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Het(aryl)isatin to het(aryl)aminoindoline scaffold hopping: A route to selective inhibitors of matrix metalloproteinases
Ivanov V.N., Agamennone M., Iusupov I.R., Laghezza A., Novoselov A.M., Manasova E.V., Altieri A., Tortorella P., Shtil A.A., Kurkin A.V.
Publication type: Journal Article
Publication date: 2022-01-01
scimago Q1
wos Q2
SJR: 0.888
CiteScore: 10.4
Impact factor: 5.2
ISSN: 18785352, 18785379
General Chemistry
General Chemical Engineering
Abstract
Matrix metalloproteinases (MMPs) are a large family of zinc-dependent endoproteases known to exert multiple regulatory roles in tumor progression. A variety of chemical classes have been explored for targeting individual MMP isoforms. In the present study, we further developed our isatin based scaffold BB0223107 capable of binding to and inactivating MMP-2 in a zinc-independent manner (Agamennone et al., 2016). Forty four new compounds were synthesized based on the modified BB0223107 . All compounds were tested in enzyme inhibition assays against MMP-2, −8 and −13. SAR studies demonstrated that 5-het(aryl)-3-aminoindolin-2-ones ( 37 – 39 ) were active toward MMP-2 and MMP-13. The most potent compounds 33 and 37 displayed an IC 50 of 3 µM against MMP-13 and showed a negligible activity toward MMP-8; almost all new compounds were inactive toward MMP-8. Replacement of the isatin ring with a biaryl system (compound 33 ) did not decrease the potency against MMP-13 but reduced the selectivity. Structure-based computational studies were carried out to rationalize the inhibitory activity data. The analysis of binding geometries confirmed that all fragments occupied the S1′ site in the three enzymes while no ligand was able to bind the catalytic zinc ion. To the best of our knowledge, this is the first example of 3-aminoindolin-2-one-based MMP inhibitors that, based on the computer modeling study, do not coordinate the zinc ion. Thus, the het(aryl)-3-aminoindolin-2-one derivatives emerge as a drug-like and promising chemotype that, along with the hetaryl variations, represents an alternative and thrifty tool for chemical space exploration aimed at MMP inhibitor design.
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Ivanov V. N. et al. Het(aryl)isatin to het(aryl)aminoindoline scaffold hopping: A route to selective inhibitors of matrix metalloproteinases // Arabian Journal of Chemistry. 2022. Vol. 15. No. 1. p. 103492.
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Ivanov V. N., Agamennone M., Iusupov I. R., Laghezza A., Novoselov A. M., Manasova E. V., Altieri A., Tortorella P., Shtil A. A., Kurkin A. V. Het(aryl)isatin to het(aryl)aminoindoline scaffold hopping: A route to selective inhibitors of matrix metalloproteinases // Arabian Journal of Chemistry. 2022. Vol. 15. No. 1. p. 103492.
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TY - JOUR
DO - 10.1016/j.arabjc.2021.103492
UR - https://doi.org/10.1016/j.arabjc.2021.103492
TI - Het(aryl)isatin to het(aryl)aminoindoline scaffold hopping: A route to selective inhibitors of matrix metalloproteinases
T2 - Arabian Journal of Chemistry
AU - Ivanov, V N
AU - Agamennone, M
AU - Iusupov, I R
AU - Laghezza, A
AU - Novoselov, A M
AU - Manasova, E V
AU - Altieri, A
AU - Tortorella, P
AU - Shtil, A A
AU - Kurkin, A V
PY - 2022
DA - 2022/01/01
PB - King Saud University
SP - 103492
IS - 1
VL - 15
SN - 1878-5352
SN - 1878-5379
ER -
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@article{2022_Ivanov,
author = {V N Ivanov and M Agamennone and I R Iusupov and A Laghezza and A M Novoselov and E V Manasova and A Altieri and P Tortorella and A A Shtil and A V Kurkin},
title = {Het(aryl)isatin to het(aryl)aminoindoline scaffold hopping: A route to selective inhibitors of matrix metalloproteinases},
journal = {Arabian Journal of Chemistry},
year = {2022},
volume = {15},
publisher = {King Saud University},
month = {jan},
url = {https://doi.org/10.1016/j.arabjc.2021.103492},
number = {1},
pages = {103492},
doi = {10.1016/j.arabjc.2021.103492}
}
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Ivanov, V. N., et al. “Het(aryl)isatin to het(aryl)aminoindoline scaffold hopping: A route to selective inhibitors of matrix metalloproteinases.” Arabian Journal of Chemistry, vol. 15, no. 1, Jan. 2022, p. 103492. https://doi.org/10.1016/j.arabjc.2021.103492.
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