Literature DB >> 33184583

CRISPR-Mediated Isogenic Cell-SELEX Approach for Generating Highly Specific Aptamers Against Native Membrane Proteins.

Jonah C Rosch1, Emma H Neal1, Daniel A Balikov2,3, Mohsin Rahim1, Ethan S Lippmann1,2,4,5.   

Abstract

INTRODUCTION: The generation of affinity reagents that bind native membrane proteins with high specificity remains challenging. Most in vitro selection paradigms utilize different cell types for positive and negative rounds of selection (where the positive selection is against a cell that expresses the desired membrane protein and the negative selection is against a cell that lacks the protein). However, this strategy can yield affinity reagents that bind unintended membrane proteins on the target cells. To address this issue, we developed a systematic evolution of ligands by exponential enrichment (SELEX) scheme that utilizes isogenic pairs of cells generated via CRISPR techniques.
METHODS: Using a Caco-2 epithelial cell line with constitutive Cas9 expression, we knocked out the SLC2A1 gene (encoding the GLUT1 glucose transporter) via lipofection with synthetic gRNAs. Cell-SELEX rounds were carried out against wild-type and GLUT1-null cells using a single-strand DNA (ssDNA) library. Next-generation sequencing (NGS) was used to quantify enrichment of prospective binders to the wild-type cells.
RESULTS: 10 rounds of cell-SELEX were conducted via simultaneous exposure of ssDNA pools to wild-type and GLUT1-null Caco-2 cells under continuous perfusion. The top binders identified from NGS were validated by flow cytometry and immunostaining for their specificity to the GLUT1 receptor.
CONCLUSIONS: Our data indicate that highly specific aptamers can be isolated with a SELEX strategy that utilizes isogenic cell lines. This approach may be broadly useful for generating affinity reagents that selectively bind to membrane proteins in their native conformations on the cell surface. © Biomedical Engineering Society 2020.

Entities:  

Keywords:  Affinity reagents; Aptamer; CRISPR; Nucleic acid therapeutics; SELEX

Year:  2020        PMID: 33184583      PMCID: PMC7596163          DOI: 10.1007/s12195-020-00651-y

Source DB:  PubMed          Journal:  Cell Mol Bioeng        ISSN: 1865-5025            Impact factor:   2.321


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Review 5.  The SLC2 (GLUT) family of membrane transporters.

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7.  Identification of DNA aptamers toward epithelial cell adhesion molecule via cell-SELEX.

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Review 2.  An Update of Nucleic Acids Aptamers Theranostic Integration with CRISPR/Cas Technology.

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