Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome

Ana Ricobaraza; Maria Bunuales; Manuela Gonzalez-Aparicio; Saja Fadila; Moran Rubinstein; Irene Vides-Urrestarazu; Julliana Banderas; Noemi Sola-Sevilla; Rocio Sanchez-Carpintero; Jose Luis Lanciego; Elvira Roda; Adriana Honrubia; Patricia Arnaiz; Ruben Hernandez-Alcoceba

doi:10.1007/s00109-023-02383-8

Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome

Ana Ricobaraza, Maria Bunuales, Manuela Gonzalez-Aparicio, Saja Fadila, Moran Rubinstein, Irene Vides-Urrestarazu, Julliana Banderas, Noemi Sola-Sevilla, Rocio Sanchez-Carpintero, Jose Luis Lanciego, Elvira Roda, Adriana Honrubia, Patricia Arnaiz, Ruben Hernandez-Alcoceba^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Abstract: The SCN1A gene encodes the alpha subunit of a voltage-gated sodium channel (Na_v1.1), which is essential for the function of inhibitory neurons in the brain. Mutations in this gene cause severe encephalopathies such as Dravet syndrome (DS). Upregulation of SCN1A expression by different approaches has demonstrated promising therapeutic effects in preclinical models of DS. Limiting the effect to inhibitory neurons may contribute to the restoration of brain homeostasis, increasing the safety and efficacy of the treatment. In this work, we have evaluated different approaches to obtain preferential expression of the full SCN1A cDNA (6 Kb) in GABAergic neurons, using high-capacity adenoviral vectors (HC-AdV). In order to favour infection of these cells, we considered ErbB4 as a surface target. Incorporation of the EGF-like domain from neuregulin 1 alpha (NRG1α) in the fiber of adenovirus capsid allowed preferential infection in cells lines expressing ErbB4. However, it had no impact on the infectivity of the vector in primary cultures or in vivo. For transcriptional control of transgene expression, we developed a regulatory sequence (DP3V) based on the Distal-less homolog enhancer (Dlx), the vesicular GABA transporter (VGAT) promoter, and a portion of the SCN1A gene. The hybrid DP3V promoter allowed preferential expression of transgenes in GABAergic neurons both in vitro and in vivo. A new HC-AdV expressing SCN1A under the control of this promoter showed improved survival and amelioration of the epileptic phenotype in a DS mouse model. These results increase the repertoire of gene therapy vectors for the treatment of DS and indicate a new avenue for the refinement of gene supplementation in this disease. Key messages: Adenoviral vectors can deliver the SCN1A cDNA and are amenable for targeting.An adenoviral vector displaying an ErbB4 ligand in the capsid does not target GABAergic neurons.A hybrid promoter allows preferential expression of transgenes in GABAergic neurons.Preferential expression of SCN1A in GABAergic cells is therapeutic in a Dravet syndrome model.

Original language	English
Pages (from-to)	1587-1601
Number of pages	15
Journal	Journal of Molecular Medicine
Volume	101
Issue number	12
DOIs	https://doi.org/10.1007/s00109-023-02383-8
State	Published - Dec 2023

Funding

Funders	Funder number
American Dravet Syndrome Foundation
Apoyo Dravet Foundation
Desafia Dravet Association
Fundacion Sindrome de Dravet Spain	EU-PRTR RD21/0017/0034
Yoran Institute for Human Genome Research
E-Rare
Chartered Institute of Management Accountants
Israel Science Foundation	1454/17, 214/22
Tel Aviv University
Universidad de Navarra

Keywords

Adenoviral vector
DP3V
Dlx
Dravet syndrome
Epileptic encephalopathy
ErbB4
GABAergic neuron
Nav1.1
SCN1A

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10.1007/s00109-023-02383-8

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Ricobaraza, A., Bunuales, M., Gonzalez-Aparicio, M., Fadila, S., Rubinstein, M., Vides-Urrestarazu, I., Banderas, J., Sola-Sevilla, N., Sanchez-Carpintero, R., Lanciego, J. L., Roda, E., Honrubia, A., Arnaiz, P., & Hernandez-Alcoceba, R. (2023). Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome. Journal of Molecular Medicine, 101(12), 1587-1601. https://doi.org/10.1007/s00109-023-02383-8

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title = "Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome",

abstract = "Abstract: The SCN1A gene encodes the alpha subunit of a voltage-gated sodium channel (Nav1.1), which is essential for the function of inhibitory neurons in the brain. Mutations in this gene cause severe encephalopathies such as Dravet syndrome (DS). Upregulation of SCN1A expression by different approaches has demonstrated promising therapeutic effects in preclinical models of DS. Limiting the effect to inhibitory neurons may contribute to the restoration of brain homeostasis, increasing the safety and efficacy of the treatment. In this work, we have evaluated different approaches to obtain preferential expression of the full SCN1A cDNA (6 Kb) in GABAergic neurons, using high-capacity adenoviral vectors (HC-AdV). In order to favour infection of these cells, we considered ErbB4 as a surface target. Incorporation of the EGF-like domain from neuregulin 1 alpha (NRG1α) in the fiber of adenovirus capsid allowed preferential infection in cells lines expressing ErbB4. However, it had no impact on the infectivity of the vector in primary cultures or in vivo. For transcriptional control of transgene expression, we developed a regulatory sequence (DP3V) based on the Distal-less homolog enhancer (Dlx), the vesicular GABA transporter (VGAT) promoter, and a portion of the SCN1A gene. The hybrid DP3V promoter allowed preferential expression of transgenes in GABAergic neurons both in vitro and in vivo. A new HC-AdV expressing SCN1A under the control of this promoter showed improved survival and amelioration of the epileptic phenotype in a DS mouse model. These results increase the repertoire of gene therapy vectors for the treatment of DS and indicate a new avenue for the refinement of gene supplementation in this disease. Key messages: Adenoviral vectors can deliver the SCN1A cDNA and are amenable for targeting.An adenoviral vector displaying an ErbB4 ligand in the capsid does not target GABAergic neurons.A hybrid promoter allows preferential expression of transgenes in GABAergic neurons.Preferential expression of SCN1A in GABAergic cells is therapeutic in a Dravet syndrome model.",

keywords = "Adenoviral vector, DP3V, Dlx, Dravet syndrome, Epileptic encephalopathy, ErbB4, GABAergic neuron, Nav1.1, SCN1A",

author = "Ana Ricobaraza and Maria Bunuales and Manuela Gonzalez-Aparicio and Saja Fadila and Moran Rubinstein and Irene Vides-Urrestarazu and Julliana Banderas and Noemi Sola-Sevilla and Rocio Sanchez-Carpintero and Lanciego, {Jose Luis} and Elvira Roda and Adriana Honrubia and Patricia Arnaiz and Ruben Hernandez-Alcoceba",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = dec,

doi = "10.1007/s00109-023-02383-8",

language = "אנגלית",

volume = "101",

pages = "1587--1601",

journal = "Journal of Molecular Medicine",

issn = "0946-2716",

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Ricobaraza, A, Bunuales, M, Gonzalez-Aparicio, M, Fadila, S, Rubinstein, M, Vides-Urrestarazu, I, Banderas, J, Sola-Sevilla, N, Sanchez-Carpintero, R, Lanciego, JL, Roda, E, Honrubia, A, Arnaiz, P & Hernandez-Alcoceba, R 2023, 'Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome', Journal of Molecular Medicine, vol. 101, no. 12, pp. 1587-1601. https://doi.org/10.1007/s00109-023-02383-8

TY - JOUR

T1 - Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome

AU - Ricobaraza, Ana

AU - Bunuales, Maria

AU - Gonzalez-Aparicio, Manuela

AU - Fadila, Saja

AU - Rubinstein, Moran

AU - Vides-Urrestarazu, Irene

AU - Banderas, Julliana

AU - Sola-Sevilla, Noemi

AU - Sanchez-Carpintero, Rocio

AU - Lanciego, Jose Luis

AU - Roda, Elvira

AU - Honrubia, Adriana

AU - Arnaiz, Patricia

AU - Hernandez-Alcoceba, Ruben

PY - 2023/12

Y1 - 2023/12

N2 - Abstract: The SCN1A gene encodes the alpha subunit of a voltage-gated sodium channel (Nav1.1), which is essential for the function of inhibitory neurons in the brain. Mutations in this gene cause severe encephalopathies such as Dravet syndrome (DS). Upregulation of SCN1A expression by different approaches has demonstrated promising therapeutic effects in preclinical models of DS. Limiting the effect to inhibitory neurons may contribute to the restoration of brain homeostasis, increasing the safety and efficacy of the treatment. In this work, we have evaluated different approaches to obtain preferential expression of the full SCN1A cDNA (6 Kb) in GABAergic neurons, using high-capacity adenoviral vectors (HC-AdV). In order to favour infection of these cells, we considered ErbB4 as a surface target. Incorporation of the EGF-like domain from neuregulin 1 alpha (NRG1α) in the fiber of adenovirus capsid allowed preferential infection in cells lines expressing ErbB4. However, it had no impact on the infectivity of the vector in primary cultures or in vivo. For transcriptional control of transgene expression, we developed a regulatory sequence (DP3V) based on the Distal-less homolog enhancer (Dlx), the vesicular GABA transporter (VGAT) promoter, and a portion of the SCN1A gene. The hybrid DP3V promoter allowed preferential expression of transgenes in GABAergic neurons both in vitro and in vivo. A new HC-AdV expressing SCN1A under the control of this promoter showed improved survival and amelioration of the epileptic phenotype in a DS mouse model. These results increase the repertoire of gene therapy vectors for the treatment of DS and indicate a new avenue for the refinement of gene supplementation in this disease. Key messages: Adenoviral vectors can deliver the SCN1A cDNA and are amenable for targeting.An adenoviral vector displaying an ErbB4 ligand in the capsid does not target GABAergic neurons.A hybrid promoter allows preferential expression of transgenes in GABAergic neurons.Preferential expression of SCN1A in GABAergic cells is therapeutic in a Dravet syndrome model.

AB - Abstract: The SCN1A gene encodes the alpha subunit of a voltage-gated sodium channel (Nav1.1), which is essential for the function of inhibitory neurons in the brain. Mutations in this gene cause severe encephalopathies such as Dravet syndrome (DS). Upregulation of SCN1A expression by different approaches has demonstrated promising therapeutic effects in preclinical models of DS. Limiting the effect to inhibitory neurons may contribute to the restoration of brain homeostasis, increasing the safety and efficacy of the treatment. In this work, we have evaluated different approaches to obtain preferential expression of the full SCN1A cDNA (6 Kb) in GABAergic neurons, using high-capacity adenoviral vectors (HC-AdV). In order to favour infection of these cells, we considered ErbB4 as a surface target. Incorporation of the EGF-like domain from neuregulin 1 alpha (NRG1α) in the fiber of adenovirus capsid allowed preferential infection in cells lines expressing ErbB4. However, it had no impact on the infectivity of the vector in primary cultures or in vivo. For transcriptional control of transgene expression, we developed a regulatory sequence (DP3V) based on the Distal-less homolog enhancer (Dlx), the vesicular GABA transporter (VGAT) promoter, and a portion of the SCN1A gene. The hybrid DP3V promoter allowed preferential expression of transgenes in GABAergic neurons both in vitro and in vivo. A new HC-AdV expressing SCN1A under the control of this promoter showed improved survival and amelioration of the epileptic phenotype in a DS mouse model. These results increase the repertoire of gene therapy vectors for the treatment of DS and indicate a new avenue for the refinement of gene supplementation in this disease. Key messages: Adenoviral vectors can deliver the SCN1A cDNA and are amenable for targeting.An adenoviral vector displaying an ErbB4 ligand in the capsid does not target GABAergic neurons.A hybrid promoter allows preferential expression of transgenes in GABAergic neurons.Preferential expression of SCN1A in GABAergic cells is therapeutic in a Dravet syndrome model.

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KW - DP3V

KW - Dlx

KW - Dravet syndrome

KW - Epileptic encephalopathy

KW - ErbB4

KW - GABAergic neuron

KW - Nav1.1

KW - SCN1A

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AN - SCOPUS:85173841877

SN - 0946-2716

VL - 101

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EP - 1601

JO - Journal of Molecular Medicine

JF - Journal of Molecular Medicine

IS - 12

ER -

Preferential expression of SCN1A in GABAergic neurons improves survival and epileptic phenotype in a mouse model of Dravet syndrome

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