Innovations in Designing Hydrogels for Advanced Wound Dressing Applications: An Editorial Review
1. Introduction
2. Overview of the Papers Published in This Issue
2.1. Key Highlights from Research Articles
2.2. Insights from Review Articles
3. Common Research Limitations and Technological Challenges
- Biomimicry and structural integrity: Designing hydrogels that accurately mimic the native extracellular matrix (ECM) of the skin’s architecture and dynamic physiological functions remains a significant challenge. Ensuring the appropriate combination of flexibility and mechanical strength is crucial for the effective treatment of different types of wounds.
- Mechanical stability and durability: Many hydrogels exhibit insufficient mechanical strength and low stability, limiting their use in high-stress wound environments or for extended wear.
- Biocompatibility and immunogenicity: Ensuring high biocompatibility while minimizing immunogenicity and antigenicity is essential to prevent adverse host responses.
- Controlled and sustained drug delivery: Hydrogels must support the stable encapsulation and controlled release of diverse bioactive molecules (e.g., growth factors, antibiotics) at therapeutic concentrations. Delivering sub-therapeutic concentrations can contribute to the emergence of drug-resistant microbial strains.
- Antimicrobial resistance (AMR): The improper release of antimicrobial agents from hydrogels can inadvertently promote the emergence of resistant microbial populations within the treated wounds.
- Scalability and quality control: Maintaining consistency in physicochemical and biological properties during large-scale production remains a significant hurdle. Batch-to-batch variability can affect a product’s efficacy and regulatory approval.
- Environmental and ethical considerations: The sourcing of raw materials, use of animal-derived components, and environmental impact of manufacturing processes are growing concerns that must be addressed.
4. Impact and Relevance of the Special Issue Contributions
5. Conclusions and Future Perspectives
- The development of multifunctional hydrogels capable of the controlled and sequential release of multiple bioactive agents, such as antimicrobial, anti-inflammatory, and growth-promoting agents, to support the distinct phases of wound healing.
- The incorporation of natural multi-drug-resistant antibacterial agents, including bacteriophages, into hydrogel matrices which are designed for targeted, stimuli-responsive release triggered by microbial virulence factors, thereby minimizing disruption to the beneficial native microbiota.
- The design of biodegradable, self-healing hydrogels with minimal scar formation and enhanced mechanical durability, achieved through dynamic covalent or supramolecular interactions, enabling autonomous repair and prolonged in situ functionality.
- The incorporation of oxygen-generating compounds, such as calcium peroxide or manganese dioxide, into hydrogels to improve their oxygenation in hypoxic wound environments, thereby promoting angiogenesis, collagen deposition, and overall tissue regeneration.
- The engineering of anti-biofilm hydrogels incorporating quorum-sensing inhibitors and biofilm-disrupting agents to effectively combat chronic wound infections and facilitate accelerated healing.
Conflicts of Interest
References
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Narayanan, K.B.; Bhaskar, R. Innovations in Designing Hydrogels for Advanced Wound Dressing Applications: An Editorial Review. Gels 2025, 11, 332. https://doi.org/10.3390/gels11050332
Narayanan KB, Bhaskar R. Innovations in Designing Hydrogels for Advanced Wound Dressing Applications: An Editorial Review. Gels. 2025; 11(5):332. https://doi.org/10.3390/gels11050332
Chicago/Turabian StyleNarayanan, Kannan Badri, and Rakesh Bhaskar. 2025. "Innovations in Designing Hydrogels for Advanced Wound Dressing Applications: An Editorial Review" Gels 11, no. 5: 332. https://doi.org/10.3390/gels11050332
APA StyleNarayanan, K. B., & Bhaskar, R. (2025). Innovations in Designing Hydrogels for Advanced Wound Dressing Applications: An Editorial Review. Gels, 11(5), 332. https://doi.org/10.3390/gels11050332