at the desired targets inside the brain. The first sequence aggregates drug carriers with millimeter-precision by orders of magnitude. The second sequence uncages the carrier{\textquoteright}s cargo locally to achieve high target specificity without compromising the blood-brain barrier (BBB). Upon release from the carriers, drugs locally cross the intact BBB. We show circuit-specific manipulation of sensory signaling in motor cortex in rats by locally concentrating and releasing a GABAA receptor agonist from ultrasound-controlled carriers. Our approach uses orders of magnitude (1300x) less drug than is otherwise required by systemic injection and requires very low ultrasound pressures (20-fold below FDA safety limits for diagnostic imaging). We show that the BBB remains intact using passive cavitation detection (PCD), MRI-contrast agents and, importantly, also by sensitive fluorescent dye extravasation and immunohistochemistry.",

author = "Ozdas, {Mehmet S.} and Shah, {Aagam S.} and Johnson, {Paul M.} and Nisheet Patel and Markus Marks and Yasar, {Tansel Baran} and Urs Stalder and Laurent Bigler and {von der Behrens}, Wolfger and Sirsi, {Shashank R.} and Yanik, {Mehmet Fatih}",

note = "Funding Information: This project was funded by Swiss Federal Institute of Technology (ETH) Zurich and the European Research Council (ERC) under the European Union{\textquoteright}s Horizon 2020 research and innovation program (grant agreement No 818179). Dr. Sirsi was supported in part by the National Institute of Health (R01CA235756). We thank Beat Werner for general FUS, PCD, and MRI guidance; Sophie Morse and Mostafa Rezaie for technical PCD expertise; Angel Nunez and Kevin Douglas Alloway for kindly answering questions regarding vS1-vM1 paradigm; Sonja Bamert for general laboratory help. Publisher Copyright: {\textcopyright} 2020, The Author(s).",

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Non-invasive molecularly-specific millimeter-resolution manipulation of brain circuits by ultrasound-mediated aggregation and uncaging of drug carriers

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