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* Ihre Aktion:   suchen [und] (PICA Prod.-Nr. [PPN]) 1671744829
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Online-Artikel
 
K10plusPPN: 
1671744829     Zitierlink
Aufsatz: 
Acute skin damage and late radiation-induced fibrosis and inflammation in murine ears after high-dose irradiation / Annique C. Dombrowsky, Jannis Schauer, Matthias Sammer, Andreas Blutke, Dietrich W.M. Walsh, Benjamin Schwarz, Stefan Bartzsch, Annette Feuchtinger, Judith Reindl, Stephanie E. Combs, Günther Dollinger and Thomas E. Schmid
Autorin/Autor: 
Dombrowsky, Annique [Verfasserin/Verfasser] info info
Beteiligt: 
Walsh, Dietrich [Verfasserin/Verfasser] info info
Enthalten in: 
Cancers. - Basel : MDPI, 2009-. - 11(2019,5) Artikel-Nummer 727, 21 Seiten
Sprache(n): 
Englisch
Anmerkung: 
Gesehen am 21.08.2019


Link zum Volltext: 
Digital Object Identifier (DOI): 10.3390/cancers11050727


Sonstige Schlagwörter: 
Inhaltliche
Zusammenfassung: 
The use of different scoring systems for radiation-induced toxicity limits comparability between studies. We examined dose-dependent tissue alterations following hypofractionated X-ray irradiation and evaluated their use as scoring criteria. Four dose fractions (0, 5, 10, 20, 30 Gy/fraction) were applied daily to ear pinnae. Acute effects (ear thickness, erythema, desquamation) were monitored for 92 days after fraction 1. Late effects (chronic inflammation, fibrosis) and the presence of transforming growth factor beta 1 (TGFβ1)-expressing cells were quantified on day 92. The maximum ear thickness displayed a significant positive correlation with fractional dose. Increased ear thickness and erythema occurred simultaneously, followed by desquamation from day 10 onwards. A significant dose-dependency was observed for the severity of erythema, but not for desquamation. After 4 × 20 and 4 × 30 Gy, inflammation was significantly increased on day 92, whereas fibrosis and the abundance of TGFβ1-expressing cells were only marginally increased after 4 × 30 Gy. Ear thickness significantly correlated with the severity of inflammation and fibrosis on day 92, but not with the number of TGFβ1-expressing cells. Fibrosis correlated significantly with inflammation and fractional dose. In conclusion, the parameter of ear thickness can be used as an objective, numerical and dose-dependent quantification criterion to characterize the severity of acute toxicity and allow for the prediction of late effects.
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