Death-associated protein kinase 3 mediates vascular structural remodelling via stimulating smooth muscle cell proliferation and migration

Usui, Tatsuya; Sakatsume, Tomoki; Nijima, Ryo; Otani, Kosuke; Kazama, Kyosuke; Morita, Takae; Kameshima, Satoshi; Okada, Muneyoshi; Yamawaki, Hideyuki

doi:10.1042/cs20130591

Cited by 19 publications

(28 citation statements)

References 31 publications

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“…The data presented herein reveal DI to possess similar efficacy toward both ZIPK and ROCKII activities; nevertheless, the DI compound has been used in two recent studies by Usui and colleagues to assess the role of ZIPK in cardiovascular disease3144. In the first study, the in vivo administration of DI to spontaneously-hypertensive rats was associated with decreases in blood pressure, reactive oxygen species (ROS) production, inflammatory responses, as well as vascular smooth muscle contractility and hypertrophy31.…”

Section: Discussionmentioning

confidence: 96%

“…In vitro treatment of human umbilical vein endothelial cells with DI could also suppress tumor necrosis factor (TNF)α-induced inflammatory responses via ROS-dependent mechanisms. In a second study, the DI compound was used in vitro to link ZIPK with PDGF-BB-induced vascular SMC proliferation and migration through p38MAPK and HSP27 pathways44. Additional in vivo treatments with DI were shown to attenuate vascular structural remodeling during carotid neointimal hyperplasia.…”

Section: Discussionmentioning

confidence: 99%

“…The relationship between ROCKII and COX-2 was previously investigated with results linking ROCKII with the stimulation of COX-2, and subsequent reduction of E-cadherin and α-catenin along with disruption of adherens junction formation and increased cellular motility62. Experimental approaches that applied both siRNA and DI treatments provided links between ZIPK and a group of downstream targets (HSP27, ERK1/2 and p38MAPK) involved in reorganization of the actin cytoskeleton during vascular smooth muscle remodeling44. But, there have been previously described linkages between PDGF-BB-induced SMC hypertrophy and ROCK signaling in studies employing Y2763263.…”

Section: Discussionmentioning

confidence: 99%

“…The in vitro characterization of the 2-phenyl-4-(3-pyridinylmethylene)-5(4H)-oxazolone inhibitor (also known as DI) suggested specificity and potency of this compound toward ZIPK4142. More recent applications of the DI compound in VSM revealed novel functions of ZIPK in (i) development of essential hypertension in mesenteric arteries of the spontaneously hypertensive rat31, and vascular inflammatory and hypertrophic remodeling responses44. Based on these data, we employed the DI compound in studies to define the functional targets of ZIPK in human coronary artery VSMCs, and confirmed that the DI compound possesses potent inhibitory action against ZIPK.…”

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confidence: 99%

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A novel inhibitory effect of oxazol-5-one compounds on ROCKII signaling in human coronary artery vascular smooth muscle cells

Al-Ghabkari

Deng

McDonald³

et al. 2016

Sci Rep

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The selectivity of (4Z)-2-(4-chloro-3-nitrophenyl)-4-(pyridin-3-ylmethylidene)-1,3-oxazol-5-one (DI) for zipper-interacting protein kinase (ZIPK) was previously described by in silico computational modeling, screening a large panel of kinases, and determining the inhibition efficacy. Our assessment of DI revealed another target, the Rho-associated coiled-coil-containing protein kinase 2 (ROCKII). In vitro studies showed DI to be a competitive inhibitor of ROCKII (Ki, 132 nM with respect to ATP). This finding was supported by in silico molecular surface docking of DI with the ROCKII ATP-binding pocket. Time course analysis of myosin regulatory light chain (LC20) phosphorylation catalyzed by ROCKII in vitro revealed a significant decrease upon treatment with DI. ROCKII signaling was investigated in situ in human coronary artery vascular smooth muscle cells (CASMCs). ROCKII down-regulation using siRNA revealed several potential substrates involved in smooth muscle contraction (e.g., LC20, Par-4, MYPT1) and actin cytoskeletal dynamics (cofilin). The application of DI to CASMCs attenuated LC20, Par-4, LIMK, and cofilin phosphorylations. Notably, cofilin phosphorylation was not significantly decreased with a novel ZIPK selective inhibitor (HS-38). In addition, CASMCs treated with DI underwent cytoskeletal changes that were associated with diminution of cofilin phosphorylation. We conclude that DI is not selective for ZIPK and is a potent inhibitor of ROCKII.

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Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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A novel inhibitory effect of oxazol-5-one compounds on ROCKII signaling in human coronary artery vascular smooth muscle cells

Al-Ghabkari

Deng

McDonald³

et al. 2016

Sci Rep

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“…[19] Nachdem wir biochemisch bestätigen konnten, dass Verbindung 2 DAPK3 inhibiert, entwickelten wir ein Strukturmodell, um die biochemischen Daten besser zu verstehen und ein Hit-to-Lead-Programm zu initiieren. Die Blockade von DAPK3 führt zu vaskulärer Umstrukturierung, die bereits für die Unterdrückung der Neointimalhyperplasie in vivo gezeigt werden konnte.…”

Section: Methodsunclassified

De‐novo‐Fragmententwurf für die Wirkstoffforschung und chemische Biologie

et al. 2015

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Automatisiertes De-novo-Moleküldesign führte zur Entdeckung eines neuartigen Inhibitors der Death-Associated Proteinkinase 3( DAPK3). Eine erste Kristallstruktur der inaktiven DAPK3 als Homodimer im Komplex mit dem fragmentartigen Liganden zeigt dessen Bindung in der ATP-Bindetasche.D as verwendete maschinelle Lernverfahren hat neben DAPK3 weitere Targets korrekt vorhergesagt, sowohl für den entworfenen Liganden als auch für den strukturell verwandten und bereits auf dem Markt befindlichen Wirkstoff Azosemid. Die vorliegende Studie bestätigt das Konzeptd es computergestützten ligandenbasierten De-novo-Moleküldesigns als geeignet für die Erzeugungn euartiger Liganden und potentieller Startpunkte für die Wirkstofffindung.Computerbasiertes De-novo-Design neuer chemischer

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De Novo Fragment Design for Drug Discovery and Chemical Biology

et al. 2015

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Automated molecular de novo design led to the discovery of an innovative inhibitor of death-associated protein kinase 3 (DAPK3). An unprecedented crystal structure of the inactive DAPK3 homodimer shows the fragment-like hit bound to the ATP pocket. Target prediction software based on machine learning models correctly identified additional macromolecular targets of the computationally designed compound and the structurally related marketed drug azosemide. The study validates computational de novo design as a prime method for generating chemical probes and starting points for drug discovery.

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Death-associated protein kinase 3 mediates vascular structural remodelling via stimulating smooth muscle cell proliferation and migration

Cited by 19 publications

References 31 publications

A novel inhibitory effect of oxazol-5-one compounds on ROCKII signaling in human coronary artery vascular smooth muscle cells

A novel inhibitory effect of oxazol-5-one compounds on ROCKII signaling in human coronary artery vascular smooth muscle cells

De‐novo‐Fragmententwurf für die Wirkstoffforschung und chemische Biologie

De Novo Fragment Design for Drug Discovery and Chemical Biology

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