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消化和发酵的绿奇异果可增加人体 β-防御素 1 和 2 的体外产生。

Digested and fermented green kiwifruit increases human β-defensin 1 and 2 production in vitro.

机构信息

Food and Nutrition, The New Zealand Institute for Plant & Food Research Ltd., Palmerston North, New Zealand.

出版信息

Plant Foods Hum Nutr. 2012 Sep;67(3):208-14. doi: 10.1007/s11130-012-0305-1.

Abstract

The intestinal mucosa is constantly exposed to a variety of microbial species including commensals and pathogens, the latter leaving the host susceptible to infection. Antimicrobial peptides (AMP) are an important part of the first line of defense at mucosal surfaces. Human β-defensins (HBD) are AMP expressed by colonic epithelial cells, which act as broad spectrum antimicrobials. This study explored the direct and indirect effects of green kiwifruit (KF) on human β-defensin 1 and 2 (HBD-1 and 2) production by epithelial cells. In vitro digestion of KF pulp consisted of a simulated gastric and duodenal digestion, followed by colonic microbial fermentation using nine human faecal donors. Fermenta from individual donors was sterile filtered and independently added to epithelial cells prior to analysis of HBD protein production. KF products obtained from the gastric and duodenal digestion had no effect on the production of HBD-1 or 2 by epithelial cells, demonstrating that KF does not contain substances that directly modulate defensin production. However, when the digested KF products were further subjected to in vitro colonic fermentation, the fermentation products significantly up-regulated HBD-1 and 2 production by the same epithelial cells. We propose that this effect was predominantly mediated by the presence of short-chain fatty acids (SCFA) in the fermenta. Exposure of cells to purified SCFA confirmed this and HBD-1 and 2 production was up-regulated with acetate, propionate and butyrate. In conclusion, in vitro colonic fermentation of green kiwifruit digest appears to prime defense mechanisms in gut cells by enhancing the production of antimicrobial defensins.

摘要

肠道黏膜不断暴露于各种微生物中,包括共生菌和病原体,后者使宿主易受感染。抗菌肽(AMP)是黏膜表面第一道防线的重要组成部分。人β-防御素(HBD)是结肠上皮细胞表达的 AMP,具有广谱抗菌作用。本研究探讨了绿奇异果(KF)对上皮细胞人β-防御素 1 和 2(HBD-1 和 2)产生的直接和间接影响。KF 果肉的体外消化包括模拟胃和十二指肠消化,然后用 9 位人类粪便供体进行结肠微生物发酵。来自个体供体的发酵物经过无菌过滤,在分析 HBD 蛋白产生之前,分别添加到上皮细胞中。胃和十二指肠消化的 KF 产物对上皮细胞 HBD-1 或 2 的产生没有影响,表明 KF 不含有直接调节防御素产生的物质。然而,当进一步对消化的 KF 产物进行体外结肠发酵时,发酵产物显著上调了同一上皮细胞的 HBD-1 和 2 的产生。我们提出,这种作用主要是由发酵液中短链脂肪酸(SCFA)的存在介导的。细胞暴露于纯化的 SCFA 证实了这一点,并且 HBD-1 和 2 的产生随着乙酸盐、丙酸盐和丁酸盐的增加而上调。总之,绿奇异果消化物的体外结肠发酵似乎通过增强抗菌防御素的产生来启动肠道细胞的防御机制。

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