Literature DB >> 28263913

Encapsulation, controlled release, and antitumor efficacy of cisplatin delivered in liposomes composed of sterol-modified phospholipids.

Heidi M Kieler-Ferguson1, Darren Chan2, Jonathan Sockolosky2, Lydia Finney3, Evan Maxey3, Stefan Vogt3, Francis C Szoka4.   

Abstract

We employed a recently introduced class of sterol-modified lipids (SML) to produce m-PEG-DSPE containing liposome compositions with a range of cis-platinum content release rates. SML have a cholesterol succinate attached to the phosphatidylglycerol head group and a fatty acid at the 2 position. These compositions were compared to the well-studied liposome phospholipid compositions: mPEG-DSPE/Hydrogenated Soy PC/cholesterol or mPEG-DSPE/POPC/cholesterol to determine the effect of the cis-platinum release extent on C26 tumor proliferation in the BALB/c colon carcinoma mouse model. The release rates of cis-platinum from liposomes composed of SML are a function of the acyl chain length. SML-liposomes with shorter acyl chain lengths C-8 provided more rapid cisplatin release, lower in vitro IC50, and were easier to formulate compared to liposomes using traditional phospholipid compositions. Similar to other liposome cis-platinum formulations, the half-life of m-PEG-DSPE SML liposome cisplatin is substantially longer than the free drug. This resulted in a higher tumor cisplatin concentration at 48h post-dosing compared to the free drug and higher Pt-DNA adducts in the tumor. Moreover, the maximum tolerated dose of the liposome formulations where up to four fold greater than the free drug. Using X-ray fluorescence spectroscopy on tumor sections, we compared the location of platinum, to the location of a fluorescence lipid incorporated in the liposomes. The liposome platinum co-localized with the fluorescent lipid and both were non-uniformly distributed in the tumor. Non-encapsulated Cis-platinum, albeit at a low concentration, was more uniformly distributed thorough the tumor. Three liposome formulations, including the well-studied hydrogenated HSPC composition, had better antitumor activity in the murine colon 26 carcinoma model as compared to the free drug at the same dose but the SML liposome platinum formulations did not perform better than the HSPC formulation.
Copyright © 2017 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  C26 colon carcinoma; Cisplatin; Liposome; Sterol-modified phospholipid; X-ray fluorescence microscopy

Mesh:

Substances:

Year:  2017        PMID: 28263913      PMCID: PMC5473525          DOI: 10.1016/j.ejps.2017.03.003

Source DB:  PubMed          Journal:  Eur J Pharm Sci        ISSN: 0928-0987            Impact factor:   4.384


  40 in total

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Review 3.  Nanocarriers for delivery of platinum anticancer drugs.

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5.  A Phase 2 trial of the liposomal DACH platinum L-NDDP in patients with therapy-refractory advanced colorectal cancer.

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Review 6.  Designer lipids for drug delivery: from heads to tails.

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7.  Sterol-modified phospholipids: cholesterol and phospholipid chimeras with improved biomembrane properties.

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9.  Ultrasound triggered release of cisplatin from liposomes in murine tumors.

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4.  Cisplatin liposome and 6-amino nicotinamide combination to overcome drug resistance in ovarian cancer cells.

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Review 5.  Liposomal Drug Delivery Systems and Anticancer Drugs.

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6.  Nanoencapsulation of Hirudo medicinalis proteins in liposomes as a nanocarrier for inhibiting angiogenesis through targeting VEGFA in the Breast cancer cell line (MCF-7).

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7.  Mesenchymal Stem Cells As Guideposts for Nanoparticle-Mediated Targeted Drug Delivery in Ovarian Cancer.

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8.  Enhanced Efficacy of PEGylated Liposomal Cisplatin: In Vitro and In Vivo Evaluation.

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9.  Co-Encapsulation of Fisetin and Cisplatin into Liposomes for Glioma Therapy: From Formulation to Cell Evaluation.

Authors:  Morgane Renault-Mahieux; Victoire Vieillard; Johanne Seguin; Philippe Espeau; Dang Tri Le; René Lai-Kuen; Nathalie Mignet; Muriel Paul; Karine Andrieux
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  9 in total

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