Chihiro Seki scite author profile

Background: Actin dynamics is involved in insulin secretion, but the mechanism is unknown. Results: The G-actin predominant or F-actin remodeling state in pancreatic ␤-cells, which is regulated by the balance of N-WASP and cofilin activities, determines the biphasic glucose-induced insulin secretion (GIIS). Conclusion: Actin dynamics regulated by N-WASP and cofilin underlie the biphasic GIIS. Significance: The regulation of actin dynamics in ␤-cells and its role in GIIS are clarified.

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Characteristics of repaglinide effects on insulin secretion

Takahashi

Hidaka

Seki

et al. 2018

European Journal of Pharmacology

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A Theoretical Analysis of On-Line Learning Using Correlated Examples

Seki

Sakurai

Matsuno

et al. 2008

IEICE Transactions on Fundamentals of Electronics, Communicatio

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A Novel Diphenylthiosemicarbazide Is a Potential Insulin Secretagogue for Anti-Diabetic Agent

et al. 2016

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Insulin secretagogues are used for treatment of type 2 diabetes. We attempted to discover novel small molecules to stimulate insulin secretion by using in silico similarity search using sulfonylureas as query, followed by measurement of insulin secretion. Among 38 compounds selected by in silico similarity search, we found three diphenylsemicarbazides and one quinolone that stimulate insulin secretion. We focused on compound 8 (C8), which had the strongest insulin-secreting effect. Based on the structure-activity relationship of C8-derivatives, we identified diphenylthiosemicarbazide (DSC) 108 as the most potent secretagogue. DSC108 increased the intracellular Ca2+ level in MIN6-K8 cells. Competitive inhibition experiment and electrophysiological analysis revealed sulfonylurea receptor 1 (SUR1) to be the target of DSC108 and that this diphenylthiosemicarbazide directly inhibits ATP-sensitive K+ (KATP) channels. Pharmacokinetic analysis showed that DSC108 has a short half-life in vivo. Oral administration of DSC108 significantly suppressed the rises in blood glucose levels after glucose load in wild-type mice and improved glucose tolerance in the Goto-Kakizaki (GK) rat, a model of type 2 diabetes with impaired insulin secretion. Our data indicate that DSC108 is a novel insulin secretagogue, and is a lead compound for development of a new anti-diabetic agent.

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Magnesium abnormalities in patients in palliative care units

Katayama¹,

Aoe²,

Seki³

et al. 2012

Palliat Care Res

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Chihiro Seki

Actin Dynamics Regulated by the Balance of Neuronal Wiskott-Aldrich Syndrome Protein (N-WASP) and Cofilin Activities Determines the Biphasic Response of Glucose-induced Insulin Secretion

Characteristics of repaglinide effects on insulin secretion

A Theoretical Analysis of On-Line Learning Using Correlated Examples

A Novel Diphenylthiosemicarbazide Is a Potential Insulin Secretagogue for Anti-Diabetic Agent

Magnesium abnormalities in patients in palliative care units

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