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Titel:Uremic Toxins and Organ Failure
Mitwirkende:Saito, Hideyuki [HerausgeberIn]   i
 Abe, Takaaki [HerausgeberIn]   i
Verf.angabe:edited by Hideyuki Saito, Takaaki Abe
Ausgabe:1st ed. 2020.
Verlagsort:Singapore
 Singapore
Verlag:Springer Singapore
 Imprint: Springer
E-Jahr:2020
Jahr:2020.
 2020.
Umfang:1 Online-Ressource(VIII, 180 p. 39 illus., 22 illus. in color.)
Gesamttitel/Reihe:Springer eBook Collection
ISBN:9789811577932
Abstract:1 Overview of Uremic Toxins -- 2 Review: Uremic toxins and gut microbiome -- 3 Gut microbiota and systemic uremic solute accumulation -- 4 Uremic toxin-related systemic disorders -- 5 Uremic Toxins and cardiovascular disease -- 6 Indoxyl sulfate and arteriosclerosis -- 7 Uremic Toxicity and Bone in CKD -- 8 D-serine as a novel uremic toxin -- 9 Uremic solutes and sarcopenia -- 10 Toxico-pathological role of hepatic sulfotransferase (SULT) 1A1 in acute kidney injuries -- 11 Accumulation of uremic toxins in systemic organs and the effect of AST-120.
 This book describes the latest research on the gut-kidney axis of ureic solutes; the toxico-pathological mechanisms of uremic toxin-induced organ failure, including kidney and cardiovascular tissue; and the preventive therapeutic strategies for uremia and related organ failure associated with kidney injuries and diseases. Retained uremic toxins cause a variety of symptoms, such as hypertension, fatigue, renal anemia, osteoporosis and neurologic impairment, which are apparent in chronic kidney disease (CKD) patients. The human gastrointestinal tract contains trillions of microorganisms, referred to as gut microbiota, which support the host metabolism by producing nutrients, such as vitamins and short-chain fatty acids. However, they also produce various harmful uremic toxins that show renal and cardiovascular toxicity, and correlate with an increased mortality in CKD patients. The composition and balance of gut microbiota are associated with the accumulation of uremic toxins and the pathophysiology of CKD, and as such are being considered for a novel therapeutic strategy.
DOI:doi:10.1007/978-981-15-7793-2
URL:Resolving-System: https://doi.org/10.1007/978-981-15-7793-2
 DOI: https://doi.org/10.1007/978-981-15-7793-2
Datenträger:Online-Ressource
Sprache:eng
Bibliogr. Hinweis:Erscheint auch als : Druck-Ausgabe
 Erscheint auch als : Druck-Ausgabe
 Erscheint auch als : Druck-Ausgabe
K10plus-PPN:1737524732
 
 
Lokale URL UB: Zum Volltext
 
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