A Chlamydia trachomatisUDP-N-Acetylglucosamine Acyltransferase Selective for Myristoyl-Acyl Carrier Protein

Abstract: Chlamydia trachomatis lipid A is unusual in that it is acylated with myristoyl chains at the glucosamine 3 and 3 positions. We have cloned and expressed the gene encoding UDP-N-acetylglucosamine 3-O-acyltransferase of C. trachomatis (CtlpxA), the first enzyme of lipid A biosynthesis. C. trachomatis LpxA displays ϳ20-fold selectivity for myristoyl-ACP over R/S-3-hydroxymyristoyl-ACP under standard assay conditions, consistent with the proposed structure of C. trachomatis lipid A. CtLpxA is the first reported UD… Show more

“…The in vitro fatty acyl chain length selectivity of these LpxA orthologues is consistent with the structures of the lipid A molecules isolated from E. coli and P. aeruginosa (2). The only known LpxA variant that does not require R-3-hydroxyacyl-ACP is that of Chlamydia trachomatis, which shows a strong preference for myristoyl-ACP over R-3-hydroxymyristoyl-ACP (21). E. coli LpxA is inhibited by myristoyl-ACP (8).…”

“…4). Interestingly, H99 is replaced by threonine in C. trachomatis LpxA (21). This substitution may account for loss of R-3-hydroxyacyl chain selectivity, because threonine cannot replace histidine as a hydrogen-bonding partner.…”

Structural basis for the acyl chain selectivity and mechanism of UDP- N -acetylglucosamine acyltransferase

“…The in vitro fatty acyl chain length selectivity of these LpxA orthologues is consistent with the structures of the lipid A molecules isolated from E. coli and P. aeruginosa (2). The only known LpxA variant that does not require R-3-hydroxyacyl-ACP is that of Chlamydia trachomatis, which shows a strong preference for myristoyl-ACP over R-3-hydroxymyristoyl-ACP (21). E. coli LpxA is inhibited by myristoyl-ACP (8).…”

“…4). Interestingly, H99 is replaced by threonine in C. trachomatis LpxA (21). This substitution may account for loss of R-3-hydroxyacyl chain selectivity, because threonine cannot replace histidine as a hydrogen-bonding partner.…”

Structural basis for the acyl chain selectivity and mechanism of UDP- N -acetylglucosamine acyltransferase

“…The acyl-ACP donor selectivity of LpxA has previously been studied in several systems (8,17,24,(35)(36)(37). In general, LpxA orthologs show strong preferences for acyl chain length and the presence of the R-3-hydroxyl group (8,17,24,(35)(36)(37).…”

“…In general, LpxA orthologs show strong preferences for acyl chain length and the presence of the R-3-hydroxyl group (8,17,24,(35)(36)(37). The corresponding coenzyme A thioesters are not substrates (8,25).…”

“…Furthermore, LiLpxA does not acylate UDP-GlcNAc3N with any donor other than 3-hydroxylauroyl-ACP. Although most other LpxA proteins display a high degree of specificity for a particular acyl chain length, they do in fact function with alternative acyl donors at slow rates (Tables II and III) (8,17,24,35,37).…”

Enzymatic Synthesis of Lipid A Molecules with Four Amide-linked Acyl Chains

Acyl-[acyl-carrier-protein]-UDP-N-acetylglucosamine O-acyltransferase