FTLD Patient-Derived Fibroblasts Show Defective Mitochondrial Function and Accumulation of p62

Stina Leskelä; Dorit Hoffmann; Hannah Rostalski; Nadine Huber; Rebekka Wittrahm; Päivi Hartikainen; Ville Korhonen; Ville Leinonen; Mikko Hiltunen; Eino Solje; Anne M Remes; Annakaisa Haapasalo

doi:10.1007/s12035-021-02475-x

FTLD Patient-Derived Fibroblasts Show Defective Mitochondrial Function and Accumulation of p62

Mol Neurobiol. 2021 Nov;58(11):5438-5458. doi: 10.1007/s12035-021-02475-x. Epub 2021 Jul 30.

Authors

Stina Leskelä^#¹, Dorit Hoffmann^#¹, Hannah Rostalski¹, Nadine Huber¹, Rebekka Wittrahm², Päivi Hartikainen³, Ville Korhonen^{4

5}, Ville Leinonen^{4

5}, Mikko Hiltunen², Eino Solje^{3

6}, Anne M Remes^{7

8}, Annakaisa Haapasalo⁹

Affiliations

¹ A. I. Virtanen Institute for Molecular Sciences, University of Eastern Finland, Neulaniementie 2, 70211, Kuopio, Finland.
² Institute of Biomedicine, University of Eastern Finland, Yliopistonranta 1E, 70211, Kuopio, Finland.
³ Neuro Center, Neurology, Kuopio University Hospital, 70029, Kuopio, Finland.
⁴ Neuro Center, Neurosurgery, Kuopio University Hospital, 70029, Kuopio, Finland.
⁵ Institute of Clinical Medicine - Neurosurgery, University of Eastern Finland, Yliopistonranta 1C, 70211, Kuopio, Finland.
⁶ Institute of Clinical Medicine - Neurology, University of Eastern Finland, Yliopistonranta 1C, 70211, Kuopio, Finland.
⁷ Unit of Clinical Neuroscience, Neurology, University of Oulu, P.O. Box 8000, 90014, Oulu, Finland.
⁸ MRC Oulu, Oulu University Hospital, P.O. Box 8000, 90014, Oulu, Finland.
⁹ A. I. Virtanen Institute for Molecular Sciences, University of Eastern Finland, Neulaniementie 2, 70211, Kuopio, Finland. annakaisa.haapasalo@uef.fi.

^# Contributed equally.

Abstract

Frontotemporal lobar degeneration (FTLD) is a clinically, genetically, and neuropathologically heterogeneous group of neurodegenerative syndromes, leading to progressive cognitive dysfunction and frontal and temporal atrophy. C9orf72 hexanucleotide repeat expansion (C9-HRE) is the most common genetic cause of FTLD, but pathogenic mechanisms underlying FTLD are not fully understood. Here, we compared cellular features and functional properties, especially related to protein degradation pathways and mitochondrial function, of FTLD patient-derived skin fibroblasts from C9-HRE carriers and non-carriers and healthy donors. Fibroblasts from C9-HRE carriers were found to produce RNA foci, but no dipeptide repeat proteins, and they showed unchanged levels of C9orf72 mRNA transcripts. The main protein degradation pathways, the ubiquitin-proteasome system and autophagy, did not show alterations between the fibroblasts from C9-HRE-carrying and non-carrying FTLD patients and compared to healthy controls. An increase in the number and size of p62-positive puncta was evident in fibroblasts from both C9-HRE carriers and non-carriers. In addition, several parameters of mitochondrial function, namely, basal and maximal respiration and respiration linked to ATP production, were significantly reduced in the FTLD patient-derived fibroblasts from both C9-HRE carriers and non-carriers. Our findings suggest that FTLD patient-derived fibroblasts, regardless of whether they carry the C9-HRE expansion, show unchanged proteasomal and autophagic function, but significantly impaired mitochondrial function and increased accumulation of p62 when compared to control fibroblasts. These findings suggest the possibility of utilizing FTLD patient-derived fibroblasts as a platform for biomarker discovery and testing of drugs targeted to specific cellular functions, such as mitochondrial respiration.

Keywords: Amyotrophic lateral sclerosis; Autophagy; C9orf72; Frontotemporal lobar degeneration; Mitochondrial function; Ubiquitin–proteasome system.

MeSH terms

Autophagy
C9orf72 Protein / biosynthesis
C9orf72 Protein / genetics
Cells, Cultured
DNA Repeat Expansion
DNA-Binding Proteins / metabolism
Fibroblasts / metabolism*
Frontotemporal Lobar Degeneration / metabolism*
Frontotemporal Lobar Degeneration / pathology
Heterozygote
Humans
Mitochondria / physiology*
Nerve Tissue Proteins / biosynthesis
Nerve Tissue Proteins / genetics
Oxygen Consumption
Phosphorylation
Proteasome Endopeptidase Complex / metabolism
Protein Processing, Post-Translational
Protein Transport
Proteolysis
Sequestosome-1 Protein / metabolism*

Substances

C9orf72 Protein
C9orf72 protein, human
DNA-Binding Proteins
Nerve Tissue Proteins
SQSTM1 protein, human
Sequestosome-1 Protein
TARDBP protein, human
Proteasome Endopeptidase Complex

Abstract

MeSH terms

Substances

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