Artículos de revistas
Exome sequencing of multiple-sclerosis patients and their unaffected first-degree relatives
Fecha
2017Registro en:
BMC Research Notes. 2017 Dec 12;10(1):735
10.1186/s13104-017-3072-0
Autor
Garcia-Rosa, Sheila
Amorim, Maria Galli de
Valieris, Renan
Marques, Vanessa Daccach
Lorenzi, Julio Cesar Cetrulo
Toller, Vania Balardin
Olival, Guilherme Sciascia do
Silva Júnior, Wilson Araújo da
Silva, Israel Tojal da
Barreira, Amilton Antunes
Nunes, Diana Noronha
Dias-Neto, Emmanuel
Institución
Resumen
Abstract
Objectives
The understanding of complex multifactorial diseases requires the availability of a variety of data for a large-number of affected individuals. In this data note here we provide whole exome sequencing data from a set of non-familiar multiple-sclerosis (MS) patients as well as their unaffected first-degree relatives. This data might help the identification of genomic alterations, including single nucleotide polymorphisms, de novo variations and structural genomic variations, such as copy-number alterations that may impact this disease.
Data description
This dataset comprises the full exome of 28 Brazilian subjects grouped in eight distinct families, consisting of four complete trios (mother–patient–father) plus another four complete trios with one added unaffected sibling. In total, we present the full exome data of eight patients diagnosed with recurrent remittent multiple sclerosis. Diagnoses were made by experienced neurologists and all enrolled patients had at least 5 years of follow up and specific MS treatment. Exomes were sequenced from leukocyte-derived DNA, after the capture of exons using biotinylated probes, in the Ion Proton platform. For each exome we generated an average of 66.1 million good quality mapped reads with an average length of ~ 160nt. On average, for 90% of the exome a vertical coverage above 20× was reached.