Novel PI analogues selectively block activation of the pro-survival serine/threonine kinase Akt

Alan P. Kozikowski; Haiying Sun; John Brognard; Phillip A. Dennis

doi:10.1021/ja0285159

Novel PI analogues selectively block activation of the pro-survival serine/threonine kinase Akt

Alan P. Kozikowski, Haiying Sun, John Brognard, Phillip A. Dennis

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

192 Scopus citations

Abstract

The synthesis from l-quebrachitol of a series of 3-deoxygenated ether lipid-type phosphatidylinositol (PI) analogues is reported, that selectively block activation of Akt and downstream substrates without affecting activation of the upstream kinase, PDK-1, or other kinases downstream of ras such as MAPK in H157 and H1703 lung cancer cells that have high levels of constitutively active Akt. The 2-hydroxyl in these compounds was deleted or alkylated with the intent to preclude metabolic degradation of these compounds by PI-specific phospholipase C (PI-PLC). PI analogues with phosphate linkers are more effective than those with carbonate linkers. Specific inhibition of Akt by these compounds validates ligand design targeted to the PH domains of crucial signaling proteins, thus providing a unique class of possible cancer therapeutics.

Original language	English (US)
Pages (from-to)	1144-1145
Number of pages	2
Journal	Journal of the American Chemical Society
Volume	125
Issue number	5
DOIs	https://doi.org/10.1021/ja0285159
State	Published - Feb 5 2003
Externally published	Yes

ASJC Scopus subject areas

Catalysis
Chemistry(all)
Biochemistry
Colloid and Surface Chemistry

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abstract = "The synthesis from l-quebrachitol of a series of 3-deoxygenated ether lipid-type phosphatidylinositol (PI) analogues is reported, that selectively block activation of Akt and downstream substrates without affecting activation of the upstream kinase, PDK-1, or other kinases downstream of ras such as MAPK in H157 and H1703 lung cancer cells that have high levels of constitutively active Akt. The 2-hydroxyl in these compounds was deleted or alkylated with the intent to preclude metabolic degradation of these compounds by PI-specific phospholipase C (PI-PLC). PI analogues with phosphate linkers are more effective than those with carbonate linkers. Specific inhibition of Akt by these compounds validates ligand design targeted to the PH domains of crucial signaling proteins, thus providing a unique class of possible cancer therapeutics.",

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T1 - Novel PI analogues selectively block activation of the pro-survival serine/threonine kinase Akt

AU - Kozikowski, Alan P.

AU - Sun, Haiying

AU - Brognard, John

AU - Dennis, Phillip A.

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AB - The synthesis from l-quebrachitol of a series of 3-deoxygenated ether lipid-type phosphatidylinositol (PI) analogues is reported, that selectively block activation of Akt and downstream substrates without affecting activation of the upstream kinase, PDK-1, or other kinases downstream of ras such as MAPK in H157 and H1703 lung cancer cells that have high levels of constitutively active Akt. The 2-hydroxyl in these compounds was deleted or alkylated with the intent to preclude metabolic degradation of these compounds by PI-specific phospholipase C (PI-PLC). PI analogues with phosphate linkers are more effective than those with carbonate linkers. Specific inhibition of Akt by these compounds validates ligand design targeted to the PH domains of crucial signaling proteins, thus providing a unique class of possible cancer therapeutics.

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Novel PI analogues selectively block activation of the pro-survival serine/threonine kinase Akt

Abstract

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