Germline mutations in ABL1 cause an autosomal dominant syndrome characterized by congenital heart defects and skeletal malformations

Xia Wang; Wu Lin Charng; Chun An Chen; Jill A. Rosenfeld; Aisha Al Shamsi; Lihadh Al-Gazali; Marianne McGuire; Nicholas Ah Mew; Georgianne L. Arnold; Chunjing Qu; Yan Ding; Donna M. Muzny; Richard A. Gibbs; Christine M. Eng; Magdalena Walkiewicz; Fan Xia; Sharon E. Plon; James R. Lupski; Christian P. Schaaf; Yaping Yang

doi:10.1038/ng.3815

Germline mutations in ABL1 cause an autosomal dominant syndrome characterized by congenital heart defects and skeletal malformations

Xia Wang, Wu Lin Charng, Chun An Chen, Jill A. Rosenfeld, Aisha Al Shamsi, Lihadh Al-Gazali, Marianne McGuire, Nicholas Ah Mew, Georgianne L. Arnold, Chunjing Qu, Yan Ding, Donna M. Muzny, Richard A. Gibbs, Christine M. Eng, Magdalena Walkiewicz, Fan Xia, Sharon E. Plon, James R. Lupski, Christian P. Schaaf, Yaping Yang

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Abstract

ABL1 is a proto-oncogene well known as part of the fusion gene BCR-ABL1 in the Philadelphia chromosome of leukemia cancer cells. Inherited germline ABL1 changes have not been associated with genetic disorders. Here we report ABL1 germline variants cosegregating with an autosomal dominant disorder characterized by congenital heart disease, skeletal abnormalities, and failure to thrive. The variant c.734A>G (p.Tyr245Cys) was found to occur de novo or cosegregate with disease in five individuals (families 1-3). Additionally, a de novo c.1066G>A (p.Ala356Thr) variant was identified in a sixth individual (family 4). We overexpressed the mutant constructs in HEK 293T cells and observed increased tyrosine phosphorylation, suggesting increased ABL1 kinase activities associated with both the p.Tyr245Cys and p.Ala356Thr substitutions. Our clinical and experimental findings, together with previously reported teratogenic effects of selective BCR-ABL inhibitors in humans and developmental defects in Abl1 knockout mice, suggest that ABL1 has an important role during organismal development.

Original language	English
Pages (from-to)	613-617
Number of pages	5
Journal	Nature Genetics
Volume	49
Issue number	4
DOIs	https://doi.org/10.1038/ng.3815
Publication status	Published - Mar 30 2017

ASJC Scopus subject areas

Genetics

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Wang, X., Charng, W. L., Chen, C. A., Rosenfeld, J. A., Al Shamsi, A., Al-Gazali, L., McGuire, M., Mew, N. A., Arnold, G. L., Qu, C., Ding, Y., Muzny, D. M., Gibbs, R. A., Eng, C. M., Walkiewicz, M., Xia, F., Plon, S. E., Lupski, J. R., Schaaf, C. P., & Yang, Y. (2017). Germline mutations in ABL1 cause an autosomal dominant syndrome characterized by congenital heart defects and skeletal malformations. Nature Genetics, 49(4), 613-617. https://doi.org/10.1038/ng.3815

Wang, X, Charng, WL, Chen, CA, Rosenfeld, JA, Al Shamsi, A, Al-Gazali, L, McGuire, M, Mew, NA, Arnold, GL, Qu, C, Ding, Y, Muzny, DM, Gibbs, RA, Eng, CM, Walkiewicz, M, Xia, F, Plon, SE, Lupski, JR, Schaaf, CP & Yang, Y 2017, 'Germline mutations in ABL1 cause an autosomal dominant syndrome characterized by congenital heart defects and skeletal malformations', Nature Genetics, vol. 49, no. 4, pp. 613-617. https://doi.org/10.1038/ng.3815

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abstract = "ABL1 is a proto-oncogene well known as part of the fusion gene BCR-ABL1 in the Philadelphia chromosome of leukemia cancer cells. Inherited germline ABL1 changes have not been associated with genetic disorders. Here we report ABL1 germline variants cosegregating with an autosomal dominant disorder characterized by congenital heart disease, skeletal abnormalities, and failure to thrive. The variant c.734A>G (p.Tyr245Cys) was found to occur de novo or cosegregate with disease in five individuals (families 1-3). Additionally, a de novo c.1066G>A (p.Ala356Thr) variant was identified in a sixth individual (family 4). We overexpressed the mutant constructs in HEK 293T cells and observed increased tyrosine phosphorylation, suggesting increased ABL1 kinase activities associated with both the p.Tyr245Cys and p.Ala356Thr substitutions. Our clinical and experimental findings, together with previously reported teratogenic effects of selective BCR-ABL inhibitors in humans and developmental defects in Abl1 knockout mice, suggest that ABL1 has an important role during organismal development.",

author = "Xia Wang and Charng, {Wu Lin} and Chen, {Chun An} and Rosenfeld, {Jill A.} and {Al Shamsi}, Aisha and Lihadh Al-Gazali and Marianne McGuire and Mew, {Nicholas Ah} and Arnold, {Georgianne L.} and Chunjing Qu and Yan Ding and Muzny, {Donna M.} and Gibbs, {Richard A.} and Eng, {Christine M.} and Magdalena Walkiewicz and Fan Xia and Plon, {Sharon E.} and Lupski, {James R.} and Schaaf, {Christian P.} and Yaping Yang",

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AU - Al Shamsi, Aisha

AU - Al-Gazali, Lihadh

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AU - Mew, Nicholas Ah

AU - Arnold, Georgianne L.

AU - Qu, Chunjing

AU - Ding, Yan

AU - Muzny, Donna M.

AU - Gibbs, Richard A.

AU - Eng, Christine M.

AU - Walkiewicz, Magdalena

AU - Xia, Fan

AU - Plon, Sharon E.

AU - Lupski, James R.

AU - Schaaf, Christian P.

AU - Yang, Yaping

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Germline mutations in ABL1 cause an autosomal dominant syndrome characterized by congenital heart defects and skeletal malformations

Abstract

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