Amplified segment in the ‘Down Syndrome critical region’ on HSA21 shared between Down syndrome and euploid AML-M0 excludes RUNX1, ERG and ETS2
Author:
Publisher
Wiley
Subject
Hematology
Link
http://onlinelibrary.wiley.com/wol1/doi/10.1111/j.1365-2141.2011.08985.x/fullpdf
Reference15 articles.
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2. DYRK1A-dosage imbalance perturbs NRSF/REST levels, deregulating pluripotency and embryonic stem cell fate in Down syndrome;Canzonetta;American Journal of Human Genetics,2008
3. Genome gains at chromosome 21q21/22 segment leads to co-amplification of Down Syndrome Critical Regions and known oncogenes in a case of donor cell-derived acute myeloid leukaemia following allogeneic sex mismatched umbilical cord blood transplantation for chronic myeloid leukaemia;Castleton;British Journal of Haematology,2010
4. Loss-of-function JAK3 mutations in TMD and AMKL of Down syndrome;De Vita;British Journal of Haematology,2007
5. Trisomic dose of several chromosome 21 genes perturbs haematopoietic stem and progenitor cell differentiation in Down’s syndrome;De Vita;Oncogene,2010
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1. Establishment and verification of a TME prognosis scoring model based on the acute myeloid leukemia single-cell transcriptome;Scientific Reports;2024-08-27
2. Profile of down syndrome–associated malignancies: Epidemiology, clinical features and therapeutic aspects;Pediatric Hematology Oncology Journal;2021-06
3. Searching for a signature involving 10 genes to predict the survival of patients with acute myelocytic leukemia through a combined multi-omics analysis;PeerJ;2020-06-25
4. RUNX1 deletion/amplification in therapy-related acute myeloid leukemia: A case report and review of the literature;Cancer Genetics;2019-10
5. Transient leukemia of Down syndrome;Critical Reviews in Clinical Laboratory Sciences;2019-05-19
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