Delivery of immunoglobulin G antibodies to the rat nervous system following intranasal administration: Distribution, dose-response, and mechanisms of delivery

Niyanta N. Kumar; Jeffrey J. Lochhead; Michelle E. Pizzo; Geetika Nehra; Sam Boroumand; Gretchen Greene; Robert G. Thorne

doi:10.1016/j.jconrel.2018.08.006

Delivery of immunoglobulin G antibodies to the rat nervous system following intranasal administration: Distribution, dose-response, and mechanisms of delivery

Niyanta N. Kumar, Jeffrey J. Lochhead, Michelle E. Pizzo, Geetika Nehra, Sam Boroumand, Gretchen Greene, Robert G. Thorne

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

80 Scopus citations

Abstract

The intranasal route has been hypothesized to circumvent the blood-brain and blood-cerebrospinal fluid barriers, allowing entry into the brain via extracellular pathways along olfactory and trigeminal nerves and the perivascular spaces (PVS) of cerebral blood vessels. We investigated the potential of the intranasal route to non-invasively deliver antibodies to the brain 30 min following administration by characterizing distribution, dose-response, and mechanisms of antibody transport to and within the brain after administering non-targeted radiolabeled or fluorescently-labeled full length immunoglobulin G (IgG) to normal adult female rats. Intranasal [¹²⁵I]-IgG consistently yielded highest concentrations in the olfactory bulbs, trigeminal nerves, and leptomeningeal blood vessels with their associated PVS. Intranasal delivery also resulted in significantly higher [¹²⁵I]-IgG concentrations in the CNS than systemic (intra-arterial) delivery for doses producing similar endpoint blood concentrations. Importantly, CNS targeting significantly increased with increasing dose only with intranasal administration, yielding brain concentrations that ranged from the low-to-mid picomolar range with tracer dosing (50 μg) up to the low nanomolar range at higher doses (1 mg and 2.5 mg). Finally, intranasal pre-treatment with a previously identified nasal permeation enhancer, matrix metalloproteinase-9, significantly improved intranasal [¹²⁵I]-IgG delivery to multiple brain regions and further allowed us to elucidate IgG transport pathways extending from the nasal epithelia into the brain using fluorescence microscopy. The results show that it may be feasible to achieve therapeutic levels of IgG in the CNS, particularly at higher intranasal doses, and clarify the likely cranial nerve and perivascular distribution pathways taken by antibodies to reach the brain from the nasal mucosae.

Original language	English (US)
Pages (from-to)	467-484
Number of pages	18
Journal	Journal of Controlled Release
Volume	286
DOIs	https://doi.org/10.1016/j.jconrel.2018.08.006
State	Published - Sep 28 2018
Externally published	Yes

Keywords

Antibodies
Brain
Intranasal
Olfactory
Perivascular
Trigeminal

ASJC Scopus subject areas

Pharmaceutical Science

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10.1016/j.jconrel.2018.08.006

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@article{46f800fc52a7400ab8c85c3f2d69a11d,

title = "Delivery of immunoglobulin G antibodies to the rat nervous system following intranasal administration: Distribution, dose-response, and mechanisms of delivery",

abstract = "The intranasal route has been hypothesized to circumvent the blood-brain and blood-cerebrospinal fluid barriers, allowing entry into the brain via extracellular pathways along olfactory and trigeminal nerves and the perivascular spaces (PVS) of cerebral blood vessels. We investigated the potential of the intranasal route to non-invasively deliver antibodies to the brain 30 min following administration by characterizing distribution, dose-response, and mechanisms of antibody transport to and within the brain after administering non-targeted radiolabeled or fluorescently-labeled full length immunoglobulin G (IgG) to normal adult female rats. Intranasal [125I]-IgG consistently yielded highest concentrations in the olfactory bulbs, trigeminal nerves, and leptomeningeal blood vessels with their associated PVS. Intranasal delivery also resulted in significantly higher [125I]-IgG concentrations in the CNS than systemic (intra-arterial) delivery for doses producing similar endpoint blood concentrations. Importantly, CNS targeting significantly increased with increasing dose only with intranasal administration, yielding brain concentrations that ranged from the low-to-mid picomolar range with tracer dosing (50 μg) up to the low nanomolar range at higher doses (1 mg and 2.5 mg). Finally, intranasal pre-treatment with a previously identified nasal permeation enhancer, matrix metalloproteinase-9, significantly improved intranasal [125I]-IgG delivery to multiple brain regions and further allowed us to elucidate IgG transport pathways extending from the nasal epithelia into the brain using fluorescence microscopy. The results show that it may be feasible to achieve therapeutic levels of IgG in the CNS, particularly at higher intranasal doses, and clarify the likely cranial nerve and perivascular distribution pathways taken by antibodies to reach the brain from the nasal mucosae.",

keywords = "Antibodies, Brain, Intranasal, Olfactory, Perivascular, Trigeminal",

author = "Kumar, {Niyanta N.} and Lochhead, {Jeffrey J.} and Pizzo, {Michelle E.} and Geetika Nehra and Sam Boroumand and Gretchen Greene and Thorne, {Robert G.}",

note = "Funding Information: This work was generously supported by the Michael J. Fox Foundation for Parkinson's Research (UW Reference # MSN189990 ), the Clinical and Translational Science Award program administered through the NIH National Center for Advancing Translational Sciences ( NIH UL1TR000427 and KL2TE000428 ), the Wisconsin Alumni Research Foundation Accelerator Program , the University of Wisconsin-Madison School of Pharmacy , the Graduate School at the University of Wisconsin-Madison , fellowships through the National Science Foundation Graduate Research Fellowship under Grant No. DGE-1256259 (MEP), NIH fellowships ( NRSA T32 EBO11434 – MEP), Parkinson's Foundation-American Parkinson's Disease Association Summer Student Fellowship ( PF-APDA-SFW-1730 – SB), the Hilldale Undergraduate Research Fellowship from the University of Wisconsin-Madison (SB), and the Howard Hughes Medical Institute Precollege and Undergraduate Science Education Program grant to Macalester College (GG). Laser scanning confocal microscopy was performed with training and guidance from Dr. Michael Taylor (Nikon A1R) and Dr. Arash Bashirullah (Olympus FV1000) at the University of Wisconsin-Madison School of Pharmacy. Publisher Copyright: {\textcopyright} 2018 Elsevier B.V.",

year = "2018",

month = sep,

day = "28",

doi = "10.1016/j.jconrel.2018.08.006",

language = "English (US)",

volume = "286",

pages = "467--484",

journal = "Journal of Controlled Release",

issn = "0168-3659",

publisher = "Elsevier B.V.",

}

TY - JOUR

T1 - Delivery of immunoglobulin G antibodies to the rat nervous system following intranasal administration

T2 - Distribution, dose-response, and mechanisms of delivery

AU - Kumar, Niyanta N.

AU - Lochhead, Jeffrey J.

AU - Pizzo, Michelle E.

AU - Nehra, Geetika

AU - Boroumand, Sam

AU - Greene, Gretchen

AU - Thorne, Robert G.

N1 - Funding Information: This work was generously supported by the Michael J. Fox Foundation for Parkinson's Research (UW Reference # MSN189990 ), the Clinical and Translational Science Award program administered through the NIH National Center for Advancing Translational Sciences ( NIH UL1TR000427 and KL2TE000428 ), the Wisconsin Alumni Research Foundation Accelerator Program , the University of Wisconsin-Madison School of Pharmacy , the Graduate School at the University of Wisconsin-Madison , fellowships through the National Science Foundation Graduate Research Fellowship under Grant No. DGE-1256259 (MEP), NIH fellowships ( NRSA T32 EBO11434 – MEP), Parkinson's Foundation-American Parkinson's Disease Association Summer Student Fellowship ( PF-APDA-SFW-1730 – SB), the Hilldale Undergraduate Research Fellowship from the University of Wisconsin-Madison (SB), and the Howard Hughes Medical Institute Precollege and Undergraduate Science Education Program grant to Macalester College (GG). Laser scanning confocal microscopy was performed with training and guidance from Dr. Michael Taylor (Nikon A1R) and Dr. Arash Bashirullah (Olympus FV1000) at the University of Wisconsin-Madison School of Pharmacy. Publisher Copyright: © 2018 Elsevier B.V.

PY - 2018/9/28

Y1 - 2018/9/28

N2 - The intranasal route has been hypothesized to circumvent the blood-brain and blood-cerebrospinal fluid barriers, allowing entry into the brain via extracellular pathways along olfactory and trigeminal nerves and the perivascular spaces (PVS) of cerebral blood vessels. We investigated the potential of the intranasal route to non-invasively deliver antibodies to the brain 30 min following administration by characterizing distribution, dose-response, and mechanisms of antibody transport to and within the brain after administering non-targeted radiolabeled or fluorescently-labeled full length immunoglobulin G (IgG) to normal adult female rats. Intranasal [125I]-IgG consistently yielded highest concentrations in the olfactory bulbs, trigeminal nerves, and leptomeningeal blood vessels with their associated PVS. Intranasal delivery also resulted in significantly higher [125I]-IgG concentrations in the CNS than systemic (intra-arterial) delivery for doses producing similar endpoint blood concentrations. Importantly, CNS targeting significantly increased with increasing dose only with intranasal administration, yielding brain concentrations that ranged from the low-to-mid picomolar range with tracer dosing (50 μg) up to the low nanomolar range at higher doses (1 mg and 2.5 mg). Finally, intranasal pre-treatment with a previously identified nasal permeation enhancer, matrix metalloproteinase-9, significantly improved intranasal [125I]-IgG delivery to multiple brain regions and further allowed us to elucidate IgG transport pathways extending from the nasal epithelia into the brain using fluorescence microscopy. The results show that it may be feasible to achieve therapeutic levels of IgG in the CNS, particularly at higher intranasal doses, and clarify the likely cranial nerve and perivascular distribution pathways taken by antibodies to reach the brain from the nasal mucosae.

AB - The intranasal route has been hypothesized to circumvent the blood-brain and blood-cerebrospinal fluid barriers, allowing entry into the brain via extracellular pathways along olfactory and trigeminal nerves and the perivascular spaces (PVS) of cerebral blood vessels. We investigated the potential of the intranasal route to non-invasively deliver antibodies to the brain 30 min following administration by characterizing distribution, dose-response, and mechanisms of antibody transport to and within the brain after administering non-targeted radiolabeled or fluorescently-labeled full length immunoglobulin G (IgG) to normal adult female rats. Intranasal [125I]-IgG consistently yielded highest concentrations in the olfactory bulbs, trigeminal nerves, and leptomeningeal blood vessels with their associated PVS. Intranasal delivery also resulted in significantly higher [125I]-IgG concentrations in the CNS than systemic (intra-arterial) delivery for doses producing similar endpoint blood concentrations. Importantly, CNS targeting significantly increased with increasing dose only with intranasal administration, yielding brain concentrations that ranged from the low-to-mid picomolar range with tracer dosing (50 μg) up to the low nanomolar range at higher doses (1 mg and 2.5 mg). Finally, intranasal pre-treatment with a previously identified nasal permeation enhancer, matrix metalloproteinase-9, significantly improved intranasal [125I]-IgG delivery to multiple brain regions and further allowed us to elucidate IgG transport pathways extending from the nasal epithelia into the brain using fluorescence microscopy. The results show that it may be feasible to achieve therapeutic levels of IgG in the CNS, particularly at higher intranasal doses, and clarify the likely cranial nerve and perivascular distribution pathways taken by antibodies to reach the brain from the nasal mucosae.

KW - Antibodies

KW - Brain

KW - Intranasal

KW - Olfactory

KW - Perivascular

KW - Trigeminal

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UR - http://www.scopus.com/inward/citedby.url?scp=85052134768&partnerID=8YFLogxK

U2 - 10.1016/j.jconrel.2018.08.006

DO - 10.1016/j.jconrel.2018.08.006

M3 - Article

C2 - 30081144

AN - SCOPUS:85052134768

SN - 0168-3659

VL - 286

SP - 467

EP - 484

JO - Journal of Controlled Release

JF - Journal of Controlled Release

ER -

Delivery of immunoglobulin G antibodies to the rat nervous system following intranasal administration: Distribution, dose-response, and mechanisms of delivery

Abstract

Keywords

ASJC Scopus subject areas

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