论文信息 - Exome-based mapping and variant prioritization for inherited Mendelian disorders. - 字舞流文

Exome-based mapping and variant prioritization for inherited Mendelian disorders.

Exome sequencing in families affected by rare genetic disorders has the potential to rapidly identify new disease genes (genes in which mutations cause disease), but the identification of a single causal mutation among thousands of variants remains a significant challenge. We developed a scoring algorithm to prioritize potential causal variants within a family according to segregation with the phenotype, population frequency, predicted effect, and gene expression in the tissue(s) of interest. To narrow the search space in families with multiple affected individuals, we also developed two complementary approaches to exome-based mapping of autosomal-dominant disorders. One approach identifies segments of maximum identity by descent among affected individuals; the other nominates regions on the basis of shared rare variants and the absence of homozygous differences between affected individuals. We showcase our methods by using exome sequence data from families affected by autosomal-dominant retinitis pigmentosa (adRP), a rare disorder characterized by night blindness and progressive vision loss. We performed exome capture and sequencing on 91 samples representing 24 families affected by probable adRP but lacking common disease-causing mutations. Eight of 24 families (33%) were revealed to harbor high-scoring, most likely pathogenic (by clinical assessment) mutations affecting known RP genes. Analysis of the remaining 17 families identified candidate variants in a number of interesting genes, some of which have withstood further segregation testing in extended pedigrees. To empower the search for Mendelian-disease genes in family-based sequencing studies, we implemented them in a cross-platform-compatible software package, MendelScan, which is freely available to the research community.

Jennifer D. Churchill | David E Larson | Nathaniel G. Nutter | George M Weinstock | R. Wilson | K. M. Steinberg | G. Weinstock | D. Larson | D. Koboldt | S. Daiger | S. Bowne | L. Sullivan | S. Blanton | E. Pierce | Richard K Wilson | Lori S Sullivan | Sara J Bowne | Susan H Blanton | Stephen P Daiger | Eric A Pierce | Jennifer D Churchill | Daniel C Koboldt | Karyn M Steinberg | Aimee C Buhr | Nathan Nutter | R. Wilson | S. J. Bowne

[1] Christopher A. Miller,et al. VarScan 2: somatic mutation and copy number alteration discovery in cancer by exome sequencing. , 2012, Genome research.

[2] Emily H Turner,et al. Exome sequencing identifies MLL2 mutations as a cause of Kabuki syndrome , 2010, Nature Genetics.

[3] Iuliana Ionita-Laza,et al. Finding disease variants in Mendelian disorders by using sequence data: methods and applications. , 2011, American journal of human genetics.

[4] Tom Walsh,et al. Whole exome sequencing and homozygosity mapping identify mutation in the cell polarity protein GPSM2 as the cause of nonsyndromic hearing loss DFNB82. , 2010, American journal of human genetics.

[5] Jonathan C. Cohen,et al. Exome sequencing, ANGPTL3 mutations, and familial combined hypolipidemia. , 2010, The New England journal of medicine.

[6] Joseph K. Pickrell,et al. A Systematic Survey of Loss-of-Function Variants in Human Protein-Coding Genes , 2012, Science.

[7] Stephan J Sanders,et al. Whole exome sequencing identifies recessive WDR62 mutations in severe brain malformations , 2010, Nature.

[8] P. Sieving,et al. Mutations in the small nuclear riboprotein 200 kDa gene (SNRNP200) cause 1.6% of autosomal dominant retinitis pigmentosa , 2013, Molecular vision.

[9] Murat Sincan,et al. VAR‐MD: A tool to analyze whole exome–genome variants in small human pedigrees with mendelian inheritance , 2012, Human mutation.

[10] Hatice Duzkale,et al. Prevalence of disease-causing mutations in families with autosomal dominant retinitis pigmentosa: a screen of known genes in 200 families. , 2006, Investigative ophthalmology & visual science.

[11] S. Daiger,et al. Genes and mutations causing retinitis pigmentosa , 2013, Clinical genetics.

[12] Johnny S. H. Kwan,et al. A comprehensive framework for prioritizing variants in exome sequencing studies of Mendelian diseases , 2012, Nucleic acids research.

[13] Bronwen L. Aken,et al. GENCODE: The reference human genome annotation for The ENCODE Project , 2012, Genome research.

[14] R. Fulton,et al. A dominant mutation in RPE65 identified by whole-exome sequencing causes retinitis pigmentosa with choroidal involvement , 2011, European Journal of Human Genetics.

[15] E. Morrow,et al. Genome-wide transcriptome analysis in murine neural retina using high-throughput RNA sequencing. , 2012, Genomics.

[16] P. Shannon,et al. Exome sequencing identifies the cause of a Mendelian disorder , 2009, Nature Genetics.

[17] Patrizia Sola,et al. Exome Sequencing Reveals VCP Mutations as a Cause of Familial ALS , 2011, Neuron.

[18] M. G. Reese,et al. A probabilistic disease-gene finder for personal genomes. , 2011, Genome research.

[19] S. Liebowitz. Retinitis pigmentosa. , 1979, Journal - American Intra-Ocular Implant Society.

[20] F. Rieux-Laucat,et al. Whole-exome-sequencing-based discovery of human FADD deficiency. , 2010, American journal of human genetics.

[21] G. Grant,et al. Transcriptome analyses of the human retina identify unprecedented transcript diversity and 3.5 Mb of novel transcribed sequence via significant alternative splicing and novel genes , 2013, BMC Genomics.

[22] J. Shendure,et al. Exome sequencing as a tool for Mendelian disease gene discovery , 2011, Nature Reviews Genetics.

[23] R. Lewis,et al. Genomic rearrangements of the PRPF31 gene account for 2.5% of autosomal dominant retinitis pigmentosa. , 2006, Investigative ophthalmology & visual science.

[24] Richard Durbin,et al. Sequence analysis Fast and accurate short read alignment with Burrows – Wheeler transform , 2009 .

[25] Sebastian Bauer,et al. Identity-by-descent filtering of exome sequence data identifies PIGV mutations in hyperphosphatasia mental retardation syndrome , 2010, Nature Genetics.

[26] Jennifer D. Churchill,et al. Mutations in the X-linked retinitis pigmentosa genes RPGR and RP2 found in 8.5% of families with a provisional diagnosis of autosomal dominant retinitis pigmentosa. , 2013, Investigative Ophthalmology and Visual Science.

[27] Xin Jin,et al. TGM6 identified as a novel causative gene of spinocerebellar ataxias using exome sequencing. , 2010, Brain : a journal of neurology.

[28] Christian Gilissen,et al. De novo mutations of SETBP1 cause Schinzel-Giedion syndrome , 2010, Nature Genetics.

[29] Johnny S. H. Kwan,et al. Predicting Mendelian Disease-Causing Non-Synonymous Single Nucleotide Variants in Exome Sequencing Studies , 2013, PLoS genetics.

[30] Nada Jabado,et al. Unexpected allelic heterogeneity and spectrum of mutations in Fowler syndrome revealed by next‐generation exome sequencing , 2010, Human mutation.

[31] Christian Gilissen,et al. Exome sequencing identifies WDR35 variants involved in Sensenbrenner syndrome. , 2010, American journal of human genetics.

[32] Elizabeth M. Smigielski,et al. dbSNP: the NCBI database of genetic variation , 2001, Nucleic Acids Res..