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Allelic variation of the Tas1r3 taste receptor gene selectively affects taste responses to sweeteners: evidence from 129.B6-Tas1r3 congenic mice

机译:Tas1r3味觉受体基因的等位基因变异选择性影响对甜味剂的味觉反应:来自129.B6-Tas1r3同基因小鼠的证据

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摘要

The Tas1r3 gene encodes the T1R3 receptor protein, which is involved in sweet taste transduction. To characterize ligand specificity of the T1R3 receptor and the genetic architecture of sweet taste responsiveness, we analyzed taste responses of 129.B6-Tas1r3 congenic mice to a variety of chemically diverse sweeteners and glucose polymers with three different measures: consumption in 48-h two-bottle preference tests, initial licking responses, and responses of the chorda tympani nerve. The results were generally consistent across the three measures. Allelic variation of the Tas1r3 gene influenced taste responsiveness to nonnutritive sweeteners (saccharin, acesulfame-K, sucralose, SC-45647), sugars (sucrose, maltose, glucose, fructose), sugar alcohols (erythritol, sorbitol), and some amino acids (d-tryptophan, d-phenylalanine, l-proline). Tas1r3 genotype did not affect taste responses to several sweet-tasting amino acids (l-glutamine, l-threonine, l-alanine, glycine), glucose polymers (Polycose, maltooligosaccharide), and nonsweet NaCl, HCl, quinine, monosodium glutamate, and inosine 5′-monophosphate. Thus Tas1r3 polymorphisms affect taste responses to many nutritive and nonnutritive sweeteners (all of which must interact with a taste receptor involving T1R3), but not to all carbohydrates and amino acids. In addition, we found that the genetic architecture of sweet taste responsiveness changes depending on the measure of taste response and the intensity of the sweet taste stimulus. Variation in the T1R3 receptor influenced peripheral taste responsiveness over a wide range of sweetener concentrations, but behavioral responses to higher concentrations of some sweeteners increasingly depended on mechanisms that could override input from the peripheral taste system.
机译:Tas1r3基因编码T1R3受体蛋白,该蛋白参与甜味的传递。为了表征T1R3受体的配体特异性和甜味响应性的遗传结构,我们通过三种不同的方法分析了129.B6-Tas1r3同基因小鼠对多种化学上不同的甜味剂和葡萄糖聚合物的味觉响应:在48小时内食用瓶偏好测试,初始舔食反应和鼓膜鼓膜神经反应。三种方法的结果总体上是一致的。 Tas1r3基因的等位基因变异影响对非营养性甜味剂(糖精,乙酰磺胺酸钾,三氯蔗糖,SC-45647),糖(蔗糖,麦芽糖,葡萄糖,果糖),糖醇(赤藓糖醇,山梨糖醇)和某些氨基酸( d-色氨酸,d-苯丙氨酸,l-脯氨酸)。 Tas1r3基因型不影响对几种甜味氨基酸(l-谷氨酰胺,l-苏氨酸,l-丙氨酸,甘氨酸),葡萄糖聚合物(多聚糖,麦芽低聚糖)和不甜的NaCl,HCl,奎宁,谷氨酸钠和肌苷5'-单磷酸。因此,Tas1r3多态性影响对许多营养和非营养甜味剂(所有甜味剂都必须与涉及T1R3的味觉受体相互作用)的味觉响应,但不影响所有碳水化合物和氨基酸。另外,我们发现甜味响应性的遗传结构根据味觉响应的量度和甜味刺激的强度而变化。 T1R3受体的变化会在很大范围的甜味剂浓度范围内影响周围的味觉响应性,但是对某些甜味剂的较高浓度的行为响应越来越依赖于可以超越周围味觉系统输入的机制。

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