Osteoclast-targeted delivery of anti-miRNA oligonucleotides by red blood cell extracellular vesicles

Limei Xu; Xiao Xu; Yujie Liang; Caining Wen; Kan Ouyang; Jiadai Huang; Yin Xiao; Xin Deng; Jiang Xia; Li Duan

doi:10.1016/j.jconrel.2023.04.043

Osteoclast-targeted delivery of anti-miRNA oligonucleotides by red blood cell extracellular vesicles

Limei Xu
, Xiao Xu
, Yujie Liang
, Caining Wen
, Kan Ouyang
, Jiadai Huang
, Yin Xiao
, Xin Deng
, Jiang Xia^*
, Li Duan^*

^*Corresponding author for this work

Department of Biomedical Sciences

Research output: Journal Publications and Reviews › RGC 21 - Publication in refereed journal › peer-review

57 Citations (Scopus)

Abstract

Osteoporosis (OP) affects millions worldwide but currently cannot be cured. Suppressing the level of miR-214 in osteoclasts by the anti-miRNA oligonucleotide (AMO) anti-miR-214 reverses bone absorption and provides a potential treatment. Here we report a peptide-guided delivery strategy using red blood cell extracellular vesicles (RBCEVs) as the vehicle to realize osteoclast-targeted delivery of anti-miR-214. A bi-functional peptide, TBP-CP05, which binds to both the CD63 on RBCEVs and receptors on osteoclasts, acts as the guide. TBP-CP05 binds with RBCEVs through CP05, displays the TRAP-binding peptide (TBP) on the surface of EVs, and endows RBCEVs with osteoclast-targeting capability both in vitro and in vivo. Intravenous injection of the osteoclast-targeting RBCEVs (OT-RBCEVs) led to the enrichment of EVs in the bone skeleton, significant inhibition of the osteoclast activity, elevated osteoblast activity, and improved bone density in osteoporotic mice. Altogether, this work demonstrates efficient guidance of drug-loaded EVs to the targeted cells in vivo using bi-functional fusion peptides, and showcases that targeted delivery of anti-miR-214 by OT-RBCEVs may be a viable method for OP treatment. SIGNIFICANCE STATEMENT. Surface functionalization of EVs endows these nanovesicles cell-specific targeting property which guides the drug cargos to specific tissues and cells with higher accuracy, longer retention, and minimal off-target effects. Methods to functionalize EVs with minimal procedures are highly desired for clinical applications. Here we present a facile method using a bifunctional fusion peptide to guide RBCEVs to osteoclasts. A simple incubation of the bifunctional peptide and RBCEVs results in osteoclast-targeting RBCEVs (OT-RBCEVs) that effectively deliver anti-miR-214 to osteoclasts in vivo in a mouse model of osteoporosis, bringing a potential therapy to osteoporotic patients. This is, to our knowledge, the first report on peptide functionalization of RBCEVs and osteoclast-targeted delivery using RBCEVs. © 2023 Elsevier B.V.

Original language	English
Pages (from-to)	259-272
Number of pages	14
Journal	Journal of Controlled Release
Volume	358
Online published	5 May 2023
DOIs	https://doi.org/10.1016/j.jconrel.2023.04.043
Publication status	Published - Jun 2023

Funding

National Natural Science Foundation of China (81972116, 81772394, and 82102607), Shenzhen Science and Technology Projects (SGDX20201103095800003, GJHZ20200731095606019, and JCYJ20170817172023838); Guangdong International Cooperation Project (2021A0505030011); China Postdoctoral Science Foundation (2020M682907 and 2021M702286); PhD Research Foundation of Affiliated Hospital of Jining Medical University (2022-BS-03, 2022-BS-04); Research Grants Council of Hong Kong (Research Impact Fund R5013-19).

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Research Keywords

Mice
Animals
Osteoclasts/metabolism
MicroRNAs/genetics
Oligonucleotides/genetics
Antagomirs/metabolism
Osteoporosis/metabolism
Extracellular Vesicles/metabolism
Peptides/pharmacology
Erythrocytes/metabolism
Osteoporosis
Red blood cells
Extracellular vesicles
Targeted delivery
Anti-miR-214

RGC Funding Information

RGC-funded

Access Output

10.1016/j.jconrel.2023.04.043

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Cite this

@article{a793b6ebf37b41fd8a6e1045fc360725,

title = "Osteoclast-targeted delivery of anti-miRNA oligonucleotides by red blood cell extracellular vesicles",

abstract = "Osteoporosis (OP) affects millions worldwide but currently cannot be cured. Suppressing the level of miR-214 in osteoclasts by the anti-miRNA oligonucleotide (AMO) anti-miR-214 reverses bone absorption and provides a potential treatment. Here we report a peptide-guided delivery strategy using red blood cell extracellular vesicles (RBCEVs) as the vehicle to realize osteoclast-targeted delivery of anti-miR-214. A bi-functional peptide, TBP-CP05, which binds to both the CD63 on RBCEVs and receptors on osteoclasts, acts as the guide. TBP-CP05 binds with RBCEVs through CP05, displays the TRAP-binding peptide (TBP) on the surface of EVs, and endows RBCEVs with osteoclast-targeting capability both in vitro and in vivo. Intravenous injection of the osteoclast-targeting RBCEVs (OT-RBCEVs) led to the enrichment of EVs in the bone skeleton, significant inhibition of the osteoclast activity, elevated osteoblast activity, and improved bone density in osteoporotic mice. Altogether, this work demonstrates efficient guidance of drug-loaded EVs to the targeted cells in vivo using bi-functional fusion peptides, and showcases that targeted delivery of anti-miR-214 by OT-RBCEVs may be a viable method for OP treatment. SIGNIFICANCE STATEMENT. Surface functionalization of EVs endows these nanovesicles cell-specific targeting property which guides the drug cargos to specific tissues and cells with higher accuracy, longer retention, and minimal off-target effects. Methods to functionalize EVs with minimal procedures are highly desired for clinical applications. Here we present a facile method using a bifunctional fusion peptide to guide RBCEVs to osteoclasts. A simple incubation of the bifunctional peptide and RBCEVs results in osteoclast-targeting RBCEVs (OT-RBCEVs) that effectively deliver anti-miR-214 to osteoclasts in vivo in a mouse model of osteoporosis, bringing a potential therapy to osteoporotic patients. This is, to our knowledge, the first report on peptide functionalization of RBCEVs and osteoclast-targeted delivery using RBCEVs. {\textcopyright} 2023 Elsevier B.V.",

keywords = "Mice, Animals, Osteoclasts/metabolism, MicroRNAs/genetics, Oligonucleotides/genetics, Antagomirs/metabolism, Osteoporosis/metabolism, Extracellular Vesicles/metabolism, Peptides/pharmacology, Erythrocytes/metabolism, Osteoporosis, Red blood cells, Extracellular vesicles, Targeted delivery, Anti-miR-214",

author = "Limei Xu and Xiao Xu and Yujie Liang and Caining Wen and Kan Ouyang and Jiadai Huang and Yin Xiao and Xin Deng and Jiang Xia and Li Duan",

year = "2023",

month = jun,

doi = "10.1016/j.jconrel.2023.04.043",

language = "English",

volume = "358",

pages = "259--272",

journal = "Journal of Controlled Release",

issn = "0168-3659",

publisher = "Elsevier B.V.",

}

TY - JOUR

T1 - Osteoclast-targeted delivery of anti-miRNA oligonucleotides by red blood cell extracellular vesicles

AU - Xu, Limei

AU - Xu, Xiao

AU - Liang, Yujie

AU - Wen, Caining

AU - Ouyang, Kan

AU - Huang, Jiadai

AU - Xiao, Yin

AU - Deng, Xin

AU - Xia, Jiang

AU - Duan, Li

PY - 2023/6

Y1 - 2023/6

N2 - Osteoporosis (OP) affects millions worldwide but currently cannot be cured. Suppressing the level of miR-214 in osteoclasts by the anti-miRNA oligonucleotide (AMO) anti-miR-214 reverses bone absorption and provides a potential treatment. Here we report a peptide-guided delivery strategy using red blood cell extracellular vesicles (RBCEVs) as the vehicle to realize osteoclast-targeted delivery of anti-miR-214. A bi-functional peptide, TBP-CP05, which binds to both the CD63 on RBCEVs and receptors on osteoclasts, acts as the guide. TBP-CP05 binds with RBCEVs through CP05, displays the TRAP-binding peptide (TBP) on the surface of EVs, and endows RBCEVs with osteoclast-targeting capability both in vitro and in vivo. Intravenous injection of the osteoclast-targeting RBCEVs (OT-RBCEVs) led to the enrichment of EVs in the bone skeleton, significant inhibition of the osteoclast activity, elevated osteoblast activity, and improved bone density in osteoporotic mice. Altogether, this work demonstrates efficient guidance of drug-loaded EVs to the targeted cells in vivo using bi-functional fusion peptides, and showcases that targeted delivery of anti-miR-214 by OT-RBCEVs may be a viable method for OP treatment. SIGNIFICANCE STATEMENT. Surface functionalization of EVs endows these nanovesicles cell-specific targeting property which guides the drug cargos to specific tissues and cells with higher accuracy, longer retention, and minimal off-target effects. Methods to functionalize EVs with minimal procedures are highly desired for clinical applications. Here we present a facile method using a bifunctional fusion peptide to guide RBCEVs to osteoclasts. A simple incubation of the bifunctional peptide and RBCEVs results in osteoclast-targeting RBCEVs (OT-RBCEVs) that effectively deliver anti-miR-214 to osteoclasts in vivo in a mouse model of osteoporosis, bringing a potential therapy to osteoporotic patients. This is, to our knowledge, the first report on peptide functionalization of RBCEVs and osteoclast-targeted delivery using RBCEVs. © 2023 Elsevier B.V.

AB - Osteoporosis (OP) affects millions worldwide but currently cannot be cured. Suppressing the level of miR-214 in osteoclasts by the anti-miRNA oligonucleotide (AMO) anti-miR-214 reverses bone absorption and provides a potential treatment. Here we report a peptide-guided delivery strategy using red blood cell extracellular vesicles (RBCEVs) as the vehicle to realize osteoclast-targeted delivery of anti-miR-214. A bi-functional peptide, TBP-CP05, which binds to both the CD63 on RBCEVs and receptors on osteoclasts, acts as the guide. TBP-CP05 binds with RBCEVs through CP05, displays the TRAP-binding peptide (TBP) on the surface of EVs, and endows RBCEVs with osteoclast-targeting capability both in vitro and in vivo. Intravenous injection of the osteoclast-targeting RBCEVs (OT-RBCEVs) led to the enrichment of EVs in the bone skeleton, significant inhibition of the osteoclast activity, elevated osteoblast activity, and improved bone density in osteoporotic mice. Altogether, this work demonstrates efficient guidance of drug-loaded EVs to the targeted cells in vivo using bi-functional fusion peptides, and showcases that targeted delivery of anti-miR-214 by OT-RBCEVs may be a viable method for OP treatment. SIGNIFICANCE STATEMENT. Surface functionalization of EVs endows these nanovesicles cell-specific targeting property which guides the drug cargos to specific tissues and cells with higher accuracy, longer retention, and minimal off-target effects. Methods to functionalize EVs with minimal procedures are highly desired for clinical applications. Here we present a facile method using a bifunctional fusion peptide to guide RBCEVs to osteoclasts. A simple incubation of the bifunctional peptide and RBCEVs results in osteoclast-targeting RBCEVs (OT-RBCEVs) that effectively deliver anti-miR-214 to osteoclasts in vivo in a mouse model of osteoporosis, bringing a potential therapy to osteoporotic patients. This is, to our knowledge, the first report on peptide functionalization of RBCEVs and osteoclast-targeted delivery using RBCEVs. © 2023 Elsevier B.V.

KW - Mice

KW - Animals

KW - Osteoclasts/metabolism

KW - MicroRNAs/genetics

KW - Oligonucleotides/genetics

KW - Antagomirs/metabolism

KW - Osteoporosis/metabolism

KW - Extracellular Vesicles/metabolism

KW - Peptides/pharmacology

KW - Erythrocytes/metabolism

KW - Osteoporosis

KW - Red blood cells

KW - Extracellular vesicles

KW - Targeted delivery

KW - Anti-miR-214

UR - https://www.scopus.com/pages/publications/85156268486

UR - https://www.scopus.com/record/pubmetrics.uri?eid=2-s2.0-85156268486&origin=recordpage

U2 - 10.1016/j.jconrel.2023.04.043

DO - 10.1016/j.jconrel.2023.04.043

M3 - RGC 21 - Publication in refereed journal

C2 - 37121514

SN - 0168-3659

VL - 358

SP - 259

EP - 272

JO - Journal of Controlled Release

JF - Journal of Controlled Release

ER -

Osteoclast-targeted delivery of anti-miRNA oligonucleotides by red blood cell extracellular vesicles

Abstract

Funding

UN SDGs

Research Keywords

RGC Funding Information

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