Metformin and sodium dichloroacetate effects on proliferation, apoptosis, and metabolic activity tested alone and in combination in a canine prostate and a bladder cancer cell line

Klose, K.; Packeiser, Eva-Maria; Müller, Petra; Granados-Soler, José Luis; Schille, Jan Torben; Goericke-Pesch, Sandra; Kietzmann, Manfred; Escobar, Hugo Murua; Nolte, Ingo

doi:10.1371/journal.pone.0257403

Cited by 19 publications

(19 citation statements)

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“…Equal amounts of protein (lysates) or equal volumes (medium) from samples were subjected to SDS-PAGE and immunoblotting (Materials and methods). (A) Trypan blue concentrations more commonly used in studies of an in vitro nature [21][22][23][24]. The future identification of these mechanisms with respect to the effects of DCA on APP proteolysis may lead to the development of novel therapeutics for the treatment of AD.…”

Section: Discussionmentioning

confidence: 99%

The orphan drug dichloroacetate reduces amyloid beta-peptide production whilst promoting non-amyloidogenic proteolysis of the amyloid precursor protein

et al. 2022

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The amyloid cascade hypothesis proposes that excessive accumulation of amyloid beta-peptides is the initiating event in Alzheimer’s disease. These neurotoxic peptides are generated from the amyloid precursor protein via sequential cleavage by β- and γ-secretases in the ’amyloidogenic’ proteolytic pathway. Alternatively, the amyloid precursor protein can be processed via the ’non-amyloidogenic’ pathway which, through the action of the α-secretase a disintegrin and metalloproteinase (ADAM) 10, both precludes amyloid beta-peptide formation and has the additional benefit of generating a neuroprotective soluble amyloid precursor protein fragment, sAPPα. In the current study, we investigated whether the orphan drug, dichloroacetate, could alter amyloid precursor protein proteolysis. In SH-SY5Y neuroblastoma cells, dichloroacetate enhanced sAPPα generation whilst inhibiting β–secretase processing of endogenous amyloid precursor protein and the subsequent generation of amyloid beta-peptides. Over-expression of the amyloid precursor protein partly ablated the effect of dichloroacetate on amyloidogenic and non-amyloidogenic processing whilst over-expression of the β-secretase only ablated the effect on amyloidogenic processing. Similar enhancement of ADAM-mediated amyloid precursor protein processing by dichloroacetate was observed in unrelated cell lines and the effect was not exclusive to the amyloid precursor protein as an ADAM substrate, as indicated by dichloroacetate-enhanced proteolysis of the Notch ligand, Jagged1. Despite altering proteolysis of the amyloid precursor protein, dichloroacetate did not significantly affect the expression/activity of α-, β- or γ-secretases. In conclusion, dichloroacetate can inhibit amyloidogenic and promote non-amyloidogenic proteolysis of the amyloid precursor protein. Given the small size and blood-brain-barrier permeability of the drug, further research into its mechanism of action with respect to APP proteolysis may lead to the development of therapies for slowing the progression of Alzheimer’s disease.

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Section: Discussionmentioning

confidence: 99%

The orphan drug dichloroacetate reduces amyloid beta-peptide production whilst promoting non-amyloidogenic proteolysis of the amyloid precursor protein

et al. 2022

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“…In prostate cancer, several studies revealed that metformin mediates reduction in cell viability and arrest at the G1 phase of human prostate cancer cell lines, including DU145, PC3, LNCaP, 22Rv1, C4-2 and also canine prostate cancer cells [49,51,52,[65][66][67][68][69][70][71][72][73][74][75][76][77][78][79][80], without showing evidence of an effect on normal cells (such as RWPE, PREC or P69) [52,66,77]. Due to different experimental designs, some articles did not report metformin to be an apoptotic inducer [65,66,68], and others showed different degrees of apoptotic induction [52,63,[70][71][72][73][77][78][79]81].…”

Section: Prostate Cancermentioning

confidence: 99%

“…Metformin also induced apoptosis after endoplasmic reticulum (ER) stress, promoted by expression of miR-708-5p, which suppresses neuronatin (NNAT), a protein from the endoplasmic reticulum that participates in ER stress [83]. Induction of ROS production is another mechanism involved in metformin-mediated apoptosis [71][72][73].…”

Section: Prostate Cancermentioning

confidence: 99%

“…Metformin acted as a chemosensitizer of docetaxel, one of the main therapeutic agents against metastatic prostate cancer [95]. Combination with paclitaxel induced oxidative stress and induced apoptosis in a mitochondrial-dependent pathway [73]. Inhibitors of PLK1 combined with metformin induced the p53/REDD1 pathway and induced apoptosis [96].…”

Section: Prostate Cancermentioning

confidence: 99%

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Metformin and Cancer Hallmarks: Molecular Mechanisms in Thyroid, Prostate and Head and Neck Cancer Models

2022

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Metformin is the most used drug for type 2 diabetes (T2DM). Its antitumor activity has been described by clinical studies showing reduced risk of cancer development in T2DM patients, as well as management of T2DM compared with those receiving other glucose-lowering drugs. Metformin has a plethora of molecular actions in cancer cells. This review focused on in vitro data on the action mechanisms of metformin on thyroid, prostate and head and neck cancer. AMPK activation regulating specific downstream targets is a constant antineoplastic activity in different types of cancer; however, AMPK-independent mechanisms are also relevant. In vitro evidence makes it clear that depending on the type of tumor, metformin has different actions; its effects may be modulated by different cell conditions (for instance, presence of HPV infection), or it may regulate tissue-specific factors, such as the Na+/I− symporter (NIS) and androgen receptors. The hallmarks of cancer are a set of functional features acquired by the cell during malignant development. In vitro studies show that metformin regulates almost all the hallmarks of cancer. Interestingly, metformin is one of these therapeutic agents with the potential to synergize with other chemotherapeutic agents, with low cost, low side effects and high positive consequences. Some questions are still challenging: Are metformin in vitro data able to translate from bench to bedside? Does metformin affect drug resistance? Can metformin be used as a generic anticancer drug for all types of tumors? Which are the specific actions of metformin on the peculiarities of each type of cancer? Several clinical trials are in progress or have been concluded for repurposing metformin as an anticancer drug. The continuous efforts in the field and future in vitro studies will be essential to corroborate clinical trials results and to elucidate the raised questions.

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“…However, the overall median survival time for dogs that respond to NSAIDs and chemotherapy was still relatively short (up to a few months), which led to the search for novel therapeutic agents. In the past years, multiple studies including canine BC cell lines were conducted in order to evaluate the activity of novel anticancer agents ( Table 3 ) [ 15 , 16 , 17 , 18 , 19 , 20 , 21 , 22 , 23 , 24 , 25 ]. Although many of them were not transferred to in vivo studies, novel therapeutic agents that could improve survival of dog pets with bladder TCC were also found.…”

Section: Evidence Synthesismentioning

confidence: 99%

Characteristics and Applications of Canine In Vitro Models of Bladder Cancer in Veterinary Medicine: An Up-to-Date Mini Review

Nowak

Krajewski

Małkiewicz

et al. 2022

Animals

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Bladder cancer (BC) constitutes approximately 2% of all spontaneously occurring cancers in dogs. It is characterized by a devastating clinical course in most cases, which emphasizes a constant need for the development of novel methods of disease characterization and treatment. Over the past years, advances in cell engineering have resulted in the development of various canine in vitro models of BC, emerging as complements for in vivo research. In this article, we aimed to review the available data on existing in vitro models of canine BC, focusing primarily on their characteristics, applications in veterinary medicine, as well as advantages and disadvantages. The most commonly used in vitro models of canine BC comprise immortalized cell lines grown as adherent monolayers. They provide an unlimited supply of research material, however, they do not faithfully reflect the conditions prevailing in vivo, since the spatial cellular interactions are lost. The importance of the three-dimensional (3D) features of solid tumors in relation to carcinogenesis or drug response process has resulted in the development of the first canine 3D models of BC available for in vitro research. So far, results obtained with in vitro and in vivo research should be interpreted together. With the constantly growing complexity of in vitro models of BC cancer, animal-based research might be reduced in the future.

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Metformin and sodium dichloroacetate effects on proliferation, apoptosis, and metabolic activity tested alone and in combination in a canine prostate and a bladder cancer cell line

Cited by 19 publications

References 84 publications

The orphan drug dichloroacetate reduces amyloid beta-peptide production whilst promoting non-amyloidogenic proteolysis of the amyloid precursor protein

The orphan drug dichloroacetate reduces amyloid beta-peptide production whilst promoting non-amyloidogenic proteolysis of the amyloid precursor protein

Metformin and Cancer Hallmarks: Molecular Mechanisms in Thyroid, Prostate and Head and Neck Cancer Models

Characteristics and Applications of Canine In Vitro Models of Bladder Cancer in Veterinary Medicine: An Up-to-Date Mini Review

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