中华儿科杂志
中華兒科雜誌
중화인과잡지
Chinese Journal of Pediatrics
2012年
5期
371-375
,共5页
臧莉莉%吴晔%王静敏%顾强%姜玉武%高志杰%杨艳玲%肖江喜%吴希如
臧莉莉%吳曄%王靜敏%顧彊%薑玉武%高誌傑%楊豔玲%肖江喜%吳希如
장리리%오엽%왕정민%고강%강옥무%고지걸%양염령%초강희%오희여
Alexander病%遗传变性障碍,神经系统%脑白质病%中国%突变%GFAP基因
Alexander病%遺傳變性障礙,神經繫統%腦白質病%中國%突變%GFAP基因
Alexander병%유전변성장애,신경계통%뇌백질병%중국%돌변%GFAP기인
Alexander disease%Heredodegenerative disorders, nervous system%Leukoencephalopathies%China%Mutation%GFAP
目的 了解12例中国亚历山大病(Alexander disease,AD)患儿的临床表型及遗传学特点,为在国内开展该病的分子诊断及遗传咨询打下基础.方法 根据2001年van der Knaap等提出的AD头颅MRI诊断标准进行临床诊断,对临床诊断的AD患儿及其父母进行GFAP基因突变检测,并对上述患儿进行0.50~3.67年临床随访.结果 于2007年4月至2010年6月共收集12例AD患儿.初次于我院就诊的平均年龄为4.87岁(0.75 ~12.00岁).初次就诊时主诉:运动发育落后(3例),惊厥发作(7例)或跌倒后出现下肢运动障碍(2例);体征:头围44~ 58 cm,较相应年龄平均头围高6.45%( 1.80%~13.95%);采用脑瘫粗大运动功能分级系统(gross motor function classification system,GMFCS)中文版对运动进行分级:GMFCS I级8例,GMFCSⅡ级3例,GMFCSV级1例;8例患儿自幼认知功能发育迟滞.至2010年12月进行随访时,距初次就诊间隔0.50~3.67年,患儿平均年龄8.75岁(4.10 ~13.00岁),患儿运动及认知功能基本保持稳定.其中5例病程中伴发作性加重现象(41.67%).11例病程中有惊厥发作.12例均检测到GFAP杂合错义突变,均为新发突变.共发现10种GFAP突变,其中3种为未报道的新突变.R79与R239突变为热点突变.8例的突变位于第1外显子.结论 12例中国患儿临床表型特点为:疾病进展速度较国外报道相对缓慢,病程中发作性加重较为常见,惊厥发生率高.基因型特点与国外报道一致,本研究中发现的3种GFAP新突变丰富了已知突变谱.
目的 瞭解12例中國亞歷山大病(Alexander disease,AD)患兒的臨床錶型及遺傳學特點,為在國內開展該病的分子診斷及遺傳咨詢打下基礎.方法 根據2001年van der Knaap等提齣的AD頭顱MRI診斷標準進行臨床診斷,對臨床診斷的AD患兒及其父母進行GFAP基因突變檢測,併對上述患兒進行0.50~3.67年臨床隨訪.結果 于2007年4月至2010年6月共收集12例AD患兒.初次于我院就診的平均年齡為4.87歲(0.75 ~12.00歲).初次就診時主訴:運動髮育落後(3例),驚厥髮作(7例)或跌倒後齣現下肢運動障礙(2例);體徵:頭圍44~ 58 cm,較相應年齡平均頭圍高6.45%( 1.80%~13.95%);採用腦癱粗大運動功能分級繫統(gross motor function classification system,GMFCS)中文版對運動進行分級:GMFCS I級8例,GMFCSⅡ級3例,GMFCSV級1例;8例患兒自幼認知功能髮育遲滯.至2010年12月進行隨訪時,距初次就診間隔0.50~3.67年,患兒平均年齡8.75歲(4.10 ~13.00歲),患兒運動及認知功能基本保持穩定.其中5例病程中伴髮作性加重現象(41.67%).11例病程中有驚厥髮作.12例均檢測到GFAP雜閤錯義突變,均為新髮突變.共髮現10種GFAP突變,其中3種為未報道的新突變.R79與R239突變為熱點突變.8例的突變位于第1外顯子.結論 12例中國患兒臨床錶型特點為:疾病進展速度較國外報道相對緩慢,病程中髮作性加重較為常見,驚厥髮生率高.基因型特點與國外報道一緻,本研究中髮現的3種GFAP新突變豐富瞭已知突變譜.
목적 료해12례중국아력산대병(Alexander disease,AD)환인적림상표형급유전학특점,위재국내개전해병적분자진단급유전자순타하기출.방법 근거2001년van der Knaap등제출적AD두로MRI진단표준진행림상진단,대림상진단적AD환인급기부모진행GFAP기인돌변검측,병대상술환인진행0.50~3.67년림상수방.결과 우2007년4월지2010년6월공수집12례AD환인.초차우아원취진적평균년령위4.87세(0.75 ~12.00세).초차취진시주소:운동발육락후(3례),량궐발작(7례)혹질도후출현하지운동장애(2례);체정:두위44~ 58 cm,교상응년령평균두위고6.45%( 1.80%~13.95%);채용뇌탄조대운동공능분급계통(gross motor function classification system,GMFCS)중문판대운동진행분급:GMFCS I급8례,GMFCSⅡ급3례,GMFCSV급1례;8례환인자유인지공능발육지체.지2010년12월진행수방시,거초차취진간격0.50~3.67년,환인평균년령8.75세(4.10 ~13.00세),환인운동급인지공능기본보지은정.기중5례병정중반발작성가중현상(41.67%).11례병정중유량궐발작.12례균검측도GFAP잡합착의돌변,균위신발돌변.공발현10충GFAP돌변,기중3충위미보도적신돌변.R79여R239돌변위열점돌변.8례적돌변위우제1외현자.결론 12례중국환인림상표형특점위:질병진전속도교국외보도상대완만,병정중발작성가중교위상견,량궐발생솔고.기인형특점여국외보도일치,본연구중발현적3충GFAP신돌변봉부료이지돌변보.
Objective To delineate the phenotype and genotype characteristics in 12 Chinese children with Alexander disease ( AD),which is helpful for the molecular diagnosis and genetic counseling in China.Methods Clinical diagnosis of AD was based on MRI criteria proposed by van der Knaarp in 2001.Included AD patients were followed up for 0.50-3.67 years.Mutations in GFAP were detected by DNA sequencing.Results The 12 cases of AD were clinically diagnosed.Age of first visit was 4.87 years (0.75-12.00 years),with 3 type s of chief complaints:developmental delay in 3,recurrent seizures in 7,unable to walk after falling in 2.Average head circumference was 52.34 cm (44-58 cm),which larger than age-matched average by 6.45% ( 1.80% -13.95% ).On the first visit,scaling according to Gross motor functional classification system ( GMFCS ) was performed,with GMFCS Ⅰ in 8,Ⅱ in 3,V in 1.Mild to severe cognitive dysfunction were found in 8,and seizures in 11 cases.The 12 patients were followed up for 0.50-3.67 years,their motor and cognitive function remained stable. Episodic aggravations provoked by fever or falling were observed in 5 cases (41.67%). Heterozygous missense mutations of GFAP were detected in 12 patients.All mutations were de novo; 3 out of 10 mutations identified were novel.R79 and P239 were hot mutations,which was consistent with previous reports.Mutations were located in exon 1 in 8 cases.Conclusions The phenotype in these patients is characterized by slower progression compared with reports from other population and high incidence of seizures.And episodic aggravations provoked by fever or falling were more common.The genotype characteristics are consistent with previous reports.The results of this research expanded the number of patients with Alexander disease found to have GFAP coding mutations in China.
