Mitochondrial Metabolism in a Large-Animal Model of Huntington Disease: The Hunt for Biomarkers in the Spermatozoa of Presymptomatic Minipigs
Jazyk angličtina Země Švýcarsko Médium print-electronic
Typ dokumentu časopisecké články
PubMed
28633139
DOI
10.1159/000475467
PII: 000475467
Knihovny.cz E-zdroje
- Klíčová slova
- Huntington disease, Large-animal model, Mitochondrial metabolism, Mutant huntingtin, Spermatozoa,
- MeSH
- dýchání MeSH
- geneticky modifikovaná zvířata MeSH
- Huntingtonova nemoc komplikace genetika patologie MeSH
- kyseliny trikarboxylové metabolismus MeSH
- lidé MeSH
- miniaturní prasata MeSH
- mitochondriální proteiny metabolismus MeSH
- mitochondrie metabolismus MeSH
- mutace genetika MeSH
- oxidativní fosforylace MeSH
- prasata MeSH
- protein huntingtin genetika MeSH
- pyruvátdehydrogenasový komplex metabolismus MeSH
- sperma metabolismus MeSH
- spermie metabolismus patologie MeSH
- trinukleotidové repetice genetika MeSH
- věkové faktory MeSH
- zvířata MeSH
- Check Tag
- lidé MeSH
- mužské pohlaví MeSH
- zvířata MeSH
- Publikační typ
- časopisecké články MeSH
- Názvy látek
- HTT protein, human MeSH Prohlížeč
- kyseliny trikarboxylové MeSH
- mitochondriální proteiny MeSH
- protein huntingtin MeSH
- pyruvátdehydrogenasový komplex MeSH
BACKGROUND: Huntington disease (HD) is a fatal neurodegenerative disorder involving reduced muscle coordination, mental and behavioral changes, and testicular degeneration. In order to further clarify the decreased fertility and penetration ability of the spermatozoa of transgenic HD minipig boars (TgHD), we applied a set of mitochondrial metabolism (MM) parameter measurements to this promising biological material, which can be collected noninvasively in longitudinal studies. OBJECTIVE: We aimed to optimize methods for MM measurements in spermatozoa and to establish possible biomarkers of HD in TgHD spermatozoa expressing the N-terminal part of mutated human huntingtin. METHODS: Semen samples from 12 TgHD and wild-type animals, aged 12-65 months, were obtained repeatedly during the study. Respiration was measured by polarography, MM was assessed by the detection of oxidation of radiolabeled substrates (mitochondrial energy-generating system; MEGS), and the content of the oxidative phosphorylation system subunits was detected by Western blot. Three possibly interfering factors were statistically analyzed: the effect of HD, generation and aging. RESULTS: We found 5 MM parameters which were significantly diminished in TgHD spermatozoa and propose 3 specific MEGS incubations and complex I-dependent respiration as potential biomarkers of HD in TgHD spermatozoa. CONCLUSIONS: Our results suggest a link between the gain of toxic function of mutated huntingtin in TgHD spermatozoa and the observed MM and/or glycolytic impairment. We determined 4 biomarkers useful for HD phenotyping and experimental therapy monitoring studies in TgHD minipigs.
Citace poskytuje Crossref.org
Large Animal Models of Huntington's Disease: What We Have Learned and Where We Need to Go Next
Transgenic minipig model of Huntington's disease exhibiting gradually progressing neurodegeneration
