RESUMO
Alzheimer's disease (AD) is a challenging neurodegenerative condition, necessitating early diagnosis and intervention. This research leverages machine learning (ML) and graph theory metrics, derived from resting-state functional magnetic resonance imaging (rs-fMRI) data to predict AD. Using Southwest University Adult Lifespan Dataset (SALD, age 21-76 years) and the Open Access Series of Imaging Studies (OASIS, age 64-95 years) dataset, containing 112 participants, various ML models were developed for the purpose of AD prediction. The study identifies key features for a comprehensive understanding of brain network topology and functional connectivity in AD. Through a 5-fold cross-validation, all models demonstrate substantial predictive capabilities (accuracy in 82-92% range), with the support vector machine model standing out as the best having an accuracy of 92%. Present study suggests that top 13 regions, identified based on most important discriminating features, have lost significant connections with thalamus. The functional connection strengths were consistently declined for substantia nigra, pars reticulata, substantia nigra, pars compacta, and nucleus accumbens among AD subjects as compared to healthy adults and aging individuals. The present finding corroborate with the earlier studies, employing various neuroimagining techniques. This research signifies the translational potential of a comprehensive approach integrating ML, graph theory and rs-fMRI analysis in AD prediction, offering potential biomarker for more accurate diagnostics and early prediction of AD.
RESUMO
This paper advances the self-attention mechanism in the standard transformer network specific to the modeling of the protein sequences. We introduce a novel context-window based scaled self-attention mechanism for processing protein sequences that is based on the notion of (i) local context and (ii) large contextual pattern. Both notions are essential to building a good representation for protein sequences. The proposed context-window based scaled self-attention mechanism is further used to build the multi context-window based scaled (MCWS) transformer network for the protein function prediction task at the protein sub-sequence level. Overall, the proposed MCWS transformer network produced improved predictive performances, outperforming existing state-of-the-art approaches by substantial margins. With respect to the standard transformer network, the proposed network produced improvements in F1-score of +2.30% and +2.08% on the biological process (BP) and molecular function (MF) datasets, respectively. The corresponding improvements over the state-of-the-art ProtVecGen-Plus+ProtVecGen-Ensemble approach are +3.38% (BP) and +2.86% (MF). Equally important, robust performances were obtained across protein sequences of different lengths.
Assuntos
Sequência de Aminoácidos , Proteínas , Design de Software , Proteínas/químicaRESUMO
The order of amino acids in a protein sequence enables the protein to acquire a conformation suitable for performing functions, thereby motivating the need to analyze these sequences for predicting functions. Although machine learning based approaches are fast compared to methods using BLAST, FASTA, etc., they fail to perform well for long protein sequences (with more than 300 amino acids). In this paper, we introduce a novel method for construction of two separate feature sets for protein using bi-directional long short-term memory network based on the analysis of fixed 1) single-sized segments and 2) multi-sized segments. The model trained on the proposed feature set based on multi-sized segments is combined with the model trained using state-of-the-art Multi-label Linear Discriminant Analysis (MLDA) features to further improve the accuracy. Extensive evaluations using separate datasets for biological processes and molecular functions demonstrate not only improved results for long sequences, but also significantly improve the overall accuracy over state-of-the-art method. The single-sized approach produces an improvement of +3.37 percent for biological processes and +5.48 percent for molecular functions over the MLDA based classifier. The corresponding numbers for multi-sized approach are +5.38 and +8.00 percent. Combining the two models, the accuracy further improves to +7.41 and +9.21 percent, respectively.
