Epigallocatechin Gallate-Modified Gelatin Sponges Treated by Vacuum Heating as a Novel Scaffold for Bone Tissue Engineering

Honda, Yoshitomo; Takeda, Yoshihiro; Li, Peiqi; Huang, Anqi; Sasayama, Shígetake; Hara, Eiki; Uemura, Naoya; Ueda, Mitsuharu; Hashimoto, Masanori; Arita, Kenji; Matsumoto, Naoyuki; Hashimoto, Yoshiya; Baba, Shigeaki; Tanaka, Tomonari

doi:10.3390/molecules23040876

Cited by 29 publications

(51 citation statements)

References 46 publications

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“…4-(4,6-Dimethoxy-1,3,5-triazin-2-yl)-4-methylmorpholinium chloride (DMT-MM) and N-methylmorpholine (NMM) were obtained from Tokyo Chemical Industry Co. Ltd. (Tokyo, Japan) and Nacalai Tesque Inc. (Kyoto, Japan), respectively. The AC-vhEGCG-GS was prepared according to previous methods 18) . Briefly, 0.07 mg of EGCG, 100 mg of gelatin, 27.5 μl of NMM, and 69.2 mg DMT-MM were mixed in 5 ml of MilliQ water at 23 o C. The dose of EGCG and gelatin determined in our previous study to result in superior bone formation was used 18,24) .…”

Section: Sample Preparation and Characterizationmentioning

confidence: 99%

“…Consequently, numerous delivery systems have been developed to provide localized release of these therapeutic agents in biomedical engineering 17) . For EGCG, various techniques have been developed to retain or deliver EGCG in the affected areas; these techniques include chemical bonding to polymers 14,16,18) , layer by layer technique 19) , hydrophobic and/or hydrogen bonding 20,21) , EGCG-coating associated with Na + -mediated physical self-assembly 22) and oxidative polymerization 3) , and en-capsulation in drug carriers 23) . Although our understanding of the application of this molecule in bone regenerative therapy remains limited when compared with that in other medical fields, we previously found that gelatin sponges chemically modified with EGCG using an aqueous chemical synthesis method (hereafter designated as AC-EGCG-GS) induced superior bone formation in critical-sized bone defects (4.2 mm of diameter) in mouse calvaria 14) .…”

Section: Introductionmentioning

confidence: 99%

“…Although our understanding of the application of this molecule in bone regenerative therapy remains limited when compared with that in other medical fields, we previously found that gelatin sponges chemically modified with EGCG using an aqueous chemical synthesis method (hereafter designated as AC-EGCG-GS) induced superior bone formation in critical-sized bone defects (4.2 mm of diameter) in mouse calvaria 14) . More recently, we showed that the bone-forming ability of vacuum-heated AC-EGCG-GS (AC-vhEGCG-GS) was greater than that of vacuum-heated gelatin sponges (without EGCG) in critical-sized bone defects (9 mm of diameter) of rat calvaria 18) . Alteration of the quantity of EGCG and gelatin in AC-vhEGCG-GSs affected the bone formation results 18,24) .…”

Section: Introductionmentioning

confidence: 99%

“…More recently, we showed that the bone-forming ability of vacuum-heated AC-EGCG-GS (AC-vhEGCG-GS) was greater than that of vacuum-heated gelatin sponges (without EGCG) in critical-sized bone defects (9 mm of diameter) of rat calvaria 18) . Alteration of the quantity of EGCG and gelatin in AC-vhEGCG-GSs affected the bone formation results 18,24) . Although both AC-vhEGCG-GSs and vacuum-heated gelatin sponges successfully served as scaffolds for cells, the combination of AC-vhEGCG-GS with multipotent progenitor cells (dedifferentiated fat cells or adipose-derived stem cells) formed more bone in the congenital bone defects of rat jaws than the combination of vacuum-heated gelatin sponge with the above cells 25) .…”

Section: Introductionmentioning

confidence: 99%

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Sustained Release of Catechin from Gelatin and Its Effect on Bone Formation in Critical Sized Defects in Rat Calvaria

Honda

Huang

Zhao

et al. 2020

J. Hard Tissue Biology.

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The potential of plant-derived polyphenols in bone tissue engineering has not been fully realized owing to difficulties in maintaining their stability in affected parts. Catechins, such as epigallocatechin gallate (EGCG), are not fully utilized in bone regenerative medicine. Here, we demonstrated that chemical and non-chemical modifications of gelatin with EGCG resulted in distinct bone-forming abilities in critical-sized bone defects (9 mm) in rat calvaria. We prepared two EG-CG-containing gelatin sponges: vacuum-heated gelatin sponges modified chemically with EGCG (AC-vhEGCG-GS) and vacuum-heated gelatin sponges with EGCG (no chemical modification; NC-vhEGCG-GS). Both sponges were characterized using scanning electron microscopy and degradability and EGCG-retention tests. The bone-forming ability of the sponges were estimated using micro-computed tomography and hematoxylin-eosin staining; the quality of newly formed bone (collagen maturation) was determined using picrosirius red staining and polarized microscopy. Both sponges had a spongy and soft texture with macropores ranging 50-150 µm with negligible differences in degradability. The NC-vhEG-CG-GSs released all their EGCG content within 1 h, whereas AC-vhEGCG-GSs retained 75% of the EGCG for up to 24 h. In addition, AC-vhEGCG-GSs resulted in a significantly greater bone formation than NC-vhEGCG-GSs 4 w after implantation, with negligible differences in collagen maturation. These results suggest that the chemical modification of gelatin with EGCG might be a promising strategy to fully utilize the pharmacological effects of EGCG for natural polymer-based sponges. Moreover, the release rate of EGCG from gelatin is possibly a screening parameter affecting the function of EGCG in vivo.

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Section: Sample Preparation and Characterizationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Sustained Release of Catechin from Gelatin and Its Effect on Bone Formation in Critical Sized Defects in Rat Calvaria

Honda

Huang

Zhao

et al. 2020

J. Hard Tissue Biology.

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“…Gelatin, denatured collagen, has been widely utilized as a substrate for biomaterials and drug carriers [25][26][27]. Various groups, including our own group, have utilized this protein as a controlled release carrier for polyphenol [28], growth factors, and antibiotics [27]. A vacuum-heating technique (dehydrothermal treatment: DHT) has been utilized to promote intermolecular bonding based on esterification between the carboxyl and hydroxyl groups in polymers [29].…”

Section: Introductionmentioning

confidence: 99%

Releasing Behavior of Lipopolysaccharide from Gelatin Modulates Inflammation, Cellular Senescence, and Bone Formation in Critical-Sized Bone Defects in Rat Calvaria

et al. 2019

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Lipopolysaccharide (LPS) is a well-known strong inducer of inflammation. However, there is little information regarding how LPS-release behavior affects cellular senescence at the affected area. In this paper, we demonstrate that a vacuum-heating technique (dehydrothermal treatment) can be utilized to prepare an LPS sustained-release gelatin sponge (LS-G). LPS sustained release from gelatin leads to the long-term existence of senescent cells in critical-sized bone defects in rat calvaria. Three types of gelatin sponges were prepared in this study: a medical-grade gelatin sponge with extremely low LPS levels (MG), LS-G, and a LPS rapid-release gelatin sponge (LR-G). Histological (H-E) and immunohistochemical (COX-2, p16, and p21) staining were utilized to evaluate inflammatory reactions and cellular senescence one to three weeks after surgery. Soft X-ray imaging was utilized to estimate new bone formation in the defects. The LR-G led to stronger swelling and COX-2 expression in defects compared to the MG and LS-G at 1 week. Despite a small inflammatory reaction, LS-G implantation led to the long-term existence of senescent cells and hampered bone formation compared to the MG and LR-G. These results suggest that vacuum heating is a viable technique for preparing different types of materials for releasing bacterial components, which is helpful for developing disease models for elucidating cellular senescence and bone regeneration.

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A Senomorphic‐Conjugated Scaffold for Application of Senescent Cells in Regenerative Medicine

Deng

Tanaka

et al. 2023

Advanced Therapeutics

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Procuring a sufficient amount of cells is essential for cell-based regenerative therapy. However, the application of senescent cells replicated using cell culture is limited because the cells have lost their regenerative ability or produce deleterious senescence-associated secretory phenotypes (SASPs). In this study, using a senomorphic (epigallocatechin gallate [EGCG]), which could modulate SASP secretion from senescent cells, nonsenescent and senescent dedifferentiated fat cells from rats (rDFAT cells), and congenital cleft-jaw defects in rats, the authors show that the senomorphic (EGCG)-conjugated cellular scaffold restores the bone regenerative ability of senescent multipotent progenitor cells, even in vivo. In this osteogenic process, the EGCG-conjugated scaffold attenuates the production of representative SASPs (i.e., interleukin [IL]-6 and tumor necrosis factor-𝜶) and reactive oxygen species in vivo and in vitro. In polymerase chain reaction arrays in vitro, the EGCG-conjugated cellular scaffold suppresses the expression of genes associated with deleterious SASP factors for bone formation (e.g., Csf2, IL-1a, and others) from senescent rDFAT cells and elevates the expression of potential osteogenesis-and bone remodelingrelated gene (e.g., Cxcl13 and Spp1). These results provide insights to expand the application of senomorphics and senescent stem/multipotent progenitor cells in cell-based regenerative medicine.

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Epigallocatechin Gallate-Modified Gelatin Sponges Treated by Vacuum Heating as a Novel Scaffold for Bone Tissue Engineering

Cited by 29 publications

References 46 publications

Sustained Release of Catechin from Gelatin and Its Effect on Bone Formation in Critical Sized Defects in Rat Calvaria

Sustained Release of Catechin from Gelatin and Its Effect on Bone Formation in Critical Sized Defects in Rat Calvaria

Releasing Behavior of Lipopolysaccharide from Gelatin Modulates Inflammation, Cellular Senescence, and Bone Formation in Critical-Sized Bone Defects in Rat Calvaria

A Senomorphic‐Conjugated Scaffold for Application of Senescent Cells in Regenerative Medicine

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