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Adipogenin promotes the development of lipid droplets by binding a dodecameric seipin complex

Author(s)
Li, ChaoSun, Xue-NanFuncke, Jan-BerndVanharanta, LauriPrasanna, XavierGov, KaitlynnLi, YanVirostek, MeganJoung, ChanminJoffin, NolwennKanerva, KristiinaSzkalisity, AbelKulig, WaldemarStraub, LeonChen, ShiuhweiVelasco, JoselinCobb, AyannaLa Padula, DavideWang, May-YunOnodera, ToshiharuVoros, CsabaKim, Dae-SeokKim, MinVarlamov, OlegLi, YangLiu, ChenNawrocki, Andrea R.Zhao, ShangangOh, Da YoungWang, Zhao V.Gordillo, RuthGoodman, Joel M.Wynn, R. MaxHenne, W. MikeVattulainen, IlpoHan, YanIkonen, ElinaScherer, Philipp E.
Issued Date
2025-11
DOI
10.1126/science.adr9755
URI
https://scholarworks.unist.ac.kr/handle/201301/91388
Fulltext
https://www.science.org/doi/10.1126/science.adr9755
Citation
SCIENCE, v.390, no.6773, pp.eadr9755
Abstract
The microprotein adipogenin (Adig) is predominantly expressed in adipose tissues. Here, we found that Adig interacts with seipin to form a stable, rigid complex. We present the structure of the seipin-Adig complex at an overall resolution of similar to 3.0 angstroms. The structure revealed that mammalian seipin assembles into two distinct oligomeric forms: undecamers and dodecamers. Adig selectively bound to the dodecameric form and enhanced seipin assembly by bridging and stabilizing adjacent subunits. Functionally, this complex promoted lipid droplet development at both early and late stages. In transgenic mice, adipocyte-specific overexpression of Adig increased fat mass and enlarged lipid droplets, whereas Adig deletion disrupted triglyceride accumulation in brown adipose tissues. Thus, Adig can modulate lipid storage through its structural and functional interactions with seipin.
Publisher
AMER ASSOC ADVANCEMENT SCIENCE
ISSN
0036-8075
Keyword
BIOGENESISCONGENITAL LIPODYSTROPHY 2/SEIPINPROTEINMOLPROBITYEXPRESSIONDYNAMICS

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