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The structure of SSO2064, the first representative of Pfam family PF01796, reveals a novel two‐domain zinc‐ribbon OB‐fold architecture with a potential acyl‐CoA‐binding role
- Krishna, S Sri;
- Aravind, L;
- Bakolitsa, Constantina;
- Caruthers, Jonathan;
- Carlton, Dennis;
- Miller, Mitchell D;
- Abdubek, Polat;
- Astakhova, Tamara;
- Axelrod, Herbert L;
- Chiu, Hsiu-Ju;
- Clayton, Thomas;
- Deller, Marc C;
- Duan, Lian;
- Feuerhelm, Julie;
- Grant, Joanna C;
- Han, Gye Won;
- Jaroszewski, Lukasz;
- Jin, Kevin K;
- Klock, Heath E;
- Knuth, Mark W;
- Kumar, Abhinav;
- Marciano, David;
- McMullan, Daniel;
- Morse, Andrew T;
- Nigoghossian, Edward;
- Okach, Linda;
- Reyes, Ron;
- Rife, Christopher L;
- van den Bedem, Henry;
- Weekes, Dana;
- Xu, Qingping;
- Hodgson, Keith O;
- Wooley, John;
- Elsliger, Marc-André;
- Deacon, Ashley M;
- Godzik, Adam;
- Lesley, Scott A;
- Wilson, Ian A
- et al.
Published Web Location
https://doi.org/10.1107/s1744309110002514Abstract
SSO2064 is the first structural representative of PF01796 (DUF35), a large prokaryotic family with a wide phylogenetic distribution. The structure reveals a novel two-domain architecture comprising an N-terminal, rubredoxin-like, zinc ribbon and a C-terminal, oligonucleotide/oligosaccharide-binding (OB) fold domain. Additional N-terminal helical segments may be involved in protein-protein interactions. Domain architectures, genomic context analysis and functional evidence from certain bacterial representatives of this family suggest that these proteins form a novel fatty-acid-binding component that is involved in the biosynthesis of lipids and polyketide antibiotics and that they possibly function as acyl-CoA-binding proteins. This structure has led to a re-evaluation of the DUF35 family, which has now been split into two entries in the latest Pfam release (v.24.0).
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