Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands

Han Kun Zhang; J. Brek Eaton; Li Fang Yu; Mieke Nys; Angelica Mazzolari; René Van Elk; August B. Smit; Vadim Alexandrov; Taleen Hanania; Emily Sabath; Allison Fedolak; Daniela Brunner; Ronald J. Lukas; Giulio Vistoli; Chris Ulens; Alan P. Kozikowski

doi:10.1021/jm3008739

Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands

Han Kun Zhang, J. Brek Eaton, Li Fang Yu, Mieke Nys, Angelica Mazzolari, René Van Elk, August B. Smit, Vadim Alexandrov, Taleen Hanania, Emily Sabath, Allison Fedolak, Daniela Brunner, Ronald J. Lukas, Giulio Vistoli, Chris Ulens, Alan P. Kozikowski

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

20 Scopus citations

Abstract

Structure-based drug design can potentially accelerate the development of new therapeutics. In this study, a cocrystal structure of the acetylcholine binding protein (AChBP) from Capitella teleta (Ct) in complex with a cyclopropane-containing selective α4β2-nicotinic acetylcholine receptor (nAChR) partial agonist (compound 5) was acquired. The structural determinants required for ligand binding obtained from this AChBP X-ray structure were used to refine a previous model of the human α4β2- nAChR, thus possibly providing a better understanding of the structure of the human receptor. To validate the potential application of the structure of the Ct-AChBP in the engineering of new α4β2-nAChR ligands, homology modeling methods, combined with in silico ADME calculations, were used to design analogues of compound 5. The most promising compound, 12, exhibited an improved metabolic stability in comparison to the parent compound 5 while retaining favorable pharmacological parameters together with appropriate behavioral end points in the rodent studies.

Original language	English (US)
Pages (from-to)	8028-8037
Number of pages	10
Journal	Journal of medicinal chemistry
Volume	55
Issue number	18
DOIs	https://doi.org/10.1021/jm3008739
State	Published - Sep 27 2012
Externally published	Yes

ASJC Scopus subject areas

Molecular Medicine
Drug Discovery

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Zhang, H. K., Eaton, J. B., Yu, L. F., Nys, M., Mazzolari, A., Van Elk, R., Smit, A. B., Alexandrov, V., Hanania, T., Sabath, E., Fedolak, A., Brunner, D., Lukas, R. J., Vistoli, G., Ulens, C., & Kozikowski, A. P. (2012). Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands. Journal of medicinal chemistry, 55(18), 8028-8037. https://doi.org/10.1021/jm3008739

Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands. / Zhang, Han Kun; Eaton, J. Brek; Yu, Li Fang et al.
In: Journal of medicinal chemistry, Vol. 55, No. 18, 27.09.2012, p. 8028-8037.

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

Zhang, HK, Eaton, JB, Yu, LF, Nys, M, Mazzolari, A, Van Elk, R, Smit, AB, Alexandrov, V, Hanania, T, Sabath, E, Fedolak, A, Brunner, D, Lukas, RJ, Vistoli, G, Ulens, C & Kozikowski, AP 2012, 'Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands', Journal of medicinal chemistry, vol. 55, no. 18, pp. 8028-8037. https://doi.org/10.1021/jm3008739

Zhang HK, Eaton JB, Yu LF, Nys M, Mazzolari A, Van Elk R et al. Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands. Journal of medicinal chemistry. 2012 Sep 27;55(18):8028-8037. doi: 10.1021/jm3008739

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title = "Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands",

abstract = "Structure-based drug design can potentially accelerate the development of new therapeutics. In this study, a cocrystal structure of the acetylcholine binding protein (AChBP) from Capitella teleta (Ct) in complex with a cyclopropane-containing selective α4β2-nicotinic acetylcholine receptor (nAChR) partial agonist (compound 5) was acquired. The structural determinants required for ligand binding obtained from this AChBP X-ray structure were used to refine a previous model of the human α4β2- nAChR, thus possibly providing a better understanding of the structure of the human receptor. To validate the potential application of the structure of the Ct-AChBP in the engineering of new α4β2-nAChR ligands, homology modeling methods, combined with in silico ADME calculations, were used to design analogues of compound 5. The most promising compound, 12, exhibited an improved metabolic stability in comparison to the parent compound 5 while retaining favorable pharmacological parameters together with appropriate behavioral end points in the rodent studies.",

author = "Zhang, {Han Kun} and Eaton, {J. Brek} and Yu, {Li Fang} and Mieke Nys and Angelica Mazzolari and {Van Elk}, Ren{\'e} and Smit, {August B.} and Vadim Alexandrov and Taleen Hanania and Emily Sabath and Allison Fedolak and Daniela Brunner and Lukas, {Ronald J.} and Giulio Vistoli and Chris Ulens and Kozikowski, {Alan P.}",

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AU - Zhang, Han Kun

AU - Eaton, J. Brek

AU - Yu, Li Fang

AU - Nys, Mieke

AU - Mazzolari, Angelica

AU - Van Elk, René

AU - Smit, August B.

AU - Alexandrov, Vadim

AU - Hanania, Taleen

AU - Sabath, Emily

AU - Fedolak, Allison

AU - Brunner, Daniela

AU - Lukas, Ronald J.

AU - Vistoli, Giulio

AU - Ulens, Chris

AU - Kozikowski, Alan P.

PY - 2012/9/27

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N2 - Structure-based drug design can potentially accelerate the development of new therapeutics. In this study, a cocrystal structure of the acetylcholine binding protein (AChBP) from Capitella teleta (Ct) in complex with a cyclopropane-containing selective α4β2-nicotinic acetylcholine receptor (nAChR) partial agonist (compound 5) was acquired. The structural determinants required for ligand binding obtained from this AChBP X-ray structure were used to refine a previous model of the human α4β2- nAChR, thus possibly providing a better understanding of the structure of the human receptor. To validate the potential application of the structure of the Ct-AChBP in the engineering of new α4β2-nAChR ligands, homology modeling methods, combined with in silico ADME calculations, were used to design analogues of compound 5. The most promising compound, 12, exhibited an improved metabolic stability in comparison to the parent compound 5 while retaining favorable pharmacological parameters together with appropriate behavioral end points in the rodent studies.

AB - Structure-based drug design can potentially accelerate the development of new therapeutics. In this study, a cocrystal structure of the acetylcholine binding protein (AChBP) from Capitella teleta (Ct) in complex with a cyclopropane-containing selective α4β2-nicotinic acetylcholine receptor (nAChR) partial agonist (compound 5) was acquired. The structural determinants required for ligand binding obtained from this AChBP X-ray structure were used to refine a previous model of the human α4β2- nAChR, thus possibly providing a better understanding of the structure of the human receptor. To validate the potential application of the structure of the Ct-AChBP in the engineering of new α4β2-nAChR ligands, homology modeling methods, combined with in silico ADME calculations, were used to design analogues of compound 5. The most promising compound, 12, exhibited an improved metabolic stability in comparison to the parent compound 5 while retaining favorable pharmacological parameters together with appropriate behavioral end points in the rodent studies.

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Insights into the structural determinants required for high-affinity binding of chiral cyclopropane-containing ligands to α4β2-nicotinic acetylcholine receptors: An integrated approach to behaviorally active nicotinic ligands

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