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Alternative splicing of the bicistronic gene molybdenum cofactor synthesis 1 (MOCS1) uncovers a novel mitochondrial protein maturation mechanism

J Biol Chem. 2020; 
Mayr SJ, Röper J, Schwarz G,
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PCR Cloning and Subcloning … used for complementation studies Cloning of MOCS1 splice variants Constructs were<br> derived from pRitaIX (kindly provided by J Reiss, Goettingen) (36) whereas exon 1a<br> was synthesized in vitro (<b>GenScript</b>) Based on the published … Get A Quote

摘要

Molybdenum cofactor (Moco) biosynthesis is a highly conserved multistep pathway. The first step, the conversion of GTP to cyclic pyranopterin monophosphate (cPMP), requires the bicistronic gene molybdenum cofactor synthesis 1 (MOCS1). Alternative splicing of MOCS1 within exons 1 and 9 produces four different N-terminal and three different C-terminal products (type I-III). Type I splicing results in bicistronic transcripts with two open reading frames, of which only the first, MOCS1A, is translated, whereas type II/III splicing produces MOCS1AB proteins. Here, we first report the cellular localization of alternatively spliced human MOCS1 proteins. Using fluorescence microscopy, fluorescence spectroscopy, and cel... More

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