W/O and O/W emulsions of tegafur (50 ㎎/5 ㎖/㎏) were orally administered to rats to compare with their mesenteric lymphatic delivery effects. And also in order to demonstrate the lymph targeting associated to the oral route, it was deemed necessar...
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https://www.riss.kr/link?id=A3042739
이용복 ; 남권호 ; 장우익 ; 오인준 ; 고익배 ( Yong Bok Lee ; Kweon Ho Nam ; Woo Ik Chang ; In Joon Oh ; Ik Bae Koh )
1995
-
500
SCOPUS,KCI등재,SCIE
학술저널
55-62(8쪽)
0
상세조회0
다운로드다국어 초록 (Multilingual Abstract)
W/O and O/W emulsions of tegafur (50 ㎎/5 ㎖/㎏) were orally administered to rats to compare with their mesenteric lymphatic delivery effects. And also in order to demonstrate the lymph targeting associated to the oral route, it was deemed necessar...
W/O and O/W emulsions of tegafur (50 ㎎/5 ㎖/㎏) were orally administered to rats to compare with their mesenteric lymphatic delivery effects. And also in order to demonstrate the lymph targeting associated to the oral route, it was deemed necessary to investigate the fate of solution after oral administration as a control. Lymph and plasma samples were periodically taken from each subject of mesenteric lymphatic duct cannulated rats. Then, lymph and plasma levels of tegafur and its active metabolite, 5-FU, were simultaneously observed. Also pharmacokinetic parameters were compared with each others. On the other hand, most previous studies of lymphatic transport have not addressed the question of whether an increase in mesenteric or thoracic lymph transport by the manipulation of a suspected variable was due to a selective delivery to the intestinal lymphatics or an overall increase availability. Therefore, based on a physiologically based pharmacokinetic model which represents the characteristics of lymphatic systems, we are also going to determine the contributions of mesenteric lymph transport versus thoracic lymph transport of tegafur reported in reference(13). In comparison with tegafur solution, AUC and mean residence time of plasma tegafur were significantly increased in W/O emulsion but significantly decreased in O/W emulsion. Lymph flow rates were similar in both solution and W/O emulsion but half in O/W emulsion. AUC of tegafur in mesenteric lymph and in plasma for W/O emulsion were 3.7 times and 2.9 times more than those for O/W emulsion, respectively. And AUC of 5-FU in thoracic lymph for W/O emulsion was 3.7 times more than that for O/W emulsion. These results suggested that lymphatic delivery of tegafur by W/O emulsion was more effective than that by O/W emulsion due to its differences of formation ability of chylomicrons.
원보 ; 수종의 스포츠 음료를 토끼에 경구 투여한 후 수분 흡수에 대한 비교연구
원보 ; 오메프라졸의 안정화를 위한 에칠렌디아민 복합체 개발
원보 ; 오메프라졸 - 에칠렌디아민 복합체를 이용한 제제설계
원보 ; 고체분산체 및 포접화합물을 이용한 난용성 약물인 이부프로펜의 용출 속도의 증가