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Improving cell-free glycoprotein synthesis by characterizing and enriching native membrane vesicles

https://doi.org/10.1038/s41467-021-22329-3

Hershewe, Jasmine M. ; Warfel, Katherine F. ; Iyer, Shaelyn M. ; Peruzzi, Justin A. ; Sullivan, Claretta J. ; Roth, Eric W. ; DeLisa, Matthew P. ; Kamat, Neha P. ; Jewett, Michael C. ( December 2021 , Nature Communications)
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Abstract Cell-free gene expression (CFE) systems from crude cellular extracts have attracted much attention for biomanufacturing and synthetic biology. However, activating membrane-dependent functionality of cell-derived vesicles in bacterial CFE systems has been limited. Here, we address this limitation by characterizing native membrane vesicles in Escherichia coli- based CFE extracts and describing methods to enrich vesicles with heterologous, membrane-bound machinery. As a model, we focus on bacterial glycoengineering. We first use multiple, orthogonal techniques to characterize vesicles and show how extract processing methods can be used to increase concentrations of membrane vesicles in CFE systems. Then, we show that extracts enriched in vesicle number also display enhanced concentrations of heterologous membrane protein cargo. Finally, we apply our methods to enrich membrane-bound oligosaccharyltransferases and lipid-linked oligosaccharides for improving cell-free N- linked and O -linked glycoprotein synthesis. We anticipate that these methods will facilitate on-demand glycoprotein production and enable new CFE systems with membrane-associated activities.
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On-demand biomanufacturing of protective conjugate vaccines

https://doi.org/10.1126/sciadv.abe9444

Stark, Jessica C. ; Jaroentomeechai, Thapakorn ; Moeller, Tyler D. ; Hershewe, Jasmine M. ; Warfel, Katherine F. ; Moricz, Bridget S. ; Martini, Anthony M. ; Dubner, Rachel S. ; Hsu, Karen J. ; Stevenson, Taylor C. ; et al ( February 2021 , Science Advances)
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Conjugate vaccines are among the most effective methods for preventing bacterial infections. However, existing manufacturing approaches limit access to conjugate vaccines due to centralized production and cold chain distribution requirements. To address these limitations, we developed a modular technology for in vitro conjugate vaccine expression (iVAX) in portable, freeze-dried lysates from detoxified, nonpathogenic Escherichia coli. Upon rehydration, iVAX reactions synthesize clinically relevant doses of conjugate vaccines against diverse bacterial pathogens in 1 hour. We show that iVAX-synthesized vaccines against Francisella tularensis subsp. tularensis (type A) strain Schu S4 protected mice from lethal intranasal F. tularensis challenge. The iVAX platform promises to accelerate development of new conjugate vaccines with increased access through refrigeration-independent distribution and portable production.
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Ribosome Stalling of N -Linked Glycoproteins in Cell-Free Extracts

https://doi.org/10.1021/acssynbio.2c00311

Chung, Sean S. ; Bidstrup, Erik J. ; Hershewe, Jasmine M. ; Warfel, Katherine F. ; Jewett, Michael C. ; DeLisa, Matthew P. ( November 2022 , ACS Synthetic Biology)