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Regulation of ER-mitochondria contacts by Parkin via Mfn2.

Pharmacol. Res.. 2018; 
BassoValentina,MarchesanElena,PeggionCaterina,ChakrabortyJoy,von StockumSophia,GiacomelloMarta,OttoliniDenis,DebattistiValentina,CaicciFederico,TascaElisabetta,PegoraroValentina,AngeliniCorrado,AntoniniAngelo,BertoliAlessandro,BriniMarisa,ZivianiE
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Proteins, Expression, Isolation and Analysis Proteins transferred from the gel matrix to Polyvinylidene difluoride (PVDF) membrane were loaded in ExpressPlus™ PAGE Gel,10×8, 8% (GenScript) or NuPAGE™ 3 -8% Tris-Acetate Protein Gels, 1. Get A Quote

摘要

Parkin, an E3 ubiquitin ligase and a Parkinson's disease (PD) related gene, translocates to impaired mitochondria and drives their elimination via autophagy, a process known as mitophagy. Mitochondrial pro-fusion protein Mitofusins (Mfn1 and Mfn2) were found to be a target for Parkin mediated ubiquitination. Mfns are transmembrane GTPase embedded in the outer membrane of mitochondria, which are required on adjacent mitochondria to mediate fusion. In mammals, Mfn2 also forms complexes that are capable of tethering mitochondria to endoplasmic reticulum (ER), a structural feature essential for mitochondrial energy metabolism, calcium (Ca) transfer between the organelles and Ca dependent cell death. D... More

关键词

Drosophila model of PD,ER-mitochondria synthetic tether,ER-mitochondria tethering,Mitochondria,Mitofusin,PINK1,Parkin,Parkinson’s disease,Ubiquitina