Lead Optimization of Benzoxazolone Carboxamides as Orally Bioavailable and CNS Penetrant Acid Ceramidase Inhibitors

Di Martino Simona; Tardia Piero; Cilibrasi Vincenzo; Caputo Samantha; Mazzonna Marco; Russo Debora; Penna Ilaria; Realini Natalia; Margaroli Natasha; Migliore Marco; Pizzirani Daniela; Ottonello Giuliana; Bertozzi Sine Mandrup; Armirotti Andrea; Duc Nguyen; Sun Ying; Bongarzone Ernesto R.; Lansbury Peter; Liu Min; Skerlj Renato; Scarpelli Rita

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Lead Optimization of Benzoxazolone Carboxamides as Orally Bioavailable and CNS Penetrant Acid Ceramidase Inhibitors

机译：Benzoxazolone羧胺的铅优化是口服生物可利用和CNS渗透酸陶瓷酶抑制剂

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Sphingolipids (SphLs) are a diverse class of molecules that are regulated by a complex network of enzymatic pathways. A disturbance in these pathways leads to lipid accumulation and initiation of several SphL-related disorders. Acid ceramidase is one of the key enzymes that regulate the metabolism of ceramides and glycosphingolipids, which are important members of the SphL family. Herein, we describe the lead optimization studies of benzoxazolone carboxamides resulting in piperidine 22m, where we demonstrated target engagement in two animal models of neuropathic lysosomal storage diseases (LSDs), Gaucher's and Krabbe's diseases. After daily intraperitoneal administration at 90 mg kg(-1), 22m significantly reduced the brain levels of the toxic lipids glucosylsphingosine (GluSph) in 4L;C* mice and galactosylsphingosine (GalSph) in Twitcher mice. We believe that 22m is a lead molecule that can be further developed for the correction of severe neurological LSDs where GluSph or GalSph play a significant role in disease pathogenesis.

机译：鞘磷脂（SPHL）是由复杂的酶途径网络调节的各种分子。这些途径中的扰动导致脂质积累和起始几种与SPHL相关的疾病。酸陶瓷酶是调节神经酰胺和糖磷脂的代谢的关键酶之一，这是SPHL家族的重要成员。在此，我们描述了苯并恶唑酮羧酰胺导致哌啶22M的铅优化研究，在其中我们证明了两种动物模型的神经病溶酶体储存疾病（LSD），Gaucher和Krabbe疾病的目标接合。在每日腹膜内给药以90mg kg（-1）时，22米显着降低了毒性脂质葡萄糖囊氨酸（Glusph）的胃部血糖素（glusph）的脑水平; C *小鼠和旋流孔小鼠的半乳糖基氏糖苷（甘氨酸）。我们认为22M是一种铅分子，可以进一步开发用于校正严重的神经系统LSD，其中Glusph或Galsph在疾病发病机制中发挥着重要作用。

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《Journal of Medicinal Chemistry》 |2020年第7期|共31页
作者
Di Martino Simona; Tardia Piero; Cilibrasi Vincenzo; Caputo Samantha; Mazzonna Marco; Russo Debora; Penna Ilaria; Realini Natalia; Margaroli Natasha; Migliore Marco; Pizzirani Daniela; Ottonello Giuliana; Bertozzi Sine Mandrup; Armirotti Andrea; Duc Nguyen; Sun Ying; Bongarzone Ernesto R.; Lansbury Peter; Liu Min; Skerlj Renato; Scarpelli Rita;
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作者单位

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol D3 Pharma Chem I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol D3 Pharma Chem I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Analyt Chem Lab I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Analyt Chem Lab I-16163 Genoa Italy;

Fdn Ist Italiano Tecnol Analyt Chem Lab I-16163 Genoa Italy;

Univ Illinois Coll Med Dept Anat &

Cell Biol Myelin Regenerat Grp Chicago IL 60612 USA;

Univ Cincinnati Coll Med Cincinnati Childrens Hosp Med Ctr Dept Pediat Div Human Genet Cincinnati OH 45229 USA;

Univ Illinois Coll Med Dept Anat &

Cell Biol Myelin Regenerat Grp Chicago IL 60612 USA;

Lysosomal Therapeut Inc Cambridge MA 02139 USA;

Lysosomal Therapeut Inc Cambridge MA 02139 USA;

Lysosomal Therapeut Inc Cambridge MA 02139 USA;

Fdn Ist Italiano Tecnol Drug Discovery &

Dev D3 Validat I-16163 Genoa Italy;

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1. Lead Optimization of Benzoxazolone Carboxamides as Orally Bioavailable and CNS Penetrant Acid Ceramidase Inhibitors [J] . Di Martino Simona, Tardia Piero, Cilibrasi Vincenzo, Journal of Medicinal Chemistry . 2020,第7期

机译：Benzoxazolone羧胺的铅优化是口服生物可利用和CNS渗透酸陶瓷酶抑制剂
2. Benzoxazolone Carboxamides: Potent and Systemically Active Inhibitors of Intracellular Acid Ceramidase [J] . Pizzirani Daniela, Bach Anders, Realini Natalia, Angewandte Chemie . 2015,第2期

机译：苯并恶唑酮羧酰胺：细胞内酸性神经酰胺酶的强效和全身活性抑制剂
3. Development of Orally Bioavailable and CNS Penetrant Biphenylaminocyclopropane Carboxamide Bradykinin B_1 Receptor Antagonists [J] . Scott D.Kuduk, Christina N.Di Marco, Ronald K.Chang Journal of Medicinal Chemistry . 2007,第2期

机译：口服生物利用性和中枢神经系统渗透性联苯氨基环丙烷羧酰胺缓激肽B_1受体拮抗剂的开发
4. CNX-774, an Irreversible, Selective and Orally Bioavailable Inhibitor of Bruton's Tyrosine Kinase: In Vitro ADME, Selectivity, and Pharmacokinetic Properties [C] . Prasoon Chaturvedi, Matthew Labenski, Erica Evans, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2011

机译：CNX-774，Bruton的酪氨酸激酶的不可逆转，选择性和口服生物可利用的抑制剂：体外Adme，选择性和药代动力学性能
5. Combination of FasL gene therapy and acid ceramidase inhibitors: A novel therapeutic approach for the treatment of head and neck cancer. [D] . Elojeimy, Saeed. 2009

机译：FasL基因疗法和酸性神经酰胺酶抑制剂的组合：一种治疗头颈癌的新型治疗方法。
6. Benzoxazolone Carboxamides: Potent and Systemically Active Inhibitors of Intracellular Acid Ceramidase [O] . Daniela Pizzirani, Anders Bach, Natalia Realini, -1

机译：苯并恶唑酮羧酰胺：细胞内酸性神经酰胺酶的强效和全身活性抑制剂
7. Benzoxazolone Carboxamides as Potent Acid Ceramidase Inhibitors: Synthesis and Structure–Activity Relationship (SAR) Studies [O] . Anders Bach, Daniela Pizzirani, Natalia Realini, 2015

机译：Benzoxazolone羧酰胺作为有效的酸陶瓷酶抑制剂：合成和结构 - 活性关系（SAR）研究

Lead Optimization of Benzoxazolone Carboxamides as Orally Bioavailable and CNS Penetrant Acid Ceramidase Inhibitors

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