Targeting extracellular vesicles to injured tissue using membrane cloaking and surface display

被引:190
作者
Antes, Travis J. [1 ]
Middleton, Ryan C. [1 ]
Luther, Kristin M. [1 ]
Ijichi, Takeshi [1 ]
Peck, Kiel A. [1 ]
Liu, Weixin Jane [1 ]
Valle, Jackie [1 ]
Echavez, Antonio K. [1 ]
Marban, Eduardo [1 ]
机构
[1] Cedars Sinai Med Ctr, Smidt Heart Inst, 8700 Beverly Blvd,Davis Bldg, Los Angeles, CA 90048 USA
关键词
Extracellular vesicles; EV; Exosome; Phospholipid; Membrane anchor; Streptavidin; Biotin; Homing peptides; Targeting antibodies; Qdots; Myoblasts; Cardiomyocytes; Ischemia/reperfusion injury; Infarction; Biodistribution; NanoSight NTA; Surface display; Lactadherin; C1 C2 domain fusions; MUSCLE-BINDING PEPTIDES; VIVO PHAGE DISPLAY; DELIVERY VEHICLES; DRUG-DELIVERY; CELL THERAPY; EXOSOMES; CARDIOMYOCYTE; FIBROBLASTS; PROLIFERATION; REGENERATION;
D O I
10.1186/s12951-018-0388-4
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
Background: Extracellular vesicles (EVs) and exosomes are nano-sized, membrane-bound vesicles shed by most eukaryotic cells studied to date. EVs play key signaling roles in cellular development, cancer metastasis, immune modulation and tissue regeneration. Attempts to modify exosomes to increase their targeting efficiency to specific tissue types are still in their infancy. Here we describe an EV membrane anchoring platform termed "cloaking" to directly embed tissue-specific antibodies or homing peptides on EV membrane surfaces ex vivo for enhanced vesicle uptake in cells of interest. The cloaking system consists of three components: DMPE phospholipid membrane anchor, polyethylene glycol spacer and a conjugated streptavidin platform molecule, to which any biotinylated molecule can be coupled for EV decoration. Results: We demonstrate the utility of membrane surface engineering and biodistribution tracking with this technology along with targeting EVs for enhanced uptake in cardiac fibroblasts, myoblasts and ischemic myocardium using combinations of fluorescent tags, tissue-targeting antibodies and homing peptide surface cloaks. We compare cloaking to a complementary approach, surface display, in which parental cells are engineered to secrete EVs with fusion surface targeting proteins. Conclusions: EV targeting can be enhanced both by cloaking and by surface display; the former entails chemical modification of preformed EVs, while the latter requires genetic modification of the parent cells. Reduction to practice of the cloaking approach, using several different EV surface modifications to target distinct cells and tissues, supports the notion of cloaking as a platform technology.
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页数:15
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