Structure-activity relationship and biochemical evaluation of novel fibroblast activation protein and prolyl endopeptidase inhibitors with α-ketoamide warheads

Šimková, Adéla; Ormsby, Tereza; Sidej, Natan; Poštová Slavětínská, Lenka; Brynda, Jiří; Beranová, Jana; Šácha, Pavel; Majer, Pavel; Konvalinka, Jan

doi:https://dx.doi.org/10.1016/j.ejmech.2021.113717

Počet záznamů: 1

Structure-activity relationship and biochemical evaluation of novel fibroblast activation protein and prolyl endopeptidase inhibitors with α-ketoamide warheads

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SYSNO ASEP	0544791
Druh ASEP	J - Článek v odborném periodiku
Zařazení RIV	J - Článek v odborném periodiku
Poddruh J	Článek ve WOS
Název	Structure-activity relationship and biochemical evaluation of novel fibroblast activation protein and prolyl endopeptidase inhibitors with α-ketoamide warheads
Tvůrce(i)	Šimková, Adéla (UOCHB-X)_{ORCID, RID} Ormsby, Tereza (UOCHB-X)_{ORCID, RID} Sidej, Natan (UOCHB-X)_ORCID Poštová Slavětínská, Lenka (UOCHB-X)_RID Brynda, Jiří (UOCHB-X)_{RID, ORCID} Beranová, Jana (UOCHB-X)_ORCID Šácha, Pavel (UOCHB-X)_{RID, ORCID} Majer, Pavel (UOCHB-X) Konvalinka, Jan (UOCHB-X)_{RID, ORCID}
Číslo článku	113717
Zdroj.dok.	European Journal of Medicinal Chemistry. - : Elsevier - ISSN 0223-5234 Roč. 224, Nov 15 (2021)
Poč.str.	9 s.
Jazyk dok.	eng - angličtina
Země vyd.	FR - Francie
Klíč. slova	fibroblast activation protein ; seprase ; FAP inhibitor ; serine protease inhibition ; prolyl endopeptidase ; α-Ketoamide inhibitor
Obor OECD	Medicinal chemistry
CEP	GA19-10280S GA ČR - Grantová agentura ČR
	NV15-31379A GA MZd - Ministerstvo zdravotnictví
	EF16_019/0000729 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
	LM2015064 GA MŠMT - Ministerstvo školství, mládeže a tělovýchovy
Způsob publikování	Open access
Institucionální podpora	UOCHB-X - RVO:61388963
UT WOS	000703110000046
EID SCOPUS	85111985613
DOI	10.1016/j.ejmech.2021.113717
Anotace	Peptidomimetic inhibitors of fibroblast activation protein (FAP) are regarded as promising tools for tumor targeting in vivo. Even though several peptidomimetic compounds with nanomolar potency have been described, broad chemical space for further modification remained unexplored. Therefore, we set to analyze the structure-activity relationship (SAR) of pseudopeptide compound series with α-ketoamide warheads in order to explore the contributions of the P1′ and P2′ moieties to the inhibitory potency. A series of novel inhibitors bearing varied P1′ and/or P2’ moieties was synthesized by combining a Passerini reaction-Amine Deprotection-Acyl Migration (PADAM) approach with peptide coupling and subsequent oxidation. The resulting compounds inhibited FAP and the related prolyl endopeptidase (PREP) with potencies in the nanomolar to sub-nanomolar range. The most potent FAP inhibitor IOCB22-AP446 (6d, IC50 = 89 pM) had about 36-fold higher inhibition potency than the most potent inhibitor published to date. The compounds were selective over FAP's closest homolog DPP-IV, were stable in human and mouse plasma and in mouse microsomes, and displayed minimal cytotoxicity in tissue cultures.
Pracoviště	Ústav organické chemie a biochemie
Kontakt	asep@uochb.cas.cz ; Kateřina Šperková, Tel.: 232 002 584 ; Jana Procházková, Tel.: 220 183 418
Rok sběru	2022
Elektronická adresa	https://doi.org/10.1016/j.ejmech.2021.113717

Počet záznamů: 1