Your search keyword '"Guo, D.E."' showing total 3 results

1. Genome-wide association study of sporadic brain arteriovenous malformations

Author

Weinsheimer, S., Bendjilali, N., Nelson, J., Guo, D.E., Zaroff, J.G., Sidney, S., McCulloch, C.E., Salman, R. Al-Shahi, Berg, J.N., Koeleman, B.P.C., Simon, M., Bostroem, A., Fontanella, M., Sturiale, C.L., Pola, R., Puca, A., Lawton, M.T., Young, W.L., Pawlikowska, L., Klijn, C.J.M., Kim, H., Weinsheimer, S., Bendjilali, N., Nelson, J., Guo, D.E., Zaroff, J.G., Sidney, S., McCulloch, C.E., Salman, R. Al-Shahi, Berg, J.N., Koeleman, B.P.C., Simon, M., Bostroem, A., Fontanella, M., Sturiale, C.L., Pola, R., Puca, A., Lawton, M.T., Young, W.L., Pawlikowska, L., Klijn, C.J.M., and Kim, H.

Abstract

Item does not contain fulltext, BACKGROUND: The pathogenesis of sporadic brain arteriovenous malformations (BAVMs) remains unknown, but studies suggest a genetic component. We estimated the heritability of sporadic BAVM and performed a genome-wide association study (GWAS) to investigate association of common single nucleotide polymorphisms (SNPs) with risk of sporadic BAVM in the international, multicentre Genetics of Arteriovenous Malformation (GEN-AVM) consortium. METHODS: The Caucasian discovery cohort included 515 BAVM cases and 1191 controls genotyped using Affymetrix genome-wide SNP arrays. Genotype data were imputed to 1000 Genomes Project data, and well-imputed SNPs (>0.01 minor allele frequency) were analysed for association with BAVM. 57 top BAVM-associated SNPs (51 SNPs with p<10(-05) or p<10(-04) in candidate pathway genes, and 6 candidate BAVM SNPs) were tested in a replication cohort including 608 BAVM cases and 744 controls. RESULTS: The estimated heritability of BAVM was 17.6% (SE 8.9%, age and sex-adjusted p=0.015). None of the SNPs were significantly associated with BAVM in the replication cohort after correction for multiple testing. 6 SNPs had a nominal p<0.1 in the replication cohort and map to introns in EGFEM1P, SP4 and CDKAL1 or near JAG1 and BNC2. Of the 6 candidate SNPs, 2 in ACVRL1 and MMP3 had a nominal p<0.05 in the replication cohort. CONCLUSIONS: We performed the first GWAS of sporadic BAVM in the largest BAVM cohort assembled to date. No GWAS SNPs were replicated, suggesting that common SNPs do not contribute strongly to BAVM susceptibility. However, heritability estimates suggest a modest but significant genetic contribution.

Published

2016

2. Association between Venous Angioarchitectural Features of Sporadic Brain Arteriovenous Malformations and Intracranial Hemorrhage

Author

Alexander, M.D., primary, Cooke, D.L., additional, Nelson, J., additional, Guo, D.E., additional, Dowd, C.F., additional, Higashida, R.T., additional, Halbach, V.V., additional, Lawton, M.T., additional, Kim, H., additional, and Hetts, S.W., additional

Published

2015

3. A genome-wide investigation of copy number variation in patients with sporadic brain arteriovenous malformation

Author

Bendjilali, N., Kim, H., Weinsheimer, S., Guo, D.E., Kwok, P.Y., Zaroff, J.G., Sidney, S., Lawton, M.T., McCulloch, C.E., Koeleman, B.P.C., Klijn, C.J., Young, W.L., Pawlikowska, L., Bendjilali, N., Kim, H., Weinsheimer, S., Guo, D.E., Kwok, P.Y., Zaroff, J.G., Sidney, S., Lawton, M.T., McCulloch, C.E., Koeleman, B.P.C., Klijn, C.J., Young, W.L., and Pawlikowska, L.

Abstract

Contains fulltext : 169573.PDF (publisher's version ) (Open Access), BACKGROUND: Brain arteriovenous malformations (BAVM) are clusters of abnormal blood vessels, with shunting of blood from the arterial to venous circulation and a high risk of rupture and intracranial hemorrhage. Most BAVMs are sporadic, but also occur in patients with Hereditary Hemorrhagic Telangiectasia, a Mendelian disorder caused by mutations in genes in the transforming growth factor beta (TGFbeta) signaling pathway. METHODS: To investigate whether copy number variations (CNVs) contribute to risk of sporadic BAVM, we performed a genome-wide association study in 371 sporadic BAVM cases and 563 healthy controls, all Caucasian. Cases and controls were genotyped using the Affymetrix 6.0 array. CNVs were called using the PennCNV and Birdsuite algorithms and analyzed via segment-based and gene-based approaches. Common and rare CNVs were evaluated for association with BAVM. RESULTS: A CNV region on 1p36.13, containing the neuroblastoma breakpoint family, member 1 gene (NBPF1), was significantly enriched with duplications in BAVM cases compared to controls (P = 2.2x10(-9)); NBPF1 was also significantly associated with BAVM in gene-based analysis using both PennCNV and Birdsuite. We experimentally validated the 1p36.13 duplication; however, the association did not replicate in an independent cohort of 184 sporadic BAVM cases and 182 controls (OR = 0.81, P = 0.8). Rare CNV analysis did not identify genes significantly associated with BAVM. CONCLUSION: We did not identify common CNVs associated with sporadic BAVM that replicated in an independent cohort. Replication in larger cohorts is required to elucidate the possible role of common or rare CNVs in BAVM pathogenesis.

Published

2013