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Limitations and challenges in protein stability prediction upon genome variations: towards future applications in precision medicine

Tiziana SanaviaDepartment of Medical Sciences, University of Torino, Via Santena 19, 10126 Torino, ItalyGiovanni BiroloDepartment of Medical Sciences, University of Torino, Via Santena 19, 10126 Torino, ItalyLudovica MontanucciDepartment of Comparative Biomedicine and Food Science (BCA), University of Padova, Viale dell’Università 16, 35020 Legnaro, ItalyPaola TurinaDepartment of Pharmacy and Biotechnology (FaBiT), University of Bologna, Via F. Selmi 3, 40126 Bologna, ItalyEmidio CapriottiDepartment of Pharmacy and Biotechnology (FaBiT), University of Bologna, Via F. Selmi 3, 40126 Bologna, ItalyPiero FariselliDepartment of Medical Sciences, University of Torino, Via Santena 19, 10126 Torino, Italy
2020en
ABI

Аннотация

Protein stability predictions are becoming essential in medicine to develop novel immunotherapeutic agents and for drug discovery. Despite the large number of computational approaches for predicting the protein stability upon mutation, there are still critical unsolved problems: 1) the limited number of thermodynamic measurements for proteins provided by current databases; 2) the large intrinsic variability of ΔΔG values due to different experimental conditions; 3) biases in the development of predictive methods caused by ignoring the anti-symmetry of ΔΔG values between mutant and native protein forms; 4) over-optimistic prediction performance, due to sequence similarity between proteins used in training and test datasets. Here, we review these issues, highlighting new challenges required to improve current tools and to achieve more reliable predictions. In addition, we provide a perspective of how these methods will be beneficial for designing novel precision medicine approaches for several genetic disorders caused by mutations, such as cancer and neurodegenerative diseases.

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