22 april 2017: Lees ook dit artikel: 

https://kanker-actueel.nl/NL/13-cis-retinoinezuur-aanvullend-gegeven-naast-en-na-chemo-en-myeloablatieve-therapie-abmt-verbetert-de-langjarige-overall-overleving-van-kinderen-met-een-neuroblastoom-graad-3-en-4-tot-100-procent-op-5-jaars-meting.html

6 juli 2012: Duitse en Belgische onderzoekers hebben aan de hand van studies met muizen aangetoond dat een mutatie van het zogeheten ALK gen neuroblastomen worden gevomd. Neuroblastoom is een vorm van kanker die vooral bij kinderen voorkomt. Maar uit de studie bleek ook dat longkanker en lymfomen een relatie hebben met dit ALK gen. De onderzoekers zeggen dat met een moleculaire aanpak deze ALK gen mutatie zou kunnen worden geremd of wellicht voorkomen. Hier het abstract van de dierstudie:

Activating mutation within the ALK kinase domain is sufficient to induce neuroblastoma development, and ALK inhibitors show promise for treating human neuroblastomas harboring ALK mutations.

Sci Transl Med
Vol. 4, Issue 141, p. 141ra91
Sci. Transl. Med. DOI: 10.1126/scitranslmed.3003967
  • Research Article

Neuroblastoma

Targeted Expression of Mutated ALK Induces Neuroblastoma in Transgenic Mice

  1. Johannes H. Schulte2,

+ Author Affiliations

  1. 1Institute of Pathology, University Hospital Cologne, Kerpenerstrasse 62, 50924 Cologne, Germany.
  2. 2Department of Pediatric Oncology and Hematology, University Children’s Hospital Essen, Hufelandstrasse 55, 45147 Essen, Germany.
  3. 3Center for Medical Genetics Ghent, Ghent University Hospital, De Pintelaan 185, 9000 Ghent, Belgium.
  4. 4Max Planck Institute for Neurological Research with Klaus-Joachim-Zülch Laboratories of the Max Planck Society and the Medical Faculty of the University of Cologne, Gleueler Strasse 50, 50931 Köln, Germany.
  5. 5Institute of Translational Genomics, University of Cologne, Weyertal 155b, 50931 Cologne, Germany.

+ Author Notes

  • * These authors contributed equally to this work.

  1. To whom correspondence should be addressed. E-mail: johannes.schulte@uni-due.de

Abstract

Activating anaplastic lymphoma kinase (ALK) mutations were recently detected in most familial and 10% of sporadic neuroblastomas. However, the role of mutated ALK in tumorigenesis remains elusive. We demonstrate that targeted expression of the most frequent and aggressive variant, ALKF1174L, is tumorigenic in mice. Tumors resembled human neuroblastomas in morphology, metastasis pattern, gene expression, and the presence of neurosecretory vesicles as well as synaptic structures. This ALK-driven neuroblastoma mouse model precisely recapitulated the genetic spectrum of the disease. Chromosomal aberrations were syntenic to those in human neuroblastoma, including 17q gain and MYCN oncogene amplification. Targeted ALKF1174L and MYCN coexpression revealed a strong synergism in inducing neuroblastoma with minimal chromosomal aberrations, suggesting that fewer secondary hits are required for tumor induction if both oncoproteins are targeted. Treatment of ALKF1174L transgenic mice with the ALK inhibitor TAE-684 induced complete tumor regression, indicating that tumor cells were addicted to ALKF1174L activity. We conclude that an activating mutation within the ALK kinase domain is sufficient to induce neuroblastoma development, and ALK inhibitors show promise for treating human neuroblastomas harboring ALK mutations.

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ALK gen, neuroblastoom


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