Selective targeting by preS1 domain of hepatitis B surface antigen conjugated with phosphorylcholine‐based amphiphilic block copolymer micelles as a biocompatible, drug delivery carrier for treatment of human hepatocellular carcinoma with paclitaxel

Abstract: Using dithioester-capped 2-methacryloyloxyethyl phosphorylcholine (MPC) as a macro chain transfer agent, a diblock copolymer was synthesized with n-butyl methacrylate (BMA) as hydrophobic core-forming blocks. The MPC-BMA unit was copolymerized with an immobilizable unit, p-nitrophenylcarbonyloxyethyl methacrylate (NPMA). The NPMA moiety then was modified by the addition of preS1 domain of hepatitis B surface antigen (HBsAg). This micelle-forming nanoparticle, the poly (MPC-co-BMA-co-NPMA) (PMBN) conjugated wit… Show more

“…The poly(MPC-co-BMA) (PMB), which forms nanoassemblies (polymeric aggregates) or nanoparticles in aqueous media depending on the degree of hydrophobicity and molecular weight of the polymers, has considerable potential for therapeutic nanomaterials [13]. Previously, a PMB carrying an antineoplastic drug was demonstrated to exhibit antitumor effects on cancer cells without cytotoxicity both in vitro and in vivo [14][15][16]; however, the mechanism whereby the drug in the PMB was delivered across the plasma membrane of cells remains poorly understood. In this study, we discovered direct penetration mechanism across the plasma membrane of living mammalian cells using fluorescence-tagged PMBs.…”

Cell-penetrating macromolecules: Direct penetration of amphipathic phospholipid polymers across plasma membrane of living cells

“…The poly(MPC-co-BMA) (PMB), which forms nanoassemblies (polymeric aggregates) or nanoparticles in aqueous media depending on the degree of hydrophobicity and molecular weight of the polymers, has considerable potential for therapeutic nanomaterials [13]. Previously, a PMB carrying an antineoplastic drug was demonstrated to exhibit antitumor effects on cancer cells without cytotoxicity both in vitro and in vivo [14][15][16]; however, the mechanism whereby the drug in the PMB was delivered across the plasma membrane of cells remains poorly understood. In this study, we discovered direct penetration mechanism across the plasma membrane of living mammalian cells using fluorescence-tagged PMBs.…”

Cell-penetrating macromolecules: Direct penetration of amphipathic phospholipid polymers across plasma membrane of living cells

“…This might be related to both disulfide ratio and MPC content in the phosphorylcholine micelles, because high disulfide ratio in copolymer molecules could speed up the drug release under reduction condition ( Figure 4); at the same time, the intact shield of PC of PCL 20 -ss-PMPC 10 micelles could make the micelles easily pass through cell membranes and enter into tumor cells. 23 Both comprehensive effects lead to that PCL 20 -ss-PMPC 10 /DOX micelles showed higher cytotoxicity against HeLa cells than the other PCL-ss-PMPC/DOX micelles. cellular uptake and intracellular drug release It is known that DOX fluorescence is self-quenched inside micelles.…”

“…The phosphorylcholine micelles exhibit excellent properties, eg, good biocompatibility, high drug-loading ability, excellent prolonged circulation and prominent tumor therapy effect. 16,[19][20][21][22][23][24] Zhao et al 16 investigated in detail the drug loading, in vitro phagocytic uptake, blood clearance and biodistribution in vivo of random copolymer phosphorylcholine micelles with different compositions. However, investigations on the relation between the component of phosphorylcholine micelles and their properties are far from enough.…”

Effects of copolymer component on the properties of phosphorylcholine micelles

“…PreS1 conjugated PMBN (PMBN-preS1) strongly enhanced the synergistic inhibitory effect of PTX on HepG2 cells in vitro. Tumor growth of a HepG2 xenograft was strongly inhibited after intraperitoneal injection of PTX/PMBN-preS1 [34].…”

Zwitterionic drug nanocarriers: A biomimetic strategy for drug delivery