This technology is a therapeutic for glucose transporter type 1 (Glut1) deficiency syndrome that rescues glucose transport to the brain by delivering and integrating functional copies of the Glut1 gene into the genome.
Glut1 deficiency syndrome is a severe neurological disorder caused by mutations in the glucose transporter type 1 (Glut1) gene, which impair the expression of functional Glut1 protein in the brain and lead to reduced glucose transport across the blood-brain barrier. The lack of sufficient glucose to support the energetic demand of the brain is known to cause seizures, cognitive impairment, and other neurological symptoms. The current treatment for this disease is a ketogenic diet that allows for increased ketone metabolism to supplement the lack of glucose; however, the diet can be difficult to maintain for a lifetime, is not guaranteed to be effective, and can lead to other side effects from nutritional deficiencies. Additional therapies that directly rescue Glut1 function and the transport of glucose to the brain are needed to treat the disease.
This technology is a therapeutic for Glut1 deficiency syndrome that rescues Glut1 expression in the brain through the transport of functional copies of the Glut1 gene via adeno-associated virus (AAV), which can cross the blood-brain barrier. The functional gene gets inserted into the genome of brain cells, which allows for permanent reestablishment of Glut1 expression. Expression of functional Glut1 in the brain rescues glucose transport into the brain to support energy demands.
This technology has been validated with mouse models.
Darryl De Vivo, M.D.
Patent Pending (US20210069292)
IR CU15054
Licensing Contact: Kristin Neuman