Hi-C Identifies Complex Genomic Rearrangements and TAD-Shuffling in Developmental Diseases

Uirá Souto Melo; Robert Schöpflin; Rocio Acuna-Hidalgo; Martin Atta Mensah; Björn Fischer-Zirnsak; Manuel Holtgrewe; Marius Konstantin Klever; Seval Türkmen; Verena Heinrich; Ilina Datkhaeva Pluym; Eunice Matoso; Sérgio Bernardo de Sousa; Pedro Louro; Wiebke Hülsemann; Monika Cohen; Andreas Dufke; Anna Latos-Bieleńska; Martin Vingron; Vera Kalscheuer; Fabiola Quintero-Rivera; Malte Spielmann; Stefan Mundlos

doi:10.1016/j.ajhg.2020.04.016

Hi-C Identifies Complex Genomic Rearrangements and TAD-Shuffling in Developmental Diseases

Uirá Souto Melo, Robert Schöpflin, Rocio Acuna-Hidalgo, Martin Atta Mensah, Björn Fischer-Zirnsak, Manuel Holtgrewe, Marius Konstantin Klever, Seval Türkmen, Verena Heinrich, Ilina Datkhaeva Pluym, Eunice Matoso, Sérgio Bernardo de Sousa, Pedro Louro, Wiebke Hülsemann, Monika Cohen, Andreas Dufke, Anna Latos-Bieleńska, Martin Vingron, Vera Kalscheuer, Fabiola Quintero-RiveraMalte Spielmann^*, Stefan Mundlos

^*Korrespondierende/r Autor/-in für diese Arbeit

Institut für Humangenetik

96 Zitate (Scopus)

Abstract

Genome-wide analysis methods, such as array comparative genomic hybridization (CGH) and whole-genome sequencing (WGS), have greatly advanced the identification of structural variants (SVs) in the human genome. However, even with standard high-throughput sequencing techniques, complex rearrangements with multiple breakpoints are often difficult to resolve, and predicting their effects on gene expression and phenotype remains a challenge. Here, we address these problems by using high-throughput chromosome conformation capture (Hi-C) generated from cultured cells of nine individuals with developmental disorders (DDs). Three individuals had previously been identified as harboring duplications at the SOX9 locus and six had been identified with translocations. Hi-C resolved the positions of the duplications and was instructive in interpreting their distinct pathogenic effects, including the formation of new topologically associating domains (neo-TADs). Hi-C was very sensitive in detecting translocations, and it revealed previously unrecognized complex rearrangements at the breakpoints. In several cases, we observed the formation of fused-TADs promoting ectopic enhancer-promoter interactions that were likely to be involved in the disease pathology. In summary, we show that Hi-C is a sensible method for the detection of complex SVs in a clinical setting. The results help interpret the possible pathogenic effects of the SVs in individuals with DDs.

Originalsprache	Englisch
Zeitschrift	American Journal of Human Genetics
Jahrgang	106
Ausgabenummer	6
Seiten (von - bis)	872-884
Seitenumfang	13
ISSN	0002-9297
DOIs	https://doi.org/10.1016/j.ajhg.2020.04.016
Publikationsstatus	Veröffentlicht - 04.06.2020

Fördermittel

We would like to thank the individuals and families for their collaboration and contribution to this project. Technical assistance: We thank Susanne Rothe, Vanessa Suckow, and Celina São-José for their excellent work. We thank Angela Maria Vianna-Morgante for assistance in reviewing the cytogenetics nomenclature. Funding: M.S. and S.M. are supported by grants from the Deutsche Forschungsgemeinschaft ( DFG ) ( SP1532/3-1 , SP1532/4-1 , SP1532/5-1 , and MU 880/16-1 ) and the Max Planck Foundation . U.S.M. is a fellow of the Capes-Alexander von Humboldt Foundation .

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Strategische Forschungsbereiche und Zentren

Querschnittsbereich: Medizinische Genetik

Dokumente

10.1016/j.ajhg.2020.04.016

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Melo, U. S., Schöpflin, R., Acuna-Hidalgo, R., Mensah, M. A., Fischer-Zirnsak, B., Holtgrewe, M., Klever, M. K., Türkmen, S., Heinrich, V., Pluym, I. D., Matoso, E., Bernardo de Sousa, S., Louro, P., Hülsemann, W., Cohen, M., Dufke, A., Latos-Bieleńska, A., Vingron, M., Kalscheuer, V., ... Mundlos, S. (2020). Hi-C Identifies Complex Genomic Rearrangements and TAD-Shuffling in Developmental Diseases. American Journal of Human Genetics, 106(6), 872-884. https://doi.org/10.1016/j.ajhg.2020.04.016

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abstract = "Genome-wide analysis methods, such as array comparative genomic hybridization (CGH) and whole-genome sequencing (WGS), have greatly advanced the identification of structural variants (SVs) in the human genome. However, even with standard high-throughput sequencing techniques, complex rearrangements with multiple breakpoints are often difficult to resolve, and predicting their effects on gene expression and phenotype remains a challenge. Here, we address these problems by using high-throughput chromosome conformation capture (Hi-C) generated from cultured cells of nine individuals with developmental disorders (DDs). Three individuals had previously been identified as harboring duplications at the SOX9 locus and six had been identified with translocations. Hi-C resolved the positions of the duplications and was instructive in interpreting their distinct pathogenic effects, including the formation of new topologically associating domains (neo-TADs). Hi-C was very sensitive in detecting translocations, and it revealed previously unrecognized complex rearrangements at the breakpoints. In several cases, we observed the formation of fused-TADs promoting ectopic enhancer-promoter interactions that were likely to be involved in the disease pathology. In summary, we show that Hi-C is a sensible method for the detection of complex SVs in a clinical setting. The results help interpret the possible pathogenic effects of the SVs in individuals with DDs.",

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Melo, US, Schöpflin, R, Acuna-Hidalgo, R, Mensah, MA, Fischer-Zirnsak, B, Holtgrewe, M, Klever, MK, Türkmen, S, Heinrich, V, Pluym, ID, Matoso, E, Bernardo de Sousa, S, Louro, P, Hülsemann, W, Cohen, M, Dufke, A, Latos-Bieleńska, A, Vingron, M, Kalscheuer, V, Quintero-Rivera, F, Spielmann, M & Mundlos, S 2020, 'Hi-C Identifies Complex Genomic Rearrangements and TAD-Shuffling in Developmental Diseases', American Journal of Human Genetics, Jg. 106, Nr. 6, S. 872-884. https://doi.org/10.1016/j.ajhg.2020.04.016

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T1 - Hi-C Identifies Complex Genomic Rearrangements and TAD-Shuffling in Developmental Diseases

AU - Melo, Uirá Souto

AU - Schöpflin, Robert

AU - Acuna-Hidalgo, Rocio

AU - Mensah, Martin Atta

AU - Fischer-Zirnsak, Björn

AU - Holtgrewe, Manuel

AU - Klever, Marius Konstantin

AU - Türkmen, Seval

AU - Heinrich, Verena

AU - Pluym, Ilina Datkhaeva

AU - Matoso, Eunice

AU - Bernardo de Sousa, Sérgio

AU - Louro, Pedro

AU - Hülsemann, Wiebke

AU - Cohen, Monika

AU - Dufke, Andreas

AU - Latos-Bieleńska, Anna

AU - Vingron, Martin

AU - Kalscheuer, Vera

AU - Quintero-Rivera, Fabiola

AU - Spielmann, Malte

AU - Mundlos, Stefan

PY - 2020/6/4

Y1 - 2020/6/4

N2 - Genome-wide analysis methods, such as array comparative genomic hybridization (CGH) and whole-genome sequencing (WGS), have greatly advanced the identification of structural variants (SVs) in the human genome. However, even with standard high-throughput sequencing techniques, complex rearrangements with multiple breakpoints are often difficult to resolve, and predicting their effects on gene expression and phenotype remains a challenge. Here, we address these problems by using high-throughput chromosome conformation capture (Hi-C) generated from cultured cells of nine individuals with developmental disorders (DDs). Three individuals had previously been identified as harboring duplications at the SOX9 locus and six had been identified with translocations. Hi-C resolved the positions of the duplications and was instructive in interpreting their distinct pathogenic effects, including the formation of new topologically associating domains (neo-TADs). Hi-C was very sensitive in detecting translocations, and it revealed previously unrecognized complex rearrangements at the breakpoints. In several cases, we observed the formation of fused-TADs promoting ectopic enhancer-promoter interactions that were likely to be involved in the disease pathology. In summary, we show that Hi-C is a sensible method for the detection of complex SVs in a clinical setting. The results help interpret the possible pathogenic effects of the SVs in individuals with DDs.

AB - Genome-wide analysis methods, such as array comparative genomic hybridization (CGH) and whole-genome sequencing (WGS), have greatly advanced the identification of structural variants (SVs) in the human genome. However, even with standard high-throughput sequencing techniques, complex rearrangements with multiple breakpoints are often difficult to resolve, and predicting their effects on gene expression and phenotype remains a challenge. Here, we address these problems by using high-throughput chromosome conformation capture (Hi-C) generated from cultured cells of nine individuals with developmental disorders (DDs). Three individuals had previously been identified as harboring duplications at the SOX9 locus and six had been identified with translocations. Hi-C resolved the positions of the duplications and was instructive in interpreting their distinct pathogenic effects, including the formation of new topologically associating domains (neo-TADs). Hi-C was very sensitive in detecting translocations, and it revealed previously unrecognized complex rearrangements at the breakpoints. In several cases, we observed the formation of fused-TADs promoting ectopic enhancer-promoter interactions that were likely to be involved in the disease pathology. In summary, we show that Hi-C is a sensible method for the detection of complex SVs in a clinical setting. The results help interpret the possible pathogenic effects of the SVs in individuals with DDs.

UR - https://www.scopus.com/pages/publications/85085579515

U2 - 10.1016/j.ajhg.2020.04.016

DO - 10.1016/j.ajhg.2020.04.016

M3 - Journal articles

C2 - 32470376

AN - SCOPUS:85085579515

SN - 0002-9297

VL - 106

SP - 872

EP - 884

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 6

ER -

Hi-C Identifies Complex Genomic Rearrangements and TAD-Shuffling in Developmental Diseases

Abstract

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