Computational and Experimental Tools of miRNAs in Cancer
Publish place: Middle East Journal of Cancer، Vol: 11، Issue: 4
Publish Year: 1399
نوع سند: مقاله ژورنالی
زبان: English
View: 50
This Paper With 9 Page And PDF Format Ready To Download
- Certificate
- من نویسنده این مقاله هستم
استخراج به نرم افزارهای پژوهشی:
شناسه ملی سند علمی:
JR_MISJ-11-4_001
تاریخ نمایه سازی: 25 آبان 1402
Abstract:
MicroRNAs (miRNAs) are short non-protein coding and single-stranded small RNA molecules with a critical role in the regulation of gene expression. These molecules are crucial regulatory elements in diverse biological processes such as apoptosis, development, and progression. miRNA genes have been associated with various human diseases, particularly cancer, and considered as a new biomarker. After the discovery of miRNAs, many researches have focused on identifying and characterizing miRNA genes in cancer. The various expression levels of miRNAs between cancer cells and normal cells are very crucial to diagnosis, prognosis, and treatment of many cancers. Many computational and experimental tools have been employed to characterize miRNAs. However, there exist some challenges in identifying miRNA using both computational and experimental tools due to miRNA features. The present review briefly introduced miRNA biology and certain computational and experimental tools for identifying and profiling miRNAs in cancer. Furthermore, we presented the advantages and challenges of these tools.
Keywords:
Authors
Esen Çakmak
Kirşehir Ahi Evran University, Mucur Health Services Vocational School, Department of Medical Services and Techniques, Medical Laboratory Techniques Program, Mucur Campus, Kirşehir, Turkey
مراجع و منابع این Paper:
لیست زیر مراجع و منابع استفاده شده در این Paper را نمایش می دهد. این مراجع به صورت کاملا ماشینی و بر اساس هوش مصنوعی استخراج شده اند و لذا ممکن است دارای اشکالاتی باشند که به مرور زمان دقت استخراج این محتوا افزایش می یابد. مراجعی که مقالات مربوط به آنها در سیویلیکا نمایه شده و پیدا شده اند، به خود Paper لینک شده اند :