Hypergonadotrophic Hypogonadism with Cerebellar Ataxia in a Twenty-Six-Year-Old Female: A Case Report

Gordon Holmes Syndrome is a rare inherited disease characterized by both neurological and reproductive signs and symptoms. Most patients develop neurologic challenges in early adulthood and cerebellar ataxia occurs as the disease progresses. In the majority of patients, hypogonadism is hypogonadotropic but rarely hypergonadotropic. We report a case of a 26-year-old female in Nigeria, with hypergonadotropic hypogonadism and cerebellar atrophy from a non-consanguineous marriage and no family history.

Molecular diagnosis of autosomal recessive cerebellar ataxia in the whole exome/genome sequencing era

Autosomal recessive cerebellar ataxias(ARCA) are a clinically and genetically heterogeneous group of rare neurodegenerative disorders characterized by autosomal recessive inheritance and an early age of onset. Progressive ataxia is usually the prominent symptom and is often associated with other neurological or additional features. ARCA classification still remains controversial even though different approaches have been proposed over the years. Furthermore, ARCA molecular diagnosis has been a challenge due to phenotypic overlap and increased genetic heterogeneity observed within this group of disorders. Friedreich's ataxia and ataxia telangiectasia have been reported as the most frequent and well-studied forms of ARCA. Significant progress in understanding the genetic etiologies of the ARCA has been achieved during the last 15 years. The methodological revolution that has been observed in genetics over the last few years has contributed significantly to the molecular diagnosis of rare diseases including the ARCAs. Development of high throughput technologies has resulted in the identification of new ARCA genes and novel mutations in known ARCA genes. Therefore,an improvement in the molecular diagnosis of ARCA is expected. Moreover, based on the fact that many patients still remain undiagnosed, additional forms of ataxia are expected to be identified. We hereby review the current knowledge on the ARCAs, focused on the genetic findings of the most common forms that were molecularly characterized before the whole exome/genome era, as well as the most recently described forms that have been elucidated with the use of these novel technologies. The significant contribution of wholeexome sequencing or whole-genome sequencing in the molecular diagnosis of ARCAs is discussed.

Genetic spectrum and clinical features in a cohort of Chinese patients with autosomal recessive cerebellar ataxias

Background:Although many causative genes have been uncovered in recent years,genetic diagnosis is still missing for approximately 50%of autosomal recessive cerebellar ataxia(ARCA)patients.Few studies have been performed to determine the genetic spectrum and clinical profile of ARCA patients in the Chinese population.Methods:Fifty-four Chinese index patients with unexplained autosomal recessive or sporadic ataxia were investigated by whole-exome sequencing(WES)and copy number variation(CNV)calling with ExomeDepth.Likely causal CNV predictions were validated by CNVseq.Results:Thirty-eight mutations including 29 novel ones were identified in 25 out of the 54 patients,providing a 46.3%positive molecular diagnostic rate.Ten different genes were involved,of which four most common genes were SACS,SYNE1,ADCK3 and SETX,which accounted for 76.0%(19/25)of the positive cases.The de novo microdeletion in SACS was reported for the first time in China and the uniparental disomy of ADCK3 was reported for the first time worldwide.Clinical features of the patients carrying SACS,SYNE1 and ADCK3 mutations were summarized.Conclusions:Our results expand the genetic spectrum and clinical profiles of ARCA patients,demonstrate the high efficiency and reliability of WES combined with CNV analysis in the diagnosis of suspected ARCA,and emphasize the importance of complete bioinformatics analysis of WES data for accurate diagnosis.

Electricity: Past and Future or Black Holes and Green Planet

“Something is rotten in the state of Denmark”. These words of Shakespeare remember us that any small case can be connected with wider situation in the Globe. We would like to understand how changes electrical systems in time and what we will get in future. But what we know today about our home? Prominent scientists - physicists connect the past and future of our world with the formation and changes of black holes. “A black hole is a region of space-time whose gravitational attraction is so strong that even objects moving at the speed of light cannot leave it.” “A super massive black hole is a black hole with a mass of 105 - 1011 solar masses. Super massive black holes have been found at the center of many galaxies, including the Milky Way. Our galaxy revolves around a super massive black hole. This position of stellar bodies should be preserved for hundreds of millions of years.”

奥法妥木单抗治疗免疫检查点抑制剂相关副肿瘤性小脑性共济失调综合征1例

报告应用奥法妥木单抗(Ofatumumab,OFA)治疗免疫检查点抑制剂(immune checkpoint inhibitors,ICI)引起的副肿瘤性小脑性共济失调综合征1例。患者,男,57岁,既往小细胞肺癌病史,应用“卡瑞丽珠单抗”免疫治疗,主因“行走不稳1年余,头部不自主晃动1月余”入院。入院后完善头颅核磁、胸部CT、脑电图、腰椎穿刺等相关检查,副肿瘤综合征抗体谱抗GAD65抗体IgG(+),确诊免疫检查点抑制剂相关神经系统副肿瘤综合征(paraneoplastic neurological syndromes,PNS),给予OFA治疗(20mg/次)后症状明显改善。本文通过分析该病例的临床特点及诊疗思路,以提高临床医师对该疾病的认识,为类似病例的临床诊治提供参考。

儿童急性小脑性共济失调1例报告

回顾性分析1例新型冠状病毒(SARS-CoV-2)感染后急性小脑性共济失调患儿的临床资料和诊治过程,并进行相关文献复习。患儿,女,4岁11个月,因“咳嗽2周,发热3天”入院。入院第2天出现吟诗样语言,独坐不稳,走路不稳。予静脉人免疫球蛋白注射液总量2 g/kg(分4天)及静脉甲基强的松龙2 mg·kg^(-1)·d^(-1)治疗,病情明显好转后予醋酸泼尼松片口服(1 mg·kg^(-1)·d^(-1))并出院。出院11天电话随访患儿已基本恢复正常,遂停醋酸泼尼松治疗。文献报道3例患儿,均为男性,年龄分别为5岁、13岁、15岁;均为SARS-CoV-2感染后1~2周发病;临床表现均有共济失调步态;2例予静脉甲基强的松龙治疗,1例未予特殊治疗,3例均在2月内恢复正常。SARS-CoV-2感染所致急性小脑性共济失调一般为感染后1~2周出现,临床多表现为共济失调步态,多为感染后免疫反应所致,预后良好。

Changes in a cerebellar peduncle lesion in a patient with Dandy-Walker malformation A diffusion tensor imaging study

We report a patient with severe ataxia due to Dandy-Walker malformation, who showed functional recovery over 10 months corresponding to a change in a cerebellar peduncle lesion. A 20-month-old female patient who was diagnosed with Dandy-Walker syndrome and six age- and sex-matched healthy control subjects were enrolled. The superior cerebellar peduncle, the middle cerebellar peduncle, and the inferior cerebellar peduncle were evaluated using fractional anisotropy and the apparent diffusion coefficient. The patients＇ functional ambulation category was 0 at the initial visit, but improved to 2 at the follow-up evaluation, and Berg＇s balance scale score also improved from 0 to 7. Initial diffusion tensor tractography revealed that the inferior cerebellar peduncle was not detected, that the fractional anisotropy of the superior cerebellar peduncle and middle cerebellar peduncle decreased by two standard deviations below, and that the apparent diffusion coefficient increased by two standard deviations over normal control values. However, on follow-up diffusion tensor tractography, both inferior cerebellar peduncles could be detected, and the fractional anisotropy of superior cerebellar peduncle increased to within two standard deviations of normal controls. The functional improvement in this patient appeared to correspond to changes in these cerebellar peduncles. We believe that evaluating cerebellar peduncles using diffusion tensor imaging is useful in cases when a cerebellar peduncle lesion is suspected.

Ataxia Telangiectasia Syndrome Revealed by Severe Pneumonia

Ataxia Telangiectasia (AT) is a rare autosomal recessive multisystem disease. The diagnosis is often made on a clinical triad that combines neurological signs dominated by a progressive cerebellar ataxia, oculocutaneous signs (telangiectasia, coffee stain milk), immunodeficiency (humoral and cellular) with sinopulmonary infections and elevated alphaphetoprotein. The diagnosis of AT is usually early, however, some forms may be revealed late. We reported a case of a 19-year-old patient, admitted for severe pneumonia with Klebsiella Pneumonia. In its history, it was found a notion of recurrent respiratory infections and bronchiectasis. In its clinical examination, it had been discovered cerebellar ataxia and occulocutaneous telangiectasia. The determination of plasmatic alphafoetoprotein was elevated, and the search of immunodeficiency showed a mixed deficit (humoral and cellular) suggesting the diagnosis of AT.

Clinico-Radiological Correlation in Children with Ataxia Telangiectasia in Qatar

Introduction: Ataxia telangiectasia (AT) is a rare disease characterized by immunodeficiency and neurological manifestations. Ataxia, resulting from cerebella atrophy, runs a progressive incapacitating course. Clinical monitoring of the disease course is mandatory for early treatment. Aim: To study clinical severity of AT and correlate it with the degree of cerebellar atrophy. Patients and Methods: We retrospectively studied all children (less than 14 years) with AT seen at Hamad General Hospital Clinics between 1998-2013. We collected basic demographic data, parental consan-guinity, family history, AT clinical severity scores, and reviewed CBC with differential counts;alpha-fetoprotein, serum immunoglobulins and lymphocyte subsets. Cranial MRI scans of each subject were reviewed by a neuroradiologist. Cerebellar atrophy was visually and semi-quantitatively scored. Results: We analyzed data on 18 AT children (10 males and 8 females), mean age of 76.9 months. 77.8% had a positive family history of AT and 41.7% parental consanguinity. Lymphopenia was observed in 77.8% and high serum alpha-fetoprotein in 87.5% of children. Clinical severity of ataxia was 17.1 ± 8.4 (mean ± SD);86.7% of patients were moderate-severe. MRI cerebellar atrophy score was 1.9 ± 1.3 (mean ± SD), and moderate in 51% of patients. AT clinical severity score correlated (coefficient r = 0.566) but not statistically significant p = 0.088) with MRI cerebellar atrophy scores. Conclusions: Moderate to severe ataxia and marked cerebellar atrophy are quite common in AT children. There is a correlation between AT clinical severity and cerebellar atrophy. Larger prospective studies might further determine the significance of our observations and help practicing practitioners monitor the progression of the disease.

抗体相关自身免疫性小脑性共济失调15例分析

目的总结抗体相关自身免疫性小脑性共济失调(ACA)15例的特点及潜在意义。方法收集2015年1月至2021年12月在首都医科大学宣武医院神经内科患者住院治疗、自身免疫抗体阳性且以小脑性共济失调为主要临床表现的患者,整理统计患者的临床资料。结果15例患者均以头晕、走路不稳伴或不伴构音障碍的神经系统症状为首发和主要表现,4例患者有眼震,有8例患者在之后的筛查中发现肿瘤。15例患者,男性3例,女性12例,年龄34~69岁,平均年龄(55.5±3.79)岁。抗Yo抗体阳性3例,抗Hu抗体阳性2例,抗Tr抗体阳性2例,抗Ri抗体阳性、抗Amphiphysin抗体阳性、抗GAD抗体阳性、抗SOX1抗体阳性、抗PNMA2抗体阳性各1例,有3例为多重抗神经元抗体阳性。15例抗体阳性中有9例脑脊液相应抗体阳性,15例血清抗神经元抗体全部阳性。15例脑脊液常规、生化均未见明显异常,7例脑脊液特异性寡克隆区带阳性(46.67%)。7例寡克隆区带阳性中有5例脑脊液抗体阳性(阳性率71.42%)。8例寡克隆区带阴性中只有4例脑脊液抗体阳性(阳性率50%)。5例头颅MRI有小脑萎缩,均为双侧萎缩(阳性率33.33%)。糖皮质激素或静脉注射免疫球蛋白治疗后MRS评分显示神经系统症状均有改善。结论自身ACA调相关抗体以细胞内抗体为主。自身ACA以头晕、走路不稳、构音障碍、中枢性眼震等前庭小脑系统症状为首发和主要表现,眼震电图等前庭功能检查对前庭小脑系统功能的评估有重要意义。血清中检测抗神经抗体被认为足以诊断自身免疫性小脑性共济失调。脑脊液化验呈非特异性炎性表现,脑脊液寡克隆区带阳性与脑脊液神经元抗体阳性率的关系有待进一步扩大样本量研究确定。治疗应尽早开始,糖皮质激素或静脉注射免疫球蛋白治疗后MRS评分显示神经系统症状均有改善。

中脑梗死导致Wernekink连合综合征1例报告

脑梗死是最常见的缺血性脑卒中类型,临床中孤立性的中脑梗死相对少见,而Wernekink连合综合征是一种特殊类型的中脑梗死,主要表现为双侧小脑性共济失调及眼肌麻痹,该病临床罕见,现将我科收治的1例类似Miller-Fisher综合征表现的中脑梗死所致Wernekink连合综合征报道如下。1临床资料患者,男,48岁。因“视物重影4 d,肢体活动不灵活、言语不清1 d”于2022年6月6日入院。患者于入院4 d前早上7点起床后感到视物重影,双眼视物时有水平方向重影,单眼视物清晰。患者未予重视,上述症状持续不缓解,1 d前开始出现言语不清、语调低沉,肢体活动不灵活,表现为肢体动作不协调,如夹菜、刷牙等动作不准确,同时伴有步态不稳,漂浮感。无头晕、头痛,无肢体麻木、乏力等。就诊于广州医科大学附属第六医院急诊科,急诊头部CT未见明显异常,以“复视查因”收入神经内科病房。

腓骨肌萎缩症合并小脑性共济失调的临床及遗传学特点

腓骨肌萎缩症(Charcot-Marie-Tooth disease,CMT)是一组以周围神经病变为主的遗传性运动感觉神经病。主要临床症状包括进行性对称性肢体远端无力、萎缩、感觉障碍和腱反射减退或消失。根据神经电生理表现和病理特点,CMT可分为以脱髓鞘为主的CMT1型和轴索病变为主的CMT2型。除了周围神经系统病变外,CMT部分表型可同时累及中枢神经系统或其他脏器;其中小脑系统受累的CMT患者同时合并小脑性共济失调,可见于神经丝蛋白轻链(neurofilament light chain,NEFL)基因突变所致的CMT1F型和CMT2E型,MORC家族CW型锌指结构蛋白2 (MORC family CW-type zinc finger 2,MORC2)基因突变所致的CMT2Z型,溶质载体家族25成员46 (solute carrier family 25 member 46,SLC25A46)基因突变所致的伴视神经萎缩的CMT6B型,以及多核苷酸激酶3′-磷酸酶(polynucleotide kinase 3′-phosphatase,PNKP)基因突变所致的CMT2B2型等。近年来,CMT重叠表型成为研究的热点,其中CMT合并小脑性共济失调具有高度临床异质性和遗传异质性,临床上易发生误诊。该文就合并小脑性共济失调的CMT表型的临床及遗传学特点进行综述,旨在为该类患者的早期诊断和治疗提供参考。

原发性自身免疫性小脑性共济失调的临床分析

目的分析原发性自身免疫性小脑性共济失调(PACA)的临床特征,为对该类疾病的诊断及治疗提供经验。方法收集2018年1月至2023年1月中南大学湘雅三医院收治的PACA患者,回顾性分析患者的临床表现、实验室检查、影像学资料等。结果共纳入6例患者,其中男3例,女3例;中位年龄54岁。6例患者急性或亚急性起病,以步态不稳为主要症状,无前驱感染史;脑脊液常规、生化、细胞学和颅脑磁共振成像(MRI)检查基本正常;脑脊液自身免疫性小脑性共济失调抗体和血副肿瘤综合征抗体均为阴性;4例结缔组织病相关指标异常。6例患者中,4例患者接受免疫球蛋白治疗,其中2例合并激素治疗,1例合并激素及环磷酰胺治疗。6例患者经治疗后,步态不稳均有不同程度缓解,接受免疫或激素治疗患者的症状缓解明显。结论PACA是一种免疫介导的,但未发现明确病因或特定神经元抗体的自身免疫性疾病;临床表现以共济失调为主;脑脊液及影像学检查大致正常;免疫治疗对多数患者是有效的。

RNF216基因突变相关Gordon Holmes综合征的临床特征、基因分析及文献回顾

目的总结1例Gordon Holmes综合征(GHS)患者的临床特点和RNF216基因检测结果,并通过文献复习,以期提高对本病的基因特点和临床表现的认识。方法收集1例GHS患者的临床资料,抽取患者及其父母外周静脉血2 mL,提取DNA进行全外显子组基因检测,并回顾分析既往报道所有RNF216基因突变患者的基因变异和临床表现。结果青年男性患者,6岁时发现身材矮小,诊断为生长激素缺乏,至15岁仍无第二性征发育,诊断为低促性腺激素性性腺功能减退症,22岁后逐渐出现步态异常,言语、运动和认知功能进行性减退。全外显子组基因检测结果显示RNF216基因c.1549C>T(p.R517*),纯合,无义突变。父母为近亲婚配,表型正常,基因型均为该突变杂合携带者。结合文献回顾和本例报道结果显示,目前全球共发现RNF216基因突变患者21例,包含15种致病变异类型,其中7种截短突变,5种错义突变,以及同义突变、剪接突变和缺失突变各1种。该基因突变可见于GHS、亨廷顿样疾病、4H综合征多种症状重叠的神经系统退行性疾病,主要临床表现为青春期或成年早期低促性腺性性腺功能减退症和早发进行性神经功能障碍,神经系统症状中位起病年龄为28岁,以小脑共济失调、构音障碍和认知障碍,以及广泛脑白质病变和小脑萎缩的影像学表现为特征。结论RNF216基因突变导致GHS发病,基因检测有助于罕见病明确诊断和治疗指导。

透穴刺法治疗中风后小脑性共济失调临床观察

目的:观察透穴刺法治疗中风后小脑性共济失调的临床疗效并对其安全性作出评价。方法:采用随机、平行对照、单盲、多中心的研究方法,对4家医院的224例患者按1∶1的比例分为治疗组和对照组各112例。治疗组采用透穴刺法,对照组采用普通刺法,对治疗前后的症状、体征进行观察,同时观察治疗前后对经颅多普勒(TCD)的影响。结果:治疗组总有效率为93.3%,明显优于对照组的77.4%,经统计学处理(P<0.01),差异具有非常显著性意义。透穴刺法能够明显改善患者基底动脉、椎动脉及小脑后下动脉TCD(Vs、Vm、Vd、PI、RI),其作用优于对照组。结论:透穴刺法治疗中风后小脑性共济失调疗效显著,安全性好,值得临床推广应用。

透穴刺法治疗中风后小脑共济失调的疗效观察

目的 :观察透穴刺法治疗中风后小脑性共济失调的临床疗效。方法 :采用透穴刺法治疗中风后小脑性共济失调 5 0例 ,并随机设头针治疗对照组 4 0例 ,进行临床对照观察。结果 :治疗组有效率为 92 0 % ,对照组为 70 0 % ,透穴组疗效明显高于对照组 (P <0 0 1)。结论

Frenkel训练法改善小脑性共济失调患者的疗效观察

目的:观察Frenkel训练法对小脑性共济失调患者的康复治疗效果。方法:40例小脑性卒中患者随机分为治疗组(Frenkel训练法康复训练+常规治疗)和对照组(常规治疗),训练前后对患者协调能力采用Fugl-Meyer平衡功能评定、小脑性共济失调临床评定,日常生活能力(ADL)运用Barthel指数评价。结果:Fugl-Meyer平衡功能评分、小脑性共济失调临床评定评分和Barthel指数评分,治疗组治疗前和治疗后分别为3.26±5.12,11.57±6.11,45.26±10.32和10.54±4.26,6.73±4.23,80.31±11.46,对照组治疗前和治疗后则分别为3.78±4.56,11.65±5.62,43.15±10.28和7.47±5.12,9.15±3.26,62.89±11.23,两组相比患者的四肢和躯干协调运动能力都有提高,ADL水平也有提高,但治疗组效果更好(P<0.05)。结论:Frenkel训练法对改善患者的小脑性共济失调有效,并能提高ADL水平。

中枢神经系统表面含铁血黄素沉积症临床研究进展

中枢神经系统表面含铁血黄素沉积症是一种由蛛网膜下腔慢性出血造成含铁血黄素在脑和脊髓表面沉积而引起的中枢神经系统退行性变。临床主要表现为感音神经性耳聋、小脑性共济失调和锥体束损伤,腰穿可见脑脊液黄变,MR可见脑和脊髓表面沉积的含铁血黄素低信号。常见的造成出血的原因有血管畸形、动脉瘤、肿瘤、颅脑椎管内手术、硬脊膜缺损、外伤等。最根本的治疗方法是通过影像学明确出血灶并行外科手术切除,人工耳蜗植入和口服驱铁剂是目前对未发现明确病灶或病灶不能切除患者的主要治疗方法 。

头针电刺激合康复训练治疗小脑卒中共济失调临床研究

目的:观察头针电刺激联合康复训练治疗小脑卒中共济失调的疗效。方法:将140例小脑卒中共济失调患者按随机数字表法分为观察组与对照组各70例,对照组给予基本康复训练,观察组在对照组基础上加用头针电刺激,每天1次,10次1个疗程,共治疗3个疗程。治疗前后采用世界神经病联合会国际合作共济失调量表(ICARS)、Berg平衡量表(BBS)、Barthel指数(BI)及并发症进行评定。结果:2组治疗后ICARS、BBS与Barthel评分均明显优于治疗前,且观察组改善程度优于对照组;观察组有效率及减少并发症发生率方面均优于对照组。结论:头针电刺激联合康复训练治疗小脑卒中共济失调能明显改善共济失调症状,促进患者平衡能力与日常生活能力的提高,减少并发症的发生。

百优解治疗小脑性共济失调与血小板5-HT测定

目的 探讨百优解治疗小脑性共济失调的疗效和作用机制。方法 接受百优解治疗的患者 2 0例 ,治疗前后进行病情评分和血小板 5 -羟色胺 ( 5 - HT)测定 ,与毒扁豆碱治疗组 ( 2 6例 )、对照组 ( 112例健康查体者 )进行疗效对比。结果 ( 1)百优解治疗组的疗效 ( 70 .0 %)优于毒扁豆碱治疗组 ( 3 8.5 %) ( P<0 .0 5 ) ;( 2 )患者组血小板5 - HT水平低于对照组 ,具有极显著意义 ( P<0 .0 0 1) ;( 3 )百优解治疗前后血小板 5 - HT浓度改变 ,有效的 10例有下降趋势 ,无效的 5例明显增高。结论 ( 1)百优解对小脑性共济失调具有肯定的疗效 ,与 5 - HT代谢缺陷得到纠正有关 ;( 2 )血小板 5 - HT测定可能成为小脑性共济失调诊断和疗效评估的客观化验指标。