Mutations in the human Jagged1 gene are responsible for Alagille syndrome

被引：798

作者：

Oda, T

Elkahloun, AG

Pike, BL

Okajima, K

Krantz, ID

Genin, A

Piccoli, DA

Meltzer, PS

Spinner, NB

Collins, FS

Chandrasekharappa, SC

机构：

[1] NATL HUMAN GENOME RES INST,LAB GENE TRANSFER,NIH,BETHESDA,MD 20892

[2] NATL HUMAN GENOME RES INST,CANC GENET LAB,NIH,BETHESDA,MD 20892

[3] NAGOYA CITY UNIV,SCH MED,DEPT PEDIAT,NAGOYA,AICHI 467,JAPAN

[4] CHILDRENS HOSP,PHILADELPHIA,PA 19104

[5] RES GENET INC,HUNTSVILLE,AL 35801

来源：

NATURE GENETICS | 1997年 / 16卷 / 03期

关键词：

D O I：

10.1038/ng0797-235

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Alagille syndrome (AGS) is an autosomal-dominant disorder characterized by intrahepatic cholestasis and abnormalities of heart, eye and vertebrae, as well as a characteristic facial appearance. Identification of rare AGS patients with cytogenetic deletions has allowed mapping of the gene to 20p12. We have generated a cloned contig of the critical region and used fluorescent in situ hybridization on cells from patients with submicroscopic deletions to narrow the candidate region to only 250 kb. Within this region we identified JAG1, the human homologue of rat Jagged1, which encodes a ligand for the Notch receptor. Cell-cell Jagged/Notch interactions are known to be critical for determination of cell fates in early development, making this an attractive candidate gene for a developmental disorder in humans. Determining the complete exon-intron structure of JAG1 allowed detailed mutational analysis of DNA samples from non-deletion ACS patients, revealing three frame-shift mutations, two splice donor mutations and one mutation abolishing RNA expression from the altered allele. We conclude that AGS is caused by haploinsufficiency of JAG1.

引用

页码：235 / 242

页数：8

共 38 条

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