Literature DB >> 25587924

Structural insight into MtmC, a bifunctional ketoreductase-methyltransferase involved in the assembly of the mithramycin trisaccharide chain.

Jhong-Min Chen1, Caixia Hou1, Guojun Wang1, Oleg V Tsodikov1, Jürgen Rohr1.   

Abstract

More and more post-PKS tailoring enzymes are recognized as being multifunctional and codependent on other tailoring enzymes. One of the recently discovered intriguing examples is MtmC, a bifunctional TDP-4-keto-d-olivose ketoreductase-methyltransferase, which-in codependence with glycosyltransferase MtmGIV-is a key contributor to the biosynthesis of the critical trisaccharide chain of the antitumor antibiotic mithramycin (MTM), produced by Streptomyces argillaceus. We report crystal structures of three binary complexes of MtmC with its methylation cosubstrate SAM, its coproduct SAH, and a nucleotide TDP as well as crystal structures of two ternary complexes, MtmC-SAH-TDP-4-keto-d-olivose and MtmC-SAM-TDP, in the range of 2.2-2.7 Å resolution. The structures reveal general and sugar-specific recognition and catalytic structural features of MtmC. Depending on the catalytic function that is conducted by MtmC, it must bind either NADPH or SAM in the same cofactor binding pocket. A tyrosine residue (Tyr79) appears as a lid covering the sugar moiety of the substrate during the methyl transfer reaction. This residue swings out of the active site by ~180° in the absence of the substrate. This unique conformational change likely serves to release the methylated product and, possibly, to open the active site for binding the bulkier cosubstrate NADPH prior to the reduction reaction.

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Year:  2015        PMID: 25587924      PMCID: PMC4406830          DOI: 10.1021/bi501462g

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


  32 in total

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Authors:  S Torkkell; T Kunnari; K Palmu; P Mäntsälä; J Hakala; K Ylihonko
Journal:  Mol Genet Genomics       Date:  2001-10       Impact factor: 3.291

2.  The DNA-binding drugs mithramycin and chromomycin are powerful inducers of erythroid differentiation of human K562 cells.

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3.  Deoxysugar transfer during chromomycin A3 biosynthesis in Streptomyces griseus subsp. griseus: new derivatives with antitumor activity.

Authors:  Nuria Menéndez; Mohammad Nur-e-Alam; Carsten Fischer; Alfredo F Braña; José A Salas; Jürgen Rohr; Carmen Méndez
Journal:  Appl Environ Microbiol       Date:  2006-01       Impact factor: 4.792

4.  Elucidation of the glycosylation sequence of mithramycin biosynthesis: isolation of 3A-deolivosylpremithramycin B and its conversion to premithramycin B by glycosyltransferase MtmGII.

Authors:  Mohammad Nur-e-Alam; Carmen Méndez; José A Salas; Jürgen Rohr
Journal:  Chembiochem       Date:  2005-04       Impact factor: 3.164

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7.  The mtmVUC genes of the mithramycin gene cluster in Streptomyces argillaceus are involved in the biosynthesis of the sugar moieties.

Authors:  A González; L L Remsing; F Lombó; M J Fernández; L Prado; A F Braña; E Künzel; J Rohr; C Méndez; J A Salas
Journal:  Mol Gen Genet       Date:  2001-02

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9.  Tailoring modification of deoxysugars during biosynthesis of the antitumour drug chromomycin A by Streptomyces griseus ssp. griseus.

Authors:  Nuria Menéndez; Mohammad Nur-E-Alam; Alfredo F Braña; Jürgen Rohr; José A Salas; Carmen Méndez
Journal:  Mol Microbiol       Date:  2004-08       Impact factor: 3.501

10.  Durhamycin A, a potent inhibitor of HIV Tat transactivation.

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Journal:  J Nat Prod       Date:  2002-08       Impact factor: 4.050

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