Decellularized Biohybrid Nerve Promotes Motor Axon Projections

Author:

Mehta Abijeet Singh1ORCID,Zhang Sophia L.2345,Xie Xinran1,Khanna Shreyaa2,Tropp Joshua1ORCID,Ji Xudong1,Daso Rachel E.1ORCID,Franz Colin K.267ORCID,Jordan Sumannas W.23,Rivnay Jonathan1ORCID

Affiliation:

1. Department of Biomedical Engineering Northwestern University Evanston IL 60208 USA

2. Biologics Laboratory Shirley Ryan Ability Lab Chicago IL 60611 USA

3. Division of Plastic Surgery Feinberg School of Medicine Northwestern University 420 E Superior St. Chicago IL 60611 USA

4. Section for Injury Repair and Regeneration Research Stanley Manne Children's Research Institute Ann & Robert H. Lurie Children's Hospital of Chicago Chicago IL 60611 USA

5. Department of Pediatrics Division of Critical Care Northwestern University Feinberg School of Medicine Chicago IL 60611 USA

6. Physical Medicine and Rehabilitation Northwestern University Feinberg School of Medicine Chicago IL 60611 USA

7. Ken & Ruth Davee Department of Neurology Northwestern University Feinberg School of Medicine Chicago IL 60611 USA

Abstract

AbstractDeveloping nerve grafts with intact mesostructures, superior conductivity, minimal immunogenicity, and improved tissue integration is essential for the treatment and restoration of neurological dysfunctions. A key factor is promoting directed axon growth into the grafts. To achieve this, biohybrid nerves are developed using decellularized rat sciatic nerve modified by in situ polymerization of poly(3,4‐ethylenedioxythiophene) (PEDOT). Nine biohybrid nerves are compared with varying polymerization conditions and cycles, selecting the best candidate through material characterization. These results show that a 1:1 ratio of FeCl3 oxidant to ethylenedioxythiophene (EDOT) monomer, cycled twice, provides superior conductivity (>0.2 mS cm−1), mechanical alignment, intact mesostructures, and high compatibility with cells and blood. To test the biohybrid nerve's effectiveness in promoting motor axon growth, human Spinal Cord Spheroids (hSCSs) derived from HUES 3 Hb9:GFP cells are used, with motor axons labeled with green fluorescent protein (GFP). Seeding hSCS onto one end of the conduit allows motor axon outgrowth into the biohybrid nerve. The construct effectively promotes directed motor axon growth, which improves significantly after seeding the grafts with Schwann cells. This study presents a promising approach for reconstructing axonal tracts in humans.

Funder

Materials Research Science and Engineering Center, Harvard University

Office of Naval Research Global

Division of Electrical, Communications and Cyber Systems

Publisher

Wiley

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