Your search keyword '"Pensado-López, Alba"' showing total 9 results

1. An in vitro model for osteoarthritis using long‐cultured inflammatory human macrophages repeatedly stimulated with TLR agonists.

Author

Ummarino, Aldo, Pensado‐López, Alba, Migliore, Roberta, Alcaide‐Ruggiero, Lourdes, Calà, Nicholas, Caputo, Michele, Gambaro, Francesco M., Anfray, Clément, Ronzoni, Flavio L., Kon, Elizaveta, Allavena, Paola, and Torres Andón, Fernando

Subjects

MACROPHAGES, SYNOVIAL fluid, PULMONARY alveolar proteinosis, OSTEOARTHRITIS, INFLAMMATORY mediators, GENE expression profiling, DEXAMETHASONE

Abstract

Osteoarthritis (OA) is characterized by an abundance of inflammatory M1‐like macrophages damaging local tissues. The search for new potential drugs for OA suffers from the lack of appropriate methods of long‐lasting inflammation. Here we developed and characterized an in vitro protocol of long‐lasting culture of primary human monocyte‐derived macrophages differentiated with a combination of M‐CSF+GM‐CSF that optimally supported long‐cultured macrophages (LC‐Mϕs) for up to 15 days, unlike their single use. Macrophages repeatedly stimulated for 15 days with the TLR2 ligand Pam3CSK4 (LCS‐Mϕs), showed sustained levels over time of IL‐6, CCL2, and CXCL8, inflammatory mediators that were also detected in the synovial fluids of OA patients. Furthermore, macrophages isolated from the synovia of two OA patients showed an expression profile of inflammation‐related genes similar to that of LCS‐Mϕs, validating our protocol as a model of chronically activated inflammatory macrophages. Next, to confirm that these LCS‐Mϕs could be modulated by anti‐inflammatory compounds, we employed dexamethasone and/or celecoxib, two drugs widely used in OA treatment, that significantly inhibited the production of inflammatory mediators. This easy‐to‐use in vitro protocol of long‐lasting inflammation with primary human macrophages could be useful for the screening of new compounds to improve the therapy of inflammatory disorders. [ABSTRACT FROM AUTHOR]

Published

2023

2. Zebrafish as a platform to evaluate the potential of lipidic nanoemulsions for gene therapy in cancer.

Author

Cascallar, María, Hurtado, Pablo, Lores, Saínza, Pensado-López, Alba, Quelle-Regaldie, Ana, Sánchez, Laura, Piñeiro, Roberto, and de la Fuente, María

Subjects

GENE therapy, ZEBRA danio embryos, CANCER treatment, CANCER genes, BRACHYDANIO, HUMAN genome

Abstract

Gene therapy is a promising therapeutic approach that has experienced significant groth in recent decades, with gene nanomedicines reaching the clinics. However, it is still necessary to continue developing novel vectors able to carry, protect, and release the nucleic acids into the target cells, to respond to the widespread demand for new gene therapies to address current unmet clinical needs. We propose here the use of zebrafish embryos as an in vivo platform to evaluate the potential of newly developed nanosystems for gene therapy applications in cancer treatment. Zebrafish embryos have several advantages such as low maintenance costs, transparency, robustness, and a high homology with the human genome. In this work, a new type of putrescinesphingomyelin nanosystems (PSN), specifically designed for cancer gene therapy applications, was successfully characterized and demonstrated its potential for delivery of plasmid DNA (pDNA) and miRNA (miR). On one hand, we were able to validate a regulatory effect of the PSN/miR on gene expression after injection in embryos of 0 hpf. Additionally, experiments proved the potential of themodel to study the transport of the associated nucleic acids (pDNA and miR) upon incubation in zebrafish water. The biodistribution of PSN/pDNA and PSN/miR in vivo was also assessed after microinjection into the zebrafish vasculature, demonstrating that the nucleic acids remained associated with the PSN in an in vivo environment, and could successfully reach disseminated cancer cells in zebrafish xenografts. Altogether, these results demonstrate the potential of zebrafish as an in vivo model to evaluate nanotechnology-based gene therapies for cancer treatment, as well as the capacity of the developed versatile PSN formulation for gene therapy applications. [ABSTRACT FROM AUTHOR]

Published

2022

3. What Zebrafish and Nanotechnology Can Offer for Cancer Treatments in the Age of Personalized Medicine.

Author

Cascallar, María, Alijas, Sandra, Pensado-López, Alba, Vázquez-Ríos, Abi Judit, Sánchez, Laura, Piñeiro, Roberto, and de la Fuente, María

Subjects

TUMOR treatment, CLINICAL drug trials, XENOGRAFTS, INDIVIDUALIZED medicine, FISHES, NANOMEDICINE, DRUG development, DIFFUSION of innovations, MEDICAL research

Abstract

Simple Summary: Discovering new strategies for cancer treatment is critical, considering that each year millions of deaths are caused by this disease. In this sense, therapies based on nanomedicine are an innovative approach for cancer treatment, not only because they make it possible to perform targeted therapy, but also because they can improve patients' quality of life. A key step to transfer new treatments from bench to beside is in vivo evaluation of a therapy, where zebrafish as a model organism has a fundamental role. Zebrafish has several benefits that make it ideal for studying the therapeutic capacity of novel nanotechnology-based anticancer therapies. In this review, we evaluate the potential of the nanomedicine and zebrafish synergy to achieve personalized treatments for cancer. Cancer causes millions of deaths each year and thus urgently requires the development of new therapeutic strategies. Nanotechnology-based anticancer therapies are a promising approach, with several formulations already approved and in clinical use. The evaluation of these therapies requires efficient in vivo models to study their behavior and interaction with cancer cells, and to optimize their properties to ensure maximum efficacy and safety. In this way, zebrafish is an important candidate due to its high homology with the human genoma, its large offspring, and the ease in developing specific cancer models. The role of zebrafish as a model for anticancer therapy studies has been highly evidenced, allowing researchers not only to perform drug screenings but also to evaluate novel therapies such as immunotherapies and nanotherapies. Beyond that, zebrafish can be used as an "avatar" model for performing patient-derived xenografts for personalized medicine. These characteristics place zebrafish in an attractive position as a role model for evaluating novel therapies for cancer treatment, such as nanomedicine. [ABSTRACT FROM AUTHOR]

Published

2022

4. Edelfosine nanoemulsions inhibit tumor growth of triple negative breast cancer in zebrafish xenograft model.

Author

Saraiva, Sofia M., Gutiérrez-Lovera, Carlha, Martínez-Val, Jeannette, Lores, Sainza, Bouzo, Belén L., Díez-Villares, Sandra, Alijas, Sandra, Pensado-López, Alba, Vázquez-Ríos, Abi Judit, Sánchez, Laura, and de la Fuente, María

Subjects

TRIPLE-negative breast cancer, TUMOR growth, XENOGRAFTS, ANTINEOPLASTIC agents, LABORATORY zebrafish

Abstract

Triple negative breast cancer (TNBC) is known for being very aggressive, heterogeneous and highly metastatic. The standard of care treatment is still chemotherapy, with adjacent toxicity and low efficacy, highlighting the need for alternative and more effective therapeutic strategies. Edelfosine, an alkyl-lysophospholipid, has proved to be a promising therapy for several cancer types, upon delivery in lipid nanoparticles. Therefore, the objective of this work was to explore the potential of edelfosine for the treatment of TNBC. Edelfosine nanoemulsions (ET-NEs) composed by edelfosine, Miglyol 812 and phosphatidylcholine as excipients, due to their good safety profile, presented an average size of about 120 nm and a neutral zeta potential, and were stable in biorelevant media. The ability of ET-NEs to interrupt tumor growth in TNBC was demonstrated both in vitro, using a highly aggressive and invasive TNBC cell line, and in vivo, using zebrafish embryos. Importantly, ET-NEs were able to penetrate through the skin barrier of MDA-MB 231 xenografted zebrafish embryos, into the yolk sac, leading to an effective decrease of highly aggressive and invasive tumoral cells' proliferation. Altogether the results demonstrate the potential of ET-NEs for the development of new therapeutic approaches for TNBC. [ABSTRACT FROM AUTHOR]

Published

2021

5. Zebrafish Models for the Safety and Therapeutic Testing of Nanoparticles with a Focus on Macrophages.

Author

Pensado-López, Alba, Fernández-Rey, Juan, Reimunde, Pedro, Crecente-Campo, José, Sánchez, Laura, and Torres Andón, Fernando

Subjects

BRACHYDANIO, MACROPHAGES, TOXICITY testing, ZEBRA danio, NANOPARTICLES, MEDICAL research

Abstract

New nanoparticles and biomaterials are increasingly being used in biomedical research for drug delivery, diagnostic applications, or vaccines, and they are also present in numerous commercial products, in the environment and workplaces. Thus, the evaluation of the safety and possible therapeutic application of these nanomaterials has become of foremost importance for the proper progress of nanotechnology. Due to economical and ethical issues, in vitro and in vivo methods are encouraged for the testing of new compounds and/or nanoparticles, however in vivo models are still needed. In this scenario, zebrafish (Danio rerio) has demonstrated potential for toxicological and pharmacological screenings. Zebrafish presents an innate immune system, from early developmental stages, with conserved macrophage phenotypes and functions with respect to humans. This fact, combined with the transparency of zebrafish, the availability of models with fluorescently labelled macrophages, as well as a broad variety of disease models offers great possibilities for the testing of new nanoparticles. Thus, with a particular focus on macrophage–nanoparticle interaction in vivo, here, we review the studies using zebrafish for toxicological and biodistribution testing of nanoparticles, and also the possibilities for their preclinical evaluation in various diseases, including cancer and autoimmune, neuroinflammatory, and infectious diseases. [ABSTRACT FROM AUTHOR]

Published

2021

6. Cellular and Molecular Mechanisms Underlying Glioblastoma and Zebrafish Models for the Discovery of New Treatments.

Author

Reimunde, Pedro, Pensado-López, Alba, Carreira Crende, Martín, Lombao Iglesias, Vanesa, Sánchez, Laura, Torrecilla-Parra, Marta, Ramírez, Cristina M., Anfray, Clément, Torres Andón, Fernando, Wong, David, and Robe, Pierre A.

Subjects

GLIOMA treatment, BIOLOGICAL models, MOLECULAR diagnosis, BLOOD-brain barrier, INVESTIGATIONAL drugs, MICRORNA, MACROPHAGES, GENE expression, FISHES, NEUROGLIA, GENETIC techniques

Abstract

Simple Summary: Glioblastoma (GBM) is one of the greatest challenges facing neuro-oncology today. Current treatments are far from satisfactory and, given the poor prognosis of the disease, therapeutic efforts are focused on palliative management rather than curative intervention. Here, we review the cellular heterogeneity of GBM, including tumor cells and microglia/macrophages among others, as well as the genetic, epigenetic and metabolic alterations controlling its initiation and progression. Then, we describe the genetic and xenotransplantation zebrafish models established in the last few years for the study of GBM physiopathology and for testing new drugs to improve the treatment of the disease. Taking this information into account, forthcoming studies using zebrafish models of GBM are expected to shed light on better diagnosis and treatments, thus providing hope for GBM patients. Glioblastoma (GBM) is the most common of all brain malignant tumors; it displays a median survival of 14.6 months with current complete standard treatment. High heterogeneity, aggressive and invasive behavior, the impossibility of completing tumor resection, limitations for drug administration and therapeutic resistance to current treatments are the main problems presented by this pathology. In recent years, our knowledge of GBM physiopathology has advanced significantly, generating relevant information on the cellular heterogeneity of GBM tumors, including cancer and immune cells such as macrophages/microglia, genetic, epigenetic and metabolic alterations, comprising changes in miRNA expression. In this scenario, the zebrafish has arisen as a promising animal model to progress further due to its unique characteristics, such as transparency, ease of genetic manipulation, ethical and economic advantages and also conservation of the major brain regions and blood–brain–barrier (BBB) which are similar to a human structure. A few papers described in this review, using genetic and xenotransplantation zebrafish models have been used to study GBM as well as to test the anti-tumoral efficacy of new drugs, their ability to interact with target cells, modulate the tumor microenvironment, cross the BBB and/or their toxicity. Prospective studies following these lines of research may lead to a better diagnosis, prognosis and treatment of patients with GBM. [ABSTRACT FROM AUTHOR]

Published

2021

7. Morphological Abnormalities and Gene Expression Changes Caused by High Incubation Temperatures in Zebrafish Xenografts with Human Cancer Cells.

Author

Cabezas-Sainz, Pablo, Coppel, Carlos, Pensado-López, Alba, Fernandez, Pedro, Muinelo-Romay, Laura, López-López, Rafael, Rubiolo, Juan A., and Sánchez, Laura

Subjects

HIGH temperatures, CANCER cells, GENE expression, BRACHYDANIO, XENOGRAFTS

Abstract

Published studies show that most of the human cancer xenograft studies in zebrafish embryos have used incubation temperatures in the range of 32–34 °C for 3–6 days post-injection, trying to find a compromise temperature between the zebrafish embryos (28 °C) and the human injected cells (37 °C). While this experimental setup is widely used, a question remains: is possible to overcome the drawbacks caused by a suboptimal temperature for the injected cells? To clarify the effect of temperature and injected cells on the host, in this study, we analyzed the development and health of the last in response to different temperatures in the presence or absence of injected human cancer cells. Comparing different incubation temperatures (28, 34 and 36 °C), we determined morphological abnormalities and developmental effects in injected and non-injected embryos at different time points. Besides this, the expression of selected genes was determined by qPCR to determine temperature affected metabolic processes in the embryos. The results indicate that an incubation temperature of 36 °C during a period of 48 h is suitable for xenotransplantation without morphological or metabolic changes that could be affecting the host or the injected cells, allowing them to proliferate near their optimal temperature. [ABSTRACT FROM AUTHOR]

Published

2021

8. Experimental Models to Study Autism Spectrum Disorders: hiPSCs, Rodents and Zebrafish.

Author

Pensado-López, Alba, Veiga-Rúa, Sara, Carracedo, Ángel, Allegue, Catarina, and Sánchez, Laura

Subjects

AUTISM spectrum disorders, ZEBRA danio, BRACHYDANIO, ETIOLOGY of diseases, INDUCED pluripotent stem cells, RODENTS

Abstract

Autism Spectrum Disorders (ASD) affect around 1.5% of the global population, which manifest alterations in communication and socialization, as well as repetitive behaviors or restricted interests. ASD is a complex disorder with known environmental and genetic contributors; however, ASD etiology is far from being clear. In the past decades, many efforts have been put into developing new models to study ASD, both in vitro and in vivo. These models have a lot of potential to help to validate some of the previously associated risk factors to the development of the disorder, and to test new potential therapies that help to alleviate ASD symptoms. The present review is focused on the recent advances towards the generation of models for the study of ASD, which would be a useful tool to decipher the bases of the disorder, as well as to conduct drug screenings that hopefully lead to the identification of useful compounds to help patients deal with the symptoms of ASD. [ABSTRACT FROM AUTHOR]

Published

2020

9. Modeling Cancer Using Zebrafish Xenografts: Drawbacks for Mimicking the Human Microenvironment.

Author

Cabezas-Sáinz, Pablo, Pensado-López, Alba, Sáinz, Bruno, and Sánchez, Laura

Subjects

XENOGRAFTS, BRACHYDANIO, TUMOR microenvironment, XENOTRANSPLANTATION, ANIMAL species

Abstract

The first steps towards establishing xenografts in zebrafish embryos were performed by Lee et al., 2005 and Haldi et al., 2006, paving the way for studying human cancers using this animal species. Since then, the xenograft technique has been improved in different ways, ranging from optimizing the best temperature for xenografted embryo incubation, testing different sites for injection of human tumor cells, and even developing tools to study how the host interacts with the injected cells. Nonetheless, a standard protocol for performing xenografts has not been adopted across laboratories, and further research on the temperature, microenvironment of the tumor or the cell–host interactions inside of the embryo during xenografting is still needed. As a consequence, current non-uniform conditions could be affecting experimental results in terms of cell proliferation, invasion, or metastasis; or even overestimating the effects of some chemotherapeutic drugs on xenografted cells. In this review, we highlight and raise awareness regarding the different aspects of xenografting that need to be improved in order to mimic, in a more efficient way, the human tumor microenvironment, resulting in more robust and accurate in vivo results. [ABSTRACT FROM AUTHOR]

Published

2020