# Biased sweet taste signaling pathways in mice and humans

> **NIH NIH P20** · UNIVERSITY OF NEBRASKA LINCOLN · 2022 · $132,580

## Abstract

The obesity epidemic has reached alarming proportions in many parts of the world, fueled by the over 
consumption of calorie-rich foods, primarily sugars in the form of sugar-sweetened beverages and other 
sweet foods. Hence, novel strategies are needed to prevent excessive sugar consumption and to promote 
a healthy diet. Non-caloric sweeteners have been used for several decades to replace sugar-derived 
calories. However, their health benefits have been questioned and their taste profile is inferior to sugars. 
Therefore, there is a need to develop novel healthy and tasty non-caloric sweeteners. The sweet taste 
receptor - a heterodimeric G-protein coupled receptor (GPCR) formed by the TAS1R2 and TAS1R3 
subunits - is the primary receptor for sugars and non-caloric sweeteners. Studies to date have focused on 
the G-protein mediated pathway as the primary mechanism for transduction of sweet taste signaling 
downstream of the sweet taste receptor. However, it is now well known that the arrestins, adaptor proteins 
first identified as mediators of GPCR- desensitization, can transduce signals down stream of GPCRs on 
their own. The G-protein and arrestin pathways engage different downstream signaling partners and 
consequently, have different physiological effects. An exciting development in pharmacology is the 
discovery that some GPCR ligands differentially engage the G-protein and arrestin pathways, although they 
bind to the same receptor. Such biased ligands are exciting drug candidates. Using single-cell RNASeq, we 
showed that Arrb1 is the sole arrestin expressed in sweet taste receptor expressing cells. We propose to 
identify the role of arrestin signaling in sweet taste using conditional knockout (CKO) mice models and 
taste organoids cultured from this strain. We will confirm the specific expression of Arrb1 in sweet taste 
cells using in situ hybridization and immunohistochemistry and will compare the behavioral and taste nerve 
responses of Arrb1CKO and control mice to sweet and other control taste stimuli. The kinetics of arrestin 
binding to the sweet taste receptor, sweet taste adaptation, and arrestin signaling will be studied in taste 
organoids using microscopic and other assays (Specific Aim 1). Unfortunately, such mechanistic studies 
are not possible in humans, as human taste stem cells have not been identified. We will use cutting-edge 
spatial transcriptomics of human and mouse taste papillae and compare this to existing droplet-based 
scRNASeq data from mouse cells, to identify human taste cell types including stem cells and the growth 
factors required for regeneration of taste cells (Specific Aim 2). Data from this study will enable the 
development of tools and strategies to manipulate sweet taste signaling.

## Key facts

- **NIH application ID:** 10456040
- **Project number:** 5P20GM104320-09
- **Recipient organization:** UNIVERSITY OF NEBRASKA LINCOLN
- **Principal Investigator:** Sunil Kumar Sukumaran
- **Activity code:** P20 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2022
- **Award amount:** $132,580
- **Award type:** 5
- **Project period:** 2014-08-05 → 2024-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10456040

## Citation

> US National Institutes of Health, RePORTER application 10456040, Biased sweet taste signaling pathways in mice and humans (5P20GM104320-09). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/10456040. Licensed CC0.

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