中华神经医学杂志
中華神經醫學雜誌
중화신경의학잡지
CHINESE JOURNAL OF NEUROMEDICINE
2015年
4期
484-489
,共6页
邴琪%胡静%赵哲%沈宏锐%李娜
邴琪%鬍靜%趙哲%瀋宏銳%李娜
병기%호정%조철%침굉예%리나
DMD变异携带者%女性%骨骼肌活检%MRI%基因测序%X染色体失活
DMD變異攜帶者%女性%骨骼肌活檢%MRI%基因測序%X染色體失活
DMD변이휴대자%녀성%골격기활검%MRI%기인측서%X염색체실활
Duchenne muscular dystrophy manifesting carrier%Female%Skeletal muscle biopsy%MR imaging%Gene sequencing%X chromosome inactivation
目的 探讨女性有症状DMD变异携带者(MCs)临床、病理、基因变异特点及发病机制.方法 选择河北医科大学第三医院神经肌病科自2010年至2014年收治的2例女性MCs,对其家系的临床、骨骼肌病理资料进行分析,同时检测DMD基因变异和X染色体失活情况.结果 (1)2例女性MCs均表现不同程度四肢近端肌无力、萎缩,家系中有类似DMD/BMD表现者.(2)2个家系先证者骨骼肌病理符合女性MCs病理表现,家系1先证者以及家系2先证者、Ⅱ-5、Ⅲ-7常规GRQ带染色体核型分析为正常女性核型.(3)基因测序结果显示,家系1先证者和Ⅱ-7均发现DMD基因外显子61杂合性缺失.家系2先证者、Ⅱ-5和Ⅲ-7均发现DMD基因外显子12-43杂合性缺失,家系2Ⅳ-4发现外显子12-43纯合性缺失.(4)X染色体失活分析结果显示,家系1先证者、家系2先证者和Ⅲ-7X染色体失活检测均不能区分父母的等位基因.结论 (1)女性MCs临床症状严重程度差异大,与骨骼肌活检病理表现相对应;(2)女性MCs下肢骨骼肌选择性受累与DMD相似,但不对称性更为显著;(3)2个家系均发现DMD基因外显子缺失,男性患者临床表型-基因变异符合阅读框学说,女性MCs不符合.
目的 探討女性有癥狀DMD變異攜帶者(MCs)臨床、病理、基因變異特點及髮病機製.方法 選擇河北醫科大學第三醫院神經肌病科自2010年至2014年收治的2例女性MCs,對其傢繫的臨床、骨骼肌病理資料進行分析,同時檢測DMD基因變異和X染色體失活情況.結果 (1)2例女性MCs均錶現不同程度四肢近耑肌無力、萎縮,傢繫中有類似DMD/BMD錶現者.(2)2箇傢繫先證者骨骼肌病理符閤女性MCs病理錶現,傢繫1先證者以及傢繫2先證者、Ⅱ-5、Ⅲ-7常規GRQ帶染色體覈型分析為正常女性覈型.(3)基因測序結果顯示,傢繫1先證者和Ⅱ-7均髮現DMD基因外顯子61雜閤性缺失.傢繫2先證者、Ⅱ-5和Ⅲ-7均髮現DMD基因外顯子12-43雜閤性缺失,傢繫2Ⅳ-4髮現外顯子12-43純閤性缺失.(4)X染色體失活分析結果顯示,傢繫1先證者、傢繫2先證者和Ⅲ-7X染色體失活檢測均不能區分父母的等位基因.結論 (1)女性MCs臨床癥狀嚴重程度差異大,與骨骼肌活檢病理錶現相對應;(2)女性MCs下肢骨骼肌選擇性受纍與DMD相似,但不對稱性更為顯著;(3)2箇傢繫均髮現DMD基因外顯子缺失,男性患者臨床錶型-基因變異符閤閱讀框學說,女性MCs不符閤.
목적 탐토녀성유증상DMD변이휴대자(MCs)림상、병리、기인변이특점급발병궤제.방법 선택하북의과대학제삼의원신경기병과자2010년지2014년수치적2례녀성MCs,대기가계적림상、골격기병리자료진행분석,동시검측DMD기인변이화X염색체실활정황.결과 (1)2례녀성MCs균표현불동정도사지근단기무력、위축,가계중유유사DMD/BMD표현자.(2)2개가계선증자골격기병리부합녀성MCs병리표현,가계1선증자이급가계2선증자、Ⅱ-5、Ⅲ-7상규GRQ대염색체핵형분석위정상녀성핵형.(3)기인측서결과현시,가계1선증자화Ⅱ-7균발현DMD기인외현자61잡합성결실.가계2선증자、Ⅱ-5화Ⅲ-7균발현DMD기인외현자12-43잡합성결실,가계2Ⅳ-4발현외현자12-43순합성결실.(4)X염색체실활분석결과현시,가계1선증자、가계2선증자화Ⅲ-7X염색체실활검측균불능구분부모적등위기인.결론 (1)녀성MCs림상증상엄중정도차이대,여골격기활검병리표현상대응;(2)녀성MCs하지골격기선택성수루여DMD상사,단불대칭성경위현저;(3)2개가계균발현DMD기인외현자결실,남성환자림상표형-기인변이부합열독광학설,녀성MCs불부합.
Objective To analyze the clinical and pathological genetic features of two Duchenne muscular dystrophy (DMD) manifesting carriers (MCs) and their families,and investigate the possible pathogenesis of female MCs.Methods The clinical and muscle pathological data of two female MCs,admitted to our hospital from 2010 to 2014,and their families,were collected,and DMD gene mutation and X chromosome inactivation were detected.Results (1) The two female MCs had proximal limb weakness;both two families had DMD/BMD-like patients.(2) The muscle biopsy pathological presentation was in accordance with female MCs pathological features,proband of two families and Ⅱ-5 and Ⅲ-7 of family 2 were normal female karyotype.(3) Proband and Ⅱ-7 of family 1 had loss of heterozygosity of DMD gene exon61;proband,Ⅱ-5 and Ⅲ-7 of family 2 had loss of heterozygosity of exon12-43,and Ⅳ-4 of family 2 had homozygous deletions of exon12-43.(4) X chromosome inactivation analysis of two probands and Ⅲ-7 of family 2 was uninformative.Conclusions (1) The clinical manifestations of female MCs are various;the clinical symptoms are corresponding with histochemical expression of skeletal muscle biopsy.(2) The selective muscle involvement of female MCs is similar with DMD,but rectus femoris is relatively preserved.(3) The two families have exon deletion of DMD gene;the relationship between clinical phenotype and gene mutation in male patients consists with the reading frame theory,but female don' t.
