Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome

Marion G. Götz; Kacey Godwin; Rachel Price; Robert Dorn; Gabriel Merrill-Steskal; William Klemmer; Hunter Hansen; Gautam Produturi; Megan Rocha; Mathias Palmer; Lea Molacek; Zack Strater; Michael Groll

doi:10.1021/acsmedchemlett.4c00017

Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome

Marion G. Götz, Kacey Godwin, Rachel Price, Robert Dorn, Gabriel Merrill-Steskal, William Klemmer, Hunter Hansen, Gautam Produturi, Megan Rocha, Mathias Palmer, Lea Molacek, Zack Strater, Michael Groll

Lehrstuhl für Biochemie

Whitman College

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

1 Zitat (Scopus)

Abstract

Peptide macrocycles have recently gained attention as protease inhibitors due to their metabolic stability and specificity. However, the development of peptide macrocycles with improved binding potency has so far been challenging. Here we present macrocyclic peptides derived from the clinically applied proteasome inhibitor carfilzomib with an oxindole group that mimics the natural product TMC-95A. Fluorescence kinetic activity assays reveal a high potency of the oxindole group (IC₅₀ = 0.19 μM) compared with agents lacking this motif. X-ray structures of the ligands with the β5-subunit of the yeast 20S proteasome illustrate that the installed macrocycle forces strong hydrogen bonding of the oxindole group with β5-Gly23NH. Thus, the binding of our designed oxindole epoxyketones is entropically and enthalpically favored in contrast to more flexible proteasome inhibitors such as carfilzomib.

Originalsprache	Englisch
Seiten (von - bis)	533-539
Seitenumfang	7
Fachzeitschrift	ACS Medicinal Chemistry Letters
Jahrgang	15
Ausgabenummer	4
DOIs	https://doi.org/10.1021/acsmedchemlett.4c00017
Publikationsstatus	Veröffentlicht - 11 Apr. 2024

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10.1021/acsmedchemlett.4c00017

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Götz, M. G., Godwin, K., Price, R., Dorn, R., Merrill-Steskal, G., Klemmer, W., Hansen, H., Produturi, G., Rocha, M., Palmer, M., Molacek, L., Strater, Z., & Groll, M. (2024). Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome. ACS Medicinal Chemistry Letters, 15(4), 533-539. https://doi.org/10.1021/acsmedchemlett.4c00017

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title = "Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome",

abstract = "Peptide macrocycles have recently gained attention as protease inhibitors due to their metabolic stability and specificity. However, the development of peptide macrocycles with improved binding potency has so far been challenging. Here we present macrocyclic peptides derived from the clinically applied proteasome inhibitor carfilzomib with an oxindole group that mimics the natural product TMC-95A. Fluorescence kinetic activity assays reveal a high potency of the oxindole group (IC50 = 0.19 μM) compared with agents lacking this motif. X-ray structures of the ligands with the β5-subunit of the yeast 20S proteasome illustrate that the installed macrocycle forces strong hydrogen bonding of the oxindole group with β5-Gly23NH. Thus, the binding of our designed oxindole epoxyketones is entropically and enthalpically favored in contrast to more flexible proteasome inhibitors such as carfilzomib.",

keywords = "Carfilzomib, Epoxyketone, Inhibitor, Multiple myeloma, Peptide macrocycle, Proteasome",

author = "G{\"o}tz, {Marion G.} and Kacey Godwin and Rachel Price and Robert Dorn and Gabriel Merrill-Steskal and William Klemmer and Hunter Hansen and Gautam Produturi and Megan Rocha and Mathias Palmer and Lea Molacek and Zack Strater and Michael Groll",

note = "Publisher Copyright: {\textcopyright} 2024 The Authors. Published by American Chemical Society.",

year = "2024",

month = apr,

day = "11",

doi = "10.1021/acsmedchemlett.4c00017",

language = "English",

volume = "15",

pages = "533--539",

journal = "ACS Medicinal Chemistry Letters",

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Götz, MG, Godwin, K, Price, R, Dorn, R, Merrill-Steskal, G, Klemmer, W, Hansen, H, Produturi, G, Rocha, M, Palmer, M, Molacek, L, Strater, Z & Groll, M 2024, 'Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome', ACS Medicinal Chemistry Letters, Jg. 15, Nr. 4, S. 533-539. https://doi.org/10.1021/acsmedchemlett.4c00017

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T1 - Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome

AU - Götz, Marion G.

AU - Godwin, Kacey

AU - Price, Rachel

AU - Dorn, Robert

AU - Merrill-Steskal, Gabriel

AU - Klemmer, William

AU - Hansen, Hunter

AU - Produturi, Gautam

AU - Rocha, Megan

AU - Palmer, Mathias

AU - Molacek, Lea

AU - Strater, Zack

AU - Groll, Michael

PY - 2024/4/11

Y1 - 2024/4/11

N2 - Peptide macrocycles have recently gained attention as protease inhibitors due to their metabolic stability and specificity. However, the development of peptide macrocycles with improved binding potency has so far been challenging. Here we present macrocyclic peptides derived from the clinically applied proteasome inhibitor carfilzomib with an oxindole group that mimics the natural product TMC-95A. Fluorescence kinetic activity assays reveal a high potency of the oxindole group (IC50 = 0.19 μM) compared with agents lacking this motif. X-ray structures of the ligands with the β5-subunit of the yeast 20S proteasome illustrate that the installed macrocycle forces strong hydrogen bonding of the oxindole group with β5-Gly23NH. Thus, the binding of our designed oxindole epoxyketones is entropically and enthalpically favored in contrast to more flexible proteasome inhibitors such as carfilzomib.

AB - Peptide macrocycles have recently gained attention as protease inhibitors due to their metabolic stability and specificity. However, the development of peptide macrocycles with improved binding potency has so far been challenging. Here we present macrocyclic peptides derived from the clinically applied proteasome inhibitor carfilzomib with an oxindole group that mimics the natural product TMC-95A. Fluorescence kinetic activity assays reveal a high potency of the oxindole group (IC50 = 0.19 μM) compared with agents lacking this motif. X-ray structures of the ligands with the β5-subunit of the yeast 20S proteasome illustrate that the installed macrocycle forces strong hydrogen bonding of the oxindole group with β5-Gly23NH. Thus, the binding of our designed oxindole epoxyketones is entropically and enthalpically favored in contrast to more flexible proteasome inhibitors such as carfilzomib.

KW - Carfilzomib

KW - Epoxyketone

KW - Inhibitor

KW - Multiple myeloma

KW - Peptide macrocycle

KW - Proteasome

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U2 - 10.1021/acsmedchemlett.4c00017

DO - 10.1021/acsmedchemlett.4c00017

M3 - Article

AN - SCOPUS:85189028990

SN - 1948-5875

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JO - ACS Medicinal Chemistry Letters

JF - ACS Medicinal Chemistry Letters

IS - 4

ER -

Macrocyclic Oxindole Peptide Epoxyketones─A Comparative Study of Macrocyclic Inhibitors of the 20S Proteasome

Abstract

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