A toolkit for enhanced reproducibility of RNASeq analysis for synthetic biologists

Author:

Garcia Benjamin J1,Urrutia Joshua2,Zheng George3,Becker Diveena4,Corbet Carolyn4,Maschhoff Paul4,Cristofaro Alexander15ORCID,Gaffney Niall2,Vaughn Matthew2,Saxena Uma1,Chen Yi-Pei3ORCID,Gordon D Benjamin1,Eslami Mohammed3ORCID

Affiliation:

1. Department of Biological Engineering, Synthetic Biology Center, Massachusetts Institute of Technology , Cambridge, MA, USA

2. Texas Advanced Computing Center, University of Texas at Austin , Austin, TX, USA

3. Netrias LLC , Annapolis, MD, USA

4. Ginkgo Bioworks , Boston, MA, USA

5. TScan Therapeutics , Waltham, MA, USA

Abstract

Abstract Sequencing technologies, in particular RNASeq, have become critical tools in the design, build, test and learn cycle of synthetic biology. They provide a better understanding of synthetic designs, and they help identify ways to improve and select designs. While these data are beneficial to design, their collection and analysis is a complex, multistep process that has implications on both discovery and reproducibility of experiments. Additionally, tool parameters, experimental metadata, normalization of data and standardization of file formats present challenges that are computationally intensive. This calls for high-throughput pipelines expressly designed to handle the combinatorial and longitudinal nature of synthetic biology. In this paper, we present a pipeline to maximize the analytical reproducibility of RNASeq for synthetic biologists. We also explore the impact of reproducibility on the validation of machine learning models. We present the design of a pipeline that combines traditional RNASeq data processing tools with structured metadata tracking to allow for the exploration of the combinatorial design in a high-throughput and reproducible manner. We then demonstrate utility via two different experiments: a control comparison experiment and a machine learning model experiment. The first experiment compares datasets collected from identical biological controls across multiple days for two different organisms. It shows that a reproducible experimental protocol for one organism does not guarantee reproducibility in another. The second experiment quantifies the differences in experimental runs from multiple perspectives. It shows that the lack of reproducibility from these different perspectives can place an upper bound on the validation of machine learning models trained on RNASeq data. Graphical Abstract

Funder

Defense Advanced Research Projects Agency

Publisher

Oxford University Press (OUP)

Subject

Agricultural and Biological Sciences (miscellaneous),Biomedical Engineering,Biomaterials,Bioengineering,Biotechnology

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