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本文引用的文献

1
Resolution of Disease Phenotypes Resulting from Multilocus Genomic Variation.多位点基因组变异导致的疾病表型的解析
N Engl J Med. 2017 Jan 5;376(1):21-31. doi: 10.1056/NEJMoa1516767. Epub 2016 Dec 7.
2
When One Diagnosis Is Not Enough.当一个诊断不够用时。
N Engl J Med. 2017 Jan 5;376(1):83-85. doi: 10.1056/NEJMe1614384. Epub 2016 Dec 7.
3
Phenotype and natural history in 101 individuals with Pitt-Hopkins syndrome through an internet questionnaire system.通过互联网问卷系统对101例皮特-霍普金斯综合征患者的表型和自然病史研究
Orphanet J Rare Dis. 2016 Apr 12;11:37. doi: 10.1186/s13023-016-0422-2.
4
Manipulation of primer affinity improves high-resolution melting accuracy for imprinted genes.引物亲和力的调控可提高印记基因的高分辨率熔解准确性。
Genet Mol Res. 2015 Jul 14;14(3):7864-72. doi: 10.4238/2015.July.14.12.
5
If not Angelman, what is it? A review of Angelman-like syndromes.若不是天使综合征,那是什么?类天使综合征综述。
Am J Med Genet A. 2014 Apr;164A(4):975-92. doi: 10.1002/ajmg.a.36416.
6
A homozygous missense mutation in HERC2 associated with global developmental delay and autism spectrum disorder.HERC2 基因纯合错义突变导致的全面发育迟缓伴自闭症谱系障碍
Hum Mutat. 2012 Dec;33(12):1639-46. doi: 10.1002/humu.22237.
7
SIFT web server: predicting effects of amino acid substitutions on proteins.SIFT 网页服务器:预测氨基酸取代对蛋白质的影响。
Nucleic Acids Res. 2012 Jul;40(Web Server issue):W452-7. doi: 10.1093/nar/gks539. Epub 2012 Jun 11.
8
Pitt-Hopkins Syndrome.皮特-霍普金斯综合征
Mol Syndromol. 2012 Apr;2(3-5):171-180. doi: 10.1159/000335287. Epub 2011 Dec 29.
9
Pitt-Hopkins syndrome-associated mutations in TCF4 lead to variable impairment of the transcription factor function ranging from hypomorphic to dominant-negative effects.TCF4 相关的 Pitt-Hopkins 综合征基因突变导致转录因子功能的可变损伤,从低效能到显性负效应不等。
Hum Mol Genet. 2012 Jul 1;21(13):2873-88. doi: 10.1093/hmg/dds112. Epub 2012 Mar 28.
10
Prader-Willi syndrome.普拉德-威利综合征。
Genet Med. 2012 Jan;14(1):10-26. doi: 10.1038/gim.0b013e31822bead0. Epub 2011 Sep 26.

双分子诊断导致同卵双胞胎出现非典型普拉德-威利表型。

Dual molecular diagnosis contributes to atypical Prader-Willi phenotype in monozygotic twins.

作者信息

Jehee Fernanda S, de Oliveira Valdirene T, Gurgel-Giannetti Juliana, Pietra Rafaella X, Rubatino Fernando V M, Carobin Natália V, Vianna Gabrielle S, de Freitas Mariana L, Fernandes Karla S, Ribeiro Beatriz S V, Brüggenwirth Hennie T, Ali-Amin Roza, White Janson J, Akdemir Zeynep C, Jhangiani Shalini N, Gibbs Richard A, Lupski James R, Varela Monica C, Koiffmann Célia, Rosenberg Carla, Carvalho Cláudia M B

机构信息

Instituto de Ensino e Pesquisa Santa Casa de Belo Horizonte, Belo Horizonte, Minas Gerais, Brazil.

Faculdade de Medicina da Universidade Federal de Minas Gerais, Belo Horizonte, Minas Gerais, Brazil.

出版信息

Am J Med Genet A. 2017 Sep;173(9):2451-2455. doi: 10.1002/ajmg.a.38315. Epub 2017 Jun 20.

DOI:10.1002/ajmg.a.38315
PMID:28631899
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5561000/
Abstract

We describe monozygotic twin girls with genetic variation at two separate loci resulting in a blended phenotype of Prader-Willi syndrome and Pitt-Hopkins syndrome. These girls were diagnosed in early infancy with Prader-Willi syndrome, but developed an atypical phenotype, with apparent intellectual deficiency and lack of obesity. Array-comparative genomic hybridization confirmed a de novo paternal deletion of the 15q11.2q13 region and exome sequencing identified a second mutational event in both girls, which was a novel variant c.145+1G>A affecting a TCF4 canonical splicing site inherited from the mosaic mother. RNA studies showed that the variant abolished the donor splicing site, which was accompanied by activation of an alternative non-canonical splicing-site which then predicts a premature stop codon in the following exon. Clinical re-evaluation of the twins indicated that both variants are likely contributing to the more severe phenotypic presentation. Our data show that atypical clinical presentations may actually be the expression of blended clinical phenotypes arising from independent pathogenic events at two loci.

摘要

我们描述了一对单卵双胞胎女孩,她们在两个不同位点存在基因变异,导致出现普拉德-威利综合征和皮特-霍普金斯综合征的混合表型。这两个女孩在婴儿早期被诊断为普拉德-威利综合征,但出现了非典型表型,表现为明显的智力缺陷且无肥胖症状。阵列比较基因组杂交证实了15q11.2q13区域的新发父源缺失,外显子组测序在两个女孩中均发现了第二个突变事件,即一个影响TCF4经典剪接位点的新型变异c.145+1G>A,该变异遗传自嵌合型母亲。RNA研究表明,该变异消除了供体剪接位点,同时激活了一个替代的非经典剪接位点,这进而预测在下一个外显子中会出现提前终止密码子。对这对双胞胎的临床重新评估表明,这两种变异可能都导致了更严重的表型表现。我们的数据表明,非典型临床表现实际上可能是由两个位点独立致病事件引起的混合临床表型的表现。