Your search keyword '"Beatrice Cavina"' showing total 7 results

1. Dysregulation of a Subset of Circulating and Vesicle-Associated miRNA in Pancreatic Cancer

Author

Giulia Girolimetti, Iulia Andreea Pelisenco, Leonardo Henry Eusebi, Claudio Ricci, Beatrice Cavina, Ivana Kurelac, Tiziano Verri, Matteo Calcagnile, Pietro Alifano, Alessandro Salvi, Cecilia Bucci, and Flora Guerra

Subjects

miRNA, extracellular vesicles, pancreatic cancer, circulating miRNA, molecular biomarkers, chemoresistance, Genetics, QH426-470

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is one of the most aggressive neoplasia, characterized by early metastasis, low diagnostic rates at early stages, resistance to drugs, and poor prognosis. There is an urgent need to better characterize this disease in order to identify efficient diagnostic/prognostic biomarkers. Since microRNAs (miRNAs) contribute to oncogenesis and metastasis formation in PDAC, they are considered potential candidates for fulfilling this task. In this work, the levels of two miRNA subsets (involved in chemoresistance or with oncogenic/tumor suppressing functions) were investigated in a panel of PDAC cell lines and liquid biopsies of a small cohort of patients. We used RT-qPCR and droplet digital PCR (ddPCR) to measure the amounts of cellular- and vesicle-associated, and circulating miRNAs. We found that both PDAC cell lines, also after gemcitabine treatment, and patients showed low amounts of cellular-and vesicle-associated miR-155-5p, compared to controls. Interestingly, we did not find any differences when we analyzed circulating miR-155-5p. Furthermore, vesicle-related miR-27a-3p increased in cancer patients compared to the controls, while circulating let-7a-5p, miR-221-3p, miR-23b-3p and miR-193a-3p presented as dysregulated in patients compared to healthy individuals. Our results highlight the potential clinical significance of these analyzed miRNAs as non-invasive diagnostic molecular tools to characterize PDAC.

Published

2024

2. Inducing respiratory complex I impairment elicits an increase in PGC1α in ovarian cancer

Author

Monica De Luise, Manuela Sollazzo, Eleonora Lama, Camelia Alexandra Coadă, Licia Bressi, Maria Iorio, Beatrice Cavina, Luigi D’Angelo, Sara Milioni, Lorena Marchio, Stefano Miglietta, Sara Coluccelli, Greta Tedesco, Anna Ghelli, Silvia Lemma, Anna Myriam Perrone, Ivana Kurelac, Luisa Iommarini, Anna Maria Porcelli, and Giuseppe Gasparre

Subjects

Medicine, Science

Abstract

Abstract Anticancer strategies aimed at inhibiting Complex I of the mitochondrial respiratory chain are increasingly being attempted in solid tumors, as functional oxidative phosphorylation is vital for cancer cells. Using ovarian cancer as a model, we show that a compensatory response to an energy crisis induced by Complex I genetic ablation or pharmacological inhibition is an increase in the mitochondrial biogenesis master regulator PGC1α, a pleiotropic coactivator of transcription regulating diverse biological processes within the cell. We associate this compensatory response to the increase in PGC1α target gene expression, setting the basis for the comprehension of the molecular pathways triggered by Complex I inhibition that may need attention as drawbacks before these approaches are implemented in ovarian cancer care.

Published

2022

3. NDUFS3 knockout cancer cells and molecular docking reveal specificity and mode of action of anti-cancer respiratory complex I inhibitors

Author

Ivana Kurelac, Beatrice Cavina, Manuela Sollazzo, Stefano Miglietta, Agnese Fornasa, Monica De Luise, Maria Iorio, Eleonora Lama, Daniele Traversa, Hamid Razi Nasiri, Anna Ghelli, Francesco Musiani, Anna Maria Porcelli, Luisa Iommarini, and Giuseppe Gasparre

Subjects

respiratory complex I, metformin, BAY 87-2243, EVP 4593, IACS-010759, complex I inhibitors, Biology (General), QH301-705.5

Abstract

Inhibition of respiratory complex I (CI) is becoming a promising anti-cancer strategy, encouraging the design and the use of inhibitors, whose mechanism of action, efficacy and specificity remain elusive. As CI is a central player of cellular bioenergetics, a finely tuned dosing of targeting drugs is required to avoid side effects. We compared the specificity and mode of action of CI inhibitors metformin, BAY 87-2243 and EVP 4593 using cancer cell models devoid of CI. Here we show that both BAY 87-2243 and EVP 4593 were selective, while the antiproliferative effects of metformin were considerably independent from CI inhibition. Molecular docking predictions indicated that the high efficiency of BAY 87-2243 and EVP 4593 may derive from the tight network of bonds in the quinone binding pocket, although in different sites. Most of the amino acids involved in such interactions are conserved across species and only rarely found mutated in human. Our data make a case for caution when referring to metformin as a CI-targeting compound, and highlight the need for dosage optimization and careful evaluation of molecular interactions between inhibitors and the holoenzyme.

Published

2022

4. Author response for 'NDUFS3 knockout cancer cells and molecular docking reveal specificity and mode of action of anti-cancer respiratory complex I inhibitors'

Author

null Ivana Kurelac, null Beatrice Cavina, null Manuela Sollazzo, null Stefano Miglietta, null Agnese Fornasa, null Monica De Luise, null Maria Iorio, null Eleonora Lama, null Daniele Traversa, null Hamid Razi Nasiri, null Anna Ghelli, null Francesco Musiani, null Anna Maria Porcelli, null Luisa Iommarini, and null Giuseppe Gasparre

Published

2022

5. On monocytes and lymphocytes biolens clustering by in flow holographic microscopy

Author

Jaromír Běhal, Daniele Pirone, Daniele Sirico, Vittorio Bianco, Martina Mugnano, Danila del Giudice, Beatrice Cavina, Ivana Kurelac, Pasquale Memmolo, Lisa Miccio, Pietro Ferraro, Běhal, Jaromír, Pirone, Daniele, Sirico, Daniele, Bianco, Vittorio, Mugnano, Martina, Del Giudice, Danila, Cavina, Beatrice, Kurelac, Ivana, Memmolo, Pasquale, Miccio, Lisa, and Ferraro, Pietro

Subjects

Histology, white blood cells, microfluidic, digital holographic cytometry, Cell Biology, biolen, opto-biology, Pathology and Forensic Medicine

Abstract

Live cells act as biological lenses and can be employed as real-world optical components in bio-hybrid systems. Imaging at nanoscale, optical tweezers, lithography and also photonic waveguiding are some of the already proven functionalities, boosted by the advantage that cells are fully biocompatible for intra-body applications. So far, various cell types have been studied for this purpose, such as red blood cells, bacterial cells, stem cells and yeast cells. White Blood Cells (WBCs) play a very important role in the regulation of the human body activities and are usually monitored for assessing its health. WBCs can be considered bio-lenses but, to the best of our knowledge, characterization of their optical properties have not been investigated yet. Here, we report for the first time an accurate study of two model classes of WBCs (i.e., monocytes and lymphocytes) by means of a digital holographic microscope coupled with a microfluidic system, assuming WBCs bio-lens characteristics. Thus, quantitative phase maps for many WBCs have been retrieved in flow-cytometry (FC) by achieving a significant statistical analysis to prove the enhancement in differentiation among sphere-like bio-lenses according to their sizes (i.e., diameter d) exploiting intensity parameters of the modulated light in proximity of the cell optical axis. We show that the measure of the low intensity area (S: Iz

Published

2022

6. Finding intracellular lipid droplets from the single-cell biolens’ signature in a holographic flow-cytometry assay

Author

Daniele Pirone, Daniele G. Sirico, Martina Mugnano, Danila Del Giudice, Ivana Kurelac, Beatrice Cavina, Pasquale Memmolo, Lisa Miccio, Pietro Ferraro, Pirone, D., Sirico, D. G., Mugnano, M., Del Giudice, D., Kurelac, I., Cavina, B., Memmolo, P., Miccio, L., and Ferraro, P.

Subjects

Article, Atomic and Molecular Physics, and Optics, Biotechnology

Abstract

In recent years, intracellular LDs have been discovered to play an important role in several pathologies. Therefore, detection of LDs would provide an in-demand diagnostic tool if coupled with flow-cytometry to give significant statistical analysis and especially if the diagnosis is made in full non-invasive mode. Here we combine the experimental results of in-flow tomographic phase microscopy with a suited numerical simulation to demonstrate that intracellular LDs can be easily detected through a label-free approach based on the direct analysis of the 2D quantitative phase maps recorded by a holographic flow cytometer. In fact, we demonstrate that the presence of LDs affects the optical focusing lensing features of the embracing cell, which can be considered a biological lens. The research was conducted on white blood cells (i.e., lymphocytes and monocytes) and ovarian cancer cells. Results show that the biolens properties of cells can be a rapid biomarker that aids in boosting the diagnosis of LDs-related pathologies by means of the holographic flow-cytometry assay for fast, non-destructive, and high-throughput screening of statistically significant number of cells.

Published

2022

7. Respiratory complex I null cancer cells and molecular docking reveal specificity and mode of action inhibitors with anticancer activity

Author

Luisa Iommarini, Ivana Kurelac, Beatrice Cavina, Agnese Fornasa, Daniele Traversa, Maria Iorio, Manuela Sollazzo, Monica De Luise, Eleonora Lama, Hamid Razi Nasiri, Anna Ghelli, Francesco Musiani, Giuseppe Gasparre, and Anna Maria Porcelli

Subjects

Biophysics, Cell Biology, Biochemistry

Published

2022