Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects

Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects

Hong Jiang,1,* Zhi-Peng Li,1,* Gui-Xiang Tian,1,* Rui-Yan Pan,1 Chong-Mei Xu,2 Bo Zhang,2 Jing-liang Wu1 1School of Bioscience and Technology, Weifang Medical University, Weifang, Shandong, China; 2School of Pharmacy, Weifang Medical University, Weifang, Shandong, China *These authors contributed...

Full description

Bibliographic Details
Main Authors: Jiang H, Li ZP, Tian GX, Pan RY, Xu CM, Zhang B, Wu JL
Format: Article
Language:English
Published: Dove Medical Press 2019-03-01
Series:International Journal of Nanomedicine
Subjects:
Liver-targeted
LPs
curcumin
combretastatin A4 phosphate
combination therapy
Online Access:https://www.dovepress.com/liver-targeted-liposomes-for-codelivery-of-curcumin-and-combretastatin-peer-reviewed-article-IJN
id doaj-01217ca022574beb855971fa412a72ba
record_format Article
spelling doaj-01217ca022574beb855971fa412a72ba2020-11-25T01:33:49ZengDove Medical PressInternational Journal of Nanomedicine1178-20132019-03-01Volume 141789180444505Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effectsJiang HLi ZPTian GXPan RYXu CMZhang BWu JLHong Jiang,1,* Zhi-Peng Li,1,* Gui-Xiang Tian,1,* Rui-Yan Pan,1 Chong-Mei Xu,2 Bo Zhang,2 Jing-liang Wu1 1School of Bioscience and Technology, Weifang Medical University, Weifang, Shandong, China; 2School of Pharmacy, Weifang Medical University, Weifang, Shandong, China *These authors contributed equally to this work Background: Recent efforts have been focused on combining two or more therapeutic approaches with different mechanisms to enhance antitumor therapy. Moreover, nanosize drug-delivery systems for codelivering two drugs with proapoptotic and antiangiogenic activities have exhibited great potential in efficient treatment of cancers. Methods: Glycyrrhetinic acid (GA)–modified liposomes (GA LPs) for liver-targeted codelivery of curcumin (Cur) and combretastatin A4 phosphate (CA4P) were prepared and characterized. In vitro cellular uptake, cytotoxicity, cell migration, in vivo biodistribution, antitumor activity, and histopathological studies were performed. Results: Compared with unmodified LPs (Cur-CA4P LPs), Cur-CA4P/GA LPs were taken up effectively by human hepatocellular carcinoma cells (BEL-7402) and showed higher cytotoxicity than free drugs. In vivo real-time near-infrared fluorescence–imaging results indicated that GA-targeted LPs increased accumulation in the tumor region. Moreover, Cur-CA4P/GA LPs showed stronger inhibition of tumor proliferation than Cur, Cur + CA4P, and Cur-CA4P LPs in vivo antitumor studies, which was also verified by H&E staining. Conclusion: GA-modified LPs can serve as a promising nanocarrier for liver-targeted co-delivery of antitumor drugs against hepatocellular carcinoma. Keywords: liver-targeted, LPs, curcumin, combretastatin A4 phosphate, combination therapyhttps://www.dovepress.com/liver-targeted-liposomes-for-codelivery-of-curcumin-and-combretastatin-peer-reviewed-article-IJNLiver-targetedLPscurcumincombretastatin A4 phosphatecombination therapy
collection DOAJ
language English
format Article
sources DOAJ
author Jiang H
Li ZP
Tian GX
Pan RY
Xu CM
Zhang B
Wu JL
spellingShingle Jiang H
Li ZP
Tian GX
Pan RY
Xu CM
Zhang B
Wu JL
Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects
International Journal of Nanomedicine
Liver-targeted
LPs
curcumin
combretastatin A4 phosphate
combination therapy
author_facet Jiang H
Li ZP
Tian GX
Pan RY
Xu CM
Zhang B
Wu JL
author_sort Jiang H
title Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects
title_short Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects
title_full Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects
title_fullStr Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects
title_full_unstemmed Liver-targeted liposomes for codelivery of curcumin and combretastatin A4 phosphate: preparation, characterization, and antitumor effects
title_sort liver-targeted liposomes for codelivery of curcumin and combretastatin a4 phosphate: preparation, characterization, and antitumor effects
publisher Dove Medical Press
series International Journal of Nanomedicine
issn 1178-2013
publishDate 2019-03-01
description Hong Jiang,1,* Zhi-Peng Li,1,* Gui-Xiang Tian,1,* Rui-Yan Pan,1 Chong-Mei Xu,2 Bo Zhang,2 Jing-liang Wu1 1School of Bioscience and Technology, Weifang Medical University, Weifang, Shandong, China; 2School of Pharmacy, Weifang Medical University, Weifang, Shandong, China *These authors contributed equally to this work Background: Recent efforts have been focused on combining two or more therapeutic approaches with different mechanisms to enhance antitumor therapy. Moreover, nanosize drug-delivery systems for codelivering two drugs with proapoptotic and antiangiogenic activities have exhibited great potential in efficient treatment of cancers. Methods: Glycyrrhetinic acid (GA)–modified liposomes (GA LPs) for liver-targeted codelivery of curcumin (Cur) and combretastatin A4 phosphate (CA4P) were prepared and characterized. In vitro cellular uptake, cytotoxicity, cell migration, in vivo biodistribution, antitumor activity, and histopathological studies were performed. Results: Compared with unmodified LPs (Cur-CA4P LPs), Cur-CA4P/GA LPs were taken up effectively by human hepatocellular carcinoma cells (BEL-7402) and showed higher cytotoxicity than free drugs. In vivo real-time near-infrared fluorescence–imaging results indicated that GA-targeted LPs increased accumulation in the tumor region. Moreover, Cur-CA4P/GA LPs showed stronger inhibition of tumor proliferation than Cur, Cur + CA4P, and Cur-CA4P LPs in vivo antitumor studies, which was also verified by H&E staining. Conclusion: GA-modified LPs can serve as a promising nanocarrier for liver-targeted co-delivery of antitumor drugs against hepatocellular carcinoma. Keywords: liver-targeted, LPs, curcumin, combretastatin A4 phosphate, combination therapy
topic Liver-targeted
LPs
curcumin
combretastatin A4 phosphate
combination therapy
url https://www.dovepress.com/liver-targeted-liposomes-for-codelivery-of-curcumin-and-combretastatin-peer-reviewed-article-IJN
work_keys_str_mv AT jiangh livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
AT lizp livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
AT tiangx livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
AT panry livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
AT xucm livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
AT zhangb livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
AT wujl livertargetedliposomesforcodeliveryofcurcuminandcombretastatina4phosphatepreparationcharacterizationandantitumoreffects
_version_ 1725075526299680768

Similar Items