Optimization of benzodiazepinones as selective inhibitors of the X-linked inhibitor of apoptosis protein (XIAP) second baculovirus IAP repeat (BIR2) domain

Robert F. Kester; Andrew F. Donnell; Yan Lou; Stacy W. Remiszewski; Louis J. Lombardo; Shaoqing Chen; Nam T. Le; Jennifer Lo; John A. Moliterni; Xiaochun Han; J. Heather Hogg; Weiling Liang; Christophe Michoud; Kenneth C. Rupert; Steven Mischke; Kang Le; Martin Weisel; Cheryl A. Janson; Christine M. Lukacs; Adrian J. Fretland; Kyoungja Hong; Ann Polonskaia; Lin Gao; Shirley Li; Dave S. Solis; Doug Aguilar; Christine Tardell; Mark Dvorozniak; Shahid Tannu; Edmund C. Lee; Andy D. Schutt; Barry Goggin

doi:10.1021/jm400732v

Optimization of benzodiazepinones as selective inhibitors of the X-linked inhibitor of apoptosis protein (XIAP) second baculovirus IAP repeat (BIR2) domain

Robert F. Kester, Andrew F. Donnell, Yan Lou, Stacy W. Remiszewski, Louis J. Lombardo, Shaoqing Chen, Nam T. Le, Jennifer Lo, John A. Moliterni, Xiaochun Han, J. Heather Hogg, Weiling Liang, Christophe Michoud, Kenneth C. Rupert, Steven Mischke, Kang Le, Martin Weisel, Cheryl A. Janson, Christine M. Lukacs, Adrian J. FretlandKyoungja Hong, Ann Polonskaia, Lin Gao, Shirley Li, Dave S. Solis, Doug Aguilar, Christine Tardell, Mark Dvorozniak, Shahid Tannu, Edmund C. Lee, Andy D. Schutt, Barry Goggin

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

30 Scopus citations

Abstract

The IAPs are key regulators of the apoptotic pathways and are commonly overexpressed in many cancer cells. IAPs contain one to three BIR domains that are crucial for their inhibitory function. The pro-survival properties of XIAP come from binding of the BIR domains to the pro-apoptotic caspases. The BIR3 domain of XIAP binds and inhibits caspase 9, while the BIR2 domain binds and inhibits the terminal caspases 3 and 7. While XIAP BIR3 inhibitors have previously been reported, they also inhibit cIAP1/2 and promote the release of TNFα, potentially limiting their therapeutic utility. This paper will focus on the optimization of selective XIAP BIR2 inhibitors leading to the discovery of highly potent benzodiazepinone 36 (IC₅₀ = 45 nM), which has high levels of selectivity over XIAP BIR3 and cIAP1 BIR2/3 and shows efficacy in a xenograft pharmacodynamic model monitoring caspase activity while not promoting the release of TNFα in vitro.

Original language	English (US)
Pages (from-to)	7788-7803
Number of pages	16
Journal	Journal of Medicinal Chemistry
Volume	56
Issue number	20
DOIs	https://doi.org/10.1021/jm400732v
State	Published - Oct 24 2013
Externally published	Yes

ASJC Scopus subject areas

Molecular Medicine
Drug Discovery

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Kester, R. F., Donnell, A. F., Lou, Y., Remiszewski, S. W., Lombardo, L. J., Chen, S., Le, N. T., Lo, J., Moliterni, J. A., Han, X., Heather Hogg, J., Liang, W., Michoud, C., Rupert, K. C., Mischke, S., Le, K., Weisel, M., Janson, C. A., Lukacs, C. M., ... Goggin, B. (2013). Optimization of benzodiazepinones as selective inhibitors of the X-linked inhibitor of apoptosis protein (XIAP) second baculovirus IAP repeat (BIR2) domain. Journal of Medicinal Chemistry, 56(20), 7788-7803. https://doi.org/10.1021/jm400732v

Kester, RF, Donnell, AF, Lou, Y, Remiszewski, SW, Lombardo, LJ, Chen, S, Le, NT, Lo, J, Moliterni, JA, Han, X, Heather Hogg, J, Liang, W, Michoud, C, Rupert, KC, Mischke, S, Le, K, Weisel, M, Janson, CA, Lukacs, CM, Fretland, AJ, Hong, K, Polonskaia, A, Gao, L, Li, S, Solis, DS, Aguilar, D, Tardell, C, Dvorozniak, M, Tannu, S, Lee, EC, Schutt, AD & Goggin, B 2013, 'Optimization of benzodiazepinones as selective inhibitors of the X-linked inhibitor of apoptosis protein (XIAP) second baculovirus IAP repeat (BIR2) domain', Journal of Medicinal Chemistry, vol. 56, no. 20, pp. 7788-7803. https://doi.org/10.1021/jm400732v

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title = "Optimization of benzodiazepinones as selective inhibitors of the X-linked inhibitor of apoptosis protein (XIAP) second baculovirus IAP repeat (BIR2) domain",

abstract = "The IAPs are key regulators of the apoptotic pathways and are commonly overexpressed in many cancer cells. IAPs contain one to three BIR domains that are crucial for their inhibitory function. The pro-survival properties of XIAP come from binding of the BIR domains to the pro-apoptotic caspases. The BIR3 domain of XIAP binds and inhibits caspase 9, while the BIR2 domain binds and inhibits the terminal caspases 3 and 7. While XIAP BIR3 inhibitors have previously been reported, they also inhibit cIAP1/2 and promote the release of TNFα, potentially limiting their therapeutic utility. This paper will focus on the optimization of selective XIAP BIR2 inhibitors leading to the discovery of highly potent benzodiazepinone 36 (IC50 = 45 nM), which has high levels of selectivity over XIAP BIR3 and cIAP1 BIR2/3 and shows efficacy in a xenograft pharmacodynamic model monitoring caspase activity while not promoting the release of TNFα in vitro.",

author = "Kester, {Robert F.} and Donnell, {Andrew F.} and Yan Lou and Remiszewski, {Stacy W.} and Lombardo, {Louis J.} and Shaoqing Chen and Le, {Nam T.} and Jennifer Lo and Moliterni, {John A.} and Xiaochun Han and {Heather Hogg}, J. and Weiling Liang and Christophe Michoud and Rupert, {Kenneth C.} and Steven Mischke and Kang Le and Martin Weisel and Janson, {Cheryl A.} and Lukacs, {Christine M.} and Fretland, {Adrian J.} and Kyoungja Hong and Ann Polonskaia and Lin Gao and Shirley Li and Solis, {Dave S.} and Doug Aguilar and Christine Tardell and Mark Dvorozniak and Shahid Tannu and Lee, {Edmund C.} and Schutt, {Andy D.} and Barry Goggin",

year = "2013",

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doi = "10.1021/jm400732v",

language = "English (US)",

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AU - Kester, Robert F.

AU - Donnell, Andrew F.

AU - Lou, Yan

AU - Remiszewski, Stacy W.

AU - Lombardo, Louis J.

AU - Chen, Shaoqing

AU - Le, Nam T.

AU - Lo, Jennifer

AU - Moliterni, John A.

AU - Han, Xiaochun

AU - Heather Hogg, J.

AU - Liang, Weiling

AU - Michoud, Christophe

AU - Rupert, Kenneth C.

AU - Mischke, Steven

AU - Le, Kang

AU - Weisel, Martin

AU - Janson, Cheryl A.

AU - Lukacs, Christine M.

AU - Fretland, Adrian J.

AU - Hong, Kyoungja

AU - Polonskaia, Ann

AU - Gao, Lin

AU - Li, Shirley

AU - Solis, Dave S.

AU - Aguilar, Doug

AU - Tardell, Christine

AU - Dvorozniak, Mark

AU - Tannu, Shahid

AU - Lee, Edmund C.

AU - Schutt, Andy D.

AU - Goggin, Barry

PY - 2013/10/24

Y1 - 2013/10/24

N2 - The IAPs are key regulators of the apoptotic pathways and are commonly overexpressed in many cancer cells. IAPs contain one to three BIR domains that are crucial for their inhibitory function. The pro-survival properties of XIAP come from binding of the BIR domains to the pro-apoptotic caspases. The BIR3 domain of XIAP binds and inhibits caspase 9, while the BIR2 domain binds and inhibits the terminal caspases 3 and 7. While XIAP BIR3 inhibitors have previously been reported, they also inhibit cIAP1/2 and promote the release of TNFα, potentially limiting their therapeutic utility. This paper will focus on the optimization of selective XIAP BIR2 inhibitors leading to the discovery of highly potent benzodiazepinone 36 (IC50 = 45 nM), which has high levels of selectivity over XIAP BIR3 and cIAP1 BIR2/3 and shows efficacy in a xenograft pharmacodynamic model monitoring caspase activity while not promoting the release of TNFα in vitro.

AB - The IAPs are key regulators of the apoptotic pathways and are commonly overexpressed in many cancer cells. IAPs contain one to three BIR domains that are crucial for their inhibitory function. The pro-survival properties of XIAP come from binding of the BIR domains to the pro-apoptotic caspases. The BIR3 domain of XIAP binds and inhibits caspase 9, while the BIR2 domain binds and inhibits the terminal caspases 3 and 7. While XIAP BIR3 inhibitors have previously been reported, they also inhibit cIAP1/2 and promote the release of TNFα, potentially limiting their therapeutic utility. This paper will focus on the optimization of selective XIAP BIR2 inhibitors leading to the discovery of highly potent benzodiazepinone 36 (IC50 = 45 nM), which has high levels of selectivity over XIAP BIR3 and cIAP1 BIR2/3 and shows efficacy in a xenograft pharmacodynamic model monitoring caspase activity while not promoting the release of TNFα in vitro.

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Optimization of benzodiazepinones as selective inhibitors of the X-linked inhibitor of apoptosis protein (XIAP) second baculovirus IAP repeat (BIR2) domain

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