Pre-existing Anti-polyethylene Glycol Antibody Reduces the Therapeutic Efficacy and Pharmacokinetics of PEGylated Liposomes

Overview

Journal Theranostics

Date 2018 Jun 14

PMID 29896310

Citations 39

Authors

Yuan-Chin Hsieh

Hsin-Ell Wang

Wen-Wei Lin

Steve R Roffler

Ta-Chun Cheng

Yu-Cheng Su

Jia-Je Li

Chao-Cheng Chen

Chun-Han Huang

Bing-Mae Chen

Jaw-Yuan Wang

Tian-Lu Cheng

Fang-Ming Chen

Affiliations

Soon will be listed here.

Abstract

Increasing frequency of human exposure to PEG-related products means that healthy people are likely to have pre-existing anti-PEG antibodies (pre-αPEG Ab). However, the influence of pre-αPEG Abs on the pharmacokinetics (PK) and therapeutic efficacy of LipoDox is unknown. We generated two pre-αPEG Ab mouse models. First, naïve mice were immunized with PEGylated protein to generate an endogenous αPEG Ab titer (endo αPEG). Second, monoclonal αPEG Abs were passively transferred (αPEG-PT) into naïve mice to establish a αPEG titer. The naïve, endo αPEG and αPEG-PT mice were intravenously injected with in-labeled LipoDox to evaluate its PK. Tumor-bearing naïve, endo αPEG and αPEG-PT mice were intravenously injected with in-labeled LipoDox to evaluate its biodistribution. The therapeutic efficacy of LipoDox was estimated in the tumor-bearing mice. The areas under the curve (AUC) of LipoDox in endo αPEG and αPEG-PT mice were 11.5- and 15.6- fold less, respectively, than that of the naïve group. The biodistribution results suggested that pre-αPEG Ab can significantly reduce tumor accumulation and accelerate blood clearance of In-labeled LipoDox from the spleen. The tumor volumes of the tumor-bearing endo αPEG and αPEG-PT mice after treatment with LipoDox were significantly increased as compared with that of the tumor-bearing naïve mice. Pre-αPEG Abs were found to dramatically alter the PK and reduce the tumor accumulation and therapeutic efficacy of LipoDox. Pre-αPEG may have potential as a marker to aid development of personalized therapy using LipoDox and achieve optimal therapeutic efficacy.

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