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

González-Gualda, Estela; Páez-Ribes, Marta; Lozano‐Torres, Beatriz; Macías, David; Wilson, Joanne S.; 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; Muñoz‐Espín, Daniel

doi:10.1111/acel.13142

Cited by 143 publications

(119 citation statements)

References 44 publications

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“…There have been recent attempts to increase the specificity of Navitoclax to senescent cells by combining the drug with galactose. As senescent cells have higher levels of the galactosidase enzyme (SA β-galactosidase), the release of active Navitoclax is targeted to the senescent cells, potentially reducing platelet toxicity [ 93 ]. There are currently a few early phase clinical trials in progress, but unless the toxicity issue can be addressed it may not have a role in routine oncology practice.…”

Section: Senotherapiesmentioning

confidence: 99%

Senescence and Cancer: A Review of Clinical Implications of Senescence and Senotherapies

Wyld

Bellantuono

Tchkonia

et al. 2020

Cancers

143

117

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Cellular senescence is a key component of human aging that can be induced by a range of stimuli, including DNA damage, cellular stress, telomere shortening, and the activation of oncogenes. Senescence is generally regarded as a tumour suppressive process, both by preventing cancer cell proliferation and suppressing malignant progression from pre-malignant to malignant disease. It may also be a key effector mechanism of many types of anticancer therapies, such as chemotherapy, radiotherapy, and endocrine therapies, both directly and via bioactive molecules released by senescent cells that may stimulate an immune response. However, senescence may contribute to reduced patient resilience to cancer therapies and may provide a pathway for disease recurrence after cancer therapy. A new group of drugs, senotherapies, (drugs which interact with senescent cells to interfere with their pro-aging impacts by either selectively destroying senescent cells (senolytic drugs) or inhibiting their function (senostatic drugs)) are under active investigation to determine whether they can enhance the efficacy of cancer therapies and improve resilience to cancer treatments. Senolytic drugs include quercetin, navitoclax, and fisetin and preclinical and early phase clinical data are emerging of their potential role in cancer treatments, although none are yet in routine use clinically. This article provides a review of these issues.

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Section: Senotherapiesmentioning

confidence: 99%

Senescence and Cancer: A Review of Clinical Implications of Senescence and Senotherapies

Wyld

Bellantuono

Tchkonia

et al. 2020

Cancers

143

117

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“…The description of the first senolytic treatments by the combination of dasatinib with quercetin in vitro [17], or the inhibitor of the Bcl-2 family of antiapoptotic proteins navitoclax [18], was followed by many other new, and still less studied senolytic compounds [19][20][21]. In general, senolytics have been used in mouse models to alleviate senescence-related diseases [16,[22][23][24] The use of senolytic compounds has been previously reported for the treatment of type 2 diabetes in mouse models. In particular, the combination of dasatinib and quercetin was used to alleviate metabolic dysfunction in diet-induced obese mice, attaining a reduction in the senescence markers SA-βGal and Cdkn2a-p16, and improved glucose and insulin tolerance tests [25].…”

Section: Introductionmentioning

confidence: 99%

Transient metabolic improvement in obese mice treated with navitoclax or dasatinib/quercetin

Sierra-Ramirez

López-Aceituno

Costa‐Machado

et al. 2020

Aging

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Senescent cells accumulate with obesity in the white adipose tissue of mice and humans. These senescent cells enhance the pro-inflammatory environment that, with time, contributes to the onset of glucose intolerance and type 2 diabetes. Glucose intolerance in mouse models of obesity has been successfully reversed by the elimination of senescent cells with the senolytic compounds navitoclax or the combination of dasatinib and quercetin (D/Q). In this work, we generated obese mice by high-fat diet feeding, and treated them with five consecutive cycles of navitoclax or D/Q during 16 weeks. We observed an efficient reduction in the white adipose tissue of the senescence markers senescence-associated β-galactosidase activity, Cdkn2a-p16 and Cdkn2a-p19 at the end of the 5 cycles. Mice treated with both navitoclax and D/Q showed an improvement of their insulin sensitivity and glucose tolerance during a short period of time (cycles 3 and 4), that disappeared at the fifth cycle. Also, these mice tended to increase the expression at their adipose tissue of the adipogenic genes Pparg and, Cebpa, as well as their plasma adiponectin levels. Together, our work shows that two different senolytic treatments, acting through independent pathways, are transiently effective in the treatment of obesity-induced metabolic disorders.

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“…84 Cytotoxic drugs have also been targeted to senescent cells by conjugation with galactose or galacto-oligosaccharides. [85][86][87] In addition, local senolytic delivery to target organs, such as the articulations of osteoarthritic patients may also attenuate systemic side effects.…”

mentioning

confidence: 99%

Emerging use of senolytics and senomorphics against aging and chronic diseases

Martel

Ojcius

et al. 2020

Medicinal Research Reviews

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Senescence is a state of cell cycle arrest that plays an important role in embryogenesis, wound healing and protection against cancer. Senescent cells also accumulate during aging and contribute to the development of age-related disorders and chronic diseases, such as atherosclerosis, type 2 diabetes, osteoarthritis, idiopathic pulmonary fibrosis, and liver disease. Molecules that induce apoptosis of senescent cells, such as dasatinib, quercetin, and fisetin, produce health benefits and extend lifespan in animal models. We describe here the mechanism of action of senolytics and senomorphics, many of which are derived from plants and fungi. We also discuss the possibility of using such compounds to delay aging and treat chronic diseases in humans.

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

Cited by 143 publications

References 44 publications

Senescence and Cancer: A Review of Clinical Implications of Senescence and Senotherapies

Senescence and Cancer: A Review of Clinical Implications of Senescence and Senotherapies

Transient metabolic improvement in obese mice treated with navitoclax or dasatinib/quercetin

Emerging use of senolytics and senomorphics against aging and chronic diseases

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