PLoS ONE 2015-01-01

Modulation of sweet taste by umami compounds via sweet taste receptor subunit hT1R2.

Jaewon Shim, Hee Jin Son, Yiseul Kim, Ki Hwa Kim, Jung Tae Kim, Hana Moon, Min Jung Kim, Takumi Misaka, Mee-Ra Rhyu

文献索引:PLoS ONE 10(4) , e0124030, (2015)

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摘要

Although the five basic taste qualities-sweet, sour, bitter, salty and umami-can be recognized by the respective gustatory system, interactions between these taste qualities are often experienced when food is consumed. Specifically, the umami taste has been investigated in terms of whether it enhances or reduces the other taste modalities. These studies, however, are based on individual perception and not on a molecular level. In this study we investigated umami-sweet taste interactions using umami compounds including monosodium glutamate (MSG), 5'-mononucleotides and glutamyl-dipeptides, glutamate-glutamate (Glu-Glu) and glutamate-aspartic acid (Glu-Asp), in human sweet taste receptor hT1R2/hT1R3-expressing cells. The sensitivity of sucrose to hT1R2/hT1R3 was significantly attenuated by MSG and umami active peptides but not by umami active nucleotides. Inhibition of sweet receptor activation by MSG and glutamyl peptides is obvious when sweet receptors are activated by sweeteners that target the extracellular domain (ECD) of T1R2, such as sucrose and acesulfame K, but not by cyclamate, which interact with the T1R3 transmembrane domain (TMD). Application of umami compounds with lactisole, inhibitory drugs that target T1R3, exerted a more severe inhibitory effect. The inhibition was also observed with F778A sweet receptor mutant, which have the defect in function of T1R3 TMD. These results suggest that umami peptides affect sweet taste receptors and this interaction prevents sweet receptor agonists from binding to the T1R2 ECD in an allosteric manner, not to the T1R3. This is the first report to define the interaction between umami and sweet taste receptors.


相关化合物

  • 氯化钠
  • 阿斯巴甜
  • 氯化镁
  • 无水氯化钙
  • 4-羟乙基哌嗪乙磺酸
  • 安塞蜜
  • 氯化钠-35cl
  • 二水氯化钙

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