Your search keyword '"González-Gualda, Estela [0000-0003-1558-4259]"' showing total 2 results

1. A guide to assessing cellular senescence in vitro and in vivo

Author

González-Gualda, Estela, Baker, Andrew G, Fruk, Ljiljana, Muñoz-Espín, Daniel, González-Gualda, Estela [0000-0003-1558-4259], Baker, Andrew G [0000-0002-6498-3208], Muñoz-Espín, Daniel [0000-0002-0550-9514], and Apollo - University of Cambridge Repository

Subjects

Aging, Lamin Type B, assessment, detection, biomarkers, Cell Cycle Proteins, Cell Cycle Checkpoints, Mitochondria, Animals, Genetically Modified, ageing, Genetic Loci, Heterochromatin, cellular senescence, Animals, Cytokines, Humans, Lysosomes, Cell Shape, Cells, Cultured, Cell Proliferation, DNA Damage

Abstract

Cellular senescence is a physiological mechanism whereby a proliferating cell undergoes a stable cell cycle arrest upon damage or stress and elicits a secretory phenotype. This highly dynamic and regulated cellular state plays beneficial roles in physiology, such as during embryonic development and wound healing, but it can also result in antagonistic effects in age-related pathologies, degenerative disorders, ageing and cancer. In an effort to better identify this complex state, and given that a universal marker has yet to be identified, a general set of hallmarks describing senescence has been established. However, as the senescent programme becomes more defined, further complexities, including phenotype heterogeneity, have emerged. This significantly complicates the recognition and evaluation of cellular senescence, especially within complex tissues and living organisms. To address these challenges, substantial efforts are currently being made towards the discovery of novel and more specific biomarkers, optimized combinatorial strategies and the development of emerging detection techniques. Here, we compile such advances and present a multifactorial guide to identify and assess cellular senescence in cell cultures, tissues and living organisms. The reliable assessment and identification of senescence is not only crucial for better understanding its underlying biology, but also imperative for the development of diagnostic and therapeutic strategies aimed at targeting senescence in the clinic.

Published

2021

2. 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