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How the molecular weight affects the in vivo fate of exogenous hyaluronan delivered intravenously: A stable-isotope labelling strategy

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    0542790 - BFÚ 2022 RIV GB eng J - Journal Article
    Simek, M. - Nešporová, K. - Kocurková, Anna - Foglova, T. - Ambrožová, Gabriela - Velebný, V. - Kubala, Lukáš - Hermannová, M.
    How the molecular weight affects the in vivo fate of exogenous hyaluronan delivered intravenously: A stable-isotope labelling strategy.
    Carbohydrate Polymers. Roč. 263, JUL 1 2021 (2021), č. článku 117927. ISSN 0144-8617. E-ISSN 1879-1344
    Institutional support: RVO:68081707
    Keywords : chondroitin sulfate * acid * size * pharmacokinetics * biodistribution
    OECD category: Organic chemistry
    Impact factor: 10.723, year: 2021
    Method of publishing: Limited access
    https://reader.elsevier.com/reader/sd/pii/S0144861721003143?token=3B1E30F1EFFA8B688701DCC15BDDC999A5E187E791E15A519C7A4D380A7A798486099FF4C0AB22482C63D972D480C238&originRegion=eu-west-1&originCreation=20210528071650

    There is inconsistent information regarding the size effects of exogenously given hyaluronan on its in vivo fate. The data are often biased by the poor quality of hyaluronan and non-ideal labelling strategies used for resolving exogenous/endogenous hyaluronan, which only monitor the label and not hyaluronan itself. To overcome these drawbacks and establish the pharmacokinetics of intravenous hyaluronan in relation to its Mw, 13C-labelled HA of five Mws from 13.6?1562 kDa was prepared and administered to mice at doses 25-50 mg kg?1. The elimination efficiency increased with decreasing Mw. Low Mw hyaluronan was rapidly eliminated as small hyaluronan fragments in urine, while high Mw hyaluronan exhibited saturable kinetics and complete metabolization within 48 h. All tested Mws exhibited a similar uptake by liver cells and metabolization into activated sugars. 13Clabelling combined with LC?MS provides an excellent approach to elucidating in vivo fate and biological activities of hyaluronan.
    Permanent Link: http://hdl.handle.net/11104/0320137

     
     
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