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首页> 外文期刊>Journal of Extracellular Vesicles >Covalent conjugation of extracellular vesicles with peptides and nanobodies for targeted therapeutic delivery
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Covalent conjugation of extracellular vesicles with peptides and nanobodies for targeted therapeutic delivery

机译:用肽和纳米粒细胞囊泡与靶向治疗递送的共价缀合

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Natural extracellular vesicles (EVs) are ideal drug carriers due to their remarkable biocompatibility. Their delivery specificity can be achieved by the conjugation of targeting ligands. However, existing methods to engineer target‐specific EVs are tedious or inefficient, having to compromise between harsh chemical treatments and transient interactions. Here, we describe a novel method for the covalent conjugation of EVs with high copy numbers of targeting moieties using protein ligases. Conjugation of EVs with either an epidermal growth factor receptor (EGFR)‐targeting peptide or anti‐EGFR nanobody facilitates their accumulation in EGFR‐positive cancer cells, both in vitro and in vivo . Systemic delivery of paclitaxel by EGFR‐targeting EVs at a low dose significantly increases drug efficacy in a xenografted mouse model of EGFR‐positive lung cancer. The method is also applicable to the conjugation of EVs with peptides and nanobodies targeting other receptors, such as HER2 and SIRP alpha, and the conjugated EVs can deliver RNA in addition to small molecules, supporting the versatile application of EVs in cancer therapies. This simple, yet efficient and versatile method for the stable surface modification of EVs bypasses the need for genetic and chemical modifications, thus facilitating safe and specific delivery of therapeutic payloads to target cells.
机译:天然细胞外囊(EVS)是理想的药物载体,因为它们显着的生物相容性。通过靶向配体的共轭可以实现它们的递送特异性。然而,工程师目标特定的EVS的现有方法是乏味的或效率低下,在苛刻的化学处理和瞬态相互作用之间不得妥协。这里,我们描述了使用蛋白质连接酶的高拷贝数的EV的共价缀合的新方法。 EVS与表皮生长因子受体(EGFR)的缀合 - 可诱导肽或抗EGFR纳米体促进其在体外和体内的EGFR阳性癌细胞中的积累。 EGFR靶向EVS以低剂量的靶向EVS的全身递送显着增加了EGFR阳性肺癌的异种小鼠模型中的药物效力。该方法还适用于EV的肽与靶向其他受体的肽和纳米级,例如HER2和SIRPα,并且缀合的EV可以除了小分子外,还可递送RNA,支持EVS在癌症治疗中的通用应用。这种简单但高效且通用的方法对于EVS的稳定表面改性绕过遗传和化学修饰的需要,从而促进了对靶细胞的治疗性有效载荷的安全和特异性递送。
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