Prognostic Values of Gene Copy Number Alterations in Prostate Cancer

被引:4
|
作者
Alfahed, Abdulaziz [1 ]
Ebili, Henry Okuchukwu [2 ]
Almoammar, Nasser Eissa [1 ]
Alasiri, Glowi [3 ]
AlKhamees, Osama A. [4 ]
Aldali, Jehad A. [5 ]
Al Othaim, Ayoub [6 ]
Hakami, Zaki H. [7 ]
Abdulwahed, Abdulhadi M. [8 ]
Waggiallah, Hisham Ali [1 ]
机构
[1] Prince Sattam Bin Abdulaziz Univ, Coll Appl Med Sci, Dept Med Lab Sci, Alkharj 11942, Saudi Arabia
[2] Olabisi Onabanjo Univ, Dept Morbid Anat & Histopathol, PMB 2002, Ago Iwoye, Nigeria
[3] Imam Mohammad Ibn Saud Univ, Coll Med, Dept Biochem, Riyadh 13317, Saudi Arabia
[4] Imam Mohammad Ibn Saud Islamic Univ IMSIU, Coll Med, Dept Pharmacol, Riyadh 13317, Saudi Arabia
[5] Imam Mohammad Ibn Saud Islamic Univ IMSIU, Coll Med, Dept Pathol, Riyadh 13317, Saudi Arabia
[6] Majmaah Univ, Coll Appl Med Sci, Dept Med Labs, Al Majmaah 11952, Saudi Arabia
[7] Jazan Univ, Coll Appl Med Sci, Med Lab Technol Dept, Jazan 82817, Saudi Arabia
[8] King Saud Univ, Coll Appl Med Sci, Dept Clin Lab Sci, Riyadh 11362, Saudi Arabia
关键词
prostate cancer; gene copy number alterations; localised disease; advanced disease; risk stratification; progression-free survival; PTEN GENOMIC DELETION; FINGER PROTEIN 267; LYMPHOBLASTIC LEUKEMIA; ERG; PROGRESSION; METASTASIS; EXPRESSION; CARCINOMA; OVEREXPRESSION; AMPLIFICATION;
D O I
10.3390/genes14050956
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Whilst risk prediction for individual prostate cancer (PCa) cases is of a high priority, the current risk stratification indices for PCa management have severe limitations. This study aimed to identify gene copy number alterations (CNAs) with prognostic values and to determine if any combination of gene CNAs could have risk stratification potentials. Clinical and genomic data of 500 PCa cases from the Cancer Genome Atlas stable were retrieved from the Genomic Data Commons and cBioPortal databases. The CNA statuses of a total of 52 genetic markers, including 21 novel markers and 31 previously identified potential prognostic markers, were tested for prognostic significance. The CNA statuses of a total of 51/52 genetic markers were significantly associated with advanced disease at an odds ratio threshold of =1.5 or =0.667. Moreover, a Kaplan-Meier test identified 27/52 marker CNAs which correlated with disease progression. A Cox Regression analysis showed that the amplification of MIR602 and deletions of MIR602, ZNF267, MROH1, PARP8, and HCN1 correlated with a progression-free survival independent of the disease stage and Gleason prognostic group grade. Furthermore, a binary logistic regression analysis identified twenty-two panels of markers with risk stratification potentials. The best model of 7/52 genetic CNAs, which included the SPOP alteration, SPP1 alteration, CCND1 amplification, PTEN deletion, CDKN1B deletion, PARP8 deletion, and NKX3.1 deletion, stratified the PCa cases into a localised and advanced disease with an accuracy of 70.0%, sensitivity of 85.4%, specificity of 44.9%, positive predictive value of 71.67%, and negative predictive value of 65.35%. This study validated prognostic gene level CNAs identified in previous studies, as well as identified new genetic markers with CNAs that could potentially impact risk stratification in PCa.
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页数:14
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