DB code: S00905

RLCP classification	3.103.78020.387 : Transfer
CATH domain	3.40.1190.20 : UDP-N-acetylmuramoyl-L-alanine	Catalytic domain
E.C.	2.7.1.35
CSA
M-CSA
MACiE

CATH domain	Related DB codes (homologues)
3.40.1190.20 : UDP-N-acetylmuramoyl-L-alanine	S00534 S00541 S00678 S00705 S00903 S00904 S00453 D00416

Uniprot Enzyme Name
UniprotKB	Protein name	Synonyms	RefSeq	Pfam
P39610	Phosphomethylpyrimidine kinase	EC 2.7.4.7 HMP-phosphate kinase HMP-P kinase HMPP kinase	NP_391681.1 (Protein) NC_000964.3 (DNA/RNA sequence)	PF08543 (Phos_pyr_kin) [Graphical View]

KEGG enzyme name
Pyridoxal kinase Pyridoxal kinase (phosphorylating) Pyridoxal 5-phosphate-kinase Pyridoxal phosphokinase Pyridoxine kinase

UniprotKB: Accession Number	Entry name	Activity	Subunit	Subcellular location	Cofactor
P39610	PDXK_BACSU	ATP + pyridoxal = ADP + pyridoxal 5'-phosphate.	Homodimer.

KEGG Pathways
Map code	Pathways	E.C.
MAP00750	Vitamin B6 metabolism

Compound table
	Cofactors	Substrates		Products		Intermediates
KEGG-id	C00305	C00002	C00250	C00008	C00018
E.C.
Compound	Magnesium	ATP	Pyridoxal	ADP	Pyridoxal phosphate
Type	divalent metal (Ca2+, Mg2+)	amine group,nucleotide	aromatic ring (with nitrogen atoms),carbohydrate	amine group,nucleotide	aromatic ring (with nitrogen atoms),phosphate group/phosphate ion
ChEBI	18420 18420	15422 15422	17310 17310	16761 16761	18405 18405
PubChem	888 888	5957 5957	1050 1050	6022 6022	1051 1051

2i5bA00	Unbound	Unbound	Unbound	Bound:ADP	Unbound
2i5bB00	Unbound	Unbound	Unbound	Bound:ADP	Unbound
2i5bC00	Unbound	Unbound	Unbound	Bound:ADP	Unbound
2i5bD00	Unbound	Unbound	Unbound	Bound:ADP	Unbound
2i5bE00	Unbound	Unbound	Unbound	Bound:ADP	Unbound

Reference for Active-site residues
resource	references	E.C.
literature [6], [7]

Active-site residues
PDB	Catalytic residues	Cofactor-binding residues	Modified residues	Main-chain involved in catalysis	Comment

2i5bA00	LYS 182;CYS 216	ASP 107;GLU 144;THR 139(Magnesium binding)		GLY 213;ALA 214;GLY 215;CYS 216
2i5bB00	LYS 182;CYS 216	ASP 107;GLU 144;THR 139(Magnesium binding)		GLY 213;ALA 214;GLY 215;CYS 216
2i5bC00	LYS 182;CYS 216	ASP 107;GLU 144;THR 139(Magnesium binding)		GLY 213;ALA 214;GLY 215;CYS 216
2i5bD00	LYS 182;CYS 216	ASP 107;GLU 144;THR 139(Magnesium binding)		GLY 213;ALA 214;GLY 215;CYS 216
2i5bE00	LYS 182;CYS 216	ASP 107;GLU 144;THR 139(Magnesium binding)		GLY 213;ALA 214;GLY 215;CYS 216

References for Catalytic Mechanism
References	Sections	No. of steps in catalysis
[6]	Fig.6, p1815-1816
[7]	Fig.2, p.525

References
[1]
Resource
Comments	X-RAY CRYSTALLOGRAPHY (1.84 ANGSTROMS).
Medline ID
PubMed ID	9519409
Journal	Structure
Year	1998
Volume	6
Pages	183-93
Authors	Sigrell JA, Cameron AD, Jones TA, Mowbray SL
Title	Structure of Escherichia coli ribokinase in complex with ribose and dinucleotide determined to 1.8 A resolution: insights into a new family of kinase structures.
Related PDB	1rkd
Related UniProtKB	P0A9J6
[2]
Resource
Comments	X-RAY CRYSTALLOGRAPHY (1.5 ANGSTROMS) IN COMPLEX WITH SUBSTRATE, HOMOTRIMERIZATION, AND MUTAGENESIS OF CYS-198.
Medline ID
PubMed ID	10891066
Journal	Biochemistry
Year	2000
Volume	39
Pages	7868-77
Authors	Campobasso N, Mathews II, Begley TP, Ealick SE
Title	Crystal structure of 4-methyl-5-beta-hydroxyethylthiazole kinase from Bacillus subtilis at 1.5 A resolution.
Related PDB	1c3q 1esq 1esj 1ekq 1ekk
Related UniProtKB	P39593
[3]
Resource
Comments	X-RAY CRYSTALLOGRAPHY (2.3 ANGSTROMS) OF 23-266.
Medline ID
PubMed ID	11839308
Journal	Structure
Year	2002
Volume	10
Pages	225-35
Authors	Cheng G, Bennett EM, Begley TP, Ealick SE
Title	Crystal structure of 4-amino-5-hydroxymethyl-2-methylpyrimidine phosphate kinase from Salmonella typhimurium at 2.3 A resolution.
Related PDB	1jxh 1jxi
Related UniProtKB	P55882
[4]
Resource
Comments
Medline ID
PubMed ID	14675553
Journal	Curr Opin Struct Biol
Year	2003
Volume	13
Pages	739-47
Authors	Settembre E, Begley TP, Ealick SE
Title	Structural biology of enzymes of the thiamin biosynthesis pathway.
Related PDB
Related UniProtKB
[5]
Resource
Comments
Medline ID
PubMed ID
Journal	Int J Mol Sci
Year	2004
Volume	5
Pages	141-153
Authors	Edyta Dyguda, Borys Szefczyk and W. A. Sokalski
Title	The Mechanism of Phosphoryl Transfer Reaction and the Role of Active Site Residues on the Basis of Ribokinase-Like Kinases
Related PDB
Related UniProtKB
[6]
Resource
Comments	X-RAY CRYSTALLOGRAPHY (2.6 ANGSTROMS).
Medline ID
PubMed ID	15458630
Journal	Structure
Year	2004
Volume	12
Pages	1809-21
Authors	Zhang Y, Dougherty M, Downs DM, Ealick SE
Title	Crystal structure of an aminoimidazole riboside kinase from Salmonella enterica: implications for the evolution of the ribokinase superfamily.
Related PDB	1tyy 1tz3 1tz6
Related UniProtKB	Q8ZKR2
[7]
Resource
Comments
Medline ID
PubMed ID	16978644
Journal	J Mol Biol
Year	2006
Volume	363
Pages	520-30
Authors	Newman JA, Das SK, Sedelnikova SE, Rice DW
Title	The crystal structure of an ADP complex of Bacillus subtilis pyridoxal kinase provides evidence for the parallel emergence of enzyme activity during evolution.
Related PDB	2i5b
Related UniProtKB

Comments
This enzyme belongs to the ribokinase superfamily (EC 2.7.1.15, S00534 & S00541 in EzCatDB)(see [3]). In particular, this enzyme is homologous to HMP kinase (S00705 in EzCatDB). According to the literature [7], Cys216 is too weak to act as a general base. The reaction mechanism must be similar to that of HMP kinase (see S00705). Thus, this enzyme catalyzes the following reaction (see [7]): (0) Magnesium ion, which is bound to Asp107, Glu144 and mainchain carbonyl oxygen of Thr139, coordinates with both the alpha- and beta-phosphate groups of ATP, thereby stabilizing ADP as a leaving group. Moreover, anion hole composed of mainchain amide groups of Gly213-Ala214-Gly215-Cys216 stabilizes the beta- and gamma-phosphate groups, whereas sidechain of Lys182 may stabilize alpha- and beta-phosphate groups. Thereby, the transition state in the reaction can be stabilized. (1) An oxygen atom of gamma-phosphate group of ATP acts as a general base to deprotonate the hydroxyl group of pyridoxal. (2) The activated hydroxyl oxygen of pyridoxal makes a nucleophilic attack on the gamma-phosphate of ATP, to produce pyridoxal phosphate. This reaction proceeds via SN2 mechanism.

Comments

This enzyme belongs to the ribokinase superfamily (EC 2.7.1.15, S00534 & S00541 in EzCatDB)(see [3]). In particular, this enzyme is homologous to HMP kinase (S00705 in EzCatDB).
According to the literature [7], Cys216 is too weak to act as a general base. The reaction mechanism must be similar to that of HMP kinase (see S00705).
Thus, this enzyme catalyzes the following reaction (see [7]):
(0) Magnesium ion, which is bound to Asp107, Glu144 and mainchain carbonyl oxygen of Thr139, coordinates with both the alpha- and beta-phosphate groups of ATP, thereby stabilizing ADP as a leaving group. Moreover, anion hole composed of mainchain amide groups of Gly213-Ala214-Gly215-Cys216 stabilizes the beta- and gamma-phosphate groups, whereas sidechain of Lys182 may stabilize alpha- and beta-phosphate groups. Thereby, the transition state in the reaction can be stabilized.
(1) An oxygen atom of gamma-phosphate group of ATP acts as a general base to deprotonate the hydroxyl group of pyridoxal.
(2) The activated hydroxyl oxygen of pyridoxal makes a nucleophilic attack on the gamma-phosphate of ATP, to produce pyridoxal phosphate. This reaction proceeds via SN2 mechanism.

Created	Updated
2009-08-28	2011-11-22