Camouflage strategies for therapeutic exosomes evasion from phagocytosis

Nicol Parada; Alfonso Romero-Trujillo; Nicolás Georges; Francisca Alcayaga-Miranda

doi:10.1016/j.jare.2021.01.001

Camouflage strategies for therapeutic exosomes evasion from phagocytosis

J Adv Res. 2021 Jan 8:31:61-74. doi: 10.1016/j.jare.2021.01.001. eCollection 2021 Jul.

Authors

Nicol Parada^{1

2}, Alfonso Romero-Trujillo^{1

2}, Nicolás Georges^{1

2}, Francisca Alcayaga-Miranda^{1

2

3

4}

Affiliations

¹ School of Medicine, Faculty of Medicine, Universidad de los Andes, Santiago, Chile.
² Laboratory of Nano-Regenerative Medicine, Centro de Investigación e Innovación Biomédica (CIIB), Faculty of Medicine, Universidad de los Andes, Santiago, Chile.
³ Cells for Cells, Santiago, Chile.
⁴ Consorcio Regenero, Chilean Consortium for Regenerative Medicine, Santiago, Chile.

Abstract

Background: Even though exosome-based therapy has been shown to be able to control the progression of different pathologies, the data revealed by pharmacokinetic studies warn of the low residence time of exogenous exosomes in circulation that can hinder the clinical translation of therapeutic exosomes. The macrophages related to the organs of the mononuclear phagocytic system are responsible primarily for the rapid clearance and retention of exosomes, which strongly limits the amount of exosomal particles available to reach the target tissue, accumulate in it and release with high efficiency its therapeutic cargo in acceptor target cells to exert the desired biological effect.

Aim of review: Endowing exosomes with surface modifications to evade the immune system is a plausible strategy to contribute to the suppression of exosomal clearance and increase the efficiency of their targeted content delivery. Here, we summarize the current evidence about the mechanisms underlying the recognition and sequestration of therapeutic exosomes by phagocytic cells. Also, we propose different strategies to generate 'invisible' exosomes for the immune system, through the incorporation of different anti-phagocytic molecules on the exosomes' surface that allow increasing the circulating half-life of therapeutic exosomes with the purpose to increase their bioavailability to reach the target tissue, transfer their therapeutic molecular cargo and improve their efficacy profile.

Key scientific concepts of review: Macrophage-mediated phagocytosis are the main responsible behind the short half-life in circulation of systemically injected exosomes, hindering their therapeutic effect. Exosomes 'Camouflage Cloak' strategy using antiphagocytic molecules can contribute to the inhibition of exosomal clearance, hence, increasing the on-target effect. Some candidate molecules that could exert an antiphagocytic role are CD47, CD24, CD44, CD31, β2M, PD-L1, App1, and DHMEQ. Pre- and post-isolation methods for exosome engineering are compatible with the loading of therapeutic cargo and the expression of antiphagocytic surface molecules.

Keywords: Biodistribution and pharmacokinetics; Drug delivery; Evasion immune system; Evasion phagocytosis; Exosomes; Small extracellular vesicles.

Publication types

Research Support, Non-U.S. Gov't
Review

MeSH terms

B7-H1 Antigen / metabolism
Biological Availability
Biological Mimicry*
CD24 Antigen / metabolism
CD47 Antigen / metabolism
Drug Delivery Systems / methods*
Exosomes / immunology
Exosomes / metabolism*
Humans
Hyaluronan Receptors / metabolism
Immune System
Macrophages / immunology
Macrophages / metabolism
Mononuclear Phagocyte System / metabolism
Phagocytes / immunology
Phagocytes / metabolism
Phagocytosis*

Substances

B7-H1 Antigen
CD24 Antigen
CD47 Antigen
Hyaluronan Receptors