Publicaciones científicas

Liver Expression of a MiniATP7B Gene Results in Long-Term Restoration of Copper Homeostasis in a Wilson Disease Model in Mice

20-mar-2019 | Revista: Hepatology

Oihana Murillo, Daniel Moreno, Cristina Gazquez, Miren Barberia, Itziar Cenzano, Iñigo Navarro, Iker Uriarte, Victor Sebastian, Manuel Arruebo, Veronica Ferrer, Bernard Bénichou, Jean Philippe Combal, Jesus Prieto, Ruben Hernandez-Alcoceba, Gloria Gonzalez Aseguinolaza

Abstract

Gene therapy with an adeno-associated vector (AAV) serotype 8 encoding the human ATPase copper-transporting beta polypeptide (ATP7B) complementary DNA (cDNA; AAV8-ATP7B) is able to provide long-term copper metabolism correction in 6-week-old male Wilson disease (WD) mice. However, the size of the genome (5.2 kilobases [kb]) surpasses the optimal packaging capacity of the vector, which resulted in low-yield production; in addition, further analyses in WD female mice and in animals with a more advanced disease revealed reduced therapeutic efficacy, as compared to younger males.

To improve efficacy of the treatment, an optimized shorter AAV vector was generated, in which four out of six metal-binding domains (MBDs) were deleted from the ATP7B coding sequence, giving rise to the miniATP7B protein (Δ57-486-ATP7B). In contrast to AAV8-ATP7B, AAV8-miniATP7B could be produced at high titers and was able to restore copper homeostasis in 6- and 12-week-old male and female WD mice.

In addition, a recently developed synthetic AAV vector, AAVAnc80, carrying the miniATP7B gene was similarly effective at preventing liver damage, restoring copper homeostasis, and improving survival 1 year after treatment. Transduction of approximately 20% of hepatocytes was sufficient to normalize copper homeostasis, suggesting that corrected hepatocytes are acting as a sink to eliminate excess of copper. Importantly, administration of AAVAnc80-miniATP7B was safe in healthy mice and did not result in copper deficiency.

Conclusion: In summary, gene therapy using an optimized therapeutic cassette in different AAV systems provides long-term correction of copper metabolism regardless of sex or stage of disease in a clinically relevant WD mouse model. These results pave the way for the implementation of gene therapy in WD patients.

CITA DEL ARTÍCULO  Hepatology. 2019 Jul;70(1):108-126. doi: 10.1002/hep.30535. Epub 2019 Mar 20.

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Nuestros autores

Dra. Oihana Murillo Sauca
Investigadora Asociada Programa de Investigación de Terapia Génica y Regulación de la Expresión Génica
Daniel Moreno Luqui
Técnico de Investigación Programa de Investigación de Terapia Génica y Regulación de la Expresión Génica
Cristina Gázquez López
Técnico de laboratorio Programa de Investigación de Terapia Génica y Regulación de la Expresión Génica
Miren Barbería Urteaga
Predoctoral Programa de Investigación de Terapia Génica y Regulación de la Expresión Génica
Dra. Itziar Cenzano Armendáriz
Posdoctoral Grupo de Investigación en Hematología Traslacional
Iker Uriarte Díaz-Varela
Investigador Adscrito a Proyecto Programa de Investigación de Hepatología
Dr. Rubén Hernández Alcoceba Ver Curriculum
Investigador Programa de Investigación de Terapia Génica y Regulación de la Expresión Génica
Dra. Gloria González Aseguinolaza Ver Curriculum
Investigadora | Investigadora principal Grupo de Investigación en Terapia Génica de Enfermedades Hepáticas