<i>In situ</i>crosslinkable elastomeric hydrogel for long-term cell encapsulation for cardiac applications

Komeri, Remya; Jayabalan, M.

doi:10.1002/jbm.a.35833

Cited by 7 publications

(5 citation statements)

References 30 publications

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“…The initiator system candidates we screened were fabricated relative to the control TEMED gel (41 mM, 1 NR x ). This initial concentration was determined by averaging previously reported TEMED concentrations in the literature. − The concentration of APS was kept constant at 25 mM under all conditions. Each TEMED molecule displays two amine groups; therefore, the TEMED 1 NR x control gel, containing 41 mM TEMED, contains twice the amount of amine groups (82 mM).…”

Section: Methodsmentioning

confidence: 99%

Nontoxic Initiator Alternatives to TEMED for Redox Hydrogel Polymerization

Pumford,

Jackson Hoffman,

Kasko

2024

ACS Appl. Bio Mater.

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Polymeric hydrogels are versatile biomaterials, offering unique advantages in tunability and biocompatibility that make them well-suited to a range of applications. Cross-linking, a fundamental step in hydrogel fabrication, is often initiated using a toxic redox system, ammonium persulfate (APS), and tetramethylethylenediamine (TEMED), which hinders hydrogel utility in direct contact with cells (e.g., wound dressings). To overcome this limitation, we developed alternative redox gelation systems that serve as nontoxic replacements for TEMED. The alternate initiators were either synthetic or bioinspired amine-containing polymers, Glycofect and polyethylenimine (PEI). Used with APS, these initiator candidates produced hydrogels with short gelation time and comparable moduli to TEMED-based gels and underwent further mechanical testing and biocompatibility characterization. While achieving mechanical properties similar to those of the control, the gels based on Glycofect and PEI outperformed TEMEDbased gels in two cell viability studies, with Glycofect-initiated gels displaying significantly higher cytocompatibility. Taken together, these results indicate that Glycofect may serve as a drop-in replacement for TEMED to fabricate hydrogels with improved biocompatibility.

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Section: Methodsmentioning

confidence: 99%

Nontoxic Initiator Alternatives to TEMED for Redox Hydrogel Polymerization

Pumford,

Jackson Hoffman,

Kasko

2024

ACS Appl. Bio Mater.

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“…Thus, reactions with higher FA ratios required longer reaction times. It is worth to mention that, in clear contrast with the method published for synthesis of linear poly(fumarate-co-PEG-co-sebacate) s, 32,33 metallic catalysts were not required herein. Furthermore, the use of TsOH simplifies the purification of polymers and post-process operations since de catalyst is easily removed during the washing steps with ethanol/ water mixtures.…”

Section: Synthesis Of Polyestersmentioning

confidence: 99%

“…The properties and the behavior of these materials as elution systems for Cephalexin and Progesterone, as model hydrophilic and hydrophobic drugs, are also explored. It should be mentioned that although some few examples of fumarate-co-PEG-co-sebacate copolymers have been published, [31][32][33] these precursors were only employed to obtain hydrogels using high MW PEGs, and that their use for the preparation of films by light triggered reactions at the level of FA groups have so far not been explored.…”

Section: Introductionmentioning

confidence: 99%

Fumarate‐co‐PEG‐co‐sebacate photopolymer and its evaluation as a drug release system

Vaillard

Trentino

Navarro

et al. 2022

Journal of Polymer Science

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Fumarate-co-PEG-co-sebacates with different fumaric/sebacic acid ratios are prepared by a simple thermal polycondensation reaction using p-toluensulfonic acid as catalyst. These polymeric precursors are purified by washing with an appropriate organic solvent and the dried materials were photocured to yield elastic films under mild conditions. The properties of polymeric precursors and elastic materials are studied in detail and correlated with fumaric acid/sebacic acid ratios used in the thermal esterification reactions. It is shown that a higher amount of sebacic in the starting polymer leads to softer final film materials, with lower Tg and G' values, which also show higher degradation rates in vitro. Finally, the films are also evaluated as drug release carriers for in vitro release of Cephalexin and Progesterone. The results obtained in these studies indicate that the careful tailoring of the fumaric acid/sebacic acid ratio in the esterification reaction allows to finely tune the thermal, mechanical a degradation properties of the final cross-linked elastic films.

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“…One of the aspects of current research on injectable hydrogels for transporting cells is to design a hydrogel that is more compatible with cells (Lovett et al, 2009). A polyethylene glycol (PEG) PEGylated fibrin proposed by Geuss et al (2015) and an injectable hydrogel combained poly (propylene fumarate-co-sebacate-coethylene glycol) with PEGDA designed by Komeri and Muthu (2016) are also suitable for cardiomyocytes. In addition, hydrogel for CVDs should be electrically conductive to generate electrical signals to the myocardium (Sepantafar et al, 2016).…”

Section: Stem Cellsmentioning

confidence: 99%

Injectable Hydrogel-Based Nanocomposites for Cardiovascular Diseases

Liao

Yang

Deng

et al. 2020

Front. Bioeng. Biotechnol.

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Cardiovascular diseases (CVDs), including a series of pathological disorders, severely affect millions of people all over the world. To address this issue, several potential therapies have been developed for treating CVDs, including injectable hydrogels as a minimally invasive method. However, the utilization of injectable hydrogel is a bit restricted recently owing to some limitations, such as transporting the therapeutic agent more accurately to the target site and prolonging their retention locally. This review focuses on the advances in injectable hydrogels for CVD, detailing the types of injectable hydrogels (natural or synthetic), especially that complexed with stem cells, cytokines, nano-chemical particles, exosomes, genetic material including DNA or RNA, etc. Moreover, we summarized the mainly prominent mechanism, based on which injectable hydrogel present excellent treating effect of cardiovascular repair. All in all, it is hopefully that injectable hydrogel-based nanocomposites would be a potential candidate through cardiac repair in CVDs treatment.

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In situcrosslinkable elastomeric hydrogel for long-term cell encapsulation for cardiac applications

Cited by 7 publications

References 30 publications

Nontoxic Initiator Alternatives to TEMED for Redox Hydrogel Polymerization

Nontoxic Initiator Alternatives to TEMED for Redox Hydrogel Polymerization

Fumarate‐co‐PEG‐co‐sebacate photopolymer and its evaluation as a drug release system

Injectable Hydrogel-Based Nanocomposites for Cardiovascular Diseases

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