Literature DB >> 32869838

Inhibition of RAS: proven and potential vulnerabilities.

Mariyam Zuberi1,2, Imran Khan1,2, John P O'Bryan1,2.   

Abstract

RAS is a membrane localized small GTPase frequently mutated in human cancer. As such, RAS has been a focal target for developing cancer therapeutics since its discovery nearly four decades ago. However, efforts to directly target RAS have been challenging due to the apparent lack of readily discernable deep pockets for binding small molecule inhibitors leading many to consider RAS as undruggable. An important milestone in direct RAS inhibition was achieved recently with the groundbreaking discovery of covalent inhibitors that target the mutant Cys residue in KRAS(G12C). Surprisingly, these G12C-reactive compounds only target mutant RAS in the GDP-bound state thereby locking it in the inactive conformation and blocking its ability to couple with downstream effector pathways. Building on this success, several groups have developed similar compounds that selectively target KRAS(G12C), with AMG510 and MRTX849 the first to advance to clinical trials. Both have shown early promising results. Though the success with these compounds has reignited the possibility of direct pharmacological inhibition of RAS, these covalent inhibitors are limited to treating KRAS(G12C) tumors which account for <15% of all RAS mutants in human tumors. Thus, there remains an unmet need to identify more broadly efficacious RAS inhibitors. Here, we will discuss the current state of RAS(G12C) inhibitors and the potential for inhibiting additional RAS mutants through targeting RAS dimerization which has emerged as an important step in the allosteric regulation of RAS function.
© 2020 The Author(s). Published by Portland Press Limited on behalf of the Biochemical Society.

Entities:  

Keywords:  RAS GTPase; allosteric inhibitor; cancer; chemotherapy; dimerization; monobody

Year:  2020        PMID: 32869838      PMCID: PMC7875515          DOI: 10.1042/BST20190023

Source DB:  PubMed          Journal:  Biochem Soc Trans        ISSN: 0300-5127            Impact factor:   5.407


  85 in total

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2.  Analysis of binding site hot spots on the surface of Ras GTPase.

Authors:  Greg Buhrman; Casey O'Connor; Brandon Zerbe; Bradley M Kearney; Raeanne Napoleon; Elizaveta A Kovrigina; Sandor Vajda; Dima Kozakov; Evgenii L Kovrigin; Carla Mattos
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3.  Defining and Targeting Adaptations to Oncogenic KRASG12C Inhibition Using Quantitative Temporal Proteomics.

Authors:  Naiara Santana-Codina; Amrita Singh Chandhoke; Qijia Yu; Beata Małachowska; Miljan Kuljanin; Ajami Gikandi; Marcin Stańczak; Sebastian Gableske; Mark P Jedrychowski; David A Scott; Andrew J Aguirre; Wojciech Fendler; Nathanael S Gray; Joseph D Mancias
Journal:  Cell Rep       Date:  2020-03-31       Impact factor: 9.423

4.  The reactivity-driven biochemical mechanism of covalent KRASG12C inhibitors.

Authors:  Rasmus Hansen; Ulf Peters; Anjali Babbar; Yuching Chen; Jun Feng; Matthew R Janes; Lian-Sheng Li; Pingda Ren; Yi Liu; Patrick P Zarrinkar
Journal:  Nat Struct Mol Biol       Date:  2018-05-14       Impact factor: 15.369

5.  Absence of the CAAX endoprotease Rce1: effects on cell growth and transformation.

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Journal:  Mol Cell Biol       Date:  2002-01       Impact factor: 4.272

6.  Identification of the Clinical Development Candidate MRTX849, a Covalent KRASG12C Inhibitor for the Treatment of Cancer.

Authors:  Jay B Fell; John P Fischer; Brian R Baer; James F Blake; Karyn Bouhana; David M Briere; Karin D Brown; Laurence E Burgess; Aaron C Burns; Michael R Burkard; Harrah Chiang; Mark J Chicarelli; Adam W Cook; John J Gaudino; Jill Hallin; Lauren Hanson; Dylan P Hartley; Erik J Hicken; Gary P Hingorani; Ronald J Hinklin; Macedonio J Mejia; Peter Olson; Jennifer N Otten; Susan P Rhodes; Martha E Rodriguez; Pavel Savechenkov; Darin J Smith; Niranjan Sudhakar; Francis X Sullivan; Tony P Tang; Guy P Vigers; Lance Wollenberg; James G Christensen; Matthew A Marx
Journal:  J Med Chem       Date:  2020-04-06       Impact factor: 7.446

7.  Targeting KRAS Mutant Cancers with a Covalent G12C-Specific Inhibitor.

Authors:  Matthew R Janes; Jingchuan Zhang; Lian-Sheng Li; Rasmus Hansen; Ulf Peters; Xin Guo; Yuching Chen; Anjali Babbar; Sarah J Firdaus; Levan Darjania; Jun Feng; Jeffrey H Chen; Shuangwei Li; Shisheng Li; Yun O Long; Carol Thach; Yuan Liu; Ata Zarieh; Tess Ely; Jeff M Kucharski; Linda V Kessler; Tao Wu; Ke Yu; Yi Wang; Yvonne Yao; Xiaohu Deng; Patrick P Zarrinkar; Dirk Brehmer; Dashyant Dhanak; Matthew V Lorenzi; Dana Hu-Lowe; Matthew P Patricelli; Pingda Ren; Yi Liu
Journal:  Cell       Date:  2018-01-25       Impact factor: 41.582

8.  Rapid non-uniform adaptation to conformation-specific KRAS(G12C) inhibition.

Authors:  Jenny Y Xue; Yulei Zhao; Jordan Aronowitz; Trang T Mai; Alberto Vides; Besnik Qeriqi; Dongsung Kim; Chuanchuan Li; Elisa de Stanchina; Linas Mazutis; Davide Risso; Piro Lito
Journal:  Nature       Date:  2020-01-08       Impact factor: 49.962

9.  Discovery of High-Affinity Noncovalent Allosteric KRAS Inhibitors That Disrupt Effector Binding.

Authors:  Michael J McCarthy; Cynthia V Pagba; Priyanka Prakash; Ali K Naji; Dharini van der Hoeven; Hong Liang; Amit K Gupta; Yong Zhou; Kwang-Jin Cho; John F Hancock; Alemayehu A Gorfe
Journal:  ACS Omega       Date:  2019-02-08
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Authors:  Kari Kopra; Salla Valtonen; Randa Mahran; Jonas N Kapp; Nazia Hassan; William Gillette; Bryce Dennis; Lianbo Li; Kenneth D Westover; Andreas Plückthun; Harri Härmä
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2.  Identification of the nucleotide-free state as a therapeutic vulnerability for inhibition of selected oncogenic RAS mutants.

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Review 3.  RAS Nanoclusters: Dynamic Signaling Platforms Amenable to Therapeutic Intervention.

Authors:  Que N Van; Priyanka Prakash; Rebika Shrestha; Trent E Balius; Thomas J Turbyville; Andrew G Stephen
Journal:  Biomolecules       Date:  2021-03-03

Review 4.  Targeting KRAS mutant lung cancer: light at the end of the tunnel.

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Journal:  Mol Oncol       Date:  2022-01-18       Impact factor: 6.603

Review 5.  Mechanism of activation and the rewired network: New drug design concepts.

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