Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength

Greg C. Smith; Wee Kiat Ong; Jessica L. Costa; Maureen Watson; Jillian Cornish; Andrew Grey; Greg D. Gamble; Michelle Dickinson; Sophie Leung; Gordon W. Rewcastle; Weiping Han; Peter R. Shepherd

doi:10.1111/febs.12428

Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength

Greg C. Smith, Wee Kiat Ong, Jessica L. Costa, Maureen Watson, Jillian Cornish, Andrew Grey, Greg D. Gamble, Michelle Dickinson, Sophie Leung, Gordon W. Rewcastle, Weiping Han, Peter R. Shepherd

Research output: Contribution to journal › Article › Research › peer-review

21 Citations (Scopus)

Abstract

The class I phosphatidylinositol 3-kinases (PtdIns3Ks) mediate the effects of many hormones and growth factors on a wide range of cellular processes, and activating mutations or gene amplifications of class I PtdIns3K isoforms are known to contribute to oncogenic processes in a range of tumours. Consequently, a number of small-molecule PtdIns3K inhibitors are under development and in clinical trial. The central signalling role of PtdIns3K in many cellular processes suggests there will be on-target side effects associated with the use of these agents. To gain insights into what these might be we investigated the effect of extended daily dosing of eight small-molecule inhibitors of class Ia PtdIns3Ks. Animals were characterized in metabolic cages to analyse food intake, oxygen consumption and movement. Insulin tolerance and body composition were analysed at the end of the experiment, the latter using EchoMRI. Bone volume and strength was assessed by micro-CT and three-point bending, respectively. Surprisingly, after sustained dosing with pan-PtdIns3K inhibitors and selective inhibitors of the p110α isoform there was a resolution of the impairments in insulin tolerance observed in drug-naïve animals treated with the same drugs. However, pan-PtdIns3K inhibitors and selective inhibitors of the p110α have deleterious effects on animal growth, animal behaviour and bone volume and strength. Together, these findings identify a range of on target effects of PtdIns3K inhibitors and suggest use of these drugs in humans may have important adverse effects on metabolism, body composition, behaviour and skeletal health. A number of small molecule PI 3-kinase inhibitors have been developed. We investigated the effects of extended treatment of mice with eight such inhibitors. Surprisingly, defects in glucose metabolism were minimal. However, there were deleterious effects on growth, behaviour and bone health. These studies identify a range of possible side effects of long term use of PI 3-kinase inhibitors.

Original language	English
Pages (from-to)	5337-5349
Number of pages	13
Journal	FEBS Journal
Volume	280
Issue number	21
DOIs	https://doi.org/10.1111/febs.12428
Publication status	Published - Nov 2013
Externally published	Yes

Keywords

A66
BEZ235
phosphatidylinositol 3-kinase
PIK75
ZSTK474

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10.1111/febs.12428

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Smith, G. C., Ong, W. K., Costa, J. L., Watson, M., Cornish, J., Grey, A., Gamble, G. D., Dickinson, M., Leung, S., Rewcastle, G. W., Han, W., & Shepherd, P. R. (2013). Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength. FEBS Journal, 280(21), 5337-5349. https://doi.org/10.1111/febs.12428

@article{826373b86ed44c35a591b77c3d0b6c24,

title = "Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength",

abstract = "The class I phosphatidylinositol 3-kinases (PtdIns3Ks) mediate the effects of many hormones and growth factors on a wide range of cellular processes, and activating mutations or gene amplifications of class I PtdIns3K isoforms are known to contribute to oncogenic processes in a range of tumours. Consequently, a number of small-molecule PtdIns3K inhibitors are under development and in clinical trial. The central signalling role of PtdIns3K in many cellular processes suggests there will be on-target side effects associated with the use of these agents. To gain insights into what these might be we investigated the effect of extended daily dosing of eight small-molecule inhibitors of class Ia PtdIns3Ks. Animals were characterized in metabolic cages to analyse food intake, oxygen consumption and movement. Insulin tolerance and body composition were analysed at the end of the experiment, the latter using EchoMRI. Bone volume and strength was assessed by micro-CT and three-point bending, respectively. Surprisingly, after sustained dosing with pan-PtdIns3K inhibitors and selective inhibitors of the p110α isoform there was a resolution of the impairments in insulin tolerance observed in drug-na{\"i}ve animals treated with the same drugs. However, pan-PtdIns3K inhibitors and selective inhibitors of the p110α have deleterious effects on animal growth, animal behaviour and bone volume and strength. Together, these findings identify a range of on target effects of PtdIns3K inhibitors and suggest use of these drugs in humans may have important adverse effects on metabolism, body composition, behaviour and skeletal health. A number of small molecule PI 3-kinase inhibitors have been developed. We investigated the effects of extended treatment of mice with eight such inhibitors. Surprisingly, defects in glucose metabolism were minimal. However, there were deleterious effects on growth, behaviour and bone health. These studies identify a range of possible side effects of long term use of PI 3-kinase inhibitors.",

keywords = "A66, BEZ235, phosphatidylinositol 3-kinase, PIK75, ZSTK474",

author = "Smith, {Greg C.} and Ong, {Wee Kiat} and Costa, {Jessica L.} and Maureen Watson and Jillian Cornish and Andrew Grey and Gamble, {Greg D.} and Michelle Dickinson and Sophie Leung and Rewcastle, {Gordon W.} and Weiping Han and Shepherd, {Peter R.}",

year = "2013",

month = nov,

doi = "10.1111/febs.12428",

language = "English",

volume = "280",

pages = "5337--5349",

journal = "The FEBS Journal",

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Smith, GC, Ong, WK, Costa, JL, Watson, M, Cornish, J, Grey, A, Gamble, GD, Dickinson, M, Leung, S, Rewcastle, GW, Han, W & Shepherd, PR 2013, 'Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength', FEBS Journal, vol. 280, no. 21, pp. 5337-5349. https://doi.org/10.1111/febs.12428

TY - JOUR

T1 - Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength

AU - Smith, Greg C.

AU - Ong, Wee Kiat

AU - Costa, Jessica L.

AU - Watson, Maureen

AU - Cornish, Jillian

AU - Grey, Andrew

AU - Gamble, Greg D.

AU - Dickinson, Michelle

AU - Leung, Sophie

AU - Rewcastle, Gordon W.

AU - Han, Weiping

AU - Shepherd, Peter R.

PY - 2013/11

Y1 - 2013/11

N2 - The class I phosphatidylinositol 3-kinases (PtdIns3Ks) mediate the effects of many hormones and growth factors on a wide range of cellular processes, and activating mutations or gene amplifications of class I PtdIns3K isoforms are known to contribute to oncogenic processes in a range of tumours. Consequently, a number of small-molecule PtdIns3K inhibitors are under development and in clinical trial. The central signalling role of PtdIns3K in many cellular processes suggests there will be on-target side effects associated with the use of these agents. To gain insights into what these might be we investigated the effect of extended daily dosing of eight small-molecule inhibitors of class Ia PtdIns3Ks. Animals were characterized in metabolic cages to analyse food intake, oxygen consumption and movement. Insulin tolerance and body composition were analysed at the end of the experiment, the latter using EchoMRI. Bone volume and strength was assessed by micro-CT and three-point bending, respectively. Surprisingly, after sustained dosing with pan-PtdIns3K inhibitors and selective inhibitors of the p110α isoform there was a resolution of the impairments in insulin tolerance observed in drug-naïve animals treated with the same drugs. However, pan-PtdIns3K inhibitors and selective inhibitors of the p110α have deleterious effects on animal growth, animal behaviour and bone volume and strength. Together, these findings identify a range of on target effects of PtdIns3K inhibitors and suggest use of these drugs in humans may have important adverse effects on metabolism, body composition, behaviour and skeletal health. A number of small molecule PI 3-kinase inhibitors have been developed. We investigated the effects of extended treatment of mice with eight such inhibitors. Surprisingly, defects in glucose metabolism were minimal. However, there were deleterious effects on growth, behaviour and bone health. These studies identify a range of possible side effects of long term use of PI 3-kinase inhibitors.

AB - The class I phosphatidylinositol 3-kinases (PtdIns3Ks) mediate the effects of many hormones and growth factors on a wide range of cellular processes, and activating mutations or gene amplifications of class I PtdIns3K isoforms are known to contribute to oncogenic processes in a range of tumours. Consequently, a number of small-molecule PtdIns3K inhibitors are under development and in clinical trial. The central signalling role of PtdIns3K in many cellular processes suggests there will be on-target side effects associated with the use of these agents. To gain insights into what these might be we investigated the effect of extended daily dosing of eight small-molecule inhibitors of class Ia PtdIns3Ks. Animals were characterized in metabolic cages to analyse food intake, oxygen consumption and movement. Insulin tolerance and body composition were analysed at the end of the experiment, the latter using EchoMRI. Bone volume and strength was assessed by micro-CT and three-point bending, respectively. Surprisingly, after sustained dosing with pan-PtdIns3K inhibitors and selective inhibitors of the p110α isoform there was a resolution of the impairments in insulin tolerance observed in drug-naïve animals treated with the same drugs. However, pan-PtdIns3K inhibitors and selective inhibitors of the p110α have deleterious effects on animal growth, animal behaviour and bone volume and strength. Together, these findings identify a range of on target effects of PtdIns3K inhibitors and suggest use of these drugs in humans may have important adverse effects on metabolism, body composition, behaviour and skeletal health. A number of small molecule PI 3-kinase inhibitors have been developed. We investigated the effects of extended treatment of mice with eight such inhibitors. Surprisingly, defects in glucose metabolism were minimal. However, there were deleterious effects on growth, behaviour and bone health. These studies identify a range of possible side effects of long term use of PI 3-kinase inhibitors.

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JO - The FEBS Journal

JF - The FEBS Journal

SN - 1742-464X

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ER -

Extended treatment with selective phosphatidylinositol 3-kinase and mTOR inhibitors has effects on metabolism, growth, behaviour and bone strength

Abstract

Keywords

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