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CryoEM structure of MxB reveals a novel oligomerization interface critical for HIV restriction.


ABSTRACT: Human dynamin-like, interferon-induced myxovirus resistance 2 (Mx2 or MxB) is a potent HIV-1 inhibitor. Antiviral activity requires both the amino-terminal region of MxB and protein oligomerization, each of which has eluded structural determination due to difficulties in protein preparation. We report that maltose binding protein-fused, full-length wild-type MxB purifies as oligomers and further self-assembles into helical arrays in physiological salt. Guanosine triphosphate (GTP), but not guanosine diphosphate, binding results in array disassembly, whereas subsequent GTP hydrolysis allows its reformation. Using cryo-electron microscopy (cryoEM), we determined the MxB assembly structure at 4.6 Å resolution, representing the first near-atomic resolution structure in the mammalian dynamin superfamily. The structure revealed previously described and novel MxB assembly interfaces. Mutational analyses demonstrated a critical role for one of the novel interfaces in HIV-1 restriction.

SUBMITTER: Alvarez FJD 

PROVIDER: S-EPMC5600524 | biostudies-literature | 2017 Sep

REPOSITORIES: biostudies-literature

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CryoEM structure of MxB reveals a novel oligomerization interface critical for HIV restriction.

Alvarez Frances J D FJD   He Shaoda S   Perilla Juan R JR   Jang Sooin S   Schulten Klaus K   Engelman Alan N AN   Scheres Sjors H W SHW   Zhang Peijun P  

Science advances 20170915 9


Human dynamin-like, interferon-induced myxovirus resistance 2 (Mx2 or MxB) is a potent HIV-1 inhibitor. Antiviral activity requires both the amino-terminal region of MxB and protein oligomerization, each of which has eluded structural determination due to difficulties in protein preparation. We report that maltose binding protein-fused, full-length wild-type MxB purifies as oligomers and further self-assembles into helical arrays in physiological salt. Guanosine triphosphate (GTP), but not guano  ...[more]

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