Independent phenotypic plasticity axes define distinct obesity sub-types

Yang, Chih-Hsiang; Fagnocchi, Luca; Apostle, Stefanos; Wegert, Vanessa; Casaní-Galdón, Salvador; Landgraf, Kathrin; Panzeri, Ilaria; Dror, Erez; Heyne, Steffen; Wörpel, Till; Chandler, Darrell P; Lu, Di; Yang, Tao; Gibbons, Elizabeth; Guerreiro, Rita; Bras, Jose; Thomasen, Martin; Grunnet, Louise G; Vaag, Allan A; Gillberg, Linn; Grundberg, Elin; Conesa, Ana; Körner, Antje; PERMUTE,; Pospisilik, John Andrew

doi:10.1038/s42255-022-00629-2

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Independent phenotypic plasticity axes define distinct obesity sub-types

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Yang, Chih-Hsiang
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

Wegert, Vanessa
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

Panzeri, Ilaria
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

Dror, Erez
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

Heyne, Steffen
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

Wörpel, Till
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

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Pospisilik, John Andrew
Department of Epigenetics, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society;

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Citation

Yang, C.-H., Fagnocchi, L., Apostle, S., Wegert, V., Casaní-Galdón, S., Landgraf, K., et al. (2022). Independent phenotypic plasticity axes define distinct obesity sub-types. Nature Metabolism, 4, 1150-1165. doi:10.1038/s42255-022-00629-2.

Cite as: https://hdl.handle.net/21.11116/0000-000D-10C0-7

Abstract

Studies in genetically 'identical' individuals indicate that as much as 50% of complex trait variation cannot be traced to genetics or to the environment. The mechanisms that generate this 'unexplained' phenotypic variation (UPV) remain largely unknown. Here, we identify neuronatin (NNAT) as a conserved factor that buffers against UPV. We find that Nnat deficiency in isogenic mice triggers the emergence of a bi-stable polyphenism, where littermates emerge into adulthood either 'normal' or 'overgrown'. Mechanistically, this is mediated by an insulin-dependent overgrowth that arises from histone deacetylase (HDAC)-dependent β-cell hyperproliferation. A multi-dimensional analysis of monozygotic twin discordance reveals the existence of two patterns of human UPV, one of which (Type B) phenocopies the NNAT-buffered polyphenism identified in mice. Specifically, Type-B monozygotic co-twins exhibit coordinated increases in fat and lean mass across the body; decreased NNAT expression; increased HDAC-responsive gene signatures; and clinical outcomes linked to insulinemia. Critically, the Type-B UPV signature stratifies both childhood and adult cohorts into four metabolic states, including two phenotypically and molecularly distinct types of obesity.