A bioengineered peripheral nerve construct using aligned peptide amphiphile nanofibers

Andrew Li; Akishige Hokugo; Anisa Yalom; Eric J. Berns; Nicholas Stephanopoulos; Mark T. McClendon; Luis A. Segovia; Igor Spigelman; Samuel I. Stupp; Reza Jarrahy

doi:10.1016/j.biomaterials.2014.06.049

A bioengineered peripheral nerve construct using aligned peptide amphiphile nanofibers

Andrew Li, Akishige Hokugo, Anisa Yalom, Eric J. Berns, Nicholas Stephanopoulos, Mark T. McClendon, Luis A. Segovia, Igor Spigelman, Samuel I. Stupp, Reza Jarrahy

Research output: Contribution to journal › Article › peer-review

114 Scopus citations

Abstract

Peripheral nerve injuries can result in lifelong disability. Primary coaptation is the treatment of choice when the gap between transected nerve ends is short. Long nerve gaps seen in more complex injuries often require autologous nerve grafts or nerve conduits implemented into the repair. Nerve grafts, however, cause morbidity and functional loss at donor sites, which are limited in number. Nerve conduits, in turn, lack an internal scaffold to support and guide axonal regeneration, resulting in decreased efficacy over longer nerve gap lengths. By comparison, peptide amphiphiles (PAs) are molecules that can self-assemble into nanofibers, which can be aligned to mimic the native architecture of peripheral nerve. As such, they represent a potential substrate for use in a bioengineered nerve graft substitute. To examine this, we cultured Schwann cells with bioactive PAs (RGDS-PA, IKVAV-PA) to determine their ability to attach to and proliferate within the biomaterial. Next, we devised a PA construct for use in a peripheral nerve critical sized defect model. Rat sciatic nerve defects were created and reconstructed with autologous nerve, PLGA conduits filled with various forms of aligned PAs, or left unrepaired. Motor and sensory recovery were determined and compared among groups. Our results demonstrate that Schwann cells are able to adhere to and proliferate in aligned PA gels, with greater efficacy in bioactive PAs compared to the backbone-PA alone. In vivo testing revealed recovery of motor and sensory function in animals treated with conduit/PA constructs comparable to animals treated with autologous nerve grafts. Functional recovery in conduit/PA and autologous graft groups was significantly faster than in animals treated with empty PLGA conduits. Histological examinations also demonstrated increased axonal and Schwann cell regeneration within the reconstructed nerve gap in animals treated with conduit/PA constructs. These results indicate that PA nanofibers may represent a promising biomaterial for use in bioengineered peripheral nerve repair.

Original language	English (US)
Pages (from-to)	8780-8790
Number of pages	11
Journal	Biomaterials
Volume	35
Issue number	31
DOIs	https://doi.org/10.1016/j.biomaterials.2014.06.049
State	Published - Oct 2014
Externally published	Yes

Keywords

Alignment
Nanofiber
Nerve conduit
Peptide amphiphile
Peripheral nerve repair
Self assembly

ASJC Scopus subject areas

Mechanics of Materials
Ceramics and Composites
Bioengineering
Biophysics
Biomaterials

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10.1016/j.biomaterials.2014.06.049

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@article{2b8ecf42c3164a50ab186462595f2a06,

title = "A bioengineered peripheral nerve construct using aligned peptide amphiphile nanofibers",

abstract = "Peripheral nerve injuries can result in lifelong disability. Primary coaptation is the treatment of choice when the gap between transected nerve ends is short. Long nerve gaps seen in more complex injuries often require autologous nerve grafts or nerve conduits implemented into the repair. Nerve grafts, however, cause morbidity and functional loss at donor sites, which are limited in number. Nerve conduits, in turn, lack an internal scaffold to support and guide axonal regeneration, resulting in decreased efficacy over longer nerve gap lengths. By comparison, peptide amphiphiles (PAs) are molecules that can self-assemble into nanofibers, which can be aligned to mimic the native architecture of peripheral nerve. As such, they represent a potential substrate for use in a bioengineered nerve graft substitute. To examine this, we cultured Schwann cells with bioactive PAs (RGDS-PA, IKVAV-PA) to determine their ability to attach to and proliferate within the biomaterial. Next, we devised a PA construct for use in a peripheral nerve critical sized defect model. Rat sciatic nerve defects were created and reconstructed with autologous nerve, PLGA conduits filled with various forms of aligned PAs, or left unrepaired. Motor and sensory recovery were determined and compared among groups. Our results demonstrate that Schwann cells are able to adhere to and proliferate in aligned PA gels, with greater efficacy in bioactive PAs compared to the backbone-PA alone. In vivo testing revealed recovery of motor and sensory function in animals treated with conduit/PA constructs comparable to animals treated with autologous nerve grafts. Functional recovery in conduit/PA and autologous graft groups was significantly faster than in animals treated with empty PLGA conduits. Histological examinations also demonstrated increased axonal and Schwann cell regeneration within the reconstructed nerve gap in animals treated with conduit/PA constructs. These results indicate that PA nanofibers may represent a promising biomaterial for use in bioengineered peripheral nerve repair.",

keywords = "Alignment, Nanofiber, Nerve conduit, Peptide amphiphile, Peripheral nerve repair, Self assembly",

author = "Andrew Li and Akishige Hokugo and Anisa Yalom and Berns, {Eric J.} and Nicholas Stephanopoulos and McClendon, {Mark T.} and Segovia, {Luis A.} and Igor Spigelman and Stupp, {Samuel I.} and Reza Jarrahy",

note = "Funding Information: The authors are especially grateful for technical support and assistance for behavior tests from Dr. Yatendra Mulpuri, Division of Oral Biology and Medicine, UCLA School of Dentistry. This work was generously supported by the Annenberg Fund for Craniofacial Surgery and Research at UCLA. This project was also supported by National Institutes of Health/National Institute Of Biomedical Imaging And Bioengineering Award Number 5 R01EB003806-09 and the National Institute of Dental and Craniofacial Research Award Number 5R01DE015920-08 . We acknowledge the following Northwestern University facilities: IBNAM Peptide Core, IBNAM Equipment Core, and Electron Probe Instrumentation Center (EPIC). Portions of this work were performed at the DuPont-Northwestern-Dow Collaborative Access Team (DND-CAT) located at Sector 5 of the Advanced Photon Source (APS). DND-CAT is supported by E.I. DuPont de Nemours & Co., The Dow Chemical Company and Northwestern University. Use of the APS, an Office of Science User Facility operated for the U.S. Department of Energy (DOE) Office of Science by Argonne National Laboratory, was supported by the U.S. DOE under Contract No. DE-AC02-06CH11357. ",

year = "2014",

month = oct,

doi = "10.1016/j.biomaterials.2014.06.049",

language = "English (US)",

volume = "35",

pages = "8780--8790",

journal = "Biomaterials",

issn = "0142-9612",

publisher = "Elsevier BV",

number = "31",

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T1 - A bioengineered peripheral nerve construct using aligned peptide amphiphile nanofibers

AU - Li, Andrew

AU - Hokugo, Akishige

AU - Yalom, Anisa

AU - Berns, Eric J.

AU - Stephanopoulos, Nicholas

AU - McClendon, Mark T.

AU - Segovia, Luis A.

AU - Spigelman, Igor

AU - Stupp, Samuel I.

AU - Jarrahy, Reza

N1 - Funding Information: The authors are especially grateful for technical support and assistance for behavior tests from Dr. Yatendra Mulpuri, Division of Oral Biology and Medicine, UCLA School of Dentistry. This work was generously supported by the Annenberg Fund for Craniofacial Surgery and Research at UCLA. This project was also supported by National Institutes of Health/National Institute Of Biomedical Imaging And Bioengineering Award Number 5 R01EB003806-09 and the National Institute of Dental and Craniofacial Research Award Number 5R01DE015920-08 . We acknowledge the following Northwestern University facilities: IBNAM Peptide Core, IBNAM Equipment Core, and Electron Probe Instrumentation Center (EPIC). Portions of this work were performed at the DuPont-Northwestern-Dow Collaborative Access Team (DND-CAT) located at Sector 5 of the Advanced Photon Source (APS). DND-CAT is supported by E.I. DuPont de Nemours & Co., The Dow Chemical Company and Northwestern University. Use of the APS, an Office of Science User Facility operated for the U.S. Department of Energy (DOE) Office of Science by Argonne National Laboratory, was supported by the U.S. DOE under Contract No. DE-AC02-06CH11357.

PY - 2014/10

Y1 - 2014/10

N2 - Peripheral nerve injuries can result in lifelong disability. Primary coaptation is the treatment of choice when the gap between transected nerve ends is short. Long nerve gaps seen in more complex injuries often require autologous nerve grafts or nerve conduits implemented into the repair. Nerve grafts, however, cause morbidity and functional loss at donor sites, which are limited in number. Nerve conduits, in turn, lack an internal scaffold to support and guide axonal regeneration, resulting in decreased efficacy over longer nerve gap lengths. By comparison, peptide amphiphiles (PAs) are molecules that can self-assemble into nanofibers, which can be aligned to mimic the native architecture of peripheral nerve. As such, they represent a potential substrate for use in a bioengineered nerve graft substitute. To examine this, we cultured Schwann cells with bioactive PAs (RGDS-PA, IKVAV-PA) to determine their ability to attach to and proliferate within the biomaterial. Next, we devised a PA construct for use in a peripheral nerve critical sized defect model. Rat sciatic nerve defects were created and reconstructed with autologous nerve, PLGA conduits filled with various forms of aligned PAs, or left unrepaired. Motor and sensory recovery were determined and compared among groups. Our results demonstrate that Schwann cells are able to adhere to and proliferate in aligned PA gels, with greater efficacy in bioactive PAs compared to the backbone-PA alone. In vivo testing revealed recovery of motor and sensory function in animals treated with conduit/PA constructs comparable to animals treated with autologous nerve grafts. Functional recovery in conduit/PA and autologous graft groups was significantly faster than in animals treated with empty PLGA conduits. Histological examinations also demonstrated increased axonal and Schwann cell regeneration within the reconstructed nerve gap in animals treated with conduit/PA constructs. These results indicate that PA nanofibers may represent a promising biomaterial for use in bioengineered peripheral nerve repair.

AB - Peripheral nerve injuries can result in lifelong disability. Primary coaptation is the treatment of choice when the gap between transected nerve ends is short. Long nerve gaps seen in more complex injuries often require autologous nerve grafts or nerve conduits implemented into the repair. Nerve grafts, however, cause morbidity and functional loss at donor sites, which are limited in number. Nerve conduits, in turn, lack an internal scaffold to support and guide axonal regeneration, resulting in decreased efficacy over longer nerve gap lengths. By comparison, peptide amphiphiles (PAs) are molecules that can self-assemble into nanofibers, which can be aligned to mimic the native architecture of peripheral nerve. As such, they represent a potential substrate for use in a bioengineered nerve graft substitute. To examine this, we cultured Schwann cells with bioactive PAs (RGDS-PA, IKVAV-PA) to determine their ability to attach to and proliferate within the biomaterial. Next, we devised a PA construct for use in a peripheral nerve critical sized defect model. Rat sciatic nerve defects were created and reconstructed with autologous nerve, PLGA conduits filled with various forms of aligned PAs, or left unrepaired. Motor and sensory recovery were determined and compared among groups. Our results demonstrate that Schwann cells are able to adhere to and proliferate in aligned PA gels, with greater efficacy in bioactive PAs compared to the backbone-PA alone. In vivo testing revealed recovery of motor and sensory function in animals treated with conduit/PA constructs comparable to animals treated with autologous nerve grafts. Functional recovery in conduit/PA and autologous graft groups was significantly faster than in animals treated with empty PLGA conduits. Histological examinations also demonstrated increased axonal and Schwann cell regeneration within the reconstructed nerve gap in animals treated with conduit/PA constructs. These results indicate that PA nanofibers may represent a promising biomaterial for use in bioengineered peripheral nerve repair.

KW - Alignment

KW - Nanofiber

KW - Nerve conduit

KW - Peptide amphiphile

KW - Peripheral nerve repair

KW - Self assembly

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JO - Biomaterials

JF - Biomaterials

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ER -

A bioengineered peripheral nerve construct using aligned peptide amphiphile nanofibers

Abstract

Keywords

ASJC Scopus subject areas

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