中华儿科杂志
中華兒科雜誌
중화인과잡지
Chinese Journal of Pediatrics
2015年
8期
621-625
,共5页
杨小玲%张月华%许小菁%杨志仙%王爽%吴晔%吴希如
楊小玲%張月華%許小菁%楊誌仙%王爽%吳曄%吳希如
양소령%장월화%허소정%양지선%왕상%오엽%오희여
运动障碍%表型%突变%基因,PRRT2
運動障礙%錶型%突變%基因,PRRT2
운동장애%표형%돌변%기인,PRRT2
Movement disorder%Phenotype%Mutation%Gene,PRRT2
目的 探讨阵发性运动诱发的运动障碍(PKD)患儿的临床表型和富脯氨酸跨膜蛋白2(PRRT2)基因突变的特点.方法 收集2004年1月至2014年7月在北京大学第一医院儿科神经专业门诊就诊的PKD患儿及其家系成员的临床资料.共入选10例PKD患儿,均为男性,其中4例患儿为4个PKD家系中的先证者,其余6例为散发病例.对患儿的临床资料进行分析,采集患儿及其父母和家系受累成员外周血,采用PCR和Sanger测序的方法筛查PRRT2基因突变.结果 10例患儿的起病年龄为4~13岁,中位起病年龄为10岁.运动障碍表现为运动启动时出现异常姿势或不自主运动,其中表现为肌张力不全5例,舞蹈手足徐动症2例,兼有肌张力不全和舞蹈手足徐动症3例,持续时间为3 ~30 s,发作频率为每月1次至每天20次,发作时意识清楚.4个PKD家系均发现PRRT2基因突变,突变均为c.649_650insC(p.R217PfsX8);6例PKD散发病例中,2例发现有PRRT2基因突变,突变为c.649_650insC(p.R217PfsX8),且突变均遗传自无PKD症状的母亲.结论 PKD患儿的起病年龄可早至幼儿,家系受累者与散发病例临床表型无明显不同,可表现为肌张力不全、舞蹈手足徐动症或二者兼有.PKD家系或PKD散发病例均可由PRRT2基因突变导致,突变c.649_650insC是该基因的热点突变.
目的 探討陣髮性運動誘髮的運動障礙(PKD)患兒的臨床錶型和富脯氨痠跨膜蛋白2(PRRT2)基因突變的特點.方法 收集2004年1月至2014年7月在北京大學第一醫院兒科神經專業門診就診的PKD患兒及其傢繫成員的臨床資料.共入選10例PKD患兒,均為男性,其中4例患兒為4箇PKD傢繫中的先證者,其餘6例為散髮病例.對患兒的臨床資料進行分析,採集患兒及其父母和傢繫受纍成員外週血,採用PCR和Sanger測序的方法篩查PRRT2基因突變.結果 10例患兒的起病年齡為4~13歲,中位起病年齡為10歲.運動障礙錶現為運動啟動時齣現異常姿勢或不自主運動,其中錶現為肌張力不全5例,舞蹈手足徐動癥2例,兼有肌張力不全和舞蹈手足徐動癥3例,持續時間為3 ~30 s,髮作頻率為每月1次至每天20次,髮作時意識清楚.4箇PKD傢繫均髮現PRRT2基因突變,突變均為c.649_650insC(p.R217PfsX8);6例PKD散髮病例中,2例髮現有PRRT2基因突變,突變為c.649_650insC(p.R217PfsX8),且突變均遺傳自無PKD癥狀的母親.結論 PKD患兒的起病年齡可早至幼兒,傢繫受纍者與散髮病例臨床錶型無明顯不同,可錶現為肌張力不全、舞蹈手足徐動癥或二者兼有.PKD傢繫或PKD散髮病例均可由PRRT2基因突變導緻,突變c.649_650insC是該基因的熱點突變.
목적 탐토진발성운동유발적운동장애(PKD)환인적림상표형화부포안산과막단백2(PRRT2)기인돌변적특점.방법 수집2004년1월지2014년7월재북경대학제일의원인과신경전업문진취진적PKD환인급기가계성원적림상자료.공입선10례PKD환인,균위남성,기중4례환인위4개PKD가계중적선증자,기여6례위산발병례.대환인적림상자료진행분석,채집환인급기부모화가계수루성원외주혈,채용PCR화Sanger측서적방법사사PRRT2기인돌변.결과 10례환인적기병년령위4~13세,중위기병년령위10세.운동장애표현위운동계동시출현이상자세혹불자주운동,기중표현위기장력불전5례,무도수족서동증2례,겸유기장력불전화무도수족서동증3례,지속시간위3 ~30 s,발작빈솔위매월1차지매천20차,발작시의식청초.4개PKD가계균발현PRRT2기인돌변,돌변균위c.649_650insC(p.R217PfsX8);6례PKD산발병례중,2례발현유PRRT2기인돌변,돌변위c.649_650insC(p.R217PfsX8),차돌변균유전자무PKD증상적모친.결론 PKD환인적기병년령가조지유인,가계수루자여산발병례림상표형무명현불동,가표현위기장력불전、무도수족서동증혹이자겸유.PKD가계혹PKD산발병례균가유PRRT2기인돌변도치,돌변c.649_650insC시해기인적열점돌변.
Objective To investigate the clinical features and proline-rich transmembrane protein 2 (PRRT2) gene mutation in patients with paroxysmal kinesigenic dyskinesia (PKD).Method Clinical information was collected at Peking University First Hospital from January 2004 to July 2014.In total,10 patients with PKD were recruited,and all were males.Among them,four patients were the probands from four PKD families and the other six patients were sporadic cases.Clinical information was analyzed.Peripheral blood samples for DNA study were collected from PKD patients and their family members.Genomic DNA was extracted using standard procedures.Mutation analysis of PRRT2 was performed by Sanger sequencing after PCR.Result Of the 10 patients,the median age of dyskinesias onset was 10 years,ranging from 4 to 13 years.The description of their attacks were abnormal involuntary movements provoked by sudden movements,without loss of consciousness.Five patients exhibited dystonia,two patients exhibited choreoathetosis,and three patients had mixed (dystonia and choreoathetosis) dyskinesias.The duration of the attacks lasted for 3 to 30 seconds.The frequency ranged from once per month to twenty times per day.PRRT2 mutations,c.649_ 650insC (p.R217PfsX8),were found in all the four PKD families.Mutation c.649_650insC was also detected in two of the six sporadic PKD cases,inheriting from their asymptomatic mother.Conclusion The onset age of PKD could be in the early childhood.The clinical features of the familial cases and sporadic cases showed no difference.The attacks manifested as dystonia,choreathetosis,or mixed.PRRT2 mutations could be identified in familial or sporadic cases with PKD.Mutation c.649_650insC is the hotspot mutation of PRRT2 gene.
