Scalable DNA Feature Generation and Transcription Factor Binding Prediction via Deep Surrogate Models

Simulating DNA breathing dynamics, for instance Extended Peyrard-Bishop-Dauxois (EPBD) model, across the entire human genome using traditional biophysical methods like pyDNA-EPBD is computationally prohibitive due to intensive techniques such as Markov Chain Monte Carlo (MCMC) and Langevin dynamics. To overcome this limitation, we propose a deep surrogate generative model utilizing a conditional Denoising Diffusion Probabilistic Model (DDPM) trained on DNA sequence-EPBD feature pairs. This surrogate model efficiently generates high-fidelity DNA breathing features conditioned on DNA sequences, reducing computational time from months to hours–a speedup of over 1000 times. By integrating these features into the EPBDxDNABERT-2 model, we enhance the accuracy of transcription factor (TF) binding site predictions. Experiments demonstrate that the surrogate-generated features perform comparably to those obtained from the original EPBD framework, validating the model’s efficacy and fidelity. This advancement enables real-time, genome-wide analyses, significantly accelerating genomic research and offering powerful tools for disease understanding and therapeutic development.