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A real-time assay for cell-penetrating peptide-mediated delivery of molecular cargos

Schuyler B. Gentry, Scott J. Nowak, View ORCID ProfileXuelei Ni, Stephanie A. Hill, Lydia R. Wade, William R. Clark, Aidan P. Keelaghan, Daniel P. Morris, View ORCID ProfileJonathan L. McMurry
doi: https://doi.org/10.1101/2021.07.23.453555
Schuyler B. Gentry
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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Scott J. Nowak
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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Xuelei Ni
2School of Data Science & Analytics, Kennesaw State University, Kennesaw, Georgia, United States of America
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Stephanie A. Hill
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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Lydia R. Wade
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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William R. Clark
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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Aidan P. Keelaghan
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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Daniel P. Morris
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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Jonathan L. McMurry
1Department of Molecular & Cellular Biology, Kennesaw State University, Kennesaw, Georgia, United States of America
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  • ORCID record for Jonathan L. McMurry
  • For correspondence: jmcmurr1@kennesaw.edu
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Abstract

Cell-penetrating peptides (CPPs) are capable of transporting molecules to which they are tethered across cellular membranes. Unsurprisingly, CPPs have attracted attention for their potential drug delivery applications, but several technical hurdles remain to be overcome. Chief among them is the so-called ‘endosomal escape problem,’ i.e. the propensity of CPP-cargo molecules to be endocytosed but remain entrapped in endosomes rather than reaching the cytosol. Previously, a CPP fused to calmodulin that bound calmodulin binding site-containing cargos was shown to efficiently deliver cargos to the cytoplasm, effectively overcoming the endosomal escape problem. The CPP-adaptor, “TAT-CaM,” evinces delivery at nM concentrations and more rapidly than we had previously been able to measure. To better understand the kinetics and mechanism of CPP-adaptor-mediated cargo delivery, a real-time cell penetrating assay was developed in which a flow chamber containing cultured cells was installed on the stage of a confocal microscope to allow for observation ab initio. Also examined in this study was an improved CPP-adaptor that utilizes naked mole rat (Heterocephalus glaber) calmodulin in place of human and results in superior internalization, likely due to its lesser net negative charge. Adaptor-cargo complexes were delivered into the flow chamber and fluorescence intensity in the midpoint of baby hamster kidney cells was measured as a function of time. Delivery of 400 nM cargo was observed within seven minutes and fluorescence continued to increase linearly as a function of time. Cargo-only control experiments showed that the minimal uptake which occurred independently of the CPP-adaptor resulted in punctate localization consistent with endosomal entrapment. A distance analysis was performed for cell-penetration experiments in which CPP-adaptor-delivered cargo showing wider dispersions throughout cells as compared to an analogous covalently-bound CPP-cargo. Small molecule endocytosis inhibitors did not have significant effects upon delivery. The real-time assay is an improvement upon static endpoint assays and should be informative in a broad array of applications.

Competing Interest Statement

I have read the journal's policy and the authors of this manuscript have the following competing interests: JLM and SJN have equity interest in New Echota Biotechnology, which has exclusive license to patent US10654894B2 on the CPP-adaptor technology and applications thereof. The other authors have no competing interests. This does not alter our adherence to PLOS ONE policies on sharing data and materials.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY 4.0 International license.
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Posted July 23, 2021.
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A real-time assay for cell-penetrating peptide-mediated delivery of molecular cargos
Schuyler B. Gentry, Scott J. Nowak, Xuelei Ni, Stephanie A. Hill, Lydia R. Wade, William R. Clark, Aidan P. Keelaghan, Daniel P. Morris, Jonathan L. McMurry
bioRxiv 2021.07.23.453555; doi: https://doi.org/10.1101/2021.07.23.453555
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A real-time assay for cell-penetrating peptide-mediated delivery of molecular cargos
Schuyler B. Gentry, Scott J. Nowak, Xuelei Ni, Stephanie A. Hill, Lydia R. Wade, William R. Clark, Aidan P. Keelaghan, Daniel P. Morris, Jonathan L. McMurry
bioRxiv 2021.07.23.453555; doi: https://doi.org/10.1101/2021.07.23.453555

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