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DETHIOBIOTIN SYNTHETASE - THE CARBONYLATION OF 7,8-DIAMINONONANOIC ACID PROCEEDS REGIOSPECIFICALLY VIA THE N7-CARBAMATE

Authors

GIBSON KJ LORIMER GH RENDINA AR TAYLOR WS COHEN G GATENBY AA PAYNE WG ROE DC LOCKETT BA NUDELMAN A MARCOVICI D NACHUM A WEXLER BA MARSILII EL TURNER IM HOWE LD KALBACH CE CHI HJ

Citation

Kj. Gibson et al., DETHIOBIOTIN SYNTHETASE - THE CARBONYLATION OF 7,8-DIAMINONONANOIC ACID PROCEEDS REGIOSPECIFICALLY VIA THE N7-CARBAMATE, Biochemistry, 34(35), 1995, pp. 10976-10984

Citations number

Categorie Soggetti

Biology

Journal title

Biochemistry → ACNP

ISSN journal

00062960

Volume

Issue

Year of publication

1995

Pages

10976 - 10984

Database

ISI

SICI code

0006-2960(1995)34:35<10976:DS-TCO>2.0.ZU;2-H

Abstract

Dethiobiotin synthetase (DTBS) catalyzes the penultimate step in bioti n biosynthesis, the formation of the ureido ring of dethiobiotin from (7R,8S)-7,8-diaminopelargonic acid (7,8-diaminopelargonic acid, DAPA), CO2, and ATP. Solutions of DAPA at neutral pH readily formed a mixtur e of the N7- and N8-carbamates in the presence of CO2. However, four l ines of evidence together indicated that only the N7-carbamate of DAPA was an intermediate in the reaction catalyzed by DTBS. (1) Addition o f diazomethane to mixtures of DAPA and [C-14]CO2 yielded a mixture of the N7- and N8-methyl carbamate esters, consistent with carbamate form ation in free solution. In the presence of excess DTBS (over DAPA), th e ratio of N7:N8-methyl carbamate esters recovered was roughly doubled , suggesting that the enzyme preferentially bound the N7-DAPA-carbamat e. (2) Both N7- and N8-DAPA-carbamates were observed directly by H-1 a nd C-13 NMR in solutions containing DAPA and [C-13]CO2. In the presenc e of excess DTBS (over DAPA) only one carbamate was observed, showing that carbamate binding to the enzyme was regiospecific. C-13 NMR Of mi xtures containing enzyme, [7-N-15]DAPA, and [C-13]CO2 showed that the enzyme-bound carbamate was at N7 of DAPA. In addition, pulse-chase exp eriments showed that the binary complex of DTBS and N7-DAPA-carbamate became kinetically committed upon addition of MgATP. (3) The N7-DAPA-c arbamate mimic, 3-(1-aminoethyl)nonanedioic acid, in which the carbama te nitrogen was replaced with a methylene group, cyclized to the corre sponding lactam in the presence of DTBS and ATP; ADP and P-i were also formed. The K-M and V-max for this process were comparable to those f or the natural substrate, DAPA. By contrast, the N8w-DAPA-carbamate mi mic, 4-amino-3-methyldecanedioic acid, was a much poorer substrate (V/ K less than or equal to 0.1% of that for DAPA), and the compound was o nly weakly inhibitory. These experiments strongly suggest that DTB is formed predominantly through the N7-carbamate of DAPA. (4) Crystallogr aphic analysis at 1.65 Angstrom resolution of several DTBS-DAPA comple xes also reveals electron density consistent with the presence of a ca rbamate on the 7-amino group [Huang, W., Jia, J., Gibson, K. J., Taylo r, W. S., Rendina, A. R., Schneider, G., & Lindqvist, Y. (1995) Bioche mist 34, 10985-10995].