ApTOLL: A new therapeutic aptamer for cytoprotection and (re)myelination after multiple sclerosis

Author:

Fernández‐Gómez Beatriz123,Marchena Miguel A.145,Piñeiro David2,Gómez‐Martín Paula1,Sánchez Estefanía1,Laó Yolanda1,Valencia Gloria1,Nocera Sonia1,Benítez‐Fernández Rocío1,Castaño‐León Ana M.6,Lagares Alfonso6,Hernández‐Jiménez Macarena27,de Castro Fernando1ORCID

Affiliation:

1. Instituto Cajal—CSIC Madrid Spain

2. AptaTargets SL Madrid Spain

3. PhD Program in Neuroscience Universidad Autónoma de Madrid—Cajal Institute Madrid Spain

4. Facultad HM de Ciencias de la Salud de la Universidad Camilo José Cela

5. Instituto de Investigación Sanitaria HM Hospitales

6. Servicio de Neurocirugía Hospital 12 de Octubre Madrid Spain

7. Unidad de Investigación Neurovascular, Departamento de Farmacología y Toxicología, Facultad de Medicina Universidad Complutense de Madrid Madrid Spain

Abstract

AbstractBackground and PurposeApTOLL is an aptamer selected to antagonize toll‐like receptor 4 (TLR4), a relevant actor for innate immunity involved in inflammatory responses in multiple sclerosis (MS) and other diseases. The currently available therapeutic arsenal to treat MS is composed of immunomodulators but, to date, there are no (re)myelinating drugs available in clinics. In our present study, we studied the effect of ApTOLL on different animal models of MS.Experimental ApproachThe experimental autoimmune encephalomyelitis (EAE) model was used to evaluate the effect of ApTOLL on reducing the inflammatory component. A more direct effect on oligodendroglia was studied with the cuprizone model and purified primary cultures of murine and human oligodendrocyte precursor cells (OPCs) isolated through magnetic‐activated cell sorting (MACS) from samples of brain cortex. Also, we tested these effects in an ex vivo model of organotypic cultures demyelinated with lysolecithin (LPC).Key ResultsApTOLL treatment positively impacted the clinical symptomatology of mice in the EAE and cuprizone models, which was associated with better preservation plus restoration of myelin and oligodendrocytes in the demyelinated lesions of animals. Restoration was corroborated on purified cultures of rodent and human OPCs.Conclusion and ImplicationsOur findings reveal a new therapeutic approach for the treatment of inflammatory and demyelinating diseases such as MS. The molecular nature of the aptamer exerts not only an anti‐inflammatory effect but also neuroprotective and remyelinating effects. The excellent safety profile demonstrated by ApTOLL in animals and humans opens the door to future clinical trials in MS patients.

Funder

Ministerio de Ciencia e Innovación

Comunidad de Madrid

Consejo Superior de Investigaciones Científicas

Publisher

Wiley

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