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一种新型维生素C制剂可增强神经突形成和成纤维细胞黏附,并减少外源性物质诱导的T细胞过度活化。

A novel vitamin C preparation enhances neurite formation and fibroblast adhesion and reduces xenobiotic-induced T-cell hyperactivation.

作者信息

Weeks Benjamin S, Perez Pedro P

机构信息

Department of Biology and Environmental Sciences Program, Adelphi University, Garden City, NY, USA.

出版信息

Med Sci Monit. 2007 Mar;13(3):BR51-8.

PMID:17325628
Abstract

BACKGROUND

Vitamin C (ascorbic acid, ascorbate) has been shown to enhance neurite outgrowth, promote fibroblast adhesion during wound healing, and reduce xenobiotic-induced leukocyte hyperactivity and inflammatory damage. In this study, a comparison was made between Ester-C and PureWay-C on these various cellular activities.

MATERIAL/METHODS: PC12 cells were stimulated to form neurites with nerve growth factor, NIH 3T3 fibroblasts were seeded on fibronectin and H9 T-cells were stimulated to aggregate with the pyrethroid pesticide bifenthrin. The rate of neurite formation, fibroblast adhesion and T-cell homotypic aggregation was then measured in the absence and presence of various formulations of vitamin C including Ester-C and PureWay-CTM.

RESULTS

With PureWay-C treatment, 12% of PC12 cells extended neurites within one hour of treatment and 45% of the cells extended neurites by hour nine. With Ester-C, 0% and 15% extended neurites at one and nine hours, respectively. NIH-3T3 fibroblast adhesion to fibronectin was enhanced by 4.7-fold with a 30 minute PureWay-CTM treatment while Ester-C increased fibroblast adhesion by only 1.5 fold. Further, PureWay-CTM reduced pesticide-mediated T-cell homotypic aggregation by 83% within 30 minutes of treatment while the reduction seen with Ester-C was only 33%.

CONCLUSIONS

These data confirm the previous observations that vitamin C supplementation can promote neurite outgrowth, increase fibroblast adhesion and reduce xenobiotic induce immunocytes aggregation. More importantly, these data show that PureWay-C has a faster and greater beneficial effect on these parameters when compared to other vitamin C formulations.

摘要

背景

维生素C(抗坏血酸、抗坏血酸盐)已被证明可促进神经突生长,在伤口愈合过程中促进成纤维细胞黏附,并减少外源性物质诱导的白细胞活性亢进和炎症损伤。在本研究中,对酯化C和纯质C在这些不同细胞活性方面进行了比较。

材料/方法:用神经生长因子刺激PC12细胞形成神经突,将NIH 3T3成纤维细胞接种在纤连蛋白上,并用拟除虫菊酯类农药联苯菊酯刺激H9 T细胞聚集。然后在不存在和存在包括酯化C和纯质C在内的各种维生素C制剂的情况下,测量神经突形成率、成纤维细胞黏附率和T细胞同型聚集率。

结果

用纯质C处理时,12%的PC12细胞在处理后1小时内伸出神经突,45%的细胞在第9小时伸出神经突。用酯化C处理时,1小时和9小时伸出神经突的细胞分别为0%和15%。用纯质C处理30分钟可使NIH-3T3成纤维细胞对纤连蛋白的黏附增强4.7倍,而酯化C仅使成纤维细胞黏附增加1.5倍。此外,纯质C在处理30分钟内可使农药介导的T细胞同型聚集减少83%,而酯化C的减少率仅为33%。

结论

这些数据证实了先前的观察结果,即补充维生素C可促进神经突生长、增加成纤维细胞黏附并减少外源性物质诱导的免疫细胞聚集。更重要地是,这些数据表明,与其他维生素C制剂相比,纯质C在这些参数上具有更快且更大的有益作用。

相似文献

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A novel vitamin C preparation enhances neurite formation and fibroblast adhesion and reduces xenobiotic-induced T-cell hyperactivation.一种新型维生素C制剂可增强神经突形成和成纤维细胞黏附,并减少外源性物质诱导的T细胞过度活化。
Med Sci Monit. 2007 Mar;13(3):BR51-8.
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