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Cyclodextrin-mediated conjugation of macrophage and liposomes for treatment of atherosclerosis
Gao, Cheng1; Liu, Conghui2; Chen, Qian2; Wang, Yan3; Kwong, Cheryl H.T.2; Wang, Qingfu2; Xie, Beibei2; Lee, Simon M.Y.1; Wang, Ruibing1
2022-07-04
Source PublicationJOURNAL OF CONTROLLED RELEASE
ISSN0168-3659
Volume349Pages:2-15
Abstract

Current pharmacological treatments of atherosclerosis often target either cholesterol control or inflammation management, to inhibit atherosclerotic progression, but cannot lead to direct plaque lysis and atherosclerotic regression, partly due to the poor accumulation of medicine in the atherosclerotic plaques. Due to enhanced macrophage recruitment during atheromatous plaque progression, a macrophage-liposome conjugate was facilely constructed for targeted anti-atherosclerosis therapy via synergistic plaque lysis and inflammation alleviation. Endogenous macrophage is utilized as drug-transporting cell, upon membrane-modification with a β-cyclodextrin (β-CD) derivative to form β-CD decorated macrophage (CD-MP). Adamantane (ADA) modified quercetin (QT)-loaded liposome (QT-NP), can be conjugated to CD-MP via host-guest interactions between β-CD and ADA to form macrophage-liposome conjugate (MP-QT-NP). Thus, macrophage carries liposome "hand-in-hand" to significantly increase the accumulation of anchored QT-NP in the aorta plaque in response to the plaque inflammation. In addition to anti-inflammation effects of QT, MP-QT-NP efficiently regresses atherosclerotic plaques from both murine aorta and human carotid arteries via CD-MP mediated cholesterol efflux, due to the binding of cholesterol by excess membrane β-CD. Transcriptome analysis of atherosclerotic murine aorta and human carotid tissues reveal that MP-QT-NP may activate NRF2 pathway to inhibit plaque inflammation, and simultaneously upregulate liver X receptor to promote cholesterol efflux.

KeywordHost-guest Interaction Β-cyclodextrin Drug Delivery Cell-based Carriers Atherosclerosis
DOI10.1016/j.jconrel.2022.06.053
URLView the original
Indexed BySCIE
Language英語English
WOS Research AreaChemistry ; Pharmacology & Pharmacy
WOS SubjectChemistry, Multidisciplinary ; Pharmacology & Pharmacy
WOS IDWOS:000841977100002
Scopus ID2-s2.0-85138451167
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Citation statistics
Document TypeJournal article
CollectionTHE STATE KEY LABORATORY OF QUALITY RESEARCH IN CHINESE MEDICINE (UNIVERSITY OF MACAU)
Institute of Chinese Medical Sciences
DEPARTMENT OF PHARMACEUTICAL SCIENCES
Corresponding AuthorLee, Simon M.Y.; Wang, Ruibing
Affiliation1.State Key Laboratory of Quality Research in Chinese Medicine, Institute of Chinese Medical Sciences, University of Macau, Taipa, Macao 999078, China
2.Department of Pharmaceutical Sciences, Faculty of Health Sciences, University of Macau, Taipa, Macao 999078, China
3.National Integrated Traditional and Western Medicine Center for Cardiovascular Disease, China-Japan Friendship Hospital, Beijing 100029, China
First Author AffilicationInstitute of Chinese Medical Sciences
Corresponding Author AffilicationInstitute of Chinese Medical Sciences
Recommended Citation
GB/T 7714
Gao, Cheng,Liu, Conghui,Chen, Qian,et al. Cyclodextrin-mediated conjugation of macrophage and liposomes for treatment of atherosclerosis[J]. JOURNAL OF CONTROLLED RELEASE, 2022, 349, 2-15.
APA Gao, Cheng., Liu, Conghui., Chen, Qian., Wang, Yan., Kwong, Cheryl H.T.., Wang, Qingfu., Xie, Beibei., Lee, Simon M.Y.., & Wang, Ruibing (2022). Cyclodextrin-mediated conjugation of macrophage and liposomes for treatment of atherosclerosis. JOURNAL OF CONTROLLED RELEASE, 349, 2-15.
MLA Gao, Cheng,et al."Cyclodextrin-mediated conjugation of macrophage and liposomes for treatment of atherosclerosis".JOURNAL OF CONTROLLED RELEASE 349(2022):2-15.
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