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一种波长可调谐激光器的特性研究 被引量:1
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作者 李小飞 税静 +2 位作者 张金良 叶进 黄莎莉 《光通信技术》 CSCD 北大核心 2013年第9期9-12,共4页
FRL15TCWx-D86是由12个DFB激光器构成的波长可调谐激光器,具有较宽的波长调谐范围,较高的波长稳定度与功率稳定度。介绍了FRL15TCWx-D86激光器的结构和工作原理。通过系统测试及特性分析,提出了一种具有较高波长稳定度和功率稳定度的波... FRL15TCWx-D86是由12个DFB激光器构成的波长可调谐激光器,具有较宽的波长调谐范围,较高的波长稳定度与功率稳定度。介绍了FRL15TCWx-D86激光器的结构和工作原理。通过系统测试及特性分析,提出了一种具有较高波长稳定度和功率稳定度的波长可调激光器实现方法。 展开更多
关键词 frl1 5TCWx-D86 波长可调谐 特性研究 DWDM
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Human Macrophages Utilize the Podosome Formin FMNL1 for Adhesion and Migration
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作者 Matthew R. Miller Scott D. Blystone 《CellBio》 2015年第1期1-11,共11页
Macrophages play a crucial role in detecting, regulating, and resolving immune crises, requiring migration through complex extracellular matrices. Unwarranted macrophage inflammatory activity potentiates kidney diseas... Macrophages play a crucial role in detecting, regulating, and resolving immune crises, requiring migration through complex extracellular matrices. Unwarranted macrophage inflammatory activity potentiates kidney disease, rheumatoid arthritis, and transplant rejection. Proper remodeling of the actin cytoskeleton, especially at adhesion structures, is essential to the translocation of macrophages. Macrophages form actin-rich adhesions termed “podosomes”, giving them the capacity to make contacts with the substratum for traction through interstitial tissues. Macrophages express multiple formins, including FMNL1, Dia1, and Fhod1, with potential to impact actin remodeling involved in migration. Formins are a family of proteins that are best known for modifying the actin cytoskeleton via nucleation, elongation, bundling, and/or severing actin filaments. In this study we demonstrate that the formin FMNL1 is a key regulator of podosomes and is required for normal macrophage migration. Additionally, this is the first study to demonstrate defects in primary human cell migration resulting from specific formin silencing. Pharmacologic inhibition of all formin activity results in a significant decrease in podosome formation and normal macrophage migration. Furthermore, targeted suppression of FMNL1 results in decreases in macrophage migration similar to inhibition of all expressed macrophage formins. These novel findings suggest FMNL1 as a possible chemotherapeutic target to hinder macrophage migration, which could offer an innovative method for limiting unnecessary macrophage-mediated inflammation. We hypothesize that formins are required in podosome actin dynamics to support macrophage migration. 展开更多
关键词 frl1 MONOCYTE EXTRAVASATION CHEMOTAXIS
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