Rescue of GM3 synthase deficiency by spatially controlled, rAAV-mediated ST3GAL5 delivery
Huiya Yang, … , Kevin A. Strauss, Guangping Gao
Huiya Yang, … , Kevin A. Strauss, Guangping Gao
Published April 4, 2023
Citation Information: JCI Insight. 2023;8(9):e168688. https://doi.org/10.1172/jci.insight.168688.
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Research Article Neuroscience Therapeutics

Rescue of GM3 synthase deficiency by spatially controlled, rAAV-mediated ST3GAL5 delivery

Abstract

GM3 synthase deficiency (GM3SD) is an infantile-onset epileptic encephalopathy syndrome caused by biallelic loss-of-function mutations in ST3GAL5. Loss of ST3GAL5 activity in humans results in systemic ganglioside deficiency and severe neurological impairment. No disease-modifying treatment is currently available. Certain recombinant adeno-associated viruses (rAAVs) can cross the blood-brain barrier to induce widespread, long-term gene expression in the CNS and represent a promising therapeutic strategy. Here, we show that a first-generation rAAV-ST3GAL5 replacement vector using a ubiquitous promoter restored tissue ST3GAL5 expression and normalized cerebral gangliosides in patient-derived induced pluripotent stem cell neurons and brain tissue from St3gal5-KO mice but caused fatal hepatotoxicity when administered systemically. In contrast, a second-generation vector optimized for CNS-restricted ST3GAL5 expression, administered by either the intracerebroventricular or i.v. route at P1, allowed for safe and effective rescue of lethality and behavior impairment in symptomatic GM3SD mice up to a year. These results support further clinical development of ST3GAL5 gene therapy.

Authors

Huiya Yang, Robert H. Brown Jr., Dan Wang, Kevin A. Strauss, Guangping Gao

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Figure 8

Codelivery of ST3GAL5 and B4GALNT1 vectors normalize the St3gal5–/–/B4galnt1–/– mouse model.

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Codelivery of ST3GAL5 and B4GALNT1 vectors normalize the St3gal5–/–/B4ga...
(A) Schematic of ICV codelivery of AAV vectors expressing ST3GAL5 and B4GALNT1 cDNA, respectively, in the St3gal5–/–/B4galnt1–/– mouse model. (B) Median survival of St3gal5–/–/B4galnt1–/– mice with or without co-delivery of ST3GAL5 and B4GALNT1. Data from 8 to 20 animals are plotted as probability of survival. Statistical analysis was performed by log-rank (Mantel-Cox) test. (C) A time-course BW of postnatal pups aged 3–21 days old. Data are reported as the mean ± SD of 10 animals. Statistical analysis was performed by 2-way ANOVA, followed by Sidak’s multiple comparisons test. (D) BW of male and female mice at the postweaning stage. Data are reported as the mean ± SD of 3–5 animals. (E) Negative-geotaxis success rate of postnatal pups aged 9–15 days old. Data are normalized from 7–9 animals. (F) Quantification of rotarod assay for St3gal5+/–/B4galnt1–/– mice and scAAV9.ST3GAL5.v2 or dual vector–treated St3gal5–/–/B4galnt1–/– mice at 6 and 10 weeks old. Data are reported as the mean ± SD of 5–8 animals. (G) Representative images of mouse hindlimb from the St3gal5–/–/B4galnt1–/– mouse with dual-vector treatment or the St3gal5+/-/B4galnt1–/– mouse. **P < 0.01, ****P < 0.0001.