Design and synthesis of novel phenylaminopyrimidines with antiproliferative activity against colorectal cancer

Henidi, Hanan A.; Al‐Abd, Ahmed M.; BinMahfouz, Hawazen A.; El‐Deeb, Ibrahim M.

doi:10.1039/c9ra03359a

Cited by 7 publications

(4 citation statements)

References 30 publications

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“…The results explained that compound 30 was highly selective towards the Src kinase enzyme with EC 50 of 1.3 μM. This derivative showed hydrogen bond interactions with Gln278, Lys298, and Thr341 amino acids and steric interaction with Met344 and Ile339 residue of Src kinase [38] …”

Section: Recent Development Of Src Kinase Inhibitorsmentioning

confidence: 90%

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Medicinal Chemistry Perspectives on Recent Advances in Src Kinase Inhibitors as a Potential Target for the Development of Anticancer Agents: Biological Profile, Selectivity, Structure‐Activity Relationship

Teli¹,

Pal²,

Maji³

et al. 2023

Chemistry & Biodiversity

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The physiological Src proto‐oncogene is a protein tyrosine kinase receptor that served as the essential signalling pathway in different types of cancer. The etiology of cancer involved various signalling pathways and Src signalling pathways are also involved in those clusters. Although the dysregulation of Src kinase resulted in cancer being discovered in the late 19th century it is still considered a cult pathway because it is not much explored by different medicinal chemists and oncologists. In this review, we have elaborated about the structure and activation of Src kinase, as well as the development of Src kinase inhibitors. Our group also provided a comprehensive overview of Src inhibitors throughout the last two decades, including their biological activity, structure‐activity relationship, and Src kinase selectivity. The Src binding pocket has been investigated in detail to better comprehend the interaction of Src inhibitors with amino acid residues. We have strengthened the literature with our contribution in terms of molecular docking and ADMET studies of top compounds. We hope that the current analysis will be a useful resource for researchers and provide glimpse of direction toward the design and development of more specific, selective, and potent Src kinase inhibitors.

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Section: Recent Development Of Src Kinase Inhibitorsmentioning

confidence: 90%

“…This derivative showed hydrogen bond interactions with Gln278, Lys298, and Thr341 amino acids and steric interaction with Met344 and Ile339 residue of Src kinase. [38] Schoene et al designed and synthesized 2H-Indazoles candidates. These candidates had been screened as inhibitors of Src, Tie2 and SGK1.…”

Section: Recent Development Of Src Kinase Inhibitorsmentioning

confidence: 99%

Medicinal Chemistry Perspectives on Recent Advances in Src Kinase Inhibitors as a Potential Target for the Development of Anticancer Agents: Biological Profile, Selectivity, Structure‐Activity Relationship

Teli¹,

Pal²,

Maji³

et al. 2023

Chemistry & Biodiversity

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“…Asciminib is a potent and selective allosteric ABL1 [20,21] inhibitor patented by Novartis Oncology [6,8] . Asciminib exhibited reduction in the side effects as compared to another TKI drug [10,23] basutinib. Various other approved CML drugs [11,12] have been discontinued after four years in use for cancer [7–9,19] treatment due to the problem of resistance which has arisen due to point mutations in BCR‐ABL [2,4,8,15,21] .…”

Section: Introductionmentioning

confidence: 99%

Synthesis, Biological Evaluation, Molecular Docking and ADME Profiling of Methylpiperidin‐4‐ylphenyl‐nicotinamide Derivatives

Mohan Mulik,

Srivastava,

Pendharkar

2024

ChemistrySelect

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In this paper, we designed, synthesized, and biologically screened a series of methyl‐piperidine‐phenyl‐nicotinamide derivatives with the aim of novel derivatives as effective anticancer agents. Compounds (9 a), (9 e) and (9 k) exhibited potent anticancer activity with an IC50 value of 5.9 μM, 5.9 μM and 5.0 μM, respectively using MV411 (Acute Myeloid Leukemia) and K562 (Chronic Myeloid Leukemia) cell line. Our docking studies show good binding affinity of these compounds for ABL1 kinase. Furthermore, these compounds exhibited a favourable in silico ADME profile with good solubility and low clearance in Human Liver Microsomes (HLM). These derivatives represent a promising approach to initiate the development of new anticancer drugs in oncology programs.

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“…[13][14][15] Phenyl amino pyrimidine and hydroxysubstituted phenyl amino pyrimidine showed a selective src kinase inhibitory response and excellent anticancer response against the HT29CRC and HCT-116 cell lines. 16 Mohammed et al reported on in vitro anti-proliferative studies of trimethoxy phenyl-substituted pyridine against the MCF7, HEPG-2 and HCT116 cancer cell lines. 4-Nitro-substituted trimethoxy phenyl pyridine showed a signicant anticancer response against the HCT116, HEPG-2 and MCF7 cancer cell lines compared with hydroxy-, methoxy-, methyl-substituted and chloro trimethoxy phenyl pyridine.…”

Section: Introductionmentioning

confidence: 99%

2-Chloro-3-cyano-4-nitrobenzyl pyridinium bromide as a potent anti-lung cancer molecule prepared using a single-step solvent-free method

Govindaraj,

Ganesan,

Elumalai

et al. 2024

RSC Adv.

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Design and synthesis of novel phenylaminopyrimidines with antiproliferative activity against colorectal cancer

Abstract: A new series of phenylaminopyrimidine (PAP) derivatives was designed and synthesized to act against tyrosine kinases for the treatment of cancer.

Cited by 7 publications

References 30 publications

Medicinal Chemistry Perspectives on Recent Advances in Src Kinase Inhibitors as a Potential Target for the Development of Anticancer Agents: Biological Profile, Selectivity, Structure‐Activity Relationship

Medicinal Chemistry Perspectives on Recent Advances in Src Kinase Inhibitors as a Potential Target for the Development of Anticancer Agents: Biological Profile, Selectivity, Structure‐Activity Relationship

Synthesis, Biological Evaluation, Molecular Docking and ADME Profiling of Methylpiperidin‐4‐ylphenyl‐nicotinamide Derivatives

2-Chloro-3-cyano-4-nitrobenzyl pyridinium bromide as a potent anti-lung cancer molecule prepared using a single-step solvent-free method

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