Database of articles cited by EMDB/PDB/SASBDB data

Keywords
Structure methods	All X-ray diffraction NMR electron microscopy small angle scattering neutron diffraction fiber diffraction powder diffraction infrared spectroscopy EPR fluorescence transfer theoretical model Hybrid
Author
Journal
IF	>30 >20 >10 >5 all

Title	Segmental, Domain-Selective Perdeuteration and Small-Angle Neutron Scattering for Structural Analysis of Multi-Domain Proteins.
Journal, issue, pages	Angew Chem Int Ed Engl, Vol. 56, Issue 32, Page 9322-9325, Year 2017
Publish date	Aug 1, 2017
Authors	Miriam Sonntag / Pravin Kumar Ankush Jagtap / Bernd Simon / Marie-Sousai Appavou / Arie Geerlof / Ralf Stehle / Frank Gabel / Janosch Hennig / Michael Sattler /
PubMed Abstract	Multi-domain proteins play critical roles in fine-tuning essential processes in cellular signaling and gene regulation. Typically, multiple globular domains that are connected by flexible linkers ...Multi-domain proteins play critical roles in fine-tuning essential processes in cellular signaling and gene regulation. Typically, multiple globular domains that are connected by flexible linkers undergo dynamic rearrangements upon binding to protein, DNA or RNA ligands. RNA binding proteins (RBPs) represent an important class of multi-domain proteins, which regulate gene expression by recognizing linear or structured RNA sequence motifs. Here, we employ segmental perdeuteration of the three RNA recognition motif (RRM) domains in the RBP TIA-1 using Sortase A mediated protein ligation. We show that domain-selective perdeuteration combined with contrast-matched small-angle neutron scattering (SANS), SAXS and computational modeling provides valuable information to precisely define relative domain arrangements. The approach is generally applicable to study conformational arrangements of individual domains in multi-domain proteins and changes induced by ligand binding.
External links	Angew Chem Int Ed Engl / PubMed:28636238
Methods	SAS (X-ray in house) / NMR (solution) / X-ray diffraction
Resolution	2.97 Å
Structure data	SASDCC3: Nucleolysin TIA-1 isoform p40 in complex with U15 RNA Method: SAXS/SANS SASDCD3: Nucleolysin TIA-1 isoform p40 (LPQTG containing construct for sortase mediated protein ligation) Method: SAXS/SANS SASDCE3: Nucleolysin TIA-1 isoform p40 in complex with U15 RNA (LPQTG containing construct for sortase mediated protein ligation) Method: SAXS/SANS SASDCF3: Nucleolysin TIA-1 isoform p40 (TIA-1 wild type) Method: SAXS/SANS SASDCG3: Nucleolysin TIA-1 isoform p40 (LPATG containing construct for sortase mediated protein ligation) Method: SAXS/SANS SASDCH3: Nucleolysin TIA-1 isoform p40 in complex with U15 RNA (LPATG containing construct for sortase mediated protein ligation) Method: SAXS/SANS PDB-5o2v: NMR structure of TIA-1 RRM1 domain Method: SOLUTION NMR PDB-5o3j: Crystal structure of TIA-1 RRM2 in complex with RNA Method: X-RAY DIFFRACTION / Resolution: 2.97 Å
Source	homo sapiens (human)
Keywords	RNA BINDING PROTEIN / RRM / TIA-1