Design, Synthesis, In Silico Studies and In Vitro Anticancer Activity of 3‐(4‐Methoxyphenyl)azetidine Derivatives

Parmar, Deepa R.; Rayani, Rahul H.; Vala, Anand; Kusurkar, Rakesh V.; Manvar, Roshani K.; Talukdar, Sahista N.; Preeti, .; Zunjar, Vishwanath; Battula, Satyanarayana; Soni, Jigar Y.

doi:10.1002/slct.202003654

Cited by 6 publications

(6 citation statements)

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“…cell lines were seeded in 96 well plate and incubated for 24 h to achieve its morphology as showed in Figure 1. Post CCK 8 assay [43] it was observed that the ethyl 2‐(2‐(4‐((2‐ethoxyphenyl)carbamoyl)piperazin‐1‐yl)acetamido)‐5‐methyl‐4‐phenylthiophene‐3‐carboxylate (AP‐C12) extract showed highest inhibition in U87‐MG cell line. The inhibition was compared with the positive control Temozolomide.…”

Section: Resultsmentioning

confidence: 99%

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Synthesis, Characterization, Molecular Docking and in vitro Anticancer Screening of Some Novel Thiophene Derivatives

Patel

et al. 2023

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One of the diseases in the 21 st century is still cancer and there is significant research being done all over the world to find a medicine that is more effective and has fewer adverse effects. More than 19 million new cases of cancer have been reported by global statistics and an estimated 10 million people have died from it in 2020. We continue to work on the development of new pharmacological entities because we are motivated in the research area. We have created novel thiophene derivatives and have screened them against the U87-MG cell line to see whether they have any anticancer properties. It was observed that the AP-C12 extract showed the highest inhibition in the U87-MG cell line (EC 50 : 9.1 μM) which was a very good comparison to Temozolomide (EC 50 : 61.2 μM). Similarly, AP-C7 exhibited considerable potency against the U87-MG cell line with EC 50 values of 12.3 μM.

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Section: Resultsmentioning

confidence: 99%

“…cell lines were seeded in 96 well plate and incubated for 24 h to achieve its morphology as showed in Figure 1. Post CCK 8 assay [43]…”

Section: In Vitro Cytotoxicity Studiesmentioning

confidence: 99%

Synthesis, Characterization, Molecular Docking and in vitro Anticancer Screening of Some Novel Thiophene Derivatives

Patel

et al. 2023

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“…Thus, their design and synthesis serve as a key part of synthetic chemical research. [ 33 ] In among varieties of heterocycles, azetidines constitute a vital and very significant place but the least explored group. The azetidine skeletons displayed a good balance between molecular rigidity and stability.…”

Section: Introductionmentioning

confidence: 99%

“…[ 33,34 ] This ring permits an effectual modification of pharmacological properties [ 35 ] and that's why azetidine serves as a core part of many existing drugs such as azelnidipine, tebanicline, delafloxacin, baricitinib, cobimetinib, and tebipenem. [ 33 ] In the earlier research, [ 36 ] it was illustrated that azetidine moiety as a linker with phenyl ring act as a pharmacophore. Thiazole‐containing skeletons are one of the most revered skeletons and key pharmacophores with many applications and pharmacological activities attributed to them such as antimicrobials, [ 37 ] antioxidant, [ 38 ] anticandida and cytotoxicity, [ 39 ] and anti‐inflammatory.…”

Section: Introductionmentioning

confidence: 99%

“…The azetidine skeletons displayed a good balance between molecular rigidity and stability. [33,34] This ring permits an effectual modification of pharmacological properties [35] and that's why azetidine serves as a core part of many existing drugs such as azelnidipine, tebanicline, delafloxacin, baricitinib, cobimetinib, and tebipenem. [33] In the earlier research, [36] it was illustrated that azetidine moiety as a linker with phenyl ring act as a pharmacophore.…”

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Design, synthesis, and in silico study of hybrid oxoazetidine conjugated thiazoles as anti‐EGFR with cytotoxicity activity

Pathak

Gupta

Grishina

et al. 2022

J Biochem & Molecular Tox

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We report a series of hybrid oxoazetidine conjugated thiazoles as epidermal growth factor receptor (EGFR) inhibitors, which were synthesized and tested using a variety of in silico and in vitro studies. The compounds were found to be active against breast and hepatic cancer cell lines, with Compounds 7a, 7b, and 7e being the most potent ones. The derivatives were also evaluated for molecular docking and complementarity studies to explicate fundamental substituent groups essential for their bioactivity. Moreover, the structural activity relationship of the analogues was performed for future compound optimization. These studies advocated that the analogues have a high affinity towards EGFR with favorable anticancer potential.The study advised that the derivatives have potency against breast and hepatic cancer and can assist as an initial scaffold for further development of anti-EGFR compounds.antitumor activity, hybrid oxoazetidine conjugated thiazoles, rational drug design | INTRODUCTIONCancer, a malignant disease, is the leading cause of death worldwide, and due to this millions of people lose their lives each year. [1] World Health Organization (WHO) propounded that the spread of cancers is higher in low-and middle-economic countries. [2,3] WHO official webpage [4] stated that cancer was accountable for 10 million deaths in 2020. It is also noted that patients with cancer have been impacted considerably due to increased morbidity and mortality from COVID-19 infection and delays in cancer therapy. [5] Much literature illustrates that numerous enzymes are intricate in signal recognition, transduction, and amplification followed by cell growth and division but among them, tyrosine kinases (TKs) are contemplated as one of the most important ones. [6,7] TKs generally participate in cell proliferation, metabolism, and apoptosis. Therefore, disturbance in TKs function leads to tumor growth and progression. [8] Functionally, TKs can be classified either as epidermal growth factor receptor (EGFR) or nonreceptor kinases. [9] EGFR belongs to the erbB/HERfamily of TKs, which is a transmembrane protein. These receptors comprise an extracellular ligand-binding domain, cysteine-binding domain, intracellular domain, and alpha-helix transmembrane domain with TK activity within the carboxy terminus (except for HER3). [10] EGFRs contribute to the regulatory molecular transcription through cell proliferation, differentiation, apoptosis, invasion, and angiogenesis followed by organ development. In tumor cells, EGFR signaling is changed, frequently develops dysregulated, and overexpresses and/ or obtains a gain-of-function mutation. [11][12][13][14][15][16] This performance facilitates the proliferation of tumor cells and invasion of the

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Discovery of Anti‐Breast Cancer Thiophene Sulfonamide Derivatives: Design, Synthesis, Molecular Docking against EGFR, MM‐PBSA, MD Simulations, ADME/Tox, and in vitro Studies

Patel

Shah²,

Soni³

et al. 2023

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With aim of developing the crucial pharmacophoric properties of the reported EGFR inhibitors (EGFRIs), a series of thiophene compounds having ethyl 5-methylthiophene-3-carboxylate core were designed. The designed compounds were subjected to molecular docking studies that indicated the potentialities of compounds APÀ A8, A9, A13 and A15 to be EGFRIs. Then, the MD simulations studies confirmed the stability and the correct binding of compound APÀ A15 -EGFR complex at both energetic and conformational levels. Furthermore, in silico ADMET prediction revealed that the majority of the proposed compounds had drug-like characteristics and have minimal toxicity and unfavourable side effects. The designed compounds were synthesized and there in vitro anticancer activity against the cancer cell line (MCF-7) was measured. Ethyl 5methyl-4-phenyl-2-(2-(4-(thiophen-2-ylsulfonyl)piperazin-1yl)acetamido)thiophene-3-carboxylate (APÀ A15) was found to be most potent compound with EC 50 values 3.5 μM, which was very close to Tamoxifen and Brigatinib. Majority compounds showed good to moderate cytotoxic activities ranging from 3.5 μM to 35.9 μM.

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Design, Synthesis, In Silico Studies and In Vitro Anticancer Activity of 3‐(4‐Methoxyphenyl)azetidine Derivatives

Cited by 6 publications

References 31 publications

Synthesis, Characterization, Molecular Docking and in vitro Anticancer Screening of Some Novel Thiophene Derivatives

Synthesis, Characterization, Molecular Docking and in vitro Anticancer Screening of Some Novel Thiophene Derivatives

Design, synthesis, and in silico study of hybrid oxoazetidine conjugated thiazoles as anti‐EGFR with cytotoxicity activity

Discovery of Anti‐Breast Cancer Thiophene Sulfonamide Derivatives: Design, Synthesis, Molecular Docking against EGFR, MM‐PBSA, MD Simulations, ADME/Tox, and in vitro Studies

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