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The human bitter taste receptor, hTAS2R16, discriminates slight differences in the configuration of disaccharides |
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| Authors: | Sakurai Takanobu Misaka Takumi Ueno Yohei Ishiguro Masaji Matsuo Shinji Ishimaru Yoshiro Asakura Tomiko Abe Keiko |
| Institution: | a General Research Institute of Food Science and Technology, Nissin Foods Holdings Co. Ltd., Shiga 525-0058, Japan b Department of Applied Biological Chemistry, Graduate School of Agricultural and Life Sciences, The University of Tokyo, Tokyo 113-8657, Japan c Niigata University of Pharmacy and Applied Life Sciences, Niigata 956-8503, Japan |
| Abstract: | Sweetness and bitterness are key determinants of food acceptance and rejection, respectively. Sugars, such as sucrose and fructose, are generally recognized as sweet. However, not all sugars are sweet, and even anomers may have quite different tastes. For example, gentiobiose is bitter, whereas its anomer, isomaltose, is sweet. Despite this unique sensory character, the molecular basis of the bitterness of gentiobiose remains to be clarified. In this study, we used calcium imaging analysis of human embryonic kidney 293T cells that heterologously expressed human taste receptors to demonstrate that gentiobiose activated hTAS2R16, a bitter taste receptor, but not hT1R2/hT1R3, a sweet taste receptor. In contrast, isomaltose activated hT1R2/hT1R3. As a result, these anomers elicit different taste sensations. Mutational analysis of hTAS2R16 also indicated that gentiobiose and β-d-glucopyranosides, such as salicin share a common binding site of hTAS2R16. |
| Keywords: | Bitter Sweet Taste Calcium imaging Gentiobiose Binding site |
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