Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP)

Maximilian A. Seiter; Stefan Salcher; Martina Rupp; Judith Hagenbuchner; Ursula Kiechl-Kohlendorfer; Jérémie Mortier; Gerhard Wolber; Judith M. Rollinger; Petra Obexer; Michael J. Ausserlechner

doi:10.1016/j.fob.2014.07.001

Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP)

Maximilian A. Seiter
, Stefan Salcher
, Martina Rupp
, Judith Hagenbuchner
, Ursula Kiechl-Kohlendorfer
, Jérémie Mortier
, Gerhard Wolber
, Judith M. Rollinger
, Petra Obexer
, Michael J. Ausserlechner

Publications: Contribution to journal › Article › Peer Reviewed

Abstract

Defects in the regulation of apoptosis are one main cause of cancer development and may result from overexpression of anti-apoptotic proteins such as the X-linked inhibitor of apoptosis protein (XIAP). XIAP is frequently overexpressed in human leukemia and prostate and breast tumors. Inhibition of apoptosis by XIAP is mainly coordinated through direct binding to the initiator caspase-9 via its baculovirus-IAP-repeat-3 (BIR3) domain. XIAP inhibits caspases directly making it to an attractive target for anti-cancer therapy. In the search for novel, non-peptidic XIAP inhibitors in this study we focused on the chemical constituents of sāng bái pí (mulberry root bark). Most promising candidates of this plant were tested biochemically in vitro by a fluorescence polarization (FP) assay and in vivo via protein fragment complementation analysis (PCA). We identified the Diels Alder adduct Sanggenon G (SG. 1) as a novel, small-molecular weight inhibitor of XIAP. As shown by FP and PCA analyses, SG. 1 binds specifically to the BIR3 domain of XIAP with a binding affinity of 34.26. μM. Treatment of the transgenic leukemia cell line Molt3/XIAP with SG. 1 enhances caspase-8, -3 and -9 cleavage, displaces caspase-9 from XIAP as determined by immunoprecipitation experiments and sensitizes these cells to etoposide-induced apoptosis. SG. 1 not only sensitizes the XIAP-overexpressing leukemia cell line Molt3/XIAP to etoposide treatment but also different neuroblastoma cell lines endogenously expressing high XIAP levels. Taken together, Sanggenon G (SG. 1) is a novel, natural, non-peptidic, small-molecular inhibitor of XIAP that can serve as a starting point to develop a new class of improved XIAP inhibitors.

Original language	English
Pages (from-to)	659-671
Number of pages	13
Journal	FEBS Open Bio
Volume	4
Issue number	1
DOIs	https://doi.org/10.1016/j.fob.2014.07.001
Publication status	Published - 2014
Externally published	Yes

Funding

The authors thank Gerhard Gaedicke for support and valuable discussion, John Silke for donating plasmids and Soeren Heiderstadt for technical assistance in re-isolation of natural compounds. This work was supported by grants by the COMET Center ONCOTYROL, which is funded by the Austrian Federal Ministries BMVIT/BMWFJ (via FFG) and the TirolerZukunftsstiftung/Standortagentur Tirol, by the ”Kinderkrebshilfe Tirol und Vorarlberg”, the “Kinderkrebshilfe Südtirol-Regenbogen”, the “Krebshilfe Südtirol”, the “SVP-Frauen”, the “Provita Kinderleukämie Stiftung” and the “MFF-Tirol”. The Tyrolean Cancer Research Institute and this study are supported by the “Tiroler Landeskrankenanstalten Ges.m.b.H. (TILAK)” and the Tyrolean Cancer Society.

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Austrian Fields of Science 2012

301204 Pharmacognosy

Keywords

Cell permeable
Natural
Sanggenon G
Small-molecular weight
XIAP inhibitor

Access to Document

10.1016/j.fob.2014.07.001Licence: CC BY-NC-ND 3.0

Cite this

Seiter, M. A., Salcher, S., Rupp, M., Hagenbuchner, J., Kiechl-Kohlendorfer, U., Mortier, J., Wolber, G., Rollinger, J. M., Obexer, P., & Ausserlechner, M. J. (2014). Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP). FEBS Open Bio, 4(1), 659-671. https://doi.org/10.1016/j.fob.2014.07.001

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title = "Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP)",

abstract = "Defects in the regulation of apoptosis are one main cause of cancer development and may result from overexpression of anti-apoptotic proteins such as the X-linked inhibitor of apoptosis protein (XIAP). XIAP is frequently overexpressed in human leukemia and prostate and breast tumors. Inhibition of apoptosis by XIAP is mainly coordinated through direct binding to the initiator caspase-9 via its baculovirus-IAP-repeat-3 (BIR3) domain. XIAP inhibits caspases directly making it to an attractive target for anti-cancer therapy. In the search for novel, non-peptidic XIAP inhibitors in this study we focused on the chemical constituents of sāng b{\'a}i p{\'i} (mulberry root bark). Most promising candidates of this plant were tested biochemically in vitro by a fluorescence polarization (FP) assay and in vivo via protein fragment complementation analysis (PCA). We identified the Diels Alder adduct Sanggenon G (SG. 1) as a novel, small-molecular weight inhibitor of XIAP. As shown by FP and PCA analyses, SG. 1 binds specifically to the BIR3 domain of XIAP with a binding affinity of 34.26. μM. Treatment of the transgenic leukemia cell line Molt3/XIAP with SG. 1 enhances caspase-8, -3 and -9 cleavage, displaces caspase-9 from XIAP as determined by immunoprecipitation experiments and sensitizes these cells to etoposide-induced apoptosis. SG. 1 not only sensitizes the XIAP-overexpressing leukemia cell line Molt3/XIAP to etoposide treatment but also different neuroblastoma cell lines endogenously expressing high XIAP levels. Taken together, Sanggenon G (SG. 1) is a novel, natural, non-peptidic, small-molecular inhibitor of XIAP that can serve as a starting point to develop a new class of improved XIAP inhibitors.",

keywords = "Cell permeable, Natural, Sanggenon G, Small-molecular weight, XIAP inhibitor",

author = "Seiter, \{Maximilian A.\} and Stefan Salcher and Martina Rupp and Judith Hagenbuchner and Ursula Kiechl-Kohlendorfer and J{\'e}r{\'e}mie Mortier and Gerhard Wolber and Rollinger, \{Judith M.\} and Petra Obexer and Ausserlechner, \{Michael J.\}",

note = "Funding Information: The authors thank Gerhard Gaedicke for support and valuable discussion, John Silke for donating plasmids and Soeren Heiderstadt for technical assistance in re-isolation of natural compounds. This work was supported by grants by the COMET Center ONCOTYROL, which is funded by the Austrian Federal Ministries BMVIT/BMWFJ (via FFG) and the TirolerZukunftsstiftung/Standortagentur Tirol, by the ”Kinderkrebshilfe Tirol und Vorarlberg”, the “Kinderkrebshilfe S{\"u}dtirol-Regenbogen”, the “Krebshilfe S{\"u}dtirol”, the “SVP-Frauen”, the “Provita Kinderleuk{\"a}mie Stiftung” and the “MFF-Tirol”. The Tyrolean Cancer Research Institute and this study are supported by the “Tiroler Landeskrankenanstalten Ges.m.b.H. (TILAK)” and the Tyrolean Cancer Society. Copyright: Copyright 2014 Elsevier B.V., All rights reserved.",

year = "2014",

doi = "10.1016/j.fob.2014.07.001",

language = "English",

volume = "4",

pages = "659--671",

journal = "FEBS Open Bio",

issn = "2211-5463",

publisher = "Wiley",

number = "1",

}

Seiter, MA, Salcher, S, Rupp, M, Hagenbuchner, J, Kiechl-Kohlendorfer, U, Mortier, J, Wolber, G, Rollinger, JM, Obexer, P & Ausserlechner, MJ 2014, 'Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP)', FEBS Open Bio, vol. 4, no. 1, pp. 659-671. https://doi.org/10.1016/j.fob.2014.07.001

TY - JOUR

T1 - Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP)

AU - Seiter, Maximilian A.

AU - Salcher, Stefan

AU - Rupp, Martina

AU - Hagenbuchner, Judith

AU - Kiechl-Kohlendorfer, Ursula

AU - Mortier, Jérémie

AU - Wolber, Gerhard

AU - Rollinger, Judith M.

AU - Obexer, Petra

AU - Ausserlechner, Michael J.

N1 - Funding Information: The authors thank Gerhard Gaedicke for support and valuable discussion, John Silke for donating plasmids and Soeren Heiderstadt for technical assistance in re-isolation of natural compounds. This work was supported by grants by the COMET Center ONCOTYROL, which is funded by the Austrian Federal Ministries BMVIT/BMWFJ (via FFG) and the TirolerZukunftsstiftung/Standortagentur Tirol, by the ”Kinderkrebshilfe Tirol und Vorarlberg”, the “Kinderkrebshilfe Südtirol-Regenbogen”, the “Krebshilfe Südtirol”, the “SVP-Frauen”, the “Provita Kinderleukämie Stiftung” and the “MFF-Tirol”. The Tyrolean Cancer Research Institute and this study are supported by the “Tiroler Landeskrankenanstalten Ges.m.b.H. (TILAK)” and the Tyrolean Cancer Society. Copyright: Copyright 2014 Elsevier B.V., All rights reserved.

PY - 2014

Y1 - 2014

N2 - Defects in the regulation of apoptosis are one main cause of cancer development and may result from overexpression of anti-apoptotic proteins such as the X-linked inhibitor of apoptosis protein (XIAP). XIAP is frequently overexpressed in human leukemia and prostate and breast tumors. Inhibition of apoptosis by XIAP is mainly coordinated through direct binding to the initiator caspase-9 via its baculovirus-IAP-repeat-3 (BIR3) domain. XIAP inhibits caspases directly making it to an attractive target for anti-cancer therapy. In the search for novel, non-peptidic XIAP inhibitors in this study we focused on the chemical constituents of sāng bái pí (mulberry root bark). Most promising candidates of this plant were tested biochemically in vitro by a fluorescence polarization (FP) assay and in vivo via protein fragment complementation analysis (PCA). We identified the Diels Alder adduct Sanggenon G (SG. 1) as a novel, small-molecular weight inhibitor of XIAP. As shown by FP and PCA analyses, SG. 1 binds specifically to the BIR3 domain of XIAP with a binding affinity of 34.26. μM. Treatment of the transgenic leukemia cell line Molt3/XIAP with SG. 1 enhances caspase-8, -3 and -9 cleavage, displaces caspase-9 from XIAP as determined by immunoprecipitation experiments and sensitizes these cells to etoposide-induced apoptosis. SG. 1 not only sensitizes the XIAP-overexpressing leukemia cell line Molt3/XIAP to etoposide treatment but also different neuroblastoma cell lines endogenously expressing high XIAP levels. Taken together, Sanggenon G (SG. 1) is a novel, natural, non-peptidic, small-molecular inhibitor of XIAP that can serve as a starting point to develop a new class of improved XIAP inhibitors.

AB - Defects in the regulation of apoptosis are one main cause of cancer development and may result from overexpression of anti-apoptotic proteins such as the X-linked inhibitor of apoptosis protein (XIAP). XIAP is frequently overexpressed in human leukemia and prostate and breast tumors. Inhibition of apoptosis by XIAP is mainly coordinated through direct binding to the initiator caspase-9 via its baculovirus-IAP-repeat-3 (BIR3) domain. XIAP inhibits caspases directly making it to an attractive target for anti-cancer therapy. In the search for novel, non-peptidic XIAP inhibitors in this study we focused on the chemical constituents of sāng bái pí (mulberry root bark). Most promising candidates of this plant were tested biochemically in vitro by a fluorescence polarization (FP) assay and in vivo via protein fragment complementation analysis (PCA). We identified the Diels Alder adduct Sanggenon G (SG. 1) as a novel, small-molecular weight inhibitor of XIAP. As shown by FP and PCA analyses, SG. 1 binds specifically to the BIR3 domain of XIAP with a binding affinity of 34.26. μM. Treatment of the transgenic leukemia cell line Molt3/XIAP with SG. 1 enhances caspase-8, -3 and -9 cleavage, displaces caspase-9 from XIAP as determined by immunoprecipitation experiments and sensitizes these cells to etoposide-induced apoptosis. SG. 1 not only sensitizes the XIAP-overexpressing leukemia cell line Molt3/XIAP to etoposide treatment but also different neuroblastoma cell lines endogenously expressing high XIAP levels. Taken together, Sanggenon G (SG. 1) is a novel, natural, non-peptidic, small-molecular inhibitor of XIAP that can serve as a starting point to develop a new class of improved XIAP inhibitors.

KW - Cell permeable

KW - Natural

KW - Sanggenon G

KW - Small-molecular weight

KW - XIAP inhibitor

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U2 - 10.1016/j.fob.2014.07.001

DO - 10.1016/j.fob.2014.07.001

M3 - Article

AN - SCOPUS:84904897865

SN - 2211-5463

VL - 4

SP - 659

EP - 671

JO - FEBS Open Bio

JF - FEBS Open Bio

IS - 1

ER -

Discovery of Sanggenon G as a natural cell-permeable small-molecular weight inhibitor of X-linked inhibitor of apoptosis protein (XIAP)

Abstract

Funding

UN SDGs

Austrian Fields of Science 2012

Keywords

Access to Document

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