М. С. Бабаев scite author profile

Cancer persists as a global challenge due to the extent to which conventional anticancer therapies pose high risks counterbalanced with their therapeutic benefit. Naturally occurring substances stand as an important safer alternative source for anticancer drug development. In the current study, a series of modified lupane and ursane derivatives was subjected to in vitro screening on the NCI-60 cancer cell line panel. Compounds 6 and 7 have been identified as highly active with GI50 values ranging from 0.03 µM to 5.9 µM (compound 6) and 0.18–1.53 µM (compound 7). Thus, these two compounds were further assessed in detail in order to identify a possible antiproliferative mechanism of action. DAPI (4′,6-diamidino-2-phenylindole) staining revealed that both compounds induced nuclei condensation and overall cell morphological changes consistent with apoptotic cell death. rtPCR analysis showed that both compounds induced upregulation of proapoptotic Bak and Bad genes while downregulating Bcl-XL and Bcl-2 antiapoptotic genes. Molecular docking analysis revealed that both compounds exhibited high scores for Bcl-XL inhibition, while compound 7 showed higher in silico Bcl-XL inhibition potential as compared to the native inhibitor ATB-737, suggesting that compounds may induce apoptotic cell death through targeted antiapoptotic protein inhibition, as well.

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Copolymer of N,N-diallyl-N,N-dimethylammonium chloride with maleic acid as drug carrier

Воробьева

Бабаев

Спирихин

et al. 2016

Russ J Appl Chem

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pH-sensitive particles of polymer-surfactant complexes based on a copolymer of N,N′-diallyl-N,N′-dimethylammonium chloride with maleic acid and sodium dodecyl sulfate

Бабаев

Лобов²,

Шишлов³

et al. 2022

Reactive and Functional Polymers

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Allobetulone rearrangement to l8αH,19βH-ursane triterpenoids with antiviral activity

Бабаев

Khusnutdinova

Лобов

et al. 2020

Natural Product Research

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Allobetulone E-ring rearrangement under treating with HClO 4 in Ac 2 O under reflux afforded new triterpenoids: 3,28-diacetoxy-21-acetyl-2(3),20(21)-18α,19βH-ursandiene 3 and 3,28diacetoxy-2(3),18(19)-oleandiene 4. 18α,19βH-Ursanes were transformed at A-and E-rings into indolo-and bis-furfurylidene 7 derivatives. Structure elucidation was performed using COSY, NOESY, HSQC and HMBC experiments, and X-Ray analysis for 3. The potential of newly obtained 18α,19βH-ursanes was evaluated against HCMV and HPV-11, the NCI-60 cancer cell panel and inhibition of α-glucosidase. All of the compounds have shown viral inhibition towards HCMV compared to standard drug Acyclovir. 3-Acetoxy-21β-acetyl-20,28-epoxy-18,19Нursane 1 showed moderate activity (EC 50 4.87 μM) towards the HCMV-resistant isolate (GDGr K17) compared to standard drug Cidofovir and was four times more potent than Ganciclovir.Compound 7 inhibited the cell growth of the three melanoma and one colon cancer cell. 3-Oxo-21β-acetyl-20,28-epoxy-18,19Н-ursane 5 and compound 7 inhibited α-glucosidase with IC 50 28.0 µM and 4.0 µM being from 6 to 44 times more active than acarbose.

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