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香豆素/β-环糊精包合物促进伤口愈合的加速和改善。

Coumarin/β-Cyclodextrin Inclusion Complexes Promote Acceleration and Improvement of Wound Healing.

机构信息

Departamento de Ciências Naturais, Universidade Federal de São João del-Rei, Campus Dom Bosco, Praça Dom Helvécio 74, Fábricas, 36301-160 São João del-Rei, Minas Gerais, Brazil.

Departamento de Química, Universidade Federal do Espírito Santo, Centro de Ciências Exatas, Avenida Fernando Ferrari, S/N, Goiabeiras, 29060-900 Vitoria, Espírito Santo, Brazil.

出版信息

ACS Appl Mater Interfaces. 2024 Jun 19;16(24):30900-30914. doi: 10.1021/acsami.4c05069. Epub 2024 Jun 7.

Abstract

Coumarins have great pharmacotherapeutic potential, presenting several biological and pharmaceutical applications, like antibiotic, fungicidal, anti-inflammatory, anticancer, anti-HIV, and healing activities, among others. These molecules are practically insoluble in water, and for biological applications, it became necessary to complex them with cyclodextrins (CDs), which influence their bioavailability in the target organism. In this work, we studied two coumarins, and it was possible to conclude that there were structural differences between 4,7-dimethyl-2-chromen-2-one (DMC) and 7-methoxy-4-methyl-2-chromen-2-one (MMC)/β-CD that were solubilized in ethanol, frozen, and lyophilized (FL) and the mechanical mixtures (MM). In addition, the inclusion complex formation improved the solubility of DMC and MMC in an aqueous medium. According to the data, the inclusion complexes were formed and are more stable at a molar ratio of 2:1 coumarin/β-CD, and hydrogen bonds along with π-π stacking interactions are responsible for the better stability, especially for (MMC)@β-CD. wound healing studies in mice showed faster re-epithelialization and the best deposition of collagen with the (DMC)@β-CD (FL) and (MMC)@β-CD (FL) inclusion complexes, demonstrating clearly that they have potential in wound repair. Therefore, (DMC)@β-CD (FL) deserves great attention because it presented excellent results, reducing the granulation tissue and mast cell density and improving collagen remodeling. Finally, the protein binding studies suggested that the anti-inflammatory activities might exert their biological function through the inhibition of MEK, providing the possibility of development of new MEK inhibitors.

摘要

香豆素具有巨大的药物治疗潜力,具有多种生物和药物应用,如抗生素、杀真菌剂、抗炎、抗癌、抗 HIV 和愈合活性等。这些分子在实际上不溶于水,并且对于生物应用,有必要将它们与环糊精(CDs)络合,这会影响它们在靶生物中的生物利用度。在这项工作中,我们研究了两种香豆素,并且可以得出结论,4,7-二甲基-2-色烯-2-酮(DMC)和 7-甲氧基-4-甲基-2-色烯-2-酮(MMC)/β-CD 之间存在结构差异,这些差异在乙醇中溶解、冷冻和冻干(FL)以及机械混合物(MM)中存在。此外,包合复合物的形成提高了 DMC 和 MMC 在水介质中的溶解度。根据数据,在摩尔比为 2:1 的香豆素/β-CD 时形成了包含复合物,并且更稳定,氢键以及π-π堆积相互作用负责更好的稳定性,特别是对于(MMC)@β-CD。在小鼠中的伤口愈合研究表明,(DMC)@β-CD(FL)和(MMC)@β-CD(FL)包含复合物具有更快的再上皮化和更好的胶原蛋白沉积,清楚地表明它们在伤口修复中有潜力。因此,(DMC)@β-CD(FL)值得高度关注,因为它表现出出色的效果,减少了肉芽组织和肥大细胞密度,并改善了胶原蛋白重塑。最后,蛋白质结合研究表明,抗炎活性可能通过抑制 MEK 发挥其生物学功能,为开发新的 MEK 抑制剂提供了可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/457a/11194811/18308183db45/am4c05069_0001.jpg

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