Enhancing Infected Diabetic Wound Healing through Multifunctional Nanocomposite‐Loaded Microneedle Patch: Inducing Multiple Regenerative Sites

Enhancing Infected Diabetic Wound Healing through Multifunctional Nanocomposite‐Loaded Microneedle Patch: Inducing Multiple Regenerative Sites

Infected diabetic wound (DW) presents a prolonged and challenging healing process within the field of regenerative medicine. The effectiveness of conventional drug therapies is hindered by their limited ability to reach deep tissues and promote adequate wound healing rates. Therefore, there is an im...

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Veröffentlicht in:Advanced healthcare materials 2024-08, Vol.13 (20), p.e2301985-n/a
Hauptverfasser: Yu, Daojiang, Chen, Lei, Yan, Tao, Zhang, Yuanyuan, Sun, Xiaodong, Lv, Guozhong, Zhang, Shuyu, Xu, Yong, Li, Changlong
Format: Artikel
Sprache:eng
Schlagworte:
Angiogenesis
Cerium oxides
Core-shell structure
Diabetes
Diabetes mellitus
diabetic wound healing
Drug delivery
Drug delivery systems
Ecological niches
Macrophages
multifunctional microneedle
Nanocomposites
nanoparticle
Nanoparticles
Needles
Reactive oxygen species
Regeneration (physiology)
Regenerative medicine
regenerative sites
skin tissue engineering
System effectiveness
Tissue engineering
Wound healing
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Zusammenfassung:Infected diabetic wound (DW) presents a prolonged and challenging healing process within the field of regenerative medicine. The effectiveness of conventional drug therapies is hindered by their limited ability to reach deep tissues and promote adequate wound healing rates. Therefore, there is an imperative to develop drug delivery systems that can penetrate deep tissues while exhibiting multifunctional properties to expedite wound healing. In this study, w e devised a soluble microneedle (MN) patch made of γ‐PGA, featuring multiple arrays, which w as loaded with core‐shell structured nanoparticles (NPs) known as Ag@MSN@CeO2, to enhance the healing of infected DWs. The NP comprises a cerium dioxide (CeO2) core with anti‐inflammatory and antioxidant properties, a mesoporous silica NP (MSN) shell with angiogenic characteristics, and an outermost layer doped with Ag to combat bacterial infections. W e demonstrated that the MN platform loaded with Ag@MSN@CeO2 successfully penetrated deep tissues for effective drug delivery. These MN tips induced the formation of multiple regenerative sites at various points, leading to antibacterial, reactive oxygen species‐lowering, macrophage ecological niche‐regulating, vascular regeneration‐promoting, and collagen deposition‐promoting effects, thus significantly expediting the healing process of infected DWs. Considering these findings, the multifunctional MN@Ag@MSN@CeO2 patch exhibits substantial potential for clinical applications in the treatment of infected DW. A soluble microneedle patch made of γ‐PGA, loaded with core‐shell structured nanoparticles (Ag@MSN@CeO2), is developed to treat infected diabetic wounds. This patch effectively penetrates deep tissues, delivering antibacterial, anti‐inflammatory, and antioxidant properties while promoting vascular regeneration and collagen deposition, significantly enhancing wound healing. The multifunctional patch shows promise for clinical applications.
ISSN:2192-2640
2192-2659
2192-2659
DOI:10.1002/adhm.202301985