Genetically modified animal models of hereditary diseases for testing of gene-directed therapy

Polikarpova, Anna V.; Егорова, Т. В.; Bardina, Maryana V.

doi:10.3897/rrpharmacology.8.82618

Cited by 2 publications

(2 citation statements)

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“…Personalized medicine holds a huge promise for severe genetic diseases ( Kim et al, 2019 ; Wang et al, 2020 ; Diener et al, 2022 ), and requires the appropriate animal models ( Kalmykov et al, 2018 ; Aartsma-Rus and van Putten, 2019 ; Polikarpova et al, 2022 ; Vázquez-Domínguez and Garanto, 2022 ). Sequence-specific RNA-based drugs, such as antisense oligonucleotides (ASO) and RNAi therapeutics ( Zhu et al, 2022 ; Zogg et al, 2022 ), are currently in development as a new generation of medicine to treat dominant neurological disorders such as Huntington’s disease, amyotrophic lateral sclerosis, spinocerebellar ataxia, and several others ( Zhao et al, 2017 ; Iannitti et al, 2018 ; Miniarikova et al, 2018 ; Southwell et al, 2018 ; Martier et al, 2019 ; Aimiuwu et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

CRISPR/Cas9-generated mouse model with humanizing single-base substitution in the Gnao1 for safety studies of RNA therapeutics

et al. 2023

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The development of personalized medicine for genetic diseases requires preclinical testing in the appropriate animal models. GNAO1 encephalopathy is a severe neurodevelopmental disorder caused by heterozygous de novo mutations in the GNAO1 gene. GNAO1 c.607 G>A is one of the most common pathogenic variants, and the mutant protein Gαo-G203R likely adversely affects neuronal signaling. As an innovative approach, sequence-specific RNA-based therapeutics such as antisense oligonucleotides or effectors of RNA interference are potentially applicable for selective suppression of the mutant GNAO1 transcript. While in vitro validation can be performed in patient-derived cells, a humanized mouse model to rule out the safety of RNA therapeutics is currently lacking. In the present work, we employed CRISPR/Cas9 technology to introduce a single-base substitution into exon 6 of the Gnao1 to replace the murine Gly203-coding triplet (GGG) with the codon used in the human gene (GGA). We verified that genome-editing did not interfere with the Gnao1 mRNA or Gαo protein synthesis and did not alter localization of the protein in the brain structures. The analysis of blastocysts revealed the off-target activity of the CRISPR/Cas9 complexes; however, no modifications of the predicted off-target sites were detected in the founder mouse. Histological staining confirmed the absence of abnormal changes in the brain of genome-edited mice. The created mouse model with the “humanized” fragment of the endogenous Gnao1 is suitable to rule out unintended targeting of the wild-type allele by RNA therapeutics directed at lowering GNAO1 c.607 G>A transcripts.

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Section: Discussionmentioning

confidence: 99%

CRISPR/Cas9-generated mouse model with humanizing single-base substitution in the Gnao1 for safety studies of RNA therapeutics

et al. 2023

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“…The effectiveness of modern methods of UC treatment is fairy moderate, which makes it urgent to search for new ways of treating it (Le Berre et al 2023). Considering the important role of genetic factors in the development of UC, innovative methods, including gene therapy, have an undoubted future (Polikarpova et al 2022); however, new directions for the use of the already known drugs are also important.…”

Section: Introductionmentioning

confidence: 99%

The effect of dalargin on growth factors content in experimental ulcerative colitis

Liashev,

Mal,

Solin

et al. 2023

RRP

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Introduction: The effectiveness of ulcerative colitis (UC) treatment is fairy moderate and it gives a rise to search for new ways of treating it. Considering the combination of dalargineffects, studying the dalargin influence on the UC development is of undoubted interest. The aim of the study was to evaluate the dalargin effect on the content of transforming growth factor-β (TGF-β) and epidermal growth factor (EGF) in the colonic wall in mice with experimental ulcerative colitis. Materials and methods: UC was simulated by replacing water with a 5% solution of dextran sodium sulfate in boiled water for 5 days. The mice were killed on the 5th, 7th and 28th days. The concentrations of TGF-β and EGF in the homogenate of the medial colon were determined by enzyme-linked immunosorbent assay using standard kits. Results and discussion: The dalargin daily subcutaneous administration (dose of 100 μg/kg) for 7 days led to a decrease in TGF-β levels on the 5th and 7th days compared to the control group. In chronic UC, the concentration of TGF-β was higher than in the control group. The EGF concentration was increased in mice with UC treated with dalargin throughout the experiment. There were no differences in dalargin and sulfasalazine effects on the content of TGF-β, and the concentration of EGF throughout the experiment was significantly higher in the animals treated with dalargin. Conclusion: Effect of dalargin on the TGF-β and EGF concentrations was explained by its stimulating action to opioid μ-receptors localized on immune cells of the colon.

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Genetically modified animal models of hereditary diseases for testing of gene-directed therapy

Cited by 2 publications

References 92 publications

CRISPR/Cas9-generated mouse model with humanizing single-base substitution in the Gnao1 for safety studies of RNA therapeutics

CRISPR/Cas9-generated mouse model with humanizing single-base substitution in the Gnao1 for safety studies of RNA therapeutics

The effect of dalargin on growth factors content in experimental ulcerative colitis

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