International journal of molecular sciences

Testing gene therapy to deliver a skin-repair gene in rats and pigs and checking its safety for treating ARCI

Updated

Abstract

A significant increase in TGM1 mRNA, protein levels, and enzymatic activity was observed with the AAV2-TGM1 gene therapy.

  • Adeno-associated viral vector AAV2-TGM1 targets caused by TGM1 mutations.
  • In vitro studies showed enhanced TGM1 mRNA and protein levels in several cell types.
  • In vivo applications in rats and pigs demonstrated increased TGM1 protein levels in the skin.
  • Safety assessments indicated no significant histological, biochemical, or cellular changes.

Simplified

Key numbers

16.3×
Increase in TGM1 Activity
Activity in transduced HEK293 cells vs. native cells.
1.41×
Increase in TGM1 Protein Expression
Protein expression in rat epidermis after topical application.
4.21×
Increase in Fluorescence Intensity
Fluorescence intensity compared to control group.

Full Text

What this is

  • This research evaluates the efficacy and safety of AAV2-TGM1 gene therapy for , a severe skin disorder caused by TGM1 deficiency.
  • The study involved in vitro tests on various human cell lines and in vivo tests on rats and pigs to assess transgene expression and safety.
  • Findings indicate significant increases in TGM1 expression and activity following treatment, with no major adverse effects observed.

Essence

  • AAV2-TGM1 gene therapy effectively increases TGM1 expression in skin cells of rats and pigs, showing promise for treating without significant toxicity.

Key takeaways

  • AAV2-TGM1 treatment led to a 16.3-fold increase in TGM1 enzymatic activity in HEK293 cells compared to native cells, indicating effective gene delivery.
  • In vivo studies in rats showed a 1.41-fold increase in TGM1 protein expression following topical application of AAV2-TGM1, confirming its functionality.
  • No significant histological changes or signs of toxicity were observed in the skin or internal organs of treated rats and pigs, supporting the safety of AAV2-TGM1.

Caveats

  • The study did not assess long-term effects or chronic toxicity, which are important for evaluating the full safety profile of AAV2-TGM1.
  • Variability in expression levels and the transient nature of the gene expression highlight the need for further optimization of the delivery method.

Definitions

  • Lamellar ichthyosis: A severe hereditary skin disorder characterized by thick, scaly skin due to TGM1 enzyme deficiency.
  • Adeno-associated virus (AAV): A viral vector used in gene therapy that has low immunogenicity and does not integrate into the host genome.

Simplified

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