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口服给药后,通过肠-脑轴起作用的一种新型大豆衍生抗焦虑样十一肽的合理鉴定。

Rational identification of a novel soy-derived anxiolytic-like undecapeptide acting via gut-brain axis after oral administration.

作者信息

Ota Ami, Yamamoto Akane, Kimura Saeko, Mori Yukiha, Mizushige Takafumi, Nagashima Yoshiki, Sato Masaru, Suzuki Hideyuki, Odagiri Saori, Yamada Daisuke, Sekiguchi Masayuki, Wada Keiji, Kanamoto Ryuhei, Ohinata Kousaku

机构信息

Division of Food Science and Biotechnology, Graduate School of Agriculture, Kyoto University, Gokasho Fuji, Kyoto 611-0011, Japan.

Division of Food Science and Biotechnology, Graduate School of Agriculture, Kyoto University, Gokasho Fuji, Kyoto 611-0011, Japan; Research Unit for Physiological Chemistry, C-PIER, Kyoto University, Kyoto 606-8501, Japan.

出版信息

Neurochem Int. 2017 May;105:51-57. doi: 10.1016/j.neuint.2016.12.020. Epub 2017 Jan 6.

DOI:10.1016/j.neuint.2016.12.020
PMID:28065795
Abstract

Here we found that the chymotryptic digest of soy β-conglycinin, a major storage protein, exhibited anxiolytic-like effects in mice. We then searched for anxiolytic-like peptides in the digest. Based on a comprehensive peptide analysis of the chymotryptic digest by high performance liquid chromatograph connected to an LTQ Orbitrap mass spectrometer and the structure-activity relationship of known peptides, we explored anxiolytic-like peptides present in the digest. FLSSTEAQQSY, which corresponds to 323-333 of the β-conglycinin α subunit [βCGα(323-333)] emerged as a candidate. Oral administration of synthetic βCGα(323-333) exhibited anxiolytic-like effects in the elevated plus-maze and open-field test in male mice. Orally administered βCGα(323-333) exhibited anxiolytic-like effects in sham-operated control mice but not in vagotomized mice. In addition, oral administration of βCGα(323-333) increased the expression of c-Fos, a marker of neuronal activity, in the nucleus of the solitary tract, which receives inputs from the vagus nerve. These results suggest that the anxiolytic-like effects were mediated by the vagus nerve. The anxiolytic-like effects of βCGα(323-333) were also blocked by antagonists of the serotonin 5-HT, dopamine D and GABA receptors. However βCGα(323-333) had no affinity for these receptors, suggesting it stimulates the release of endogenous neurotransmitters to activate the receptors. Taken together, a soy-derived undecapeptide, βCGα(323-333), may exhibit anxiolytic-like effects after oral administration via the vagus nerve and 5-HT, D and GABA systems.

摘要

在此我们发现,大豆主要储存蛋白β -伴大豆球蛋白的胰凝乳蛋白酶消化物在小鼠中表现出抗焦虑样作用。然后我们在该消化物中寻找抗焦虑样肽段。基于通过连接到LTQ Orbitrap质谱仪的高效液相色谱对胰凝乳蛋白酶消化物进行的全面肽段分析以及已知肽段的构效关系,我们探究了该消化物中存在的抗焦虑样肽段。对应于β -伴大豆球蛋白α亚基[βCGα(323 - 333)] 323 - 333位的FLSSTEAQQSY成为一个候选肽段。合成的βCGα(323 - 333)经口服给药在雄性小鼠的高架十字迷宫和旷场试验中表现出抗焦虑样作用。口服给予βCGα(323 - 333)在假手术对照小鼠中表现出抗焦虑样作用,但在迷走神经切断的小鼠中则没有。此外,口服给予βCGα(323 - 333)增加了孤束核中c - Fos(一种神经元活动标志物)的表达,孤束核接收来自迷走神经的传入信息。这些结果表明抗焦虑样作用是由迷走神经介导的。βCGα(323 - 333)的抗焦虑样作用也被5 -羟色胺5 - HT、多巴胺D和GABA受体的拮抗剂所阻断。然而βCGα(323 - 333)对这些受体没有亲和力,这表明它刺激内源性神经递质的释放以激活这些受体。综上所述,一种源自大豆的十一肽βCGα(323 - 333)经口服给药后可能通过迷走神经以及5 - HT、D和GABA系统表现出抗焦虑样作用。

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