中国医药指南
中國醫藥指南
중국의약지남
CHINA MEDICINE GUIDE
2014年
18期
73-75
,共3页
于顺江%姜翠莲%杨新爱%杨宁康%肖明
于順江%薑翠蓮%楊新愛%楊寧康%肖明
우순강%강취련%양신애%양저강%초명
葡萄糖激酶活化剂(GKA)%葡萄糖激酶(GCK)%2型糖尿病(T2DM)%抗糖尿病药物%临床试验%三酰甘油
葡萄糖激酶活化劑(GKA)%葡萄糖激酶(GCK)%2型糖尿病(T2DM)%抗糖尿病藥物%臨床試驗%三酰甘油
포도당격매활화제(GKA)%포도당격매(GCK)%2형당뇨병(T2DM)%항당뇨병약물%림상시험%삼선감유
Glucokinase activator (GKA)%Glucokinase (GCK)%Type 2 diabetes (T2DM)%Anti-diabetic drugs%Clinical trials%Triacylglycerol
2型糖尿病是一种常见的代谢性疾病,目前临床上仍然缺乏有效的治疗药物。葡萄糖激酶(Glucokinase,GCK)是调节体内葡萄糖代谢和参与血糖动态平衡的主要调节者。早在20世纪90年代葡萄糖激酶作为一个潜在的药物作用靶点已引起科技人员高度的关注。葡萄糖激酶活化剂(又称葡萄糖激酶激动剂,Glucokinase activators,GKAs)是直接作用于葡萄糖激酶且代表一类富有希望和前景的抗2型糖尿病(T2DM)药物。糖尿病动物模型和T2DM患者的短期给药研究已显示TKA能降低血糖和糖化血红蛋白水平,但与此同时,胰腺胰岛β-细胞GCK活化后产生低血糖的风险也日益受到关注,虽然当时学者们普遍认为GKAs对肝脏可能没有明显的不良反应。但在《英国药理学杂志》刊登的文章中,De Ceunick等报告了以GKA进行短期和长期治疗血糖水平正常和高血糖的啮齿动物却导致三酰甘油在肝脏明显的沉积,表明GCK活化后引起的肝脏葡萄糖吸收和抑制肝脏内源性葡萄糖生成作用可能会带来显著的不良反应,GKA可引发肝脏脂肪变性,这就指出了关于GKA药物的重大安全问题。因此,这些GKAs小分子化合物所引起的血浆和肝脏三酰甘油水平的升高在将来研究中应值得密切的关注。另外,最近完成的几个Ⅱ期临床试验结果很令人失望,在T2DM患者治疗时,发现GKA用药几个月后逐渐失去疗效,在一些或一定比例患者治疗时产生高血脂和高血压。这些结果已使人们对GKAs药物的疗效和安全产生怀疑。因此,在将来的临床研究中,强烈建议对GKAs这一类药物的有效性和安全性进行重新评价。
2型糖尿病是一種常見的代謝性疾病,目前臨床上仍然缺乏有效的治療藥物。葡萄糖激酶(Glucokinase,GCK)是調節體內葡萄糖代謝和參與血糖動態平衡的主要調節者。早在20世紀90年代葡萄糖激酶作為一箇潛在的藥物作用靶點已引起科技人員高度的關註。葡萄糖激酶活化劑(又稱葡萄糖激酶激動劑,Glucokinase activators,GKAs)是直接作用于葡萄糖激酶且代錶一類富有希望和前景的抗2型糖尿病(T2DM)藥物。糖尿病動物模型和T2DM患者的短期給藥研究已顯示TKA能降低血糖和糖化血紅蛋白水平,但與此同時,胰腺胰島β-細胞GCK活化後產生低血糖的風險也日益受到關註,雖然噹時學者們普遍認為GKAs對肝髒可能沒有明顯的不良反應。但在《英國藥理學雜誌》刊登的文章中,De Ceunick等報告瞭以GKA進行短期和長期治療血糖水平正常和高血糖的齧齒動物卻導緻三酰甘油在肝髒明顯的沉積,錶明GCK活化後引起的肝髒葡萄糖吸收和抑製肝髒內源性葡萄糖生成作用可能會帶來顯著的不良反應,GKA可引髮肝髒脂肪變性,這就指齣瞭關于GKA藥物的重大安全問題。因此,這些GKAs小分子化閤物所引起的血漿和肝髒三酰甘油水平的升高在將來研究中應值得密切的關註。另外,最近完成的幾箇Ⅱ期臨床試驗結果很令人失望,在T2DM患者治療時,髮現GKA用藥幾箇月後逐漸失去療效,在一些或一定比例患者治療時產生高血脂和高血壓。這些結果已使人們對GKAs藥物的療效和安全產生懷疑。因此,在將來的臨床研究中,彊烈建議對GKAs這一類藥物的有效性和安全性進行重新評價。
2형당뇨병시일충상견적대사성질병,목전림상상잉연결핍유효적치료약물。포도당격매(Glucokinase,GCK)시조절체내포도당대사화삼여혈당동태평형적주요조절자。조재20세기90년대포도당격매작위일개잠재적약물작용파점이인기과기인원고도적관주。포도당격매활화제(우칭포도당격매격동제,Glucokinase activators,GKAs)시직접작용우포도당격매차대표일류부유희망화전경적항2형당뇨병(T2DM)약물。당뇨병동물모형화T2DM환자적단기급약연구이현시TKA능강저혈당화당화혈홍단백수평,단여차동시,이선이도β-세포GCK활화후산생저혈당적풍험야일익수도관주,수연당시학자문보편인위GKAs대간장가능몰유명현적불량반응。단재《영국약이학잡지》간등적문장중,De Ceunick등보고료이GKA진행단기화장기치료혈당수평정상화고혈당적교치동물각도치삼선감유재간장명현적침적,표명GCK활화후인기적간장포도당흡수화억제간장내원성포도당생성작용가능회대래현저적불량반응,GKA가인발간장지방변성,저취지출료관우GKA약물적중대안전문제。인차,저사GKAs소분자화합물소인기적혈장화간장삼선감유수평적승고재장래연구중응치득밀절적관주。령외,최근완성적궤개Ⅱ기림상시험결과흔령인실망,재T2DM환자치료시,발현GKA용약궤개월후축점실거료효,재일사혹일정비례환자치료시산생고혈지화고혈압。저사결과이사인문대GKAs약물적료효화안전산생부의。인차,재장래적림상연구중,강렬건의대GKAs저일류약물적유효성화안전성진행중신평개。
Type 2 diabetes is a common metabolic disease, currently it still lack clinically of effective therapeutic agents. Glucokinase (GCK) is a main regulator of glucose metabolism and glucose homeostasis in vivo. As a potential target for drug action, glucokinase has caused much attention of researchers early since the last century 90's.Glucokinase activators (GKAs) are the drugs against the type 2 diabetes which will effect directly on glucokinase and represent a class full of hope and promise agents. Studies with animal models of diabetes and T2DM patients with short-term administration have shown that GKAs can reduce the blood glucose and glycated hemoglobin levels, but at the same time, there exists a big concern that the GCK activation in pancreatic islet cells-risk could induce hypoglycemia, although scientists at that time believe generally that it may have no obvious side-effects of GKAs on the liver. But De Ceunick reported byan article which was published in British Journal of Pharmacology that short and long term treatment with GKA can cause obviously deposition and accumulation of triglyceridein rodent liver with normal blood glucose level and hyperglycemia animal models, which showed that activation of GCK prohibits hepatic glucose uptake and endogenous glucose production in liver, this may bring significant side-effects of GKA treatment such as hepatic steatosis, triglyceride elevation, and may raise security problems in management of the T2DM patients. Therefore, triglyceride level changes caused by GKA in plasma and in liver should be monitored carefully in future studies. In addition, the results of several recent phase II trials completed were quite disappointing because patients developed hyperlipidemia and vascular hypertension, and the drug lost efficacy within several months. These results have raised doubts and brought a puzzle about the efficacy and safety of GKA, and it’s strongly suggested that it’s necessary of re-evaluation of the efficacy, and especially safety of GKAs in future clinical studies.
