Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs

Research output: Contribution to journalJournal articleResearchpeer-review

Standard

Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs. / Winther, Anne-Marie Lund; Liu, Huizhen; Sonntag, Yonathan; Olesen, Claus; le Maire, Marc; Søhoel, Helmer; Olsen, C Erik; Christensen, Søren Brøgger; Nissen, Poul; Møller, Jesper Vuust.

In: Journal of Biological Chemistry, Vol. 285, No. 37, 2010, p. 28883-28892.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Winther, A-ML, Liu, H, Sonntag, Y, Olesen, C, le Maire, M, Søhoel, H, Olsen, CE, Christensen, SB, Nissen, P & Møller, JV 2010, 'Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs', Journal of Biological Chemistry, vol. 285, no. 37, pp. 28883-28892. https://doi.org/10.1074/jbc.M110.136242

APA

Winther, A-M. L., Liu, H., Sonntag, Y., Olesen, C., le Maire, M., Søhoel, H., Olsen, C. E., Christensen, S. B., Nissen, P., & Møller, J. V. (2010). Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs. Journal of Biological Chemistry, 285(37), 28883-28892. https://doi.org/10.1074/jbc.M110.136242

Vancouver

Winther A-ML, Liu H, Sonntag Y, Olesen C, le Maire M, Søhoel H et al. Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs. Journal of Biological Chemistry. 2010;285(37):28883-28892. https://doi.org/10.1074/jbc.M110.136242

Author

Winther, Anne-Marie Lund ; Liu, Huizhen ; Sonntag, Yonathan ; Olesen, Claus ; le Maire, Marc ; Søhoel, Helmer ; Olsen, C Erik ; Christensen, Søren Brøgger ; Nissen, Poul ; Møller, Jesper Vuust. / Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs. In: Journal of Biological Chemistry. 2010 ; Vol. 285, No. 37. pp. 28883-28892.

Bibtex

@article{a033a390ba6b11df825b000ea68e967b,
title = "Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs",
abstract = "Thapsigargin (Tg), a specific inhibitor of sarco/endoplasmic Ca(2+)-ATPases (SERCA), binds with high affinity to the E2 conformation of these ATPases. SERCA inhibition leads to elevated calcium levels in the cytoplasm, which in turn induces apoptosis. We present x-ray crystallographic and intrinsic fluorescence data to show how Tg and chemical analogs of the compound with modified or removed side chains bind to isolated SERCA 1a membranes. This occurs by uptake via the membrane lipid followed by insertion into a resident intramembranous binding site with few adaptative changes. Our binding data indicate that a balanced hydrophobicity and accurate positioning of the side chains, provided by the central guaianolide ring structure, defines a pharmacophore of Tg that governs both high affinity and access to the protein-binding site. Tg analogs substituted with long linkers at O-8 extend from the binding site between transmembrane segments to the putative N-terminal Ca(2+) entry pathway. The long chain analogs provide a rational basis for the localization of the linker, the presence of which is necessary for enabling prostate-specific antigen to cleave peptide-conjugated prodrugs targeting SERCA of cancer cells (Denmeade, S. R., Jakobsen, C. M., Janssen, S., Khan, S. R., Garrett, E. S., Lilja, H., Christensen, S. B., and Isaacs, J. T. (2003) J. Natl. Cancer Inst. 95, 990-1000). Our study demonstrates the usefulness of a simple in vitro system to test and direct development toward the formulation of new Tg derivatives with improved properties for SERCA targeting. Finally, we propose that the Tg binding pocket may be a regulatory site that, for example, is sensitive to cholesterol.",
keywords = "Former Faculty of Life Sciences",
author = "Winther, {Anne-Marie Lund} and Huizhen Liu and Yonathan Sonntag and Claus Olesen and {le Maire}, Marc and Helmer S{\o}hoel and Olsen, {C Erik} and Christensen, {S{\o}ren Br{\o}gger} and Poul Nissen and M{\o}ller, {Jesper Vuust}",
year = "2010",
doi = "10.1074/jbc.M110.136242",
language = "English",
volume = "285",
pages = "28883--28892",
journal = "Journal of Biological Chemistry",
issn = "0021-9258",
publisher = "American Society for Biochemistry and Molecular Biology, Inc.",
number = "37",

}

RIS

TY - JOUR

T1 - Critical roles of hydrophobicity and orientation of side chains for inactivation of sarcoplasmic reticulum Ca2+-ATPase with thapsigargin and thapsigargin analogs

AU - Winther, Anne-Marie Lund

AU - Liu, Huizhen

AU - Sonntag, Yonathan

AU - Olesen, Claus

AU - le Maire, Marc

AU - Søhoel, Helmer

AU - Olsen, C Erik

AU - Christensen, Søren Brøgger

AU - Nissen, Poul

AU - Møller, Jesper Vuust

PY - 2010

Y1 - 2010

N2 - Thapsigargin (Tg), a specific inhibitor of sarco/endoplasmic Ca(2+)-ATPases (SERCA), binds with high affinity to the E2 conformation of these ATPases. SERCA inhibition leads to elevated calcium levels in the cytoplasm, which in turn induces apoptosis. We present x-ray crystallographic and intrinsic fluorescence data to show how Tg and chemical analogs of the compound with modified or removed side chains bind to isolated SERCA 1a membranes. This occurs by uptake via the membrane lipid followed by insertion into a resident intramembranous binding site with few adaptative changes. Our binding data indicate that a balanced hydrophobicity and accurate positioning of the side chains, provided by the central guaianolide ring structure, defines a pharmacophore of Tg that governs both high affinity and access to the protein-binding site. Tg analogs substituted with long linkers at O-8 extend from the binding site between transmembrane segments to the putative N-terminal Ca(2+) entry pathway. The long chain analogs provide a rational basis for the localization of the linker, the presence of which is necessary for enabling prostate-specific antigen to cleave peptide-conjugated prodrugs targeting SERCA of cancer cells (Denmeade, S. R., Jakobsen, C. M., Janssen, S., Khan, S. R., Garrett, E. S., Lilja, H., Christensen, S. B., and Isaacs, J. T. (2003) J. Natl. Cancer Inst. 95, 990-1000). Our study demonstrates the usefulness of a simple in vitro system to test and direct development toward the formulation of new Tg derivatives with improved properties for SERCA targeting. Finally, we propose that the Tg binding pocket may be a regulatory site that, for example, is sensitive to cholesterol.

AB - Thapsigargin (Tg), a specific inhibitor of sarco/endoplasmic Ca(2+)-ATPases (SERCA), binds with high affinity to the E2 conformation of these ATPases. SERCA inhibition leads to elevated calcium levels in the cytoplasm, which in turn induces apoptosis. We present x-ray crystallographic and intrinsic fluorescence data to show how Tg and chemical analogs of the compound with modified or removed side chains bind to isolated SERCA 1a membranes. This occurs by uptake via the membrane lipid followed by insertion into a resident intramembranous binding site with few adaptative changes. Our binding data indicate that a balanced hydrophobicity and accurate positioning of the side chains, provided by the central guaianolide ring structure, defines a pharmacophore of Tg that governs both high affinity and access to the protein-binding site. Tg analogs substituted with long linkers at O-8 extend from the binding site between transmembrane segments to the putative N-terminal Ca(2+) entry pathway. The long chain analogs provide a rational basis for the localization of the linker, the presence of which is necessary for enabling prostate-specific antigen to cleave peptide-conjugated prodrugs targeting SERCA of cancer cells (Denmeade, S. R., Jakobsen, C. M., Janssen, S., Khan, S. R., Garrett, E. S., Lilja, H., Christensen, S. B., and Isaacs, J. T. (2003) J. Natl. Cancer Inst. 95, 990-1000). Our study demonstrates the usefulness of a simple in vitro system to test and direct development toward the formulation of new Tg derivatives with improved properties for SERCA targeting. Finally, we propose that the Tg binding pocket may be a regulatory site that, for example, is sensitive to cholesterol.

KW - Former Faculty of Life Sciences

U2 - 10.1074/jbc.M110.136242

DO - 10.1074/jbc.M110.136242

M3 - Journal article

C2 - 20551329

VL - 285

SP - 28883

EP - 28892

JO - Journal of Biological Chemistry

JF - Journal of Biological Chemistry

SN - 0021-9258

IS - 37

ER -

ID: 21858369