Correlation of non-random chromosomal aberrations in lymphocytes of prostate cancer patients with specific clinical parameters.

  • Authors:
    • M Ozen
    • V L Hopwood
    • M D Balbay
    • D A Johnston
    • R J Babaian
    • C J Logothetis
    • A C von Eschenbach
    • S Pathak
  • View Affiliations

  • Published online on: July 1, 2000     https://doi.org/10.3892/ijo.17.1.113
  • Pages: 113-120
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Abstract

The purpose of this research was to correlate non-random chromosomal aberrations in the peripheral blood lymphocytes (PBLs) of prostate cancer patients with specific clinical parameters. Peripheral blood samples were analyzed from 59 informative prostate cancer patients. Non-random chromosomal alterations detected in the PBLs and their correlation with any specific clinical parameters were analyzed statistically. A comparison was made between specific chromosomal abnormalities in the patients having an early (<65 years) or late (> or =65 years) age at disease onset, low-grade (Gleason grade <7) or high-grade (Gleason grade > or =7) tumors, a low (<10 ng/ml) or high (> or =10 ng/ml) prostate-specific antigen (PSA) level, and androgen-sensitive or -insensitive disease. In examining the specific chromosomal breakpoints, the regions 1p13, 2q21, 3p21, 4q13, 5q31, 6p21, 7p15, 7p13, 7q32, 10p11, 10q26, 11p15, 11p11, 14q12, and 16q12 showed breaks in at least four cases. Chromosome 15 (P=0. 045) was significantly altered in patients having a PSA value greater than or equal to 10, while it (P=0.017) and chromosome 19 (P=0.036) were significantly altered in patients having a PSA value greater than or equal to 20. In addition, chromosomes 5 (P=0.032), 8 (P=0.020), 16 (P=0.009), and 20 (P=0.047) were significantly altered in patients having a Gleason grade greater than 7. Also, chromosomes 2 (P=0.020) and 3 (P=0.044) were significantly altered in patients who had early disease onset. Additionally, chromosome 10 (P=0.041) was significantly altered in patients having metastasis, and chromosomes 4 (P=0.006) and 7 (P=0.028) were significantly altered in patients having androgen-insensitive disease. In spite of the small subset of patients, chromosome 8 (p=0.003) was significantly altered in patients having small cell carcinoma of the prostate. From these results we conclude that non-random chromosomal aberrations present in PBLs of prostate cancer patients can be correlated with specific clinical parameters. These correlations can be used to identify a prostate cancer patient's risk response to therapy.

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Jul 2000
Volume 17 Issue 1

Print ISSN: 1019-6439
Online ISSN:1791-2423

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Spandidos Publications style
Ozen M, Hopwood V, Balbay M, Johnston D, Babaian R, Logothetis C, von Eschenbach A and Pathak S: Correlation of non-random chromosomal aberrations in lymphocytes of prostate cancer patients with specific clinical parameters.. Int J Oncol 17: 113-120, 2000.
APA
Ozen, M., Hopwood, V., Balbay, M., Johnston, D., Babaian, R., Logothetis, C. ... Pathak, S. (2000). Correlation of non-random chromosomal aberrations in lymphocytes of prostate cancer patients with specific clinical parameters.. International Journal of Oncology, 17, 113-120. https://doi.org/10.3892/ijo.17.1.113
MLA
Ozen, M., Hopwood, V., Balbay, M., Johnston, D., Babaian, R., Logothetis, C., von Eschenbach, A., Pathak, S."Correlation of non-random chromosomal aberrations in lymphocytes of prostate cancer patients with specific clinical parameters.". International Journal of Oncology 17.1 (2000): 113-120.
Chicago
Ozen, M., Hopwood, V., Balbay, M., Johnston, D., Babaian, R., Logothetis, C., von Eschenbach, A., Pathak, S."Correlation of non-random chromosomal aberrations in lymphocytes of prostate cancer patients with specific clinical parameters.". International Journal of Oncology 17, no. 1 (2000): 113-120. https://doi.org/10.3892/ijo.17.1.113