Allosteric therapies for lung cancer

Ye, Ling; Jing, Meiling; Wang, Xiangdong

doi:10.1007/s10555-015-9567-z

Cited by 9 publications

(3 citation statements)

References 81 publications

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“…There have been recent developments in compounds targeting the allosteric site in order to produce an alternative medicine that might solve the resistance issue to drugs used in current therapy [ 101 ]. Furthermore, the ligands binding to this site, which are also called allosteric modulators of EGFR, lead to conformational changes that may enhance the protein activity and orthosteric ligand binding, or vice versa [ 102 , 103 , 104 ]. They are divided into three types based on their properties, namely positive (PAM), neutral, and negative allosteric modulators (NAM) [ 103 , 105 ].…”

Section: Allosteric Sitementioning

confidence: 99%

Structural Insight and Development of EGFR Tyrosine Kinase Inhibitors

et al. 2022

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Lung cancer has a high prevalence, with a growing number of new cases and mortality every year. Furthermore, the survival rate of patients with non-small-cell lung carcinoma (NSCLC) is still quite low in the majority of cases. Despite the use of conventional therapy such as tyrosine kinase inhibitor for Epidermal Growth Factor Receptor (EGFR), which is highly expressed in most NSCLC cases, there was still no substantial improvement in patient survival. This is due to the drug’s ineffectiveness and high rate of resistance among individuals with mutant EGFR. Therefore, the development of new inhibitors is urgently needed. Understanding the EGFR structure, including its kinase domain and other parts of the protein, and its activation mechanism can accelerate the discovery of novel compounds targeting this protein. This study described the structure of the extracellular, transmembrane, and intracellular domains of EGFR. This was carried out along with identifying the binding pose of commercially available inhibitors in the ATP-binding and allosteric sites, thereby clarifying the research gaps that can be filled. The binding mechanism of inhibitors that have been used clinically was also explained, thereby aiding the structure-based development of new drugs.

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Section: Allosteric Sitementioning

confidence: 99%

Structural Insight and Development of EGFR Tyrosine Kinase Inhibitors

et al. 2022

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“…This region is not directly involved with the pharmacotherapeutic response. The binding of effector to the allosteric site on the protein leads to conformational changes at the active or binding site, which regulates protein activity [42]. Allosteric ligands/effectors or drugs are of two types (1) non-covalent and (2) covalent binding agents.…”

Section: Egfr-allosteric Site As a Potential Target And Its Advantagesmentioning

confidence: 99%

“…EAI001 has only one chain (A) of which 28% is composed of the helix, and 14% is the β-plated sheet, which comprises 355 amino acids ranging from residue 675 to 1022 [47]. EAI001 has one inhibitory residue, namely 9LLA 1101 [42]. The figure states the residue sequence of both the compound along with this interaction site with the protein in the allosteric site of EGFR.…”

Section: Secondary Structure Assessment Of Egfr Eai045 and Eai001mentioning

confidence: 99%

Advances in targeting EGFR allosteric site as anti-NSCLC therapy to overcome the drug resistance

2020

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Background The epidermal growth factor receptor (EGFR) inhibitors represent the first-line therapy regimen for non-small cell lung cancer (NSCLC). Most of these inhibitors target the ATP-site to stop the aggressive development of NSCLC. Stabilization of the ATP-binding on EGFR is difficult due to autophosphorylation of the EGFR domain. This leads to activation of nonintrinsic influence of the tumor microenvironment and expression of anti-apoptotic pathways and drug resistance. Methods The NSCLC related literature search was carried out using online databases such as Scopus, Web of Sciences, PubMed, Protein Data Bank and UniPort for the last ten years and selected articles are referred for discussion in this review. Results To overcome the problem of mutations in NSCLC, the allosteric site of EGFR was targeted, which shows significant therapeutic outcome without causing resistance. Compounds like EAI001, EAI045 JBJ-04-125-02, DDC4002 and a series of small molecules with an affinity towards the EGFR allosteric site are reported and are under the investigational stage. These compounds are categorized under fourth-generation anti-NSCLC agents. Conclusion Composition of this review highlights the advantage of inhibiting allosteric site in the EGFRTK receptor domains and presents a comparative analysis of the new fourth-generation anti-NSCLC agents to overcome the drug resistance.

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