| Literature DB >> 26544061 |
Min Hyung Kang1, Hyun Joon Yoo1, Yie Hyuk Kwon1, Ho Yub Yoon1, Sang Gon Lee1, Sung Rae Kim1, Dong Woo Yeom1, Myung Joo Kang2, Young Wook Choi1.
Abstract
As a novel carrier for folate receptor (FR)-targeted intracellular delivery, we designed two types of targetable liposomal systems using Pep-1 peptide (Pep1) and folic acid as a cell-penetrating peptide (CPP) and target molecule, respectively. Folate-linked Pep1 (Fol-Pep1) was synthesized by solid phase peptide synthesis (SPPS) and verified using (1)H NMR and far-ultraviolet (UV) circular dichroism (CD). The chimeric ligand (Fol-Pep1)-modified liposome (cF-P-L) was prepared by coupling Fol-Pep1 to maleimide-derivatized liposomes at various ratios. The dual ligand (folate and Pep1)-modified liposome (dF/P-L) was prepared by separately attaching both ligands to the liposomal surface via a short (PEG2000) or long (PEG3400) linker. The physical and conformational characteristics including vesicle size, zeta potential, and the number of conjugated ligands were determined. Intracellular uptake specificities of various fluorescent probe-containing cF-P-L and dF/P-L systems were assessed using FR-positive HeLa and FR-negative HaCaT cells. Cellular uptake behavior was visualized by confocal laser scanning microscopy (CLSM). Internalization was time-dependent. Fol-Pep1 and Pep-1 cytotoxicities were negligible up to 25 μM in FR-positive and FR-negative cells. Empty cF-P-L and dF/P-L were nontoxic at the concentration used. The optimized dF3/P2(450/90) system carrying 450 PEG3400-linked folate and 90 PEG2000-linked Pep1 molecules could be a good candidate for FR-specific intracellular drug delivery.Entities:
Keywords: Pep-1; cell penetrating peptide; drug targeting; dual-ligand; folic acid; intracellular delivery; liposome
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Year: 2015 PMID: 26544061 DOI: 10.1021/acs.molpharmaceut.5b00399
Source DB: PubMed Journal: Mol Pharm ISSN: 1543-8384 Impact factor: 4.939