Development of a macrophage-targeting and phagocytosis-inducing bio-nanocapsule-based nanocarrier for drug delivery

Hao Li; Kenji Tatematsu; Masaharu Somiya; Masumi Iijima; Shun'ichi Kuroda

doi:10.1016/j.actbio.2018.04.023

Development of a macrophage-targeting and phagocytosis-inducing bio-nanocapsule-based nanocarrier for drug delivery

Acta Biomater. 2018 Jun:73:412-423. doi: 10.1016/j.actbio.2018.04.023. Epub 2018 Apr 16.

Authors

Hao Li¹, Kenji Tatematsu¹, Masaharu Somiya¹, Masumi Iijima¹, Shun'ichi Kuroda²

Affiliations

¹ The Institute of Scientific and Industrial Research, Osaka University, Ibaraki 567-0047, Japan.
² The Institute of Scientific and Industrial Research, Osaka University, Ibaraki 567-0047, Japan. Electronic address: skuroda@sanken.osaka-u.ac.jp.

PMID: 29673839
DOI: 10.1016/j.actbio.2018.04.023

Abstract

Macrophage hyperfunction or dysfunction is tightly associated with various diseases, such as osteoporosis, inflammatory disorder, and cancers. However, nearly all conventional drug delivery system (DDS) nanocarriers utilize endocytosis for entering target cells; thus, the development of macrophage-targeting and phagocytosis-inducing DDS nanocarriers for treating these diseases is required. In this study, we developed a hepatitis B virus (HBV) envelope L particle (i.e., bio-nanocapsule (BNC)) outwardly displaying a tandem form of protein G-derived IgG Fc-binding domain and protein L-derived IgG Fab-binding domain (GL-BNC). When conjugated with the macrophage-targeting ligand, mouse IgG2a (mIgG2a), the GL-BNC itself, and the liposome-fused GL-BNC (i.e., GL-virosome) spontaneously initiated aggregation by bridging between the Fc-binding domain and Fab-binding domain with mIgG2a. The aggregates were efficiently taken up by macrophages, whereas this was inhibited by latrunculin B, a phagocytosis-specific inhibitor. The mIgG2a-GL-virosome containing doxorubicin exhibited higher cytotoxicity toward macrophages than conventional liposomes and other BNC-based virosomes. Thus, GL-BNCs and GL-virosomes may constitute promising macrophage-targeting and phagocytosis-inducing DDS nanocarriers.

Statement of significance: We have developed a novel macrophage-targeting and phagocytosis-inducing bio-nanocapsule (BNC)-based nanocarrier named GL-BNC, which comprises a hepatitis B virus envelope L particle outwardly displaying protein G-derived IgG Fc- and protein L-derived IgG Fab-binding domains in tandem. The GL-BNC alone or liposome-fused form (GL-virosomes) could spontaneously aggregate when conjugated with macrophage-targeting IgGs, inducing phagocytosis by the interaction between IgG Fc of aggregates and FcγR on phagocytes. Thereby these aggregates were efficiently taken up by macrophages. GL-virosomes containing doxorubicin exhibited higher cytotoxicity towards macrophages than ZZ-virosomes and liposomes. Our results suggested that GL-BNCs and GL-virosomes would serve as promising drug delivery system nanocarriers for targeting delivery to macrophages.

Keywords: Antibody; Bio-nanocapsule; Macrophage; Phagocyte; Phagocytosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Bridged Bicyclo Compounds, Heterocyclic / chemistry
Cell Line
Cell Line, Tumor
Coculture Techniques
Dendritic Cells / cytology
Doxorubicin / chemistry
Drug Carriers / chemistry*
Endocytosis*
Gene Products, env / chemistry
Hepatitis B virus
Immunoglobulin G / chemistry
Liposomes / chemistry
Macrophages / cytology*
Mice
Microfluidics
Nanocapsules / chemistry*
Phagocytosis
RAW 264.7 Cells
Saccharomyces cerevisiae
Thiazolidines / chemistry

Substances

Bridged Bicyclo Compounds, Heterocyclic
Drug Carriers
Gene Products, env
Immunoglobulin G
Liposomes
Nanocapsules
Thiazolidines
Doxorubicin
latrunculin B