BRIP1 overexpression is correlated with clinical features and survival outcome of luminal breast cancer subtypes
| المؤلف | Gupta I. |
| المؤلف | Ouhtit A. |
| المؤلف | Al-Ajmi A. |
| المؤلف | Rizvi S.G.A. |
| المؤلف | Al-Riyami H. |
| المؤلف | Al-Riyami M. |
| المؤلف | Tamimi Y. |
| تاريخ الإتاحة | 2020-04-07T11:46:17Z |
| تاريخ النشر | 2018 |
| اسم المنشور | Endocrine Connections |
| المصدر | Scopus |
| الرقم المعياري الدولي للكتاب | 20493614 |
| الملخص | In Oman, breast cancer is most common, representing approximately more than 25% of all cancers in women. Relatively younger populations of patients (25-40 years) present surprisingly with an aggressive phenotype and advanced tumor stages. In this study, we investigated differential gene expressions in Luminal A, Luminal B, triple-negative and Her2+ breast cancer subtypes and compared data to benign tumor samples. We identified a potential candidate gene BRIP1, showing differential expression in the four breast cancer subtypes examined, suggesting that BRIP1 has the profile of a useful diagnostic marker, suitable for targeted therapeutic intervention. RT-qPCR and Western blotting analysis showed higher BRIP1 expression in luminal samples as compared to triple-negative subtype patient's samples. We further screened BRIP1 for eventual mutations/SNPs/deletions by sequencing the entire coding region. Four previously identified polymorphisms were detected, one within the 5'-UTR region (c.141-64G > A) and three in the BRCA-binding domain (c.2755T > C, c.2647G > A and c.3411T > C). Kaplan-Meier analysis revealed that patients with overexpression of BRIP1 displayed a poor survival rate (P < 0.05). BRIP1 has a dual function of an oncogene and a tumor suppressor gene in addition to its role as a potential biomarker to predict survival and prognosis. Data obtained in this study suggest that BRIP1 can plausibly have an oncogenic role in sporadic cancers. |
| اللغة | en |
| الناشر | BioScientifica Ltd. |
| الموضوع | Biomarkers Breast cancer BRIP1 Oncogene Overexpression |
| النوع | Article |
| الصفحات | 65-77 |
| رقم العدد | 1 |
| رقم المجلد | 7 |
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