To study the genetic basis of tumor progression, we have screened 37 hormone-refractory prostate carcinomas for genetic changes by comparative genomic hybridization (CGH). All recurrent tumors showed genetic aberrations , with a mean total number of changes per tumor of 11.4 (range , 3 to 23). The most common genetic aberrations were losses of 8p (72.5%) , 13q (50%) , 1p (50%) , 22 (45%) , 19 (45%), 10q (42.5%) , and 16q (42.5%) and gains of 8q (72.5%), 7q (40%) , Xq (32.5%) , and 18q (32.5%). The CGH results were further validated with fluorescence in situ hybridization (FISH) using probes for pericentromeric regions of chromosomes 7 , 8 , and 18 as well as probes for caveolin (7q31) , c-myc (8q24) , and bcl-2 (18q21.3). In addition , the samples had previously been analyzed for androgen receptor gene copy number. CGH and FISH results were concordant in 78% of cases. Seventeen of twenty-two tumors showed an increased copy number of c-myc by FISH. However, only 5 of 17 (29%) of the cases showed high-level (more than threefold) amplification. Both CGH and FISH findings suggested that in most of the cases 8q gain involves the whole q-arm of the chromosome. Four of seventeen (24%) cases showed increased copy number of bcl-2 by FISH; however , no high-level amplifications were found. To evaluate the clonal relationship of the primary and recurrent tumors, six primary-recurrent tumor pairs from the same patients were studied by CGH. In three of six cases (50%) , the recurrent tumor had more than one-half of the aberrations found in the corresponding primary tumor , indicating a close clonal relationship. In the rest of the cases , such a linear clonal relationship was less evident. Altogether , these results suggest that recurrent prostate carcinomas are genetically unstable. The resulting heterogeneity may well underlie the poor responsiveness of hormone-refractory tumors to treatment. (Am J Pathol 1998, 153:141-148)Prostate cancer is the most common malignancy among men in many Western industrialized countries. Despite the improved early diagnosis of prostate cancer, approximately one-third of the patients are still diagnosed at a clinically advanced stage.
