| Form of presentation | Articles in international journals and collections |
| Year of publication | 2024 |
| Язык | английский |
|
Bondar Oksana Viktorovna, author
Gnezdilov Oleg Ivanovich, author
Pavelev Roman Sergeevich, author
Pugachev Mikhail Vladimirovich, author
Shtyrlin Yuriy Grigorevich, author
|
|
Kadyrova Aysylu Suleymanovna, postgraduate kfu
Karut Rauda , postgraduate kfu
|
|
Alrkhmun Salekh , author
Mokhammad Taraa , author
|
| Bibliographic description in the original language |
Karwt R. Anticancer Potential of Pyridoxine-Based Doxorubicin Derivatives, in vitro Study / R. Karwt, O.V. Bondar, M.V. Pugachev, T. Mohammad, R.S. Pavelyev, S. Al-rhmoun, O.I. Gnezdilov, Y.G. Shtyrlin / Life. 2024; 14(3):282. PMID: 38541608 PMCID: PMC10970924 DOI: 10.3390/life14030282 |
| Annotation |
Doxorubicin (DOX) is a prevalent anticancer agent; however, it is unfortunately characterized
by high cardiotoxicity, myelosuppression, and multiple other side effects. To overcome DOX
limitations, two novel pyridoxine-derived doxorubicin derivatives were synthesized (DOX-1 and
DOX-2). In the present study, their antitumor activity and mechanism of action were investigated.
Of these two compounds, DOX-2, in which the pyridoxine fragment is attached to the doxorubicin
molecule via a C3 linker, revealed higher selectivity against specific cancer cell types compared to
doxorubicin and a promising safety profile for conditionally normal cells. However, the compound
with a C1 linker (DOX-1) was not characterized by selectivity of antitumor action. It was revealed that
DOX-2 obstructs cell cycle progression, induces apoptosis via the mitochondrial pathway without
the development of necrosis, and showcases antioxidant capabilities, underlining its cell-regulatory
roles. In contrast to doxorubicin's DNA-centric mechanism, DOX-2 does not interact with nuclear
DNA. Given these findings, DOX-2 presents a new promising direction in cancer therapeutics, which
is deserving of further in vivo exploration. |
| Keywords |
doxorubicin; anticancer agents; doxorubicin derivatives; pyridoxine; vitamin B6; apoptosis induction; DNA intercalation; cell-cycle arrest; antioxidants |
| The name of the journal |
Life
|
| URL |
https://www.mdpi.com/2075-1729/14/3/282 |
| Please use this ID to quote from or refer to the card |
https://repository.kpfu.ru/eng/?p_id=302492&p_lang=2 |
| Resource files | |
|
|
Full metadata record  |
| Field DC |
Value |
Language |
| dc.contributor.author |
Bondar Oksana Viktorovna |
ru_RU |
| dc.contributor.author |
Gnezdilov Oleg Ivanovich |
ru_RU |
| dc.contributor.author |
Pavelev Roman Sergeevich |
ru_RU |
| dc.contributor.author |
Pugachev Mikhail Vladimirovich |
ru_RU |
| dc.contributor.author |
Shtyrlin Yuriy Grigorevich |
ru_RU |
| dc.contributor.author |
Alrkhmun Salekh |
ru_RU |
| dc.contributor.author |
Mokhammad Taraa |
ru_RU |
| dc.contributor.author |
Kadyrova Aysylu Suleymanovna |
ru_RU |
| dc.contributor.author |
Karut Rauda |
ru_RU |
| dc.date.accessioned |
2024-01-01T00:00:00Z |
ru_RU |
| dc.date.available |
2024-01-01T00:00:00Z |
ru_RU |
| dc.date.issued |
2024 |
ru_RU |
| dc.identifier.citation |
Karwt R. Anticancer Potential of Pyridoxine-Based Doxorubicin Derivatives, in vitro Study / R. Karwt, O.V. Bondar, M.V. Pugachev, T. Mohammad, R.S. Pavelyev, S. Al-rhmoun, O.I. Gnezdilov, Y.G. Shtyrlin / Life. 2024; 14(3):282. PMID: 38541608 PMCID: PMC10970924 DOI: 10.3390/life14030282 |
ru_RU |
| dc.identifier.uri |
https://repository.kpfu.ru/eng/?p_id=302492&p_lang=2 |
ru_RU |
| dc.description.abstract |
Life |
ru_RU |
| dc.description.abstract |
Doxorubicin (DOX) is a prevalent anticancer agent; however, it is unfortunately characterized
by high cardiotoxicity, myelosuppression, and multiple other side effects. To overcome DOX
limitations, two novel pyridoxine-derived doxorubicin derivatives were synthesized (DOX-1 and
DOX-2). In the present study, their antitumor activity and mechanism of action were investigated.
Of these two compounds, DOX-2, in which the pyridoxine fragment is attached to the doxorubicin
molecule via a C3 linker, revealed higher selectivity against specific cancer cell types compared to
doxorubicin and a promising safety profile for conditionally normal cells. However, the compound
with a C1 linker (DOX-1) was not characterized by selectivity of antitumor action. It was revealed that
DOX-2 obstructs cell cycle progression, induces apoptosis via the mitochondrial pathway without
the development of necrosis, and showcases antioxidant capabilities, underlining its cell-regulatory
roles. In contrast to doxorubicin's DNA-centric mechanism, DOX-2 does not interact with nuclear
DNA. Given these findings, DOX-2 presents a new promising direction in cancer therapeutics, which
is deserving of further in vivo exploration. |
ru_RU |
| dc.language.iso |
ru |
ru_RU |
| dc.subject |
|
ru_RU |
| dc.title |
Anticancer Potential of Pyridoxine-Based Doxorubicin Derivatives, in vitro Study |
ru_RU |
| dc.type |
Articles in international journals and collections |
ru_RU |
|
RUS 
中文 
ES 
Sitemap
