Статья

First‐in‐human clinical trial of allogeneic, platelet‐derived extracellular vesicles as a potential therapeutic for delayed wound healing

Jancy JohnsonDepartment of Biochemistry and Pharmacology University of Melbourne Parkville VIC AustraliaSam Q. K. LawExopharm Ltd Melbourne VIC AustraliaMozhgan ShojaeeExopharm Ltd Melbourne VIC AustraliaA. HallExopharm Ltd Melbourne VIC AustraliaSadman BhuiyanExopharm Ltd Melbourne VIC AustraliaMelissa B. L. LimExopharm Ltd Melbourne VIC AustraliaAnabel SilvaExopharm Ltd Melbourne VIC AustraliaKarmen J. W. KongExopharm Ltd Melbourne VIC AustraliaMelanie SchoppetExopharm Ltd Melbourne VIC AustraliaChantelle BlythExopharm Ltd Melbourne VIC AustraliaHansi N. RanasingheExopharm Ltd Melbourne VIC AustraliaNenad SejicExopharm Ltd Melbourne VIC AustraliaMun Joo ChueiExopharm Ltd Melbourne VIC AustraliaOwen C. TatfordExopharm Ltd Melbourne VIC AustraliaAnna Cifuentes‐RiusExopharm Ltd Melbourne VIC AustraliaPatrick F. JamesExopharm Ltd Melbourne VIC AustraliaAngus M. TesterExopharm Ltd Melbourne VIC AustraliaIan DixonExopharm Ltd Melbourne VIC AustraliaGregor F. LichtfussDepartment of Biochemistry and Pharmacology University of Melbourne Parkville VIC Australia

2023en

ABI

Аннотация

The release of growth factors, cytokines and extracellular matrix modifiers by activated platelets is an important step in the process of healthy wound healing. Extracellular vesicles (EVs) released by activated platelets carry this bioactive cargo in an enriched form, and may therefore represent a potential therapeutic for the treatment of delayed wound healing, such as chronic wounds. While EVs show great promise in regenerative medicine, their production at clinical scale remains a critical challenge and their tolerability in humans is still to be fully established. In this work, we demonstrate that Ligand-based Exosome Affinity Purification (LEAP) chromatography can successfully isolate platelet EVs (pEVs) of clinical grade from activated platelets, which retain the regenerative properties of the parent cell. LEAP-isolated pEVs display the expected biophysical features of EV populations and transport essential proteins in wound healing processes, including insulin growth factor (IGF) and transforming growth factor beta (TGF-ß). In vitro studies show that pEVs induce proliferation and migration of dermal fibroblasts and increase dermal endothelial cells' angiogenic potential, demonstrating their wound healing potential. pEV treatment activates the ERK and Akt signalling pathways within recipient cells. In a first-in-human, double-blind, placebo-controlled, phase I clinical trial of healthy volunteer adults, designed primarily to assess safety in the context of wound healing, we demonstrate that injections of LEAP-purified pEVs in formulation buffer are safe and well tolerated (Plexoval II study, ACTRN12620000944932). As a secondary objective, biological activity in the context of wound healing rate was assessed. In this cohort of healthy participants, in which the wound bed would not be expected to be deficient in the bioactive cargo that pEVs carry, all wounds healed rapidly and completely and no difference in time to wound closure of the treated and untreated wounds was observed at the single dose tested. The outcomes of this study evidence that pEVs manufactured through the LEAP process can be injected safely in humans as a potential wound healing treatment, and warrant further study in clinical trials designed expressly to assess therapeutic efficacy in patients with delayed or disrupted wound healing.

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Идентификаторы

DOI: 10.1002/jev2.12332

Цитирования и источники

Цитирований: 2Использованных источников: 0

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