Gene/Protein
Disease
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Enzyme
Compound
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Gene/Protein
Disease
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Target Concepts:
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Query: EC:2.3.1.21 (
CPT
)
4,580
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Vascular smooth muscle Kv1 delayed rectifier K+ channels (KDR) containing
Kv1.2
control membrane potential and thereby regulate contractility. Vasodilatory agonists acting via protein kinase A (PKA) enhance vascule smooth muscle Kv1 activity, but the molecular basis of this regulation is uncertain. We characterized the role of a C-terminal phosphorylation site, Ser-449, in
Kv1.2
expressed in HEK 293 cells by biochemical and electrophysiological methods. We found that 1) in vitro phosphorylation of
Kv1.2
occurred exclusively at serine residues, 2) one major phosphopeptide that co-migrated with 449pSASTISK was generated by proteolysis of in vitro phosphorylated
Kv1.2
, 3) the peptide 445KKSRSASTISK exhibited stoichiometric phosphorylation by PKA in vitro, 4) matrix-assisted laser desorption ionization time-of-flight (MALDI-TOF) mass spectroscopy (MS) and MS/MS confirmed in vitro Ser-449 phosphorylation by PKA, 5) in situ phosphorylation at Ser-449 was detected in HEK 293 cells by MALDI-TOF MS followed by MS/MS. MIDAS (multiple reaction monitoring-initiated detection and sequencing) analysis revealed additional phosphorylated residues, Ser-440 and Ser-441, 6) in vitro 32P incorporation was significantly reduced in
Kv1.2
-S449A,
Kv1.2
-S449D, and
Kv1.2
-S440A/S441A/S449A mutant channels, but
Kv1.2
-S440A/S441A was identical to wild-type
Kv1.2
(
Kv1.2
-WT), and 7) bath applied 8-Br-cAMP or dialysis with PKA catalytic subunit (cPKA) increased
Kv1.2
-WT but not
Kv1.2
-S449A current amplitude. cPKA increased
Kv1.2
-WT current in inside-out patches. Rp-
CPT
-cAMPS reduced
Kv1.2
-WT current, blocked the increase due to 8-Br-cAMP, but had no effect on
Kv1.2
-S449A. cPKA increased current due to double mutant
Kv1.2
-S440A/S441A but had no effect on
Kv1.2
-S449D or
Kv1.2
-S440A/S441A/S449A. We conclude that Ser-449 in
Kv1.2
is a site of PKA phosphorylation and a potential molecular mechanism for Kv1-containing KDR channel modulation by agonists via PKA activation.
...
PMID:Identification and functional characterization of protein kinase A-catalyzed phosphorylation of potassium channel Kv1.2 at serine 449. 1938 10
