ID | 116267 |
著者 |
Kozma, Gergely Tibor
Semmelweis University|SeroScience
Szebeni, Janos
Semmelweis University|SeroScience|Miskolc University
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キーワード | Complement
Drug targeting
Immunogenicity
Liposomes
Nanomedicines
Pharmacokinetics
Biologicals
Hypersensitivity reactions
C activation-related pseudoallergy (CARPA)
Adverse drug reactions (ADRs)
Anti-drug antibodies
Accelerated blood clearance (ABC)
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資料タイプ |
学術雑誌論文
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抄録 | Conjugation of polyethylene glycols (PEGs) to proteins or drug delivery nanosystems is a widely accepted method to increase the therapeutic index of complex nano-biopharmaceuticals. Nevertheless, these drugs and agents are often immunogenic, triggering the rise of anti-drug antibodies (ADAs). Among these ADAs, anti-PEG IgG and IgM were shown to account for efficacy loss due to accelerated blood clearance of the drug (ABC phenomenon) and hypersensitivity reactions (HSRs) entailing severe allergic symptoms with occasionally fatal anaphylaxis. In addition to recapitulating the basic information on PEG and its applications, this review expands on the physicochemical factors influencing its immunogenicity, the prevalence, features, mechanism of formation and detection of anti-PEG IgG and IgM and the mechanisms by which these antibodies (Abs) induce ABC and HSRs. In particular, we highlight the in vitro, animal and human data attesting to anti-PEG Ab-induced complement (C) activation as common underlying cause of both adverse effects. A main message is that correct measurement of anti-PEG Abs and individual proneness for C activation might predict the rise of adverse immune reactions to PEGylated drugs and thereby increase their efficacy and safety.
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掲載誌名 |
Advanced Drug Delivery Reviews
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ISSN | 0169409X
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cat書誌ID | AA10689127
AA1152215X
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出版者 | Elsevier
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巻 | 154-155
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開始ページ | 163
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終了ページ | 175
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発行日 | 2020-08-01
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権利情報 | This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
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出版社版DOI | |
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フルテキストファイル | |
言語 |
eng
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著者版フラグ |
出版社版
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部局 |
薬学系
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