Genomic rearrangements of the c-myc proto-oncogene in human malignant lymphomas

Chromosome translocations involving 8q24, the band to which c-myc has been mapped (Dalla-Favera et a/., 1982). are a uniform finding in Burkitt's lymphoma (Bernheim et a/., 1981). However, in only a minority of the tumors is the rearrangement of the cmyc locus sufficiently close to the gene to be de

Amplification without structural rearrangements of the c-myc proto-oncogene was found in 14 of 44 primary cervical neoplasms. There was no apparent correlation with stage of disease or degree of cellular differentiation. The prognostic significance of c-myc amplification cannot be determined from th

## Abstract The human large B‐cell lymphoma cell line RC‐K8 has a rearranged __REL__ locus that is transcribed into a chimeric mRNA, termed __REL‐NRG__ (__N__on‐__R__el __G__ene). By analyzing the recently completed human genome sequence, we have found that the normal __REL__ and __NRG__ loci are s

## Abstract Total cellular polyadenylated RNA from a variety of fresh human lymphoma and leukemia cells, characterized by histopathology and certain cell surface markers, was analyzed for the expression of three distinct cellular oncogenes (__c‐oncgenes__), __c‐erbB, c‐myc__ and __c‐myb__ by dotblo

Molecular probes for cellular proto-oncogenes have recently been extensively used in order to search for functional and structural alterations in tumor tissues. Variable, and sometimes contradictory, results have been obtained regarding the frequency and clinical significance of amplification of the