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Hiding in plain sight : optimizing topoisomerase IIα inhibitors into Hsp90β selective binders
ID
Dernovšek, Jaka
(
Author
),
ID
Zajec, Živa
(
Author
),
ID
Urbančič, Dunja
(
Author
),
ID
Jug, Ana
(
Author
),
ID
Skok, Žiga
(
Author
),
ID
Ilaš, Janez
(
Author
),
ID
Zidar, Nace
(
Author
),
ID
Tomašič, Tihomir
(
Author
), et al.
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https://www.sciencedirect.com/science/article/pii/S0223523424008158
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Abstract
Due to their impact on several oncogenic client proteins, the Hsp90 family of chaperones has been widely studied for the development of potential anticancer agents. Although several Hsp90 inhibitors have entered clinical trials, most were unsuccessful because they induced a heat shock response (HSR). This issue can be circumvented by using isoform-selective inhibitors, but the high similarity in the ATP-binding sites between the isoforms presents a challenge. Given that Hsp90 shares a conserved Bergerat fold with bacterial DNA gyrase B and human topoisomerase IIα, we repurposed our ATP-competitive inhibitors of these two proteins for Hsp90 inhibition. We virtually screened a library of in-house inhibitors and identified eleven hits for evaluation of Hsp90 binding. Among these, compound 11 displayed low micromolar affinity for Hsp90 and demonstrated a 12-fold selectivity for Hsp90β over its closest isoform, Hsp90α. Out of 29 prepared analogs, 16 showed a preference for Hsp90β over Hsp90α. Furthermore, eleven of these compounds inhibited the growth of several cancer cell lines in vitro. Notably, compound 24e reduced intracellular levels of Hsp90 client proteins in MCF-7 cells, leading to cell cycle arrest in the G0/G1 phase without inducing HSR. This inhibitor exhibited at least a 27-fold preference for Hsp90β and was selective against topoisomerase IIα, a panel of 22 representative protein kinases, and proved to be non-toxic in a zebrafish larvae toxicology model. Finally, molecular modeling, corroborated by STD NMR studies, and the binding of 24e to the S52A mutant of Hsp90α confirmed that the serine to alanine switch drives the selectivity between the two cytoplasmic isoforms.
Language:
English
Keywords:
cancer
,
Hsp90
,
isoform selectivity
,
topoisomerase II
Work type:
Article
Typology:
1.01 - Original Scientific Article
Organization:
FFA - Faculty of Pharmacy
Publication status:
Published
Publication version:
Version of Record
Year:
2024
Number of pages:
37 str.
Numbering:
Vol. 280, art. 116934
PID:
20.500.12556/RUL-163785
UDC:
615.4:54:616-006-085
ISSN on article:
0223-5234
DOI:
10.1016/j.ejmech.2024.116934
COBISS.SI-ID:
210758915
Publication date in RUL:
10.10.2024
Views:
119
Downloads:
34
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Record is a part of a journal
Title:
European journal of medicinal chemistry
Shortened title:
Eur. j. med. chem.
Publisher:
Elsevier
ISSN:
0223-5234
COBISS.SI-ID:
25429760
Licences
License:
CC BY 4.0, Creative Commons Attribution 4.0 International
Link:
http://creativecommons.org/licenses/by/4.0/
Description:
This is the standard Creative Commons license that gives others maximum freedom to do what they want with the work as long as they credit the author.
Secondary language
Language:
Slovenian
Keywords:
Hsp90
,
izoformna selektivnost
,
topoizomeraza II
,
rak
,
medicina
,
farmacevtska kemija
Projects
Funder:
ARRS - Slovenian Research Agency
Project number:
P1-0208
Name:
Farmacevtska kemija: načrtovanje, sinteza in vrednotenje učinkovin
Funder:
ARRS - Slovenian Research Agency
Project number:
P1-0010
Name:
Folding in dinamika biomolekularnih sistemov
Funder:
ARRS - Slovenian Research Agency
Project number:
J1-1717
Name:
Razvoj novih zaviralcev Hsp90 s protitumornim delovanjem
Funder:
ARRS - Slovenian Research Agency
Project number:
BI-AT/23-24-008
Name:
Razvoj zaviralcev C-končne domene Hsp90 za zdravljenje otroških sarkomov
Funder:
ARRS - Slovenian Research Agency
Project number:
N1-0172
Name:
Fotokemijski pristop za odkrivanje naprednih ATP-kompetitivnih prob z zaviralnim delovanjem na topoizomerazo IIalfa
Funder:
ARRS - Slovenian Research Agency
Project number:
J1-4400
Name:
Vrednotenje prehodnih stanj proteinov
Funder:
ARRS - Slovenian Research Agency
Project number:
J1-50038
Name:
Nove terapije Ewingovega sarkoma, osnovane na zaviralcih Hsp90
Funder:
Other - Other funder or multiple funders
Funding programme:
Austrian Research Promotion Agency (FFG)
Project number:
858071
Acronym:
Danio4Can
Funder:
Other - Other funder or multiple funders
Funding programme:
Austrian Research Promotion Agency (FFG)
Project number:
7940628
Acronym:
Danio4Can
Funder:
FWF - Austrian Science Fund
Funding programme:
Principal Investigator Projects International
Project number:
I 6685
Name:
HSP90IES
Funder:
Other - Other funder or multiple funders
Funding programme:
American Lebanese Syrian Associated Charities
Funder:
NIH - National Institutes of Health
Project number:
R35GM142772
Funder:
Other - Other funder or multiple funders
Funding programme:
BMBWF, OeAD
Project number:
SI 29/2023
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