Fragment-Based Discovery of a Potent, Orally Bioavailable Inhibitor That Modulates the Phosphorylation and Catalytic Activity of ERK1/2

Heightman Tom D.; Berdini Valerio; Braithwaite Hannah; Buck Ildiko M.; Cassidy Megan; Castro Juan; Courtin Aurelie; Day James E. H.; East Charlotte; Fazal Lynsey; Graham Brent; Griffiths-Jones Charlotte M.; Lyons John F.; Martins Vanessa; Muench Sandra; Munck Joanne M.; Norton David; OReilly Marc; Palmer Nick; Pathuri Puja; Reader Michael; Rees David C.; Rich Sharna J.; Richardson Caroline; Saini Harpreet; Thompson Neil T.; Wallis Nicola G.; Walton Hugh; Wilsher Nicola E.; Woolford Alison J. -A.; Cooke Michael; Cousin David; Onions Stuart; Shannon Jonathan; Watts John; Murray Christopher W.

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Fragment-Based Discovery of a Potent, Orally Bioavailable Inhibitor That Modulates the Phosphorylation and Catalytic Activity of ERK1/2

机译：基于片段的有效，口服生物可利用抑制剂的发现，可调节ERK1 / 2的磷酸化和催化活性

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Aberrant activation of the MAPK pathway drives cell proliferation in multiple cancers. Inhibitors of BRAF and MEK kinases are approved for the treatment of BRAF mutant melanoma, but resistance frequently emerges, often mediated by increased signaling through ERK1/2. Here, we describe the fragment-based generation of ERK1/2 inhibitors that block catalytic phosphorylation of downstream substrates such as RSK but also modulate phosphorylation of ERK1/2 by MEK without directly inhibiting MEK. X-ray crystallographic and biophysical fragment screening followed by structure-guided optimization and growth from the hinge into a pocket proximal to the C-alpha helix afforded highly potent ERK1/2 inhibitors with excellent kinome selectivity. In BRAF mutant cells, the lead compound suppresses pRSK and pERK levels and inhibits proliferation at low nanomolar concentrations. The lead exhibits tumor regression upon oral dosing in BRAF mutant xenograft models, providing a promising basis for further optimization toward clinical pERK1/2 modulating ERK1/2 inhibitors.

机译：MAPK途径的异常激活驱动多种癌症中细胞增殖。 BRAF和MEK激酶的抑制剂被批准用于治疗BRAF突变体黑素瘤，但抗性经常出现，通常通过ERK1 / 2增加信号传导。在这里，我们描述了基于片段的生成阻断下游底物如RSK也没有直接抑制MEK ERK1 / 2的MEK的磷酸化调制的催化磷酸化ERK1 / 2抑制剂。 X射线结晶和生物物理片段筛选，然后通过将铰链的结构引导优化和生长成近端的袋，得到了高效的ERK1 / 2抑制剂，具有优异的Kinome选择性。在BRAF突变细胞中，铅化合物抑制PRSK和PERK水平并抑制低纳米摩尔浓度的增殖。在BRAF突变体异种移植模型中，铅在口服给药时表现出肿瘤回归，为进一步优化临床PERK1 / 2调节ERK1 / 2抑制剂提供了有望的基础。

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《Journal of Medicinal Chemistry》 |2018年第11期|共15页
作者
Heightman Tom D.; Berdini Valerio; Braithwaite Hannah; Buck Ildiko M.; Cassidy Megan; Castro Juan; Courtin Aurelie; Day James E. H.; East Charlotte; Fazal Lynsey; Graham Brent; Griffiths-Jones Charlotte M.; Lyons John F.; Martins Vanessa; Muench Sandra; Munck Joanne M.; Norton David; OReilly Marc; Palmer Nick; Pathuri Puja; Reader Michael; Rees David C.; Rich Sharna J.; Richardson Caroline; Saini Harpreet; Thompson Neil T.; Wallis Nicola G.; Walton Hugh; Wilsher Nicola E.; Woolford Alison J. -A.; Cooke Michael; Cousin David; Onions Stuart; Shannon Jonathan; Watts John; Murray Christopher W.;
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Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

Sygnature Discovery Ltd BioCity Pennyfoot St Nottingham NG1 1GF England;

Sygnature Discovery Ltd BioCity Pennyfoot St Nottingham NG1 1GF England;

Sygnature Discovery Ltd BioCity Pennyfoot St Nottingham NG1 1GF England;

Sygnature Discovery Ltd BioCity Pennyfoot St Nottingham NG1 1GF England;

Sygnature Discovery Ltd BioCity Pennyfoot St Nottingham NG1 1GF England;

Astex Pharmaceut 436 Cambridge Sci Pk Cambridge CB4 0QA England;

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1. Fragment-Based Discovery of a Potent, Orally Bioavailable Inhibitor That Modulates the Phosphorylation and Catalytic Activity of ERK1/2 [J] . Heightman Tom D., Berdini Valerio, Braithwaite Hannah, Journal of Medicinal Chemistry . 2018,第11期

机译：基于片段的有效，口服生物可利用抑制剂的发现，可调节ERK1 / 2的磷酸化和催化活性
2. Discovery of Potent, Selective, and Orally Bioavailable Inhibitors of USP7 with In Vivo Antitumor Activity [J] . Leger Paul R., Hu Dennis X., Biannic Berenger, Journal of Medicinal Chemistry . 2020,第10期

机译：在体内抗肿瘤活动中发现USP7的有效，选择性和口服生物可利用的抑制剂
3. Discovery of Orally Bioavailable, Quinoline-Based Aldehyde Dehydrogenase 1A1 (ALDH1A1) Inhibitors with Potent Cellular Activity [J] . Yang Shyh-Ming, Martinez Natalia J., Yasgar Adam, Journal of Medicinal Chemistry . 2018,第11期

机译：发现口服生物的喹啉基醛脱氢酶1A1（ALDH1A1）抑制剂，具有有效的细胞活性
4. Discovery of Novel α-Amylase Inhibitors as Type Two Diabetes Mellitus Therapy through Fragment-Based Drug Design [C] . Muhammad Fauzi Hidayat, Eka Gunarti Ningsih, Ahmad Husein Alkaff International Conference on Science and Technology . 2020

机译：通过碎片的药物设计发现新型α-淀粉酶抑制剂作为两种糖尿病疗法
5. Development of Orally Bioavailable 4(1H)-Quinolones and 1,2,3,4-Tetrahydroacridin-9(10H)-ones with Potent Anti-malarial Activity [D] . Maignan, Jordany R. 2015

机译：具有有效抗疟疾活性的口服生物可利用的4（1H）-喹诺酮和1,2,3,4-Tetrahydroacridin-9（10H）-ones的开发
6. Discovery of INCB9471 a Potent Selective and Orally Bioavailable CCR5 Antagonist with Potent Anti-HIV-1 Activity [O] . Chu-Biao Xue, *, Lihua Chen, 2010

机译：发现具有有效抗HIV-1活性的有效选择性和口服生物利用CCR5拮抗剂INCB9471
7. Discovery of Aminoquinazolines as Potent, Orally Bioavailable Inhibitors of Lymphocyte-Specific Kinase: Synthesis, Structure-Activity Relationship, and in Vivo Anti-Inflammatory Activity [O] . -1

机译：发现氨基喹唑啉，作为淋巴细胞特异性激酶的有效性，口服生物可利用的抑制剂：合成，结构 - 活性关系，体内抗炎活性

Fragment-Based Discovery of a Potent, Orally Bioavailable Inhibitor That Modulates the Phosphorylation and Catalytic Activity of ERK1/2

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