Effect of viscous additives on the absorption and hepatic disposition of 5-fluorouracil (5-FU) after application to liver surface in rats

Kodama, Yukinobu; Horishita, Miyuki; Fumoto, Shintaro; Mine, Toyoharu; Miyamoto, Hirotaka; Yoshikawa, Naoki; Hirata, Haruna; Sasaki, Hidetada; Nakamura, Junzo; Nishida, Koyo

doi:10.1111/j.2042-7158.2012.01514.x

Cited by 6 publications

(10 citation statements)

References 35 publications

(52 reference statements)

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“…[13][14][15][16][17][18][19][20]23) Because 5-FU is mostly catabolized and inactivated by DPD, 28) we expected that combining DPD inhibitors enable us to increase 5-FU availability at the admin- istration site. In this study, we chose gimeracil and uridine as candidates for promising DPD inhibitors that can be applied to the rat liver surface.…”

Section: Discussionmentioning

confidence: 99%

“…The applied dose of 5-FU was set according to our previous study. 23) A piece of aluminum foil was placed on the top of the diffusion cell to prevent evaporation.…”

Section: Methodsmentioning

confidence: 99%

“…19,20) We have also investigated other organs as an administration route of 5-FU. 21,22) Although viscous additives to 5-FU solution improved site-selective accumulation of 5-FU, 23) the increase in 5-FU concentration at the application site was not large enough.…”

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confidence: 99%

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Effect of Metabolic Inhibitors on the Hepatic Disposition of 5-Fluorouracil after Application to the Rat Liver Surface

Shimokawa

Wakasugi

Tomonaga

et al. 2016

Biological & Pharmaceutical Bulletin

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We evaluated the effects of 5-fluorouracil (5-FU) metabolic inhibitors, gimeracil or uridine, on the hepatic disposition of 5-FU after application to the liver surface in rats, aiming to enhance the availability of 5-FU in the liver. 5-FU solution with or without metabolic inhibitors was applied to the rat liver surface using a cylindrical diffusion cell. The liver, blood and the remaining solution in the diffusion cell were collected at specified times, and assayed for 5-FU content. 5-FU absorption properties were not altered by addition of gimeracil and uridine. The 5-FU concentration in the diffusion cell attachment site of the rat liver (site 1) at 0.1-0.4 M ratios of gimeracil to 5-FU was significantly higher than that of the control. On the contrary, the addition of uridine did not increase the 5-FU concentration at site 1. At a 0.1 M ratio of gimeracil to 5-FU, the maximum 5-FU plasma concentration was the lowest, and the area under the 5-FU concentration-time curve at site 1 was 3.4 times greater than that of the control. We demonstrated that applying 5-FU with gimeracil to the rat liver surface could increase the availability of 5-FU in the liver.Key words liver surface; 5-fluorouracil; disposition; dihydropyrimidine dehydrogenase; gimeracil; uridine Hepatocellular carcinoma (HCC) is the second most frequent cause of cancer-related death worldwide. 1) In many cases, chronic hepatitis and hepatic cirrhosis trigger the development of HCC. 2) Even radical surgery, a potentially curative treatment for HCC, is limited by cancer progression and hepatic functional reserve. 3) In addition, HCC frequently recurs after radical surgery in the residual liver tissue because of progressive disease. 4) Although chemotherapy has been applied to treat the advanced or recurrent HCC, most of anticancer drugs cannot exert the desired effect on HCC because of high chemoresistance rate. 5,6) Local therapies such as percutaneous ethanol injection, 7,8) intratumoral injection 9-11) and intra-arterial infusion 12) have been performed to enhance the therapeutic effect of anticancer drugs on HCC. However, optimal delivery of anticancer drugs to HCC lesion is difficult through these routes because of distribution in the normal surrounding tissue or rapid efflux into the systemic circulation from the injection site.Therefore, we have proposed that the liver surface is a new drug administration route, and investigated the absorption and disposition characteristics of several marker compounds after direct application to the rat liver surface. [13][14][15][16][17][18] To use this route as a local HCC therapy, we showed that 5-fluorouracil (5-FU), a pyrimidine anticancer drug, was site-selectively and continuously delivered in the liver after application to the liver surface in rats. 19,20) We have also investigated other organs as an administration route of 5-FU. 21,22) Although viscous additives to 5-FU solution improved site-selective accumulation of 5-FU, 23) the increase in 5-FU concentration at the application site was not large ...

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Section: Discussionmentioning

confidence: 99%

“…The applied dose of 5-FU was set according to our previous study. 23) A piece of aluminum foil was placed on the top of the diffusion cell to prevent evaporation.…”

Section: Methodsmentioning

confidence: 99%

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Effect of Metabolic Inhibitors on the Hepatic Disposition of 5-Fluorouracil after Application to the Rat Liver Surface

Shimokawa

Wakasugi

Tomonaga

et al. 2016

Biological & Pharmaceutical Bulletin

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“…previously developed a direct route of application to the liver surface and found it to be a useful method for drug targeting (Nishida, Sato, Sasaki, & Nakamura, ; Nishida, Sato, Sasaki, & Nakamura, ; Nishida, Sato, Sasaki, & Nakamura, ; Nishida et al ., ; Nishida et al ., ). Furthermore, liver surface application could achieve the site‐selective delivery of an anticancer drug, 5‐fluorouracil (5‐FU), to the liver (Kodama et al ., ; Kodama et al ., ). However, there remain several problems to be overcome, including poor penetration into tumor tissue, short retention and low availability for time‐dependent anticancer drugs, such as 5‐FU.…”

Section: Introductionmentioning

confidence: 97%

Influence of vasomodulators and tumor transplantation on the disposition of 5‐fluorouracil after application to the liver surface in rats

Kodama

Horishita

Tokunaga

et al. 2017

Biopharm & Drug Disp

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This study investigated the effect of epinephrine (a vasoconstrictor) and hydralazine (a vasodilator) on the hepatic disposition of 5-fluorouracil (5-FU) after application to the surface of the liver in rats. Normal livers were compared with a Walker 256 carcinoma cell tumor model. A cylindrical diffusion cell was attached to the liver surface. 5-Fluorouracil was added into the diffusion cell in combination with vasomodulators or after pretreatment with epinephrine. After selected treatment times, the 5-FU concentrations were assayed at three sites in the excised livers. The 5-FU concentration in the region under the cell attachment site (site 1) was significantly higher after concomitant application of 5-FU and epinephrine, compared with 5-FU alone, and increased in an epinephrine dose-dependent manner. On the other hand, preferential distribution of 5-FU at site 1 was not seen when applied in combination with hydralazine. After 10 min of epinephrine pretreatment, the concentration of 5-FU at site 1 was approximately two times higher than that for the control. Furthermore, the 5-FU concentration at site 1 of the tumor model was greatly increased compared with the normal liver. These results suggest that application of epinephrine to the liver surface might enhance the accumulation of 5-FU at the desired target site.

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“…In previous studies, we have shown that application of low-molecular-weight compounds such as phenolsulfonphthalein and 5-fluorouracil to the liver surface enhanced drug delivery to desired sites in the liver. [1][2][3][4][5] The absorbability of macromolecules as well as their targeting efficacy were also improved. 2,5) The liver surface application might be useful for reduction of side effect and improve the effect of drugs because drugs administered to liver surface were selectivity accumulate into applied site.…”

Section: Introductionmentioning

confidence: 99%

Influence of Liver Intoxication by Carbon Tetrachloride or D-Galactosamine on Absorption of Fluorescein Isothiocyanate-Dextran-10 and Other Marker Compounds with Different Molecular Weights from the Rat Liver Surface

Miyamoto

Tsuda

Honda

et al. 2020

Biological & Pharmaceutical Bulletin

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We examined the influence of liver disease on the absorption from the liver surface of fluorescein isothiocyanate (FITC)-dextran 10 (FD-10, MW: 11000) and several marker compounds with different molecular weights. The purpose of this study was to determine the feasibility of liver surface application of macromolecular compounds in the disease state. We used male Wistar rats treated with carbon tetrachloride (CCl 4) or D-galactosamine (GAL). FD-10 and other marker compounds were applied to the liver surface using a cylindrical diffusion cell in liver-intoxicated rats. The blood, bile, urine, and the remaining solution in the diffusion cell were collected for assay. FD-10 was absorbed by first-order kinetics from the liver surface in the liver-intoxicated rat models. The calculated rate constant k a values in the normal, CCl 4 and GAL groups were 0.000965, 0.00125 and 0.00104 min 1 , respectively. Increased absorption of FITC-dextrans in the liverintoxicated rats was observed. In both CCl 4 and GAL groups, an inverse relationship was observed between the molecular weight and k a from the rat liver surface of the marker compounds. The limits of the molecular weight absorbed from the liver surface were extrapolated to be 71200, 135000, and 105000 in the normal, CCl 4 , and GAL groups, respectively. In conclusion, increased absorbability from the rat liver surface indicates that liver surface application for liver targeting of macromolecules in the diseased state is indeed feasible. Therefore, our findings can support further research on liver surface application of drugs under liver disease.

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Effect of viscous additives on the absorption and hepatic disposition of 5-fluorouracil (5-FU) after application to liver surface in rats

Cited by 6 publications

References 35 publications

Effect of Metabolic Inhibitors on the Hepatic Disposition of 5-Fluorouracil after Application to the Rat Liver Surface

Effect of Metabolic Inhibitors on the Hepatic Disposition of 5-Fluorouracil after Application to the Rat Liver Surface

Influence of vasomodulators and tumor transplantation on the disposition of 5‐fluorouracil after application to the liver surface in rats

Influence of Liver Intoxication by Carbon Tetrachloride or D-Galactosamine on Absorption of Fluorescein Isothiocyanate-Dextran-10 and Other Marker Compounds with Different Molecular Weights from the Rat Liver Surface

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