Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing

Andy Itsara; Lisenka E.L.M. Vissers; Karyn Meltz Steinberg; Kevin J. Meyer; Michael C. Zody; David A. Koolen; Joep De Ligt; Edwin Cuppen; Carl Baker; Choli Lee; Tina A. Graves; Richard K. Wilson; Robert B. Jenkins; Joris A. Veltman; Evan E. Eichler

doi:10.1016/j.ajhg.2012.02.013

Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing

Andy Itsara
, Lisenka E.L.M. Vissers
, Karyn Meltz Steinberg
, Kevin J. Meyer
, Michael C. Zody
, David A. Koolen
, Joep De Ligt
, Edwin Cuppen
, Carl Baker
, Choli Lee
, Tina A. Graves
, Richard K. Wilson
, Robert B. Jenkins
, Joris A. Veltman
, Evan E. Eichler

McDonnell Genome Institute (MGI)

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Recurrent deletions have been associated with numerous diseases and genomic disorders. Few, however, have been resolved at the molecular level because their breakpoints often occur in highly copy-number-polymorphic duplicated sequences. We present an approach that uses a combination of somatic cell hybrids, array comparative genomic hybridization, and the specificity of next-generation sequencing to determine breakpoints that occur within segmental duplications. Applying our technique to the 17q21.31 microdeletion syndrome, we used genome sequencing to determine copy-number-variant breakpoints in three deletion-bearing individuals with molecular resolution. For two cases, we observed breakpoints consistent with nonallelic homologous recombination involving only H2 chromosomal haplotypes, as expected. Molecular resolution revealed that the breakpoints occurred at different locations within a 145 kbp segment of >99% identity and disrupt KANSL1 (previously known as KANSL1). In the remaining case, we found that unequal crossover occurred interchromosomally between the H1 and H2 haplotypes and that this event was mediated by a homologous sequence that was once again missing from the human reference. Interestingly, the breakpoints mapped preferentially to gaps in the current reference genome assembly, which we resolved in this study. Our method provides a strategy for the identification of breakpoints within complex regions of the genome harboring high-identity and copy-number-polymorphic segmental duplication. The approach should become particularly useful as high-quality alternate reference sequences become available and genome sequencing of individuals' DNA becomes more routine.

Original language	English
Pages (from-to)	599-613
Number of pages	15
Journal	American journal of human genetics
Volume	90
Issue number	4
DOIs	https://doi.org/10.1016/j.ajhg.2012.02.013
State	Published - Apr 6 2012

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Itsara, A., Vissers, L. E. L. M., Steinberg, K. M., Meyer, K. J., Zody, M. C., Koolen, D. A., De Ligt, J., Cuppen, E., Baker, C., Lee, C., Graves, T. A., Wilson, R. K., Jenkins, R. B., Veltman, J. A., & Eichler, E. E. (2012). Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing. American journal of human genetics, 90(4), 599-613. https://doi.org/10.1016/j.ajhg.2012.02.013

@article{fe52b3248fab454db96b8d0c01b76c0f,

title = "Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing",

abstract = "Recurrent deletions have been associated with numerous diseases and genomic disorders. Few, however, have been resolved at the molecular level because their breakpoints often occur in highly copy-number-polymorphic duplicated sequences. We present an approach that uses a combination of somatic cell hybrids, array comparative genomic hybridization, and the specificity of next-generation sequencing to determine breakpoints that occur within segmental duplications. Applying our technique to the 17q21.31 microdeletion syndrome, we used genome sequencing to determine copy-number-variant breakpoints in three deletion-bearing individuals with molecular resolution. For two cases, we observed breakpoints consistent with nonallelic homologous recombination involving only H2 chromosomal haplotypes, as expected. Molecular resolution revealed that the breakpoints occurred at different locations within a 145 kbp segment of >99\% identity and disrupt KANSL1 (previously known as KANSL1). In the remaining case, we found that unequal crossover occurred interchromosomally between the H1 and H2 haplotypes and that this event was mediated by a homologous sequence that was once again missing from the human reference. Interestingly, the breakpoints mapped preferentially to gaps in the current reference genome assembly, which we resolved in this study. Our method provides a strategy for the identification of breakpoints within complex regions of the genome harboring high-identity and copy-number-polymorphic segmental duplication. The approach should become particularly useful as high-quality alternate reference sequences become available and genome sequencing of individuals' DNA becomes more routine.",

author = "Andy Itsara and Vissers, \{Lisenka E.L.M.\} and Steinberg, \{Karyn Meltz\} and Meyer, \{Kevin J.\} and Zody, \{Michael C.\} and Koolen, \{David A.\} and \{De Ligt\}, Joep and Edwin Cuppen and Carl Baker and Choli Lee and Graves, \{Tina A.\} and Wilson, \{Richard K.\} and Jenkins, \{Robert B.\} and Veltman, \{Joris A.\} and Eichler, \{Evan E.\}",

note = "Funding Information: We thank B. Coe, S. Ng and J. Hehir-Kwa for thoughtful discussion, T. Brown for assistance with manuscript preparation, A. Mackenzie, C. Igartua, C. Fields, S. Casadei, L. Vives, members of the Mayo Medical Laboratories, members of The Genome Institute at Washington University, and members of the Hubrecht Institute for assistance with data generation, and B. de Vries for clinical collection and evaluation of individuals with 17q microdeletions and their parents. K.M.S. was supported by a Ruth L. Kirschstein National Research Service Award (NRSA) Fellowship (F32GM097807). This work was supported by National Institutes of Health grants HG002385 and HG004120 to E.E.E, and the Netherlands Organization for Health Research and Development (ZonMW 916.86.016 to L.E.L.M.V., and 917.66.363 to JAV). E.E.E. is an investigator of the Howard Hughes Medical Institute. E.E.E. is on the scientific advisory boards for Pacific Biosciences, Inc. and SynapDx Corp. ",

year = "2012",

month = apr,

day = "6",

doi = "10.1016/j.ajhg.2012.02.013",

language = "English",

volume = "90",

pages = "599--613",

journal = "American journal of human genetics",

issn = "0002-9297",

number = "4",

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Itsara, A, Vissers, LELM, Steinberg, KM, Meyer, KJ, Zody, MC, Koolen, DA, De Ligt, J, Cuppen, E, Baker, C, Lee, C, Graves, TA, Wilson, RK, Jenkins, RB, Veltman, JA & Eichler, EE 2012, 'Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing', American journal of human genetics, vol. 90, no. 4, pp. 599-613. https://doi.org/10.1016/j.ajhg.2012.02.013

TY - JOUR

T1 - Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing

AU - Itsara, Andy

AU - Vissers, Lisenka E.L.M.

AU - Steinberg, Karyn Meltz

AU - Meyer, Kevin J.

AU - Zody, Michael C.

AU - Koolen, David A.

AU - De Ligt, Joep

AU - Cuppen, Edwin

AU - Baker, Carl

AU - Lee, Choli

AU - Graves, Tina A.

AU - Wilson, Richard K.

AU - Jenkins, Robert B.

AU - Veltman, Joris A.

AU - Eichler, Evan E.

N1 - Funding Information: We thank B. Coe, S. Ng and J. Hehir-Kwa for thoughtful discussion, T. Brown for assistance with manuscript preparation, A. Mackenzie, C. Igartua, C. Fields, S. Casadei, L. Vives, members of the Mayo Medical Laboratories, members of The Genome Institute at Washington University, and members of the Hubrecht Institute for assistance with data generation, and B. de Vries for clinical collection and evaluation of individuals with 17q microdeletions and their parents. K.M.S. was supported by a Ruth L. Kirschstein National Research Service Award (NRSA) Fellowship (F32GM097807). This work was supported by National Institutes of Health grants HG002385 and HG004120 to E.E.E, and the Netherlands Organization for Health Research and Development (ZonMW 916.86.016 to L.E.L.M.V., and 917.66.363 to JAV). E.E.E. is an investigator of the Howard Hughes Medical Institute. E.E.E. is on the scientific advisory boards for Pacific Biosciences, Inc. and SynapDx Corp.

PY - 2012/4/6

Y1 - 2012/4/6

N2 - Recurrent deletions have been associated with numerous diseases and genomic disorders. Few, however, have been resolved at the molecular level because their breakpoints often occur in highly copy-number-polymorphic duplicated sequences. We present an approach that uses a combination of somatic cell hybrids, array comparative genomic hybridization, and the specificity of next-generation sequencing to determine breakpoints that occur within segmental duplications. Applying our technique to the 17q21.31 microdeletion syndrome, we used genome sequencing to determine copy-number-variant breakpoints in three deletion-bearing individuals with molecular resolution. For two cases, we observed breakpoints consistent with nonallelic homologous recombination involving only H2 chromosomal haplotypes, as expected. Molecular resolution revealed that the breakpoints occurred at different locations within a 145 kbp segment of >99% identity and disrupt KANSL1 (previously known as KANSL1). In the remaining case, we found that unequal crossover occurred interchromosomally between the H1 and H2 haplotypes and that this event was mediated by a homologous sequence that was once again missing from the human reference. Interestingly, the breakpoints mapped preferentially to gaps in the current reference genome assembly, which we resolved in this study. Our method provides a strategy for the identification of breakpoints within complex regions of the genome harboring high-identity and copy-number-polymorphic segmental duplication. The approach should become particularly useful as high-quality alternate reference sequences become available and genome sequencing of individuals' DNA becomes more routine.

AB - Recurrent deletions have been associated with numerous diseases and genomic disorders. Few, however, have been resolved at the molecular level because their breakpoints often occur in highly copy-number-polymorphic duplicated sequences. We present an approach that uses a combination of somatic cell hybrids, array comparative genomic hybridization, and the specificity of next-generation sequencing to determine breakpoints that occur within segmental duplications. Applying our technique to the 17q21.31 microdeletion syndrome, we used genome sequencing to determine copy-number-variant breakpoints in three deletion-bearing individuals with molecular resolution. For two cases, we observed breakpoints consistent with nonallelic homologous recombination involving only H2 chromosomal haplotypes, as expected. Molecular resolution revealed that the breakpoints occurred at different locations within a 145 kbp segment of >99% identity and disrupt KANSL1 (previously known as KANSL1). In the remaining case, we found that unequal crossover occurred interchromosomally between the H1 and H2 haplotypes and that this event was mediated by a homologous sequence that was once again missing from the human reference. Interestingly, the breakpoints mapped preferentially to gaps in the current reference genome assembly, which we resolved in this study. Our method provides a strategy for the identification of breakpoints within complex regions of the genome harboring high-identity and copy-number-polymorphic segmental duplication. The approach should become particularly useful as high-quality alternate reference sequences become available and genome sequencing of individuals' DNA becomes more routine.

UR - https://www.scopus.com/pages/publications/84859510490

U2 - 10.1016/j.ajhg.2012.02.013

DO - 10.1016/j.ajhg.2012.02.013

M3 - Article

C2 - 22482802

AN - SCOPUS:84859510490

SN - 0002-9297

VL - 90

SP - 599

EP - 613

JO - American journal of human genetics

JF - American journal of human genetics

IS - 4

ER -

Resolving the breakpoints of the 17q21.31 microdeletion syndrome with next-generation sequencing

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