Quantifying Kinematic Tremor in an NGLY1-Deficient Individual: A Case Study

NGLY1 Deficiency is an autosomal recessive congenital disorder that has been identified in less than 100 individuals. Most individuals with NGLY1 Deficiency display hyperkinetic movement disorders, including choreiform, athetoid, dystonic myoclonic, dyskinetic, and dysmetric movements. Developing a consistent and concise consensus on the classification and evaluation of tremors is essential to forward the research and treatment of tremors. It has also been reported that some individuals with NGLY1 Deficiency demonstrate tremor, but such tremor has never been formally investigated. The primary objective of this study is to determine if an individual with NGLY1 Deficiency demonstrates an identifiable tremor during a series of arm movements and, if so, describe the frequency and power characteristics of that tremor. Arm movement kinematics were obtained using a 16-camera Vicon system, and time series trajectory waveforms for three planes of a marker placed on the hand were developed. Custom MATLAB scripts were utilized to compute Fast Fourier Transformations of the data within the identified waveform segments. A mean frequency of 2.30 Hz (SD = 1.05) with a mean power of 5.02 |P1(f)| (SD = 4.63) suggests that our participant’s kinematic data did display a persistent tremor in both hands across all tasks and movement planes. Analyses of the reaching hand and the non-reaching hand suggest the participant displayed an action tremor in both postural and intention (kinetic) tremors. Future directions should include assessing additional individuals with NGLY1 Deficiency to determine if the tremor is a distinguishable disorder behavior. Additionally, evaluating other anatomical sites, such as the elbow, head, and lower limbs, would provide further insights into the characteristics of this tremor.

3-Dimensional Kinematic Comparison of Arm Movements between an Individual with NGLY1 Deficiency and a Neurotypical Individual

NGLY1 Deficiency is an ultra-rare autosomal recessively inherited disorder. Characteristic symptoms include among others, developmental delays, movement disorders, liver function abnormalities, seizures, and problems with tear formation. Movements are hyperkinetic and may include dysmetric, choreo-athetoid, myoclonic and dystonic movement elements. To date, there have been no quantitative reports describing arm movements of individuals with NGLY1 Deficiency. This report provides quantitative information about a series of arm movements performed by an individual with NGLY1 Deficiency and an aged-matched neurotypical participant. Three categories of arm movements were tested: 1) open ended reaches without specific end point targets;2) goal-directed reaches that included grasping an object;3) picking up small objects from a table placed in front of the participants. Arm movement kinematics were obtained with a camera-based motion analysis system and “initiation” and “maintenance” phases were identified for each movement. The combination of the two phases was labeled as a “complete” movement. Three-dimensional analysis techniques were used to quantify the movements and included hand trajectory pathlength, joint motion area, as well as hand trajectory and joint jerk cost. These techniques were required to fully characterize the movements because the NGLY1 individual was unable to perform movements only in the primary plane of progression instead producing motion across all three planes of movement. The individual with NGLY1 Deficiency was unable to pick up objects from a table or effectively complete movements requiring crossing the midline. The successfully completed movements were analyzed using the above techniques and the results of the two participants were compared statistically. Almost all comparisons revealed significant differences between the two participants, with a notable exception of the 3D initiation area as a percentage of the complete movement. The statistical tests of these measures revealed no significant differences between the two participants, possibly suggesting a common underlying motor control strategy. The 3D techniques used in this report effectively characterized arm movements of an individual with NGLY1 deficiency and can be used to provide information to evaluate the effectiveness of genetic, pharmacological, or physical rehabilitation therapies.

NGLY1基因突变致先天性糖基化障碍Ⅳ型一家系报告

目的分析NGLY1基因突变导致先天性糖基化障碍Ⅳ型的临床特征、诊断及治疗。方法回顾同一家系中2例先天性糖基化障碍Ⅳ型姐妹的临床资料及基因检测结果,并结合文献进行分析。结果先证者,女,8个月,临床表现为精神运动发育迟缓、少汗、泪少、眼睑闭合差、手小、脚小等;胎龄6个月时其母行唐氏综合征产前筛查提示高风险,羊水穿刺结果未见异常,超声提示胎儿宫内发育迟缓。先证者姐姐4岁,临床表现及生长发育史与先证者相似。患儿父母非近亲结婚,表型无异常。先证者染色体核型分析及染色体微缺失分析无异常。先证者以及父母全外显子基因测序均存在NGLY 1基因突变;先证者胞姐也存在相同的NGLY 1来源于父亲的移码突变(可导致氨基酸p.S 546 Ffs*12改变)和来源于母亲的剪切位点突变。NGLY1基因已被国外文献报道与先天性糖基化障碍Ⅳ型有关,目前在中国知网、万方、PubMed和Clinvar数据库中未检索到与此相同的NGLY 1基因1003+3位点点突变及1637位点移码突变,推测其可能为新的突变。结论先证者及其胞姐NGLY1基因突变分别源自父母,NGLY1基因突变可导致先天性糖基化障碍Ⅳ型,其临床表型与文献报道相吻合。

森林地区PM2.5中氨基酸的水平、来源及转化

在春季采集了南昌森林地区(28.75°N,115.71°E)大气PM2.5样品,测定了其结合氨基酸(CAAs)和游离氨基酸(FAAs)的浓度以及甘氨酸(Gly)的氮同位素.结果表明,大气气溶胶中总CAAs的浓度为272.8~4761.5pmol/m^3,总FAAs浓度为56.4~494.0pmol/m^3.通过分析PM2.5中氨基酸的百分比组成,得出CAAs中Pro、Gly、Glu、Leu和Ala为主要氨基酸,分别占总CAAs的(19.5±12.0)%,(19.4±10.6)%,(15.3±4.9)%,(12.8±5.4)%和(9.1±1.6)%.在FAAs中,Gly为最丰富的氨基酸,占总FAAs的(71.1±9.2)%,其他单个FAAs的百分比却很小(占比范围为0.1%~14.3%).FAAs中的中性氨基酸百分占比明显高于其在CAAs中的百分占比,这可能与远距离传输过程中氨基酸的光化学反应有关.通过氨基酸浓度与O3、NO2和温度的相关性分析,发现森林地区气溶胶中FAAs形成与大气光化学过程和热反应有关.气溶胶中δ^15NC-Gly值(-1.0‰~+17.5‰)和δ^15NF-Gly值(-5.5‰~+13.0‰)均接近于土壤源的δ^15NGly值,说明森林地区PM2.5中氨基酸可能主要来源于土壤源.

橙花醇-β-D-吡喃葡萄糖苷的热行为及热分解动力学

为研究一种天然等同结构的键合态香料前体橙花醇-β-D-吡喃葡萄糖苷的热稳定性及热降解机理,采用热重分析/同步差示热分析(DTA/SDTG)法分析糖苷在5,10,15℃/min的升温速率下,30~500℃范围内其热行为,利用Friedman法和Flynn-Wall-Ozawa法计算其热降解参数。结果显示:TGDTG曲线表明其热降解温度主要受升温速率(B)的影响,橙花醇糖苷质量开始损失的温度T_0=1.102 3B+199.4,质量损失最大速率时的温度T_p=2.102 3B+251.9,质量损失最终的温度T_f=2.602 3B+315.23,均随升温速率的提高而按照一定的线性规律增加;DSC曲线表明其降解过程中熔融与分解同时发生;据Friedman法和Flynn-Wall-Ozawa法得到的热降解表观活化能Ea相关性较好,分别为180.90,168.76kJ/mol。研究结果可为糖苷类香料前体的性质及其应用研究提供基础数据。