Quantitative chemoproteomic profiling reveals multiple target interactions of spongiolactone derivatives in leukemia cells

M. H. Wright; Y. Tao; J. Drechsel; J. Krysiak; S. Chamni; A. Weigert-Munoz; N. L. Harvey; D. Romo; S. A. Sieber

doi:10.1039/c7cc04990k

Quantitative chemoproteomic profiling reveals multiple target interactions of spongiolactone derivatives in leukemia cells

M. H. Wright, Y. Tao, J. Drechsel, J. Krysiak, S. Chamni, A. Weigert-Munoz, N. L. Harvey, D. Romo, S. A. Sieber

Lehrstuhl für Organische Chemie II

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

15 Zitate (Scopus)

Abstract

The spongiolactones are marine natural products with an unusual rearranged spongiane skeleton and a fused β-lactone ring. These compounds have potential anticancer properties but their mode of action has yet to be explored. Here we employ activity-based protein profiling to identify the targets of a more potent spongiolactone derivative in live cancer cells, and compare these to the targets of a simpler β-lactone. These hits provide the first insights into the covalent mechanism of action of this natural product class.

Originalsprache	Englisch
Seiten (von - bis)	12818-12821
Seitenumfang	4
Fachzeitschrift	Chemical Communications
Jahrgang	53
Ausgabenummer	95
DOIs	https://doi.org/10.1039/c7cc04990k
Publikationsstatus	Veröffentlicht - 2017

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abstract = "The spongiolactones are marine natural products with an unusual rearranged spongiane skeleton and a fused β-lactone ring. These compounds have potential anticancer properties but their mode of action has yet to be explored. Here we employ activity-based protein profiling to identify the targets of a more potent spongiolactone derivative in live cancer cells, and compare these to the targets of a simpler β-lactone. These hits provide the first insights into the covalent mechanism of action of this natural product class.",

author = "Wright, \{M. H.\} and Y. Tao and J. Drechsel and J. Krysiak and S. Chamni and A. Weigert-Munoz and Harvey, \{N. L.\} and D. Romo and Sieber, \{S. A.\}",

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doi = "10.1039/c7cc04990k",

language = "English",

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AU - Wright, M. H.

AU - Tao, Y.

AU - Drechsel, J.

AU - Krysiak, J.

AU - Chamni, S.

AU - Weigert-Munoz, A.

AU - Harvey, N. L.

AU - Romo, D.

AU - Sieber, S. A.

PY - 2017

Y1 - 2017

N2 - The spongiolactones are marine natural products with an unusual rearranged spongiane skeleton and a fused β-lactone ring. These compounds have potential anticancer properties but their mode of action has yet to be explored. Here we employ activity-based protein profiling to identify the targets of a more potent spongiolactone derivative in live cancer cells, and compare these to the targets of a simpler β-lactone. These hits provide the first insights into the covalent mechanism of action of this natural product class.

AB - The spongiolactones are marine natural products with an unusual rearranged spongiane skeleton and a fused β-lactone ring. These compounds have potential anticancer properties but their mode of action has yet to be explored. Here we employ activity-based protein profiling to identify the targets of a more potent spongiolactone derivative in live cancer cells, and compare these to the targets of a simpler β-lactone. These hits provide the first insights into the covalent mechanism of action of this natural product class.

UR - https://www.scopus.com/pages/publications/85035788477

U2 - 10.1039/c7cc04990k

DO - 10.1039/c7cc04990k

M3 - Article

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AN - SCOPUS:85035788477

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VL - 53

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EP - 12821

JO - Chemical Communications

JF - Chemical Communications

IS - 95

ER -

Quantitative chemoproteomic profiling reveals multiple target interactions of spongiolactone derivatives in leukemia cells

Abstract

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