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Prevention of Decompression Sickness by Novel Artificial Oxygen Carriers (CROSBI ID 321356)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Mayer, Dirk ; Guerrero, Francois ; Goanvec, Christelle ; Hetzel, Lisa ; Linders, Juergen ; Ljubković, Marko ; Kreczy, Alfons ; Mayer, Christian ; Kirsch, Michael ; Ferenz, Katja Bettina Prevention of Decompression Sickness by Novel Artificial Oxygen Carriers // Medicine and science in sports and exercise, 52 (2020), 10; 2127-2135. doi: 10.1249/mss.0000000000002354

Podaci o odgovornosti

Mayer, Dirk ; Guerrero, Francois ; Goanvec, Christelle ; Hetzel, Lisa ; Linders, Juergen ; Ljubković, Marko ; Kreczy, Alfons ; Mayer, Christian ; Kirsch, Michael ; Ferenz, Katja Bettina

engleski

Prevention of Decompression Sickness by Novel Artificial Oxygen Carriers

For three decades, studies have demonstrated the therapeutic efficacy of perfluorocarbon (PFC) in reducing the onset of decompression trauma. However, none of these emulsion-based preparations are accepted for therapeutic use in the western world, mainly because of severe side effects and a long organ retention time. A new development to guarantee a stable dispersion without these disadvantages is the encapsulation of PFC in nanocapsules with an albumin shell. Purpose Newly designed albumin-derived perfluorocarbon-based artificial oxygen carriers (A-AOC) are used in a rodentin vivomodel as a preventive therapy for decompression sickness (DCS). Methods Thirty-seven rats were treated with A-AOC (n= 12), albumin nanocapsules filled with neutral oil (A-O-N, n= 12), or 5% human serum albumin solution (A-0-0, n= 13) before a simulated dive. Eleven rats, injected with A-AOC, stayed at normal pressure (A-AOC surface). Clinical, laboratory, and histological evaluations were performed. Results The occurrence of DCS depended on the treatment group. A-AOC significantly reduced DCS appearance and mortality. Furthermore, a significant improvement of survival time was found (A-AOC compared with A- 0-0). Histological assessment of A-AOC-dive compared with A-0-0-dive animals revealed significantly higher accumulation of macrophages, but less blood congestion in the spleen and significantly less hepatic circulatory disturbance, vacuolization, and cell damage. Compared with nondiving controls, lactate and myoglobin showed a significant increase in the A- 0-0- but not in the A-AOC-dive group. Conclusion Intravenous application of A-AOC was well tolerated and effective in reducing the occurrence of DCS, and animals showed significantly higher survival rates and less symptoms compared with the albumin group (A-0-0). Analysis of histological results and fast reacting plasma parameters confirmed the preventive properties of A-AOC.

ALBUMIN-DERIVED PERFLUOROCARBON-BASED ARTIFICIAL OXYGEN CARRIERS ; NANOCAPSULES ; NONRECOMPRESSIVE THERAPY ; RODENTIN VIVOMODEL

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Podaci o izdanju

52 (10)

2020.

2127-2135

objavljeno

0195-9131

1530-0315

10.1249/mss.0000000000002354

Povezanost rada

Temeljne medicinske znanosti

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