Whole-Exome sequencing identifies FAM20A mutations as a cause of amelogenesis imperfecta and gingival hyperplasia syndrome.

OSullivan J; Bitu CC; Daly SB; Urquhart JE; Barron MJ; Bhaskar SS; Martelli Junior H; dos Santos Neto PE; Mansilla MA; Murray JC; Coletta RD; Black GC; Dixon MJ

首页> 外文期刊>The American Journal of Human Genetics >Whole-Exome sequencing identifies FAM20A mutations as a cause of amelogenesis imperfecta and gingival hyperplasia syndrome.

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Whole-Exome sequencing identifies FAM20A mutations as a cause of amelogenesis imperfecta and gingival hyperplasia syndrome.

机译：全外显子组测序确定FAM20A突变是牙釉质生成不全和牙龈增生综合征的原因。

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Amelogenesis imperfecta (AI) describes a clinically and genetically heterogeneous group of disorders of biomineralization resulting from failure of normal enamel formation. AI is found as an isolated entity or as part of a syndrome, and an autosomal-recessive syndrome associating AI and gingival hyperplasia was recently reported. Using whole-exome sequencing, we identified a homozygous nonsense mutation in exon 2 of FAM20A that was not present in the Single Nucleotide Polymorphism database (dbSNP), the 1000 Genomes database, or the Centre d'Etude du Polymorphisme Humain (CEPH) Diversity Panel. Expression analyses indicated that Fam20a is expressed in ameloblasts and gingivae, providing biological plausibility for mutations in FAM20A underlying the pathogenesis of this syndrome.

机译：牙釉质发育不全（AI）描述了由于正常牙釉质形成失败而导致的生物矿化疾病的临床和遗传异质性组。人们发现AI是孤立的实体或作为综合征的一部分，最近报道了常染色体隐性综合征将AI与牙龈增生相关。使用全外显子组测序，我们在单核苷酸多态性数据库（dbSNP），1000基因组数据库或Hut中心爱迪德多态性中心（CEPH）多样性小组中发现了FAM20A外显子2的纯合性无义突变。。表达分析表明，Fam20a在成釉细胞和牙龈中表达，为该综合征发病机理的FAM20A突变提供了生物学上的可行性。

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《The American Journal of Human Genetics》 |2011年第5期|共5页
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OSullivan J; Bitu CC; Daly SB; Urquhart JE; Barron MJ; Bhaskar SS; Martelli Junior H; dos Santos Neto PE; Mansilla MA; Murray JC; Coletta RD; Black GC; Dixon MJ;
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中图分类医学遗传学;
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入库时间 2022-08-18 17:42:37

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1. Whole-Exome sequencing identifies FAM20A mutations as a cause of amelogenesis imperfecta and gingival hyperplasia syndrome. [J] . OSullivan J, Bitu CC, Daly SB, The American Journal of Human Genetics . 2011,第5期

机译：全外显子组测序确定FAM20A突变是牙釉质生成不全和牙龈增生综合征的原因。
2. Whole-exome sequencing, without prior linkage, identifies a mutation in LAMB3 as a cause of dominant hypoplastic amelogenesis imperfecta [J] . PoulterJ.A., El-SayedW., ShoreR.C., European journal of human genetics: EJHG . 2014,第1期

机译：全基因组测序，没有事先的联系，确定LAMB3中的突变是显性发育不良性釉突形成不全的原因
3. Whole-exome sequencing, without prior linkage, identifies a mutation in LAMB3 as a cause of dominant hypoplastic amelogenesis imperfecta [J] . PoulterJ.A., El-SayedW., ShoreR.C., European journal of human genetics: EJHG . 2014,第1期

机译：在没有先前联系的情况下，全末端测序识别Lamb3中的突变，作为主要的假软质杂志生成的原因
4. A Bioinformatics Procedure to Identify and Annotate Somatic Mutations in Whole-Exome Sequencing Data [C] . Roberta Spinelli, Rocco Piazza, Alessandra Pirola, International meeting on computational intelligence methods for bioinformatics and biostatistics . 2012

机译：在整个外显子组测序数据中识别和注释体细胞突变的生物信息学程序
5. Analysis of somatic mutations identified by whole-exome sequencing in colorectal cancer metastasis [D] . Zhao, Bixiao 2016

机译：通过全外显子测序鉴定的大肠癌转移中的体细胞突变分析
6. Whole-Exome Sequencing Identifies FAM20A Mutations as a Cause of Amelogenesis Imperfecta and Gingival Hyperplasia Syndrome [O] . James OSullivan, Carolina C. Bitu, Sarah B. Daly, 2011

机译：全外显子组测序确定FAM20A突变为成釉不全和牙龈增生综合征的原因
7. Whole-Exome Sequencing Identifies FAM20A Mutations as a Cause of Amelogenesis Imperfecta and Gingival Hyperplasia Syndrome [O] . O'Sullivan, James, Bitu, Carolina C., Daly, Sarah B., 2011

机译：全外显子组测序确定FAM20A突变为成釉不全和牙龈增生综合征的原因

Whole-Exome sequencing identifies FAM20A mutations as a cause of amelogenesis imperfecta and gingival hyperplasia syndrome.

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