肾脏药理学研究进展及趋势

目前慢性肾病发病率不断上升,但缺乏有效防治肾病药物。发现和确认治疗肾病新的药物靶点、研发和合理应用防治肾病药物是人类健康的迫切需求,也是肾脏药理学的热点研究领域。近年来,肾脏药理学领域的基础研究热点和临床关注重点包括治疗免疫相关肾病药物、新型糖皮质激素、治疗多囊肾病药物、治疗尿酸性肾病药物、治疗肾结石药物、治疗肾性贫血药物和利尿药等新药研发,以及对肾有损伤作用的药物和肾损伤标志物研究。本文对肾脏药理学未来发展趋势亦予以了展望。

杂质残留量对不同栽培方式下灵芝多糖肽定值的影响

目的依据国家标准样品定值要求,为提高标准样品纯度,降低杂质残留量,选择最佳栽培方式的灵芝子实体用于灵芝多糖肽(Ganoderma lucidum polysaccharide peptide,GL-PPSQ_(2))标准样品的研制。方法基于高效液相色谱法(high performance liquid chromatography,HPLC),采用面积归一法对GL-PPSQ_(2)主成分进行定量分析,卡尔费休库伦法(K-F)测定水分,热重分析法(thermogravimetricanalysis,TG)测定灰分,微波消解-电感耦合等离子体质谱法(inductively coupled plasma-mass spectrometry,ICP-MS)测定14种微量元素,顶空-气相色谱法(headspace-gas chromatography,HS-GC)测量溶剂残留;质量平衡法对菌草层架(A)、菌草覆土(B)、苡仁壳层架(C)、短段木覆土(D)4组不同栽培方式所得GL-PPSQ_(2)进行定值。结果GL-PPSQ_(2)定值依次为:C(97.38%)>A(96.58%)>D(96.02%)>B(95.15%);得率分别为:B(0.29%)>D(0.18%)>A(0.15%)>C(0.07%);杂质残留量为:C(1.81%)<A(2.63%)<D(3.20%)<B(4.05%)。结论宜选择短段木覆土或菌草层架栽培灵芝子实体作为GL-PPSQ2标准样品制备原料。

新思路·新技术——中药复方新药研发相关重大科学和技术问题

"第十二届全国中药与天然药物药理学术会议"于2019年10月11-13日在天津市社会山国际会议中心酒店举行。会议期间,中国药理学会中药与天然药物药理专业委员会召开了"中药复方新药研发相关重大科学和技术问题"专题研讨会。研讨会分为主题报告和综合讨论2部分。主题报告由中国药理学会中药与天然药物药理专业委员会副主任委员吴春福教授主持,刘建勋、孙晓波、段大跃和吕圭源教授作主题报告。中国药理学会理事长兼中药与天然药物药理专业委员会主任委员张永祥研究员主持综合讨论,国家卫生健康委员会科技教育司重大专项处顾金辉处长全程参加。与会专家围绕中药复方新药研发相关重大科学和技术问题进行了广泛、深入的讨论。本文整理了专家们的主要观点和建议,希望能为中药复方新药研发提供新思路和新技术,为提高我国中药复方新药的研发水平发挥积极的推动作用。

Ganoderma lucidum polysaccharide peptide alleviates hepatoteatosis via modulating bile acid metabolism dependent on FXR-SHP/FGF

OBJECTIVE Ganoderma lucidum polysaccharide peptide(GLPP)is a group of extract from Ganoderma lucidum with a molecular mass of approximately 5×10^5,which ratio of polysaccharide to peptide is approximately 95%/5%.The purpose of this study was to determine whether GLPP has therapeutic effect on Non-alcoholic fatty liver disease(NAFLD).METHODS Ob/ob mouse model and ApoC3 transgenic mouse model were used for exploring the effect of GLPP on NAFLD.Key metabolic pathways and enzymes were identified by metabolomics combining with KEGG and PIUmet analyses and key enzymes were detected by Western blotting.Hepatosteatosis models of HepG2 cells and primary hepatocytes were used to further confirm the therapeutic effect of GLPP on NAFLD.RESULTS GLPP administrated for a month alleviated hepatosteatosis,dyslipidemia,liver dysfunction and liver insulin resistance.Pathways of glycerophos⁃pholipid metabolism,fatty acid metabolism and primary bile acid biosynthesis were involved in the therapeutic effect of GLPP on NAFLD.Detection of key enzymes revealed that GLPP reversed low expression of CYP7A1,CYP8B1,FXR,SHP and high expression of FGFR4 in ob/ob mice and ApoC3 mice.Besides,GLPP inhibited fatty acid synthesis by reducing the expression of SREBP1c,FAS and ACC via a FXR-SHP dependent mechanism.Additionally,GLPP reduced the accumulation of lipid droplets and the content of TG in HepG2 cells and primary hepatocytes induced by oleic acid and palmitic acid.CONCLUSION GLPP significantly improves NAFLD via regulating bile acid synthesis dependent on FXR-SHP/FGF pathway,which finally inhibits fatty acid synthesis,indicating that GLPP might be developed as a ther⁃apeutic drug for NAFLD.

灵芝子实体标志性成分与生物活性的研究

目的 研究灵芝子实体标志性成分——多糖肽和灵芝酸,旨在研究制备活性物质工艺,建立专属性强的分析方法,为提升灵芝质量标准提供参考。方法 采用中空纤维膜分离技术,截留不同分子量组分,再通过色谱法分离纯化得到标志性成分并验证其药理活性。结果 灵芝水提液通过膜分离技术和制备液相可同时得到灵芝多糖肽组分和灵芝酸单体,并作为衡量灵芝子实体质量的标准物质。药理实验表明,灵芝多糖肽具有免疫激活作用和灵芝酸具有抗炎活性。结论 用灵芝活性组分多糖肽和灵芝酸标识灵芝质量,为育种栽培、灵芝提取物生产工艺及产品质量控制提供理论依据。