Poly(epsilon-caprolactone) with pendant natural peptides:
an old polymeric biomaterial with new properties
Ju, YY (Ju, Yuanyuan)[ 1 ] ; Zhang, MM (Zhang, Mingming)[ 2,3 ] ; Zhao, HY (Zhao, Hanying)[ 1 ]
POLYMER
CHEMISTRY, 2017, 8(35): 5415-5426
DOI: 10.1039/c7py01012e
WOS:000411268700018
Abstract
The
bio-functionalization of poly(epsilon-caprolactone) (P epsilon CL) provides an
approach to broaden the applications of the polymer in medical and biological
engineering fields. In this research, PeCL with pendant glutathione (GSH) or
L-carnosine was synthesized by a combination of ring-opening copolymerization,
Cu(I)-catalyzed Huisgen 1,3-dipolar cycloaddition reaction (click reaction) and
thiol-disulfide exchange reaction. The ring-opening copolymerization of epsilon
CL and a-chloro-epsilon-caprolactone (aCl-epsilon CL) was employed in the
synthesis of the PeCL-co-P(aCl-epsilon CL) copolymer. The pendent chlorides
were converted into azides by a reaction with sodium azide.
N-Hydroxysuccinimide (NHS) groups were introduced into the polymer backbones by
the click reaction. PeCL with pendant pyridyl disulfide groups was prepared by
a reaction of N-hydroxysuccinimide (NHS) activated ester and pyridine
dithioethylamine. Peptide modified P epsilon CL were synthesized by
thiol-disulfide exchange reactions between thiol groups on GSH (or
thiolmodified L-carnosine) and the pendant pyridyl disulfide groups on the
polymer chains. The synthesized copolymers were analyzed by size exclusion
chromatography, FTIR, H-1 NMR and differential scanning calorimetry. The bio-graft
copolymers are able to self-assemble into micelles or vesicles in aqueous
solutions, depending on the pH values of the solutions. The assembled
structures formed by the bio-graft copolymers in aqueous solutions are
essentially nontoxic toward MCF-7 and COS-7 cells. The functionalization of the
peptide-stabilized assembled structures with lysozyme was also investigated in
this research.
