TY - JOUR
T1 - Conformational Heterogeneity of Karyopherinβ2 Is Segmental
AU - Cansizoglu, Ahmet E.
AU - Chook, Yuh Min
N1 - Funding Information:
We thank Mischa Machius and Shae Padrick for critical discussions, and Diana Tomchick and Chad Brautigam for expert assistance with data collection. The U.S. Department of Energy, Offices of Science and Basic Energy Sciences (contract W-31-109-ENG-38) supported the Advanced Photon Source use. Y.M.C. is funded by National Institutes of Health grant R01-GM069909, Welch Foundation grant I-1532, and the University of Texas Southwestern Endowed Scholars Program.
PY - 2007/11/13
Y1 - 2007/11/13
N2 - Karyopherinβ2 (Kapβ2) or transportin imports numerous RNA binding proteins into the nucleus. Kapβ2 binds substrates in the cytoplasm and targets them through the nuclear pore complex, where RanGTP dissociates them in the nucleus. Here we report the 3.0 Å crystal structure of unliganded Kapβ2, which consists of a superhelix of 20 HEAT repeats. Together with previously reported structures of NLS and Ran complexes, this structure provides understanding of conformational heterogeneity that accompanies ligand binding. The Kapβ2 superhelix is divided into three major segments. Two of them (HEAT repeats 9-13 and 14-18), which constitute the substrate binding site, are rigid elements that rotate relative to each other about a flexible hinge. The third (HEAT repeats 1-8), which constitutes the Ran binding site, exhibits conformational changes throughout its length. An analogous segmental architecture is also observed in Importinβ, suggesting that it is functionally significant and may be conserved in other import karyopherins.
AB - Karyopherinβ2 (Kapβ2) or transportin imports numerous RNA binding proteins into the nucleus. Kapβ2 binds substrates in the cytoplasm and targets them through the nuclear pore complex, where RanGTP dissociates them in the nucleus. Here we report the 3.0 Å crystal structure of unliganded Kapβ2, which consists of a superhelix of 20 HEAT repeats. Together with previously reported structures of NLS and Ran complexes, this structure provides understanding of conformational heterogeneity that accompanies ligand binding. The Kapβ2 superhelix is divided into three major segments. Two of them (HEAT repeats 9-13 and 14-18), which constitute the substrate binding site, are rigid elements that rotate relative to each other about a flexible hinge. The third (HEAT repeats 1-8), which constitutes the Ran binding site, exhibits conformational changes throughout its length. An analogous segmental architecture is also observed in Importinβ, suggesting that it is functionally significant and may be conserved in other import karyopherins.
KW - CELLBIO
KW - PROTEINS
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U2 - 10.1016/j.str.2007.09.009
DO - 10.1016/j.str.2007.09.009
M3 - Article
C2 - 17997969
AN - SCOPUS:35748960826
SN - 0969-2126
VL - 15
SP - 1431
EP - 1441
JO - Structure
JF - Structure
IS - 11
ER -