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ABSTRACT: Statement of significance
Although biomaterials comprising full-length recombinant human collagen and extracted animal collagen have been evaluated and used clinically, these macromolecules provide only a limited number of functional groups amenable to chemical modification or crosslinking and are demanding to process. Synthetic, customizable analogs that are functionally equivalent, and can be readily scaled-up are therefore very desirable for pre-clinical to clinical translation. Here, we demonstrate, using cornea regeneration as our test bed, that collagen-like-peptides conjugated to multifunctional polyethylene glycol (CLP-PEG) when grafted into mini-pigs as corneal implants were functionally equivalent to recombinant human collagen-based implants that were successfully tested in patients. We also show for the first time that these materials affected regeneration through stimulation of extracellular vesicle production by endogenous host cells that have migrated into the CLP-PEG scaffolds.
SUBMITTER: Jangamreddy JR
PROVIDER: S-EPMC5842042 | biostudies-literature | 2018 Mar
REPOSITORIES: biostudies-literature
Jangamreddy Jaganmohan R JR Haagdorens Michel K C MKC Mirazul Islam M M Lewis Philip P Samanta Ayan A Fagerholm Per P Liszka Aneta A Ljunggren Monika K MK Buznyk Oleksiy O Alarcon Emilio I EI Zakaria Nadia N Meek Keith M KM Griffith May M
Acta biomaterialia 20180131
Short collagen-like peptides (CLPs) are being proposed as alternatives to full-length collagen for use in tissue engineering, on their own as soft hydrogels, or conjugated to synthetic polymer for mechanical strength. However, despite intended clinical use, little is known about their safety and efficacy, mechanism of action or degree of similarity to the full-length counterparts they mimic. Here, we show the functional equivalence of a CLP conjugated to polyethylene glycol (CLP-PEG) to full-len ...[more]