Literature DB >> 29947926

OSBP-related protein-2 (ORP2): a novel Akt effector that controls cellular energy metabolism.

Henriikka Kentala1, Annika Koponen1, Helena Vihinen2, Juho Pirhonen1,3, Gerhard Liebisch4, Zoltan Pataj4, Annukka Kivelä1, Shiqian Li1,3, Leena Karhinen3, Eeva Jääskeläinen1, Robert Andrews5, Leena Meriläinen2, Silke Matysik4, Elina Ikonen1,3, You Zhou1,5,6, Eija Jokitalo2, Vesa M Olkkonen7,8.   

Abstract

ORP2 is a ubiquitously expressed OSBP-related protein previously implicated in endoplasmic reticulum (ER)-lipid droplet (LD) contacts, triacylglycerol (TG) metabolism, cholesterol transport, adrenocortical steroidogenesis, and actin-dependent cell dynamics. Here, we characterize the role of ORP2 in carbohydrate and lipid metabolism by employing ORP2-knockout (KO) hepatoma cells (HuH7) generated by CRISPR-Cas9 gene editing. The ORP2-KO and control HuH7 cells were subjected to RNA sequencing, analyses of Akt signaling, carbohydrate and TG metabolism, the extracellular acidification rate, and the lipidome, as well as to transmission electron microscopy. The loss of ORP2 resulted in a marked reduction of active phosphorylated Akt(Ser473) and its target Glycogen synthase kinase 3β(Ser9), consistent with defective Akt signaling. ORP2 was found to form a physical complex with the key controllers of Akt activity, Cdc37, and Hsp90, and to co-localize with Cdc37 and active Akt(Ser473) at lamellipodial plasma membrane regions, in addition to the previously reported ER-LD localization. ORP2-KO reduced glucose uptake, glycogen synthesis, glycolysis, mRNA-encoding glycolytic enzymes, and SREBP-1 target gene expression, and led to defective TG synthesis and storage. ORP2-KO did not reduce but rather increased ER-LD contacts under basal culture conditions and interfered with their expansion upon fatty acid loading. Together with our recently published work (Kentala et al. in FASEB J 32:1281-1295, 2018), this study identifies ORP2 as a new regulatory nexus of Akt signaling, cellular energy metabolism, actin cytoskeletal function, cell migration, and proliferation.

Entities:  

Keywords:  Akt signaling; CRISPR-Cas9; Glycolysis; OSBP-related protein; OSBPL2; Triacylglycerol

Mesh:

Substances:

Year:  2018        PMID: 29947926     DOI: 10.1007/s00018-018-2850-8

Source DB:  PubMed          Journal:  Cell Mol Life Sci        ISSN: 1420-682X            Impact factor:   9.261


  55 in total

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Journal:  Cell Metab       Date:  2011-07-06       Impact factor: 27.287

4.  ORP2, a homolog of oxysterol binding protein, regulates cellular cholesterol metabolism.

Authors:  Saara Laitinen; Markku Lehto; Sanna Lehtonen; Kati Hyvärinen; Sanna Heino; Eero Lehtonen; Christian Ehnholm; Elina Ikonen; Vesa M Olkkonen
Journal:  J Lipid Res       Date:  2002-02       Impact factor: 5.922

5.  Combined analysis of oligonucleotide microarray data from transgenic and knockout mice identifies direct SREBP target genes.

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7.  The FATP1-DGAT2 complex facilitates lipid droplet expansion at the ER-lipid droplet interface.

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8.  Endoplasmic reticulum remains continuous and undergoes sheet-to-tubule transformation during cell division in mammalian cells.

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10.  Sterol transfer, PI4P consumption, and control of membrane lipid order by endogenous OSBP.

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5.  OSBPL2 Is Required for the Binding of COPB1 to ATGL and the Regulation of Lipid Droplet Lipolysis.

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  5 in total

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