Your search keyword '"Fanini, Francesca"' showing total 19 results

1. In vitro CAR-T cell killing: validation of the potency assay.

Author

Piccinini, Claudia, Carloni, Silvia, Arienti, Chiara, Pancisi, Elena, Fanini, Francesca, Pignatta, Sara, Soldati, Valentina, Stefanelli, Monica, Granato, Anna Maria, Martinelli, Giovanni, Ridolfi, Laura, and Petrini, Massimiliano

Subjects

KINETIC control, CD19 antigen, CHIMERIC antigen receptors, INTRACLASS correlation, CELL lines

Abstract

For advanced therapy medicinal products, the development and validation of potency assays are required, in accordance with international guidelines, to characterise the product and obtain reliable and consistent data. Our purpose was to validate the killing assay for the evaluation of autologous anti-CD19 chimeric antigen receptor (CAR) T potency. We used CD4 + and CD8 + lymphocytes or anti-CD19 CAR-T cells as effector cells and REH (CD19 +) or MOLM-13 (CD19 −) cell lines as target cells. After co-culturing target and effector cells (1:1 ratio) for 24 h, samples were labelled with 7-AAD, anti-CD3 and anti-CD19 antibodies and the frequency of CD19 + dead cells was evaluated by flow cytometry. In order to verify the CAR-T specificity for the CD19 + target, the co-culture between CAR-T and REH or MOLM-13 at different effector-to-target ratios was scheduled. Moreover, not transduced CD4 + and CD8 + lymphocytes were tested in comparison with CAR-T from the same donor to demonstrate the assay specificity. Linearity and accuracy were evaluated, and established acceptance criteria were compiled for both parameters (r2 ≥ 0.97 for linearity and average relative error ≤ 10% for accuracy). Furthermore, the method was considered robust when performed between 23 and 25 h of co-culture, and the intra-assay, inter-assay and inter-day precision was obtained. Finally, in order to verify the inter-analyst precision, the test was executed by three different operators and the intra-class correlation coefficient was > 0.4 in both cases. In conclusion, we consider this CAR-T potency assay as validated and usable in all steps of product development and quality control. [ABSTRACT FROM AUTHOR]

Published

2024

2. Stability Program in Dendritic Cell Vaccines: A "Real-World" Experience in the Immuno-Gene Therapy Factory of Romagna Cancer Center.

Author

Pancisi, Elena, Granato, Anna Maria, Scarpi, Emanuela, Ridolfi, Laura, Carloni, Silvia, Moretti, Cinzia, Guidoboni, Massimo, De Rosa, Francesco, Pignatta, Sara, Piccinini, Claudia, Soldati, Valentina, Calabrò, Luana, Framarini, Massimo, Stefanelli, Monica, Bulgarelli, Jenny, Tazzari, Marcella, Fanini, Francesca, and Petrini, Massimiliano

Subjects

DENDRITIC cells, CANCER vaccines, VACCINES, MEDICAL supplies, THERAPEUTICS

Abstract

Advanced therapy medical products (ATMPs) are rapidly growing as innovative medicines for the treatment of several diseases. Hence, the role of quality analytical tests to ensure consistent product safety and quality has become highly relevant. Several clinical trials involving dendritic cell (DC)-based vaccines for cancer treatment are ongoing at our institute. The DC-based vaccine is prepared via CD14+ monocyte differentiation. A fresh dose of 10 million DCs is administered to the patient, while the remaining DCs are aliquoted, frozen, and stored in nitrogen vapor for subsequent treatment doses. To evaluate the maintenance of quality parameters and to establish a shelf life of frozen vaccine aliquots, a stability program was developed. Several parameters of the DC final product at 0, 6, 12, 18, and 24 months were evaluated. Our results reveal that after 24 months of storage in nitrogen vapor, the cell viability is in a range between 82% and 99%, the expression of maturation markers remains inside the criteria for batch release, the sterility tests are compliant, and the cell costimulatory capacity unchanged. Thus, the data collected demonstrate that freezing and thawing do not perturb the DC vaccine product maintaining over time its functional and quality characteristics. [ABSTRACT FROM AUTHOR]

Published

2022

3. ACE2 and TMPRSS2 Potential Involvement in Genetic Susceptibility to SARS-COV-2 in Cancer Patients.

Author

Ravaioli, Sara, Tebaldi, Michela, Fonzi, Eugenio, Angeli, Davide, Mazza, Massimiliano, Nicolini, Fabio, Lucchesi, Alessandro, Fanini, Francesca, Pirini, Francesca, Tumedei, Maria Maddalena, Cerchione, Claudio, Viale, Pierluigi, Sambri, Vittorio, Martinelli, Giovanni, and Bravaccini, Sara

Subjects

CANCER patients, SARS-CoV-2, ANGIOTENSIN converting enzyme, MEMBRANE proteins, GENE expression

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has caused a global pandemic. One open question is whether genetics could influence the severity of symptoms. Considering the limited data on cancer patients, we analyzed public data repositories limited to investigate angiotensin-converting enzyme 2 (ACE2) and the transmembrane serine protease 2 (TMPRSS2) expressions and genetic variants to identify the basis of individual susceptibility to SARS-CoV-2. Gene expression and variant data were retrieved from Tissue Cancer Genome Atlas, Genotype-Tissue Expression, and gnomAD. Differences in gene expression were tested with Mann-Whitney U-test. Allele frequencies of germline variants were explored in different ethnicities, with a special focus on ACE2 variants located in the binding site to SARS-CoV-2 spike protein. The analysis of ACE2 and TMPRSS2 expressions in healthy tissues showed a higher expression in the age class 20 to 59 years (false discovery rate [FDR] < 0.0001) regardless of gender. ACE2 and TMPRSS2 were more expressed in tumors from males than females (both FDR < 0.0001) and, opposite to the regulation in tissues from healthy individuals, more expressed in elderly patients (FDR = 0.005; FDR < 0.0001, respectively). ACE2 and TMPRSS2 expressions were higher in cancers of elderly patients compared with healthy individuals (FDR < 0.0001). Variants were present at low frequency (range 0% to 3%) and among those with the highest frequency, the variant S19P belongs to the SARS-CoV-2 spike protein binding site and it was exclusively present in Africans with a frequency of 0.2%. The mechanisms of ACE2 and TMPRSS2 regulation could be targeted for preventive and therapeutic purposes in the whole population and especially in cancer patients. Further studies are needed to show a direct correlation of ACE2 and TMPRSS2 expressions in cancer patients and the incidence of COVID-19. [ABSTRACT FROM AUTHOR]

Published

2020

4. MicroRNAs and Androgen Receptor: Emerging Players in Breast Cancer.

Author

Bandini, Erika and Fanini, Francesca

Subjects

ANDROGEN receptors, BREAST cancer, DEVELOPMENTAL biology, HORMONE receptors

Abstract

Breast cancer (BC) is the most common cause of cancer among women, with a high incidence rate occurrence every year worldwide despite advances in its management. BC is characterized by a spectrum of subtypes which respond differently to treatments due to their biological features, representing the main issue in the control of this type of malignancy. Androgen receptor (AR) is emerging as a target to investigate among hormone receptors, since it seems to play a role at various stages of development of specific BC subsets. For this reason, in recent years AR has become very important in the clinical practice, although its role remains controversial. A number of studies have proposed a correlation between microRNAs (miRNAs), a class of gene expression modulators, and AR in prostate cancer (PC), but there are still few evidences about the relationship between miRNAs and AR in BC. The purpose of this review is to present a state of the art scenario with consideration to the most recent discoveries about miRNAs involved in the AR associated pathogenesis of BC, in order to provide new insights into the role of miRNAs as key drivers in the modulation of AR, and possible actors in the development and progression of BC. Moreover, we consider findings about involvement of AR signaling in all stages of BC, highlighting its association with different subsets of breast carcinomas and with pre- and postmenopausal state of patients. [ABSTRACT FROM AUTHOR]

Published

2019

5. Transcribed ultraconserved region 339 promotes carcinogenesis by modulating tumor suppressor microRNAs.

Author

Vannini, Ivan, Wise, Petra M., Challagundla, Kishore B., Plousiou, Meropi, Raffini, Mirco, Bandini, Erika, Fanini, Francesca, Paliaga, Giorgia, Crawford, Melissa, Ferracin, Manuela, Ivan, Cristina, Fabris, Linda, Davuluri, Ramana V., Zhiyi Guo, Angelica Cortez, Maria, Xinna Zhang, Lu Chen, Shuxing Zhang, Fernandez-Cymering, Cecilia, and Leng Han

Abstract

The transcribed ultraconserved regions (T-UCRs) encode long non-coding RNAs implicated in human carcinogenesis. Their mechanisms of action and the factors regulating their expression in cancers are poorly understood. Here we show that high expression of uc.339 correlates with lower survival in 210 non-small cell lung cancer (NSCLC) patients. We provide evidence from cell lines and primary samples that TP53 directly regulates uc.339. We find that transcribed uc.339 is upregulated in archival NSCLC samples, functioning as a decoy RNA for miR-339-3p, -663b-3p, and -95-5p. As a result, Cyclin E2, a direct target of all these microRNAs is upregulated, promoting cancer growth and migration. Finally, we find that modulation of uc.339 affects microRNA expression. However, overexpression or downregulation of these microRNAs causes no significant variations in uc.339 levels, suggesting a type of interaction for uc.339 that we call “entrapping”. Our results support a key role for uc.339 in lung cancer. [ABSTRACT FROM AUTHOR]

Published

2017

6. Prolonged Pemetrexed Infusion Plus Gemcitabine in Refractory Metastatic Colorectal Cancer: Preclinical Rationale and Phase II Study Results.

Author

Passardi, Alessandro, Fanini, Francesca, Turci, Livia, Foca, Flavia, Rosetti, Paola, Ruscelli, Silvia, Casadei Gardini, Andrea, Valgiusti, Martina, Dazzi, Claudio, and Marangolo, Maurizio

Subjects

ANTIMETABOLITES, COMBINATION drug therapy, CLINICAL trials, COLON tumors, INTRAVENOUS therapy, METASTASIS, RECTUM tumors, TREATMENT effectiveness, PEMETREXED

Abstract

Lessons Learned: Difficulties in translating in vitro results into clinical practice are inevitable.Further efforts to verify the efficacy of alternative schedules of pemetrexed in solid tumors are encouraged. Background: We investigated the cytotoxic activity of pemetrexed in combination with several drugs (gemcitabine, carboplatin, vinorelbine, and mitomycin C) using different exposure schedules in three colon cancer cell lines. The best results were obtained with the following schedule: a prolonged pemetrexed exposure followed by a 48‐hour wash‐out and then gemcitabine. This combination was then advanced to a phase II clinical trial. Methods: Patients with metastatic colorectal cancer in progression after standard treatment were included in the study. Adequate bone marrow reserve, normal hepatic and renal function, and an Eastern Cooperative Oncology Group (ECOG) performance status of 0–2 were required. Treatment consisted of an 8‐hour intravenous infusion of pemetrexed 150 mg/m2 on day 1 and a 30‐minute intravenous infusion of gemcitabine 1,000 mg/m2 on day 3 of each cycle, repeated every 14 days. Results: Fourteen patients were enrolled onto the study (first step). No objective responses were seen, and evidence of stable disease was observed in only one of the 12 evaluable patients. The most important grade 3–4 side effects were hematological toxicity (neutropenia 64.2%, thrombocytopenia 71.4%, anemia 28.7%), fatigue (50.0%), and stomatitis (21.5%). Median overall survival and time to progression were 5.8 months (95% confidence interval [CI]: 3.9–7.1) and 2.1 months (95% CI: 1.7–2.8), respectively. Conclusion: The experimental pemetrexed‐gemcitabine combination proved to be inactive and moderately toxic. 经验总结 • 将体外结果转化为临床实践时, 遇到困难在所难免。 • 鼓励开展进一步工作来验证培美曲塞替代方案治疗实体瘤的疗效。 摘要 背景. 我们在3种结肠癌细胞系中考察了培美曲塞以不同给药方案与数种药物（吉西他滨、卡铂、长春瑞滨和丝裂霉素C）联用时的细胞毒活性。使用以下方案时获得了最佳结果：延长培美曲塞给药时间, 48小时洗脱期之后再给予吉西他滨。随后将这一联合用药方案推进至II期临床试验阶段。 方法. 本研究纳入了标准治疗后疾病进展的转移性结直肠癌患者。要求患者具有适当的骨髓储备、肝肾功能正常且美国东部肿瘤协作组（ECOG）体力状态评分为0‐2。治疗方案为在每个周期的第1天静脉输注培美曲塞150 mg/m2, 输注8小时, 并在第3天静脉输注吉西他滨1 000 mg/m2, 输注30分钟, 每14天为一个周期。 结果. 14例患者入组研究（第1步）。未观察到客观缓解, 12例可评价患者中仅有1例观察到疾病稳定证据。最重要的3‐4级副作用为血液学毒性（中性粒细胞减少症64.2%, 血小板减少症71.4%, 贫血28.7%）、疲乏（50.0%）和口腔炎（21.5%）。中位总生存期和至疾病进展时间分别为5.8个月[95%置信区间（CI）：3.9‐7.1]和2.1个月（95% CI：1.7‐2.8）。 结论. 本研究证明, 培美曲塞与吉西他滨的实验性联合治疗方案无效且具有中等毒性。 [ABSTRACT FROM AUTHOR]

Published

2017

7. MiR-30 Family Potentially Targeting PI3K-SIAH2 Predicted Interaction Network Represents a Novel Putative Theranostic Panel in Non-small Cell Lung Cancer.

Author

Chan, Lawrence W. C., Fengfeng Wang, Fei Meng, Lili Wang, Sze Chuen Cesar Wong, Au, Joseph S. K., Sijun Yang, Cho, William C. S., Fanini, Francesca, and Bowen, Timothy

Subjects

LUNG cancer, PROTEIN-tyrosine kinase inhibitors, ERLOTINIB, THERAPEUTICS

Abstract

Non-small cell lung cancer (NSCLC) comprises about 84% of all lung cancers. Many treatment options are available but the survival rate is still very low due to drug resistance. It has been found that phosphoinositide-3-kinase (PI3K) affects sensitivity to tyrosine kinase inhibitors (TKIs), including gefitinib and erlotinib. Expression level of seven in absentia homolog 2 (SIAH2), an E3 ubiquitin-protein ligase, is upregulated in NSCLC and correlated with tumor grade. However, the relationship between PI3K and SIAH2 remains unclear and therefore it is not known whether they can act as treatment co-targets and theranostic dual markers for overcoming TKI resistance. It is worthy to note that PI3K and SIAH2 are potentially regulated by a common group of microRNAs in miR-30 family. Our bioinformatics analyses showed upregulated SIAH2 expression in NSCLC based on mass spectrometry data, explored its indirect interaction with PI3K and predicted their targeting microRNAs in common. We have also explored the potential role of miR-30 family in the modulation of PI3K-SIAH2 interaction in NSCLC. [ABSTRACT FROM AUTHOR]

Published

2017

8. Exosome-Mediated Transfer of microRNAs Within the Tumor Microenvironment and Neuroblastoma Resistance to Chemotherapy.

Author

Challagundla, Kishore B., Wise, Petra M., Neviani, Paolo, Chava, Haritha, Murtadha, Mariam, Tong Xu, Kennedy, Rebekah, Ivan, Cristina, Xinna Zhang, Vannini, Ivan, Fanini, Francesca, Amadori, Dino, Calin, George A., Hadjidaniel, Michael, Hiroyuki Shimada, Jong, Ambrose, Seeger, Robert C., Asgharzadeh, Shahab, Goldkorn, Amir, and Fabbri, Muller

Subjects

EXOSOMES, MICRORNA, DRUG resistance in cancer cells, MONOCYTES, NEUROBLASTOMA, CANCER chemotherapy, REVERSE transcriptase polymerase chain reaction

Abstract

Background: How exosomic microRNAs (miRNAs) contribute to the development of drug resistance in the context of the tumor microenvironment has not been previously described in neuroblastoma (NBL). Methods: Coculture experiments were performed to assess exosomic transfer of miR-21 from NBL cells to human monocytes and miR-155 from human monocytes to NBL cells. Luciferase reporter assays were performed to assess miR- 155 targeting of TERF1 in NBL cells. Tumor growth was measured in NBL xenografts treated with Cisplatin and peritumoral exosomic miR-155 (n = 6 mice per group) CD163, miR-155, and TERF1 levels were assessed in 20 NBL primary tissues by Human Exon Arrays and quantitative real-time polymerase chain reaction. Student's t test was used to evaluate the differences between treatment groups. All statistical tests were two-sided. Results: miR-21 mean fold change (f.c.) was 12.08 ± 0.30 (P < .001) in human monocytes treated with NBL derived exosomes for 48 hours, and miR-155 mean f.c. was 4.51 ± 0.25 (P < .001) in NBL cells cocultured with human monocytes for 48 hours. TERF1 mean luciferase activity in miR-155 transfected NBL cells normalized to scrambled was 0.36 ± 0.05 (P <.001). Mean tumor volumes in Dotap-miR-155 compared with Dotap-scrambled were 322.80 ± 120 mm³ and 76.00 ± 39.3 mm³, P = .002 at day 24, respectively. Patients with high CD163 infiltrating NBLs had statistically significantly higher intratumoral levels of miR-155 (P = .04) and lower levels of TERF1 mRNA (P = .02). Conclusions: These data indicate a unique role of exosomic miR-21 and miR-155 in the cross-talk between NBL cells and human monocytes in the resistance to chemotherapy, through a novel exosomic miR-21/TLR8-NF-κB/exosomic miR-155/ TERF1 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2015

9. MicroRNAs and dendritic cell-based vaccination in melanoma patients.

Author

de Rosa, Francesco, Fanini, Francesca, Guidoboni, Massimo, Vannini, Ivan, Amadori, Dino, Ridolfi, Ruggero, Ridolfi, Laura, and Fabbri, Muller

Published

2014

10. microRNAs in the tumor microenvironment: solving the riddle for a better diagnostics.

Author

Challagundla, Kishore B, Fanini, Francesca, Vannini, Ivan, Wise, Petra, Murtadha, Mariam, Malinconico, Lawrence, Cimmino, Amelia, and Fabbri, Muller

Abstract

miRNAs are small noncoding RNAs with gene regulatory functions, frequently dysregulated in human cancers. Specific signatures of differentially expressed miRNAs can be used in the diagnosis of cancer and in some cases harbor prognostic implications. The biology of cancer is dictated not only by cancer cells but also by the surrounding tumor microenvironment. In particular, the role of miRNAs within the tumor microenvironment is emerging as of paramount importance. This review will focus on the current knowledge of the role of miRNAs and both cellular and stromal components of the tumor microenvironment. We will also discuss more recent findings, showing that miRNAs can be found inside of exosomes and mediate the cross-talk between cancer cells and surrounding cells, leading to the discovery of new fascinating molecular mechanisms leading to a better understanding of the cancer 'niche' and how these noncoding RNAs can become very promising diagnostic molecules. [ABSTRACT FROM AUTHOR]

Published

2014

11. MicroRNAs and drug modulation in cancer: an intertwined new story.

Author

Fanini, Francesca, Vannini, Ivan, and Fabbri, Muller

Abstract

MicroRNAs (miRNAs) are endogenous small non-coding RNAs (ncRNAs) which play important regulatory roles in physiological processes such as cellular differentiation, proliferation, development, apoptosis and stem cell self-renewal. An increasing number of papers have clearly claimed their involvement in cancer, providing, in some cases, also the molecular mechanisms implicated. Several studies led to the conclusion that miRNAs can be effectively used as anticancer agents alone or in combination with existing anticancer drugs. In particular, miRNAs can be effectively used to overcome drug resistance, one of the main factors responsible for anticancer treatment insuccess. One of the main questions remains how to modulate the expression of miRNAs in cancer cells. Interestingly, a few studies have shown that the expression of miRNAs is affected by drugs (including some drugs currently used as anticancer agents), therefore providing the rationale for an intertwined scenario in which miRNAs can be modulated by drugs and, in turn, can affect drug sensitivity of cancer cells. [ABSTRACT FROM AUTHOR]

Published

2011

12. Association of a MicroRNA/TP53 Feedback Circuitry With Pathogenesis and Outcome of B-Cell Chronic Lymphocytic Leukemia.

Author

Fabbri, Muller, Bottoni, Arianna, Shimizu, Masayoshi, Spizzo, Riccardo, Nicoloso, Milena S., Rossi, Simona, Barbarotto, Elisa, Cimmino, Amelia, Adair, Brett, Wojcik, Sylwia E., Valeri, Nicola, Calore, Federica, Sampath, Deepa, Fanini, Francesca, Vannini, Ivan, Musuraca, Gerardo, Dell'Aquila, Marie, Alder, Hansjuerg, Davuluri, Ramana V., and Rassenti, Laura Z.

Subjects

CHRONIC lymphocytic leukemia, TUMOR proteins, TUMOR markers, CHROMOSOME abnormalities, RNA, NEURAL circuitry, CARCINOGENESIS

Abstract

The article discusses a study which determined whether the microRNA miR-15a/miR-16-1 cluster, tumor protein p53 and miR-34b/mir-34c cluster are linked in a molecular pathway that explains the pathogenetic and prognostic implications of recurrent chromosomal abnormalities 13q, 17p and 11q deletions in chronic lymphocytic leukemia (CLL). The study's design, setting and patients employed are described. Main outcome measures include cytogenetic abnormalities, downstream effectors cyclin-dependent kinase inhibitor and ZAP70 gene. The study found that there is an association between a microRNA/TP53 feedback circuitry and CLL pathogenesis and outcome.

Published

2011

13. Enzymatic descemetic lamellar keratoplasty: pilot study.

Author

Bonci, Paolo, Bonci, Paola, Della Valle, Vincenzo, Fanini, Francesca, and Nardi-Pantoli, Angela

Published

2010

14. Modulation of mismatch repair and genomic stability by miR-155.

Author

Valeri, Nicola, Gasparini, Pierluigi, Fabbri, Muller, Braconi, Chiara, Veronese, Angelo, Lovat, Francesca, Adair, Brett, Vannini, Ivan, Fanini, Francesca, Bottoni, Arianna, Costinean, Stefan, Sandhu, Sukhinder K., Nuovo, Gerard J., Alder, Hansjuerg, Gafa, Roberta, Calore, Federica, Ferracin, Manuela, Lanza, Giovanni, Volinia, Stefano, and Negrini, Massimo

Subjects

DISEASE susceptibility, CANCER, DNA repair, COLON cancer, MICROSATELLITE repeats, CARCINOGENESIS

Abstract

Inactivation of mismatch repair (MMR) is the cause of the common cancer predisposition disorder Lynch syndrome (LS), also known as hereditary nonpolyposis colorectal cancer (HNPCC), as well as 10-40% of sporadic colorectal, endometrial, ovarian, gastric, and urothelial cancers. Elevated mutation rates (mutator phenotype), including simple repeat instability [microsatellite instability (MSI)] are a signature of MMR defects. MicroRNAs (miRs) have been implicated in the control of critical cellular pathways involved in development and cancer. Here we show that overexpression of miR-155 significantly down-regulates the core MMR proteins, hMSH2, hMSH6, and hMLH1, inducing a mutator phenotype and MSI. An inverse correlation between the expression of miR-155 and the expression of MLH1 or MSH2 proteins was found in human colorectal cancer. Finally, a number of MSI tumors with unknown cause of MMR inactivation displayed miR-155 overexpression. These data provide support for miR-155 modulation of MMR as a mechanism of cancer pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2010

15. Epigenetics, miRNAs, and human cancer: a new chapter in human gene regulation.

Author

Valeri, Nicola, Vannini, Ivan, Fanini, Francesca, Calore, Federica, Adair, Brett, and Fabbri, Muller

Subjects

GENETIC regulation, RNA, GENETIC carriers, CANCER, GENE expression

Abstract

Cancer is a genetic and epigenetic disease. MicroRNAs (miRNAs), a class of small noncoding RNAs, have been shown to be deregulated in many diseases including cancer. An intertwined connection between epigenetics and miRNAs has been supported by the recent identification of a specific subgroup of miRNAs called “epi-miRNAs” that can directly and indirectly modulate the activity of the epigenetic machinery. The complexity of this connection is enhanced by the epigenetic regulation of miRNA expression that generates a fine regulatory feedback loop. This review focuses on how epigenetics affects the miRNome and how the recently identified epi-miRNAs regulate the epigenome in human cancers, ultimately contributing to human carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2009

16. MicroRNA-16 Restores Sensitivity to Tyrosine Kinase Inhibitors and Outperforms MEK Inhibitors in KRAS -Mutated Non-Small Cell Lung Cancer.

Author

Fanini, Francesca, Bandini, Erika, Plousiou, Meropi, Carloni, Silvia, Wise, Petra, Neviani, Paolo, Murtadha, Mariam, Foca, Flavia, Fabbri, Francesco, Vannini, Ivan, and Fabbri, Muller

Subjects

NON-small-cell lung carcinoma, PROTEIN-tyrosine kinase inhibitors, RAS oncogenes

Abstract

Background: Non-small cell lung cancer (NSCLC) is the leading cause of cancer death worldwide. Chemotherapy, the treatment of choice in non-operable cases, achieves a dismal success rate, raising the need for new therapeutic options. In about 25% of NSCLC, the activating mutations of the KRAS oncogene define a subclass that cannot benefit from tyrosine kinase inhibitors (TKIs). The tumor suppressor miR-16 is downregulated in many human cancers, including NSCLC. The main objectives of this study were to evaluate miR-16 treatment to restore the TKI sensitivity and compare its efficacy to MEK inhibitors in KRAS-mutated NSCLC. Methods: We performed in vitro and in vivo studies to investigate whether miR-16 could be exploited to overcome TKI resistance in KRAS-mutated NSCLC. We had three goals: first, to identify the KRAS downstream effectors targeted by mir-16, second, to study the effects of miR-16 restoration on TKI resistance in KRAS-mutated NSCLC both in vitro and in vivo, and finally, to compare miR-16 and the MEK inhibitor selumetinib in reducing KRAS-mutated NSCLC growth in vitro and in vivo. Results: We demonstrated that miR-16 directly targets the three KRAS downstream effectors MAPK3, MAP2K1, and CRAF in NSCLC, restoring the sensitivity to erlotinib in KRAS-mutated NSCLC both in vitro and in vivo. We also provided evidence that the miR-16–erlotinib regimen is more effective than the selumetinib–erlotinib combination in KRAS-mutated NSCLC. Conclusions: Our findings support the biological preclinical rationale for using miR-16 in combination with erlotinib in the treatment of NSCLC with KRAS-activating mutations. [ABSTRACT FROM AUTHOR]

Published

2021

17. Microbiota-Derived Metabolites in Tumor Progression and Metastasis.

Author

Rossi, Tania, Vergara, Daniele, Fanini, Francesca, Maffia, Michele, Bravaccini, Sara, and Pirini, Francesca

Subjects

CANCER invasiveness, METASTASIS, METABOLITES, EPITHELIAL-mesenchymal transition, TUMOR microenvironment, MICROBIAL communities, SECONDARY metabolism, CELL metabolism

Abstract

Microbial communities and human cells, through a dynamic crosstalk, maintain a mutualistic relationship that contributes to the maintenance of cellular metabolism and of the immune and neuronal systems. This dialogue normally occurs through the production and regulation of hormonal intermediates, metabolites, secondary metabolites, proteins, and toxins. When the balance between host and microbiota is compromised, the dynamics of this relationship change, creating favorable conditions for the development of diseases, including cancers. Microbiome metabolites can be important modulators of the tumor microenvironment contributing to regulate inflammation, proliferation, and cell death, in either a positive or negative way. Recent studies also highlight the involvement of microbiota metabolites in inducing epithelial–mesenchymal transition, thus favoring the setup of the metastatic niche. An investigation of microbe-derived metabolites in "liquid" human samples, such as plasma, serum, and urine, provide further information to clarify the relationship between host and microbiota. [ABSTRACT FROM AUTHOR]

Published

2020

18. Ki67 and PR in Patients Treated with CDK4/6 Inhibitors: A Real-World Experience.

Author

Palleschi, Michela, Maltoni, Roberta, Ravaioli, Sara, Vagheggini, Alessandro, Mannozzi, Francesca, Fanini, Francesca, Pirini, Francesca, Tumedei, Maria Maddalena, Barzotti, Eleonora, Cecconetto, Lorenzo, Sarti, Samanta, Manunta, Silvia, Possanzini, Paola, Fedeli, Anna, Curcio, Annalisa, Altini, Mattia, De Giorgi, Ugo, Rocca, Andrea, and Bravaccini, Sara

Subjects

PROGESTERONE receptors, ESTROGEN receptors, HORMONE therapy, PROGRESSION-free survival, BONE cysts

Abstract

CDK4/6 inhibitors (CDK4/6i) are recommended in patients with estrogen receptor (ER)-positive, HER2-negative advanced breast cancer (ABC). Up to now, no prognostic biomarkers have been identified in this setting. We retrospectively analyzed the expression of progesterone receptor (PR) and Ki67, assessed by immunohistochemistry, in 71 ABC patients treated with CDK4/6i and analyzed the impact of these markers on progression-free survival (PFS). The majority of patients 63/71 (88.7%) received palbociclib, 4 (5.6%) received ribociclib, and 4 (5.6%) received abemaciclib. A higher median value of Ki67 was observed in cases undergoing second-line treatment (p = 0.047), whereas the luminal B subtype was more prevalent (p = 0.005). In the univariate analysis of the first-line setting, luminal A subtype showed a trend towards a correlation with a longer PFS (p = 0.053). A higher continuous Ki67 value led to a significantly shorter PFS. When the interaction between pathological characteristics and line of treatment was considered, luminal B subtype showed a significantly (p = 0.043) worse outcome (Hazard Ratio (HR) 2.84; 1.03–7.82 95% Confidence Interval (CI)). PFS in patients undergoing endocrine therapy plus CDK4/6i was inversely correlated with Ki67 expression but not with PR, suggesting that tumor proliferation has a greater impact on cell cycle inhibitors combined with endocrine therapy than PR expression. [ABSTRACT FROM AUTHOR]

Published

2020

19. Exosome-mediated transfer of microRNAs within the tumor microenvironment and neuroblastoma resistance to chemotherapy.

Author

Challagundla, Kishore B, Wise, Petra M, Neviani, Paolo, Chava, Haritha, Murtadha, Mariam, Xu, Tong, Kennedy, Rebekah, Ivan, Cristina, Zhang, Xinna, Vannini, Ivan, Fanini, Francesca, Amadori, Dino, Calin, George A, Hadjidaniel, Michael, Shimada, Hiroyuki, Jong, Ambrose, Seeger, Robert C, Asgharzadeh, Shahab, Goldkorn, Amir, and Fabbri, Muller

Subjects

PROTEIN metabolism, RNA metabolism, ANIMAL experimentation, ANTINEOPLASTIC agents, CELL communication, CELL physiology, CELL receptors, CELLULAR signal transduction, CISPLATIN, DRUG resistance in cancer cells, GENES, RESEARCH methodology, MONOCYTES, NEUROBLASTOMA, POLYMERASE chain reaction, RESEARCH funding, TISSUE culture, XENOGRAFTS, DNA-binding proteins, EXOSOMES, PHARMACODYNAMICS

Abstract

Background: How exosomic microRNAs (miRNAs) contribute to the development of drug resistance in the context of the tumor microenvironment has not been previously described in neuroblastoma (NBL).Methods: Coculture experiments were performed to assess exosomic transfer of miR-21 from NBL cells to human monocytes and miR-155 from human monocytes to NBL cells. Luciferase reporter assays were performed to assess miR-155 targeting of TERF1 in NBL cells. Tumor growth was measured in NBL xenografts treated with Cisplatin and peritumoral exosomic miR-155 (n = 6 mice per group) CD163, miR-155, and TERF1 levels were assessed in 20 NBL primary tissues by Human Exon Arrays and quantitative real-time polymerase chain reaction. Student's t test was used to evaluate the differences between treatment groups. All statistical tests were two-sided.Results: miR-21 mean fold change (f.c.) was 12.08±0.30 (P < .001) in human monocytes treated with NBL derived exosomes for 48 hours, and miR-155 mean f.c. was 4.51±0.25 (P < .001) in NBL cells cocultured with human monocytes for 48 hours. TERF1 mean luciferase activity in miR-155 transfected NBL cells normalized to scrambled was 0.36 ± 0.05 (P <.001). Mean tumor volumes in Dotap-miR-155 compared with Dotap-scrambled were 322.80±120mm(3) and 76.00±39.3mm(3), P = .002 at day 24, respectively. Patients with high CD163 infiltrating NBLs had statistically significantly higher intratumoral levels of miR-155 (P = .04) and lower levels of TERF1 mRNA (P = .02).Conclusions: These data indicate a unique role of exosomic miR-21 and miR-155 in the cross-talk between NBL cells and human monocytes in the resistance to chemotherapy, through a novel exosomic miR-21/TLR8-NF-кB/exosomic miR-155/TERF1 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2015