Počet záznamů: 1  

Aberrant DR5 transport through disruption of lysosomal function suggests a novel mechanism for receptor activation

    1.
    SYSNO ASEP0471956
    Druh ASEPJ - Článek v odborném periodiku
    Zařazení RIVJ - Článek v odborném periodiku
    Poddruh JČlánek ve WOS
    NázevAberrant DR5 transport through disruption of lysosomal function suggests a novel mechanism for receptor activation
    Tvůrce(i) Akpinar, B. (SE)
    Šafaříková, Barbora (BFU-R)
    Lauková, Jarmila (BFU-R)
    Debnath, S. (SE)
    Vaculová, Alena (BFU-R) RID, ORCID
    Zhivotovsky, B. (SE)
    Olsson, M. (SE)
    Celkový počet autorů7
    Zdroj.dok.OncoTarget. - : Impact Journals LLC - ISSN 1949-2553
    Roč. 7, č. 36 (2016), s. 58286-58301
    Poč.str.16 s.
    Forma vydáníTištěná - P
    Jazyk dok.eng - angličtina
    Země vyd.US - Spojené státy americké
    Klíč. slovadeath ligand trail ; dependent apoptosis ; cancer-cells ; autophagy
    Vědní obor RIVBO - Biofyzika
    CEPGA15-06650S GA ČR - Grantová agentura ČR
    Institucionální podporaBFU-R - RVO:68081707
    UT WOS000387153200067
    DOI https://doi.org/10.18632/oncotarget.11073
    AnotaceTo examine reciprocal or unilateral implications between two cell destruction processes, autophagy and apoptosis, in 5-Fluorouracil (5-FU)-treated tumor cells, a combination of chemical inhibitors, RNAi and genetic approaches were used. In contrast to cancer cells harboring obstructed apoptosis, either at the DISC or the mitochondrial level, p53-deficiency generated signs of autophagy deregulation upon chemotherapy. On the other, hand disruption of lysosomal function by chloroquine, caused a profound decrease in apoptotic markers appearing in response to 5-FU. DR5, which is essential for 5-FU-induced apoptosis, accumulated in lysosomes and autophagosomes upon chloroquine treatment. Since neither 3-MA, RNAi of critical autophagy regulators or inhibition of cathepsins reversed apoptosis in a similar manner, it is likely that not autophagy per se but rather correct receptor transport is an important factor for 5-FU cytotoxicity. We found that apoptosis generated by TRAIL, the cognate ligand for DR5, remained unchanged upon chloroquine lysosomal interference, indicating that 5-FU activates the receptor by a discrete mechanism. In support, depletion of membrane cholesterol or hampering cholesterol transport drastically reduced 5-FU cytotoxicity. We conclude that targeting of lysosomes by chloroquine deregulates DR5 trafficking and abrogates 5-FU-but not TRAIL-stimulated cell elimination, hence suggesting a novel mechanism for receptor activation.
    PracovištěBiofyzikální ústav
    KontaktJana Poláková, polakova@ibp.cz, Tel.: 541 517 244
    Rok sběru2017
Počet záznamů: 1  

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