4.6 Article

Screening and Identification of Key Common and Specific Genes and Their Prognostic Roles in Different Molecular Subtypes of Breast Cancer

期刊

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fmolb.2021.619110

关键词

breast cancer; molecular subtypes; prognosis; biomarkers; diagnosis-breast cancer

资金

  1. National Natural Science Foundation of China [81102030]
  2. Natural Science Foundation of Chongqing [cstc2020jcyj-msxmX0419]
  3. Military Medical Staff Innovation Plan of Army Medical University [XZ-2019-505-042]

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This study analyzed gene expression profiles of breast cancer patients, identifying key common and specific differentially expressed genes (DEGs) and conducting functional enrichment and signaling pathway analyses, laying the foundation for more refined molecular typing of breast cancer and new therapeutic targets.
Breast cancer is one of the most common cancers. Although the present molecular classification improves the treatment effect and prognosis of breast cancer, the heterogeneity of the molecular subtype remains very complex, and the applicability and effectiveness of treatment methods are still limited leading to poorer patient prognosis than expected. Further identification of more refined molecular typing based on gene expression profile will yield better understanding of the heterogeneity, improving treatment effects and prolonging prognosis of patients. Here, we downloaded the mRNA expression profiles and corresponding clinical data of patients with breast cancer from public databases and performed typical molecular typing using PAM50 (Prediction Analysis of Microarray 50) method. Comparative analyses were performed to screen the common and specific differentially expressed genes (DEGs) between cancer and corresponding para-cancerous tissues in each breast cancer subtype. The GO and KEGG analyses of the DEGs were performed to enrich the common and specific functional progress and signaling pathway involved in breast cancer subtypes. A total of 38 key common and specific DEGs were identified and selected based on the validated results, GO/KEGG enrichments, and the priority of expression, including four common DEGs and 34 specific DEGs in different subtypes. The prognostic value of these key common and specific DEGs was further analyzed to obtain useful potential markers in clinic. Finally, the potential roles and the specific prognostic values of the common and specific DEGs were speculated and summarized in total breast cancer and different subtype breast cancer based on the results of these analyses. The findings of our study provide the basis of more refined molecular typing of breast cancer, potential new therapeutic targets and prognostic markers for different breast cancer subtypes

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