Abstract
Polymyxin B (PMXB) blocks the action of insulin on glucose uptake in vitro. In vivo, it reverses hypoglycemia induced by exogenous insulin. Here we have treated mature male rats daily with PMXB over a period of two weeks. This therapy has decreased body weight by 11%, adipose fat mass by 46% and triglyceride levels by 39%, with no indication of liver or kidney toxicity. Two suboptimal parameters, however, were a decrease in food intake in the first week of treatment and some increase in fasting glucose levels. We have screened for PMXB-analogs having less associating affinity with rat-muscle phospholipids, and revealed that the same therapy using PMXB-derived peptide (nona-PMXB) is most optimal. This PMXB-analog is devoid of antibacterial activity and is four times less toxic than PMXB. Nona-PMXB therapy lower by 10, 32, 35 and 6% body weight gain, fat mass, circulating triglycerides and fasting glucose levels, respectively, in spite of normal or even elevated food intake in nona-PMXB treated rats. In summary, we found that nona-PMXB therapy is capable if inducing leanness in mature rats, particularly at the expense of decreasing fat-mass in adipose tissue. By and large, we suggest that lowering the action of insulin, on fat build-up solely, may be a therapeutically feasible task to fight with human adiposity in the future.
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
Abbreviations
- HPLC:
-
high-pressure liquid chromatography
- IRKO-mice:
-
insulin-receptor knockout mice
- nona-colistin:
-
colistin-nonapeptide
- nona-PMXB:
-
polymyxin B nonapeptide
- PMXB:
-
polymyxin B
References
Amir S., Sasson S., Kaiser N., Meyerovitch J., Shechter Y., 1987, J. Biol. Chem. 262: 6663–6667
Amir S., Shechter Y., 1985, Eur. J. Pharmacol. 110: 283–285
Arner P., 2002, Diabetes Metab. Res. Rev. 18: 55–59
Arner P., 2003, Trends Endocrinol. Metab. 14: 137–145
Bergman R. N., 2001, J. Invest. Med. 49: 119–126
Bertrand H. A., Lynd F. T., Masoro E. J., Yu B. P., 1980, J. Gerontol. 35: 827–835
Blueher M., Kahn B. B., Kahn C. R., 2003, Science 299: 572–574
Blueher M., Michael M. D., Peroni O. D., Ueki K., Carter N., Kahn B. B., Kahn C. R., 2002, Dev. Cell 3: 25–38
Boden G., Shulman G. I., 2002, Eur. J. Clin. Invest. 32: 14–23
Borst S. E., Bagby G. J., 2002, Metabolism 51: 1061–1064
Bruning J. C., Michael M. D., Winnay J. M., Hayashi T., Horsch D., Accili D., Goodyear L. J., Kahn C. R., 1998, Mol. Cell 2: 559–569
Chalkley S. M., Hettiarachchi M., Chisholm D. J., Kraegen E. W., 2002, Am. J. Physiol. Endocrinol. Metab. 282: E1231–E1238
Colditz G. A., Willett W. C., Stampfer M. J., Manson J. E., Hennekens C. H., Arky R. A., Speizer F. E., 1990, Am. J. Epidemiol. 132: 501–513
Czech M. P., 1985, Ann. Rev. Physiol. 47: 357–381
Danner R. L., Joiner K. A., Rubin M., Paterson W. H., Johnson N., Ayers K. M., Parrillo J. E., 1989, Antimicrob. Agents Chemother. 33: 1428–1434
Flier J. S., 1998, J. Clin. Endocrinol. Metab. 83: 1407–1413
Gabriely I., Ma X. H., Atzmon G., Rajala M. W., Berg A. H., Scherer P., Rossetti L., Barzilai N., 2002, Diabetes 10: 2951–2958
Gupta G., Cases J. A., She L., Ma X. H., Yang X. M., Hu M., Wu J., Rossetti L., Barzilai N., 2000, Am. J. Physiol. Endocrinol. Metab. 278: E985–E991
Harrison D. E., Archer J. R., Astle C. M., 1984, Proc. Natl. Acad. Sci. USA 81: 1835–1838
Hissin P. J., Foley J. E., Wardzala L. J., Karnieli E., Simpson I. A., Salans L. B., Cushman S. W., 1982, J. Clin. Invest. 70: 780–790
Hotamisiligil G. C., 2000, Int. J. Obes. Relat. Metab. Disord. 24: S23–S27
Kahn B. B., Flier J. S., 2000, J. Clin. Invest. 106: 473–481
Kahn, C. R. and Shechter, Y.: 1990, in A. G. Gilman, T. W. Rall, A. S. Nies, and P. Taylor (eds.), Goodman and Gilman Handbook of Pharmacology, New York/Oxford, Pergamon Press, pp. 1463–1495
Kitamura T., Kahn C. R., Accili D., 2003, Ann. Rev. Physiol. 65: 313–332
Kulkarni R. N., Bruning J. C., Winnay J. M., Postic C., Magnuson M. A., Kahn C. R., 1999, Cell 96: 329–339
Ma X. H., Muzumdar R., Yang X. M., Gabriely I., Berger R., Barzilai N., 2002, J. Gerontol. A Biol. Sci. Med. Sci. 57: B225–B231
Michael M. D., Kulkarni R. N., Postic C., Previs S. F., Shulman G. I., Magnuson M. A., Kahn C. R., 2000, Mol. Cell 6: 87–97
Mokdad A. H., Bowman B. A., Ford E. S., Vinicor F., Marks J. S., Koplan J. P., 2001, J. Am. Med. Assoc. 286: 1195–1200
Moody A. J., Stan M., Gliemann J., 1974, Horm. Metab. Res. 6: 12–16
Narimiya M., Azhar S., Dolkas C. B., Mondon C. E., Sims C., Wright D. W., Reaven G. M., 1984, Am. J. Physiol. 246: E397–E404
Peraldi, P. and Spiegelman, B.: 1998, Mol. Cell. Biochem. 182, 169–175
Reaven G. M., 1995, Physiol. Rev. 75: 473–486
Rodbell M., 1964, J. Biol. Chem. 239: 375–380
Shechter Y., 1985, Studies on Insulin Receptors: Implication for Insulin Action Academic Press Inc Orlando, FL
Shechter Y., Chang K. J., Jacobs S., Cuatrecasas P., 1979, Proc. Natl. Acad. Sci. USA 76: 2720–2724
Shechter Y., Goldwaser I., Mironchik M., Fridkin M., Gefel D., 2003, Coor. Chem. Rev. 237: 3–11
Shechter Y., Meyerovitch J., Amir S., 1988, Biochem. Pharmacol. 37: 1891–1896
Shechter Y., Tsubery H., Fridkin M., 2002, J. Med. Chem. 45: 4264–4270
Steppan C. M., Bailey S. T., Bhat S., Brown E. J., Banerjee R. R., Wright C. M., Patel H. R., Ahima R. S., Lazar M. A., 2001, Nature 409: 307–312
Tsubery H., Ofek I., Cohen S., Fridkin M., 2000, Biochemistry 39: 11837–11844
Acknowledgments
We thank Elana Friedman for typing the manuscript and Yigal Avivi for editing it. M.F. is the Lester Pearson Professor of Protein Chemistry; Y.S. is the incumbent of the C.H. Hollenberg Chair in Metabolic and Diabetes Research established by the friends and associates of Dr. C.H. Hollenberg of Toronto, Canada.
Author information
Authors and Affiliations
Corresponding author
Rights and permissions
About this article
Cite this article
Shechter, Y., Mironchik, M., Amir, S. et al. Polymyxin B and Related Cyclic Peptides Facilitate Leanness and Reduce Fat Mass and Triglyceride Content in Ageing Rats: Potential Prototype Drugs Against Obesity. Int J Pept Res Ther 12, 121–129 (2006). https://doi.org/10.1007/s10989-005-9009-9
Received:
Accepted:
Published:
Issue Date:
DOI: https://doi.org/10.1007/s10989-005-9009-9