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Atlas of Genetics and Cytogenetics in Oncology and Haematology INIST-CNRS OPEN ACCESS JOURNAL Leukaemia Section Short Communication t(X;7)(q22;q34) IRS4/TCRB Kristina Karrman Department of Clinical Genetics, Lund University Hospital, SE-221 85 Lund, Sweden (KK) Published in Atlas Database: June 2012 Online updated version : http://AtlasGeneticsOncology.org/Anomalies/t0X07q22q34ID1610.html DOI: 10.4267/2042/48369 This work is licensed under a Creative Commons Attribution-Noncommercial-No Derivative Works 2.0 France Licence. © 2012 Atlas of Genetics and Cytogenetics in Oncology and Haematology positive for CD2, CD7 and CD3 but negative for CD4 and CD8. A diagnose of T-cell acute lymphoblastic leukaemia was made. Clinics and pathology Cytology Lymphoblasts; positive for CD2/CD3/CD7, negative for CD4/CD8. Cytogenetics Cytogenetics morphological t(X;7)(q22;q34) Cytogenetics molecular Partial karyotype of the t(X;7)(q22;q34) showing the normal chromosome 7 (chr(7)), the der(7)t(X;7) and the der(X)t(X;7). Rearrangement of the TRB@ and IRS4 loci was detected by FISH. Probes used for detecting TRB@ rearrangement: RP11-1220K2 and RP11-556I13. Probes used for detecting IRS4 rearrangement: RP11815E21 and RP11-105F23. RQ-PCR and Western blot analysis confirmed overexpression of IRS4 at the gene and protein level. Disease T-cell acute lymphoblastic leukemia Epidemiology Very rare. Clinics Additional anomalies A 12-year-old boy presented with a white blood cell count of 130 x 109/l and haemoglobin of 97g/l. The bone marrow was dominated by lymphoblasts Deletion of 6q, STIL/TAL1 fusion and NOTCH1 mutation. The reciprocal nature of the t(X;7) was confirmed with metaphase FISH using the Poseidon whole chromosome probes (Kreatech Diagnostics, Amsterdam, The Netherlands) for chromosomes 7 (green) and X (red). Atlas Genet Cytogenet Oncol Haematol. 2012; 16(12) 927 t(X;7)(q22;q34) IRS4/TCRB Karrman K Genes involved and proteins TRB@/TCRB IRS4 Result of the chromosomal anomaly Location Xq22 Note The IRS family includes IRS1-4 which play a central role in maintaining basic cellular functions, e.g., growth and metabolism. They act as mediators between multiple growth factor receptors that possess tyrosine kinase activity, such as the insulin and insulin growth factor receptors, and a complex network of intracellular signalling molecules, resulting in activation of, for example, the PI3K and RAS/ERK pathways and subsequent transcription of target genes. Relatively little is known about the tumorigenic potential of the IRS proteins. Expression of IRS1, IRS2 or IRS4 in the 32D haematopoietic cell line leads to proliferation of the myeloid progenitor cells and expression of activated IRS4 has recently been demonstrated in the human hepatoblastoma cell line HepG2, with inhibition of IRS4 resulting in diminished growth. Atlas Genet Cytogenet Oncol Haematol. 2012; 16(12) Hybrid gene Note The translocation does not result in a fusion gene. The t(X;7) results in juxtaposition of the TRB@ to the IRS4 leading to dysregulation of IRS4. References Karrman K, Kjeldsen E, Lassen C, Isaksson M, Davidsson J, Andersson A, Hasle H, Fioretos T, Johansson B. The t(X;7)(q22;q34) in paediatric T-cell acute lymphoblastic leukaemia results in overexpression of the insulin receptor substrate 4 gene through illegitimate recombination with the Tcell receptor beta locus. Br J Haematol. 2009 Feb;144(4):54651 This article should be referenced as such: Karrman K. t(X;7)(q22;q34) IRS4/TCRB. Atlas Cytogenet Oncol Haematol. 2012; 16(12):927-928. 928 Genet