MTOR抑制剂在癌症治疗中的应用

Click to edit Master title style,Click to edit Master text styles,Second level,Third level,Fourth level,mTOR Inhibitors(mTOR,抑制剂,),in Cancer Therapy,mTOR,Mammalian Target of Rapamycin,(,哺乳,动物雷帕霉素靶蛋白,),A central regulator of cell growth and metabolism,(,控制细胞的生长和代谢,),mTOR is an intracellular serine-threonine kinase(,丝氨酸,-,苏氨酸激酶,),mTOR is downstream of growth factor/nutrient and PI3k/AKT signalling pathway(,信号通路中的下游分子,),mTOR is a central regulator of protein synthesis,Activated by mutations in cancer,Nutrients,Growth Factors,IGF,EGF,VEGF etc,PI3K,glucose,amino,acids,etc,Mutations in cancer,AKT,S6k,eif-4e,Protein Synthesis,Growth&,Proliferation,Bioenergetics,Angiogenesis,mTOR,(,哺乳动物雷帕霉素靶蛋白,),mTOR Pathway Activation,Protein,Synthesis,Growth Factors,Cell Growth&,Proliferation,Bioenergetics,Angiogenesis,mTOR,PI3K,EGF,IGF,VEGF,AKT,RAS,ER,ABL,AMPK,RAS,TSC1,TSC2,PTEN,LKB1,Regulators of mTOR activity,mTOR activating,mTOR deactivating,Mutations of PI3K,Akt,Ras,GFRs,TSC1/2,PTEN.)may result in inappropriate activation of the pathway and loss of control of functions normally regulated by mTOR,Activation of mTOR can result in loss of cell growth control and enhanced cell metabolism in cancer cells(,无限制的癌细胞生长和扩散,),mTOR Activation,Increased synthesis of multiple proteins,including:,Hypoxia-Inducible Factors(HIFs,低氧诱导因子,):expression of angiogenic growth factors(eg,VEGF/PDGF)(RCC),Cyclin D1:promotes progression through the cell cycle(MCL),Proteins necessary to transport nutrients(amino acids and glucose)into the cell,mTOR-Linked Pathway Activation in Selected Cancers,Breast,NET,Colorectal,Lung,Renal Cell,p-Akt,42%,PTEN,15%41%,HER2,30%36%,PI3-K,18%26%,TSC1/TSC2,IGF-1/IGF-1R,VHL,Ras,50%,p-Akt,46%,PTEN,35%,PI3-K,20%32%,EGFR,70%,EGFR,32%60%,p-Akt,23%50%,Ras,30%,PTEN,24%,TGF,a,/TGF,b,1,60%100%,VHL,30%50%,IGF-1/IGF-IR,39%-69%,p-Akt,38%,PTEN,31%,TSC1/TSC2,NF-,k,B,33%,Lymphoma,ALK,p-Akt,NF-,k,B,Cyclin D1,Rapamycin(sirolimus)-,雷帕霉素,Isolated in 1975 on the island of Rapa Nui,Approved for prevention of kidney transplant rejection in the US and Europe,Found to have broad anticancer activity against a panel of human cancer cell lines by the U.S.NCI in the 1980s,Rapamycin derivatives with improved pharmacokinetic properties Clinical development of mTOR inhibitors as anticancer agents,Clinical Development of mTOR Inhibitors(Derivates of rapamycin),Temsirolimus(CCI-779,Torisel,Wyeth Pharmaceuticals),Everolimus(RAD001,Afinitor,Novartis),Deforolimus(AP23573,ARIAD Pharmaceuticals and Merck&Co),mTOR inhibition:Similar Mechanism,of Action,mTOR inhibition,(,Similar mechanism of action),mTOR Inhibitors:Derivates of Rapamycin,Formulation,and administration:,different,Temsirolimus:Administered,Intravenously,Deforolimus:administered,Intravenously,Everolimus:administered,Orally,mRCC,Standards for RCC Therapy by Phase III Trial after ASCO 2007,Setting,Phase III,Treatment-nave,Good or intermediate risk*,Sunitinib,Bevacizumab+IFN-,Poor risk*,TemsirolimusSunitinib,Previously treated,Prior cytokine,Sorafenib,Prior VEGFr-TKI,?,Prior mTOR inhibitor,*,MSKCC risk status,RAD001,(everolimus),O,O,O,H,O,O,O,N,O,O,O,O,O,O,H,O,O,H,10 mg/5 mg,Everolimus,(RAD001)(,口服,mTOR,抑制剂,),Rapamycin derivative,Selective inhibitor of mTOR,Metabolized by CYP3A4 isozyme,T,1/2,30 hours,Crosses bloodbrain barrier,Biomarker-guided monotherapy dose selection,10 mg/day,70 mg/week,Everolimus(RAD001,Afinitor),in RCC,Rationale,About 75%of clear cell carcinomas,the function of the von Hippel Lindau(,VHL,)gene is lost,causing accumulation of HIF(,低氧诱导因子,)/expression of VEGF and PDGF.,Other proteins in the PI3K-AKT-mTOR pathway are often deregulated in RCC,Unmet medical needs for Patients who have failed VEGFt-TKI therapy,Everolimus has both antiangiogenic and antiproliferative activity;response were observed in previously treated mRCC(uncontrolled phase II study),Better Inhibition of p70S6 Kinase With Daily Schedule,0,1,2,3,4,5,6,7,Tumor,0,50,100,Time,days,Inhibition of p70S6 Kinase Activity,%,50,20,70,30,10,5,10,Daily dosing,mg,Weekly dosing,mg,Continuous target inhibition is predicted to be achievable,through the use of daily dosing schedules,Tanaka,et al.,manuscript in preparation 2007.,Phase II Trial of RAD001 in mRCC,(Amato),Jac et al.ASCO,2007.Abstract 5107,N=37,N=39,Median=11.17+(2.00 31.53+)Months,Median=24.17+Months,Progression-Free Survival,Overall Survival,Time(months),Time(months),Objectives(end Point),Primary:,PFS,Secondary:,Safety;Response;Patients reported outcome;OS,RECORD-1(,RE,nal,C,ell cancer treatment with,O,ral,R,AD001 given,D,aily),随机,III,期试验,:,比较,RAD001,与安慰剂,(phase III,double-blind,randomized trial of,RAD001,+BSC vs,Placebo,+BSC,),RECORD-1 Phase III study design,(,随机,III,期试验,:,比较,RAD001,与安慰剂,),410 patients randomized between September 2006 and October 2007,Second interim analysis cut-off:October 15,2007,based on 191 PFS events,Independent Data Monitoring Committee recommended termination of study,R,A,N,D,O,M,I,Z,A,T,I,O,N,2:1,Placebo+BSC,(n=138),Upon Disease Progression,I