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LPS对心脏微血管内皮细胞ICAM-1表达的影响及rHDL的调控作用 被引量:4
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作者 宋耀明 孟素荣 《中国血液流变学杂志》 CAS 1999年第1期10-12,共3页
目的:观察 PLS作用下心脏微血管内皮(CMECs)细胞间粘附分子 (ICAM)-1的表达情况及rHDL的调控作用,为CHD的防治提供实验依据。方 法:利用培养的血管内皮细胞,采用流式细胞仪检测正常细胞、LPS作用和L... 目的:观察 PLS作用下心脏微血管内皮(CMECs)细胞间粘附分子 (ICAM)-1的表达情况及rHDL的调控作用,为CHD的防治提供实验依据。方 法:利用培养的血管内皮细胞,采用流式细胞仪检测正常细胞、LPS作用和LPS与 rHDL协同作用下0、1、2、6、12小时不同时相点 ICAM-1表达阳性细胞数及荧光 强度。结果:LPS和CMECs共同孵育下,随时间延长ICAM-1表达的阳性细胞数 和荧光强度上升,rHDL有抑制ICAM-1表达作用。结论:PLS可以刺激CMECs 表达ICAM-1,rHDL对血管内波细胞的损伤有保护作用。 展开更多
关键词 心脏 微血管 内皮细胞 冠心病 LPS rhdl
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硬件描述语言RHDL及模拟系统TJRS的实现
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作者 王向东 林福平 黄雨田 《太原工业大学学报》 1996年第3期18-22,共5页
本文介绍了一个多层次结构化的硬件描述语言RHDL:它的组成、结构和特性。叙述了与之相适配的数字系统CAD工具——寄存器级模拟系统TJRS,讨论了该系统的功能、结构和设计实现方法。
关键词 硬件描述语言 寄存器级模拟 rhdl CAD 模拟系统
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High density lipoprotein as a therapeutic target:Focus on its functionality
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作者 LEONARDO GÓMEZ ROSSO BELÉN DAVICO +4 位作者 EZEQUIEL LOZANO CHIAPPE WALTER TETZLAFF LAURA BOERO FERNANDO BRITES MAXIMILIANO MARTÍN 《BIOCELL》 SCIE 2023年第11期2361-2383,共23页
Cardiovascular diseases(CVDs)are the leading cause of death globally.CVDs are a group of disorders of the heart and blood vessels and include coronary heart disease,cerebrovascular disease and rheumatic heart disease ... Cardiovascular diseases(CVDs)are the leading cause of death globally.CVDs are a group of disorders of the heart and blood vessels and include coronary heart disease,cerebrovascular disease and rheumatic heart disease among other conditions.There are multiple independent risk factors for CVD,including hypertension,age,smoking,insulin resistance,elevated low-density lipoprotein cholesterol(LDL-C)levels,and triglyceride levels.LDL-C levels have traditionally been the target for therapies aimed at reducing CVD risk.High density lipoprotein(HDL)constitutes the only lipoprotein fraction with atheroprotective functions.Early HDL-targeted therapies have focused on increasing HDL-C levels.However,clinical trials have shown that raising HDL-C with niacin failed to achieve CVD reduction.A possible explanation for these findings is that these drugs could interfere with lipid metabolism and cause alterations in HDL structure and composition,leading to loss of functionality.As a result,targeting HDL-C levels would be insufficient to achieve CVD risk reduction,making HDL functionality a more desirable focus for HDL-directed therapies.There are several drugs which show the potential to improve HDL functionality.These drugs include molecules already approved for human use,such as statins and niacin,and particularly,compounds currently undergoing development such as apolipoprotein A-I mimetics and reconstituted HDL preparations.These therapies show promising potential to improve HDL functionality specifically.Future therapeutic strategies should incorporate HDL functionality as a main target of interest. 展开更多
关键词 HDL Cholesterol efflux rhdl Apo A-I mimetics STATINS PARAOXONASE
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