4.4 Article

A CD24-p53 axis contributes to African American prostate cancer disparities

期刊

PROSTATE
卷 80, 期 8, 页码 609-618

出版社

WILEY
DOI: 10.1002/pros.23973

关键词

CD24; metastasis; prostate cancer; racial disparity; TP53

资金

  1. NCI NIH HHS [P30 CA013148, CA118948, U54 CA118638, U54 CA118948] Funding Source: Medline
  2. NIAID NIH HHS [R01 AI137255] Funding Source: Medline

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Background Using a functional analysis of prostate cancer cells, we found a CD24-dependent inactivation of mutant p53, but the clinical significance of this observation remained uncertain. Here, we validated these results with samples of human prostate cancer and explored the role of a CD24-p53 axis in racial disparities of prostate cancer. Methods Samples of formalin-fixed, paraffin-embedded prostate cancer from 141 European Americans (EAs) and 147 African Americans (AAs) in two independent sample cohorts were assessed for protein expression of CD24, mutant p53, mouse double minute 2 human homolog (MDM2), and cyclin dependent kinase inhibitor 2A (ARF) using immunohistochemical analyses. All samples were analyzed for TP53(R175H) and TP53(R273H). Results CD24, mutant p53, MDM2, and ARF proteins were expressed in 55%, 24%, 39%, and 68% of prostate cancer samples, respectively. CD24 and mutant p53 were present more frequently in late-stage and metastatic prostate cancer. The presence of CD24 was associated with a greater than fourfold risk of metastasis, which included lymph node and distant metastases. H score analysis showed positive correlations of CD24 expression with mutant p53 (r = .308, P < .001) and MDM2 (r = .227, P = .004). There was a negative correlation for CD24 with ARF (r = -.280, P < .001). A racial disparity was evident for CD24 (AAs/EAs: 64% vs 47%; P = .004) but not for mutant p53 (AA/EA: 28% vs 21%; P = .152). In 32 CD24(+)/mutant p53(+) cases, a TP53(R273H) mutation was found in five cases, but no TP53(R175H) mutation was found. Conclusion The CD24-p53 axis may contribute to aggressive and metastatic prostate cancers, especially those of AAs. This observation enhances understanding of the pathogenesis of prostate cancer and its associated racial disparities.

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