Novel unit B cryptophycin analogues as payloads for targeted therapy

Eduard Figueras; Adina Borbély; Mohamed Ismail; Marcel Frese; Norbert Sewald

doi:10.3762/bjoc.14.109

Novel unit B cryptophycin analogues as payloads for targeted therapy

Eduard Figueras, Adina Borbély, Mohamed Ismail, Marcel Frese, Norbert Sewald

Bielefeld University

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

Abstract

Cryptophycins are naturally occurring cytotoxins with great potential for chemotherapy. Since targeted therapy provides new perspectives for treatment of cancer, new potent analogues of cytotoxic agents containing functional groups for conjugation to homing devices are required. We describe the design, synthesis and biological evaluation of three new unit B cryptophycin analogues. The O-methyl group of the unit B D-tyrosine analogue was replaced by an O-(allyloxyethyl) moiety, an O-(hydroxyethyl) group, or an O-(((azidoethoxy)ethoxy)ethoyxethyl) substituent. While the former two maintain cytotoxicity in the subnanomolar range, the attachment of the triethylene glycol spacer with a terminal azide results in a complete loss of activity. Docking studies of the novel cryptophycin analogues to β-tubulin provided a rationale for the observed cytotoxicities.

Original language	English
Pages (from-to)	1281-1286
Number of pages	6
Journal	Beilstein Journal of Organic Chemistry
Volume	14
DOIs	https://doi.org/10.3762/bjoc.14.109
Publication status	Published - 2018
Externally published	Yes

Free keywords

Cryptophycin
Cytotoxic agents
Novel payloads
Tubulin inhibitors
Tumour targeting

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

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10.3762/bjoc.14.109Licence: CC BY

Cite this

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title = "Novel unit B cryptophycin analogues as payloads for targeted therapy",

abstract = "Cryptophycins are naturally occurring cytotoxins with great potential for chemotherapy. Since targeted therapy provides new perspectives for treatment of cancer, new potent analogues of cytotoxic agents containing functional groups for conjugation to homing devices are required. We describe the design, synthesis and biological evaluation of three new unit B cryptophycin analogues. The O-methyl group of the unit B D-tyrosine analogue was replaced by an O-(allyloxyethyl) moiety, an O-(hydroxyethyl) group, or an O-(((azidoethoxy)ethoxy)ethoyxethyl) substituent. While the former two maintain cytotoxicity in the subnanomolar range, the attachment of the triethylene glycol spacer with a terminal azide results in a complete loss of activity. Docking studies of the novel cryptophycin analogues to β-tubulin provided a rationale for the observed cytotoxicities.",

keywords = "Cryptophycin, Cytotoxic agents, Novel payloads, Tubulin inhibitors, Tumour targeting",

author = "Eduard Figueras and Adina Borb{\'e}ly and Mohamed Ismail and Marcel Frese and Norbert Sewald",

year = "2018",

doi = "10.3762/bjoc.14.109",

language = "English",

volume = "14",

pages = "1281--1286",

journal = "Beilstein Journal of Organic Chemistry",

issn = "1860-5397",

publisher = "Beilstein-Institut Zur Forderung der Chemischen Wissenschaften",

}

TY - JOUR

T1 - Novel unit B cryptophycin analogues as payloads for targeted therapy

AU - Figueras, Eduard

AU - Borbély, Adina

AU - Ismail, Mohamed

AU - Frese, Marcel

AU - Sewald, Norbert

PY - 2018

Y1 - 2018

N2 - Cryptophycins are naturally occurring cytotoxins with great potential for chemotherapy. Since targeted therapy provides new perspectives for treatment of cancer, new potent analogues of cytotoxic agents containing functional groups for conjugation to homing devices are required. We describe the design, synthesis and biological evaluation of three new unit B cryptophycin analogues. The O-methyl group of the unit B D-tyrosine analogue was replaced by an O-(allyloxyethyl) moiety, an O-(hydroxyethyl) group, or an O-(((azidoethoxy)ethoxy)ethoyxethyl) substituent. While the former two maintain cytotoxicity in the subnanomolar range, the attachment of the triethylene glycol spacer with a terminal azide results in a complete loss of activity. Docking studies of the novel cryptophycin analogues to β-tubulin provided a rationale for the observed cytotoxicities.

AB - Cryptophycins are naturally occurring cytotoxins with great potential for chemotherapy. Since targeted therapy provides new perspectives for treatment of cancer, new potent analogues of cytotoxic agents containing functional groups for conjugation to homing devices are required. We describe the design, synthesis and biological evaluation of three new unit B cryptophycin analogues. The O-methyl group of the unit B D-tyrosine analogue was replaced by an O-(allyloxyethyl) moiety, an O-(hydroxyethyl) group, or an O-(((azidoethoxy)ethoxy)ethoyxethyl) substituent. While the former two maintain cytotoxicity in the subnanomolar range, the attachment of the triethylene glycol spacer with a terminal azide results in a complete loss of activity. Docking studies of the novel cryptophycin analogues to β-tubulin provided a rationale for the observed cytotoxicities.

KW - Cryptophycin

KW - Cytotoxic agents

KW - Novel payloads

KW - Tubulin inhibitors

KW - Tumour targeting

U2 - 10.3762/bjoc.14.109

DO - 10.3762/bjoc.14.109

M3 - Article

AN - SCOPUS:85048224750

SN - 1860-5397

VL - 14

SP - 1281

EP - 1286

JO - Beilstein Journal of Organic Chemistry

JF - Beilstein Journal of Organic Chemistry

ER -

Novel unit B cryptophycin analogues as payloads for targeted therapy

Abstract

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