Literature DB >> 14992578

Structural basis for differences in substrate selectivity in Kex2 and furin protein convertases.

Todd Holyoak1, Charles A Kettner, Gregory A Petsko, Robert S Fuller, Dagmar Ringe.   

Abstract

Kex2 is the yeast prototype of a large family of serine proteases that are highly specific for cleavage of their peptide substrates C-terminal to paired basic sites. This paper reports the 2.2 A resolution crystal structure of ssKex2 in complex with an Ac-Arg-Glu-Lys-Arg peptidyl boronic acid inhibitor (R = 19.7, R(free) = 23.4). By comparison of this structure with the structure of the mammalian homologue furin [Henrich, S., et al. (2003) Nat. Struct. Biol. 10, 520-526], we suggest a structural basis for the differences in substrate recognition at the P(2) and P(4) positions between Kex2 and furin and provide a structural rationale for the lack of P(6) recognition in Kex2. In addition, several monovalent cation binding sites are identified, and a mechanism of activation of Kex2 by potassium ion is proposed.

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Year:  2004        PMID: 14992578     DOI: 10.1021/bi035849h

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  15 in total

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4.  Structure of the unliganded form of the proprotein convertase furin suggests activation by a substrate-induced mechanism.

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9.  A study of human furin specificity using synthetic peptides derived from natural substrates, and effects of potassium ions.

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10.  A novel enediynyl peptide inhibitor of furin that blocks processing of proPDGF-A, B and proVEGF-C.

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