18.2.3 Hydrogels Based on Zwitterionic Polymers
Zwitterionic polymers can mimic cell membranes and can be an ideal candidate to en
gineer biomaterials able to avert hostile interactions with biological cells. Sulfobetaine/
carbobetaine/phosphobetaine polyelectrolytes are highly biocompatible, encompassing
some natural analogs such as taurine, glycine betaine, etc. prospects in biomedical devices
and other such applications are being explored. Zwitterionic polymer is a special kind of
polymer that consists of both cationic and anionic groups on each monomer throughout
the polymeric backbone. Due to the presence of an equal number of anionic and cationic
groups in the polymeric backbone, they are highly hydrophilic and antifouling. They
interact with water via strong ion-dipole interaction and form a stable and dense hy
dration shell. Polyzwitterions can interact with water molecules via electrostatic inter
actions and the hydration layers around them can “distance” any other biomolecules
including protein. They are an ideal replacement for PEG. Their application as a drug
delivery vehicle has been recently reviewed [8].
Gels with a polyzwitterionic backbone were extensively reported. The potential use of
zwitterionic hydrogels is constrained by their poor mechanical strength. Mechanical
properties of non-fouling zwitterionic hydrogels were improved by substituting the
methacrylate backbone of sulfobetaine methacrylate (SBMA) by a vinyl imidazole back
bone (SBVI)]; the non-fouling characteristics of the zwitterionic sulfobetaine group were
retained while aiding on mechanical properties diffusion behavior of fluorescence-labeled
model proteins in PEG, polySBMA and mixed PEG-sulfobetaine methacrylate hydrogels
(SBMA:PEG 4:1, SBMA:PEG 1:4) was studied [9]. Four hydrogels showed varied diffusion
characteristics for either a negatively charged protein or positively charged protein de
pending on protein-polymer interaction and the labile water content available in the
hydrogel matrix.
Protein loading efficiency may increase as stronger interaction between protein-PEG is
observed than protein-polySBMA and controlled release is expected by changing the ratio
of PEG to SBMA in a hydrogel [10]. A narrowly dispersed zwitterionic poly(amido
amine) (PAA) nanogels tethered with N,Ndimethylethylenediamine having a positive
surface charge were developed for drug delivery and imaging. They showed excellent
stability in serum and minimal cytotoxicity. Stretchable tissue adhesive and antibacterial
hydrogels with zwitterionic monomers (strong dipole−dipole interaction, electrostatic
interaction, and hydrogen bonding with the skin surface) seem promising for wound
dressings and implantable devices. A polymer with phosphorylcholine (PC) and poly
(propylene glycol) (PPG) showed a steady release of insulin. On injecting the polymer
aqueous solution subcutaneously, a hydrogel was formed in the injection site and very
mild tissue responses around the injection site were observed. Overall, zwitterionic
polymer-based hydrogels possess remarkable characteristics such as being thermo
responsive, good cytocompatibility, anti-biofouling nature, controlled protein adsorption,
cell adhesiveness, implantable nature, and many more.
18.2.4 Ion Conductive Hydrogels
Hydrogels consist of free ions from ionic electrolytes usually exhibit higher conductivity
and found good application in bioelectronics applications. Ionic salts like NaCl, LiCl,
CaSO4, Na2SO4, etc. are generally added to hydrogels to make them ionically conductive.
The resulting ionic hydrogels exhibit greater ionic conductivity, higher stretchability, and
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