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Interactions of inhaled liposome with macrophages and neutrophils determine particle biofate and anti-inflammatory effect in acute lung inflammation
Chang Liu1; Yihan Liu1; Long Xi1; Yuan He2; Yingmin Liang3; Judith Choi Wo Mak3; Shirui Mao4; Zhenping Wang5; Ying Zheng1
2022-12-30
Source PublicationACS Applied Materials & Interfaces
ISSN1944-8244
Volume15Issue:1Pages:479–493
Abstract

Since most current studies have focused on exploring how phagocyte internalization of drug-loaded nanovesicles by macrophages would affect the function and therapeutic effects of infiltrated neutrophils or monocytes, research has evaluated the specificity of the inhaled nanovesicles for targeting various phagocytes subpopulations. In this study, liposomes with various charges (including neutral (L1), anionic (L2), and cationic at inflammatory sites (L3)) were constructed to investigate how particle charge determined their interactions with key phagocytes (including macrophages and neutrophils) in acute lung injury (ALI) models and to establish correlations with their biofate and overall anti-inflammatory effect. Our results clearly indicated that neutrophils were capable of rapidly sequestering L3 with a 3.2-fold increase in the cellular liposome distribution, compared to that in AMs, while 70.5% of L2 were preferentially uptaken by alveolar macrophages (AMs). Furthermore, both AMs and the infiltrated neutrophils performed as the potential vesicles for the inhaled liposomes to prolong their lung retention in ALI models, whereas AMs function as sweepers to recognize and process liposomes in the healthy lung. Finally, inhaled roflumilast-loaded macrophage or neutrophil preferential liposomes (L2 or L3) exhibited optimal anti-inflammatory effect because of the decreased AMs phagocytic capacity or the prolonged circulation times of neutrophils. Such findings will be beneficial in exploiting a potential pathway to specifically manipulate lung phagocyte functions in lung inflammatory diseases where these cells play crucial roles.

KeywordAcute Lung Inflammation Bio−nano Interaction Inhaled Liposome Lung Phagocytes Lung Retention
DOI10.1021/acsami.2c17660
Indexed BySCIE
Language英語English
WOS Research AreaScience & Technology - Other Topics ; Materials Science
WOS SubjectNanoscience & Nanotechnology ; Materials Science, Multidisciplinary
WOS IDWOS:000907810700001
Scopus ID2-s2.0-85145469060
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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
Corresponding AuthorYing Zheng
Affiliation1.State Key Laboratory of Quality Research in Chinese Medicine, Institute of Chinese Medical Sciences, University of Macau, Macau 999078, China
2.Department of Pharmacy, Xuzhou Medical University, Xuzhou 221004, China
3.School of Clinical Medicine, Department of Medicine, LKS Faculty of Medicine, The University of Hong Kong, Hong Kong 999077, China
4.School of Pharmacy, Shenyang Pharmaceutical University, Shenyang 110016, China
5.Department of Dermatology, School of Medicine, University of California, San Diego, San Diego, California 92093, United States
First Author AffilicationInstitute of Chinese Medical Sciences
Corresponding Author AffilicationInstitute of Chinese Medical Sciences
Recommended Citation
GB/T 7714
Chang Liu,Yihan Liu,Long Xi,et al. Interactions of inhaled liposome with macrophages and neutrophils determine particle biofate and anti-inflammatory effect in acute lung inflammation[J]. ACS Applied Materials & Interfaces, 2022, 15(1), 479–493.
APA Chang Liu., Yihan Liu., Long Xi., Yuan He., Yingmin Liang., Judith Choi Wo Mak., Shirui Mao., Zhenping Wang., & Ying Zheng (2022). Interactions of inhaled liposome with macrophages and neutrophils determine particle biofate and anti-inflammatory effect in acute lung inflammation. ACS Applied Materials & Interfaces, 15(1), 479–493.
MLA Chang Liu,et al."Interactions of inhaled liposome with macrophages and neutrophils determine particle biofate and anti-inflammatory effect in acute lung inflammation".ACS Applied Materials & Interfaces 15.1(2022):479–493.
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