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本文(缺血性脑卒中机理以及新药研究进展.pptx)为本站会员(h****)主动上传,文客久久仅提供信息存储空间,仅对用户上传内容的表现方式做保护处理,对上载内容本身不做任何修改或编辑。 若此文所含内容侵犯了您的版权或隐私,请立即通知文客久久(发送邮件至hr@wenke99.com或直接QQ联系客服),我们立即给予删除!

缺血性脑卒中机理以及新药研究进展.pptx

1、The science of ischemic stroke:,mechanisms and therapies,What is cerebral ischemic strokeWhat cause cerebral ischemic strokeWhat are the prominent mechanisms of strokeCurrent approaches for stroke therapeutics,Cerebral ischemic stroke,Cerebral ischemic is a condition in which there is insufficient b

2、lood flow to the brain to meet metabolic demand.This leads to poor oxygen supply or cerebral hypoxia and thus to the death of brain tissue or cerebral infarction / ischemic stroke.It is a sub-type of stroke along with subarachnoid hemorrhage and intrace- rebral hemorrhage.,Stroke is responsible for

3、9% of deaths worldwide, making it the second most common cause of mortality . More than 25% of stroke survivors become permanently disabled and lose independence in performing day-to-day activities .These figures will continue to rise with the population living longer than previous generations. As s

4、uch, effective treatments for stroke are urgently needed.,Stroke Risk Factors and Triggers,Mechanisms of Stroke,ExcitotoxicityMitochondrial responseReactive oxygen species (ROS) Endoplasmic reticulum stressInflammatory ApoptosisInflammatoryRepair,Acute Period,Subacute Period,Chronic Period,Depolariz

5、ation,Na+/ K+ pump failure,CNS ischemia,Deficiency of glucose and oxygen,Unable to maintain the ionic gradients,Excessiveglutamate release,Excitotoxicity,Excitotoxicity,Mitochondrial response,Reactive oxygen species (ROS),Endoplasmic reticulum stress,Inflammatory,Current approaches for stroke therap

6、eutics,Blocking Excitotoxic Events.,TABLE 1: Examples of proposed neuroprotectants attempting to mitigate excitotoxicity, and the progression from preclinical experimental stroke models to clinical trials,Noncompetitive NMDA Antagonists,Magnesium The mechanism of neuroprotection by magnesium remains

7、 uncertain: increasing magnesium concentration reduces presynaptic release of the neurotransmitter glutamate,blocks glutamatergic N-methyl-Daspartate receptors,potentiates adenosine action,improves mitochondrial calcium buffering, and blocks calcium entry via voltage-gated channels. Furthermore, it

8、has cardiovascular effects, notably enhanced cerebral perfusion after MCAO9 and raised cardiac output.,Preclinical Output,Fig.1 the effects of MgSO4 pretreatment on infarct volumes,Magnesium has demonstrated its neuroprotective effect in animal studies as well as in a phase II study on stroke patien

9、ts.,Preclinical Output,Fig.2 Representative tracings of (TTC)stained brain slices.,Fig.3 slice infarction volumes in control and MgSO4-treated animals,PhaseIII,Currently, the FAST-MAG (Field Administration of Stroke Therapy Magnesium) trial includes 1,700 stroke patients receiving a dose of 4 g (int

10、ravenously) over 15 min, followed by a maintenance infusion of 16 g over 24 h after arrival at the hospital; it was started in January 2005 and is still in progress,Clinical Output,Clinical Output,Fig 4: Kaplan-meier plot of cumulative mortality,TABLE2:Examples of proposed neuroprotective attempts t

11、o against oxidative stress,Free-Radical Scavenging,Mechanisms:Proposed interaction of edaravone with free radicals.,Edaravone.(依达拉奉),Preclinical Output,Figure1 B, Infarct volume was compared between the control and different edaravone groups,Figure 1. A, Coronal sections from ischemic mice brain sta

12、ined with TTC,Preclinical Output,Figure 3. Edaravone protected HT22 cells against glutamate-induced oxidative stress,Figure 2. Glutamate-induced oxidative damage in the HT22 neuronal cell line,Preclinical Output,Figure 4. Hydrogen peroxide (H2O2)-induced cell damage in cultured rat astrocytes,Figure

13、 5 .Alteration of the lesion size,Clinical OutputEdaravone ameliorated the size of ischemic stroke lesions and neurological deficits in patients with small-vessel occlusion, i.e. lacunar infarction, within 1 year, while there were no significant differences in outcome after 1 year. In a study compar

14、ing edaravone and citicoline in acute ischemic stroke, edaravone wasmore effective with a better neurological outcome at 3 months than citicoline,Clinical Output,Figure 6 . Alteration of the lesion size by different stroke subtypes.,cardioembolism,the large-arteryatherosclerosis,the small-vessel occ

15、lusion,Table3 Brif overview of ongoing phase III trials of neuroprotective agents,LOREM,Preclinical Output,Clinical Output,Failed?,Time window,short time windowslonger time windows,1,Target,ischemic penumbra NOT,2,Duration,the optimal durationis unknown,3,Outcome,early outcomes late assessments,4,Di

16、versity of stroke types,middle cerebral artery occlusion as a model of ischemic stroke pathophysiological heterogeneity,5,Differences in comorbidities,young healthy rodents stroke patients often suffer from several severe comorbidities,6,preclinical studies clinical trials,v,Future Directions,Establ

17、ish animal models resembling the human diseaseFrom neuroprotection to full“cerebroprotectionFrom neuronal function to neurovascular unitUnderstanding Biphasic SignalingStroke treatments and “Precision Medicine”,1. Moskowitz MA1,Lo EH,Iadecola C. The science of stroke: mechanisms in search of treatme

18、nts.Neuron.2010 Jul 29;67(2):181-98. doi: 10.1016/j.neuron.2010.07.0022. Kinga Szydlowska a,b, Michael Tymianski. Calcium, ischemia and excitotoxicity CellCalcium.2010 Feb;47(2):122-9. doi: 10.1016/j.ceca.2010.01.003. Epub 2010 Feb 18.3. George PM1,Steinberg GK2. NovelStrokeTherapeutics:UnravelingSt

19、rokePathophysiologyand ItsImpactonClinicalTreatments. Neuron.2015 Jul 15;87(2):297-309. doi: 10.1016/j.neuron.2015.05.041.4. Kaur H, Prakash A, Medhi B. Drugtherapyinstroke: frompreclinicaltoclinicalstudies. Pharmacology. 2013; 92(5-6):324-34. Epub 2013 Dec 12.5. Turner RC1,Dodson SC,Rosen CL. Thesc

20、ienceofcerebralischemiaand thequestforneuroprotection:navigatingpastfailuretofuturesuccess. J Neurosurg.2013 May;118(5):1072-85. doi: 10.3171/2012.11.JNS12408. Epub 2013 Jan 18.6. Bae ON1,Serfozo K,Baek SH et al. Safetyandefficacyevaluationofcarnosine, anendogenousneuroprotectiveagentforischemicstroke. Stroke.2013 Jan;44(1):205-12. doi: 10.1161/STROKEAHA.112.673954. Epub 2012 Dec 18.,References,THANKYOU,

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