Oral bioavailability of ICS such as fluticasone, ciclesonide and mometasone is minimal, as a result of their essentially complete first-pass metabolism in the liver.

 
  • ICS(如氟替卡松、环索奈德和莫美他松)的口服生物利用度最小,因为这些药物主要经过肝脏的首过代谢消除。
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