Newly Synthesized 6-Substituted Piperazine/Phenyl-9-cyclopentyl Containing Purine Nucleobase Analogs Act as Potent Anticancer Agents and Induce Apoptosis <i>via</I> Inhibiting Src in Hepatocellular Carcinoma Cells

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Date

2023

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Royal Soc Chemistry

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Green Open Access

Yes

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Abstract

Newly synthesized 6-substituted piperazine/phenyl-9-cyclopentyl-containing purine nucleobase analogs were tested for their in vitro anticancer activity against human cancer cells. Compounds 15, 17-24, 49, and 56 with IC50 values less than 10 mu M were selected for further examination on an enlarged panel of liver cancer cell lines. Experiments revealed that compound 19 utilizes its high cytotoxic potential (IC50 < 5 mu M) to induce apoptosis in vitro. Compound 19 displayed a KINOMEscan selectivity score S35 of 0.02 and S10 of 0.01 and demonstrated a significant selectivity against anaplastic lymphoma kinase (ALK) and Bruton's tyrosine kinase (BTK) over other kinases. Compounds 19, 21, 22, 23, and 56 complexed with ALK, BTK, and (discoidin domain-containing receptor 2) DDR2 were analyzed structurally for binding site interactions and binding affinities via molecular docking and molecular dynamics simulations. Compounds 19 and 56 displayed similar interactions with the activation loop of the kinases, while only compound 19 reached toward the multiple subsites of the active site. Cell cycle and signaling pathway analyses exhibited that compound 19 decreases phosho-Src, phospho-Rb, cyclin E, and cdk2 levels in liver cancer cells, eventually inducing apoptosis.

Description

Sahin, Irem Durmaz/0000-0001-5037-7883; Servili, Burak/0000-0001-8869-6302; Essiz, Sebnem/0000-0002-5476-4722; Bilget Guven, Ebru/0000-0001-9734-9679

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RSC Medicinal Chemistry

Volume

14

Issue

12

Start Page

2658

End Page

2676
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