Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
10769203 | Biochemical and Biophysical Research Communications | 2005 | 6 Pages |
Abstract
The microtubule interacting and trafficking (MIT) domain is a small protein module of unknown function that is conserved in proteins of diverse function, such as Vps4, sorting nexin 15 (SNX15), and spastin. One non-synonymous single nucleotide polymorphism was reported, which results in a Ile58-to-Met (I58M) substitution in hVps4b. Here, we have determined the solution structure of the MIT domain isolated from the NH2-terminus of human Vps4b, an AAA-ATPase involved in multivesicular body formation. The MIT domain adopts an 'up-and-down' three-helix bundle. Comparison with the sequences of other MIT domains clearly shows that the residues involved in inter-helical contacts are well conserved. The Ile58-to-Met substitution resulted a substantial thermal instability. In addition, we found a shallow crevice between helices A and C that may serve as a protein-binding site. We propose that the MIT domain serves as a putative adaptor domain for the ESCRT-III complex involved in endosomal trafficking.
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Authors
Hirotoshi Takasu, Jun Goo Jee, Ayako Ohno, Natsuko Goda, Kenichiro Fujiwara, Hidehito Tochio, Masahiro Shirakawa, Hidekazu Hiroaki,