PARENTAL ORIGIN AND GERMLINE MOSAICISM OF DELETIONS AND DUPLICATIONS OF THE DYSTROPHIN GENE - A EUROPEAN STUDY

被引：80

作者：

VANESSEN, AJ

ABBS, S

BAIGET, M

BAKKER, E

BOILEAU, C

VANBROECKHOVEN, C

BUSHBY, K

CLARKE, A

CLAUSTRES, M

COVONE, AE

FERRARI, M

FERLINI, A

GALLUZZI, G

GRIMM, T

GRUBBEN, C

JEANPIERRE, M

KAARIAINEN, H

LIECHTIGALLATI, S

MELIS, MA

VANOMMEN, GJB

PONCIN, JE

SCHEFFER, H

SCHWARTZ, M

SPEER, A

STUHRMANN, M

VERELLENDUMOULIN, C

WILCOX, DE

TENKATE, LP

机构：

[1] GUYS HOSP,PRINCE PHILIP RES LABS,DIV MED & MOLEC GENET,PAEDIAT RES UNIT,LONDON SE1 9RT,ENGLAND

[2] HOSP SANTA CRUZ & SAN PABLO,UNITAT GENET MOLEC,E-08025 BARCELONA,SPAIN

[3] SYLVIUS LABS,DEPT HUMAN GENET,2333 AL LEIDEN,NETHERLANDS

[4] HOP AMBROISE PARE,CENT BIOCHIM & GENET MOLEC LAB,F-92104 BOULOGNE,FRANCE

[5] UNIV NEWCASTLE UPON TYNE,DEPT HUMAN GENET,NEWCASTLE TYNE NE2 4AA,ENGLAND

[6] S RAFFAELE HOSP,ANAL CLIN LAB,MILAN,ITALY

[7] CNR,INST BIOL CELLULARE,UILDM ROME SECT,I-00137 ROME,ITALY

[8] UNIV ZIEKENHUIZEN LEUVEN,CENTRUM MENSELIJKE ERFELIJKHEID,B-3000 LOUVAIN,BELGIUM

[9] CHU LIEGE,GENET MED LAB,B-4000 LIEGE,BELGIUM

[10] ZENT INST MOLEK BIOL,MOLEK HUMANGENET ABT,O-1115 BERLIN,GERMANY

[11] UNIV GLASGOW,DUNCAN GUTHRIE INST MED GENET,DEPT MED GENET,GLASGOW G3 8SJ,SCOTLAND

[12] UNIV HELSINKI,DEPT MED GENET,SF-00290 HELSINKI 29,FINLAND

[13] INSELSPITAL BERN,MED GENET ABT,CH-3010 BERN,SWITZERLAND

[14] UNIV CAGLIARI,INST CLIN & BIOL ETA EVOLUT,I-09100 CAGLIARI,ITALY

[15] CHU LIEGE,CHIM MED LAB,B-4000 LIEGE,BELGIUM

[16] RIGSHOSP,DEPT CLIN GENET,DK-2100 COPENHAGEN,DENMARK

[17] FREE UNIV BERLIN,INST HUMANGENET,W-1000 BERLIN 19,GERMANY

[18] CATHOLIC UNIV LOUVAIN,CTR GENET MED,B-1200 BRUSSELS,BELGIUM

[19] UNIV INSTELLING ANTWERP,DEPT BIOCHEM,B-2610 WILRIJK,BELGIUM

[20] UNIV HOSP WALES,INST MED GENET,CARDIFF CF4 4XN,S GLAM,WALES

[21] CNRS,CTR RECH BIOCHIM MACROMOLEC,INST BIOL,INSERM,U249,F-34060 MONTPELLIER,FRANCE

[22] IST GIANNINA GASLINI,GENET MOLEC LAB,I-16148 GENOA,ITALY

[23] UNIV MODENA,CATTEDRA ISTOL & EMBRIOL GEN,I-41100 MODENA,ITALY

[24] UNIV WURZBURG,INST HUMANGENET,W-8700 WURZBURG,GERMANY

[25] FAC MED COCHIN,SERV BIOCHIM GENET,F-75674 PARIS 14,FRANCE

[26] FAC MED COCHIN,INSERM,U129,F-75674 PARIS 14,FRANCE

来源：

HUMAN GENETICS | 1992年 / 88卷 / 03期

关键词：

D O I：

10.1007/BF00197255

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Knowledge about the parental origin of new mutations and the occurrence of germline mosaicism is important for estimating recurrence risks in Duchenne (DMD) and Becker muscular dystrophy (BMD). However, there are problems in resolving these issues partly because not all mutations can as yet be directly detected, and additionally because genetic ratios are very sensitive to ascertainment bias. In the present study, therefore, analysis was restricted to currently detectable mutations (deletions and duplications) in particular types of families which tend to be rare. In order to obtain sufficient data we pooled results from 25 European centers. In mothers of affected patients who were the first in their family with a dystrophin gene deletion or duplication, the ratio between the paternal and the maternal origin of this new mutation was 32:49 (binomial test P = 0.075) for DMD. In five BMD families the ratio between paternal and maternal origin of new mutations was 3:2. Recurrence risk because of maternal germline mosaicism was studied in sisters or subsequent sibs of isolated cases with an apparently new detectable mutation. In 12 out of 59 (0.20; 95% CI 0.10-0.31) transmissions of the risk haplotype the DMD mutation was transmitted as well. No recurrences were found in nine BMD families.

引用

页码：249 / 257

页数：9

共 56 条

[1] PRENATAL-DIAGNOSIS OF DUCHENNE MUSCULAR-DYSTROPHY - A 3-YEAR EXPERIENCE IN A RAPIDLY EVOLVING FIELD [J].