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AJMB-Avicenna Journal of Medical Biotechnology. 2016; 8 (1): 36-41
in English | IMEMR | ID: emr-174774

ABSTRACT

Background: Piwi-interacting RNAs [piRNAs] are small non-coding RNAs [ncRNAs], with a length of about 24-32 nucleotides, which have been discovered recently. These ncRNAs play an important role in germline development, transposon silencing, epigenetic regulation, protecting the genome from invasive transposable elements, and the pathophysiology of diseases such as cancer. piRNA identification is challenging due to the lack of conserved piRNA sequences and structural elements


Methods: To detect piRNAs, an appropriate feature set, including 8 diverse feature groups to encode each RNA was applied. In addition, a Support Vector Machine [SVM] classifier was used with optimized parameters for RNA classification. According to the obtained results, the classification performance using the optimized feature subsets was much higher than the one in previously published studies


Results: Our results revealed 98% accuracy, Mathew' correlation coefficient of 98% and 99% specificity in discriminating piRNAs from the other RNAs. Also, the obtained results show that the proposed method outperforms its competitors


Conclusion: In this paper, a prediction method was proposed to identify piRNA in human. Also, 48 heterogeneous features [sequence and structural features] were used to encode RNAs. To assess the performance of the method, a benchmark dataset containing 515 piRNAs and 1206 types of other RNAs was constructed. Our method reached the accuracy of 99% on the benchmark dataset. Also, our analysis revealed that the structural features are the most contributing features in piRNA prediction

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