Nature Search

CRISPRoff enables spatio-temporal control of CRISPR editing

Uncontrolled gene editing can lead to off-target effects and chromosomal translocations. Here the authors develop CRISPRoff, light degradable sgRNAs for titratable and spatially defined gene editing.

Jared Carlson-Stevermer
Reed Kelso
Travis Maures
ResearchOpen Access07 Oct 2020
Nature Communications

Volume: 11, P: 1-7
Design of efficacious somatic cell genome editing strategies for recessive and polygenic diseases

Gene correction of multiple alleles is a promising therapeutic strategy. Here the authors present bi-allelic correction of Pompe disease and provide an in silico model for predicting in vivo somatic editing outcomes.

Jared Carlson-Stevermer
Amritava Das
Krishanu Saha
ResearchOpen Access08 Dec 2020
Nature Communications

Volume: 11, P: 1-18
CRISPR/Cas9 editing of APP C-terminus attenuates β-cleavage and promotes α-cleavage

Gene editing strategies are typically designed to correct mutant genes, but most neurodegenerative diseases are sporadic. Here the authors describe a strategy to selectively edit the C-terminus of APP and attenuate amyloid-β production, while upregulating neuroprotective α-cleavage.

Jichao Sun
Jared Carlson-Stevermer
Subhojit Roy
ResearchOpen Access03 Jan 2019
Nature Communications

Volume: 10, P: 1-11
Proteomic and genetic analyses of influenza A viruses identify pan-viral host targets

Using a multi-OMICS approach, Haas et al identify 54 human genes and 16 host-targeting chemical compounds that regulate influenza A virus infection in lung epithelial cells, including AHNAK and COBP1 which are also essential for SARS-CoV-2 infection.

Kelsey M. Haas
Michael J. McGregor
Nevan J. Krogan
ResearchOpen Access27 Sept 2023
Nature Communications

Volume: 14, P: 1-27
Identification of DAXX as a restriction factor of SARS-CoV-2 through a CRISPR/Cas9 screen

Here, Mac Kain and Maarifi et al. perform a functional CRISPR/Cas9 screen to identify SARS-CoV-2 restriction factors in A549 cells. They identify DAXX, a scaffold protein of nuclear bodies with diverse functions, that has anti-viral activity post SARS-CoV-2 entry, while SARS-CoV-2 has evolved a mechanism to counteract its action via PLpro-mediated proteasomal degradation.

Alice Mac Kain
Ghizlane Maarifi
Ferdinand Roesch
ResearchOpen Access04 May 2022
Nature Communications

Volume: 13, P: 1-13
BRD2 inhibition blocks SARS-CoV-2 infection by reducing transcription of the host cell receptor ACE2

Samelson et al. report that BRD2 inhibition suppresses SARS-CoV-2 infection in epithelial cells and Syrian hamsters via reducing the transcription of host cell surface receptor ACE2.

Avi J. Samelson
Quang Dinh Tran
Martin Kampmann
Research13 Jan 2022
Nature Cell Biology

Volume: 24, P: 24-34
Assembly of CRISPR ribonucleoproteins with biotinylated oligonucleotides via an RNA aptamer for precise gene editing

Using CRISPR to write specific genetic sequences can sometimes be difficult due to the preference of mammalian cells to repair breaks using NHEJ. Here the authors form nanoparticles to localize the template sequence to the nuclease, shifting repair in favor of HDR.

Jared Carlson-Stevermer
Amr A. Abdeen
Krishanu Saha
ResearchOpen Access23 Nov 2017
Nature Communications

Volume: 8, P: 1-13

Search

Filter By:

CRISPRoff enables spatio-temporal control of CRISPR editing

Design of efficacious somatic cell genome editing strategies for recessive and polygenic diseases

CRISPR/Cas9 editing of APP C-terminus attenuates β-cleavage and promotes α-cleavage

Proteomic and genetic analyses of influenza A viruses identify pan-viral host targets

Identification of DAXX as a restriction factor of SARS-CoV-2 through a CRISPR/Cas9 screen

BRD2 inhibition blocks SARS-CoV-2 infection by reducing transcription of the host cell receptor ACE2

Assembly of CRISPR ribonucleoproteins with biotinylated oligonucleotides via an RNA aptamer for precise gene editing

Search

Quick links