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Insulin: The Receptor and Signaling Pathways01:28

Insulin: The Receptor and Signaling Pathways

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Insulin action is mediated through a receptor tyrosine kinase, akin to the IGF-1 receptor. The number of receptors per cell varies significantly, from 40 on erythrocytes to 300,000 on adipocytes and hepatocytes. The insulin receptor consists of linked α/β subunit dimers, forming a heterotetramer glycoprotein with two extracellular α subunits and two β subunits spanning the membrane. The α subunits inhibit the inherent tyrosine kinase activity of the β subunits, but...
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Glucagon-like Receptor Agonists01:24

Glucagon-like Receptor Agonists

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Incretins include glucagon-like peptide-1 (GLP-1) and glucose-dependent insulinotropic polypeptide (GIP), which stimulate insulin secretion post-meals. In type 2 diabetes, GIP's efficacy is reduced, making GLP-1 a viable drug target. GIP originates from preproGIP.
GLP-1, when administered in high doses intravenously, triggers insulin secretion, inhibits glucagon release, slows gastric emptying, reduces food intake, and restores normal insulin secretion. However, its rapid inactivation by...
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cAMP-dependent Protein Kinase Pathways01:25

cAMP-dependent Protein Kinase Pathways

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Cyclic Adenosine Monophosphate (cAMP) is an essential second messenger that activates protein kinase A (PKA) and regulates various biological processes. A single epinephrine molecule binds to GPCR and activates several heterotrimeric G proteins, each stimulating multiple adenylyl cyclase, amplifying the signal, and synthesizing large numbers of cAMP molecules. Small changes in cAMP concentration affect PKA activity. The binding of four cAMP molecules induces a conformational change in PKA,...
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Hormones Regulating Blood Glucose01:16

Hormones Regulating Blood Glucose

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Insulin is released by beta cells of the pancreas when blood glucose levels are high. It facilitates glucose absorption and utilization in insulin-dependent cells with insulin receptors on their plasma membranes. Insulin promotes glucose uptake by increasing the number of glucose transport proteins in the cell membrane, allowing glucose to enter the cell. As a result, glucose utilization and ATP production are enhanced.
In addition to accelerating glucose uptake and utilization, insulin has...
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Dipeptidyl Peptidase 4 Inhibitors01:23

Dipeptidyl Peptidase 4 Inhibitors

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Dipeptidyl peptidase 4 (DPP-4) is a serine protease widely distributed in the body. It's involved in the inactivation of GLP-1 and GIP hormones, which are crucial for insulin regulation. DPP-4 inhibitors, such as sitagliptin (Januvia), saxagliptin (Onglyza), linagliptin (Tradjenta), alogliptin (Nesina), and vildagliptin (Galvus), help increase the proportion of active GLP-1, enhancing insulin secretion. These inhibitors work by competitively binding to DPP-4. This binding causes a...
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Hypoglycemia and Glucagon01:15

Hypoglycemia and Glucagon

334
Without prolonged fasting, healthy individuals maintain blood glucose levels above 3.5 mM due to a well-adapted neuroendocrine counterregulatory system that effectively prevents acute hypoglycemia, a potentially life-threatening condition. The primary clinical scenarios for hypoglycemia encompass diabetes treatment, inappropriate production of endogenous insulin or insulin-like substances by tumors, and the use of glucose-lowering agents in non-diabetic individuals. Notably, hypoglycemia in the...
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  2. 糖脂代謝と糖尿病における潜在的な標的
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  2. 糖脂代謝と糖尿病における潜在的な標的

関連する実験動画

Live Images of GLUT4 Protein Trafficking in Mouse Primary Hypothalamic Neurons Using Deconvolution Microscopy
08:47

Live Images of GLUT4 Protein Trafficking in Mouse Primary Hypothalamic Neurons Using Deconvolution Microscopy

Published on: December 7, 2017

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糖脂代謝と糖尿病における潜在的な標的

Ruifeng Xiao1, Cong Shen1, Wen Shen1

  • 1Department of Endocrinology and Metabolism, Affiliated Hospital of Jiangsu University, Institute of Endocrine and Metabolic Diseases, Jiangsu University, Zhenjiang 212000, China.

Current issues in molecular biology
|August 27, 2025

PubMed で要約を見る

まとめ
この要約は機械生成です。

タンパク質Fynキナーゼは脂肪の蓄積とインスリン抵抗性を促進し,2型糖尿病とその合併症に寄与する. Fynを抑制することは,糖尿病および関連する代謝障害の管理のための治療戦略を提供することができる.

キーワード:
ファインキナーゼ糖尿病 糖尿病糖尿病の合併症グルコロリピドの代謝炎症インスリン

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関連する実験動画

Live Images of GLUT4 Protein Trafficking in Mouse Primary Hypothalamic Neurons Using Deconvolution Microscopy
08:47

Live Images of GLUT4 Protein Trafficking in Mouse Primary Hypothalamic Neurons Using Deconvolution Microscopy

Published on: December 7, 2017

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A Model of Chronic Nutrient Infusion in the Rat
08:18

A Model of Chronic Nutrient Infusion in the Rat

Published on: August 14, 2013

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Optimized Analysis of In Vivo and In Vitro Hepatic Steatosis
08:58

Optimized Analysis of In Vivo and In Vitro Hepatic Steatosis

Published on: March 11, 2017

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科学分野:

  • 生物化学
  • 細胞生物学
  • 内分泌学

背景:

  • 成長,生存,エネルギー代謝などの細胞プロセスに 関与しています.
  • フィンキナーゼの調節不全は,インスリン抵抗性,脂肪の蓄積,糖尿病の合併症と関連しています.
  • Fynによって悪化する炎症的ストレスが 糖尿病の病原性の重要な要因です

研究 の 目的:

  • エネルギー代謝の調節におけるFynキナーズの役割を検討する.
  • 糖尿病とその合併症の発達におけるフィンのメカニズムを探求する.
  • 2型糖尿病の潜在的治療標的としてFynを特定する.

主な方法:

  • フィンキナーゼに関する既存の研究を統合した文献レビュー.
  • 脂質代謝とインスリン信号伝達経路におけるFynの関与の分析
  • 糖尿病に関連する炎症経路におけるFynの役割の検討

主要な成果:

  • Fynキナーゼは,AMP活性化タンパク質キナーゼ (AMPK) を阻害することによって,脂肪の蓄積とインスリン抵抗性を促進する.
  • Fynは,CD36,脂肪細胞の分化,およびインスリン信号伝達を含む経路を通じてエネルギー恒常性を調節する.
  • FynはAkt/GSK-3β/Fyn/Nrf2のようなシグナリングカスケードを通して糖尿病の炎症を悪化させる.
  • 結論:

    • 糖脂代謝を調節し,糖尿病の発症を促進する上で重要な役割を果たします.
    • 2型糖尿病の管理には有望な治療法である.
    • ファインの仕組みを理解することは 効果的な糖尿病治療法の開発に不可欠です