4.8 Article

Structural insights into SUN-KASH complexes across the nuclear envelope

Journal

CELL RESEARCH
Volume 22, Issue 10, Pages 1440-1452

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/cr.2012.126

Keywords

crystal structure; SUN2; KASH; LINC complexes; mechanical force transduction; nuclear envelope

Categories

Funding

  1. 973 program of the Ministry of Science and Technology of China [2010CB529701, 2012CB910204]
  2. National Natural Science Foundation of China [30970566, 10979005, 30971647, 31171414]
  3. Shanghai Committee of Science and Technology [11JC14140000]

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Linker of the nucleoskeleton and the cytoskeleton (LINC) complexes are composed of SUN and KASH domain-containing proteins and bridge the inner and outer membranes of the nuclear envelope. LINC complexes play critical roles in nuclear positioning, cell polarization and cellular stiffness. Previously, we reported the homotrimeric structure of human SUN2. We have now determined the crystal structure of the human SUN2-KASH complex. In the complex structure, the SUN domain homotrimer binds to three independent hook-like KASH peptides. The overall conformation of the SUN domain in the complex closely resembles the SUN domain in its apo state. A major conformational change involves the AA'-loop of KASH-bound SUN domain, which rearranges to form a mini beta-sheet that interacts with the KASH peptide. The PPPT motif of the KASH domain fits tightly into a hydrophobic pocket on the homotrimeric interface of the SUN domain, which we termed the BI-pocket. Moreover, two adjacent protomers of the SUN domain homotrimer sandwich the KASH domain by hydrophobic interaction and hydrogen bonding. Mutations of these binding sites disrupt or reduce the association between the SUN and KASH domains in vitro. In addition, transfection of wild-type, but not mutant, SUN2 promotes cell migration in Ovcar-3 cells. These results provide a structural model of the LINC complex, which is essential for additional study of the physical and functional coupling between the cytoplasm and the nucleoplasm.

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