Cholesterol-modified sphingomyelin chimeric lipid bilayer for improved therapeutic delivery

Cholesterol-modified sphingomyelin chimeric lipid bilayer for improved therapeutic delivery

Cholesterol (Chol) fortifies packing and reduces fluidity and permeability of the lipid bilayer in vesicles (liposomes)-mediated drug delivery. However, under the physiological environment, Chol is rapidly extracted from the lipid bilayer by biomembranes, which jeopardizes membrane stability and res...

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Veröffentlicht in:Nature communications 2024-03, Vol.15 (1), p.2073-2073, Article 2073
Hauptverfasser: Wang, Zhiren, Li, Wenpan, Jiang, Yanhao, Park, Jonghan, Gonzalez, Karina Marie, Wu, Xiangmeng, Zhang, Qing-Yu, Lu, Jianqin
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Sprache:eng
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Animal diseases
Animal models
Animals
Anticancer properties
Antitumor activity
B-cell lymphoma
Beta cells
Cancer
Cholesterol
Cholesterol - chemistry
Colorectal carcinoma
Dexamethasone
Doxorubicin
Drug delivery
Drug resistance
Effectiveness
Female
Females
Fluidity
Glycoproteins
Humanities and Social Sciences
Humans
Irinotecan
Leakage
Lipid bilayers
Lipid Bilayers - chemistry
Lipids
Liposomes - chemistry
Lung cancer
Lymphoma
Membranes
Metastases
Mice
multidisciplinary
Multidrug resistance
P-Glycoprotein
Pancreas
Pancreatic cancer
Payloads
Permeability
Pharmacokinetics
Pharmacology
Phospholipids
Phospholipids - chemistry
Science
Science (multidisciplinary)
siRNA
Sphingomyelin
Sphingomyelins - chemistry
Stability
Xenotransplantation
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Zusammenfassung:Cholesterol (Chol) fortifies packing and reduces fluidity and permeability of the lipid bilayer in vesicles (liposomes)-mediated drug delivery. However, under the physiological environment, Chol is rapidly extracted from the lipid bilayer by biomembranes, which jeopardizes membrane stability and results in premature leakage for delivered payloads, yielding suboptimal clinic efficacy. Herein, we report a Chol-modified sphingomyelin (SM) lipid bilayer via covalently conjugating Chol to SM (SM-Chol), which retains membrane condensing ability of Chol. Systemic structure activity relationship screening demonstrates that SM-Chol with a disulfide bond and longer linker outperforms other counterparts and conventional phospholipids/Chol mixture systems on blocking Chol transfer and payload leakage, increases maximum tolerated dose of vincristine while reducing systemic toxicities, improves pharmacokinetics and tumor delivery efficiency, and enhances antitumor efficacy in SU-DHL-4 diffuse large B-cell lymphoma xenograft model in female mice. Furthermore, SM-Chol improves therapeutic delivery of structurally diversified therapeutic agents (irinotecan, doxorubicin, dexamethasone) or siRNA targeting multi-drug resistant gene (p-glycoprotein) in late-stage metastatic orthotopic KPC-Luc pancreas cancer, 4T1-Luc2 triple negative breast cancer, lung inflammation, and CT26 colorectal cancer animal models in female mice compared to respective FDA-approved nanotherapeutics or lipid compositions. Thus, SM-Chol represents a promising platform for universal and improved drug delivery. Cholesterol (Chol) transfer from lipid bilayer jeopardizes membrane stability and causes premature payload leakage, yielding suboptimal efficacy. Here, the authors report a Chol-modified sphingomyelin (SM) bilayer via covalently conjugating Chol to SM, which retains Chol condensing ability and improves pharmacokinetics and therapeutic delivery of various drugs in diverse disease animal models.
ISSN:2041-1723
2041-1723
DOI:10.1038/s41467-024-46331-7