Počet záznamů: 1  

LONGITUDINAL VIEW OF MITOCHONDRIAL BIOENERGETICS IN SKELETAL MUSCLE OF PREMANIFEST TRANSGENIC MINIPIG MODEL FOR HUNTINGTON'S DISEASE

    1.
    SYSNO ASEP0498981
    Druh ASEPA - Abstrakt
    Zařazení RIVO - Ostatní
    NázevLONGITUDINAL VIEW OF MITOCHONDRIAL BIOENERGETICS IN SKELETAL MUSCLE OF PREMANIFEST TRANSGENIC MINIPIG MODEL FOR HUNTINGTON'S DISEASE
    Tvůrce(i) Rodinová, M. (CZ)
    Křížová, J. (CZ)
    Štufková, H. (CZ)
    Bohuslavová, Božena (UZFG-Y) ORCID
    Askeland, G. (NO)
    Dosoudilová, Z. (CZ)
    Juhás, Štefan (UZFG-Y) RID, ORCID
    Ellederová, Zdeňka (UZFG-Y) RID, ORCID
    Zeman, J. (CZ)
    Eide, L. (NO)
    Motlík, Jan (UZFG-Y) RID, ORCID
    Hansíková, H. (CZ)
    Zdroj.dok.Journal of Neurology Neurosurgery and Psychiatry - ISSN 0022-3050
    Roč. 89, S1 (2018), A23-A24
    Poč.str.2 s.
    AkcePlenary Meeting of the European Huntington´s Disease Network (EHDN)
    Datum konání14.09.2018 - 16.09.2018
    Místo konáníVienna
    ZeměAT - Rakousko
    Typ akceEUR
    Jazyk dok.eng - angličtina
    Země vyd.GB - Velká Británie
    Klíč. slovatransgenic minipig model ; Huntington´s disease
    Vědní obor RIVFH - Neurologie, neurochirurgie, neurovědy
    Obor OECDNeurosciences (including psychophysiology
    CEPLO1609 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
    Institucionální podporaUZFG-Y - RVO:67985904
    UT WOS000446126000065
    DOI10.1136/jnnp-2018-EHDN.64
    AnotaceSkeletal muscle wasting and atrophy is one of the severe clinical impairment connected with progression of Huntington’s disease (HD). Mitochondrial dysfunction may play significant role in aetiology of the HD but exact condition of mitochondria as the major energy-producing organelles during development of the HD in muscle has not yet been carefully investigated.
    The aim of the study was the longitudinal monitoring of mitochondrial function in skeletal muscle of transgenic minipigs expressing the N-terminal part of human mutated huntingtin (TgHD). We investigated muscle (q. femoris) from 24, 36, 48 and 66 month old TgHD and age-matched wild-type (WT) siblings (6 TgHD + 6 WT in each age).
    Results Ultrastructural analyses in 48 month-old TgHD revealed local disorganization of myotubules, dilatation of sarcoplasmic reticulum, increased content of glycogen, higher density of mitochondria and incipient cristae disarrangement in comparison with WT. Activity of CS and RCC complex IV were significantly decreased in TgHD. Oxygen consumption showed significantly decreased ratio CII/CIV in TgHD contrary to WT. Protein analyses proved lower content of OPA1 protein which is necessary for correct mitochondrial fusion and quality control from 48 month-old TgHD animals. Genotype specific effect on mitochondrial DNA (mtDNA) damage but not on mtDNA copy number or nuclear DNA damage in TgHD was observed in the age of 66 month.
    Conclusions Our results showed that mitochondrial function in muscle decreases slowly during premanifest stage of HD and biochemical phenotype appears at the age of 48 months. Mitochondrial disturbances may contribute to energetic depression of skeletal muscle in HD and are in concordance with mobility problems observed in this large animal model after 48 month of life.
    PracovištěÚstav živočišné fyziologie a genetiky
    KontaktJana Zásmětová, knihovna@iapg.cas.cz, Tel.: 315 639 554
    Rok sběru2019
Počet záznamů: 1  

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