4.4 Article

A low-fat diet up-regulates expression of fatty acid taste receptor gene FFAR4 in fungiform papillae in humans: a co-twin randomised controlled trial

期刊

BRITISH JOURNAL OF NUTRITION
卷 122, 期 11, 页码 1212-1220

出版社

CAMBRIDGE UNIV PRESS
DOI: 10.1017/S0007114519002368

关键词

Fat intake; Fatty acid taste; Randomised controlled trials; Free fatty acid receptor 4; G protein-coupled receptor 120

资金

  1. National Health and Medical Research Council (NHMRC) [104780]
  2. Centre for Advanced Sensory Science at Deakin University
  3. Centre of Research Excellence Grant from the NHMRC [1079102]

向作者/读者索取更多资源

Fatty acid taste (FAT) perception is involved in the regulation of dietary fat intake, where impaired FAT is associated with increased fatty food intake. There are a number of FAT receptors identified on human taste cells that are potentially responsible for FAT perception. Manipulating dietary fat intake, and in turn FAT perception, would elucidate the receptors that are associated with long-term regulation of FAT perception. The present study aimed to assess associations between diet-mediated changes to FAT receptors and FAT perception in humans. A co-twin randomised controlled trial was conducted, where each matching twin within a pair were randomly allocated to either an 8-week low-fat (LF; <20 % energy fat) or an 8-week high-fat (HF; >35 % energy fat) diet. At baseline and week 8, fungiform papillae were biopsied in the fasted state and FAT receptor gene expressions (cluster of differentiation 36 (CD36), free fatty acid receptor 2 (FFAR2), FFAR4, G protein-coupled receptor 84 (GPR84) and a delayed rectifying K+ channel (K+ voltage-gated channel subfamily A member 2; KCNA2)) were measured using RT-PCR; and FAT threshold (FATT) was assessed using three-alternate forced choice methodology. Linear mixed models were fitted, adjusting for correlation between co-twins. Intake was compliant with the study design, with the LF and HF groups consuming 14 center dot 8 and 39 center dot 9 % energy from fat, respectively. Expression of FFAR4 increased by 38 % in the LF group (P = 0 center dot 023; time-diet interaction P = 0 center dot 063). Delta FFAR4 (Delta, week 8-baseline) was associated with Delta fat intake (g) ( = -159 center dot 4; P < 0 center dot 001) and Delta FATT ( = -8 center dot 8; P = 0 center dot 016). In summary, FFAR4 is involved in long-term diet-mediated changes to FAT perception. Manipulating dietary fat intake, and therefore FFAR4 expression, might aid in reducing taste-mediated passive overconsumption of fatty foods.

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