Your search keyword '"chemotherapy-induced senescence"' showing total 5 results

1. The lack of functional DNMT2/TRDMT1 gene modulates cancer cell responses during drug-induced senescence.

Author

Bloniarz D, Adamczyk-Grochala J, Lewinska A, and Wnuk M

Subjects

5-Methylcytosine metabolism, Autophagy drug effects, Cell Cycle Checkpoints drug effects, Cell Line, Tumor, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Cytoplasm metabolism, DNA Breaks, Double-Stranded, Gene Knockout Techniques, Humans, Oxidative Stress drug effects, beta-Galactosidase metabolism, tRNA Methyltransferases metabolism, Cellular Senescence genetics, DNA (Cytosine-5-)-Methyltransferases genetics, Doxorubicin pharmacology, Etoposide pharmacology, Neoplasms genetics, Neoplasms pathology

Abstract

Cellular senescence may be a side effect of chemotherapy and other anti-cancer treatments that may promote inflammation and paracrine secondary senescence in healthy tissues. DNMT2/TRDMT1 methyltransferase is implicated in the regulation of cellular lifespan and DNA damage response (DDR). In the present study, the responses to senescence inducing concentrations of doxorubicin and etoposide in different cancer cells with DNMT2/TRDMT1 gene knockout were evaluated, namely changes in the cell cycle, apoptosis, autophagy, interleukin levels, genetic stability and DDR, and 5-mC and NSUN1-6 levels. Moreover, the effect of azacytidine post-treatment was considered. Diverse responses were revealed that was based on type of cancer cells (breast and cervical cancer, osteosarcoma and glioblastoma cells) and anti-cancer drugs. DNMT2/TRDMT1 gene knockout in drug-treated glioblastoma cells resulted in decreased number of apoptotic and senescent cells, IL-8 levels and autophagy, and increased number of necrotic cells, DNA damage and affected DDR compared to drug-treated glioblastoma cells with unmodified levels of DNMT2/TRDMT1. We suggest that DNMT2/TRDMT1 gene knockout in selected experimental settings may potentiate some adverse effects associated with chemotherapy-induced senescence.

Published

2021

2. Galacto‐conjugation of Navitoclax as an efficient strategy to increase senolytic specificity and reduce platelet toxicity.

Author

González‐Gualda, Estela, Pàez‐Ribes, Marta, Lozano‐Torres, Beatriz, Macias, David, Wilson, Joseph R., González‐López, Cristina, Ou, Hui‐Ling, Mirón‐Barroso, Sofía, Zhang, Zhenguang, Lérida‐Viso, Araceli, Blandez, Juan F., Bernardos, Andrea, Sancenón, Félix, Rovira, Miguel, Fruk, Ljiljana, Martins, Carla P., Serrano, Manuel, Doherty, Gary J., Martínez‐Máñez, Ramón, and Muñoz‐Espín, Daniel

Subjects

*CELLULAR aging, *CANCER cells, *BLOOD platelets, *MOUSE diseases, *LUNG cancer, *BLOOD sampling, *LYSOSOMES, *PLATELET count

Abstract

Pharmacologically active compounds with preferential cytotoxic activity for senescent cells, known as senolytics, can ameliorate or even revert pathological manifestations of senescence in numerous preclinical mouse disease models, including cancer models. However, translation of senolytic therapies to human disease is hampered by their suboptimal specificity for senescent cells and important toxicities that narrow their therapeutic windows. We have previously shown that the high levels of senescence‐associated lysosomal β‐galactosidase (SA‐β‐gal) found within senescent cells can be exploited to specifically release tracers and cytotoxic cargoes from galactose‐encapsulated nanoparticles within these cells. Here, we show that galacto‐conjugation of the BCL‐2 family inhibitor Navitoclax results in a potent senolytic prodrug (Nav‐Gal), that can be preferentially activated by SA‐β‐gal activity in a wide range of cell types. Nav‐Gal selectively induces senescent cell apoptosis and has a higher senolytic index than Navitoclax (through reduced activation in nonsenescent cells). Nav‐Gal enhances the cytotoxicity of standard senescence‐inducing chemotherapy (cisplatin) in human A549 lung cancer cells. Concomitant treatment with cisplatin and Nav‐Gal in vivo results in the eradication of senescent lung cancer cells and significantly reduces tumour growth. Importantly, galacto‐conjugation reduces Navitoclax‐induced platelet apoptosis in human and murine blood samples treated ex vivo, and thrombocytopenia at therapeutically effective concentrations in murine lung cancer models. Taken together, we provide a potentially versatile strategy for generating effective senolytic prodrugs with reduced toxicities. [ABSTRACT FROM AUTHOR]

Published

2020

3. The lack of functional

Author

Dominika, Bloniarz, Jagoda, Adamczyk-Grochala, Anna, Lewinska, and Maciej, Wnuk

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Cytoplasm, tRNA Methyltransferases, anti-cancer drugs, Cell Cycle Checkpoints, beta-Galactosidase, DNMT2/TRDMT1, chemotherapy-induced senescence, Gene Knockout Techniques, Oxidative Stress, Doxorubicin, Cell Line, Tumor, Neoplasms, 5-Methylcytosine, Autophagy, cancer cells, Humans, DNA Breaks, Double-Stranded, DNA (Cytosine-5-)-Methyltransferases, Cellular Senescence, Etoposide, Research Paper

Abstract

Cellular senescence may be a side effect of chemotherapy and other anti-cancer treatments that may promote inflammation and paracrine secondary senescence in healthy tissues. DNMT2/TRDMT1 methyltransferase is implicated in the regulation of cellular lifespan and DNA damage response (DDR). In the present study, the responses to senescence inducing concentrations of doxorubicin and etoposide in different cancer cells with DNMT2/TRDMT1 gene knockout were evaluated, namely changes in the cell cycle, apoptosis, autophagy, interleukin levels, genetic stability and DDR, and 5-mC and NSUN1-6 levels. Moreover, the effect of azacytidine post-treatment was considered. Diverse responses were revealed that was based on type of cancer cells (breast and cervical cancer, osteosarcoma and glioblastoma cells) and anti-cancer drugs. DNMT2/TRDMT1 gene knockout in drug-treated glioblastoma cells resulted in decreased number of apoptotic and senescent cells, IL-8 levels and autophagy, and increased number of necrotic cells, DNA damage and affected DDR compared to drug-treated glioblastoma cells with unmodified levels of DNMT2/TRDMT1. We suggest that DNMT2/TRDMT1 gene knockout in selected experimental settings may potentiate some adverse effects associated with chemotherapy-induced senescence.

Published

2021

4. Galacto-conjugation of Navitoclax as an efficient strategy to increase senolytic specificity and reduce platelet toxicity

Author

Estela González-Gualda, Miguel Rovira, Araceli Lérida-Viso, Joseph R. Wilson, Marta Paez-Ribes, Ljiljana Fruk, Beatriz Lozano-Torres, Zhenguang Zhang, Cristina González-López, Hui Ling Ou, Daniel Muñoz-Espín, Gary J. Doherty, Félix Sancenón, Ramón Martínez-Máñez, Sofía Mirón-Barroso, Manuel Serrano, David Macías, Carla P. Martins, Andrea Bernardos, Juan F. Blandez, González-Gualda, Estela [0000-0003-1558-4259], Martínez-Máñez, Ramón [0000-0001-5873-9674], Muñoz-Espín, Daniel [0000-0002-0550-9514], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Aging, Apoptosis, thrombocytopenia, Mice, SCID, chemistry.chemical_compound, Mice, QUIMICA ORGANICA, 0302 clinical medicine, Tumor Cells, Cultured, Cytotoxic T cell, cellular senescence, Prodrugs, chemotherapy‐induced senescence, Cytotoxicity, Sulfonamides, Navitoclax, Aniline Compounds, Molecular Structure, Prodrug, chemotherapy-induced senescence, 3. Good health, Original Article, Female, prodrug, medicine.drug, Blood Platelets, Cell Survival, Antineoplastic Agents, Biology, 03 medical and health sciences, QUIMICA ANALITICA, medicine, Animals, Humans, Senolytic, Cisplatin, QUIMICA INORGANICA, Cancer, Galactose, Original Articles, Cell Biology, Neoplasms, Experimental, medicine.disease, Mice, Inbred C57BL, lung cancer, 030104 developmental biology, chemistry, senolytics, Cancer research, Navitoclax (ABT-263), Drug Screening Assays, Antitumor, 030217 neurology & neurosurgery, Ex vivo

Abstract

[EN] Pharmacologically active compounds with preferential cytotoxic activity for senescent cells, known as senolytics, can ameliorate or even revert pathological manifestations of senescence in numerous preclinical mouse disease models, including cancer models. However, translation of senolytic therapies to human disease is hampered by their suboptimal specificity for senescent cells and important toxicities that narrow their therapeutic windows. We have previously shown that the high levels of senescence-associated lysosomal beta-galactosidase (SA-beta-gal) found within senescent cells can be exploited to specifically release tracers and cytotoxic cargoes from galactose-encapsulated nanoparticles within these cells. Here, we show that galacto-conjugation of the BCL-2 family inhibitor Navitoclax results in a potent senolytic prodrug (Nav-Gal), that can be preferentially activated by SA-beta-gal activity in a wide range of cell types. Nav-Gal selectively induces senescent cell apoptosis and has a higher senolytic index than Navitoclax (through reduced activation in nonsenescent cells). Nav-Gal enhances the cytotoxicity of standard senescence-inducing chemotherapy (cisplatin) in human A549 lung cancer cells. Concomitant treatment with cisplatin and Nav-Gal in vivo results in the eradication of senescent lung cancer cells and significantly reduces tumour growth. Importantly, galacto-conjugation reduces Navitoclax-induced platelet apoptosis in human and murine blood samples treated ex vivo, and thrombocytopenia at therapeutically effective concentrations in murine lung cancer models. Taken together, we provide a potentially versatile strategy for generating effective senolytic prodrugs with reduced toxicities., Royal Society, Grant/Award Number: RG160806; Medical Research Council, Grant/Award Number: MR/R000530/1; Cancer Research UK, Grant/Award Number: C62187/A26989 and C62187/A29760; CRUK Cambridge Centre Early Detection Programme, Grant/Award Number: RG86786

Published

2020

5. Galacto-conjugation of Navitoclax as an efficient strategy to increase senolytic specificity and reduce platelet toxicity

Author

González-Gualda, Estela, Pàez-Ribes, Marta, Lozano-Torres, Beatriz, Macias, David, Wilson, Joseph R, González-López, Cristina, Ou, Hui-Ling, Mirón-Barroso, Sofía, Zhang, Zhenguang, Lérida-Viso, Araceli, Blandez, Juan F, Bernardos, Andrea, Sancenón, Félix, Rovira, Miguel, Fruk, Ljiljana, Martins, Carla P, Serrano, Manuel, Doherty, Gary J, Martínez-Máñez, Ramón, and Muñoz-Espín, Daniel

Subjects

Blood Platelets, Cell Survival, thrombocytopenia, Antineoplastic Agents, Apoptosis, Mice, SCID, Mice, Tumor Cells, Cultured, cellular senescence, Animals, Humans, Prodrugs, Sulfonamides, Aniline Compounds, Molecular Structure, Galactose, Neoplasms, Experimental, chemotherapy-induced senescence, 3. Good health, Mice, Inbred C57BL, lung cancer, senolytics, Navitoclax (ABT-263), Female, prodrug, Drug Screening Assays, Antitumor

Abstract

Pharmacologically active compounds with preferential cytotoxic activity for senescent cells, known as senolytics, can ameliorate or even revert pathological manifestations of senescence in numerous preclinical mouse disease models, including cancer models. However, translation of senolytic therapies to human disease is hampered by their suboptimal specificity for senescent cells and important toxicities that narrow their therapeutic windows. We have previously shown that the high levels of senescence-associated lysosomal β-galactosidase (SA-β-gal) found within senescent cells can be exploited to specifically release tracers and cytotoxic cargoes from galactose-encapsulated nanoparticles within these cells. Here, we show that galacto-conjugation of the BCL-2 family inhibitor Navitoclax results in a potent senolytic prodrug (Nav-Gal), that can be preferentially activated by SA-β-gal activity in a wide range of cell types. Nav-Gal selectively induces senescent cell apoptosis and has a higher senolytic index than Navitoclax (through reduced activation in nonsenescent cells). Nav-Gal enhances the cytotoxicity of standard senescence-inducing chemotherapy (cisplatin) in human A549 lung cancer cells. Concomitant treatment with cisplatin and Nav-Gal in vivo results in the eradication of senescent lung cancer cells and significantly reduces tumour growth. Importantly, galacto-conjugation reduces Navitoclax-induced platelet apoptosis in human and murine blood samples treated ex vivo, and thrombocytopenia at therapeutically effective concentrations in murine lung cancer models. Taken together, we provide a potentially versatile strategy for generating effective senolytic prodrugs with reduced toxicities.