The Ile191Val is a partial loss-of-function variant of the TAS1R2 sweet-taste receptor and is associated with reduced glucose excursions in humans

Serrano, Joan; Šeflová, Jaroslava; Park, Jihye; Pribadi, Marsha P.; Sanematsu, Keisuke; Shigemura, Noriatsu; Serna, Vanida A.; Yi, Fanchao; Mari, Andrea; Procko, Erik; Pratley, Richard E.; Robia, Seth L.; Kyriazis, George A.

doi:10.1016/j.molmet.2021.101339

Cited by 12 publications

(14 citation statements)

References 24 publications

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“…Postprandial hyperglycemia significantly contributes to total daytime hyperglycemia and strongly correlates with HbA 1c ( 30 ). This finding is aligned with the reduced OGTT glucose excursions seen in metabolically healthy lean Val/_ participants ( 10 ). However, we did not observe a direct genotype effects in glucose or insulin responses during an OGTT.…”

Section: Discussionsupporting

confidence: 75%

“…Taken together these observations suggest that, like in mice, TAS1R2 may have functional roles in peripheral tissues beyond taste perception. We recently used biochemical approaches to show that the Ile191Val substitution causes a partial loss-of-function of TAS1R2 by reducing the availability of the STR dimer in the plasma membrane ( 10 ). Healthy lean Val carriers had reduced glucose excursions during an OGTT ( 10 ), which resembles the effects seen in mice with a genetic loss-of-function of TAS1R2 ( 5 , 27 ), confirming that the Val substitution causes a partial loss-of-function of STRs.…”

Section: Discussionmentioning

confidence: 99%

“…We recently demonstrated that the TAS1R2 (Ile191Val) polymorphism reduces the levels of STR in the plasma membrane, causing partial loss-of-function ( 10 ). Consequently, Val carriers had a mild reduction in glucose excursions in response to the ingestion of a glucose load, recapitulating the phenotype seen in TAS1R2-KO mice ( 5 ).…”

Section: Introductionmentioning

confidence: 99%

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The Ile191Val Variant of the TAS1R2 Subunit of Sweet Taste Receptors Is Associated With Reduced HbA1c in a Human Cohort With Variable Levels of Glucose Homeostasis

Serrano

Smith

et al. 2022

Front. Nutr.

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The Ile191Val variant of the TAS1R2 gene of sweet taste receptors causes a partial loss-of-function and is associated with reduced glucose excursions in a healthy lean cohort. However, it is unclear whether this polymorphism contributes to the regulation of glucose homeostasis in metabolically unhealthy individuals. Thus, we used participants with variable glycemic profiles and obesity to assess the effects of the TAS1R2-Ile191Val variant. We found that the Val minor allele carriers had lower HbA1c at all levels of fasting glucose and glucose tolerance. These effects were not due to differences in beta-cell function or insulin sensitivity assessed with a frequently sampled intravenous glucose tolerance test. This study extends our previous findings and provides further evidence that sweet taste receptor function may contribute to glucose regulation in humans.

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Section: Discussionsupporting

confidence: 75%

Section: Discussionmentioning

confidence: 99%

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The Ile191Val Variant of the TAS1R2 Subunit of Sweet Taste Receptors Is Associated With Reduced HbA1c in a Human Cohort With Variable Levels of Glucose Homeostasis

Serrano

Smith

et al. 2022

Front. Nutr.

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“…Sweet taste sensing and signaling requires the formation of a T1R2/T1R3 heterodimer [ 14 , 41 ]. Although the mRNA expression of T1r2 and T1r3 has been previously reported in whole mouse islets [ 8 , 9 ], commercially available antibodies targeting STR are not specific.…”

Section: Discussionmentioning

confidence: 99%

Saccharin Stimulates Insulin Secretion Dependent on Sweet Taste Receptor-Induced Activation of PLC Signaling Axis

et al. 2022

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Background: Saccharin is a common artificial sweetener and a bona fide ligand for sweet taste receptors (STR). STR can regulate insulin secretion in beta cells, so we investigated whether saccharin can stimulate insulin secretion dependent on STR and the activation of phospholipase C (PLC) signaling. Methods: We performed in vivo and in vitro approaches in mice and cells with loss-of-function of STR signaling and specifically assessed the involvement of a PLC signaling cascade using real-time biosensors and calcium imaging. Results: We found that the ingestion of a physiological amount of saccharin can potentiate insulin secretion dependent on STR. Similar to natural sweeteners, saccharin triggers the activation of the PLC signaling cascade, leading to calcium influx and the vesicular exocytosis of insulin. The effects of saccharin also partially require transient receptor potential cation channel M5 (TRPM5) activity. Conclusions: Saccharin ingestion may transiently potentiate insulin secretion through the activation of the canonical STR signaling pathway. These physiological effects provide a framework for understanding the potential health impact of saccharin use and the contribution of STR in peripheral tissues.

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“…Serrano et al. subsequently found that T1R2 gene variant Ile191Val causes a partial loss of function and results in reduced glucose excursions during an OGTT, which is independent of the variations in beta-cell function or insulin sensitivity ( Serrano et al., 2021 ). Additionally, bitter taste receptors have also been revealed of the function to evoke airway smooth muscle relaxation via localized calcium flux, predicting the potential role in counteracting asthmatic bronchoconstriction ( Deshpande et al., 2010 ).…”

Section: Regulation Of Taste Receptors On Oral Microbiota-host Intera...mentioning

confidence: 99%

Oral Microbiota-Host Interaction Mediated by Taste Receptors

Dong

Liu

Zhu

et al. 2022

Front. Cell. Infect. Microbiol.

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Taste receptors, originally identified in taste buds, function as the periphery receptors for taste stimuli and play an important role in food choice. Cohort studies have revealed that single nucleotide polymorphisms of taste receptors such as T1R1, T1R2, T2R38 are associated with susceptibility to oral diseases like dental caries. Recent studies have demonstrated the wide expression of taste receptors in various tissues, including intestinal epithelia, respiratory tract, and gingiva, with an emerging role of participating in the interaction between mucosa surface and microorganisms via monitoring a wide range of metabolites. On the one hand, individuals with different oral microbiomes exhibited varied taste sensitivity, suggesting a potential impact of the oral microbiota composition on taste receptor function. On the other hand, animal studies and in vitro studies have uncovered that a variety of oral cells expressing taste receptors such as gingival solitary chemosensory cells, gingival epithelial cells (GECs), and gingival fibroblasts can detect bacterial signals through bitter taste receptors to trigger host innate immune responses, thus regulating oral microbial homeostasis. This review focuses on how taste receptors, particularly bitter and sweet taste receptors, mediate the oral microbiota-host interaction as well as impact the occurrence and development of oral diseases. Further studies delineating the role of taste receptors in mediating oral microbiota-host interaction will advance our knowledge in oral ecological homeostasis establishment, providing a novel paradigm and treatment target for the better management of dental infectious diseases.

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The Ile191Val is a partial loss-of-function variant of the TAS1R2 sweet-taste receptor and is associated with reduced glucose excursions in humans

Cited by 12 publications

References 24 publications

The Ile191Val Variant of the TAS1R2 Subunit of Sweet Taste Receptors Is Associated With Reduced HbA1c in a Human Cohort With Variable Levels of Glucose Homeostasis

The Ile191Val Variant of the TAS1R2 Subunit of Sweet Taste Receptors Is Associated With Reduced HbA1c in a Human Cohort With Variable Levels of Glucose Homeostasis

Saccharin Stimulates Insulin Secretion Dependent on Sweet Taste Receptor-Induced Activation of PLC Signaling Axis

Oral Microbiota-Host Interaction Mediated by Taste Receptors

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