期刊
EMBO JOURNAL
卷 24, 期 4, 页码 663-673出版社
WILEY
DOI: 10.1038/sj.emboj.7600573
关键词
adenylyl cyclase; crystal structure; half-of-sites-reactivity; Mycobacterium tuberculosis; homodimer
资金
- NIDDK NIH HHS [R56 DK046371, R01 DK046371, DK46371] Funding Source: Medline
Rv1900c, a Mycobacterium tuberculosis adenylyl cyclase, is composed of an N- terminal alpha/beta- hydrolase domain and a C- terminal cyclase homology domain. It has an unusual 7% guanylyl cyclase side- activity. A canonical substrate-defining lysine and a catalytic asparagine indispensable for mammalian adenylyl cyclase activity correspond to N342 and H402 in Rv1900c. Mutagenic analysis indicates that these residues are dispensable for activity of Rv1900c. Structures of the cyclase homology domain, solved to 2.4Angstrom both with and without an ATP analog, form isologous, but asymmetric homodimers. The noncanonical N342 and H402 do not interact with the substrate. Subunits of the unliganded open dimer move substantially upon binding substrate, forming a closed dimer similar to the mammalian cyclase heterodimers, in which one interfacial active site is occupied and the quasi- dyad- related active site is occluded. This asymmetry indicates that both active sites cannot simultaneously be catalytically active. Such a mechanism of half- of- sites- reactivity suggests that mammalian heterodimeric adenylyl cyclases may have evolved from gene duplication of a primitive prokaryote- type cyclase, followed by loss of function in one active site.
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