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Tas1r3 味觉受体基因的等位基因变异影响 F1 杂交鼠的甜味反应和葡萄糖代谢。

Allelic variation of the Tas1r3 taste receptor gene affects sweet taste responsiveness and metabolism of glucose in F1 mouse hybrids.

机构信息

Pavlov Institute of Physiology, Russian Academy of Sciences, Saint Petersburg, Russia.

出版信息

PLoS One. 2020 Jul 16;15(7):e0235913. doi: 10.1371/journal.pone.0235913. eCollection 2020.

DOI:10.1371/journal.pone.0235913
PMID:32673349
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7365461/
Abstract

In mammals, inter- and intraspecies differences in consumption of sweeteners largely depend on allelic variation of the Tas1r3 gene (locus Sac) encoding the T1R3 protein, a sweet taste receptor subunit. To assess the influence of Tas1r3 polymorphisms on feeding behavior and metabolism, we examined the phenotype of F1 male hybrids obtained from crosses between the following inbred mouse strains: females from 129SvPasCrl (129S2) bearing the recessive Tas1r3 allele and males from either C57BL/6J (B6), carrying the dominant allele, or the Tas1r3-gene knockout strain C57BL/6J-Tas1r3tm1Rfm (B6-Tas1r3-/-). The hybrids 129S2B6F1 and 129S2B6-Tas1r3-/-F1 had identical background genotypes and different sets of Tas1r3 alleles. The effect of Tas1r3 hemizygosity was analyzed by comparing the parental strain B6 (Tas1r3 homozygote) and hemizygous F1 hybrids B6 × B6-Tas1r3-/-. Data showed that, in 129S2B6-Tas1r3-/-F1 hybrids, the reduction of glucose tolerance, along with lower consumption of and lower preference for sweeteners during the initial licking responses, is due to expression of the recessive Tas1r3 allele. Hemizygosity of Tas1r3 did not influence these behavioral and metabolic traits. However, the loss of the functional Tas1r3 allele was associated with a small decline in the long-term intake and preference for sweeteners and reduction of plasma insulin and body, liver, and fat mass.

摘要

在哺乳动物中,物种间和物种内对甜味剂的摄入差异在很大程度上取决于 Tas1r3 基因(位点 Sac)的等位基因变异,该基因编码 T1R3 蛋白,是一种甜味受体亚基。为了评估 Tas1r3 多态性对摄食行为和代谢的影响,我们检查了以下近交系小鼠杂交产生的 F1 雄性杂种的表型:携带隐性 Tas1r3 等位基因的 129SvPasCrl(129S2)雌性和携带显性等位基因的 C57BL/6J(B6)雄性,或 Tas1r3 基因敲除品系 C57BL/6J-Tas1r3tm1Rfm(B6-Tas1r3-/-)雄性。129S2B6F1 和 129S2B6-Tas1r3-/-F1 杂种具有相同的背景基因型和不同的 Tas1r3 等位基因集。通过比较亲本品系 B6(Tas1r3 纯合子)和半合子 F1 杂种 B6×B6-Tas1r3-/-,分析了 Tas1r3 半合性的影响。数据表明,在 129S2B6-Tas1r3-/-F1 杂种中,葡萄糖耐量降低,以及初始舔舐反应中甜味剂的消耗量和偏好性降低,是由于隐性 Tas1r3 等位基因的表达所致。Tas1r3 的半合性并不影响这些行为和代谢特征。然而,功能性 Tas1r3 等位基因的缺失与长期甜味剂摄入和偏好的轻微下降、血浆胰岛素和体质量、肝质量和脂肪质量的减少有关。

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本文引用的文献

1
The Effect of the Taste Receptor Protein T1R3 on the Development of Islet Tissue of the Murine Pancreas.味觉受体蛋白T1R3对小鼠胰腺胰岛组织发育的影响
Dokl Biol Sci. 2019 May;484(1):1-4. doi: 10.1134/S0012496619010010. Epub 2019 Apr 23.
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[EFFECT OF T1R3 RECEPTOR PROTEIN DELETION ON GLUCONEOGENESIS AND LIPID METABOLISM IN MICE].[T1R3受体蛋白缺失对小鼠糖异生和脂质代谢的影响]
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Salivary leptin and TAS1R2/TAS1R3 polymorphisms are related to sweet taste sensitivity and carbohydrate intake from a buffet meal in healthy young adults.
选择特征分析揭示了在绵羊驯化过程中视觉方面所执行的关键功能。
Arch Anim Breed. 2023 Feb 23;66(1):81-91. doi: 10.5194/aab-66-81-2023. eCollection 2023.
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Oral Microbiota-Host Interaction Mediated by Taste Receptors.味觉受体介导的口腔微生物组-宿主相互作用。
Front Cell Infect Microbiol. 2022 Mar 29;12:802504. doi: 10.3389/fcimb.2022.802504. eCollection 2022.
唾液瘦素和TAS1R2/TAS1R3基因多态性与健康年轻成年人的甜味敏感度及自助餐碳水化合物摄入量有关。
Br J Nutr. 2017 Nov;118(10):763-770. doi: 10.1017/S0007114517002872. Epub 2017 Nov 7.
4
Correction: T1R3 homomeric sweet taste receptor regulates adipogenesis through Gαs-mediated microtubules disassembly and Rho activation in 3T3-L1 cells.更正:T1R3 同源甜味受体通过 Gαs 介导的微管解聚和 Rho 激活调控 3T3-L1 细胞中的脂肪生成。
PLoS One. 2017 Jul 7;12(7):e0181293. doi: 10.1371/journal.pone.0181293. eCollection 2017.
5
Ablation of TRPM5 in Mice Results in Reduced Body Weight Gain and Improved Glucose Tolerance and Protects from Excessive Consumption of Sweet Palatable Food when Fed High Caloric Diets.小鼠中瞬时受体电位阳离子通道亚家族M成员5(TRPM5)的消融导致体重增加减少、葡萄糖耐量改善,并且在喂食高热量饮食时可防止过度食用美味食物。
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Sugar-induced cephalic-phase insulin release is mediated by a T1r2+T1r3-independent taste transduction pathway in mice.在小鼠中,糖诱导的头期胰岛素释放是由一条不依赖T1r2+T1r3的味觉转导途径介导的。
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