November 22, 2024

A Breakthrough in Genome Editing: How NICER Outperforms CRISPR/Cas9

NICER, a new gene editing technique established by Japanese scientists, provides a much safer alternative to CRISPR/Cas9 by substantially lowering unintentional DNA mutations, boosting genetic disease treatment.
Scientists led by Osaka University develop a new gene adjustment method understood as NICER that considerably reduces off-target anomalies in DNA.
The gene modifying strategy CRISPR/Cas9 has enabled scientists to make impactful and precise changes to an organisms DNA to fix anomalies that cause genetic disease. Nevertheless, the CRISPR/Cas9 technique can likewise result in unintentional DNA anomalies that might have negative effects. Recently, researchers in Japan have established a new gene modifying method that is as efficient as CRISPR/Cas9 while considerably reducing these unintended anomalies.
Off-target anomalies resulting from standard genome editing methods. Due to the mutagenic nature of DNA double-strand break repair work, even if the gene anomaly is effectively remedied, there is an increased danger of off-target anomalies in areas unique from the initial target of CRISPR/Cas9. Credit: S. Nakada
Comprehending NICERs Methodology
In a brand-new research study published in the journal Nature Communications, scientists led by Osaka University introduced an unique method called NICER, which is based upon the development of several little cuts in single DNA strands by an enzyme called a nickase.

The gene editing method CRISPR/Cas9 has actually allowed researchers to make accurate and impactful modifications to an organisms DNA to repair anomalies that cause genetic disease. The CRISPR/Cas9 method can also result in unexpected DNA mutations that may have negative impacts. Due to the mutagenic nature of DNA double-strand break repair work, even if the gene mutation is effectively corrected, there is an increased risk of off-target mutations in areas distinct from the original target of CRISPR/Cas9. Cellular repair work of double-strand breaks can lead to unexpected DNA mutations, as well as the integration of exogenous DNA to the human genome, which raises security concerns for scientific applications of CRISPR/Cas9 technology. To lessen these unintentional mutations, the Osaka University-led research team examined the use of Cas9 nickase, which creates single-strand breaks or “nicks” in DNA that are typically fixed without triggering anomalies
.

Cellular repair of double-strand breaks can lead to unexpected DNA anomalies, as well as the integration of exogenous DNA to the human genome, which raises safety issues for scientific applications of CRISPR/Cas9 innovation. To decrease these unintended mutations, the Osaka University-led research group investigated the usage of Cas9 nickase, which develops single-strand breaks or “nicks” in DNA that are usually repaired without triggering mutations
.
NICERs Applications and benefits.
Nicks are usually repaired without triggering anomalies. Even if nicks appear at websites different from nickases initial target, new gene mutations are seldom seen at these places. This method allows for precise gene correction with minimal off-target mutations.
” Each chromosome in the genome has a homologous copy,” states lead author of the study Akiko Tomita. “Using the NICER strategy, heterozygous anomalies– in which an anomaly appears in one chromosome but not its homologous copy– are fixed utilizing the unmutated homologous chromosome as a template.”.
For their initial experiments, the research team used human lymphoblast cells with a recognized heterozygous mutation in a gene called TK1. When these cells were treated with nickase to cause a single cut in the TK1 area, TK1 activity was recuperated at a low rate. Nevertheless, when the nickase caused several nicks in this area on both homologous chromosomes, gene correction performance was boosted around seventeen-fold through activation of a cellular repair work mechanism.
A nick is made near the anomaly (and is unique to the mutant allele). Simply presenting a nick close to the mutation prompts homologous recombination between homologous chromosomes but at a very low rate.
” Further genomic analysis showed that the NICER method rarely induced off-target anomalies,” states senior author Shinichiro Nakada. “We were likewise pleased to discover that NICER had the ability to bring back the expression of disease-causing genes in cells obtained from hereditary illness including compound heterozygous mutations.”.
Since the NICER technique does not include DNA double-strand breaks or the use of exogenous DNA, this strategy seems a safe option to standard CRISPR/Cas9 techniques. NICER may represent a novel technique for the treatment of hereditary diseases brought on by heterozygous mutations.
Recommendation: “Inducing several nicks promotes interhomolog homologous recombination to correct heterozygous anomalies in somatic cells” by Akiko Tomita, Hiroyuki Sasanuma, Tomoo Owa, Yuka Nakazawa, Mayuko Shimada, Takahiro Fukuoka, Tomoo Ogi and Shinichiro Nakada, 15 September 2023, Nature Communications.DOI: 10.1038/ s41467-023-41048-5.