变性高效液相色谱在检测肝豆状核变性基因突变中的作用

目的　建立变性高效液相色谱 (denaturinghighperformanceliquidchromatography,DHPLC)技术检测肝豆状核变性 (WD)基因第 8外显子突变。方法　利用聚合酶链式反应 (PCR)扩增WD基因第 8外显子片段 ,扩增产物直接进行DHPLC分析 ;对峰型有改变的样品经测序分析确认突变。结果　在 5 1例WD先证者中共发现两种错义突变 (Arg778Leu和Arg778Gln)、一种插入突变 (Ins2 30 2C)和一种多态性位点 (C2 310G)。其中 12例先证者带有Arg778Leu杂合错义突变 ,3例为Arg778Leu纯合错义突变 ,1例为Arg778Gln杂合错义突变 ,1例为杂合 2 30 2C插入突变。多态位点C2 310G与Arg778Leu突变完全连锁。结论　WD基因第 8外显子阳性检出率为 33 3% (17/ 5 1) ,说明DHPLC技术是一种可用于临床WD基因诊断的高效、灵敏和操作简便的方法     

X连锁腓骨肌萎缩症Cx32基因的突变、临床和电生理特点

目的 分析X连锁腓骨肌萎缩症（CMTX）患者Cx32基凶的突变及其临床表现和电生理特点、方法应用多聚酶链反应一单链构象多态性分析结合DNA直接测序的方法,对24例无周围髓鞘蛋白（PMP）22基因大片段重复突变,家系中无男传男的腓骨肌萎缩症（CMT）先证者进行Cx32基因的突变分析;对先证者及其家系内患者进行临床和电生理检查。结果 在6个X连锁遗传家系和1例散发患者中发现了7个不同的Cx32基因突变,其中4个家系临床分型为CMTI型,2个家系为CMT中间型,散发病例为CMT1型检测到有Cx32基因突变的家系成员共38例,其巾男性20例,全部为CMTX患者;女性18例,其中6例为CMTX患者,12例为无临床症状的携带者;26例患者均为周围神经轻、中度受累。结论 CMTX的遗传方式可为X连锁显性、X连锁隐性遗传,也可为散发。根据临床和电生理特点分为CMTI型或CMT中间型,多为周围神经轻、中度受累,男性患者的症状通常较女性重。在没有检测到PMP22基因大片段重复突变和无男传男的CMT家系中应首先进行Cx32基因突变分析。     

伴皮质下梗死及白质脑病常染色体显性遗传性脑动脉病的NOTCH3基因诊断

目的 分析伴皮质下梗死及白质脑病常染色体显性遗传性脑动脉病((CADASIL)的NOTCH3基因突变类型.方法 对临床诊断为CADASIL的4例先证者、来自3个家系10例患者及4例无类似临床表现成员、以及100名健康对照者进行NOTCH3基因PCR扩增及变性高压液相色谱分析(DHPLC)检测;对DHPLC阳性结果进行DNA双向测序,明确致病性突变或多态类型.结果 在CADASIL先证者及其家系患者中共发现134半胱氨酸→酪氨酸(Cys134Tyr)、141精氨酸→半胱氨酸(Arg141Cys)、90精氨酸→半胱氨酸(Arg90Cys)3种突变类型,存在于第3、第4外显子,为杂合错义突变.同时发现15种多态类型.其中家系1和家系2中分别发现1名成员与先证者存在相同位点的NOTCH3基因致病性突变,尚未出现与先证者相应的临床表现,被确定为临床前期患者.结论 NOTCH3单基因突变是CADASIL的分子遗传学基础,第3、4外显子可能是中国CADASIL家系的热点突变区.第4外显子Cys134Tyr突变类型为国内首次报告.     

河南一腓骨肌萎缩症家系分析并文献复习

目的报道一腓骨肌萎缩症(peroneal muscular atrophy)家系的临床表现、影像学特征、基因特点和遗传方式,并结合文献进行复习。方法分析一腓骨肌萎缩症家系中患有糖尿病的先证者以进行性对称性远端肌无力和肌肉萎缩、腱反射减弱或消失、远端感觉减退为临床表现,行电生理、基因检测等检查,并对其家属行多重链接探针扩增技术(MLPA)检测周围神经髓鞘蛋白22(peripheral nervemyelinprotein 22,PMP22)基因外显子缺失/重复变异情况。结果本家系先证者为中年男性,肌电图提示四肢多发性周围神经病,脱髓鞘继发轴索损害。患者有家族史,基因检测先证者、先证者女儿、先证者哥哥PMP22基因外显子及附近区域存在大片段重复。结论腓骨肌萎缩症临床表现典型,有特征性电生理,PMP22基因外显子大片段重复是确诊金标准,合并糖尿病会加重腓骨肌萎缩症的周围神经损害。     

家族性阿尔茨海默病的早老素-1基因突变三例报告

目的 探讨早老素-1基因突变在家族性阿尔茨海默病(FAD)发病机制中的作用。方法采用美国国立神经病、语言机能障碍和卒中研究所及阿尔茨海默病和相关疾病协会(NINCDSADRDA)AD诊断标准对AD家系的三代人共23名进行筛查和诊断，并应用聚合酶链反应-单链构象多态性(PCR-SSCP)、变性高效液相(DHPLC)和DNA序列分析技术对该家系以及对照组的早老素-1(PS-1)基因第4、5号外显子进行检测。结果 家系23名中有3例被确诊为FAD。研究发现这3例FAD患者的PCR-SSCP泳动发生异常，又经DHPLC检测有双峰出现，提示有突变存在的可能。最后经DNA序列分析确认，PS-1基因第4号外显子的97号密码子发生了GTG→TTG错义突变(289位点发生G→T突变)，此密码子的氨基酸由缬氨酸变为亮氨酸(Val 97Leu)，第5号外显子未发现突变。家系内健康人及对照组的第4、5号外显子经以上检测也未发现突变。结论 该AD家系中的AD患者存在早老素-1第4号外显子的突变，此突变点与中国人FAD发病有关。     

X连锁Charcot-Marie-Tooth病1型六个家系的病理和基因突变特点

目的 报道6个X连锁Charcot-Marie-Tooth病1型(CMTX1)家系的神经病理和基因型改变特点.方法 6个CMTX1家系的先证者均为男性,发病年龄11 ～24岁,出现下肢远端为主的肌无力、腱反射减低和轻度感觉减退.先证者1伴随发作性白质脑病,先证者5伴随小脑性共济失调.12名家系成员也出现周围神经损害症状,另7名存在高弓足或腱反射减低.对6例先证者行腓肠神经活体组织检查,并对6例先证者、8名受累家庭成员和10名无症状家系成员及50名健康女性进行缝隙连接蛋白32( Cx32)基因测序.结果 6例先证者有髓神经纤维出现轻-中度减少伴轴索再生变性,5例出现薄髓鞘神经纤维,其中3例伴洋葱球样结构,2例伴炎细胞浸润.6个家系的Cx32基因存在5种新突变和1种同义突变,即L20T、I127F、D178G、A197V错义突变,403_404T insT插入突变和L10L沉默突变,10名无症状家系成员中有4名女性为携带者,6名男性和健康对照均没有这些基因突变.结论 该组CMTX1患者的周围神经病理改变以慢性轴索损害为主,Cx32基因较多新突变的出现提示我国CMTX1患者具有个体突变特点.     

腓骨肌萎缩症伴神经性耳聋一家系临床和分子遗传学分析

目的探讨一个X连锁腓骨肌萎缩症(CMTX)伴常染色体隐性遗传的神经性耳聋家系的临床特点并研究其分子遗传学病因。方法对9名家系成员进行详细的临床检查，先证者进行了神经肌电图、听觉诱发电位和神经活检，3名耳聋患者进行电测听检查。运用聚合酶链反应一单链构象多态性分析技术(PCR-SSCP)结合直接测序法进行间隙连接蛋白32(eonnexin32)的突变分析，直接测序法进行间隙连接蛋白26(connexin26)的突变分析。结果家系中3名腓骨肌萎缩症患者为X连锁显性遗传，3名神经性耳聋患者为常染色体隐性遗传，其中1名患者同时出现腓骨肌萎缩症和神经性耳聋的临床症状。CMTX由connexin32错义突变C223T(Arg75Trp)引起。耳聋症状与connexin32点突变无共分离现象，对connexin26直接测序亦未发现突变，耳聋的致病基因有待进一步探讨。结论该家系腓骨肌萎缩症和耳聋分别由不同基因突变引起，这种在一个家系中同时出现两种不同遗传方式，不同致病基因的遗传病罕有报道。     

腓骨肌萎缩症X1型1个家系的临床、电生理和Connexin32基因突变分析

目的观察腓骨肌萎缩症(CMT)X1型的临床、电生理特点和Connexin32(Cx32)基因突变情况.方法对1个无基因重复的临床可疑的CMTX1家系中的3例患者进行详尽的临床和神经电生理检查,并应用变性高效液相色谱结合混和样品池法和DNA序列测定对包括先证者在内的3名成员的Cx32基因进行突变检测.结果 该家系中的病人发生了Gly12Ser,50名正常人中未发现上述改变,提示该突变为致病性突变.家系中男性病人临床症状重于女性;电生理特点为脱髓鞘改变;同一病人的不同神经间存在异质性.结论 Gly12Ser突变可能导致原发性脱髓鞘性神经病,不伴有特殊的临床表现.     

Dravet综合征的SCNlA基因突变

目的筛查9个Dravet综合征患者的钠通道α1（5CN1A）基因，明确该综合征与SCN1A基因的关系。方法总结9个中国人Dravet综合征患者的临床特点，收集Dravet综合征患者血样，应用变性高效液相色谱（DHPLC）技术对该综合征患者进行SCN1A基因全部26个外显子筛查，对发现异常洗脱峰者进行测序并分析结果。结果编号为EP91的先证者经DHPLC筛查发现SCNIA基因26号外显子有双峰，经测序证实26号外显子发生错义突变．造成1765位氨基酸-苯丙氨酸突变为亮氨酸（Phel 765Leu），该突变为杂合突变。结论中国人Dravet综合征与．SCN1A基因突变有一定的关系。     

一个2A型肢带型肌营养不良家系CAPN3基因的突变分析

目的对一个2A型肢带型肌营养不良(limb-girdle muscular dystrophy type 2A)家系进行CAPN3基因的致病突变分析。方法收集先证者及家系成员的外周血,提取DNA,应用全外显子测序技术对先证者进行致病基因检测,然后用Sanger测序技术对先证者家系成员进行突变位点的验证。结果全外显子测序发现先证者携带CAPN3基因c. 1194-9A G和c. 1437C T (p. ser479=)的复合杂合突变。Sanger测序验证先证者母亲为CAPN3基因c. 1194-9A G变异携带者。家系中其他患者均存在相同的复合杂合突变,其未发病的姐姐和女儿为CAPN3基因c. 1437C T (p. ser479=)变异携带者,先证者的女婿未检测到上述位点变异。结论 CAPN3基因c. 1194-9A G和c. 1437C T (p. ser479=)的复合杂合突变为该家系的致病原因。     

Epilepsy and anomalies of neuronal migration: MRI and clinical aspects

Neuronal migration disorders are the result of disturbed brain development. In such disorders, neurons are abnormally located. In diagnosing these conditions, magnetic resonance imaging is superior to any other imaging technique. This enables us to improve our knowledge of the clinical correlates of neuronal migration. With reference to migrational disorder, a retrospective study of all 303 patients with epileptic seizures referred for magnetic resonance imaging during a 3-year period was performed, 13 patients (aged 12-41, mean age 27) were identified. They represent 4.3% of the entire study group. Of the patients with known epilepsy, 6.7% and of the mentally retarded, 13.7% had migrational disorders. Four patients had schizencephaly as the dominant finding, one was classified as hemimegalencephaly, 2 had isolated heterotopias, and 6 had localized pachy- and/or poly-microgyria. The clinical pictures are complex. Ectopias of grey matter are recognised foci of epilepsy, but from an epileptological and a clinical viewpoint little attention has been given to these disorders. The present study shows that malmigration is not rare in epilepsy patients, especially not in the mentally retarded.     

Hepatic Considerations in the Use of Antiepileptic Drugs

Summary: Virtually all of the major antiepileptic drugs (AEDs) can cause hepatotoxicity, although fatal hepatic reactions are rare. The mechanisms, incidences, and risk profiles for such reactions differ from drug to drug. With carbamazepine and phenytoin, hepatotoxicity may be due to drug hypersensitivity. Although the profiles of patients at risk have not been well-defined for these two antiepileptic drugs, it would appear from reports in the literature that older adolescents and adults are at higher risk than children of developing serious or fatal hepatotoxicity. Once hepatotoxicity develops, mortality rates are 10–38% with phenytoin and 25% for carbamazepine. The risk profile for valproate fatal hepatotoxicity has been more clearly defined. Those at primary risk of fatal hepatic dysfunction are children under the age of 2 years who are receiving multiple anticonvulsants and also have significant medical problems in addition to severe epilepsy. The risk is considerably lower for patients over the age of 2 years on valproate monotherapy. In contrast to the risk profile with other AEDs, adults receiving valproate as monotherapy have the lowest risk of hepatotoxicity. Fatal hepatic dysfunction coincident with valproate may be the result of aberrant drug metabolism. Concomitant use of AEDs that induce microsomal P450 enzymes (e.g., phenytoin and phenobarbital) may enhance the production of a toxic metabolite, and hence the greater risk of hepatotoxicity with polypharmacy.     

Vascular Malformations and Epilepsy: Clinical Considerations and Basic Mechanisms

Summary: Vascular malformations (VMs) are associated with epilepsy. The natural history of the various VMs, clinical presentation, and tendency to provoke epilepsy determine treatment strategies. Investigations have probed the mechanisms of epileptogenesis associated with these lesions. Electrophysiologic changes are associated with epileptogenic cortex adjacent to VMs. Putative pathophysiologic mechanisms of epileptogenesis include neuronal cell loss, glial proliferation and abnormal glial physiology, altered neurotransmitter levels, free radical formation, and aberrant second messenger physiology.     

Classification of methods in transcranial Electrical Stimulation (tES) and evolving strategy from historical approaches to contemporary innovations

Transcranial Electrical Stimulation (tES) encompasses all methods of non-invasive current application to the brain used in research and clinical practice. We present the first comprehensive and technical review, explaining the evolution of tES in both terminology and dosage over the past 100 years of research to present day. Current transcranial Pulsed Current Stimulation (tPCS) approaches such as Cranial Electrotherapy Stimulation (CES) descended from Electrosleep (ES) through Cranial Electro-stimulation Therapy (CET), Transcerebral Electrotherapy (TCET), and NeuroElectric Therapy (NET) while others like Transcutaneous Cranial Electrical Stimulation (TCES) descended from Electroanesthesia (EA) through Limoge, and Interferential Stimulation. Prior to a contemporary resurgence in interest, variations of transcranial Direct Current Stimulation were explored intermittently, including Polarizing current, Galvanic Vestibular Stimulation (GVS), and Transcranial Micropolarization. The development of these approaches alongside Electroconvulsive Therapy (ECT) and pharmacological developments are considered. Both the roots and unique features of contemporary approaches such as transcranial Alternating Current Stimulation (tACS) and transcranial Random Noise Stimulation (tRNS) are discussed. Trends and incremental developments in electrode montage and waveform spanning decades are presented leading to the present day. Commercial devices, seminal conferences, and regulatory decisions are noted. We conclude with six rules on how increasing medical and technological sophistication may now be leveraged for broader success and adoption of tES.     

Carbamazepine Efficacy and Utilization in Children

Summary: Carbamazepine is effective for preventing partial and generalized tonic-clonic seizures in children. Although absence epilepsies are more common in children than adults, an estimated 80% of children with epilepsy have seizure types or epilepsies that are potentially responsive to carbamazepine. The differential diagnosis of ictal staring is an especially important issue in children because absence and atypical absence seizures are more prevalent in children than adults. Age-related pharmacokinetic differences and drug interactions are major considerations in children. On average, children have higher clearance rates of carbamazepine, shorter half-lives, and higher ratios of carbamazepine-10, 11-epoxide to carbamazepine than adults. In addition, children with severe epilepsy are more likely to require multiple-drug therapy, which can lead to complex drug interactions. When carbamazepine is administered along with valproate, drug protein binding interactions can cause intermittent side effects.     

Neonatal Seizures: Problems in Diagnosis and Classification

Summary: The clinical identification of neonatal seizures is critical for the recognition of brain dysfunction; however, diagnosis is often difficult because of the poorly organized and varied nature of these behaviors. Current classification systems are limited in their ability to communicate motor, autonomic, and electroencephalo-graphic features of seizures precisely and to provide a basis for uniform effective diagnosis, therapy, and determination of prognosis. Recent investigations of neonates, utilizing bedside electroencephalographic/polygraphic/ video monitoring techniques, have provided the basis for improved diagnosis and classification of seizures in the newborn. These studies have demonstrated that not all clinical phenomena currently considered to be seizures require electrocortical epileptiform activity for their initiation or elaboration. In addition, the specific clinical character of the phenomena considered to be seizures, the clinical state of the infant, and the character of the EEG indicate the probable pathophysiological mechanisms involved and suggest probable etiologies, prognosis, and therapy. Similarities between animal models that demonstrate reflex physiology and neonates with motor automatisms and tonic posturing suggest that these clinical behaviors may not be epileptic in origin but, rather, primitive movements of progression and posture mediated by brainstem mechanisms. Although not all clinical behaviors currently considered to be neonatal seizures may have similar pathophysiological mechanisms, they are clinically significant because they all indicate brain dysfunction.     

Valproate Monotherapy in the Management of Generalized and Partial Seizures

Summary: For decades, therapeutic tradition has promoted the concept of polypharmacy in the management of epilepsy. In recent years, however, studies have shown that, for most patients, monotherapy can provide comparable or better seizure control than administration of multiple anticonvulsants, while diminishing the potential for adverse reactions, drug interactions, and poor compliance. Valproate is an important monotherapeutic agent that is highly effective in the control of idiopathic primary and secondarily generalized epilepsies, and partial seizures that do not generalize. Comparative studies have found that valproate is at least as effective as phenytoin and carbamazepine in the treatment of generalized and partial seizures. Given the similar efficacy, other factors such as pharmacokinetics and side effects may therefore determine anticonvulsant selection for monotherapy.     

Un nouveau cadre conceptuel de travail pour la psychiatrie

In an attempt to place psychiatric thinking and the training of future psychiatrists more centrally into the context of modern biology, the author outlines the beginnings of a new intellectual framework for psychiatry that derives from current biological thinking about the relationship of mind to brain. The purpose of this framework is twofold. First, it is designed to emphasize that the professional requirements for future psychiatrists will demand a greater knowledge of the structure and functioning of the brain than is currently available in most training programs. Second, it is designed to illustrate that the unique domain which psychiatry occupies within academic medicine, the analysis of the interaction between social and biological determinants of behavior, can best be studied by also having a full understanding of the biological components of behavior.