Deregulation of c-myc by Translocation of the α-Locus of the T-Cell Receptor in T-Cell Leukemias

J Erikson, L Finger, L Sun, A Ar-Rushdi, K Nishikura… - Science, 1986 - science.org
J Erikson, L Finger, L Sun, A Ar-Rushdi, K Nishikura, J Minowada, J Finan, BS Emanuel
Science, 1986science.org
Two human T-cell leukemias carrying at (8; 14)(q24; q11) chromosome translocation were
studied for rearrangements and expression of the c-myc oncogene. For one leukemia,
rearrangement was detected in a region immediately distal (3′) to the c-myc locus; no
rearrangements of c-myc were observed in the second case (DeF). However, studies with
hybrids between human and mouse leukemic T cells indicated that in the leukemic cells of
DeF, the breakpoint in chromosome 14 occurred between genes for the variable (Vα) and …
Two human T-cell leukemias carrying a t(8;14)(q24;q11) chromosome translocation were studied for rearrangements and expression of the c-myc oncogene. For one leukemia, rearrangement was detected in a region immediately distal (3′) to the c-myc locus; no rearrangements of c-myc were observed in the second case (DeF). However, studies with hybrids between human and mouse leukemic T cells indicated that in the leukemic cells of DeF, the breakpoint in chromosome 14 occurred between genes for the variable (Vα) and the constant (Cα) regions for the α chain of the T-cell receptor. The Cα locus had translocated to a region more than 38 kilobases 3′ to the involved c-myc oncogene. Since human c-myc transcripts were expressed only in hybrids carrying the 8q+ chromosome but not in hybrids containing the normal chromosome 8, it is concluded that the translocation of the Cα locus 3′ to the c-myc oncogene can result in its transcriptional deregulation.
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