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膳食 GABA 诱导小鼠骨骼肌内源性合成新型咪唑肽同型瓜氨酸。

Dietary GABA induces endogenous synthesis of a novel imidazole peptide homocarnosine in mouse skeletal muscles.

机构信息

Graduate School of Integrated Sciences for Life, Hiroshima University, Higashi-Hiroshima City, 1-4-4 Kagamiyama, Hiroshima, 739-8528, Japan.

NH Foods Ltd. R&D Center, Tsukuba, Ibaraki, 300-2646, Japan.

出版信息

Amino Acids. 2020 May;52(5):743-753. doi: 10.1007/s00726-020-02848-x. Epub 2020 May 2.

Abstract

Carnosine (β-alanyl-L-histidine) is an imidazole dipeptide present at high concentrations in skeletal muscles, where it plays a beneficial role. However, oral intake of carnosine or β-alanine to increase skeletal muscle carnosine levels has disadvantages such as low efficiency and side effects. Therefore, we proposed homocarnosine (γ-aminobutyryl-L-histidine) as a novel alternative imidazole peptide for skeletal muscle based on its structural similarity to carnosine. To induce endogenous homocarnosine synthesis in skeletal muscles, mice were fed a basal diet mixed with 0, 0.5, 2, or 5% γ-aminobutyric acid (GABA) for 6 weeks. As expected, in the control group (0% GABA), GABA and homocarnosine were present in trace concentrations. Skeletal muscle homocarnosine levels were significantly increased in the 2% and 5% GABA intake groups (tenfold, P < 0.01 and 53-fold, P < 0.01; respectively) relative to those of the control group, whereas 0.5% GABA intake induced no such effect. GABA intake had no effect on the levels of carnosine, anserine, and β-alanine. Vigabatrin (inhibitor of GABA transaminase (GABA-T)) administration to mice receiving 2% GABA intake for 2 weeks led to GABA-T inhibition in the liver. Subsequently, a 43-fold increase in circulating GABA levels and a tendency increase in skeletal muscle homocarnosine levels were observed. Therefore, skeletal muscle homocarnosine synthesis can be induced by supplying its substrate GABA in tissues. As GABA availability is tightly regulated by GABA-T via GABA degradation, inhibitors of GABA or β-alanine degradation could be novel potential interventions for increasing skeletal muscle imidazole dipeptides.

摘要

肌肽(β-丙氨酰-L-组氨酸)是一种高浓度存在于骨骼肌中的咪唑二肽,在骨骼肌中发挥有益作用。然而,口服肌肽或β-丙氨酸来提高骨骼肌肌肽水平存在效率低和副作用等缺点。因此,我们基于其与肌肽的结构相似性,提出了同型肌肽(γ-氨基丁酸-L-组氨酸)作为一种新型的骨骼肌咪唑肽替代物。为了在骨骼肌中诱导内源性同型肌肽合成,用含有 0、0.5、2 或 5%γ-氨基丁酸(GABA)的基础饲料喂养小鼠 6 周。正如预期的那样,在对照组(0%GABA)中,GABA 和同型肌肽的浓度很低。与对照组相比,2%和 5%GABA 摄入组的骨骼肌同型肌肽水平显著增加(分别增加 10 倍,P<0.01 和 53 倍,P<0.01),而 0.5%GABA 摄入没有这种效果。GABA 摄入对肌肽、鹅肌肽和β-丙氨酸的水平没有影响。维加特林(GABA 转氨酶(GABA-T)抑制剂)给予接受 2%GABA 摄入 2 周的小鼠,导致肝脏中 GABA-T 抑制。随后,观察到循环 GABA 水平增加 43 倍,骨骼肌同型肌肽水平呈增加趋势。因此,通过在组织中提供其底物 GABA,可以诱导骨骼肌同型肌肽合成。由于 GABA 的可用性通过 GABA 降解由 GABA-T 严格调节,因此 GABA 或 β-丙氨酸降解的抑制剂可能是增加骨骼肌咪唑二肽的新的潜在干预措施。

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