Journal of Textile Research ›› 2026, Vol. 47 ›› Issue (03): 44-51.doi: 10.13475/j.fzxb.20250900401

• Biomedical Materials • Previous Articles     Next Articles

Short-fiber-reconstructed composite dressings integrating glycose-triggered bacterial resistance and exudate management and its performance

YANG Xiao1,2, ZHANG Yumo1,2, LI Yan1,2,3, WANG Lu1,2,3, WANG Fujun1,2,3()   

  1. 1 College of Textiles, Donghua University, Shanghai 201620, China
    2 Key Laboratory of Textiles Science & Technology, Ministry of Education, Donghua University, Shanghai 201620, China
    3 Shanghai Frontiers Science Center of Advanced Textiles, Donghua University, Shanghai 201620, China
  • Received:2025-09-01 Revised:2025-12-19 Online:2026-03-15 Published:2026-03-15
  • Contact: WANG Fujun E-mail:wfj@dhu.edu.cn

Abstract:

Objective Diabetic foot ulcers (DFUs) characteristically present a hyperglycaemic, alkaline, and highly exudative microenvironment that fosters recurrent infection and impedes healing. This work aims to construct a nanofiber composite dressing that couples antibiotic-free, glucose-triggered antibacterial activity with directional exudate management, thereby addressing both microbial control and moisture regulation at DFU wound beds within a single materials platform.

Method A bilayer architecture was designed comprising a hydrophobic polypropylene (PP) nonwoven substrate and a reconstructed hydrophilic top layer of short poly(vinylidene fluoride) (PVDF) fibers. Gold nanoparticles (Au NPs; glucose oxidase-like) and Fe-MIL-88NH2 metal-organic framework (MOF; peroxidase-like) nanozymes were immobilized on PVDF via a tannic-acid-based adhesive (TBA). Short-fiber dispersions were prepared by high-shear homogenization and spray-reassembled onto PP to establish a wettability gradient. Catalytic performance was verified by methyl-red pH transition and 3,3',5,5'-tetramethylbenzidine (TMB) assays. Unidirectional wetting, mechanical behavior, antibacterial efficacy against Staphylococcus aureus (S.aureus) and Escherichia coli (E.coli), and cytocompatibility with human foreskin fibroblasts (HFFs) were systematically evaluated.

Results The nanozyme Fe-MIL-88NH2 displayed a uniform octahedral morphology with an average particle size near 281 nm and reached maximal peroxidase-mimicking activity at approximately pH=4, while activity diminished under alkaline conditions. The PP substrate and reconstructed PVDF layer were assembled into a porous, interpenetrating network with clearly distinct fiber scales, measured as (15.68±0.26) μm for PP and (515±19.8) nm for PVDF. Methanol activation shifted PVDF toward a more polar state and reduced the static water contact angle from roughly (132.13°±1.63)° to (75.80±2.24)°, while the bilayer preserved a pronounced hydrophobic-hydrophilic asymmetry that is essential for moisture management. Ink-drop tracking confirmed stable unidirectional transport, where droplets placed on the hydrophobic PP face were drawn across the interface into the hydrophilic PVDF layer with an onset near 10 s, whereas droplets deposited on the hydrophilic face were rapidly absorbed and spread within about 5 s and did not seep backward over a 60 s observation window. Tensile testing showed that adding the reconstructed PVDF layer increased strength toward skin-like levels, with machine-direction strength around 11.4 MPa and cross-direction strength around 7.3 MPa, while elongation remained compliant for body motion at (53±8)% in the machine direction and (142±20)% in the cross direction. Cascade catalysis proceeded under physiologically relevant buffers. Au NPs oxidized glucose and lowered the local pH value over roughly 60 min, which activated Fe-MIL-88NH2 to decompose in-situ-generated hydrogen peroxide and yield hydroxyl radicals (·OH), as indicated by the characteristic blue TMB product. This glucose-responsive cascade translated into potent broad-spectrum antibacterial performance in vitro, with inhibition rate against S.aureus and E.coli exceeding 97% by plate counting relative to controls. Cytocompatibility testing indicated minimal mammalian cell toxicity, with HFF viability maintained at or above 84% after 24 h of co-culture, supporting the safety of the immobilization strategy and matrix selection.

Conclusion The proposed dressing integrates a bilayer with a glucose-triggered Au-NP/Fe-MIL-88NH2 nanozyme cascade, aligning exudate drainage and on-demand reactive oxygen species (ROS) generation within a single textile construct. The wettability gradient drives liquid unidirectionally from the hydrophobic interior to the hydrophilic exterior, preventing backflow and maintaining a drier wound interface, while the cascade efficiently suppresses bacteria under DFU-relevant glucose levels with ≥97% inhibition rate and preserves fibroblast viability (≥84%). Mechanically, the composite approximates skin-like strength and extensibility, supporting conformal coverage. The short-fiber reconstruction route achieves uniform, stable nanozyme anchoring throughout a porous hydrophilic layer, preserving catalytic accessibility and enhancing mass transfer. Collectively, these findings substantiate a materials strategy that couples exudate management with antibiotic-free antibacterial activity, offering translational promise for managing chronic, infection-prone DFUs. Future work may extend to in vivo validation under dynamic exudate flux, long-term stability of immobilized nanozymes, and optimization of layer thickness and fiber morphology for scalable manufacturing.

Key words: nanoenzyme, cascade antibacterial, unidirectional moisture transfer, nanofiber dressing, diabetic foot ulcers, polypropylene nonwoven, poly(vinylidene fluoride) fiber, medical textiles

CLC Number: 

  • TQ 340.64

Fig.1

Schematic diagram of preparation of composite dressing"

Fig.2

SEM images of Fe-MIL-88NH2"

Fig.3

Absorbance of Fe-MIL-88NH2 solution at different pH values"

Fig.4

Surface (a)and cross-section (b) SEM images of lower PP nonwoven fabric and upper reconstituted PVDF fiber membrane of composite dressing"

Fig.5

FT-IR spectra of PVDF, methanol-treated PVDF, and PVDF/PP short-fiber membrane"

Tab.1

Water contact angles of materials before and after preparing composite dressing"

试样名称 接触角/(°)
PP非织造布 137.94±1.09a
PVDF膜 132.13±1.63a
甲醇处理PVDF膜 75.80±2.24b
PVDF/PP复合敷料 75.51±6.65b

Fig.6

Unidirectional wetting properties of ink droplets on upper and lower surfaces of dressings. (a)Diffusion process;(b)Transport path"

Fig.7

Stress-strain curves of PP nonworen and PVDF/PP composite dressing in MD and CD directions"

Tab.2

Time-dependent pH change of reaction system with composite dressing"

时间/min 颜色变化 pH值区间
0 黄色 >6.2
30 橙色 4.4~6.2
60 浅红 <4.4
90 红色 <4.4
120 深红 <4.4

Fig.8

TMB colorimetric reaction results for composite dressing"

Fig.9

Antibacterial properties of composite dressings. (a) Control samples; (b) Composite dressings"

Tab.3

Cytotoxicity of composite dressings"

试样名称 细胞存活率/%
空白对照样 99.81±1.87a
PP非织造布 84.88±6.07b
PVDF重构层 87.41±8.94b
PVDF/PP复合敷料 83.91±0.67b
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