神经性肌强直一例并文献复习

目的探讨神经性肌强直(neuromyotonia,NMT)的临床特点、发病机制及诊疗方法。方法选取2023年10月解放军总医院第八医学中心神经内科NMT患者1例,回顾分析患者的临床资料,并复习2014年3月至2024年3月国内发表的NMT患者的文献报道。结果本例患者女,15岁,主要表现为双下肢疼痛、无力,伴肌肉颤搐,口服苯妥英钠后临床症状改善。结合既往文献报道,17例NMT患者中男10例、女7例,年龄27~69岁,平均(43.7±12.4)岁。17例患者均有肌肉颤搐、肌肉痉挛等表现,仅2例患者以下肢疼痛起病,12例患者血或脑脊液免疫相关抗体阳性,予对症治疗联合免疫调节后预后良好。结论肌肉颤搐、肌肉痉挛是神经性肌强直典型的临床特点,以肢体疼痛起病少见,易造成误诊;对于免疫相关抗体阴性或病因未明确者,对症治疗后仍需长期随访,在排除肿瘤或潜在肿瘤风险后,免疫治疗可能长期获益。

获得性神经性肌强直的临床、电生理及其免疫学异常(附并发于肺癌且有肌无力综合征肌电图特征的神经性肌强直1例报告)

本文报告1例38岁女性肺癌患者伴进行性全身肌肉连续性抽搐、痉挛、僵硬和无力，胸片和胸部CT提示右上肺中心型肺癌、肺不张。脑脊液IgG增高，寡克隆区带阳性。肌电图呈连续性高频肌强直放电，发作间期可见束颤电位。周围神经封闭可缓解全部肌强直症状，并消除肌电图异常连续性放电。低频重复电刺激出现衰减，高频重复电刺激动作电位波幅增高300％。患者同时有神经性肌强直和肌无力综合征肌电图特征，并与中心型肺癌和神经系统免疫学异常并存。上述改变可能与肺癌有关，提示患者神经系统IgG介导的自身免疫异常在神经性肌强直的发病机理中起重要作用。

中国遗传性神经性肌强直家系调查和遗传学特征分析

目的寻找遗传性神经性肌强直表型缺陷,并进行家系分析。方法对家系成员进行实地调查,并绘制系谱图;对调查的家系成员进行病史、神经系统检查3,例患者进行了肌电图检查。结果收集到一个5代53人的遗传性神经性肌强直家系1,7人患有该病症,其中男性13人,女性4人,发病年龄为10～20岁。临床主要表现为肌肉强直和肌肉颤搐,受累肌群包括颈部、腹部、四肢和咽喉肌肉,无发作性共济失调和癫痫发作。家系分析表明为常染色体显性遗传。结论该家系为常染色体显性遗传,主要累及周围神经系统,无中枢神经系统异常表现。受累肌肉广泛,包括极为罕见的咽喉肌。不能除外为新的致病基因所致。

抗富亮氨酸胶质瘤失活蛋白1抗体和抗接触蛋白相关蛋白2抗体脑炎28例临床特征

目的:抗富亮氨酸胶质瘤失活蛋白1(leucine-rich glioma-inactivated protein 1,LGI1)抗体、抗接触蛋白相关蛋白2(contactin-associated protein-like 2,CASPR2)抗体引起的自身免疫性脑炎较为罕见,临床异质性大,极易漏诊、误诊。本研究旨在总结抗LGI1抗体及抗CASPR2抗体脑炎患者的临床特征。方法:收集2018年1月至2021年1月中南大学湘雅医院神经内科收治的抗LGI1抗体、抗CASPR2抗体脑炎患者共28例,所有患者进行自身免疫性脑炎相关抗体谱及副肿瘤抗原谱抗体筛查。回顾性分析28例患者的临床表现、辅助检查资料、治疗及随访情况,采用改良Rankin量表评估患者治疗前后的生活能力,并对这2种自身免疫性脑炎的临床特征进行比较和分析。结果:28例中抗LGI1抗体脑炎17例,发病年龄28~83(53.18±19.08)岁,男女患者之比为9꞉8。临床表现为认知功能障碍的患者有10例,癫痫发作7例,面臂肌张力障碍发作4例,精神行为异常1例。实验室检查发现低钠血症7例;脑脊液检查异常4例,表现为白细胞数或蛋白质含量轻度上升各2例;脑电图异常13例,主要表现为慢波增多(8/13)及痫性放电(5/13);颅脑磁共振成像(magnetic resonance imaging,MRI)异常13例,主要表现为颞叶、海马及基底节区T2加权成像(T_(2)-weighted imaging,T_(2)WI)及水抑制反转恢复序列(fluid attenuated inversion recovery,FLAIR)呈高信号。抗CASPR2抗体脑炎患者11例,发病年龄17~68(47.18±16.20)岁,男女患者之比为5꞉6。7例为边缘性脑炎,1例为莫旺综合征,3例为获得性神经性肌强直;临床表现为癫痫发作者4例,精神行为异常、认知障碍和意识障碍各1例;脑脊液异常3例,主要表现为白细胞数及蛋白质含量轻度升高;脑电图异常5例,主要表现为慢波增多(3/5)及痫性放电(2/5);颅脑MRI异常2例,主要表现为颞叶、海马T_(2)WI及FLAIR高信号。16例抗LGI1抗体脑炎及8例抗CASPR2抗体脑炎患者使用糖皮质激素、免疫球蛋白及血浆置换等一线免疫治疗,均反应良好,其中1例抗LGI1抗体脑炎及3例抗CASPR2抗体脑炎患者同时口服吗替麦考酚酯维持治疗;采用免疫治疗的患者除2例失访外,随访期内(6~36个月)均未见明显复发。2种抗体脑炎在认知障碍、低钠血症、颅脑MRI异常上差异均有统计学意义(均P<0.05)。结论:抗LGI1抗体及抗CASPR2抗体脑炎均可表现为边缘性脑炎,抗LGI1抗体脑炎以认知障碍为主要表现,面臂肌张力障碍发作及低钠血症为特征性表现,易出现颅脑MRI异常;抗CASPR2抗体脑炎以癫痫发作为最常见临床表现,可累及周围神经系统而出现神经性肌强直、莫旺综合征且易合并肿瘤。2种抗体脑炎均对免疫治疗敏感,预后良好。

儿童神经性肌强直3例报告并文献复习

目的提高对儿童神经性肌强直病的认识。方法回顾分析3例儿童神经性肌强直的临床、肌电图表现及治疗。结果3例病例的临床表现和肌电图符合神经性肌强直的临床特征,应用卡马西平或苯妥英钠治疗有效。结论儿童神经性肌强直可能是一种罕见的自身免疫性疾病,需与强直性肌病等相鉴别。

4例神经性肌强直患者电生理学和临床特点探讨

目的:探讨神经性肌强直(NMT)的临床表现、肌电图及治疗特点。方法:回顾性分析临床确诊的4例NMT患者的临床表现、肌电图及治疗特点。结果:4例患者临床表现均以静息状态下肌肉颤搐为主,肌电图显示自发的、连续的、不规则的多重单个运动单元高频率放电,其中3例单纯卡马西平或苯妥英钠效果不佳,加用激素治疗后获痊愈。结论:卡马西平或苯妥英钠治疗获得性NMT可缓解症状,效果不佳时结合激素治疗,疗效显著,支持获得性NMT与免疫功能紊乱相关。

一个中国神经性肌强直家系致病基因初步研究

目的对一遗传性神经性肌强直家系2个已知致病基因进行初步筛查。方法应用外显子高通量测序分析方法对家系患者的KCNA1基因和KCNQ2基因进行DNA测序。结果基因检测未发现KCNA1基因和KCNQ2基因外显子突变。结论该神经性肌强直家系的发病与KCNA1基因和KCNQ2基因无关。

Oxaliplatin induced hyperexcitability syndrome in patient with appendiceal adenocarcinoma

Oxaliplatin is a novel platinum compound with clinical activity against several solid tumors. It has been associated with sensory neuropathies and, rarely, a neuromyotonia-like hyperexcitability syndrome;a form of peripheral neuropathy manifested by tremor and twitching activity of muscles. We present a case of hyperexcitability syndrome developed during the treatment of stage III appendiceal adenocarcinoma with oxaliplatin-containing regimen and was successfully treated with Pregabalin.

Case Report: A 72 Years Old Man with Isaacs’ Syndrome: A Rare Entity with Different Outcomes

Neuromyotonia is a neuromuscular hyperexitability disorder characterized by muscle stiffness caused by continuous muscle fiber activity. It is an immune mediated disorder with elevated antibody level against presynaptic, voltage gated potassium channels, either as isolation or as a paraneoplastic process. Symptoms usually include muscle twitching during rest (myokymia), cramps, peudomyotonia (delayed relaxation), increased sweating, and sometimes motor weakness. In this case report, we present a seventy-two years old man who presented with pain in both thighs for one month. It gradually became worse to involve feet and chest. His brain CT scan showed features of brain atrophy. EMG showed fasciculation along neuromyotonic discharges with characteristic wave in frequency and amplitude typical of Isaacs’ syndrome. Potassium channel antibodies were very high. Diagnosis of Isaacs’ syndrome was made. He was followed up for two months with treatment by three-day course of methyl prednisolone followed by oral steroid and methotrexate with much improvement. This is the first case of Isaacs’ syndrome in Kurdistan.

神经性肌强直5例报告并文献复习

目的探讨Isaacs综合征临床表现、肌电图特点及临床转归。方法分析5例神经性肌强直病例的临床症候、肌电图表现、诊断及治疗情况,并进行文献回顾。结果 5例病例临床主要表现为肌肉颤搐、多汗等;肌电图表现为持续快速的二联、三联或多联的运动单位放电活动;应用卡马西平可缓解临床症状。结论神经性肌强直是一种少见的周围神经病变,自发性连续性肌肉活动为其主要表现;肌电图特点为持续快速的二联、三联或多联运动单位放点活动;应用卡马西平治疗有效,但仍需定期随访。

抗富亮氨酸胶质瘤失活蛋白1抗体相关的神经性肌强直1例并文献复习

本文报道1例临床表现为肌肉颤搐、血清LGI1抗体阳性,诊断为抗LGI1抗体相关的神经性肌强直的病例,并通过复习文献论述其病因及发病机制。1临床资料患者,女性,30岁,慢性病程,进行性加重;主因“发现肌肉蠕动1 y余”入院;1 y前无明显诱因出现双下肢乏力、酸痛,小腿肌肉蠕动,发作性、静止状态出现,疲劳后明显,睡眠时有发作并伴有肌肉痉挛,未在意。

罕见眼球运动障碍1例

患者男性,47岁,主诉右眼睑裂变小伴发作性复视4年。检查发现患者为发作性内斜视。非发作期(静息期)表现为右侧动眼神经麻痹:右眼上睑下垂,外斜位,右眼内、上、下转不到位。患者向上方过度注视可诱发双侧动眼神经肌强直发作:所支配的肌肉发生强直收缩,包括双眼上睑提肌、内直肌、上直肌和右眼下直肌,表现为上睑抬高,尤其是向下方注视时上睑不能跟随下落,内转和垂直运动受限。双眼瞳孔未见明显异常。每次发作持续约10 s~1 min,闭眼休息可终止发作。患者25年前曾因鼻咽癌行放疗。最终诊断:眼神经肌强直(双侧动眼神经受累),鼻咽癌放疗后。卡马西平治疗后,患者症状得到有效控制。讨论体会:眼神经肌强直是导致发作性复视的罕见病因,其最常见于鞍区及颅底放疗后,本病卡马西平治疗有效。

HINT1基因变异致常染色体隐性遗传轴索型神经病伴神经性肌强直藏族家系及文献复习

目的分析HINT1基因变异致常染色体隐性遗传轴索型神经病伴神经性肌强直(ARAN-NM)的特点。方法回顾性病例总结。分析2023年8月在北京大学第一医院儿科确诊为ARAN-NM的2例藏族兄妹的临床资料。检索各个数据库收录的相关中国病例的文献并进行分析。结果先证者及其兄分别为13岁和19岁,均于11岁出现步态异常,其后出现足内翻及跛行、拇指力弱,先证者合并神经性肌强直。查体先证者及其兄均四肢肌力下降,拇指和下肢远端为著,先证者下肢远端肌肉萎缩,先证者兄双手肌肉萎缩,二人双足均马蹄内翻畸形。先证者肌电图(EMG)检查示周围神经病损(运动和感觉纤维轴索受累,远端受累为重)和肌强直电位。家系全外显子组测序检测到二人HINT1基因纯合致病性变异[c.169A>G(p.K57E)],确诊ARAN-NM。先证者口服卡马西平后神经性肌强直症状缓解,麻木、无力症状明显改善。先证者和其兄行骨科手术治疗和康复治疗后足部畸形及步态明显改善。检索到符合条件的中文文献2篇(2例),英文文献4篇(8例)。加上本例先证者及其兄共12例,10例有临床资料,起病年龄为2~16岁(1例未知),诊断年龄为13~33岁,9例有肌无力,肌无力以远端为著,8例伴神经性肌强直,9例出现肌肉萎缩,7例合并足畸形,2例合并感觉障碍,9例检测肌酸激酶的患者均有升高,EMG均提示神经源性损伤,6例可见神经性肌强直放电,3例接受卡马西平治疗,部分症状缓解。12例均有遗传学资料,均为错义突变/无义突变,高频变异为c.112T>C(p.C38R)。结论ARAN-NM是由HINT1基因变异引起的常染色体隐性遗传性罕见神经肌肉病,临床表现无民族差异,主要为肢体远端无力伴神经性肌强直,卡马西平可缓解部分症状,骨科矫形治疗可改善足部畸形和步态。

电压门控性钾通道抗体病及其治疗

越来越多的证据显示,某些抗体如电压门控性钙通道及钾通道等抗体病与神经系统疾病密切相关,并且这些疾病大多免疫抑制治疗有效。本文就电压门控性钾通道抗体病:神经性肌强直。

获得性神经肌强直的临床特征分析

目的探讨获得性神经肌强直主要临床表现和电生理特征。方法回顾性分析3例获得性神经肌强直男性患者的临床和肌电图特点,并结合文献进行分析。结果 3例患者发病年龄21~64岁。3例患者均无中枢损害,其中2例表现为典型的骨骼肌游走性波浪状蠕动,另1例为肌肉疼痛、痉挛和肌无力、多汗。3例患者经电生理检查提示神经传导均正常,2例肌电图均可见特征性肌纤维颤搐表现。结论获得性神经肌强直主要表现为肌肉不自主颤搐、痉挛和假性肌强直,可合并多汗等植物神经损害表现。

Prediction of post-progression survival in patientswith advanced hepatocellular carcinoma treated with sorafenib by using time-dependent changes inclinical characteristics

Aim: Sorafenib has been shown to improve time to tumor progression (TTP) and overall survival (OS) in patients with hepatocellular carcinoma (HCC);however, post-progression survival (PPS) has not been well characterized in these patients. This study aimed to evaluate the predictors of PPS by using time-dependent and dynamic changes in radiologic progression patterns, liver function, and performance status (PS) in patients with advanced HCC receiving sorafenib treatment. Methods: We retrospectively analyzed the clinical characteristics of 128 advanced HCC patients with Child-Pugh scores ≤ 7 at the initiation of sorafenib treatment. Results: The median TTP, OS, and PPS were 3.8, 15.6, and 9.9 months, respectively. At the time of confirmation of radiologic progressive disease (PD), a total of 46 (35.6%) patients showed impairments in their PS of ≥ +1 points over time. For the Child-Pugh score, 27 (21.1%) and 26 (10.9%) patients exhibited an impairment of ≥ +1 and ≥ +2 points, respectively. Multivariate analysis identified the following independent predictors of PPS: impairment in the PS score of ≥+1 point [hazard ratio (HR) 1.81, 95% confidence interval (CI) 1.16-2.82], impairment in the Child-Pugh score of ≥ +2 points (HR 3.70, 95% CI 1.68-8.15), radiologic pattern of progression (target lesion growth and emergence of a new lesion) (HR 2.91, 95% CI 1.79-2.91), a TTP < 4 months(HR 1.87, 95% CI 1.21-2.91), second-line treatment after radiologic confirmation of PD (HR 0.16, 95% CI 0.08-0.32), and continuous sorafenib treatment after radiologic confirmation of PD (HR 1.76, 95% CI 1.06-3.00). Conclusion: PPS in patients with advanced HCC can be characterized by using time-dependent dynamic changes in clinical parameters.

Neurological diseases associated with autoantibodies targeting the voltage-gated potassium channel complex:immunobiology and clinical characteristics

Voltage-gated potassium channels(VGKCs)represent a group of tetrameric signaling proteins with several functions,including modulation of neuronal excitability and neurotransmitter release.Moreover,VGKCs give a key contribution to the generation of the action potential.VGKCs are complexed with other neuronal proteins,and it is now widely known that serum autoantibodies directed against VGKCs are actually directed against the potassium channel subunits only in a minority of patients.By contrast,these autoantibodies more commonly target three proteins that are complexed with alpha-dendrotoxin-labeled potassium channels in brain extracts.These three proteins are contactin-associated protein-2(Caspr-2),leucine-rich,glioma inactivated 1(LGI-1)protein and the protein Tag-1/contactin-2.Neoplasms are detected only in a minority of seropositive patients for VGKC complex-IgG and do not significantly associate with Caspr-2 or LGI-1.Among all the cancers described in association with VGKC complex-IgG,lung carcinoma,thymoma,and hematologic malignancies are the most commonly detected.We will review all the major neurological conditions associated with VGKC complex-IgG.These include Isaacs’syndrome,Morvan syndrome,limbic encephalitis,facio-brachial dystonic seizures,chorea and other movement disorders,epilepsy,psychosis,gastrointestinal neuromuscular diseases,a subacute encephalopathy that mimics Creutzfeldt-Jakob prion disease both clinically and radiologically and autoimmune chronic pain.The vast majority of these conditions are reversible by immunotherapy,and it is becoming increasingly recognized that early diagnosis and detection of VGKC complex-IgG is critical in order to rapidly start the treatment.As a result,VGKC complex-IgG are now part of the investigation of patients with unexplained subacute onset of epilepsy,memory or cognitive problems,or peripheral nerve hyperexcitability syndromes.

Steroids and plasma exchange in Isaacs' syndromewith anti-Caspr2 antibodies

Isaacs' syndrome is a disease characterized by nerve hyperexcitability. The patients are commonly treated with symptomatic therapies and immunomodulatory approaches, but no clinical trials are available to date. Here, we report the case of an anti-Caspr2-positive patient, presenting with continuous muscle twitches and diffuse muscle pain. He experienced a nearly complete clinical response to intravenous high-dose steroids combined with plasma exchange, sustained for at least 1 year. Our experience suggests that methylprednisolone 1000 mg/day × 5 days and consecutive tapering followed by plasma exchange may be efficient and well tolerated in patient with Isaacs' syndrome due to anti-Caspr2 antibodies.

周围神经过度兴奋综合征

周围神经过度兴奋综合征(peripheral nerve hyperexcitability syndromes,PNHS)是一组异质性疾病,临床和神经电生理均有不同程度的神经过度兴奋表现。主要包括Isaacs综合征、Morvan综合征和痉挛-束颤综合征,其中Isaacs综合征最常见。常以肌肉抽搐、痉挛、僵硬和神经性疼痛为主要表现。针电极肌电图对PNHS的诊断具有重要作用,可发现肌颤搐、神经性肌强直、痉挛电位和束颤电位等。文中就PNHS的临床表型、病理生理学、神经电生理特点及治疗进展进行综述。

一例神经性肌强直与轴索型神经病患者的HINT1基因变异研究

目的探讨1个神经性肌强直与轴索型神经病(neuromyotonia and axonal neuropathy,NMAN)家系的临床及遗传学特点。方法收集先证者及其双亲的临床资料与外周血样,应用三联重复引物PCR联合毛细管电泳检测先证者强直性肌营养不良致病基因DMPK与ZNF9的动态突变;应用高通量测序筛查神经系统遗传病致病基因的变异,用Sanger测序验证检出的基因变异;应用Sanger测序分析双亲及100名非病个体的变异位点基因型;分析基因变异的致病性。结果未发现DMPK与ZNF9基因动态突变位点的异常扩展;测序结果显示先证者HINT1基因第3外显子存在c.335C>T(p.R119W)纯合错义变异,其表型正常的双亲均为上述变异的携带者,对照群体未检出该变异。基于ACMG指南的评价提示为致病性变异。结论在NMAN患者中发现的这个新的致病变异(c.335C>T,p.R119W)为HINT1基因与NMAN的关系提供了更多的证据,填补了中国人群HINT1基因突变谱的空白。