Division of Applied Biosciences, Graduate School of Agriculture, Kyoto University, Kyoto, 606-8502, Japan.
Faculty of Bioscience, Nagahama Institute of Bio-Science and Technology, Nagahama, 526-0829, Japan.
Arch Biochem Biophys. 2022 Sep 30;727:109341. doi: 10.1016/j.abb.2022.109341. Epub 2022 Jun 28.
Carnosine, which is abundant in meat, is a dipeptide composed of β-alanine and histidine, known to afford various health benefits. It has been suggested that carnosine can elicit an anti-obesity effect via induction and activation of brown/beige adipocytes responsible for non-shivering thermogenesis. However, the relationship between carnosine and brown/beige adipocytes has not been comprehensively elucidated. We hypothesized that β-alanine directly modulates brown/beige adipogenesis and performed an in vitro assessment to test this hypothesis. HB2 brown preadipocytes were differentiated using insulin from day 0. Cells were treated with various concentrations of β-alanine (12.5-100 μM) during adipogenesis (days 0-8) and differentiation (days 8-10). Then, cells were further stimulated with or without forskolin, an activator of the cAMP-dependent protein kinase pathway, on day 8 or day 10 for 4 h before harvesting. We observed that HB2 cells expressed molecules related to the transport and signal transduction of β-alanine. Treatment with β-alanine during brown adipogenesis dose-dependently enhanced forskolin-induced Ucp1 expression; this was not observed in differentiated brown adipocytes. Consistent with these findings, treatment with β-alanine during days 0-8 increased phosphorylation levels of CREB in forskolin-treated HB2 cells. In addition, β-alanine treatment during brown adipogenesis increased the expression of Pparα, known to induce brown/beige adipogenesis, in a dose-dependent manner. These findings revealed that β-alanine could target HB2 adipogenic cells and enhance forskolin-induced Ucp1 expression during brown adipogenesis, possibly by accelerating phosphorylation and activation of CREB. Thus, β-alanine, a carnosine-constituting amino acid, might directly act on brown adipogenic cells to stimulate energy expenditure.
肌肽,富含于肉类,是由β-丙氨酸和组氨酸组成的二肽,具有多种健康益处。有研究表明,肌肽通过诱导和激活负责非颤抖性产热的棕色/米色脂肪细胞,发挥抗肥胖作用。然而,肌肽与棕色/米色脂肪细胞之间的关系尚未得到全面阐明。我们假设β-丙氨酸可直接调节棕色/米色脂肪生成,并进行了体外评估来验证这一假设。HB2 棕色前体脂肪细胞在第 0 天用胰岛素分化。在脂肪生成(第 0-8 天)和分化(第 8-10 天)期间,用不同浓度的β-丙氨酸(12.5-100 μM)处理细胞。然后,在第 8 天或第 10 天,在没有或有 forskolin(cAMP 依赖性蛋白激酶途径的激活剂)刺激的情况下,将细胞再孵育 4 小时,然后收获。我们观察到 HB2 细胞表达与β-丙氨酸的转运和信号转导有关的分子。在棕色脂肪生成期间,β-丙氨酸处理以剂量依赖的方式增强了 forskolin诱导的 Ucp1 表达;而在分化的棕色脂肪细胞中则未观察到。与这些发现一致,在第 0-8 天期间用β-丙氨酸处理增加了 HB2 细胞中 forskolin 处理后的 CREB 磷酸化水平。此外,在棕色脂肪生成期间,β-丙氨酸处理以剂量依赖的方式增加了 Pparα的表达,已知 Pparα可诱导棕色/米色脂肪生成。这些发现表明,β-丙氨酸可以作用于 HB2 脂肪生成细胞,并在棕色脂肪生成期间增强 forskolin 诱导的 Ucp1 表达,可能通过加速 CREB 的磷酸化和激活。因此,肌肽的组成氨基酸β-丙氨酸可能直接作用于棕色脂肪生成细胞,刺激能量消耗。
