| Literature DB >> 34054331 |
Zain Siddiqui1, Biplab Sarkar1, Ka Kyung Kim1, Arjun Kumar1, Reshma Paul1, Aryan Mahajan1, Jonathan M Grasman1, Jian Yang2, Vivek A Kumar1,3,4.
Abstract
One of the major constraints against using polymeric scaffolds as tissue-regenerative matrices is a lack of adequate implant vascularization. Self-assembling peptide hydrogels can sequester small molecules and biological macromolecules, and they can support infiltrating cells in vivo. Here we demonstrate the ability of self-assembling peptide hydrogels to facilitate angiogenic sprouting into polymeric scaffolds after subcutaneous implantation. We constructed two-component scaffolds that incorporated microporous polymeric scaffolds and viscoelastic nanoporous peptide hydrogels. Nanofibrous hydrogels modified the biocompatibility and vascular integration of polymeric scaffolds with microscopic pores (pore diameters: 100-250 μm). In spite of similar amphiphilic sequences, charges, secondary structures, and supramolecular nanostructures, two soft hydrogels studied herein had different abilities to aid implant vascularization, but had similar levels of cellular infiltration. The functional difference of the peptide hydrogels was predicted by the difference in the bioactive moieties inserted into the primary sequences of the peptide monomers. Our study highlights the utility of soft supramolecular hydrogels to facilitate host-implant integration and control implant vascularization in biodegradable polyester scaffolds in vivo. Our study provides useful tools in designing multi-component regenerative scaffolds that recapitulate vascularized architectures of native tissues.Entities:
Keywords: acellular scaffolds; angiogenesis; hydrogel; implant vascularization; multi-functional scaffolds; peptide nanofibers; self-assembly; tissue regeneration
Year: 2021 PMID: 34054331 PMCID: PMC8158327 DOI: 10.1016/j.cej.2021.130145
Source DB: PubMed Journal: Chem Eng J ISSN: 1385-8947 Impact factor: 16.744