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RISSThere have been many reports that large doses of teracycline induce fatty infiltration of the liver in rats, and when it is given intravenously to pregnant women who have pyelonephritis, it may give rise to severe hepatic injuries. Although the mecha...
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RISS 인기검색어
Estrogen이 Tetracycline의 肝毒性에 미치는 影響에 關한 實驗的 硏究 = An experimental study on the influence of estrogen to tetracycline-induced hepatotoxicity
한글로보기https://www.riss.kr/link?id=A40016200
- 저자
- 발행기관
- 학술지명
- 권호사항
-
발행연도
1977
-
작성언어
Korean
-
KDC
510.000
-
자료형태
학술저널
-
수록면
77-90(14쪽)
- 제공처
-
0
상세조회 -
0
다운로드
부가정보
다국어 초록 (Multilingual Abstract)
There have been many reports that large doses of teracycline induce fatty infiltration of the liver in rats, and when it is given intravenously to pregnant women who have pyelonephritis, it may give rise to severe hepatic injuries.
Although the mechanism is uncertain, tetracycline in high concentration seems to impair metabolism of fat and removal of triglycerides from the liver. While the toxic effect of tetracycline in obstetric patients is known, the effect of sex hormones on liver tissue damaged by tetracycline is not understood.
The author performed biochemical and histopathologic studies to clarify the effect of estrogen on tetracycline-induced hepatic damage in male albino rats weighing about 200 grams.
The experimental animal were grouped into four categories:
Group Ⅰ, normal control group, was intraperitoneally injected with 1㎖/day of normal saline for 4 weeks.
Group Ⅱ, tetracycline administered group, was intraperitoneally injected with 75.5㎎/㎏/day of tetracycline for 4 weeks.
Group Ⅲ, estrogen administered group, was intramuscularly injected with 6.25㎎/㎏/day of estradiol for 4 weeks.
Group Ⅳ, tetracycline and estrogen combined administered group, was injected in the same manner as group Ⅱ and Ⅲ in combination. For 4 weeks.
The results obtained were as follows:
1. In group Ⅱ, the values of globulin (at 3rd & 4th week), T.T.T., ammonia, total cholesterol, G.P.Y., G.P.T and alkaline phosphatase were significantly increased more than those of the normal control group.
2. In group Ⅱ, the values of globulin (at 4th week), ammonia, total cholesterol, alkaline phosphatase, G.O.T. and G.P.T. were slightly increased more than those of the normal control group, but less than the values shown by group Ⅱ.
3. In group Ⅳ, the values of ammonia, total cholesterol, alkaline phosphatase, G.O.T and G.P.T. were slightly increased more than those of the normal control group, and revealed results similar to those of group Ⅱ, but the values were significantly lower than those shown by group Ⅲ.
4. The values of protoporphyrin were especially decreased in group Ⅱ, while those in group Ⅲ and Ⅳ were observed to be similar to those of the normal control group.
5. In the histopathologe findings of the liver, hepatocytic injuries and vacuolar degeneration, which were most severe during the 1st and 2nd week, were observed in the test groups. There was no evidence of either cholestasis of change in bile duct epithelium.
In summary the biochemical changes of the blood (liver function test) have yieled more significant data than the histopathologic changes of the liver. Comparison of the data shows that in group Ⅱ the biochemical alterations were much more significant than in group Ⅳ. The results we obtained in the experiment have indicated that estrogen exerted a protective effect against tetracycline-induced hepatic dysfunction.
Although the mechanism is uncertain, tetracycline in high concentration seems to impair metabolism of fat and removal of triglycerides from the liver. While the toxic effect of tetracycline in obstetric patients is known, the effect of sex hormones on liver tissue damaged by tetracycline is not understood.
The author performed biochemical and histopathologic studies to clarify the effect of estrogen on tetracycline-induced hepatic damage in male albino rats weighing about 200 grams.
The experimental animal were grouped into four categories:
Group Ⅰ, normal control group, was intraperitoneally injected with 1㎖/day of normal saline for 4 weeks.
Group Ⅱ, tetracycline administered group, was intraperitoneally injected with 75.5㎎/㎏/day of tetracycline for 4 weeks.
Group Ⅲ, estrogen administered group, was intramuscularly injected with 6.25㎎/㎏/day of estradiol for 4 weeks.
Group Ⅳ, tetracycline and estrogen combined administered group, was injected in the same manner as group Ⅱ and Ⅲ in combination. For 4 weeks.
The results obtained were as follows:
1. In group Ⅱ, the values of globulin (at 3rd & 4th week), T.T.T., ammonia, total cholesterol, G.P.Y., G.P.T and alkaline phosphatase were significantly increased more than those of the normal control group.
2. In group Ⅱ, the values of globulin (at 4th week), ammonia, total cholesterol, alkaline phosphatase, G.O.T. and G.P.T. were slightly increased more than those of the normal control group, but less than the values shown by group Ⅱ.
3. In group Ⅳ, the values of ammonia, total cholesterol, alkaline phosphatase, G.O.T and G.P.T. were slightly increased more than those of the normal control group, and revealed results similar to those of group Ⅱ, but the values were significantly lower than those shown by group Ⅲ.
4. The values of protoporphyrin were especially decreased in group Ⅱ, while those in group Ⅲ and Ⅳ were observed to be similar to those of the normal control group.
5. In the histopathologe findings of the liver, hepatocytic injuries and vacuolar degeneration, which were most severe during the 1st and 2nd week, were observed in the test groups. There was no evidence of either cholestasis of change in bile duct epithelium.
In summary the biochemical changes of the blood (liver function test) have yieled more significant data than the histopathologic changes of the liver. Comparison of the data shows that in group Ⅱ the biochemical alterations were much more significant than in group Ⅳ. The results we obtained in the experiment have indicated that estrogen exerted a protective effect against tetracycline-induced hepatic dysfunction.
There have been many reports that large doses of teracycline induce fatty infiltration of the liver in rats, and when it is given intravenously to pregnant women who have pyelonephritis, it may give rise to severe hepatic injuries.
Although the mechanism is uncertain, tetracycline in high concentration seems to impair metabolism of fat and removal of triglycerides from the liver. While the toxic effect of tetracycline in obstetric patients is known, the effect of sex hormones on liver tissue damaged by tetracycline is not understood.
The author performed biochemical and histopathologic studies to clarify the effect of estrogen on tetracycline-induced hepatic damage in male albino rats weighing about 200 grams.
The experimental animal were grouped into four categories:
Group Ⅰ, normal control group, was intraperitoneally injected with 1㎖/day of normal saline for 4 weeks.
Group Ⅱ, tetracycline administered group, was intraperitoneally injected with 75.5㎎/㎏/day of tetracycline for 4 weeks.
Group Ⅲ, estrogen administered group, was intramuscularly injected with 6.25㎎/㎏/day of estradiol for 4 weeks.
Group Ⅳ, tetracycline and estrogen combined administered group, was injected in the same manner as group Ⅱ and Ⅲ in combination. For 4 weeks.
The results obtained were as follows:
1. In group Ⅱ, the values of globulin (at 3rd & 4th week), T.T.T., ammonia, total cholesterol, G.P.Y., G.P.T and alkaline phosphatase were significantly increased more than those of the normal control group.
2. In group Ⅱ, the values of globulin (at 4th week), ammonia, total cholesterol, alkaline phosphatase, G.O.T. and G.P.T. were slightly increased more than those of the normal control group, but less than the values shown by group Ⅱ.
3. In group Ⅳ, the values of ammonia, total cholesterol, alkaline phosphatase, G.O.T and G.P.T. were slightly increased more than those of the normal control group, and revealed results similar to those of group Ⅱ, but the values were significantly lower than those shown by group Ⅲ.
4. The values of protoporphyrin were especially decreased in group Ⅱ, while those in group Ⅲ and Ⅳ were observed to be similar to those of the normal control group.
5. In the histopathologe findings of the liver, hepatocytic injuries and vacuolar degeneration, which were most severe during the 1st and 2nd week, were observed in the test groups. There was no evidence of either cholestasis of change in bile duct epithelium.
In summary the biochemical changes of the blood (liver function test) have yieled more significant data than the histopathologic changes of the liver. Comparison of the data shows that in group Ⅱ the biochemical alterations were much more significant than in group Ⅳ. The results we obtained in the experiment have indicated that estrogen exerted a protective effect against tetracycline-induced hepatic dysfunction.
목차 (Table of Contents)
- Ⅰ. 緖論
- Ⅱ. 實驗材料 및 方法
- Ⅲ. 實驗成績
- 1. 血液化學的 檢査
- 1) 血淸蛋白質
- Ⅰ. 緖論
- Ⅱ. 實驗材料 및 方法
- Ⅲ. 實驗成績
- 1. 血液化學的 檢査
- 1) 血淸蛋白質
- (1) Ablumin 量
- (2) Globulin 量
- (3) Albumin/Globulin 比
- 2) Thymol Turbidity Test(T. T. T.)
- 3) Ammonia 量
- 4) 總 Cholesterol 量
- 5) 血淸酵素 活性値
- (1) Alkaline Phosphatase
- (2) Glutamic Oxalacetic Transaminase(G. O. T.)
- (3) Glutamic Pyruvic Transaminase(G. P. T.)
- 6) Protoporphyrin 量
- 2. 肝의 病理組織學的 所見
- 1) Hematoxylin-Eosin 染色 所見
- 2) Sudan Ⅲ 染色 所見
- Ⅳ. 總括 및 考按
- Ⅴ. 結論
- 參考文獻
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