Literature DB >> 29794036

Deep phenotyping in zebrafish reveals genetic and diet-induced adiposity changes that may inform disease risk.

James E N Minchin1,2, Catherine M Scahill3, Nicole Staudt3, Elisabeth M Busch-Nentwich3,4, John F Rawls2,4.   

Abstract

The regional distribution of adipose tissues is implicated in a wide range of diseases. For example, proportional increases in visceral adipose tissue increase the risk for insulin resistance, diabetes, and CVD. Zebrafish offer a tractable model system by which to obtain unbiased and quantitative phenotypic information on regional adiposity, and deep phenotyping can explore complex disease-related adiposity traits. To facilitate deep phenotyping of zebrafish adiposity traits, we used pairwise correlations between 67 adiposity traits to generate stage-specific adiposity profiles that describe changing adiposity patterns and relationships during growth. Linear discriminant analysis classified individual fish according to an adiposity profile with 87.5% accuracy. Deep phenotyping of eight previously uncharacterized zebrafish mutants identified neuropilin 2b as a novel gene that alters adipose distribution. When we applied deep phenotyping to identify changes in adiposity during diet manipulations, zebrafish that underwent food restriction and refeeding had widespread adiposity changes when compared with continuously fed, equivalently sized control animals. In particular, internal adipose tissues (e.g., visceral adipose) exhibited a reduced capacity to replenish lipid following food restriction. Together, these results in zebrafish establish a new deep phenotyping technique as an unbiased and quantitative method to help uncover new relationships between genotype, diet, and adiposity.
Copyright © 2018 Minchin et al.

Entities:  

Keywords:  adipose tissue; fat distribution; obesity

Mesh:

Year:  2018        PMID: 29794036      PMCID: PMC6071777          DOI: 10.1194/jlr.D084525

Source DB:  PubMed          Journal:  J Lipid Res        ISSN: 0022-2275            Impact factor:   5.922


  37 in total

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10.  MicroCT-based phenomics in the zebrafish skeleton reveals virtues of deep phenotyping in a distributed organ system.

Authors:  Matthew Hur; Charlotte A Gistelinck; Philippe Huber; Jane Lee; Marjorie H Thompson; Adrian T Monstad-Rios; Claire J Watson; Sarah K McMenamin; Andy Willaert; David M Parichy; Paul Coucke; Ronald Y Kwon
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3.  Quantitative analyses of adiposity dynamics in zebrafish.

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5.  Starvation causes changes in the intestinal transcriptome and microbiome that are reversed upon refeeding.

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