A New Structural Form in the SAM/Metal-Dependent O;#8209;Methyltransferase Family: MycE from the Mycinamicin Biosynthetic Pathway

Akey, David L; Li, Shengying; Konwerski, Jamie R; Confer, Laura A; Bernard, Steffen M; Anzai, Yojiro; Kato, Fumio; Sherman, David H; Smith, Janet L

doi:10.1016/j.jmb.2011.08.040

Title: A New Structural Form in the SAM/Metal-Dependent O;#8209;Methyltransferase Family: MycE from the Mycinamicin Biosynthetic Pathway

Journal Article · Wed Aug 01 00:00:00 EDT 2012 · Journal of Molecular Biology

DOI:https://doi.org/10.1016/j.jmb.2011.08.040· OSTI ID:1046242

Akey, David L; Li, Shengying; Konwerski, Jamie R; Confer, Laura A; Bernard, Steffen M; Anzai, Yojiro; Kato, Fumio; Sherman, David H; Smith, Janet L ^[1]

Michigan

O-linked methylation of sugar substituents is a common modification in the biosynthesis of many natural products and is catalyzed by multiple families of S-adenosyl-l-methionine (SAM or AdoMet)-dependent methyltransferases (MTs). Mycinamicins, potent antibiotics from Micromonospora griseorubida, can be methylated at two positions on a 6-deoxyallose substituent. The first methylation is catalyzed by MycE, a SAM- and metal-dependent MT. Crystal structures were determined for MycE bound to the product S-adenosyl-l-homocysteine (AdoHcy) and magnesium, both with and without the natural substrate mycinamicin VI. This represents the first structure of a natural product sugar MT in complex with its natural substrate. MycE is a tetramer of a two-domain polypeptide, comprising a C-terminal catalytic MT domain and an N-terminal auxiliary domain, which is important for quaternary assembly and for substrate binding. The symmetric MycE tetramer has a novel MT organization in which each of the four active sites is formed at the junction of three monomers within the tetramer. The active-site structure supports a mechanism in which a conserved histidine acts as a general base, and the metal ion helps to position the methyl acceptor and to stabilize a hydroxylate intermediate. A conserved tyrosine is suggested to support activity through interactions with the transferred methyl group from the SAM methyl donor. The structure of the free enzyme reveals a dramatic order-disorder transition in the active site relative to the S-adenosyl-L-homocysteine complexes, suggesting a mechanism for product/substrate exchange through concerted movement of five loops and the polypeptide C-terminus.

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Research Organization:: Argonne National Lab. (ANL), Argonne, IL (United States). Advanced Photon Source (APS)

Sponsoring Organization:: OTHERNIH

OSTI ID:: 1046242

Journal Information:: Journal of Molecular Biology, Vol. 413, Issue 2; ISSN 0022-2836

Country of Publication:: United States

Language:: ENGLISH

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Related Subjects

60 APPLIED LIFE SCIENCES
ANTIBIOTICS
BIOSYNTHESIS
CRYSTAL STRUCTURE
ENZYMES
HISTIDINE
INTERACTIONS
IONS
MAGNESIUM
METALS
METHYLATION
MODIFICATIONS
MONOMERS
POLYPEPTIDES
SACCHAROSE
SUBSTRATES
TYROSINE

Title: A New Structural Form in the SAM/Metal-Dependent O;#8209;Methyltransferase Family: MycE from the Mycinamicin Biosynthetic Pathway

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