Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes

Jan J. Molenaar; Jan Koster; Danny A. Zwijnenburg; Peter van Sluis; Linda J. Valentijn; Ida van der Ploeg; Mohamed Hamdi; Johan van Nes; Bart A. Westerman; Jennemiek van Arkel; Marli E. Ebus; Franciska Haneveld; Arjan Lakeman; Linda Schild; Piet Molenaar; Peter Stroeken; Max M. van Noesel; Ingrid Ora; Evan E. Santo; Huib N. Caron; Ellen M. Westerhout; Rogier Versteeg

doi:10.1038/nature10910

Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes

Jan J. Molenaar
, Jan Koster
, Danny A. Zwijnenburg
, Peter van Sluis
, Linda J. Valentijn
, Ida van der Ploeg
, Mohamed Hamdi
, Johan van Nes
, Bart A. Westerman
, Jennemiek van Arkel
, Marli E. Ebus
, Franciska Haneveld
, Arjan Lakeman
, Linda Schild
, Piet Molenaar
, Peter Stroeken
, Max M. van Noesel
, Ingrid Ora
, Evan E. Santo
, Huib N. Caron

Ellen M. Westerhout, Rogier Versteeg

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

Abstract

Neuroblastomais a childhood tumour of the peripheral sympathetic nervous system. The pathogenesis has for a long time been quite enigmatic, as only very few gene defects were identified in this often lethal tumour(1). Frequently detected gene alterations are limited to MYCN amplification (20%) and ALK activations (7%)(2-5). Here we present a whole-genome sequence analysis of 87 neuroblastoma of all stages. Few recurrent amino-acid-changing mutations were found. In contrast, analysis of structural defects identified a local shredding of chromosomes, known as chromothripsis, in 18% of high-stage neuroblastoma(6). These tumours are associated with a poor outcome. Structural alterations recurrently affected ODZ3, PTPRD and CSMD1, which are involved in neuronal growth cone stabilization(7-9). In addition, ATRX, TIAM1 and a series of regulators of the Rac/Rho pathway were mutated, further implicating defects in neuritogenesis in neuroblastoma. Most tumours with defects in these genes were aggressive high-stage neuroblastomas, but did not carry MYCN amplifications. The genomic landscape of neuroblastoma therefore reveals two novel molecular defects, chromothripsis and neuritogenesis gene alterations, which frequently occur in high-risk tumours

Original language	English
Pages (from-to)	589-U107
Journal	Nature
Volume	483
Issue number	7391
DOIs	https://doi.org/10.1038/nature10910
Publication status	Published - 2012

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Molenaar, J. J., Koster, J., Zwijnenburg, D. A., van Sluis, P., Valentijn, L. J., van der Ploeg, I., Hamdi, M., van Nes, J., Westerman, B. A., van Arkel, J., Ebus, M. E., Haneveld, F., Lakeman, A., Schild, L., Molenaar, P., Stroeken, P., van Noesel, M. M., Ora, I., Santo, E. E., ... Versteeg, R. (2012). Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes. Nature, 483(7391), 589-U107. https://doi.org/10.1038/nature10910

@article{33c468ec125f4cd5a82d7fa4411eb41b,

title = "Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes",

abstract = "Neuroblastomais a childhood tumour of the peripheral sympathetic nervous system. The pathogenesis has for a long time been quite enigmatic, as only very few gene defects were identified in this often lethal tumour(1). Frequently detected gene alterations are limited to MYCN amplification (20\%) and ALK activations (7\%)(2-5). Here we present a whole-genome sequence analysis of 87 neuroblastoma of all stages. Few recurrent amino-acid-changing mutations were found. In contrast, analysis of structural defects identified a local shredding of chromosomes, known as chromothripsis, in 18\% of high-stage neuroblastoma(6). These tumours are associated with a poor outcome. Structural alterations recurrently affected ODZ3, PTPRD and CSMD1, which are involved in neuronal growth cone stabilization(7-9). In addition, ATRX, TIAM1 and a series of regulators of the Rac/Rho pathway were mutated, further implicating defects in neuritogenesis in neuroblastoma. Most tumours with defects in these genes were aggressive high-stage neuroblastomas, but did not carry MYCN amplifications. The genomic landscape of neuroblastoma therefore reveals two novel molecular defects, chromothripsis and neuritogenesis gene alterations, which frequently occur in high-risk tumours",

author = "Molenaar, \{Jan J.\} and Jan Koster and Zwijnenburg, \{Danny A.\} and \{van Sluis\}, Peter and Valentijn, \{Linda J.\} and \{van der Ploeg\}, Ida and Mohamed Hamdi and \{van Nes\}, Johan and Westerman, \{Bart A.\} and \{van Arkel\}, Jennemiek and Ebus, \{Marli E.\} and Franciska Haneveld and Arjan Lakeman and Linda Schild and Piet Molenaar and Peter Stroeken and \{van Noesel\}, \{Max M.\} and Ingrid Ora and Santo, \{Evan E.\} and Caron, \{Huib N.\} and Westerhout, \{Ellen M.\} and Rogier Versteeg",

year = "2012",

doi = "10.1038/nature10910",

language = "English",

volume = "483",

pages = "589--U107",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Publishing Group",

number = "7391",

}

Molenaar, JJ, Koster, J , Zwijnenburg, DA, van Sluis, P, Valentijn, LJ, van der Ploeg, I, Hamdi, M, van Nes, J, Westerman, BA, van Arkel, J, Ebus, ME, Haneveld, F , Lakeman, A, Schild, L, Molenaar, P, Stroeken, P, van Noesel, MM, Ora, I, Santo, EE, Caron, HN, Westerhout, EM & Versteeg, R 2012, 'Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes', Nature, vol. 483, no. 7391, pp. 589-U107. https://doi.org/10.1038/nature10910

TY - JOUR

T1 - Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes

AU - Molenaar, Jan J.

AU - Koster, Jan

AU - Zwijnenburg, Danny A.

AU - van Sluis, Peter

AU - Valentijn, Linda J.

AU - van der Ploeg, Ida

AU - Hamdi, Mohamed

AU - van Nes, Johan

AU - Westerman, Bart A.

AU - van Arkel, Jennemiek

AU - Ebus, Marli E.

AU - Haneveld, Franciska

AU - Lakeman, Arjan

AU - Schild, Linda

AU - Molenaar, Piet

AU - Stroeken, Peter

AU - van Noesel, Max M.

AU - Ora, Ingrid

AU - Santo, Evan E.

AU - Caron, Huib N.

AU - Westerhout, Ellen M.

AU - Versteeg, Rogier

PY - 2012

Y1 - 2012

N2 - Neuroblastomais a childhood tumour of the peripheral sympathetic nervous system. The pathogenesis has for a long time been quite enigmatic, as only very few gene defects were identified in this often lethal tumour(1). Frequently detected gene alterations are limited to MYCN amplification (20%) and ALK activations (7%)(2-5). Here we present a whole-genome sequence analysis of 87 neuroblastoma of all stages. Few recurrent amino-acid-changing mutations were found. In contrast, analysis of structural defects identified a local shredding of chromosomes, known as chromothripsis, in 18% of high-stage neuroblastoma(6). These tumours are associated with a poor outcome. Structural alterations recurrently affected ODZ3, PTPRD and CSMD1, which are involved in neuronal growth cone stabilization(7-9). In addition, ATRX, TIAM1 and a series of regulators of the Rac/Rho pathway were mutated, further implicating defects in neuritogenesis in neuroblastoma. Most tumours with defects in these genes were aggressive high-stage neuroblastomas, but did not carry MYCN amplifications. The genomic landscape of neuroblastoma therefore reveals two novel molecular defects, chromothripsis and neuritogenesis gene alterations, which frequently occur in high-risk tumours

AB - Neuroblastomais a childhood tumour of the peripheral sympathetic nervous system. The pathogenesis has for a long time been quite enigmatic, as only very few gene defects were identified in this often lethal tumour(1). Frequently detected gene alterations are limited to MYCN amplification (20%) and ALK activations (7%)(2-5). Here we present a whole-genome sequence analysis of 87 neuroblastoma of all stages. Few recurrent amino-acid-changing mutations were found. In contrast, analysis of structural defects identified a local shredding of chromosomes, known as chromothripsis, in 18% of high-stage neuroblastoma(6). These tumours are associated with a poor outcome. Structural alterations recurrently affected ODZ3, PTPRD and CSMD1, which are involved in neuronal growth cone stabilization(7-9). In addition, ATRX, TIAM1 and a series of regulators of the Rac/Rho pathway were mutated, further implicating defects in neuritogenesis in neuroblastoma. Most tumours with defects in these genes were aggressive high-stage neuroblastomas, but did not carry MYCN amplifications. The genomic landscape of neuroblastoma therefore reveals two novel molecular defects, chromothripsis and neuritogenesis gene alterations, which frequently occur in high-risk tumours

U2 - 10.1038/nature10910

DO - 10.1038/nature10910

M3 - Article

C2 - 22367537

SN - 0028-0836

VL - 483

SP - 589-U107

JO - Nature

JF - Nature

IS - 7391

ER -

Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes

Abstract

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