第十六章-神经系统遗传病课件.ppt
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- 第十六 神经系统 遗传病 课件
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1、第十六章 神经系统遗传病Genetic Disease of the Nervous SystemDepartment of Neurology Second Affiliated Hospital Harbin Medical UniversityGenetic disease of nervous system 1、Introduction 2、Friedreich Ataxia 3、Spinocerebellar Ataxia(SCA)4、Charcot-Marie-Tooth Disease掌握:掌握:1、Friedreich型共济失调的主要临床特征、临床表现。2、脊髓小脑性共济失调的
2、临床表现、诊断及鉴别诊断。熟悉:熟悉:1、Friedreich型共济失调的病因、发病机制。2、脊髓小脑性共济失调的病因、发病机制。3、腓骨肌萎缩症(CMT)的临床表现、诊断及鉴别诊断。第一节 General Introduction 1.Conception Genetic disease of the nervous system 是指由于生殖细胞(germ cell)或受精卵(zygote)中的遗传物质在数量、结构或功能上发生改变,使发育的个体出现以神经系统缺欠(deficiency)为主要临床表现的疾病。Congenital Disease Family DiseaseClassific
3、ation and Genetic patternlMonogenic DisorderslPolygenic DisorderslMitochondrial DisorderslChromosome Disorders1.Monogenic disorders:The base replacement,Insert,Deletion,repeat or abnormal expansion of single gene.Autosomal dominant disorders Autosomal recessive disorders X-linked dominant disorders
4、X-linked recessive disorders 动态突变性遗传Common Diseases:Charcot-Marie-Tooth,Duchenne muscular dystrophy,Wilson Disease,Hereditary Ataxia2.polygenic disorders:are influenced by genes in complex ways which are poorly understood but involve the interaction of multiple genes and interactions between genes a
5、nd environmental factors The common polygenic disorders:Epilepsy,migraine and arteriosclerosis.3.线粒体遗传病(mitochondrial disorders)Mitochondrial disorders are caused by mutation of mitochondrion(number or structure),They are maternal inheritance.optic atrophy and mitochondrial encephalomyopathy.4.Chrom
6、osome disordersChromosome disorders are caused by the number or construction abnormalities of chromosome.for example:Downsyndrome Symptoms and physical signsClinical features are of diversity,include common and specific symptoms Common symptoms:Specific symptoms 1.Common symptoms:Mental retardation
7、and Disturbance of behavior Language dysfunction,dementia Seizure、Nystagmus,Paraesthesia(感觉异常)Involuntary movement(不自主运动)、Ataxia and Dystonia(肌张力障碍)Muscle atrophy还可有五官畸形、脊柱裂、弓型足、指(趾)畸形、皮肤毛发异常和肝脾肿大;2.Specific symptom:肝豆状核变性K-F环、共济失调毛细血管扩张症结合膜毛细血管扩张 结节性硬化症面部皮脂腺瘤 神经纤维瘤皮肤牛奶咖啡斑 4.Diagnosis:(1).临床资料的搜集:尤其
8、是发病年龄、性别、独特的症状和体征,如牛奶咖啡斑(2).系谱分析(pedigree analysis)可判断有无遗传病和区分类型(3).常规辅助检查:Include biochemistry,Electrophysiology,Imaging studies and Pathology对诊断和鉴别诊断具有重要意义,如:假肥大型肌营养不良血清学;肝豆状核变性血清铜兰蛋白、血清铜和尿铜;腓骨肌萎缩症神经活检;脊髓小脑性共济失调,橄榄脑桥小脑萎缩的头颅MRI;(4).genetic diagnosis:1)染色体检查(karyotype analysis):染色体数目异常;染色体结构畸变(const
9、ructive aberration):2)基因诊断(gene detection):方法包括:Southern Hybridization,PCR 3)Gene production detection:假性肥大肌营养不良-测定肌细胞膜上抗肌萎缩蛋白(dystrophin)5.treatment and Prevention No effective treatment 基因治疗(gene therapy)是指应用基因工程技术来更换、校正或增补基因,以达到治疗遗传病的目的,但目前基因治疗还很不成熟;其他治疗包括:Operation;medicine therapy;Diet therapy;
10、symptom therapy;rehabilitation。Prevention:important 遗传咨询(genetic counseling);避免近亲结婚;携带者检测(carrier detection);产前诊断;选择性人工流产(selective abortion);第二节 hereditary ataxia 1.Conception:Hereditary ataxia is a group of inherited and degenerative disorders of CNS.Characterized by slowly progressive ataxia.Thes
11、e disorders show considerable clinic variability.But,genetic background,ataxia and spinocerebellar lesion are mainly clinical features of them.2.Classification:Traditional classification by pathologic findings:Spinal Ataxia;Spinocerebellar Ataxia;Cerebellar ataxia;New classification by the onset of
12、age,clinical features,Genetic pattern and location of gene mutation(参考表16-1)by Harding(1993)p.270 Friedreich 型共济失调 Friedreich report this disease firstly in 1863,Its incidence rate is 2/100000,It is a early-onset ataxia and transmitted by autosomal recessive inheritance 1.Etioligy and Pathogenesis F
13、riedreich ataxia(FRDA)是由位于9号染色体长臂(9q13-21.1)基因缺陷所致。95%以上的病人有该基因第18号内含子(intron)GAA异常扩增(661700次),正常人GAA重复42次以下,扩增的GAA形成的异常螺旋结构可抑制基因转录(gene transcription)。Friedreich共济失调的基因产物Frataxin蛋白主要位于spinal cord、Skeleton muscle、heart and liver 细胞线粒体(mitochondrion)的内膜,可导致线粒体功能障碍而发病。2.Pathology Posterior columns and
14、 lateral column of spinal cord are mainly involved ,the spinal cord is thin,especially in thoracal spinal cord。Microscope can find that cell loss of posterior column,spinocerebellar tract,pyramidal tract degenerate,dorsal root ganglia and Clarkes column;peripheral nerve demyelination and gliosis;bra
15、instem、cerebellum and brain are rarely involved;Cardiomyopathy and heart cell hypertrophy。3.clinical findings(1)The age of onset is 8-15 years older commonly,with more expanded repeats correlating with earlier onset。(2).The initial symptom is progressive gait ataxia,followed by ataxia of all limbs w
16、ithin 2 years.usually,both legs are affected simultaneously,difficulty in standing and walking steadily;the hands usually become clumsy month or years after the gait disorder with intention tremor;Dysarthric speech appears after the arms are involved(rarely is this an early symptom)。(3)Physical exam
17、ination:可见水平眼震(horizontal nystagmus),垂直性(vertical)和旋转性(rotatory)眼震较少;双下肢肌无力,肌张力低(muscle tone decreased),跟膝胫试验(Heel-knee-shin)和闭目难立征(Romberg sign)阳性;下肢音叉震动觉(vibration sense)和关节位置觉(joint position sense)减退是早期体征;后期可有Babinski sign,Muscle atrophy,occasionally,sphincter distubances;约25%患者有视神经萎缩(optic atrop
18、hy);75%有上胸段脊柱侧(kyphoscoliosis),50%有弓形足(pes cavus);85%有心律紊乱、心脏杂音;10%20%伴有糖尿病(diabetes)。(4)通常起病15年后卧床(bedridden),多于4050岁死于感染或心脏病。4.investigative studies(1).skeleton film show skeletal abnormalities;CT或MRI示脊髓变细,cerebellum and brainstem are rarely involved;(2).心电图(electrocardiograph):常有T波倒置、心律紊乱及传导阻滞;(3
19、).Echocardiography:Hypertrophy;(4).视诱发电位(visual evoked potential):Amplitude decreased;(5).脑脊液(cerebrospinal fluid):normal protein;(6).DNA分析FRDA基因18号内含子GAA大于66次重复。5.Diagnosis and differential diagnosis (1).Diagnosis:Early onset;Slowly Progressive Ataxia from both legs to arms;Dysarthria,Nystagmus,ten
20、don reflex absent and Babinski sign;loss of vibratory and joint position sense;Kyphoscoliosis,Pes vacus,heart lesion;MRI显示脊髓萎缩,则不难诊断;FRDA基因GAA异常扩增,可确定诊断。(2)不典型病例需与其他疾病鉴别 慢性变性疾病和脱髓鞘性疾病(demyelinative disease),Charcot-Marie-Tooth Disease;还应与VitE缺乏和-脂蛋白缺乏引起的共济失调鉴别,后两者可查血清VitE和-脂蛋白的含量以鉴别之。6.treatment no
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