Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration.

Colby Chiang; Jessie C Jacobsen; Carl Ernst; Carrie Hanscom; Adrian Heilbut; Ian Blumenthal; Ryan E Mills; Andrew Kirby; Amelia M Lindgren; Skye R Rudiger; Clive J McLaughlan; C Simon Bawden; Suzanne J Reid; Richard L M Faull; Russell G Snell; Ira M Hall; Yiping Shen; Toshiro K Ohsumi; Mark L Borowsky; Mark J Daly; Charles Lee; Cynthia C Morton; Marcy E MacDonald; James F Gusella; Michael E Talkowski

doi:10.1038/ng.2202

Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration.

Colby Chiang, Jessie C Jacobsen, Carl Ernst, Carrie Hanscom, Adrian Heilbut, Ian Blumenthal, Ryan E Mills, Andrew Kirby, Amelia M Lindgren, Skye R Rudiger, Clive J McLaughlan, C Simon Bawden, Suzanne J Reid, Richard L M Faull, Russell G Snell, Ira M Hall, Yiping Shen, Toshiro K Ohsumi, Mark L Borowsky, Mark J DalyCharles Lee, Cynthia C Morton, Marcy E MacDonald, James F Gusella, Michael E Talkowski

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

Abstract

We defined the genetic landscape of balanced chromosomal rearrangements at nucleotide resolution by sequencing 141 breakpoints from cytogenetically interpreted translocations and inversions. We confirm that the recently described phenomenon of 'chromothripsis' (massive chromosomal shattering and reorganization) is not unique to cancer cells but also occurs in the germline, where it can resolve to a relatively balanced state with frequent inversions. We detected a high incidence of complex rearrangements (19.2%) and substantially less reliance on microhomology (31%) than previously observed in benign copy-number variants (CNVs). We compared these results to experimentally generated DNA breakage-repair by sequencing seven transgenic animals, revealing extensive rearrangement of the transgene and host genome with similar complexity to human germline alterations. Inversion was the most common rearrangement, suggesting that a combined mechanism involving template switching and non-homologous repair mediates the formation of balanced complex rearrangements that are viable, stably replicated and transmitted unaltered to subsequent generations.

Original language	English
Journal	Nature Genetics
Volume	44
Issue number	4
DOIs	https://doi.org/10.1038/ng.2202
Publication status	Published - Apr 2012

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Chiang, C., Jacobsen, J. C., Ernst, C., Hanscom, C., Heilbut, A., Blumenthal, I., Mills, R. E., Kirby, A., Lindgren, A. M., Rudiger, S. R., McLaughlan, C. J., Bawden, C. S., Reid, S. J., Faull, R. L. M., Snell, R. G., Hall, I. M., Shen, Y., Ohsumi, T. K., Borowsky, M. L., ... Talkowski, M. E. (2012). Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration. Nature Genetics, 44(4). https://doi.org/10.1038/ng.2202

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title = "Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration.",

abstract = "We defined the genetic landscape of balanced chromosomal rearrangements at nucleotide resolution by sequencing 141 breakpoints from cytogenetically interpreted translocations and inversions. We confirm that the recently described phenomenon of 'chromothripsis' (massive chromosomal shattering and reorganization) is not unique to cancer cells but also occurs in the germline, where it can resolve to a relatively balanced state with frequent inversions. We detected a high incidence of complex rearrangements (19.2%) and substantially less reliance on microhomology (31%) than previously observed in benign copy-number variants (CNVs). We compared these results to experimentally generated DNA breakage-repair by sequencing seven transgenic animals, revealing extensive rearrangement of the transgene and host genome with similar complexity to human germline alterations. Inversion was the most common rearrangement, suggesting that a combined mechanism involving template switching and non-homologous repair mediates the formation of balanced complex rearrangements that are viable, stably replicated and transmitted unaltered to subsequent generations.",

author = "Colby Chiang and Jacobsen, {Jessie C} and Carl Ernst and Carrie Hanscom and Adrian Heilbut and Ian Blumenthal and Mills, {Ryan E} and Andrew Kirby and Lindgren, {Amelia M} and Rudiger, {Skye R} and McLaughlan, {Clive J} and Bawden, {C Simon} and Reid, {Suzanne J} and Faull, {Richard L M} and Snell, {Russell G} and Hall, {Ira M} and Yiping Shen and Ohsumi, {Toshiro K} and Borowsky, {Mark L} and Daly, {Mark J} and Charles Lee and Morton, {Cynthia C} and MacDonald, {Marcy E} and Gusella, {James F} and Talkowski, {Michael E}",

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year = "2012",

month = apr,

doi = "10.1038/ng.2202",

language = "English",

volume = "44",

journal = "Nature Genetics",

issn = "1061-4036",

publisher = "Nature Research",

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Chiang, C, Jacobsen, JC, Ernst, C, Hanscom, C, Heilbut, A, Blumenthal, I, Mills, RE, Kirby, A, Lindgren, AM, Rudiger, SR, McLaughlan, CJ, Bawden, CS, Reid, SJ, Faull, RLM, Snell, RG, Hall, IM, Shen, Y, Ohsumi, TK, Borowsky, ML, Daly, MJ, Lee, C, Morton, CC, MacDonald, ME, Gusella, JF & Talkowski, ME 2012, 'Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration.', Nature Genetics, vol. 44, no. 4. https://doi.org/10.1038/ng.2202

TY - JOUR

T1 - Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration.

AU - Chiang, Colby

AU - Jacobsen, Jessie C

AU - Ernst, Carl

AU - Hanscom, Carrie

AU - Heilbut, Adrian

AU - Blumenthal, Ian

AU - Mills, Ryan E

AU - Kirby, Andrew

AU - Lindgren, Amelia M

AU - Rudiger, Skye R

AU - McLaughlan, Clive J

AU - Bawden, C Simon

AU - Reid, Suzanne J

AU - Faull, Richard L M

AU - Snell, Russell G

AU - Hall, Ira M

AU - Shen, Yiping

AU - Ohsumi, Toshiro K

AU - Borowsky, Mark L

AU - Daly, Mark J

AU - Lee, Charles

AU - Morton, Cynthia C

AU - MacDonald, Marcy E

AU - Gusella, James F

AU - Talkowski, Michael E

N1 - F32 MH087123, NIMH NIH HHS, United StatesGM061354, NIGMS NIH HHS, United StatesHD065286, NICHD NIH HHS, United StatesMH087123, NIMH NIH HHS, United StatesNS16367, NINDS NIH HHS, United StatesNS32765, NINDS NIH HHS, United StatesP01 GM061354, NIGMS NIH HHS, United StatesP01 GM061354-01A1, NIGMS NIH HHS, United StatesP01 GM061354-02, NIGMS NIH HHS, United StatesP01 GM061354-03, NIGMS NIH HHS, United StatesP01 GM061354-04, NIGMS NIH HHS, United StatesP01 GM061354-05, NIGMS NIH HHS, United StatesP01 GM061354-06A2, NIGMS NIH HHS, United StatesP01 GM061354-07, NIGMS NIH HHS, United StatesP01 GM061354-08, NIGMS NIH HHS, United StatesP01 GM061354-09, NIGMS NIH HHS, United States, Canadian Institutes of Health Research, Canada

PY - 2012/4

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N2 - We defined the genetic landscape of balanced chromosomal rearrangements at nucleotide resolution by sequencing 141 breakpoints from cytogenetically interpreted translocations and inversions. We confirm that the recently described phenomenon of 'chromothripsis' (massive chromosomal shattering and reorganization) is not unique to cancer cells but also occurs in the germline, where it can resolve to a relatively balanced state with frequent inversions. We detected a high incidence of complex rearrangements (19.2%) and substantially less reliance on microhomology (31%) than previously observed in benign copy-number variants (CNVs). We compared these results to experimentally generated DNA breakage-repair by sequencing seven transgenic animals, revealing extensive rearrangement of the transgene and host genome with similar complexity to human germline alterations. Inversion was the most common rearrangement, suggesting that a combined mechanism involving template switching and non-homologous repair mediates the formation of balanced complex rearrangements that are viable, stably replicated and transmitted unaltered to subsequent generations.

AB - We defined the genetic landscape of balanced chromosomal rearrangements at nucleotide resolution by sequencing 141 breakpoints from cytogenetically interpreted translocations and inversions. We confirm that the recently described phenomenon of 'chromothripsis' (massive chromosomal shattering and reorganization) is not unique to cancer cells but also occurs in the germline, where it can resolve to a relatively balanced state with frequent inversions. We detected a high incidence of complex rearrangements (19.2%) and substantially less reliance on microhomology (31%) than previously observed in benign copy-number variants (CNVs). We compared these results to experimentally generated DNA breakage-repair by sequencing seven transgenic animals, revealing extensive rearrangement of the transgene and host genome with similar complexity to human germline alterations. Inversion was the most common rearrangement, suggesting that a combined mechanism involving template switching and non-homologous repair mediates the formation of balanced complex rearrangements that are viable, stably replicated and transmitted unaltered to subsequent generations.

U2 - 10.1038/ng.2202

DO - 10.1038/ng.2202

M3 - Article

C2 - 22388000

SN - 1061-4036

VL - 44

JO - Nature Genetics

JF - Nature Genetics

IS - 4

ER -

Complex reorganization and predominant non-homologous repair following chromosomal breakage in karyotypically balanced germline rearrangements and transgenic integration.

Abstract

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