The HMG-CoA Reductase Inhibitor Pravastatin Stimulates Insulin Secretion through Organic Anion Transporter Polypeptides

The 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor pravastatin has been reported to have a beneficial effect on reducing the new onset of diabetes as well as lowering plasma lipids. Because pravastatin is a water-soluble organic anion, it cannot easily penetrate the lipid bilayer of the c...

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Published in:	DRUG METABOLISM AND PHARMACOKINETICS Vol. 25; no. 3; pp. 274 - 282
Main Authors:	Abe, Michiaki, Toyohara, Takafumi, Ishii, Akiko, Suzuki, Takehiro, Noguchi, Naoya, Akiyama, Yasutoshi, Shiwaku, Hiromi O., Nakagomi-Hagihara, Rie, Zheng, Guodong, Shibata, Eisuke, Souma, Tomokazu, Shindo, Tomohiko, Shima, Hirohito, Takeuchi, Yoichi, Mishima, Eikan, Tanemoto, Masayuki, Terasaki, Tetsuya, Onogawa, Tohru, Unno, Michiaki, Ito, Sadayoshi, Takasawa, Shin, Abe, Takaaki
Format:	Journal Article
Language:	English
Published:	England Elsevier Ltd 01-01-2010 Japanese Society for the Study of Xenobiotics
Subjects:	Adiponectin - blood adipose Animals Biological Transport - drug effects Cell Line, Tumor diabetes Diabetes Mellitus - drug therapy disease endobiotics HMG-CoA reductase inhibitors Hydroxymethylglutaryl CoA Reductases Immunohistochemistry insulin Insulin - agonists Insulin - metabolism Insulin Secretion islet Islets of Langerhans - cytology Islets of Langerhans - drug effects Male Mice Mice, Inbred Strains Models, Animal OATP organ Organic Anion Transporters, Sodium-Independent - analysis Organic Anion Transporters, Sodium-Independent - metabolism Pancreas - cytology Pancreas - drug effects Pravastatin - pharmacokinetics Pravastatin - pharmacology Rats Rifampin - pharmacology SLC transporters SLCO (SLC21) Sulfobromophthalein - pharmacology xenobiotics organ endobiotics disease insulin HMG-CoA reductase inhibitors xenobiotics SLC transporters adipose OATP islet diabetes SLCO (SLC21)
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Abstract	The 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor pravastatin has been reported to have a beneficial effect on reducing the new onset of diabetes as well as lowering plasma lipids. Because pravastatin is a water-soluble organic anion, it cannot easily penetrate the lipid bilayer of the cell membrane. As the precise mechanisms of the effect of pravastatin on glucose metabolism and diabetes have not been clarified, we examined the roles of the organic anion transporter family on pravastatin-treated islet and adipocyte functions. Rat oatp1/slco1a1, oatp2/slco1a4 and oatp3/slco1a5 were expressed in the pancreas, and rat oatp3/slco1a5 was also detected in rat insulinoma cell line INS-1e. Pravastatin was transported not only by oatp1/slco1a1 and oatp2/slco1a4, but also by rat oatp3/slco1a5. Pravastatin uptake into INS-1e cells was detected and this transport was inhibited by sulfobromophthalein and rifampicin, both of which are known to inhibit oatp family-mediated uptake. In addition, pravastatin enhanced the glucose-stimulated insulin secretion from INS-1e cells. When fat-loaded db/db mice were treated with pravastatin, glucose intolerance and insulin resistance were prevented. In addition, insulin secretion from isolated islets was enhanced by pravastatin. These data suggest that pravastatin has pleiotropic effects on islets through membrane transport under high fat/glucose conditions.
AbstractList	Summary: The 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor pravastatin has been reported to have a beneficial effect on reducing the new onset of diabetes as well as lowering plasma lipids. Because pravastatin is a water-soluble organic anion, it cannot easily penetrate the lipid bilayer of the cell membrane. As the precise mechanisms of the effect of pravastatin on glucose metabolism and diabetes have not been clarified, we examined the roles of the organic anion transporter family on pravastatin-treated islet and adipocyte functions. Rat oatp1/slco1a1, oatp2/slco1a4 and oatp3/slco1a5 were expressed in the pancreas, and rat oatp3/slco1a5 was also detected in rat insulinoma cell line INS-1e. Pravastatin was transported not only by oatp1/slco1a1 and oatp2/slco1a4, but also by rat oatp3/slco1a5. Pravastatin uptake into INS-1e cells was detected and this transport was inhibited by sulfobromophthalein and rifampicin, both of which are known to inhibit oatp family-mediated uptake. In addition, pravastatin enhanced the glucose-stimulated insulin secretion from INS-1e cells. When fat-loaded db/db mice were treated with pravastatin, glucose intolerance and insulin resistance were prevented. In addition, insulin secretion from isolated islets was enhanced by pravastatin. These data suggest that pravastatin has pleiotropic effects on islets through membrane transport under high fat/glucose conditions. The 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor pravastatin has been reported to have a beneficial effect on reducing the new onset of diabetes as well as lowering plasma lipids. Because pravastatin is a water-soluble organic anion, it cannot easily penetrate the lipid bilayer of the cell membrane. As the precise mechanisms of the effect of pravastatin on glucose metabolism and diabetes have not been clarified, we examined the roles of the organic anion transporter family on pravastatin-treated islet and adipocyte functions. Rat oatp1/slco1a1, oatp2/slco1a4 and oatp3/slco1a5 were expressed in the pancreas, and rat oatp3/slco1a5 was also detected in rat insulinoma cell line INS-1e. Pravastatin was transported not only by oatp1/slco1a1 and oatp2/slco1a4, but also by rat oatp3/slco1a5. Pravastatin uptake into INS-1e cells was detected and this transport was inhibited by sulfobromophthalein and rifampicin, both of which are known to inhibit oatp family-mediated uptake. In addition, pravastatin enhanced the glucose-stimulated insulin secretion from INS-1e cells. When fat-loaded db/db mice were treated with pravastatin, glucose intolerance and insulin resistance were prevented. In addition, insulin secretion from isolated islets was enhanced by pravastatin. These data suggest that pravastatin has pleiotropic effects on islets through membrane transport under high fat/glucose conditions.
Author	Tanemoto, Masayuki Souma, Tomokazu Suzuki, Takehiro Shibata, Eisuke Abe, Takaaki Shindo, Tomohiko Ishii, Akiko Noguchi, Naoya Takeuchi, Yoichi Ito, Sadayoshi Takasawa, Shin Zheng, Guodong Onogawa, Tohru Akiyama, Yasutoshi Unno, Michiaki Toyohara, Takafumi Nakagomi-Hagihara, Rie Mishima, Eikan Shima, Hirohito Terasaki, Tetsuya Abe, Michiaki Shiwaku, Hiromi O.
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Snippet	The 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor pravastatin has been reported to have a beneficial effect on reducing the new onset of diabetes... Summary: The 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor pravastatin has been reported to have a beneficial effect on reducing the new onset of...
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SubjectTerms	Adiponectin - blood adipose Animals Biological Transport - drug effects Cell Line, Tumor diabetes Diabetes Mellitus - drug therapy disease endobiotics HMG-CoA reductase inhibitors Hydroxymethylglutaryl CoA Reductases Immunohistochemistry insulin Insulin - agonists Insulin - metabolism Insulin Secretion islet Islets of Langerhans - cytology Islets of Langerhans - drug effects Male Mice Mice, Inbred Strains Models, Animal OATP organ Organic Anion Transporters, Sodium-Independent - analysis Organic Anion Transporters, Sodium-Independent - metabolism Pancreas - cytology Pancreas - drug effects Pravastatin - pharmacokinetics Pravastatin - pharmacology Rats Rifampin - pharmacology SLC transporters SLCO (SLC21) Sulfobromophthalein - pharmacology xenobiotics
Title	The HMG-CoA Reductase Inhibitor Pravastatin Stimulates Insulin Secretion through Organic Anion Transporter Polypeptides
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