Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy

A type of sorafenib- (SOR-) loaded long-circulating nanoliposome was constructed, and the targeting performance and antitumor effects of the prepared liposome were evaluated in the present study. Polyethylene glycol- (PEG-) modified long-circulating nanoliposomes (LC-NPs) were designed and prepared...

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Main Authors: Haiwei Ye, Liping Zhou, Haili Jin, Yunhua Chen, Die Cheng, Ying Jiang
Format: Article
Language:English
Published: Hindawi Limited 2020-01-01
Series:BioMed Research International
Online Access:http://dx.doi.org/10.1155/2020/1351046
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spelling doaj-4ceb1cc74bd64dc7804dc9a1ad69f56a2020-11-25T03:11:35ZengHindawi LimitedBioMed Research International2314-61332314-61412020-01-01202010.1155/2020/13510461351046Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer TherapyHaiwei Ye0Liping Zhou1Haili Jin2Yunhua Chen3Die Cheng4Ying Jiang5Chemical Pharmaceutical Research Institute, Taizhou Vocational & Technical College, Taizhou 318000, P. R., ChinaChemical Pharmaceutical Research Institute, Taizhou Vocational & Technical College, Taizhou 318000, P. R., ChinaChemical Pharmaceutical Research Institute, Taizhou Vocational & Technical College, Taizhou 318000, P. R., ChinaChemical Pharmaceutical Research Institute, Taizhou Vocational & Technical College, Taizhou 318000, P. R., ChinaChemical Pharmaceutical Research Institute, Taizhou Vocational & Technical College, Taizhou 318000, P. R., ChinaChemical Pharmaceutical Research Institute, Taizhou Vocational & Technical College, Taizhou 318000, P. R., ChinaA type of sorafenib- (SOR-) loaded long-circulating nanoliposome was constructed, and the targeting performance and antitumor effects of the prepared liposome were evaluated in the present study. Polyethylene glycol- (PEG-) modified long-circulating nanoliposomes (LC-NPs) were designed and prepared using reverse evaporation, and the LC-NPs were used for delivering sorafenib (LC-PEG-SOR-NPs). Then, the anti-VEGFR antibody as a targeting moiety was chemically coupled with LC-PEG-SOR-NPs to form liver cancer-targeted nanoliposomes (anti-VEGFR-LC-PEG-SOR-NPs). The drug entrapment and loading efficiency were measured. And the cancer-targeting performance and therapeutic efficiency were evaluated both in vitro and in vivo. The anti-VEGFR-LC-PEG-SOR-NPs with an average of 119.8±4.2 nm showed a uniform spherical structure. The drug entrapment and loading efficiency were 92.5% and 18.5%, respectively. The killing efficiency of anti-VEGFR-LC-PEG-SOR-NPs was up to 18% after incubating with liver cancer cells for 72 h. Furthermore, the anti-VEGFR-LC-PEG-SOR-NPs could actively target at the tumor region and could efficiently inhibit tumor growth with negligible side effects. This newly designed nanoliposomes had desirable dispersibility, high drug entrapment efficiency, tumor targeting and therapeutic efficiency, and good safety. As a biocompatible nanocomposite, it was promising to become a novel and useful tumor-targeting nanodrug for liver cancer therapy.http://dx.doi.org/10.1155/2020/1351046
collection DOAJ
language English
format Article
sources DOAJ
author Haiwei Ye
Liping Zhou
Haili Jin
Yunhua Chen
Die Cheng
Ying Jiang
spellingShingle Haiwei Ye
Liping Zhou
Haili Jin
Yunhua Chen
Die Cheng
Ying Jiang
Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy
BioMed Research International
author_facet Haiwei Ye
Liping Zhou
Haili Jin
Yunhua Chen
Die Cheng
Ying Jiang
author_sort Haiwei Ye
title Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy
title_short Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy
title_full Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy
title_fullStr Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy
title_full_unstemmed Sorafenib-Loaded Long-Circulating Nanoliposomes for Liver Cancer Therapy
title_sort sorafenib-loaded long-circulating nanoliposomes for liver cancer therapy
publisher Hindawi Limited
series BioMed Research International
issn 2314-6133
2314-6141
publishDate 2020-01-01
description A type of sorafenib- (SOR-) loaded long-circulating nanoliposome was constructed, and the targeting performance and antitumor effects of the prepared liposome were evaluated in the present study. Polyethylene glycol- (PEG-) modified long-circulating nanoliposomes (LC-NPs) were designed and prepared using reverse evaporation, and the LC-NPs were used for delivering sorafenib (LC-PEG-SOR-NPs). Then, the anti-VEGFR antibody as a targeting moiety was chemically coupled with LC-PEG-SOR-NPs to form liver cancer-targeted nanoliposomes (anti-VEGFR-LC-PEG-SOR-NPs). The drug entrapment and loading efficiency were measured. And the cancer-targeting performance and therapeutic efficiency were evaluated both in vitro and in vivo. The anti-VEGFR-LC-PEG-SOR-NPs with an average of 119.8±4.2 nm showed a uniform spherical structure. The drug entrapment and loading efficiency were 92.5% and 18.5%, respectively. The killing efficiency of anti-VEGFR-LC-PEG-SOR-NPs was up to 18% after incubating with liver cancer cells for 72 h. Furthermore, the anti-VEGFR-LC-PEG-SOR-NPs could actively target at the tumor region and could efficiently inhibit tumor growth with negligible side effects. This newly designed nanoliposomes had desirable dispersibility, high drug entrapment efficiency, tumor targeting and therapeutic efficiency, and good safety. As a biocompatible nanocomposite, it was promising to become a novel and useful tumor-targeting nanodrug for liver cancer therapy.
url http://dx.doi.org/10.1155/2020/1351046
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