Sequencing Strategy to Ensure Accurate Plasmid Assembly.

bioRxiv

Department of Chemical and Biological Engineering, Colorado State University, Fort Collins, Colorado, 80523, United States of America.

Published: June 2024

AI Article Synopsis

  • The verification of plasmid sequences is often overlooked in manufacturing, even though it’s crucial for research and clinical applications.
  • Current sequencing technologies, including short-read and long-read methods, have their own limitations, with short-reads struggling in GC-rich areas and long-reads prone to errors in repetitive regions.
  • A hybrid sequencing approach yielded the most accurate plasmid assembly and helped identify mutations, highlighting the need to focus on easier-to-sequence genetic parts in future designs.

Article Abstract

Despite the wide use of plasmids in research and clinical production, the need to verify plasmid sequences is a bottleneck that is too often underestimated in the manufacturing process. Although sequencing platforms continue to improve, the method and assembly pipeline chosen still influence the final plasmid assembly sequence. Furthermore, few dedicated tools exist for plasmid assembly, especially for assembly. Here, we evaluated short-read, long-read, and hybrid (both short and long reads) assembly pipelines across three replicates of a 24-plasmid library. Consistent with previous characterizations of each sequencing technology, short-read assemblies had issues resolving GC-rich regions, and long-read assemblies commonly had small insertions and deletions, especially in repetitive regions. The hybrid approach facilitated the most accurate, consistent assembly generation and identified mutations relative to the reference sequence. Although Sanger sequencing can be used to verify specific regions, some GC-rich and repetitive regions were difficult to resolve using any method, suggesting that easily sequenced genetic parts should be prioritized in the design of new genetic constructs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10996661PMC
http://dx.doi.org/10.1101/2024.03.25.586694DOI Listing

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