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The NHL domain of BRAT is an RNA-binding domain that directly contacts the hunchback mRNA for regulation

Titelangaben

Loedige, Inga ; Stotz, Mathias ; Qamar, Saadia ; Kramer, Katharina ; Hennig, Janosch ; Schubert, Thomas ; Löffler, Patrick ; Längst, Gernot ; Merkl, Rainer ; Urlaub, Henning ; Meister, Gunter:
The NHL domain of BRAT is an RNA-binding domain that directly contacts the hunchback mRNA for regulation.
In: Genes & Development. Bd. 28 (2014) Heft 7 . - S. 749-764.
ISSN 1549-5477
DOI: https://doi.org/10.1101/gad.236513.113

Abstract

The Drosophila protein brain tumor (Brat) forms a complex with Pumilio (Pum) and Nanos (Nos) to repress hunchback (hb) mRNA translation at the posterior pole during early embryonic development. It is currently thought that complex formation is initiated by Pum, which directly binds the hb mRNA and subsequently recruits Nos and Brat. Here we report that, in addition to Pum, Brat also directly interacts with the hb mRNA. We identify Brat-binding sites distinct from the Pum consensus motif and show that RNA binding and translational repression by Brat do not require Pum, suggesting so far unrecognized Pum-independent Brat functions. Using various biochemical and biophysical methods, we also demonstrate that the NHL (NCL-1, HT2A, and LIN-41) domain of Brat, a domain previously believed to mediate protein–protein interactions, is a novel, sequence-specific ssRNA-binding domain. The Brat-NHL domain folds into a six-bladed β propeller, and we identify its positively charged top surface as the RNA-binding site. Brat belongs to the functional diverse TRIM (tripartite motif)-NHL protein family. Using structural homology modeling, we predict that the NHL domains of all TRIM-NHL proteins have the potential to bind RNA, indicating that Brat is part of a conserved family of RNA-binding proteins.

Weitere Angaben

Publikationsform: Artikel in einer Zeitschrift
Begutachteter Beitrag: Ja
Keywords: BRAT; RNA binding; TRIM-NHL; gene regulation; hunchback; translational repression
Institutionen der Universität: Fakultäten > Fakultät für Biologie, Chemie und Geowissenschaften > Fachgruppe Chemie > Lehrstuhl Biochemie IV - Biophysikalische Chemie > Lehrstuhl Biochemie IV - Biophysikalische Chemie - Univ.-Prof. Dr. Janosch Hennig
Fakultäten
Fakultäten > Fakultät für Biologie, Chemie und Geowissenschaften
Fakultäten > Fakultät für Biologie, Chemie und Geowissenschaften > Fachgruppe Chemie
Fakultäten > Fakultät für Biologie, Chemie und Geowissenschaften > Fachgruppe Chemie > Lehrstuhl Biochemie IV - Biophysikalische Chemie
Forschungseinrichtungen > Zentrale wissenschaftliche Einrichtungen > Nordbayerisches Zentrum für NMR-Spektroskopie - NMR-Zentrum
Titel an der UBT entstanden: Nein
Themengebiete aus DDC: 500 Naturwissenschaften und Mathematik > 540 Chemie
500 Naturwissenschaften und Mathematik > 570 Biowissenschaften; Biologie
Eingestellt am: 07 Okt 2021 13:38
Letzte Änderung: 26 Sep 2024 07:27
URI: https://eref.uni-bayreuth.de/id/eprint/67246