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PDBsum entry 1j3h
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Contents |
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* Residue conservation analysis
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Enzyme class:
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E.C.2.7.11.11
- cAMP-dependent protein kinase.
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Reaction:
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1.
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L-seryl-[protein] + ATP = O-phospho-L-seryl-[protein] + ADP + H+
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2.
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L-threonyl-[protein] + ATP = O-phospho-L-threonyl-[protein] + ADP + H+
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L-seryl-[protein]
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+
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ATP
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=
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O-phospho-L-seryl-[protein]
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+
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ADP
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+
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H(+)
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L-threonyl-[protein]
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+
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ATP
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=
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O-phospho-L-threonyl-[protein]
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+
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ADP
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+
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H(+)
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Molecule diagrams generated from .mol files obtained from the
KEGG ftp site
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DOI no:
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J Mol Biol
327:159-171
(2003)
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PubMed id:
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Dynamic features of cAMP-dependent protein kinase revealed by apoenzyme crystal structure.
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P.Akamine,
Madhusudan,
J.Wu,
N.H.Xuong,
L.F.Ten Eyck,
S.S.Taylor.
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ABSTRACT
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To better understand the mechanism of ligand binding and ligand-induced
conformational change, the crystal structure of apoenzyme catalytic (C) subunit
of adenosine-3',5'-cyclic monophosphate (cAMP)-dependent protein kinase (PKA)
was solved. The apoenzyme structure (Apo) provides a snapshot of the enzyme in
the first step of the catalytic cycle, and in this unliganded form the PKA C
subunit adopts an open conformation. A hydrophobic junction is formed by
residues from the small and large lobes that come into close contact. This
"greasy" patch may lubricate the shearing motion associated with
domain rotation, and the opening and closing of the active-site cleft. Although
Apo appears to be quite dynamic, many important residues for MgATP binding and
phosphoryl transfer in the active site are preformed. Residues around the
adenine ring of ATP and residues involved in phosphoryl transfer from the large
lobe are mostly preformed, whereas residues involved in ribose binding and in
the Gly-rich loop are not. Prior to ligand binding, Lys72 and the C-terminal
tail, two important ATP-binding elements are also disordered. The surface
created in the active site is contoured to bind ATP, but not GTP, and appears to
be held in place by a stable hydrophobic core, which includes helices C, E, and
F, and beta strand 6. This core seems to provide a network for communicating
from the active site, where nucleotide binds, to the peripheral peptide-binding
F-to-G helix loop, exemplified by Phe239. Two potential lines of communication
are the D helix and the F helix. The conserved Trp222-Phe238 network, which lies
adjacent to the F-to-G helix loop, suggests that this network would exist in
other protein kinases and may be a conserved means of communicating ATP binding
from the active site to the distal peptide-binding ledge.
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Selected figure(s)
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Figure 1.
Figure 1. (A) ApoA and ApoB superimposed. The two molecules
in the asymmetric unit are superimposed to show that they differ
in overall domain rotation. ApoA is black and ApoB is gold.
Broken lines are distances of representative areas of the small
lobe. The distance between the Ser53 C^a atoms, in the Gly-rich
loop, is 1.9 Å. The distance between the C^a atoms of
Ser339 is 3.4 Å. An MPD molecule and a covalently attached
b-ME group were seen in both structures. The ApoA MPD and b-ME
modified Cys199 are pink. Residues 128-300 were superimposed.
(B) The F[o] -F[c] omit map of Cys199 and the covalently
attached b-ME, contoured at 3s. Oxygen, red; nitrogen, blue;
carbon, gray; sulfur, green.
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Figure 2.
Figure 2. (A) Closed conformation and ApoA. Superposition
of ApoA (black) and C:AlF:SP20 (green),[9] in the open and
closed conformations, respectively. Broken lines show the
distances of two representative parts of the small lobe; the
Gly-rich loop (Ser53 C^a) and the C-terminal tail (Ser339 C^a).
Residues 128-300 were superimposed. (B) Intralobe hydrophobic
contacts. The hydrophobic patch between the small and large
lobes, which may provide the "grease" for the shearing motion
associated with domain rotation, is shown. Glu91, a conserved
residue in the C helix (C), which is important for orienting the
phosphate groups of ATP during phosphoryl transfer, is preformed
and is within hydrogen-bonding distance from the amide hydrogen
atom of Phe185 in the large lobe. From the small lobe (gold
ribbon) are residues Glu91, Ile94, Val98, Phe100, Phe102,
Leu103, and Val104 (side-chains, blue). From the large lobe, the
residues shown are Thr153, Tyr156, Leu162, Tyr179, Gln181, and
Phe185 (side-chains, pink). Residues that come into close
contact are Ile94-Leu162, Phe185; Val98, Phe100 and
Leu103-Tyr156, Leu103-Phe185, and Val104-Gln181. Other hydrogen
bonding pairs are: Asn99 amide group to Tyr156 hydroxyl group,
and Val104 amide hydrogen atom to Val182 carbonyl oxygen atom.
The gray ribbon represents the E helix (E) and the black ribbon
includes the Mg-positioning loop (Mg), both from the large lobe.
Helix A (A) is shown, since Phe18, Ala22, and Phe26 contribute,
peripherally.
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The above figures are
reprinted
by permission from Elsevier:
J Mol Biol
(2003,
327,
159-171)
copyright 2003.
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Figures were
selected
by an automated process.
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Literature references that cite this PDB file's key reference
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PubMed id
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Reference
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S.S.Taylor,
and
A.P.Kornev
(2011).
Protein kinases: evolution of dynamic regulatory proteins.
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Trends Biochem Sci,
36,
65-77.
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A.C.Newton
(2010).
Protein kinase C: poised to signal.
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Am J Physiol Endocrinol Metab,
298,
E395-E402.
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J.M.Steichen,
G.H.Iyer,
S.Li,
S.A.Saldanha,
M.S.Deal,
V.L.Woods,
and
S.S.Taylor
(2010).
Global consequences of activation loop phosphorylation on protein kinase A.
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J Biol Chem,
285,
3825-3832.
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N.Brooijmans,
Y.W.Chang,
D.Mobilio,
R.A.Denny,
and
C.Humblet
(2010).
An enriched structural kinase database to enable kinome-wide structure-based analyses and drug discovery.
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Protein Sci,
19,
763-774.
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T.Li,
P.Du,
and
N.Xu
(2010).
Identifying human kinase-specific protein phosphorylation sites by integrating heterogeneous information from various sources.
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PLoS One,
5,
e15411.
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T.Takimura,
K.Kamata,
K.Fukasawa,
H.Ohsawa,
H.Komatani,
T.Yoshizumi,
I.Takahashi,
H.Kotani,
and
Y.Iwasawa
(2010).
Structures of the PKC-iota kinase domain in its ATP-bound and apo forms reveal defined structures of residues 533-551 in the C-terminal tail and their roles in ATP binding.
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Acta Crystallogr D Biol Crystallogr,
66,
577-583.
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PDB codes:
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U.Bjarnadottir,
and
J.E.Nielsen
(2010).
Calculating pKa values in the cAMP-dependent protein kinase: the effect of conformational change and ligand binding.
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Protein Sci,
19,
2485-2497.
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Y.H.Hsu,
and
J.A.Traugh
(2010).
Reciprocally coupled residues crucial for protein kinase Pak2 activity calculated by statistical coupling analysis.
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PLoS One,
5,
e9455.
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E.J.Kennedy,
J.Yang,
L.Pillus,
S.S.Taylor,
and
G.Ghosh
(2009).
Identifying critical non-catalytic residues that modulate protein kinase A activity.
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PLoS ONE,
4,
e4746.
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F.Xu,
P.Du,
H.Shen,
H.Hu,
Q.Wu,
J.Xie,
and
L.Yu
(2009).
Correlated mutation analysis on the catalytic domains of serine/threonine protein kinases.
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PLoS One,
4,
e5913.
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I.V.Khavrutskii,
B.Grant,
S.S.Taylor,
and
J.A.McCammon
(2009).
A transition path ensemble study reveals a linchpin role for Mg(2+) during rate-limiting ADP release from protein kinase A.
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Biochemistry,
48,
11532-11545.
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J.Yang,
E.J.Kennedy,
J.Wu,
M.S.Deal,
J.Pennypacker,
G.Ghosh,
and
S.S.Taylor
(2009).
Contribution of Non-catalytic Core Residues to Activity and Regulation in Protein Kinase A.
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J Biol Chem,
284,
6241-6248.
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PDB code:
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Z.Huang,
and
C.F.Wong
(2009).
Conformational selection of protein kinase A revealed by flexible-ligand flexible-protein docking.
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J Comput Chem,
30,
631-644.
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E.J.Kennedy,
G.Ghosh,
and
L.Pillus
(2008).
Identification of functionally distinct regions that mediate biological activity of the protein kinase a homolog Tpk2.
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J Biol Chem,
283,
1084-1093.
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J.Eswaran,
M.Soundararajan,
R.Kumar,
and
S.Knapp
(2008).
UnPAKing the class differences among p21-activated kinases.
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Trends Biochem Sci,
33,
394-403.
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J.Pérez,
A.Castañeda-García,
H.Jenke-Kodama,
R.Müller,
and
J.Muñoz-Dorado
(2008).
Eukaryotic-like protein kinases in the prokaryotes and the myxobacterial kinome.
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Proc Natl Acad Sci U S A,
105,
15950-15955.
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P.Singh,
B.Wang,
T.Maeda,
K.Palczewski,
and
J.J.Tesmer
(2008).
Structures of rhodopsin kinase in different ligand states reveal key elements involved in G protein-coupled receptor kinase activation.
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J Biol Chem,
283,
14053-14062.
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PDB codes:
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S.S.Taylor,
C.Kim,
C.Y.Cheng,
S.H.Brown,
J.Wu,
and
N.Kannan
(2008).
Signaling through cAMP and cAMP-dependent protein kinase: diverse strategies for drug design.
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Biochim Biophys Acta,
1784,
16-26.
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T.Li,
F.Li,
and
X.Zhang
(2008).
Prediction of kinase-specific phosphorylation sites with sequence features by a log-odds ratio approach.
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Proteins,
70,
404-414.
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A.J.Caplan,
A.K.Mandal,
and
M.A.Theodoraki
(2007).
Molecular chaperones and protein kinase quality control.
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Trends Cell Biol,
17,
87-92.
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F.S.Domingues,
J.Rahnenführer,
and
T.Lengauer
(2007).
Conformational analysis of alternative protein structures.
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Bioinformatics,
23,
3131-3138.
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J.Wu,
S.H.Brown,
S.von Daake,
and
S.S.Taylor
(2007).
PKA type IIalpha holoenzyme reveals a combinatorial strategy for isoform diversity.
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Science,
318,
274-279.
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PDB code:
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N.Kannan,
N.Haste,
S.S.Taylor,
and
A.F.Neuwald
(2007).
The hallmark of AGC kinase functional divergence is its C-terminal tail, a cis-acting regulatory module.
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Proc Natl Acad Sci U S A,
104,
1272-1277.
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N.Kannan,
S.S.Taylor,
Y.Zhai,
J.C.Venter,
and
G.Manning
(2007).
Structural and functional diversity of the microbial kinome.
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PLoS Biol,
5,
e17.
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Y.Yan,
H.Nguyen,
G.Dalmasso,
S.V.Sitaraman,
and
D.Merlin
(2007).
Cloning and characterization of a new intestinal inflammation-associated colonic epithelial Ste20-related protein kinase isoform.
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Biochim Biophys Acta,
1769,
106-116.
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A.Tomono,
M.Mashiko,
T.Shimazu,
H.Inoue,
H.Nagasawa,
M.Yoshida,
Y.Ohnishi,
and
S.Horinouchi
(2006).
Self-activation of serine/threonine kinase AfsK on autophosphorylation at threonine-168.
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J Antibiot (Tokyo),
59,
117-123.
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C.F.Wong,
J.Kua,
Y.Zhang,
T.P.Straatsma,
and
J.A.McCammon
(2005).
Molecular docking of balanol to dynamics snapshots of protein kinase A.
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Proteins,
61,
850-858.
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J.Wu,
J.Yang,
N.Kannan,
Madhusudan,
N.H.Xuong,
L.F.Ten Eyck,
and
S.S.Taylor
(2005).
Crystal structure of the E230Q mutant of cAMP-dependent protein kinase reveals an unexpected apoenzyme conformation and an extended N-terminal A helix.
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Protein Sci,
14,
2871-2879.
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PDB code:
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U.Schieborr,
M.Vogtherr,
B.Elshorst,
M.Betz,
S.Grimme,
B.Pescatore,
T.Langer,
K.Saxena,
and
H.Schwalbe
(2005).
How much NMR data is required to determine a protein-ligand complex structure?
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Chembiochem,
6,
1891-1898.
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M.Gassel,
C.B.Breitenlechner,
N.König,
R.Huber,
R.A.Engh,
and
D.Bossemeyer
(2004).
The protein kinase C inhibitor bisindolyl maleimide 2 binds with reversed orientations to different conformations of protein kinase A.
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J Biol Chem,
279,
23679-23690.
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PDB code:
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M.Y.Niv,
H.Rubin,
J.Cohen,
L.Tsirulnikov,
T.Licht,
A.Peretzman-Shemer,
E.Cna'an,
A.Tartakovsky,
I.Stein,
S.Albeck,
I.Weinstein,
M.Goldenberg-Furmanov,
D.Tobi,
E.Cohen,
M.Laster,
S.A.Ben-Sasson,
and
H.Reuveni
(2004).
Sequence-based design of kinase inhibitors applicable for therapeutics and target identification.
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J Biol Chem,
279,
1242-1255.
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T.Langer,
M.Vogtherr,
B.Elshorst,
M.Betz,
U.Schieborr,
K.Saxena,
and
H.Schwalbe
(2004).
NMR backbone assignment of a protein kinase catalytic domain by a combination of several approaches: application to the catalytic subunit of cAMP-dependent protein kinase.
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Chembiochem,
5,
1508-1516.
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C.Breitenlechner,
M.Gassel,
H.Hidaka,
V.Kinzel,
R.Huber,
R.A.Engh,
and
D.Bossemeyer
(2003).
Protein kinase A in complex with Rho-kinase inhibitors Y-27632, Fasudil, and H-1152P: structural basis of selectivity.
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Structure,
11,
1595-1607.
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PDB codes:
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The most recent references are shown first.
Citation data come partly from CiteXplore and partly
from an automated harvesting procedure. Note that this is likely to be
only a partial list as not all journals are covered by
either method. However, we are continually building up the citation data
so more and more references will be included with time.
Where a reference describes a PDB structure, the PDB
codes are
shown on the right.
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Links
