Boronic acid-containing CXCR1/2 antagonists: Optimization of metabolic stability, in vivo evaluation, and a proposed receptor binding model

Maeda Dean Y.; Peck Angela M.; Schuler Aaron D.; Quinn Mark T.; Kirpotina Liliya N.; Wicomb Winston N.; Auten Richard L.; Gundla Rambabu; Zebala John A.

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Boronic acid-containing CXCR1/2 antagonists: Optimization of metabolic stability, in vivo evaluation, and a proposed receptor binding model

机译：含硼酸的CXCR1 / 2拮抗剂：优化代谢稳定性，体内评估和拟议的受体结合模型

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Blockade of undesired neutrophil migration to sites of inflammation remains an area of substantial pharmaceutical interest. To effect this blockade, a validated therapeutic target is antagonism of the chemokine receptor CXCR2. Herein we report the discovery of 6-(2-boronic acid-5-trifluoromethoxy-benzylsulfanyl)-N-(4-fluoro-phenyl)-nicotinamide 6, an antagonist with activity at both CXCR1 and CXCR2 receptors (IC50 values 31 and 21 nM, respectively). Compound 6 exhibited potent inhibition of neutrophil influx in a rat model of pulmonary inflammation, and is hypothesized to interact with a unique intracellular binding site on CXCR2. Compound 6 (SX-576) is undergoing further investigation as a potential therapy for pulmonary inflammation. (C) 2015 Elsevier Ltd. All rights reserved.

机译：阻止不希望的嗜中性白细胞迁移到炎症部位仍然是重要的药物领域。为了实现这一封锁，有效的治疗靶点是趋化因子受体CXCR2的拮抗作用。在这里，我们报告了6-（2-硼酸-5-三氟甲氧基-苄硫基）-N-（4-氟-苯基）-烟酰胺6的发现，该拮抗剂对CXCR1和CXCR2受体均具有活性（IC50值为31和21）分别为nM）。化合物6在大鼠肺部炎症模型中显示出对中性粒细胞流入的有效抑制，并被认为与CXCR2上唯一的细胞内结合位点相互作用。化合物6（SX-576）作为肺部炎症的潜在疗法正在接受进一步研究。（C）2015 Elsevier Ltd.保留所有权利。

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《Bioorganic and Medicinal Chemistry Letters》 |2015年第11期|共5页
作者
Maeda Dean Y.; Peck Angela M.; Schuler Aaron D.; Quinn Mark T.; Kirpotina Liliya N.; Wicomb Winston N.; Auten Richard L.; Gundla Rambabu; Zebala John A.;
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正文语种 eng
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CXCR2; Antagonist; Thionicotinamide; COPD; Asthma;

机译：CXCR2拮抗剂硫代亚酰胺COPD哮喘;

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1. Boronic acid-containing CXCR1/2 antagonists: Optimization of metabolic stability, in vivo evaluation, and a proposed receptor binding model [J] . Maeda Dean Y., Peck Angela M., Schuler Aaron D., Bioorganic and Medicinal Chemistry Letters . 2015,第11期

机译：含硼酸的CXCR1 / 2拮抗剂：优化代谢稳定性，体内评估和拟议的受体结合模型
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3. Conformational and Drug-Receptor Binding Optimization Studies of Ergocalciferol (Vitamin D₂) as a Potential Metabolic Antagonist [J] . Abrar Ul Hassan, Ayesha Mohyuddin Vitamins & Minerals . 2017,第1期

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5. Sigma-1 Receptor Antagonist (BD1047) prior to Cocaine Reduces Cathepsin B Secretion in HIV-1 Models In Vivo and In Vitro [D] . Vélez-López, Omar. 2019

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6. Boronic acid-containing CXCR1/2 antagonists: optimization of metabolic stability in vivo evaluation and a proposed receptor binding model [O] . Dean Y. Maeda, Angela M. Peck, Aaron D. Schuler, -1

机译：含硼酸的CXCR1 / 2拮抗剂：优化代谢稳定性体内评估和拟议的受体结合模型
7. Boronic acid-containing CXCR1/2 antagonists: Optimization of metabolic stability, in vivo evaluation, and a proposed receptor binding model [O] . Dean Y. Maeda, Angela M. Peck, Aaron D. Schuler, 2015

机译：含硼酸的CXCR1 / 2拮抗剂：优化代谢稳定性，体内评价和提出的受体结合模型

Boronic acid-containing CXCR1/2 antagonists: Optimization of metabolic stability, in vivo evaluation, and a proposed receptor binding model

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