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Figure 12

Descrizione

Supplementary characterization or additional in vivo data from the click chemistry hydrogel study is presented. The comprehensive evaluation supports the platform's potential for translational application in diabetic wound management.

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Rheological and mechanical characterization of the click chemistry hydrogel demonstrates properties suitable for 3D bioprinting. The material's shear-thinning behavior and rapid recovery enable precise deposition of cell-laden constructs.

Figure 3

Rheological and mechanical characterization of the click chemistry hydrogel demonstrates properties suitable for 3D bioprinting. The material's shear-thinning behavior and rapid recovery enable precise deposition of cell-laden constructs.

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Bioprinting parameters and construct fidelity are evaluated for the peptide hydrogel system. The printability assessment confirms that the material maintains structural integrity while supporting embedded vascular endothelial cell viability.

Figure 4

Bioprinting parameters and construct fidelity are evaluated for the peptide hydrogel system. The printability assessment confirms that the material maintains structural integrity while supporting embedded vascular endothelial cell viability.

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VEGF165-overexpressing endothelial cells encapsulated within the hydrogel are assessed for viability and vascular network formation. The growth factor expression aims to promote angiogenesis, addressing the vascular injury central to non-healing diabetic wounds.

Figure 5

VEGF165-overexpressing endothelial cells encapsulated within the hydrogel are assessed for viability and vascular network formation. The growth factor expression aims to promote angiogenesis, addressing the vascular injury central to non-healing diabetic wounds.

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In vitro wound healing assays using the bioprinted hydrogel constructs demonstrate enhanced cell migration and proliferation. The results suggest that the all-peptide platform supports the cellular processes required for tissue regeneration.

Figure 6

In vitro wound healing assays using the bioprinted hydrogel constructs demonstrate enhanced cell migration and proliferation. The results suggest that the all-peptide platform supports the cellular processes required for tissue regeneration.

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Gene expression or protein analysis from cells cultured in the hydrogel platform reveals upregulation of angiogenic and wound healing markers. The molecular data support the functional benefits observed in cell migration and proliferation assays.

Figure 7

Gene expression or protein analysis from cells cultured in the hydrogel platform reveals upregulation of angiogenic and wound healing markers. The molecular data support the functional benefits observed in cell migration and proliferation assays.

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In vivo evaluation of the bioprinted hydrogel in a diabetic wound model shows wound closure progression over time. The cell-laden constructs demonstrate accelerated healing compared to control treatments in the high-glucose wound environment.

Figure 8

In vivo evaluation of the bioprinted hydrogel in a diabetic wound model shows wound closure progression over time. The cell-laden constructs demonstrate accelerated healing compared to control treatments in the high-glucose wound environment.

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Figure 12

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Source Paper

A click chemistry-mediated all-peptide cell printing hydrogel platform for diabetic wound healing.

Nature communications (2023)

PMID: 38030636

DOI: 10.1038/s41467-023-43364-2

Cite This Figure

![Figure 12: Supplementary characterization or additional in vivo data from the click chemistry hydrogel study is presented. The comprehensive evaluation supports the platform's potential for translational application in diabetic wound management.](https://pdfs.citedhealth.com/figures/38030636/266.png)

> Source: Jinjian Huang et al. "A click chemistry-mediated all-peptide cell printing hydrogel platform for diabe." *Nature communications*, 2023. PMID: [38030636](https://pubmed.ncbi.nlm.nih.gov/38030636/)
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  <img src="https://pdfs.citedhealth.com/figures/38030636/266.png" alt="Supplementary characterization or additional in vivo data from the click chemistry hydrogel study is presented. The comprehensive evaluation supports the platform's potential for translational application in diabetic wound management." />
  <figcaption>Figure 12. Supplementary characterization or additional in vivo data from the click chemistry hydrogel study is presented. The comprehensive evaluation supports the platform's potential for translational application in diabetic wound management.<br>  Source: Jinjian Huang et al. "A click chemistry-mediated all-peptide cell printing hydrogel platform for diabe." <em>Nature communications</em>, 2023. PMID: <a href="https://pubmed.ncbi.nlm.nih.gov/38030636/">38030636</a></figcaption>
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Evidenze correlate

B
Arginine per Wound Healing and Immune Recovery

Grado B · 8 studi