Scientific Reports (Jun 2021)

Clinicopathologic significance and race-specific prognostic association of MYB overexpression in ovarian cancer

  • Orlandric Miree,
  • Sanjeev Kumar Srivastava,
  • Mohammad Aslam Khan,
  • Fnu Sameeta,
  • Srijan Acharya,
  • Harrison Ndetan,
  • Karan Pal Singh,
  • Kate Louise Hertweck,
  • Santanu Dasgupta,
  • Luciana Madeira da Silva,
  • Rodney Paul Rocconi,
  • James Elliot Carter,
  • Seema Singh,
  • Ajay Pratap Singh

DOI
https://doi.org/10.1038/s41598-021-92352-3
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 8

Abstract

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Abstract Late diagnosis, unreliable prognostic assessment, and poorly-guided therapeutic planning result in dismal survival of ovarian cancer (OC) patients. Therefore, identifying novel functional biomarker(s) is highly desired for improved clinical management. MYB is an oncogenic transcription factor with emerging functional significance in OC. Here we examined its clinicopathologic significance by immunohistochemistry and TCGA/GTex data analyses. Aberrant MYB expression was detected in 94% of OC cases (n = 373), but not in the normal ovarian tissues (n = 23). MYB was overexpressed in all major epithelial OC histological subtypes exhibiting the highest incidence (~ 97%) and overall expression in serous and mucinous carcinomas. MYB expression correlated positively with tumor grades and stages. Moreover, MYB exhibited race-specific prognostic association. Moderate-to-high MYB levels were significantly associated with both poor overall- (p = 0.02) and progression-free (p = 0.02) survival in African American (AA), but not in the Caucasian American (CA) patients. Consistent with immunohistochemistry data, we observed significantly higher MYB transcripts in OC cases (n = 426) than normal ovary (n = 88). MYB transcripts were significantly higher in all epithelial OC subtypes, compared to normal, and its greater levels predicted poor survival in AA OC, but not CA OC, patients. Thus, MYB appears to be a useful clinical biomarker for prognostication, especially in AA patients.