Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy

Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy

We have recently developed surface oligopeptide knock-in for rapid target selection (SORTS), a novel method to isolate mammalian cells with gene modifications using FACS-sorting. It relies on CRISPR/Cas9-mediated targeted knock-in of a very short promoterless expression construct (250 bp) comprising...

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Main Authors: Dmitriy Mazurov, Alexandra Maslennikova, Dmitriy Komkov, Anastasia Zotova
Format: Article
Language:English
Published: MDPI AG 2020-06-01
Series:Proceedings
Subjects:
SORTS
CD52
HIV-1
gene editing
CRISPR-Cas9
fusion inhibitor peptides
Online Access:https://www.mdpi.com/2504-3900/50/1/13
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spelling doaj-bf7bae9709f94a988b04479f9450f0ca2020-11-25T03:11:28ZengMDPI AGProceedings2504-39002020-06-0150131310.3390/proceedings2020050013Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and TherapyDmitriy Mazurov0Alexandra Maslennikova1Dmitriy Komkov2Anastasia Zotova3Cell and Gene Technology Group, Institute of Gene Biology RAS, Moscow 119334, RussiaCell and Gene Technology Group, Institute of Gene Biology RAS, Moscow 119334, RussiaCell and Gene Technology Group, Institute of Gene Biology RAS, Moscow 119334, RussiaCell and Gene Technology Group, Institute of Gene Biology RAS, Moscow 119334, RussiaWe have recently developed surface oligopeptide knock-in for rapid target selection (SORTS), a novel method to isolate mammalian cells with gene modifications using FACS-sorting. It relies on CRISPR/Cas9-mediated targeted knock-in of a very short promoterless expression construct (250 bp) comprising a Flag or HA epitope embedded into the smallest GPI-protein CD52, and a polyA signal from the beta-globin. CD52 efficiently delivers the epitope to the cell surface, where it serves as a marker for selection, while polyA terminates transcription and silences target gene expression. Primarily, SORTS was developed to knock out genes encoding intracellular or secreted proteins, which cannot be used as markers for selection of live cells. Using in-frame modification of SORTS, we demonstrated the possibility of HIV-1 provirus inactivation via sorting of GPI-tag positive cells. In order to make the “cured” cells resistant to a subsequent HIV-1 infection, the epitope tag in the CD52 molecule was substituted by one of the fusion inhibitor peptides from the CHR-domain of gp41. We selected a series of cell-surface-expressed, GPI-anchored, C34-based peptides that confer a strong cellular resistance to HIV-1 infection mediated by NL4-3, JRFL, or ZM153 Env. These findings together with a monoclonal antibody raised against the C34 peptide provide an opportunity to generate and select HIV-resistant lymphocytes for a therapeutic goal. SORTS was also adapted to engineer transgenic HIV-1 effector Т cells and to study cell-to-cell transmission. To facilitate transgenesis, we developed a knock-in strategy to express GPI-tag from the intronic region of the human PPP1R12C gene (AAVS1 locus) and delivered FRT sites of recombination into both alleles. In summary, SORTS is a novel instrument to isolate rare cells with precise genomic modifications with broad applications, including HIV biology. This work was supported by the Russian Science Foundation (grant 18-14-00333) and the Russian Foundation for Basic Research (grants 18-29-07052, 18-04-01016).https://www.mdpi.com/2504-3900/50/1/13SORTSCD52HIV-1gene editingCRISPR-Cas9fusion inhibitor peptides
collection DOAJ
language English
format Article
sources DOAJ
author Dmitriy Mazurov
Alexandra Maslennikova
Dmitriy Komkov
Anastasia Zotova
spellingShingle Dmitriy Mazurov
Alexandra Maslennikova
Dmitriy Komkov
Anastasia Zotova
Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy
Proceedings
SORTS
CD52
HIV-1
gene editing
CRISPR-Cas9
fusion inhibitor peptides
author_facet Dmitriy Mazurov
Alexandra Maslennikova
Dmitriy Komkov
Anastasia Zotova
author_sort Dmitriy Mazurov
title Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy
title_short Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy
title_full Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy
title_fullStr Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy
title_full_unstemmed Application of SORTS, a Novel Gene-Edited Cell Selection Method for HIV Study and Therapy
title_sort application of sorts, a novel gene-edited cell selection method for hiv study and therapy
publisher MDPI AG
series Proceedings
issn 2504-3900
publishDate 2020-06-01
description We have recently developed surface oligopeptide knock-in for rapid target selection (SORTS), a novel method to isolate mammalian cells with gene modifications using FACS-sorting. It relies on CRISPR/Cas9-mediated targeted knock-in of a very short promoterless expression construct (250 bp) comprising a Flag or HA epitope embedded into the smallest GPI-protein CD52, and a polyA signal from the beta-globin. CD52 efficiently delivers the epitope to the cell surface, where it serves as a marker for selection, while polyA terminates transcription and silences target gene expression. Primarily, SORTS was developed to knock out genes encoding intracellular or secreted proteins, which cannot be used as markers for selection of live cells. Using in-frame modification of SORTS, we demonstrated the possibility of HIV-1 provirus inactivation via sorting of GPI-tag positive cells. In order to make the “cured” cells resistant to a subsequent HIV-1 infection, the epitope tag in the CD52 molecule was substituted by one of the fusion inhibitor peptides from the CHR-domain of gp41. We selected a series of cell-surface-expressed, GPI-anchored, C34-based peptides that confer a strong cellular resistance to HIV-1 infection mediated by NL4-3, JRFL, or ZM153 Env. These findings together with a monoclonal antibody raised against the C34 peptide provide an opportunity to generate and select HIV-resistant lymphocytes for a therapeutic goal. SORTS was also adapted to engineer transgenic HIV-1 effector Т cells and to study cell-to-cell transmission. To facilitate transgenesis, we developed a knock-in strategy to express GPI-tag from the intronic region of the human PPP1R12C gene (AAVS1 locus) and delivered FRT sites of recombination into both alleles. In summary, SORTS is a novel instrument to isolate rare cells with precise genomic modifications with broad applications, including HIV biology. This work was supported by the Russian Science Foundation (grant 18-14-00333) and the Russian Foundation for Basic Research (grants 18-29-07052, 18-04-01016).
topic SORTS
CD52
HIV-1
gene editing
CRISPR-Cas9
fusion inhibitor peptides
url https://www.mdpi.com/2504-3900/50/1/13
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