n-dodecyl-β-d-maltoside inhibits aggregation of human interferon-β-1b and reduces its immunogenicity

Robert A. Rifkin; Edward T. Maggio; Sonny Dike; Douglas A. Kerr; Michael Levy

doi:10.1007/s11481-010-9226-7

n-dodecyl-β-d-maltoside inhibits aggregation of human interferon-β-1b and reduces its immunogenicity

Robert A. Rifkin, Edward T. Maggio, Sonny Dike, Douglas A. Kerr, Michael Levy

School of Medicine

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

27 Scopus citations

Abstract

The development of neutralizing antibodies to the protein drug interferon-β is a significant impediment to its use in the treatment of multiple sclerosis. Neutralizing antibodies to interferon-β arise from aggregation of the peptide during manufacturing and storage. We tested the ability of dodecylmaltoside, a nontoxic alkylsaccharide surfactant, to reduce aggregation of interferon-β in vitro and to reduce its immunogenicity in vivo. Interferon-β, in solution with and without dodecylmaltoside, was periodically evaluated for aggregation by light scatter for 1 month. Interferon-β, with and without dodecylmaltoside, was given 3 days/week for 1 month to mice; the sera of these mice were analyzed for anti-interferon-β antibodies by ELISA. Dodecylmaltoside reduces the aggregation of interferon-β in vitro and its immunogenicity in vivo. Our positive findings warrant additional tests of dodecylmaltoside as a therapeutic adjuvant in rodent models of multiple sclerosis.

Original language	English (US)
Pages (from-to)	158-162
Number of pages	5
Journal	Journal of Neuroimmune Pharmacology
Volume	6
Issue number	1
DOIs	https://doi.org/10.1007/s11481-010-9226-7
State	Published - Mar 2011

Keywords

disaccharides/chemistry
excipients
interferon-beta
multiple sclerosis

ASJC Scopus subject areas

Neuroscience (miscellaneous)
Immunology and Allergy
Immunology
Pharmacology

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10.1007/s11481-010-9226-7

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title = "n-dodecyl-β-d-maltoside inhibits aggregation of human interferon-β-1b and reduces its immunogenicity",

abstract = "The development of neutralizing antibodies to the protein drug interferon-β is a significant impediment to its use in the treatment of multiple sclerosis. Neutralizing antibodies to interferon-β arise from aggregation of the peptide during manufacturing and storage. We tested the ability of dodecylmaltoside, a nontoxic alkylsaccharide surfactant, to reduce aggregation of interferon-β in vitro and to reduce its immunogenicity in vivo. Interferon-β, in solution with and without dodecylmaltoside, was periodically evaluated for aggregation by light scatter for 1 month. Interferon-β, with and without dodecylmaltoside, was given 3 days/week for 1 month to mice; the sera of these mice were analyzed for anti-interferon-β antibodies by ELISA. Dodecylmaltoside reduces the aggregation of interferon-β in vitro and its immunogenicity in vivo. Our positive findings warrant additional tests of dodecylmaltoside as a therapeutic adjuvant in rodent models of multiple sclerosis.",

keywords = "disaccharides/chemistry, excipients, interferon-beta, multiple sclerosis",

author = "Rifkin, {Robert A.} and Maggio, {Edward T.} and Sonny Dike and Kerr, {Douglas A.} and Michael Levy",

note = "Funding Information: This project was funded by philanthropic donations to Project RESTORE at The Johns Hopkins University and by Nerveda, Inc. R.A.Rifkin(*).S.Dike.M.Levy Department of Neurology, The Johns Hopkins University School of Medicine, 600 North Wolfe Street, Pathology Building, Room 506, Baltimore, MD 21287-0005, USA e-mail: rrifkin2@jhmi.edu",

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AU - Dike, Sonny

AU - Kerr, Douglas A.

AU - Levy, Michael

N1 - Funding Information: This project was funded by philanthropic donations to Project RESTORE at The Johns Hopkins University and by Nerveda, Inc. R.A.Rifkin(*).S.Dike.M.Levy Department of Neurology, The Johns Hopkins University School of Medicine, 600 North Wolfe Street, Pathology Building, Room 506, Baltimore, MD 21287-0005, USA e-mail: rrifkin2@jhmi.edu

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N2 - The development of neutralizing antibodies to the protein drug interferon-β is a significant impediment to its use in the treatment of multiple sclerosis. Neutralizing antibodies to interferon-β arise from aggregation of the peptide during manufacturing and storage. We tested the ability of dodecylmaltoside, a nontoxic alkylsaccharide surfactant, to reduce aggregation of interferon-β in vitro and to reduce its immunogenicity in vivo. Interferon-β, in solution with and without dodecylmaltoside, was periodically evaluated for aggregation by light scatter for 1 month. Interferon-β, with and without dodecylmaltoside, was given 3 days/week for 1 month to mice; the sera of these mice were analyzed for anti-interferon-β antibodies by ELISA. Dodecylmaltoside reduces the aggregation of interferon-β in vitro and its immunogenicity in vivo. Our positive findings warrant additional tests of dodecylmaltoside as a therapeutic adjuvant in rodent models of multiple sclerosis.

AB - The development of neutralizing antibodies to the protein drug interferon-β is a significant impediment to its use in the treatment of multiple sclerosis. Neutralizing antibodies to interferon-β arise from aggregation of the peptide during manufacturing and storage. We tested the ability of dodecylmaltoside, a nontoxic alkylsaccharide surfactant, to reduce aggregation of interferon-β in vitro and to reduce its immunogenicity in vivo. Interferon-β, in solution with and without dodecylmaltoside, was periodically evaluated for aggregation by light scatter for 1 month. Interferon-β, with and without dodecylmaltoside, was given 3 days/week for 1 month to mice; the sera of these mice were analyzed for anti-interferon-β antibodies by ELISA. Dodecylmaltoside reduces the aggregation of interferon-β in vitro and its immunogenicity in vivo. Our positive findings warrant additional tests of dodecylmaltoside as a therapeutic adjuvant in rodent models of multiple sclerosis.

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n-dodecyl-β-d-maltoside inhibits aggregation of human interferon-β-1b and reduces its immunogenicity

Abstract

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ASJC Scopus subject areas

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