Astrocytic glycogen accumulation drives the pathophysiology of neurodegeneration in Lafora disease

doi:10.1093/brain/awab110

. 2021 Sep 4;144(8):2349-2360.

doi: 10.1093/brain/awab110.

Astrocytic glycogen accumulation drives the pathophysiology of neurodegeneration in Lafora disease

Jordi Duran^{1

2}, Arnau Hervera^{3

4

5

6}, Kia H Markussen⁷, Olga Varea¹, Iliana López-Soldado¹, Ramon C Sun⁸, Jose Antonio Del Río^{3

4

5

6}, Matthew S Gentry⁷, Joan J Guinovart^{1

2

9}

Affiliations

¹ Institute for Research in Biomedicine (IRB Barcelona), The Barcelona Institute of Science and Technology, Barcelona 08028, Spain.
² Centro de Investigación Biomédica en Red de Diabetes y Enfermedades Metabólicas Asociadas (CIBERDEM), Madrid 28029, Spain.
³ Institute for Bioengineering of Catalonia (IBEC), The Barcelona Institute of Science and Technology, Barcelona 08028, Spain.
⁴ Centro de Investigación Biomédica en Red sobre Enfermedades Neurodegenerativas (CIBERNED), Madrid 28031, Spain.
⁵ Department of Cell Biology, Physiology and Immunology, Universitat de Barcelona, Barcelona 08028, Spain.
⁶ Institute of Neurosciences, University of Barcelona, Barcelona 08028, Spain.
⁷ Department of Molecular and Cellular Biochemistry, University of Kentucky College of Medicine, Lexington, KY 40536, USA.
⁸ Department of Neuroscience, University of Kentucky College of Medicine, Lexington, KY 40536, USA.
⁹ Department of Biochemistry and Molecular Biomedicine, Universitat de Barcelona, Barcelona 08028, Spain.

PMID: 33822008
PMCID: PMC8418345
DOI: 10.1093/brain/awab110

Astrocytic glycogen accumulation drives the pathophysiology of neurodegeneration in Lafora disease

Jordi Duran et al. Brain. 2021.

. 2021 Sep 4;144(8):2349-2360.

doi: 10.1093/brain/awab110.

Authors

Affiliations

¹ Institute for Research in Biomedicine (IRB Barcelona), The Barcelona Institute of Science and Technology, Barcelona 08028, Spain.
² Centro de Investigación Biomédica en Red de Diabetes y Enfermedades Metabólicas Asociadas (CIBERDEM), Madrid 28029, Spain.
³ Institute for Bioengineering of Catalonia (IBEC), The Barcelona Institute of Science and Technology, Barcelona 08028, Spain.
⁴ Centro de Investigación Biomédica en Red sobre Enfermedades Neurodegenerativas (CIBERNED), Madrid 28031, Spain.
⁵ Department of Cell Biology, Physiology and Immunology, Universitat de Barcelona, Barcelona 08028, Spain.
⁶ Institute of Neurosciences, University of Barcelona, Barcelona 08028, Spain.
⁷ Department of Molecular and Cellular Biochemistry, University of Kentucky College of Medicine, Lexington, KY 40536, USA.
⁸ Department of Neuroscience, University of Kentucky College of Medicine, Lexington, KY 40536, USA.
⁹ Department of Biochemistry and Molecular Biomedicine, Universitat de Barcelona, Barcelona 08028, Spain.

PMID: 33822008
PMCID: PMC8418345
DOI: 10.1093/brain/awab110

Abstract

The hallmark of Lafora disease, a fatal neurodegenerative disorder, is the accumulation of intracellular glycogen aggregates called Lafora bodies. Until recently, it was widely believed that brain Lafora bodies were present exclusively in neurons and thus that Lafora disease pathology derived from their accumulation in this cell population. However, recent evidence indicates that Lafora bodies are also present in astrocytes. To define the role of astrocytic Lafora bodies in Lafora disease pathology, we deleted glycogen synthase specifically from astrocytes in a mouse model of the disease (malinKO). Strikingly, blocking glycogen synthesis in astrocytes-thus impeding Lafora bodies accumulation in this cell type-prevented the increase in neurodegeneration markers, autophagy impairment, and metabolic changes characteristic of the malinKO model. Conversely, mice that over-accumulate glycogen in astrocytes showed an increase in these markers. These results unveil the deleterious consequences of the deregulation of glycogen metabolism in astrocytes and change the perspective that Lafora disease is caused solely by alterations in neurons.

Keywords: Lafora disease; epilepsy; glycogen; neurodegeneration; neuroinflammation.

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Figures

**Figure 1**
**Accumulation of glycogen in the brains of 3-month-old mice.** Lafora bodies are abundant in malin^KO hippocampi but greatly diminished in malin^KO+MGS^Gfap-KO hippocampi. (A) Low and high power photomicrographs illustrating the distribution of Lafora bodies after periodic acid-Schiff (PAS) staining and MGS immunostaining of the hippocampi of 3-month-old littermates from the different groups. Scale bar = 100 μm. (B) Glycogen content of total brain. Control (n = 7), malin^KO (n = 7), malin^KO+MGS^Gfap-KO (n = 6). Data are expressed as mean ± SEM. ****P < 0.0001.

**Figure 2**
**Malin^KO+MGS^Gfap-KO brains contain nLBs but not CAL.** MGS immunostainings of the CA3-CA2 region of the hippocampus (*top*), the cortex (*middle*) and the cerebellum (*bottom*) of 3-month-old mice. Scale bar = 100 μm.

**Figure 3**
**Accumulation of proteins is prevented in malin^KO+MGS^Gfap-KO brains.** Western blotting for MGS, laforin and p62 of total brain homogenates of 3-month-old mice. (A) Representative blots. (B) Quantification of the bands normalized to Revert. Data are expressed as mean ± SEM. *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001; n.s. = non-significant. n = 4 animals per group. Revert was used as loading control.

**Figure 4**
**Analysis of brain damage in malin^KO+MGS^Gfap-KO mice.** Neuroinflammation markers are increased in the brains of old malin^KO mice but normalized in malin^KO+MGS^Gfap-KO mice. (A) GFAP and Iba1 immunostainings of hippocampi from the different groups. (B) Quantification of hippocampal area of the immunostainings. Data are expressed as mean ± SEM of percentage of positive pixels [control (n = 5), malin^KO (n = 7), malin^KO+MGS^Gfap-KO (n = 7)]. (C) Quantitative PCR analysis of genes involved in the inflammatory response. Data are expressed as mean ± SEM of 2^ΔΔCt in relative units for each genotype analysed [control (n = 5), malin^KO (n = 5), malin^KO+MGS^Gfap-KO (n = 6)]. **P < 0.01; ***P < 0.001; ****P < 0.0001; n.s. = non-significant.

**Figure 5**
**Accumulation of glycogen in 9A-MGS^Gfap mice.** (A) PAS staining and MGS immunostaining of 9A-MGS^Gfap in consecutive serial coronal sections. (B) Glycogen content of total brain (n = 6 animals per group). Data are expressed as mean ± SEM. ****P < 0.0001. (C) Western blotting for MGS, laforin and p62 of total brain homogenates. Revert was used as loading control.

**Figure 6**
**Analysis of brain damage in 9A-MGS^Gfap mice.** Neuroinflammation markers are increased in the brains of 9A-MGS^Gfap mice. (A) GFAP and Iba1 immunostainings of hippocampi. (B) Quantification of the hippocampal area of the immunostainings. Data are expressed as mean ± SEM of percentage of positive pixels [control (n = 5), 9A-MGS^Gfap (n = 6)]. (C) Quantitative PCR analysis of genes involved in the inflammatory response. Data are expressed as mean ± SEM of 2^ΔΔCt in relative units for each genotype analysed (n = 6 animals per group). **P < 0.01. ***P < 0.001. ****P < 0.0001.

**Figure 7**
**Study of kainate-induced epilepsy.** Eleven-month-old mice were subjected to three kainate injections (8 mg/kg every 30 min), and epileptic responses were analysed for 180 min after the first injection. (A) Percentage of mice reaching seizure Stages I to VI and kainate-induced mortality. (B) Percentage of time spent in each stage during the course of the experiment. Data are expressed as average ± SEM. n = 6 mice/group. Two-way ANOVA P-values display *post hoc* Bonferroni differences. (C) Number of seizures experienced per animal divided by time segments after the first, second and third kainate injections. Data are expressed as average ± SEM. n = 6 animals per group. Two-way ANOVA P-values display *post hoc* Bonferroni differences.

**Figure 8**
**Metabolic profiles.** (A) Sparse partial least squares-discriminant analysis (sPLS-DA) multivariate analysis of control (red), malin^KO (blue) and malin^KO+MGS^Gfap-KO (green) brains. (B) Heat map clustering showing the 10 most affected metabolites from sPLS-DA multivariate analysis.

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References

1. Duran J, Saez I, Gruart A, Guinovart JJ, Delgado-Garcia JM.. Impairment in long-term memory formation and learning-dependent synaptic plasticity in mice lacking glycogen synthase in the brain. J Cereb Blood Flow Metab. 2013;33(4):550–556. - PMC - PubMed
1. Lopez-Ramos JC, Duran J, Gruart A, Guinovart JJ, Delgado-Garcia JM.. Role of brain glycogen in the response to hypoxia and in susceptibility to epilepsy. Front Cell Neurosci. 2015;9:431. - PMC - PubMed
1. Saez I, Duran J, Sinadinos C, et al.Neurons have an active glycogen metabolism that contributes to tolerance to hypoxia. J Cereb Blood Flow Metab. 2014;34(6):945–955. - PMC - PubMed
1. Duran J, Gruart A, Varea O, López-Soldado I, Delgado-García JM, Guinovart JJ.. Lack of neuronal glycogen impairs memory formation and learning-dependent synaptic plasticity in mice. Front Cell Neurosci. 2019;13:374. - PMC - PubMed
1. Duran J, Brewer MK, Hervera A, et al.Lack of astrocytic glycogen alters synaptic plasticity but not seizure susceptibility. Mol Neurobiol. 2020;57(11):4657–4666. - PMC - PubMed

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[1] Duran J, Saez I, Gruart A, Guinovart JJ, Delgado-Garcia JM.. Impairment in long-term memory formation and learning-dependent synaptic plasticity in mice lacking glycogen synthase in the brain. J Cereb Blood Flow Metab. 2013;33(4):550–556. - PMC - PubMed

[2] Duran J, Saez I, Gruart A, Guinovart JJ, Delgado-Garcia JM.. Impairment in long-term memory formation and learning-dependent synaptic plasticity in mice lacking glycogen synthase in the brain. J Cereb Blood Flow Metab. 2013;33(4):550–556. - PMC - PubMed

[3] Lopez-Ramos JC, Duran J, Gruart A, Guinovart JJ, Delgado-Garcia JM.. Role of brain glycogen in the response to hypoxia and in susceptibility to epilepsy. Front Cell Neurosci. 2015;9:431. - PMC - PubMed

[4] Lopez-Ramos JC, Duran J, Gruart A, Guinovart JJ, Delgado-Garcia JM.. Role of brain glycogen in the response to hypoxia and in susceptibility to epilepsy. Front Cell Neurosci. 2015;9:431. - PMC - PubMed

[5] Saez I, Duran J, Sinadinos C, et al.Neurons have an active glycogen metabolism that contributes to tolerance to hypoxia. J Cereb Blood Flow Metab. 2014;34(6):945–955. - PMC - PubMed

[6] Saez I, Duran J, Sinadinos C, et al.Neurons have an active glycogen metabolism that contributes to tolerance to hypoxia. J Cereb Blood Flow Metab. 2014;34(6):945–955. - PMC - PubMed

[7] Duran J, Gruart A, Varea O, López-Soldado I, Delgado-García JM, Guinovart JJ.. Lack of neuronal glycogen impairs memory formation and learning-dependent synaptic plasticity in mice. Front Cell Neurosci. 2019;13:374. - PMC - PubMed

[8] Duran J, Gruart A, Varea O, López-Soldado I, Delgado-García JM, Guinovart JJ.. Lack of neuronal glycogen impairs memory formation and learning-dependent synaptic plasticity in mice. Front Cell Neurosci. 2019;13:374. - PMC - PubMed

[9] Duran J, Brewer MK, Hervera A, et al.Lack of astrocytic glycogen alters synaptic plasticity but not seizure susceptibility. Mol Neurobiol. 2020;57(11):4657–4666. - PMC - PubMed

[10] Duran J, Brewer MK, Hervera A, et al.Lack of astrocytic glycogen alters synaptic plasticity but not seizure susceptibility. Mol Neurobiol. 2020;57(11):4657–4666. - PMC - PubMed

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Astrocytic glycogen accumulation drives the pathophysiology of neurodegeneration in Lafora disease

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Astrocytic glycogen accumulation drives the pathophysiology of neurodegeneration in Lafora disease

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