Hit-to-lead optimization of a pyrazinylpiperazine series against Leishmania infantum and Leishmania braziliensis

被引：4

作者：

Lapierre, Thibault Joseph William Jacques Dit ^{[1
]}

Cruz, Mariza Gabriela Faleiro de Moura Lodi ^{[2
]}

Brito, Nicolas Peterson Ferreira ^{[1
]}

Resende, Daniela de Melo ^{[2
]}

Souza, Felipe de Oliveira ^{[3
]}

Pilau, Eduardo Jorge ^{[3
]}

da Silva, Meryck Felipe Brito ^{[4
]}

Neves, Bruno Junior ^{[4
]}

Murta, Silvane Maria Fonseca ^{[2
]}

Rezende Junior, Celso de Oliveira ^{[1
]}

机构：

[1] Univ Fed Uberlandia UFU, Lab Sintese Candidatos & Farmacos, Inst Quim, BR-38400902 Uberlandia, MG, Brazil

[2] Fundacao Oswaldo Cruz FIOCRUZ Minas, Grp Genom Func Parasitos, Inst Rene Rachou, BR-30190002 Belo Horizonte, MG, Brazil

[3] Univ Estadual Maringa UEM, Lab Biomol & Espectromet Massas LaBioMass, BR-807020900 Maringa, PR, Brazil

[4] Univ Fed Goias, Fac Farm, Lab Cheminformat LabChem, BR-74605170 Goiania, GO, Brazil

来源：

EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY | 2023年 / 256卷

关键词：

Leishmania; Hit-to-lead optimization; Neglected tropical disease; Pyrazinylpiperazines; ADMET; DRUG DISCOVERY; SCREENING LIBRARIES; DECISION-MAKING; LIPOPHILICITY;

D O I：

10.1016/j.ejmech.2023.115445

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

An early hit-to-lead optimization of a novel pyrazinylpiperazine series against L. infantum and L. braziliensis has been performed after an extensive SAR focusing on the benzoyl fragment of hit (4). Deletion of the meta-Cl of (4) led to the obtention of the para-hydroxyl derivative (12), on which the design of most monosubstituted de-rivatives of the SAR was based. Further optimization of the series, involving disubstituted benzoyl fragments and the hydroxyl substituent of (12), allowed the obtention of a total of 15 compounds with increased anti-leishmanial potency (IC50 < 10 mu M), nine of which displayed activity in the low micromolar range (IC50 < 5 mu M). This optimization ultimately identified the ortho, meta-dihydroxyl derivative (46) as an early lead for this series (IC50 (L. infantum) = 2.8 mu M, IC50 (L. braziliensis) = 0.2 mu M). Additional assessment of some selected compounds against other trypanosomatid parasites revealed that this series is selective towards Leishmania parasites, and in silico ADMET predictions revealed satisfactory profiles for these compounds, allowing further lead optimization of the pyrazinylpiperazine class against Leishmania.

引用

页数：21

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