Sawan Patel

Sawan Patel, Sophia Tang, Yesol Kim et al.

Therapeutic mRNA design requires coordinating multiple interacting sequence features across the full transcript, where codon usage, untranslated regions (UTRs), and their coupling jointly determine stability, translation efficiency, and protein expression. Here, we present mRNA generation via unrolled trajectories and informed latent updates (mRNAutilus), a framework for simultaneous codon optimization and de novo UTR design directly from sequence. mRNAutilus combines a masked discrete diffusion model trained on millions of full-length mRNAs with Monte Carlo Tree Guidance to generate Pareto-efficient sequences under multiple functional objectives, using lightweight regressors over model embeddings to predict half-life, translation efficiency, and protein abundance. Unlike recent methods that design coding sequences and UTRs separately or rely on post hoc assembly and screening, mRNAutilus generates complete transcripts in a single process optimized across properties. Across diverse targets, zero-shot mRNAs encoding P. pyralis luciferase achieve over 400-fold higher expression than wild-type and outperform commercial and machine learning-designed baselines, including zero-shot generative approaches. Zero-shot SARS-CoV-2 Spike mRNAs exceed clinically used and commercial constructs and match or surpass lab-optimized designs with improved durability. We further demonstrate generality in therapeutic settings, including prime editing (PEMax) and programmable proteome modulation, where mRNAutilus-designed constructs enhance expression of peptide-guided E3 ligases (uAbs) for beta-catenin degradation. These results establish a sequence-based, multi-objective framework for generating functional mRNAs tailored to diverse biological applications.

Fred Zhangzhi Peng, Zachary Bezemek, Sawan Patel et al.

Any order generation of discrete data using masked diffusion models (MDMs) offers a compelling alternative to traditional autoregressive models, especially in domains that lack a natural causal ordering of data. However, current popular MDMs depart from their successful continuous diffusion model counterparts with simplified masked inference wherein unmasked tokens cannot be iteratively refined -- even if there is a mistake. In this paper, we extract the full power of MDMs by introducing a novel inference sampling strategy termed Path Planning (P2) that decomposes each generation step into two sub-stages: planning and denoising. Under P2, the planner at every step selects appropriate tokens that are marked to be updated, which can then be sampled using the denoiser. We demonstrate that P2 generalizes all existing sampling strategies for MDMs and critically enhances generative quality through the new capability of refining and updating existing unmasked tokens. We theoretically prove that P2 establishes a (new) expanded evidence lower bound (ELBO) on the log marginal likelihood of data. We instantiate P2 with a family of planners including: 1.) Self-Planning, 2.) BERT-Planning, and 3.) Trained-Planning with a learned planner leading to SOTA generative performance for MDMs on a suite of domains. Specifically, solely using P2 inference, we observe relative improvements of 22% in protein sequence foldability, 8% in RNA sequence pLDDT, 4% in math reasoning, 68% in story generation (ROUGE score), and 33% in code generation for the challenging pass@1 metric.