Publication Abstract from PubMed
Period (PER) is the major transcription inhibitor in metazoan circadian clocks and lies at the center of several feedback loops that regulate gene expression. Dimerization of Drosophila PER influences nuclear translocation, repressor activity, and behavioral rhythms. The structure of a central, 346-residue PER fragment reveals two associated PAS (Per-Arnt-Sim) domains followed by a protruding alpha-helical extension (alphaF). A closed, pseudo-symmetric dimer forms from a cross handshake interaction of the N-terminal PAS domain with alphaF of the opposing subunit. Strikingly, a shift of alphaF against the PAS beta-sheet generates two alternative subunit interfaces in the dimer. Taken together with a previously reported PER structure in which alphaF extends, these data indicate that alphaF unlatches to switch association of PER with itself to its partner Timeless. The variable positions of the alphaF helix provide snapshots of a helix dissociation mechanism that has relevance to other PAS protein systems. Conservation of PER interaction residues among a family of PAS-AB-containing transcription factors suggests that contacts mediating closed PAS-AB dimers serve a general function.
Structure of an enclosed dimer formed by the Drosophila period protein.,King HA, Hoelz A, Crane BR, Young MW J Mol Biol. 2011 Oct 28;413(3):561-72. Epub 2011 Sep 3. PMID:21907720[1]
From MEDLINE®/PubMed®, a database of the U.S. National Library of Medicine.
