Synthesis of Novel Derivatives of 4,6-Diarylpyrimidines and Dihydro-Pyrimidin-4-one and In Silico Screening of Their Anticancer Activity.

IF 2.5 4区化学 Q3 CHEMISTRY, ORGANIC

Current organic synthesis Pub Date : 2025-01-01 DOI:10.2174/0115701794356958241024082646

Oleksandr V Onipko, Veronika Stoianova, Oleksandr V Buravov, Valentyn A Chebanov, Alexander Kyrychenko, Eugene S Gladkov

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引用次数: 0

Abstract

Derivatives of pyrimidinone, dihydropyrimidinone, and 2,4-diaryl-substituted pyrimidines were synthesized by cyclocondensation of α-aminoamidines with various saturated carbonyl derivatives and their analogs. The therapeutic potential of the newly synthesized derivatives for cancer treatment was evaluated using molecular docking calculations. The molecular docking results indicate that some of the synthesized diaryl derivatives of pyrimidine exhibit high binding affinity towards PIK3γ.

Aims and objectives: 4,6-Diaryl-substituted pyrimidines have shown high inhibitory potency against phosphoinositide 3-kinases (PI3Ks), which are important targets in oncology. Inhibition of PI3Ks could potentially be a viable therapy for human cancers.

Materials and methods: The synthesis of pyrimidinone and dihydropyrimidinone derivatives as well as a series of 2,4-diaryl-substituted pyrimidines were described. These compounds were synthesized by cyclocondensation of α-aminoamidines with various saturated carbonyl derivatives and their analogs.

Results: Derivatives of pyrimidinone, dihydropyrimidinone, and 2,4-diaryl-substituted pyrimidines were synthesized by combining α-aminoamidines with various saturated carbonyl derivatives and their analogs. By adjusting the large substituents in the 2-position, we gained the ability to modify the therapeutic properties of the resulting compounds. The potential of the newly synthesized derivatives for cancer treatment was assessed using molecular docking calculations. The results of the docking calculations suggest that some of the synthesized diaryl derivatives of pyrimidine have a strong binding affinity towards PIK3γ, making them promising candidates for the development of new anticancer medications.

Conclusion: We synthesized some pyrimidinones, dihydropyrimidinones, and 2,4-diarylsubstituted pyrimidines by combining α-aminoamidines with various saturated carbonyl derivatives and similar compounds. Molecular docking results suggest that certain diaryl derivatives of pyrimidine have a strong binding affinity for PIK3γ. Moreover, diphenyl derivatives of pyrimidine exhibited dual inhibitory activity against PI3K and tubulin, showing promise for the development of next-generation microtubule-targeting agents for use in combination therapies.

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4,6-二芳基嘧啶和二氢嘧啶-4- 1新型衍生物的合成及其抗癌活性的计算机筛选

通过α-氨基脒与各种饱和羰基衍生物及其类似物的环缩合反应，合成了嘧啶酮、二氢嘧啶酮和2,4-二芳基取代嘧啶的衍生物。利用分子对接计算对新合成的癌症治疗衍生物的治疗潜力进行了评估。分子对接结果表明，一些合成的嘧啶二芳基衍生物对PIK3γ具有较高的结合亲和力。目的和目的：4,6-二芳基取代嘧啶对肿瘤中的重要靶点磷酸肌肽3激酶（PI3Ks）具有很强的抑制作用。抑制pi3k可能是治疗人类癌症的可行方法。材料与方法：介绍了嘧啶酮、二氢嘧啶酮衍生物以及一系列2,4-二芳基取代嘧啶的合成。这些化合物是由α-氨基脒与各种饱和羰基衍生物及其类似物环缩合而成的。结果：α-氨基脒与各种饱和羰基衍生物及其类似物结合，合成了嘧啶酮、二氢嘧啶酮和2,4-二芳基取代嘧啶的衍生物。通过调整2位上的大取代基，我们获得了改变所得化合物治疗性质的能力。利用分子对接计算评估了新合成的衍生物治疗癌症的潜力。对接计算的结果表明，一些合成的嘧啶二芳基衍生物对PIK3γ具有很强的结合亲和力，这使它们成为开发新的抗癌药物的有希望的候选者。结论：通过α-氨基脒与各种饱和羰基衍生物及类似化合物结合，合成了一些嘧啶类、二氢嘧啶类和2,4-二芳基取代嘧啶类化合物。分子对接结果表明，嘧啶的某些二芳基衍生物对PIK3γ具有很强的结合亲和力。此外，嘧啶的二苯基衍生物对PI3K和微管蛋白具有双重抑制活性，显示出开发下一代微管靶向药物用于联合治疗的前景。

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来源期刊

Current organic synthesis 化学-有机化学

CiteScore

3.40

自引率

5.60%

发文量

审稿时长

6-12 weeks

期刊介绍： Current Organic Synthesis publishes in-depth reviews, original research articles and letter/short communications on all areas of synthetic organic chemistry i.e. asymmetric synthesis, organometallic chemistry, novel synthetic approaches to complex organic molecules, carbohydrates, polymers, protein chemistry, DNA chemistry, supramolecular chemistry, molecular recognition and new synthetic methods in organic chemistry. The frontier reviews provide the current state of knowledge in these fields and are written by experts who are internationally known for their eminent research contributions. The journal is essential reading to all synthetic organic chemists. Current Organic Synthesis should prove to be of great interest to synthetic chemists in academia and industry who wish to keep abreast with recent developments in key fields of organic synthesis.