Furanolabdanoid–based 1,2,4‐oxadiazoles: Synthesis and cytotoxic activity

Mironov, M. E.; Pokrovsky, Mikhail A.; Kharitonov, Yurii V.; Шакиров, М. М.; Pokrovsky, Andrey G.; Шульц, Э. Э.

doi:10.1002/slct.201600042

Cited by 12 publications

(16 citation statements)

References 31 publications

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“…From this screening, compound 55 ( Figure 10) emerged for its remarkable toxicity, with GI50 values of 0.08 ± 0.03 µM on CEM-13, and 0.35 ± 0.11 µM on MT-4. Moreover, cytofluorimetric analysis demonstrated that treatment of U937 cells with 55 induced apoptosis in 46.8% of cells after 24 hours and 84.4% after 48 hours [91].…”

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Specimentioning

confidence: 96%

“…Modification of oxadiazole scaffolds through conjugation to bioactive natural products, also represent a promising approach. Mironov et al exploited Furano-diterpenoids of the labdane series, an anti-inflammatory and anti-allergic drug-like [90], to build novel and potent derivatives [91]. In detail, 1,2,4-oxadiazoles were conjugated to labda-8(9),13,15-triene or labda-8(17),13,15-triene core and their antiproliferative activity and GI50 on CEM-13, MT-4 and U937 cells were measured [91].…”

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Specimentioning

confidence: 99%

“…Mironov et al exploited Furano-diterpenoids of the labdane series, an anti-inflammatory and anti-allergic drug-like [90], to build novel and potent derivatives [91]. In detail, 1,2,4-oxadiazoles were conjugated to labda-8(9),13,15-triene or labda-8(17),13,15-triene core and their antiproliferative activity and GI50 on CEM-13, MT-4 and U937 cells were measured [91]. From this screening, compound 55 ( Figure 10) emerged for its remarkable toxicity, with GI50 values of 0.08 ± 0.03 µM on CEM-13, and 0.35 ± 0.11 µM on MT-4.…”

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Specimentioning

confidence: 99%

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Groundbreaking Anticancer Activity of Highly Diversified Oxadiazole Scaffolds

Benassi

Doria

Pirota

2020

Preprint

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Nowadays, an increasing number of heterocyclic-based drugs found application in medicinal chemistry and, in particular, as anticancer agents. In this context, oxadiazoles, five-membered aromatic rings, emerged for their interesting biological properties. Modification of oxadiazole scaffolds represents a valid strategy to increase their anticancer activity, especially on 1,2,4 and 1,3,4 regioisomers. In the last years, an increasing number of oxadiazole derivatives, with remarkable cytotoxicity for several tumor lines, were identified. Structural modifications, that ensure higher cytotoxicity towards malignant cells, represent a solid starting point in the development of novel oxadiazoles-based drugs. To increase the specificity of this strategy, outstanding oxadiazole scaffolds have been designed to selectively interact with biological targets, including enzymes, globular proteins and nucleic acids, showing more promising antitumor effects. In the present work, we aim to provide a comprehensive overview of the anticancer activity of these heterocycles, describing their effect on different targets and highlighting how their structural versatility has been exploited to modulate their biological properties.

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Section: Oxadiazoles Derivatives As Anticancer Agents Without a Specimentioning

confidence: 96%

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Specimentioning

confidence: 99%

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Specimentioning

confidence: 99%

See 1 more Smart Citation

Groundbreaking Anticancer Activity of Highly Diversified Oxadiazole Scaffolds

Benassi

Doria

Pirota

2020

Preprint

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“…Modification of oxadiazole scaffolds through conjugation to bioactive natural products also represents a promising approach. Mironov et al exploited Furano-diterpenoids of the labdane series, an anti-inflammatory and anti-allergic drug-like [ 90 ], to build novel and potent derivatives [ 91 ]. In detail, 1,2,4-oxadiazoles were conjugated to labda-8(9),13,15-triene or labda-8(17),13,15-triene core and their antiproliferative activity and GI 50 on CEM-13, MT-4 and U937 cells were measured [ 91 ].…”

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Spmentioning

confidence: 99%

“…Mironov et al exploited Furano-diterpenoids of the labdane series, an anti-inflammatory and anti-allergic drug-like [ 90 ], to build novel and potent derivatives [ 91 ]. In detail, 1,2,4-oxadiazoles were conjugated to labda-8(9),13,15-triene or labda-8(17),13,15-triene core and their antiproliferative activity and GI 50 on CEM-13, MT-4 and U937 cells were measured [ 91 ]. From this screening, compound 55 ( Figure 10 ) emerged for its remarkable toxicity, with GI 50 values of 0.08 ± 0.03 µM on CEM-13, and 0.35 ± 0.11 µM on MT-4.…”

Section: Oxadiazoles Derivatives As Anticancer Agents Without a Spmentioning

confidence: 99%

Groundbreaking Anticancer Activity of Highly Diversified Oxadiazole Scaffolds

Benassi

Doria

Pirota

2020

IJMS

View full text Add to dashboard Cite

Nowadays, an increasing number of heterocyclic-based drugs found application in medicinal chemistry and, in particular, as anticancer agents. In this context, oxadiazoles—five-membered aromatic rings—emerged for their interesting biological properties. Modification of oxadiazole scaffolds represents a valid strategy to increase their anticancer activity, especially on 1,2,4 and 1,3,4 regioisomers. In the last years, an increasing number of oxadiazole derivatives, with remarkable cytotoxicity for several tumor lines, were identified. Structural modifications, that ensure higher cytotoxicity towards malignant cells, represent a solid starting point in the development of novel oxadiazole-based drugs. To increase the specificity of this strategy, outstanding oxadiazole scaffolds have been designed to selectively interact with biological targets, including enzymes, globular proteins, and nucleic acids, showing more promising antitumor effects. In the present work, we aim to provide a comprehensive overview of the anticancer activity of these heterocycles, describing their effect on different targets and highlighting how their structural versatility has been exploited to modulate their biological properties.

show abstract