Tesi di Dottorato
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Item Charatterization of store-operated calcium entry in the neuroimmune response evoked by ischemic preconditioning in mice subjected to middle cerebral artery occlusion(Università della Calabria, 2021-06-10) Frisina, Marialaura; Andò, Sebastiano; Amantea, DianaCerebral ischemia is one of the leading causes of death and long-term disability worldwide. Currently approved therapies for ischemic stroke are limited to reperfusion through mechanical recanalization and/or pharmacological thrombolysis; however, only a small percentage of eligible patients may benefit from this treatment due to its contraindications and, furthermore, it does not provide neuroprotective effects. In this context, several studies have highlighted the potential of inducing ischemic tolerance by stimulating endogenous neuroprotection. To this aim, brain ischemic preconditioning (PC), namely a sublethal ischemic event able to increase the resistance of the brain against a subsequent, more intense ischemic insult, has been considered as a useful experimental paradigm to investigate the mechanisms implicated in brain tolerance. A deep comprehension of endogenous neuroprotection elicited by ischemic PC represents a promising approach to identify novel targets that can be translated into stroke therapy. One of the main factors involved in the progression of neuronal damage during cerebral ischemia is the alteration of cellular Ca2+ homeostasis. Indeed, cytosolic Ca2+ overload due to increased membrane permeability or to its leak from intracellular organelles could result in neuronal demise. Detrimental effects involve the activation of a series of Ca2+-dependent enzymes that degrade cellular components or activate death pathways, and the formation of cytotoxic products that cause irreversible mitochondrial damage and cellular demise. The main objective of the present research work was to investigate the involvement of store-operated calcium entry (SOCE) in brain ischemia and ischemic preconditioning in mice subjected to focal cerebral ischemia. Following an ischemic insult and depletion of Ca2+ stores, the endoplasmic reticulum Ca2+ sensor stromal interaction molecule (STIM)1 interacts with the Ca2+ selective plasmamembrane channel Orai1, to promote SOCE, that may protect neurons by re-establishing Ca2+ homeostasis or could also be the source of excessive Ca2+ influx, thus causing nonexcitotoxic neuronal death. This Ca2+ influx is regulated by SOCE-associated regulatory factor (SARAF) that associates with STIM1 and promotes a slow Ca2+- dependent inactivation of SOCE, or directly interacts with Orai1 to promote SOCE activation in the absence of STIM1. Furthermore, SOCE represents the main source of Ca2+ in immune cells, regulating several of their critical functions. Besides the pivotal role played by immune mediators in the evolution of cerebral ischemic damage, it has been demonstrated that the innate immune system is also an essential component of the delayed ischemic tolerance elicited in the brain by ischemic PC. Therefore, we investigated whether central and peripheral innate immune responses contribute to PC-induced ischemic tolerance and if modulation of different SOCE components occurs in ischemic damage (1h middle cerebral artery occlusion, MCAo, followed by 24h of reperfusion) and/or in neuroprotection conferred by ischemic PC (15 min MCAo, 72h before) in C57BL/6J adult male mice. Ischemic PC significantly reduced histological damage and neurological deficits produced in mice by a more severe ischemia of 1h. Western blot analysis revealed that Orai1 expression is not affected by the ischemic insult preceded or not by the PC stimulus in the frontoparietal ischemic cortex. However, Orai1 expression was detected in neurons, but also in Ly6B.2+ myeloid cells infiltrating the ischemic hemisphere. By contrast, STIM1 and SARAF expression, mainly found in NeuN+ neurons, was significantly reduced in the ischemic cortex. Interestingly, ischemic PC prevented SARAF downregulation in the ischemic cortex, thus suggesting that this regulatory factor may play a crucial role in SOCE-mediated tolerance. To assess the immunomodulatory effects of ischemic PC, we performed ELISA assay to demonstrate that cerebral damage was associated with increased protein levels of the proinflammatory cytokine IL-1β in the ischemic cortex, while this effect was prevented by the PC stimulus. Regarding alternatively-activated phenotypes, western blot analysis revealed a significant elevation of the expression of Ym1, marker of M2-polarized microglia/macrophages, in the ischemic cortex as compared to contralateral tissue. Interestingly, ischemic PC further increased Ym1 expression in the ipsilateral cortex as compared to MCAo group. Immunohistochemical analysis revealed that the majority of Ym1+ cells are mainly amoeboid CD11b+ myeloid cells, very likely monocytes/macrophages infiltrating from blood vessels. Thus, elevated brain infiltration of these phenotypes is very likely involved in the protective effects of ischemic PC. The involvement of the peripheral immune response was confirmed by the evidence that the 70% increase in spleen weight observed after 1h MCAo was abolished in mice pre-exposed to PC. Accordingly, flow cytometry analysis revealed that PC significantly attenuates elevation of neutrophil counts (Ly-6G+ events) induced by 1h MCAo in blood. Since the Ca2+-selective plasmamembrane channel Orai1 is crucial in the recruitment of immune cells during inflammation, we have analysed its expression in the whole population of circulating leukocytes and in neutrophils, demonstrating that the number of Orai1+ cells, mainly corresponding to Ly-6G+ neutrophils, was significantly enhanced in the blood after the ischemic insult, as compared to sham, regardless of whether mice received or not ischemic PC. In conclusion, this research project reaffirms that cerebral ischemic tolerance induced by PC involves both central and peripheral modulation of the innate immune system, further underscoring the relevance of exploiting immunomodulatory approaches for the development of effective stroke therapies and originally demonstrates that preventing SARAF downregulation could represent an important neuroprotective mechanism aimed at preserving SOCE functions, making SARAF a valuable target to protect neurons from the ischemic damage.Item A computational mechanistic study of potentially evolving platinum based anticancer drugs(Università della Calabria, 2021) Dabbish, Eslam; Andò, Sebastiano; Sicilia, EmiliaMetals are known to play a fundamental physiological role inside human body affecting many of the biological functions. Analogously, metal based drugs can also have a similar impact. Cisplatin, a simple platinum complex, is well known to be a cytotoxic agent and the first approved and most widely used metal based drug for fighting cancer. Currently, used platinum containing anticancer agents namely cisplatin, carboplatin and oxaliplatin suffer from serious toxic side effects as well as acquired and inherent drug resistance against many types of cancer. Consequently, new platinum anticancer drug families evolved to overcome the current limitations of traditional platinum drugs. Monofunctional platinum complexes, Pt(IV) complexes, platinum complexes targeting mitochondria, platinum idodio derivatives and photoactivated platinum compounds are examples of some of such newly developed platinum based cytotoxic families. Computational chemistry has strongly grown over the past years with both the increase in computers capabilities and the development of new theories and efficient algorithms that can allow to handle bigger models in a reasonable time. Molecular modelling can give a wealth of information about the studied systems in terms of energies, electronic properties, geometries, conformations, structure/activity relationships, reaction mechanisms and many others. By using quantum mechanical methods like Density Functional Theory (DFT) and its time-dependant formulation TD-DFT and molecular dynamics (MD) computational tools, the mechanism of action of some selected examples of non-traditional platinum anticancer drug families have been studied in this thesis. Phenanthriplatin is the most effective member of a new class of platinum anticancer agents (7-40 times more active than cisplatin) known as monofunctional platinum anticancer drugs. In addition, it has started its clinical trials phase. Our computational mechanistic study of phenanthriplatin highlighted the importance of the role played by its unique chemical structure in the drug activation, interaction with DNA and transcription blockage. Targeting of mitochondrial DNA by means of platinum drugs can lead to mitochondrial dysfunction in cancer cells that causes tumour cells growth inhibition and apoptosis. We have undertaken a comparative study between three different isomers of a recently prepared triphenyl phosphonium modified monofunctional platinum complexes for their mechanism of action. Pt(IV) complexes are prodrugs that are reduced inside the body by means of abundant biological reducing agents like ascorbic acid to release the equivalent cytotoxic Pt(II) complexes. This reduction step is considered to be the limiting step for the activity of such class of drugs. In a series of studies, we have carried out a detailed mechanistic study to understand the relation between the nature of Pt(IV) complexes axial and equatorial ligands and the extent and mechanism of reduction by means of ascorbic acid at physiological pH. We highlighted the particular importance and impact of the nature of axial ligands on the reduction process. Photoactivated chemotherapy (PACT) technique allows the localized activation of drugs by means of specific wavelength light. A recently synthesized complex named platicur is a cis-diammineplatinum(II) complex of curcumin in which the Pt(II) centre is bound to a curcumin molecule as the leaving ligand. Upon light irradiation curcumin molecule is released together with the doubly aquated Pt(II) complex that can exert the required cytotoxic effect. In our study, we have provided a deep insight in the photoactivated excited states and their role in the photocleavage mechanism with the release of curcumin.Item Effetto del bisfenolo A sulla vascolatura uterina materna e sull'unità feto-placentare(Università della Calabria, 2021-12-01) Barberio, Laura; Cerra, Maria Carmela; Mandalà, MaurizioItem Stromal cells in breast cancer microenvironment: molecular mechanisms involved in tumor progression and potential therapeutic targets(Università della Calabria, 2021-03-26) Augimeri, Giuseppina; Andò, Sebastiano; Bonofiglio, Daniela; Kleer, CelinaStromal cells in the tumor microenvironment (TME) play an important role in breast cancer progression, metastasis and therapeutic outcome. Among stromal cells, Tumor-Associated Macrophages (TAMs) and Mesenchymal Stem Cells (MSCs) have been shown to sustain breast tumor progression and worsen breast cancer prognosis. Elucidating the molecular mechanisms of epithelial/stromal cell interactions and discovering new therapeutic targets within the breast TME represent the main challenge of current research to increase the chances of successful treatment of breast cancer patients. Here, we firstly investigated the role of ligand-activated Peroxisome Proliferator Activator Receptor γ (PPARγ), a well-known tumor suppressor gene, to modulate breast TAM functional phenotype. We found that the treatment with natural and synthetic PPARγ ligands reduced the cytokine secretion by TAMs generated by exposure of conditioned media (CM) from breast cancer cells (BCCs). Interestingly, this effect was reversed by the PPARγ antagonist GW9662, suggesting the potential involvement of PPARγ in the attenuation of TAM polarization. Next, since it has been reported that soluble factors released in the TME mediate the tumor/stroma interactions, we mainly focused on the role of leptin which has been reported to sustain macrophage recruitment. Thus, we explored the impact of the leptin receptor knockdown (ObR sh) on BCCs in mediating the interaction between tumor cells and macrophages. In co-culture experiments between monocytes and BCCs, the absence of ObR reduced the recruitment of macrophages and affected their cytokine mRNA expression profile toward a less aggressive phenotype. We confirmed a decreased macrophage infiltration and reduced breast cancer growth in xenograft tumors of mice injected with ObR sh BCC. Furthermore, we explored the interaction between BCCs and MSCs within the breast TME. To this aim, we generated BCCs engulfing MSCs which result in hybrid cancer cells characterized by a multinucleated phenotype with increased dormancy and chemoresistance. In mouse models of breast cancer metastasis, hybrid cells had a reduced ability to form metastasis, but upon doxorubicin treatment they acquired resistance, inducing the metastatic spread of breast cancer. Collectively, our findings provide novel insights into the role of PPARγ and leptin signaling in modulating TAM polarization, opening new avenues for therapeutic intervention in breast cancer. Moreover, we identified and characterized a hybrid cell population, generated through. MSC engulfment by BBCs, with phenotypic features of malignancy, highlighting the potential of targeting stromal cells, to overcome drug resistance and metastasis in breast cancer.