Megakaryocytes derived from human embryonic stem cells: a genetically tractable system to study megakaryocytopoiesis and integrin function.

Gaur M; Kamata T; Wang S; Moran B; Shattil SJ; Leavitt AD

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Megakaryocytes derived from human embryonic stem cells: a genetically tractable system to study megakaryocytopoiesis and integrin function.

机译：源自人类胚胎干细胞的巨核细胞：研究巨核细胞生成和整合素功能的遗传易处理系统。

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BACKGROUND: The platelet fibrinogen receptor, a heterodimer consisting of integrin subunits alpha(IIb) and beta(3), is required for platelet aggregation, spreading, and hemostasis. Platelet agonists such as thrombin and adenosine diphosphate (ADP) lead to the activation of alpha(IIb)beta(3), thereby enhancing its affinity and avidity for binding fibrinogen (inside-out signaling). Furthermore, fibrinogen binding to alpha(IIb)beta(3) triggers cytoskeletal changes and granule release (outside-in signaling). AIM: Genetic approaches to characterize the molecular pathways involved in alpha(IIb)beta(3) signaling are not possible with anucleate blood platelets. Therefore, we have established an OP9 stromal cell co-culture system to generate megakaryocytes from human embryonic stem cells (hESCs). RESULTS: alpha(IIb)beta(3) activation, measured by soluble fibrinogen binding to hESC-derived megakaryocytes, /GPIbalpha(+) cells, is readily detectable following stimulation with known platelet agonists. Dose-responsecurves for peptide agonists specific for the two platelet thrombin receptors, protease-activated receptor 1 (PAR1) and PAR4, show a relative responsiveness that mirrors that of human platelets, and sub-maximal ADP responses are augmented by epinephrine. Moreover, hESC-derived megakaryocytes undergo lamellipodia formation, actin filament assembly, and vinculin localization at focal adhesions when plated on a fibrinogen-coated surface, characteristic of alpha(IIb)beta(3) outside-in signaling. Undifferentiated hESCs genetically modified by lentiviral infection can be cloned and maintained in an undifferentiated state and then differentiated into megakaryocytes capable of alpha(IIb)beta(3) activation. CONCLUSION: Using hESCs, we have developed a renewable source of human megakaryocytes, and a genetically tractable system for studying megakaryocytopoiesis and alpha(IIb)beta(3) signaling in the native cellular environment.

机译：背景：血小板血纤蛋白原受体是由整联蛋白亚基α（IIb）和β（3）组成的异二聚体，是血小板聚集，扩散和止血所必需的。血小板激动剂，例如凝血酶和二磷酸腺苷（ADP）导致alpha（IIb）beta（3）的激活，从而增强其与血纤蛋白原结合的亲和力和亲合力（由内而外的信号传导）。此外，纤维蛋白原结合到alpha（IIb）beta（3）触发细胞骨架的变化和颗粒释放（外向内信号传导）。目的：用无核血小板不可能鉴定涉及α（IIb）beta（3）信号传导的分子途径的遗传方法。因此，我们建立了OP9基质细胞共培养系统，以从人胚胎干细胞（hESCs）产生巨核细胞。结果：通过可溶性血纤蛋白原与hESC衍生的巨核细胞/ GPIbalpha（+）细胞的结合，可以测量到alpha（IIb）beta（3）激活，用已知的血小板激动剂刺激后很容易检测到。特异性针对两种血小板凝血酶受体，蛋白酶激活受体1（PAR1）和PAR4的肽激动剂的剂量反应显示相对反应，与人血小板相似，肾上腺素增强了亚最大ADP反应。此外，hESC衍生的巨核细胞在涂于纤维蛋白原包被的表面上时，会发生板层状脂蛋白形成，肌动蛋白丝组装和粘着斑在粘着斑处定位，这是alpha（IIb）beta（3）内外信号的特征。可以将通过慢病毒感染基因修饰的未分化hESC克隆并保持在未分化状态，然后分化为能够激活alpha（IIb）beta（3）的巨核细胞。结论：使用hESCs，我们已经开发了人类巨核细胞的可再生来源，以及用于研究原生细胞环境中巨核细胞生成和alpha（IIb）beta（3）信号传导的遗传易处理系统。

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《Journal of thrombosis and haemostasis: JTH》 |2006年第2期|共7页
作者
Gaur M; Kamata T; Wang S; Moran B; Shattil SJ; Leavitt AD;
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正文语种 eng
中图分类临床医学;
关键词
Megakaryocytes; Blood Platelets; Human; embryonic stem cell; 巨核细胞; 血小板;

机译：Megakaryocytes;Blood Platelets;Human;embryonic stem cell;巨核细胞;血小板;

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专利

1. Megakaryocytes derived from human embryonic stem cells: a genetically tractable system to study megakaryocytopoiesis and integrin function. [J] . Gaur M, Kamata T, Wang S, Journal of thrombosis and haemostasis: JTH . 2006,第2期

机译：源自人类胚胎干细胞的巨核细胞：研究巨核细胞生成和整合素功能的遗传易处理系统。
2. Megakaryocytes derived from embryonic stem cells implicate CalDAG-GEFI in integrin signaling [J] . Koji Eto, Ronan Murphy, Steve W. Kerrigan, Proceedings of the National Academy of Sciences of the United States of America . 2002,第20期

机译：源自胚胎干细胞的巨核细胞在整联蛋白信号传导中涉及CalDAG-GEFI。
3. The negative impact of Wnt signaling on megakaryocyte and primitive erythroid progenitors derived from human embryonic stem cells - ScienceDirect [J] . Prasuna Paluru, Kristin M. Hudock, Xin Cheng, Stem cell research . 2013,第2期

机译：Wnt信号传导对源自人类胚胎干细胞的巨核细胞和原始红系祖细胞的负面影响-ScienceDirect
4. A systems-approach to studying histone H4 and its epigenetic regulatory role in human embryonic stem cells [C] . Justin Brumbaugh, Doug Phanstiel, Samuel S. Oliver, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2009

机译：一种研究组蛋白H4的系统方法及其在人胚胎干细胞中的表观遗传调控作用
5. Genetic Selection of Cardiomyocytes and Pacemaker Cells Derived From Human Embryonic Stem Cells. [D] . Gantz, Jay Alexander. 2013

机译：源自人类胚胎干细胞的心肌细胞和起搏器细胞的遗传选择。
6. Megakaryocytes derived from embryonic stem cells implicate CalDAG-GEFI in integrin signaling [O] . Koji Eto, Ronan Murphy, Steve W. Kerrigan, 2002

机译：源自胚胎干细胞的巨核细胞在整联蛋白信号传导中涉及CalDAG-GEFI。
7. Megakaryocytes derived from human embryonic stem cells: a genetically tractable system to study megakaryocytopoiesis and integrin function [O] . M. GAUR, T. KAMATA, S. WANG, 2006

机译：衍生自人胚胎干细胞的巨核细胞：一种遗传造成巨大的巨大细胞症和整合素功能的遗传造型系统

Megakaryocytes derived from human embryonic stem cells: a genetically tractable system to study megakaryocytopoiesis and integrin function.

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