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Research ArticleEndocrine and Diabetes

Analysis of the Effect of Canagliflozin on Renal Glucose Reabsorption and Progression of Hyperglycemia in Zucker Diabetic Fatty Rats

Chiaki Kuriyama, Jun Zhi Xu, Seunghun Paul Lee, Jenson Qi, Hirotaka Kimata, Tetsuhiro Kakimoto, Keiko Nakayama, Yoshinori Watanabe, Nobuhiko Taniuchi, Kumiko Hikida, Yasuaki Matsushita, Kenji Arakawa, Akira Saito, Kiichiro Ueta and Masaharu Shiotani
Journal of Pharmacology and Experimental Therapeutics November 2014, 351 (2) 423-431; DOI: https://doi.org/10.1124/jpet.114.217992
Chiaki Kuriyama
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Jun Zhi Xu
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Seunghun Paul Lee
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Jenson Qi
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Hirotaka Kimata
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Tetsuhiro Kakimoto
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Keiko Nakayama
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Yoshinori Watanabe
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Nobuhiko Taniuchi
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Kumiko Hikida
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Yasuaki Matsushita
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Kenji Arakawa
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Akira Saito
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Kiichiro Ueta
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Masaharu Shiotani
Research Division, Mitsubishi Tanabe Pharma Corporation, Toda-shi, Saitama, Japan (C.K., H.K., T.K., K.N., Y.W., N.T., K.H., Y.M., K.A., A.S., K.U., M.S.); and Janssen Research & Development LLC, Spring House, Pennsylvania (J.Z.X., S.P.L., J.Q.)
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Abstract

Sodium–glucose cotransporter 2 (SGLT2) plays a major role in renal glucose reabsorption. To analyze the potential of insulin-independent blood glucose control, the effects of the novel SGLT2 inhibitor canagliflozin on renal glucose reabsorption and the progression of hyperglycemia were analyzed in Zucker diabetic fatty (ZDF) rats. The transporter activity of recombinant human and rat SGLT2 was inhibited by canagliflozin, with 150- to 12,000-fold selectivity over other glucose transporters. Moreover, in vivo treatment with canagliflozin induced glucosuria in mice, rats, and dogs in a dose-dependent manner. It inhibited apparent glucose reabsorption by 55% in normoglycemic rats and by 94% in hyperglycemic rats. The inhibition of glucose reabsorption markedly reduced hyperglycemia in ZDF rats but did not induce hypoglycemia in normoglycemic animals. The change in urinary glucose excretion should not be used as a marker to predict the glycemic effects of this SGLT2 inhibitor. In ZDF rats, plasma glucose and HbA1c levels progressively increased with age, and pancreatic β-cell failure developed at 13 weeks of age. Treatment with canagliflozin for 8 weeks from the prediabetic stage suppressed the progression of hyperglycemia, prevented the decrease in plasma insulin levels, increased pancreatic insulin contents, and minimized the deterioration of islet structure. These results indicate that selective inhibition of SGLT2 with canagliflozin controls the progression of hyperglycemia by inhibiting renal glucose reabsorption in ZDF rats. In addition, the preservation of β-cell function suggests that canagliflozin treatment reduces glucose toxicity via an insulin-independent mechanism.

Footnotes

    • Received June 29, 2014.
    • Accepted September 9, 2014.
  • The authors of this work are employees of Mitsubishi Tanabe Pharma Corporation or Janssen Research & Development and have not received financial support from any other institution.

  • dx.doi.org/10.1124/jpet.114.217992.

  • ↵Embedded ImageThis article has supplemental material available at jpet.aspetjournals.org.

  • Copyright © 2014 by The American Society for Pharmacology and Experimental Therapeutics
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Journal of Pharmacology and Experimental Therapeutics: 351 (2)
Journal of Pharmacology and Experimental Therapeutics
Vol. 351, Issue 2
1 Nov 2014
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Research ArticleEndocrine and Diabetes

Canagliflozin Improves Hyperglycemia in ZDF Rats

Chiaki Kuriyama, Jun Zhi Xu, Seunghun Paul Lee, Jenson Qi, Hirotaka Kimata, Tetsuhiro Kakimoto, Keiko Nakayama, Yoshinori Watanabe, Nobuhiko Taniuchi, Kumiko Hikida, Yasuaki Matsushita, Kenji Arakawa, Akira Saito, Kiichiro Ueta and Masaharu Shiotani
Journal of Pharmacology and Experimental Therapeutics November 1, 2014, 351 (2) 423-431; DOI: https://doi.org/10.1124/jpet.114.217992

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Research ArticleEndocrine and Diabetes

Canagliflozin Improves Hyperglycemia in ZDF Rats

Chiaki Kuriyama, Jun Zhi Xu, Seunghun Paul Lee, Jenson Qi, Hirotaka Kimata, Tetsuhiro Kakimoto, Keiko Nakayama, Yoshinori Watanabe, Nobuhiko Taniuchi, Kumiko Hikida, Yasuaki Matsushita, Kenji Arakawa, Akira Saito, Kiichiro Ueta and Masaharu Shiotani
Journal of Pharmacology and Experimental Therapeutics November 1, 2014, 351 (2) 423-431; DOI: https://doi.org/10.1124/jpet.114.217992
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