个体化医疗的现状与未来生物标志物(PPT) .ppt
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1、个体化医疗的现状与未来四.生物标志物研究,Outline,生物标志物的概念如何评价生物标志物?生物标志物的研究方法?,生物标志物的概念,什么是生物标志物(biomarker)?,“measurable and quantifiable biological parameters”-a Medical Subject Heading(MeSH)term,1989“A characteristic that is objectively measured and evaluated as an indicator of normal biological processes,pathogenic
2、processes or pharmacological responses to a therapeutic intervention.”-Biomarker Definitions Working Group,2001,NIH,Features of a Useful Biomarker,High sensitivity and specificityEasy accessible sampleCorrelation with histological scoringChange in advance of clinical signsTranslational from research
3、 to clinical use,不同水平生物标志物,DNA,Primary transcript,mRNA,Transcription,protein,Translation,RNA processing,Nucleus,Biomarker Examples,Cholesterol is one of the most well-known biomarkers of cardiovascular healthPhysical measurements:body temperature(fever);blood pressure(stroke risk)Other biomarkers:bl
4、ood sugar level(diabetes)antigens(hepatitis)proteins(heart attack)genetic variations(Huntingtons disease),生物标志物的临床应用,Ludwig JA et al.Nature reviews 2005,5:845-856,目前临床很多疾病的诊断依赖病理诊断,但不能作为常规筛查、监测手段众多疾病缺乏早期、特异性生物标志物治疗缺乏个体化方案,生物标志物应用现状,Clin J Am Soc Nephrol 3:18951901,2008.,Biomarkers for chronic kidney
5、 disease,Are we treating sub-populations?,From Kalow,Tyndale&Meyer,Pharmacogenomics,2001,Novel biomarkers are needed,Early,accurate diagnosis-Individualized therapy and improved treatment outcomesBetter defined populations will allow more specific drugs-Better efficacy-Fewer side effects,“The use of
6、 biomarkers will change medical practice from a population-based approach to anindividualized approach”Felix Frueh,Associate Director of Genomics at CDER,FDA,Evolution of the biomarkers research,High plasma cholesterol and cardiovascular diseases,Nearly 50 percent of all future myocardial infarction
7、 and stroke events occur in those with normal or below normal lipid levels.,EUROASPIRE Study Group,1997,%of MI,Additional biomarkers(inflammation)Hs-CRP and cardiovascular risk,Hs-CRP is the most widely studied biomarker of inflammation in cardiovascular risk.Since the early 1990s with the developme
8、nt of highly sensitive assays for its measurement,correlations of hs-CRP with both cardiovascular risk factors and future cardiovascular events has been possible.,CRP and LDLC levels and the risk of cardiovascular diseases,Increased CRP levels are associated with increased risk of cardiovascular eve
9、nts independently of LDL-C levels,Ridker PM et al.,2002,27,939 women,High CRP-high LDL,High CRP-low LDL,Low CRP-low LDL,Low CRP-high LDL,Porbability of Event-free Survival,Years of Follow-up,0.99,0.98,0.97,0.96,0.00,1.00,0,2,4,6,8,Evolution of the biomarkers research:CRP and LDL-C levels and event-f
10、ree survival among women,27,939 womenThe median values were as follows:C-reactive protein:1.52 mg/L LDL cholesterol:123.7 mg/dL or:3.20 mmol/L,CRP and LDL-C could give better prognostic information than the two markers separately.,Ridker PM et al.,2002,如何评价生物标志物?,常用评价指标,(一)敏感性(二)特异性(三)Youden指数(四)阳性似
11、然比(五)阴性似然比(六)阳性预报值(七)阴性预报值(八)ROC曲线,ECG诊断试验的结果,一、敏感性(Sensitivity):TP/(TP+FN)=TPR(true positive rate)TRP=Sen=416/(416+104)=0.8该指标只与病例组有关,反映了诊断试验检出病例的能力,ECG诊断试验的结果,二、特异性(Specificity)Spe=True negative rate(TNR)=TN(FP+TN)=171/(171+9)=0.95该指标只与对照组有关,反映了诊断试验排除非病例的能力。,灵敏度与特异度的优缺点,优点:灵敏度与特异度不受患病率的影响,其取值范围均在(
12、0,1)之间,其值越接近于1,说明其诊断准确性越好。缺点:当比较两个诊断试验时,单独使用灵敏度或特异度,可能出现矛盾。解决办法:将两指标结合:Youden指数、阳性似然比、阴性似然比等,ECG诊断试验的结果,三、Youden指数,=Sen+Spe-1=TPR-FPR=0.8-0.05=0.75Youden指数取值范围在(0,1)之间,其值越接近1,诊断准确性越好。,ECG诊断试验的结果,ECG诊断试验的结果,医生最关心的问题:1.试验阳性时患病的概率多大?2.试验阴性时不患病的概率多大?,阳性预测值是在诊断试验阳性的受试者中,标准诊断有病的病例(真阳性)所占的比例,阴性预测值则是在诊断试验为阴
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