Pathological consequences of sequence duplications in the human genome

被引:83
作者
Mazzarella, R
Schlessinger, D
机构
[1] NIA, Gerontol Res Ctr, Genet Lab, Baltimore, MD 21224 USA
[2] Washington Univ, Sch Med, Ctr Genet Med, St Louis, MO 63110 USA
[3] Washington Univ, Sch Med, Inst Biomed Comp, St Louis, MO 63110 USA
来源
GENOME RESEARCH | 1998年 / 8卷 / 10期
关键词
D O I
10.1101/gr.8.10.1007
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
As large-scale sequencing accumulates momentum, an increasing number of instances are being revealed in which genes or other relatively rare sequences are duplicated, either in tandem or at nearby locations. Such duplications are a source of considerable polymorphism in populations, and also increase the evolutionary possibilities for the coregulation of juxtaposed sequences. As a further consequence, they promote inversions and deletions that are responsible for significant inherited pathology. Here we review known examples of genomic duplications present on the human X chromosome and autosomes.
引用
收藏
页码:1007 / 1021
页数:15
相关论文
共 121 条
[1]   DNA POLYMORPHISM AND MOLECULAR PATHOLOGY OF THE HUMAN GLOBIN GENE CLUSTERS [J].
ANTONARAKIS, SE ;
KAZAZIAN, HH ;
ORKIN, SH .
HUMAN GENETICS, 1985, 69 (01) :1-14
[2]   Understanding enzyme superfamilies - Chemistry as the fundamental determinant in the evolution of new catalytic activities [J].
Babbitt, PC ;
Gerlt, JA .
JOURNAL OF BIOLOGICAL CHEMISTRY, 1997, 272 (49) :30591-30594
[3]   MOLECULAR HETEROGENEITY OF STEROID SULFATASE DEFICIENCY - A MULTICENTER STUDY ON 57 UNRELATED PATIENTS, AT DNA AND PROTEIN-LEVELS [J].
BALLABIO, A ;
CARROZZO, R ;
PARENTI, G ;
GIL, A ;
ZOLLO, M ;
PERSICO, MG ;
GILLARD, E ;
AFFARA, N ;
YATES, J ;
FERGUSONSMITH, MA ;
FRANTS, RR ;
ERIKSSON, AW ;
ANDRIA, G .
GENOMICS, 1989, 4 (01) :36-40
[4]   A DOSAGE SENSITIVE LOCUS AT CHROMOSOME XP21 IS INVOLVED IN MALE TO FEMALE SEX REVERSAL [J].
BARDONI, B ;
ZANARIA, E ;
GUIOLI, S ;
FLORIDIA, G ;
WORLEY, KC ;
TONINI, G ;
FERRANTE, E ;
CHIUMELLO, G ;
MCCABE, ERB ;
FRACCARO, M ;
ZUFFARDI, O ;
CAMERINO, G .
NATURE GENETICS, 1994, 7 (04) :497-501
[5]   IDENTIFICATION OF A NOVEL X-LINKED GENE RESPONSIBLE FOR EMERY-DREIFUSS MUSCULAR-DYSTROPHY [J].
BIONE, S ;
MAESTRINI, E ;
RIVELLA, S ;
MANCINI, M ;
REGIS, S ;
ROMEO, G ;
TONIOLO, D .
NATURE GENETICS, 1994, 8 (04) :323-327
[6]  
BOGDANOVA N, 1995, HUM GENET, V95, P645
[7]  
Bond D, 1983, OXFORD MONOGRAPHS ME, P198
[8]  
BONDESON ML, 1995, EUR J HUM GENET, V3, P219
[9]   INVERSION OF THE IDS GENE RESULTING FROM RECOMBINATION WITH IDS-RELATED SEQUENCES IS A COMMON-CAUSE OF THE HUNTER SYNDROME [J].
BONDESON, ML ;
DAHL, N ;
MALMGREN, H ;
KLEIJER, WJ ;
TONNESEN, T ;
CARLBERG, BM ;
PETTERSSON, U .
HUMAN MOLECULAR GENETICS, 1995, 4 (04) :615-621
[10]   DELETION OF THE TSC2 AND PKD1 GENES ASSOCIATED WITH SEVERE INFANTILE POLYCYSTIC KIDNEY-DISEASE - A CONTIGUOUS GENE SYNDROME [J].
BROOKCARTER, PT ;
PERAL, B ;
WARD, CJ ;
THOMPSON, P ;
HUGHES, J ;
MAHESHWAR, MM ;
NELLIST, M ;
GAMBLE, V ;
HARRIS, PC ;
SAMPSON, JR .
NATURE GENETICS, 1994, 8 (04) :328-332
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