Molecular genetic analysis of autosomal dominant late-onset cataract in a Chinese Family

Guohua Yang , Shan Zhong , Xianrong Zhang , Biwen Peng , Jun Li , Tie Ke , Hua Xu

Current Medical Science ›› 2010, Vol. 30 ›› Issue (6) : 792 -797.

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Current Medical Science ›› 2010, Vol. 30 ›› Issue (6) : 792 -797. DOI: 10.1007/s11596-010-0660-9
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Molecular genetic analysis of autosomal dominant late-onset cataract in a Chinese Family

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Abstract

Congenital cataract is a highly heterogeneous disorder at both the genetic and the clinical-phenotypic levels. A unique cataract was observed in a 4-generation Chinese family, which was characterized by autosomal dominant inheritance and late-onset. Mutations in the 13 known genes (CRYAA, CRYAB, CRYBB1, CRYBB2, CRYGC, CRYBA1/A3, CRYGD, Connexin50, Connexin46, intrinsic membrane protein LIM2, cytoskeletal protein BFSP2, the major intrinsic protein-MIP and the heat shock factor HSF4) have previously been demonstrated to be the frequent reason for isolated congenital cataracts, but the exact molecular basis and underlying mechanisms of congenital cataract still remain unclear. This study was designed to find whether these 13 genes developed any mutation in the family members and to identify the disease-causing gene. Polymerase chain reaction (PCR) and direct DNA sequence analysis were carried out to detect the 13 genes. The results showed that no mutation causing amino acid alternations was found in these potential candidate genes among all patients in the family, and only several single-nucleotide polymorphisms (SNPs) were identified. A transitional mutation in the fourth intron of CRYBB2 and some silent mutations in the first exon of BFSP2 and CRYGD were found in the cataract family, but further study showed that these mutations could also be found in normal controls. It was concluded that some unidentified genes may underlie the occurrence of late-onset cataract in this family. A genome-wide screening will be carried out in the next study.

Keywords

cataract / late-onset / gene / sequencing / mutation

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Guohua Yang, Shan Zhong, Xianrong Zhang, Biwen Peng, Jun Li, Tie Ke, Hua Xu. Molecular genetic analysis of autosomal dominant late-onset cataract in a Chinese Family. Current Medical Science, 2010, 30(6): 792-797 DOI:10.1007/s11596-010-0660-9

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References

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[1]

LimA.S.. Vision for the world. Eur J Ophthalmol, 1996, 6(1): 95
[2]

McCartyA., TaylorH.R.. The genetics of cataract. Invest Ophthalmol Vis Sci, 2001, 42(8): 1677-1678
[3]

HejtmancikJ.F.. The genetics of cataract: our vision becomes clearer (editorial). Am J Hum Genet, 1998, 62(3): 520-525

[4]

DelcourtC., CarriereI., DelageM., et al.. Associations of cataract with antioxidant enzymes and other risk factors: the French Age-Related Eye Diseases (POLA) Prospective Study. Ophthalmology, 2003, 110(12): 2318-2326

[5]

TsaiS.Y., HsuW.M., ChengC.Y., et al.. Epidemiologic study of age-related cataracts among an elderly Chinese population in Shih-Pai, Taiwan. Ophthalmology, 2003, 110(6): 1089-1095

[6]

HammondC.J., DuncanD.D., SniederH., et al.. The heritability of age-related cortical cataract: the twin eye study. Invest Ophthalmol Vis Sci, 2001, 42(3): 601-605
[7]

HammondC.J., SniederH., SpectorT.D., et al.. Genetic and environmental factors in age related nuclear cataracts in monozygotic and dizygotic twins. N Engl J Med, 2000, 342(24): 1786-1790

[8]

PrasE., FrydmanM., Levy-NissenbaumE., et al.. A nonsense mutation (W9X) in CRYAA causes autosomal recessive cataract in an inbred Jewish Persian family. Invest Ophthalmol Vis Sci, 2000, 41(11): 3511-3515
[9]

BerryV., FrancisP., ReddyM.A., et al.. Alpha-B crystalline gene (CRYAB) mutation causes dominant congenital posterior polar cataract in humans. Am J Hum Genet, 2001, 69(5): 1141-1145

[10]

MackayD.S., BoskovskaO.B., KnopfH.L., et al.. A nonsense mutation in CRYBB1 associated with autosomal dominant cataract linked to human chromosome 22q. Am J Hum Genet, 2002, 71(5): 1216-1221

[11]

LittM., Carrero-ValenzuelaR., LaMorticellaD.M., et al.. Autosomal dominant cerulean cataract is associated with a chain termination mutation in the human beta-crystallin gene CRYBB2. Human Molecular Genetics, 1997, 6(5): 665-668

[12]

BatemanJ.B., GeyerD.D., FlodmanP., et al.. A new betaA1-crystallin splice junction mutation in autosomal dominant cataract. Invest Ophthalmol Vis Sci, 2000, 41(11): 3278-3285
[13]

HeonE., PristonM., SchorderetD.F., et al.. The gamma-crystallins and human cataracts: a puzzle made clearer. Am J Hum Genet, 1999, 65(5): 1261-1267

[14]

StephanD.A., GillandersE., VanderveenD., et al.. Progressive juvenile-onset punctuate cataracts caused by mutation of the γD-crystallin gene. Proc Natl Acad Sci USA, 1999, 96(3): 1008-1012

[15]

BerryV., MackayD., KhaliqS., et al.. Connexin50 mutation in a family with congenital “zonular nuclear” pulverulent cataract of Pakistani origin. Hum Genet, 1999, 105(1–2): 168-170

[16]

PolyakovA.V., ShaginaI.A., KhlebnikovaO.V., et al.. Mutation in the connexin 50 gene (GJA8) in a Russian family with zonular pulverulent cataract. Clin Genet, 2001, 60(6): 476-478

[17]

PalJ.D., LiuX., MackayD., et al.. Connexin46 mutations linked to congenital cataract show loss of gap junction channel function. Am J Physiol Cell Physiol, 2000, 279(3): C596-C602
[18]

PrasE., Levy-NissenbaumE., BakhanT., et al.. A missense mutation in the LIM2 gene is associated with autosomal recessive presenile cataract in an inbred Iraqi Jewish family. Am J Hum Genet, 2002, 70(5): 1363-1367

[19]

ConleyY.P., ErturkD., KeverlineA., et al.. A juvenile-onset, progressive cataract locus on chromosome 3q21–q22 is associated with a missense mutation in the beaded filament structural protein-2. Am J Hum Genet, 2000, 66(4): 1426-1431

[20]

BerryV., FrancisP., KaushalS., et al.. Missense mutations in MIP underlie autosomal dominant “polymorphic” and lamellar cataracts linked to 12q. Nat Genet, 2000, 25(1): 15-17

[21]

BuL., JinY., ShiY., et al.. Mutant DNA-binding domain of HSF4 is associated with autosomal dominant lamellar and Marner cataract. Nat Genet, 2002, 31(3): 276-278

[22]

AntonarakisS.E.. Recommendations for a nomenclature system for human gene mutations. The nomenclature working group. Hum Mutat, 1998, 11(1): 1-3
[23]

GrawJ., LosterJ., SoewartoD., et al.. Characterization of a mutation in the lens-specific MP70 encoding gene of the mouse leading to a dominant cataract. Exp Eye Res, 2001, 73(6): 867-876

[24]

HeonE., PatersonA.D., FraserM., et al.. A progressive autosomal recessive cataract locus maps to chromosome 9q13–q22. Am J Hum Genet, 2001, 68(3): 772-777

[25]

ZhangS., LiuM., DongJ.M., et al.. Identification of a genetic locus for autosomal dominant infantile cataract on chromosome 20p12.1–p11.23 in a Chinese family. Mol Vis, 2008, 14: 1893-1899
[26]

HejtmancikJ.F., SmaouiN.. Molecular genetics of cataract. Dev Ophthalmol, 2003, 37: 67-82

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