Your search keyword '"Carlo M Croce"' showing total 1,434 results

151. Data from MicroRNA Gene Expression Deregulation in Human Breast Cancer

Author

Carlo M. Croce, Massimo Negrini, Patrizia Querzoli, George A. Calin, Italo Nenci, Stefano Volinia, Piero Musiani, Anne Rosenberg, Juan P. Palazzo, Sylvie Ménard, Manuela Campiglio, Muller Fabbri, Massimo Pedriali, Eros Magri, Silvia Sabbioni, Riccardo Spizzo, Angelo Veronese, Chang-Gong Liu, Manuela Ferracin, and Marilena V. Iorio

Abstract

MicroRNAs (miRNAs) are a class of small noncoding RNAs that control gene expression by targeting mRNAs and triggering either translation repression or RNA degradation. Their aberrant expression may be involved in human diseases, including cancer. Indeed, miRNA aberrant expression has been previously found in human chronic lymphocytic leukemias, where miRNA signatures were associated with specific clinicobiological features. Here, we show that, compared with normal breast tissue, miRNAs are also aberrantly expressed in human breast cancer. The overall miRNA expression could clearly separate normal versus cancer tissues, with the most significantly deregulated miRNAs being mir-125b, mir-145, mir-21, and mir-155. Results were confirmed by microarray and Northern blot analyses. We could identify miRNAs whose expression was correlated with specific breast cancer biopathologic features, such as estrogen and progesterone receptor expression, tumor stage, vascular invasion, or proliferation index.

Published

2023

152. Cardinal Manifestations of Cancer

Author

James F. Holland, Robert C. Bast, John C. Byrd, Carlo M. Croce, Ernest Hawk, Fadlo R. Khuri, Raphael E. Pollock, Apostolia M. Tsimberadou, Christopher G. Willett, and Cheryl L. Willman

Published

2022

153. Role of the miR-301a/Fra-2/GLIPR1 axis in lung cancer cisplatin resistance

Author

Gian Luca Rampioni Vinciguerra, Marina Capece, Rosario Distefano, Giovanni Nigita, Andrea Vecchione, Francesca Lovat, and Carlo M. Croce

Subjects

lung cancer, Cancer Research, Genetics

Published

2023

154. Retraction Note: EGFR and MET receptor tyrosine kinase–altered microRNA expression induces tumorigenesis and gefitinib resistance in lung cancers

Author

Michela Garofalo, Giulia Romano, Gianpiero Di Leva, Gerard Nuovo, Young-Jun Jeon, Apollinaire Ngankeu, Jin Sun, Francesca Lovat, Hansjuerg Alder, Gerolama Condorelli, Jeffrey A. Engelman, Mayumi Ono, Jin Kyung Rho, Luciano Cascione, Stefano Volinia, Kenneth P. Nephew, and Carlo M. Croce

Subjects

Male, Epithelial-Mesenchymal Transition, Lung Neoplasms, Mice, Nude, Antineoplastic Agents, Apoptosis, Gefitinib, General Medicine, Proto-Oncogene Proteins c-met, General Biochemistry, Genetics and Molecular Biology, Article, ErbB Receptors, Gene Expression Regulation, Neoplastic, Mice, MicroRNAs, Cell Transformation, Neoplastic, Drug Resistance, Neoplasm, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Quinazolines, Animals, Humans, Cell Proliferation, Signal Transduction

Abstract

The involvement of the MET oncogene in de novo and acquired resistance of non-small cell lung cancers (NSCLCs) to tyrosine kinase inhibitors (TKIs) has previously been reported, but the precise mechanism by which MET overexpression contributes to TKI-resistant NSCLC remains unclear. MicroRNAs (miRNAs) negatively regulate gene expression, and their dysregulation has been implicated in tumorigenesis. To understand their role in TKI-resistant NSCLCs, we examined changes in miRNA that are mediated by tyrosine kinase receptors. Here we report that miR-30b, miR-30c, miR-221 and miR-222 are modulated by both epidermal growth factor (EGF) and MET receptors, whereas miR-103 and miR-203 are controlled only by MET. We showed that these miRNAs have important roles in gefitinib-induced apoptosis and epithelial-mesenchymal transition of NSCLC cells in vitro and in vivo by inhibiting the expression of the genes encoding BCL2-like 11 (BIM), apoptotic peptidase activating factor 1 (APAF-1), protein kinase C ɛ (PKC-ɛ) and sarcoma viral oncogene homolog (SRC). These findings suggest that modulation of specific miRNAs may provide a therapeutic approach for the treatment of NSCLCs.

Published

2022

155. Retraction Notice to: Downregulation of p53-inducible microRNAs 192, 194, and 215 Impairs the p53/MDM2 Autoregulatory Loop in Multiple Myeloma Development

Author

Flavia Pichiorri, Sung-Suk Suh, Alberto Rocci, Luciana De Luca, Cristian Taccioli, Ramasamy Santhanam, Wenchao Zhou, Don M. Benson, Craig Hofmainster, Hansjuerg Alder, Michela Garofalo, Gianpiero Di Leva, Stefano Volinia, Huey-Jen Lin, Danilo Perrotti, Michael Kuehl, Rami I. Aqeilan, Antonio Palumbo, and Carlo M. Croce

Subjects

Cancer Research, Down-Regulation, Models, Biological, Article, Receptor, IGF Type 1, Mice, Cell Movement, Cell Line, Tumor, Animals, Homeostasis, Humans, Neoplasm Invasiveness, RNA, Messenger, Insulin-Like Growth Factor I, Promoter Regions, Genetic, Cell Proliferation, Chromosomes, Human, Pair 11, Cell Cycle, Proto-Oncogene Proteins c-mdm2, DNA Methylation, Gene Expression Regulation, Neoplastic, MicroRNAs, Oncology, Tumor Suppressor Protein p53, Multiple Myeloma, Precancerous Conditions, Mutagens

Abstract

In multiple myeloma (MM), an incurable B cell neoplasm, mutation or deletion of p53 is rarely detected at diagnosis. Using small-molecule inhibitors of MDM2, we provide evidence that miR-192, 194, and 215, which are downregulated in a subset of newly diagnosed MMs, can be transcriptionally activated by p53 and then modulate MDM2 expression. Furthermore, ectopic re-expression of these miRNAs in MM cells increases the therapeutic action of MDM2 inhibitors in vitro and in vivo by enhancing their p53-activating effects. In addition, miR-192 and 215 target the IGF pathway, preventing enhanced migration of plasma cells into bone marrow. The results suggest that these miRNAs are positive regulators of p53 and that their downregulation plays a key role in MM development.

Published

2022

156. Pan-cancer analysis of canonical and modified miRNAs enhances the resolution of the functional miRNAome in cancer

Author

Rosario Distefano, Luisa Tomasello, Gian Luca Rampioni Vinciguerra, Pierluigi Gasparini, Yujia Xiang, Marina Bagnoli, Gioacchino P. Marceca, Paolo Fadda, Alessandro Laganà, Mario Acunzo, Qin Ma, Giovanni Nigita, and Carlo M. Croce

Subjects

Adult, Cancer Research, MicroRNAs, Adenosine, Oncology, Neoplasms, Biomarkers, Tumor, Humans, Child, Article, Inosine

Abstract

Epitranscriptomic studies of miRNAs have added a new layer of complexity to the cancer field. Although there is fast-growing interest in adenosine-to-inosine (A-to-I) miRNA editing and alternative cleavage that shifts miRNA isoforms, simultaneous evaluation of both modifications in cancer is still missing. Here, we concurrently profiled multiple miRNA modification types, including A-to-I miRNA editing and shifted miRNA isoforms, in >13,000 adult and pediatric tumor samples across 38 distinct cancer cohorts from The Cancer Genome Atlas and The Therapeutically Applicable Research to Generate Effective Treatments data sets. The differences between canonical miRNAs and the wider miRNAome in terms of expression, clustering, dysregulation, and prognostic standpoint were investigated. The combination of canonical miRNAs and modified miRNAs boosted the quality of clustering results, outlining unique clinicopathologic features among cohorts. Certain modified miRNAs showed opposite expression from their canonical counterparts in cancer, potentially impacting their targets and function. Finally, a shifted and edited miRNA isoform was experimentally validated to directly bind and suppress a unique target. These findings outline the importance of going beyond the well-established paradigm of one mature miRNA per miRNA arm to elucidate novel mechanisms related to cancer progression. Significance: Modified miRNAs may act as cancer biomarkers and function as allies or antagonists of their canonical counterparts in gene regulation, suggesting the concurrent consideration of canonical and modified miRNAs can boost patient stratification.

Published

2022

157. Transcriptome Analysis of Human Endogenous Retroviruses at Locus-Specific Resolution in Non-Small Cell Lung Cancer

Author

Alessandro La Ferlita, Rosario Distefano, Salvatore Alaimo, Joal D. Beane, Alfredo Ferro, Carlo M. Croce, Philip N. Tsichlis, Alfredo Pulvirenti, and Giovanni Nigita

Subjects

Cancer Research, Oncology, human endogenous retroviruses, HERVs, lung cancer, lung adenocarcinoma, lung squamous cell carcinoma, biomarkers, RNA-seq, transcriptome analysis

Abstract

Lung cancer is the second most commonly diagnosed cancer and the leading cause of cancer deaths worldwide. Among its subtypes, lung adenocarcinoma (LUAD) and lung squamous cell carcinoma (LUSC) are the most common, accounting for more than 85% of lung cancer diagnoses. Despite the incredible efforts and recent advances in lung cancer treatments, patients affected by this condition still have a poor prognosis. Therefore, novel diagnostic biomarkers are needed. Recently, a class of transposable elements called human endogenous retroviruses (HERVs) has been found to be implicated in cancer development and later employed as novel biomarkers for several tumor types. In this study, we first ever characterized the expression of HERVs at genomic locus-specific resolution in both LUAD and LUSC cohorts available in The Cancer Genome Atlas (TCGA). Precisely, (i) we profiled the expression of HERVs in TCGA-LUAD and TCGA-LUSC cohorts; (ii) we identified the dysregulated HERVs in both lung cancer subtypes; (iii) we evaluated the impact of the dysregulated HERVs on signaling pathways using neural network-based predictions; and (iv) we assessed their association with overall survival (OS) and relapse-free survival (RFS). In conclusion, we believe this study may help elucidate another layer of dysregulation that occurs in lung cancer involving HERVs, paving the way for identifying novel lung cancer biomarkers.

Published

2022

158. MIR21-induced loss of junctional adhesion molecule A promotes activation of oncogenic pathways, progression and metastasis in colorectal cancer

Author

Joanne Edwards, Somaieh Hedayat, Claudio Murgia, Owen J. Sansom, Gabriela Kramer-Marek, Luciano Cascione, Elisa Fontana, Pierluigi Gasparini, Jens C. Hahne, Carlo M. Croce, Matteo Fassan, Carlos D. Martins, Andrea Lampis, Paul G. Horgan, Georgios Vlachogiannis, L. Terracciano, Chiara Braconi, and Nicola Valeri

Subjects

0301 basic medicine, education, Biology, medicine.disease_cause, Article, Metastasis, 03 medical and health sciences, Prognostic markers, 0302 clinical medicine, Downregulation and upregulation, medicine, Cancer genomics, Gene silencing, Tumour-suppressor proteins, Molecular Biology, Protein kinase B, fungi, Cancer, Cell Biology, medicine.disease, humanities, Bone morphogenetic protein 7, MicroRNAs, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, cardiovascular system, Carcinogenesis, Cell Adhesion Molecules, Junctional Adhesion Molecule A

Abstract

Junctional adhesion molecules (JAMs) play a critical role in cell permeability, polarity and migration. JAM-A, a key protein of the JAM family, is altered in a number of conditions including cancer; however, consequences of JAM-A dysregulation on carcinogenesis appear to be tissue dependent and organ dependent with significant implications for the use of JAM-A as a biomarker or therapeutic target. Here, we test the expression and prognostic role of JAM-A downregulation in primary and metastatic colorectal cancer (CRC) (n = 947). We show that JAM-A downregulation is observed in ~60% of CRC and correlates with poor outcome in four cohorts of stages II and III CRC (n = 1098). Using JAM-A knockdown, re-expression and rescue experiments in cell line monolayers, 3D spheroids, patient-derived organoids and xenotransplants, we demonstrate that JAM-A silencing promotes proliferation and migration in 2D and 3D cell models and increases tumour volume and metastases in vivo. Using gene-expression and proteomic analyses, we show that JAM-A downregulation results in the activation of ERK, AKT and ROCK pathways and leads to decreased bone morphogenetic protein 7 expression. We identify MIR21 upregulation as the cause of JAM-A downregulation and show that JAM-A rescue mitigates the effects of MIR21 overexpression on cancer phenotype. Our results identify a novel molecular loop involving MIR21 dysregulation, JAM-A silencing and activation of multiple oncogenic pathways in promoting invasiveness and metastasis in CRC.

Published

2021

159. Predicting ROR1/BCL2 combination targeted therapy of small cell carcinoma of the lung

Author

Walter Wang, Johan Schultz, David P. Carbone, Mohammad Hojjat-Farsangi, Håkan Mellstedt, Joseph M. Amann, Alyssa Shulman, Konstantin Shilo, and Carlo M. Croce

Subjects

Cancer Research, Lung Neoplasms, medicine.medical_treatment, Immunology, Receptor Tyrosine Kinase-like Orphan Receptors, Small-cell carcinoma, Article, Small-cell lung cancer, Targeted therapy, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Targeted therapies, Cell Line, Tumor, microRNA, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Molecular Targeted Therapy, Receptor, Cancer genetics, Protein Kinase Inhibitors, neoplasms, Sulfonamides, Tissue microarray, QH573-671, business.industry, Venetoclax, Cancer, Drug Synergism, Cell Biology, medicine.disease, Bridged Bicyclo Compounds, Heterocyclic, Small Cell Lung Carcinoma, Survival Analysis, respiratory tract diseases, chemistry, Proto-Oncogene Proteins c-bcl-2, ROR1, Cancer research, business, Cytology

Abstract

Small cell lung cancer (SCLC) remains a deadly form of cancer, with a 5-year survival rate of less than 10 percent, necessitating novel therapies. Receptor tyrosine kinase-like orphan receptor 1 (ROR1) is an oncofetal protein that is emerging as a therapeutic target and is co-expressed with BCL2 in multiple tumor types due to microRNA coregulation. We hypothesize that ROR1-targeted therapy is effective in small cell lung cancer and synergizes with therapeutic BCL2 inhibition. Tissue microarrays (TMAs) and formalin-fixed paraffin-embedded (FFPE) SCLC patient samples were utilized to determine the prevalence of ROR1 and BCL2 expression in SCLC. Eight SCLC-derived cell lines were used to determine the antitumor activity of a small molecule ROR1 inhibitor (KAN0441571C) alone and in combination with the BCL2 inhibitor venetoclax. The Chou-Talalay method was utilized to determine synergy with the drug combination. ROR1 and BCL2 protein expression was identified in 93% (52/56) and 86% (48/56) of SCLC patient samples, respectively. Similarly, ROR1 and BCL2 were shown by qRT-PCR to have elevated expression in 79% (22/28) and 100% (28/28) of SCLC patient samples, respectively. KAN0441571C displayed efficacy in 8 SCLC cell lines, with an IC50 of 500 nM or less. Synergy as defined by a combination index of

Published

2021

160. In situ hybridization to detect DNA amplification in extracellular vesicles

Author

Lucia Casadei, Patricia Sarchet, Fernanda Costas C. de Faria, Federica Calore, Giovanni Nigita, Sayumi Tahara, Luciano Cascione, Martin Wabitsch, Francis J. Hornicek, Valerie Grignol, Carlo M. Croce, and Raphael E. Pollock

Subjects

Extracellular Vesicles, Histology, Humans, DNA, Liposarcoma, Cell Biology, In Situ Hybridization

Abstract

EVs have emerged as an important component in tumour initiation, progression and metastasis. Although notable progresses have been made, the detection of EV cargoes remain significantly challenging for researchers to practically use; faster and more convenient methods are required to validate the EV cargoes, especially as biomarkers. Here we show, the possibility of examining embedded EVs as substrates to be used for detecting DNA amplification through ultrasensitive in situ hybridization (ISH). This methodology allows the visualization of DNA targets in a more direct manner, without time consuming optimization steps or particular expertise. Additionally, formalin-fixed paraffin-embedded (FFPE) blocks of EVs allows long-term preservation of samples, permitting future studies. We report here: (i) the successful isolation of EVs from liposarcoma tissues; (ii) the EV embedding in FFPE blocks (iii) the successful selective, specific ultrasensitive ISH examination of EVs derived from tissues, cell line, and sera; (iv) and the detection of MDM2 DNA amplification in EVs from liposarcoma tissues, cell lines and sera. Ultrasensitive ISH on EVs would enable cargo study while the application of ISH to serum EVs, could represent a possible novel methodology for diagnostic confirmation. Modification of probes may enable researchers to detect targets and specific DNA alterations directly in tumour EVs, thereby facilitating detection, diagnosis, and improved understanding of tumour biology relevant to many cancer types.

Published

2022

161. A concurrent canonical and modified miRNAome pan-cancer study on TCGA and TARGET cohorts leads to an enhanced resolution in cancer

Author

Rosario Distefano, Giovanni Nigita, and Carlo M. Croce

Subjects

miRNA isoforms, non-coding RNA, Epitranscriptomics, Cancer

Abstract

The repository provides the rawread counts expression data (miRNA-Seq and RNA-Seq) and the source code developed for each analysis performedin this study.

Published

2022

162. tRNA-derived fragments (tRFs) in cancer

Author

Yuri Pekarsky, Veronica Balatti, and Carlo M. Croce

Subjects

Cell Biology, Review, Molecular Biology, Biochemistry

Abstract

tRNA fragments (tRNA derived fragments or tRFs) are small single stranded RNA molecules derived from pre-tRNAs and mature tRNAs. tRFs have been known for a number of years, but previously they were believed to be not important products of tRNA degradation. tRFs can be unique, like tRF-1 s, or redundant, like tRF-3 s and tRF-5 s. Scientific interest in tRFs has drastically increased in the last 5 years. Many studies have found that tRFs are differentially expressed in many normal cellular processes as well as in transformed cancer cells. Dysregulation of tRFs expression have been reported in multiple major types of cancer including solid cancers and lymphoid malignancies. However the exact molecular role of these molecules is not entirely clear. A number of studies proposed that tRFs can work as microRNAs by targeting gene expression. Here we discuss recent studies showing differential expression of tRFs in many cancers as well as what is currently known about tRFs biological functions in cancer cells. GRAPHICAL ABSTRACT: [Image: see text]

Published

2022

163. Renato Baserga, MD: In Memoriam (1925–2023)

Author

Gary S. Stein and Carlo M. Croce

Subjects

Cancer Research, Oncology

Published

2023

164. Abstract 4823: The novel miR-15a/Fra-2/IGF1R axis drives response to starvation-induced cell stress in pancreatic ductal adenocarcinoma

Author

Gian Luca Rampioni Vinciguerra, Marina Capece, Luca Reggiani Bonetti, Paolo Magistri, Federica Calore, Giovanni Nigita, Rosario Distefano, Roberto Ballarin, Fabrizio Di Benedetto, Andrea Vecchione, Barbara Belletti, Gustavo Baldassarre, Francesca Lovat, and Carlo M. Croce

Subjects

Cancer Research, Oncology

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a relatively uncommon malignancy; however, its incidence is rising worldwide, and it is expected to become the second-leading cause of cancer-related death by 2030. From a histological point of view, PDAC is characterized by a prominent desmoplastic reaction that compresses blood vessels, limiting oxygen and nutrient availability in the tumor microenvironment. Despite that, PDAC cells are capable to adapt dynamically to these stress conditions, adopting different strategies that includes the strict regulation of the autophagic flux. Thus, studying these adaptive mechanisms is crucial to understand PDAC progression and to establish new therapeutic modalities to tackle it. Here, we explore the role of the tumor suppressor miR-15a in the regulation of its putative target Fra-2, a transcription factor, commonly activated by cell stress. By employing IPA on PDAC tumors from TCGA dataset, we found that both miR-15a and its target Fra-2 are predicted to regulate the IGF-1 signaling pathway. In an independent cohort of 44 PDAC samples, miR-15a levels inversely correlated with both Fra-2 and IGF1R expression; conversely, Fra-2 significantly correlated with IGF1R. By chromatin immunoprecipitation and luciferase assay, we assessed that miR-15a directly targeted Fra-2 and IGF1R that, in turn, is transcriptionally regulated by Fra-2 activity. Then, we investigated the role of miR-15a/Fra-2 regulation of IGF1R in the response to starvation-induced cell stress. In starved PDAC cell lines, Fra-2 transcriptional activity triggered IGF1R promoter, causing IGF1R overexpression in control cells but not in miR-15a-overexpressing cells. Consistently, the IGF1 release after starvation induced phosphorylation of IGF1R and activation of the downstream mTOR pathway in control cells but not in miR-15a-overexpressing cells. Therefore, TEM and western blot analysis demonstrated that activation of mTOR via IGF1 release reduced the autophagic flux of PDAC control cell lines compared to miR-15a overexpressing cells under starvation. To assess our results in vivo, we injected PDAC cells wild type or Fra-2 knockout into the flank of nude mice. At tumor onset, mice were randomly divided in two groups and fed with control or hypoproteic diet for three weeks. Hypoproteic diet did not interfere with the growth of wild-type tumors, by contrast, significantly impaired Fra-2KO tumors growth rate. Tumor analysis revealed that hypoproteic diet potently induced IGF1R overexpression and mTOR pathway activation in wild-type tumors but not in Fra-2KO tumors. Our findings demonstrate that IGF1R expression is regulated by miR-15a directly and indirectly via Fra-2 in PDAC. This novel miR-15a/Fra-2/IGF1R axis, triggered by starvation, regulates the autophagic flux and growth of PDAC cells in stress condition, and could be targeted by specific small inhibitors. Citation Format: Gian Luca Rampioni Vinciguerra, Marina Capece, Luca Reggiani Bonetti, Paolo Magistri, Federica Calore, Giovanni Nigita, Rosario Distefano, Roberto Ballarin, Fabrizio Di Benedetto, Andrea Vecchione, Barbara Belletti, Gustavo Baldassarre, Francesca Lovat, Carlo M. Croce. The novel miR-15a/Fra-2/IGF1R axis drives response to starvation-induced cell stress in pancreatic ductal adenocarcinoma. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 4823.

Published

2023

165. Abstract 3903: Role of the miR-301a/Fra-2/GLIPR1 axis in lung cancer cisplatin resistance

Author

Francesca Lovat, Gian Luca Rampioni Vinciguerra, Marina Capece, Rosario Distefano, Giovanni Nigita, Andrea Vecchione, and Carlo M. Croce

Subjects

Cancer Research, Oncology

Abstract

Lung cancer is the leading cause of cancer-related mortality in both men and women worldwide. Despite the administration of platinum compounds represents the main treatment, the majority of tumors remains intrinsically resistant. In lung cancer, miR-301a exerts a main role by modulating the activity of transcription factors like NF-kB and Stat3. Here, we dissected the contribution of miR-301a in the regulation of its new identified target Fos-related antigen-2 (Fra-2), a transcription factor that belongs to the Fos/AP-1 family. By microarray analysis, we discovered that Fra-2 overexpression increased glioma pathogenesis-related protein 1 (GLIPR1) levels, a mediator of cisplatin resistance in lung cancer. Its mechanism of regulation is still unclear. We demonstrated that GLIPR1 is also a miR-301a target. In vitro, modulation of miR-301a reduced Fra-2 and GLIPR1 levels; conversely, Fra-2 overexpression significantly increased GLIPR1 and miR-301a. Then, by chromatin immunoprecipitation assay, we confirmed that Fra-2 interacts with the promoter regions of both GLIPR1 and MIR301A genes, supporting that miR-301a/Fra-2/GLIPR1 axis could be autoregulated by feedback loop in which Fra-2 promotes the transcription of MIR301A gene. Investigating the effect of this new axis on the response to cisplatin, we observed that both Fra-2/GLIPR1 overexpression and miR-301a silencing induced cisplatin resistance in lung cancer cells. By contrast, silencing of GLIPR1 and combined administration of low doses of Fos/AP-1 inhibitor restored the cisplatin sensitivity in Fra-2 overexpressing cells. In the lung adenocarcinoma samples from the TCGA dataset, miR-301a overexpression inversely correlated with Fra-2 and GLIPR1 expression. Consistently, the overexpression of miR-301a identified a fraction of tumors with low expression of Fra-2 and GLIPR1 in an internal cohort of lung cancer samples. Altogether, our findings identify the miR-301a/Fra-2/GLIPR1 axis that contributes to cisplatin resistance in lung cancer cells and could serve as biomarker to stratify patients who may benefit from cisplatin administration, alone or in combination with Fos/AP-1 inhibitors. Citation Format: Francesca Lovat, Gian Luca Rampioni Vinciguerra, Marina Capece, Rosario Distefano, Giovanni Nigita, Andrea Vecchione, Carlo M. Croce. Role of the miR-301a/Fra-2/GLIPR1 axis in lung cancer cisplatin resistance. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 3903.

Published

2023

166. Deletion of Micro RNA-15/16 Clusters Promotes Leukemic Initiation in AML Via the Deregulation of Hematopoietic Progenitors

Author

Anita Ng, Yuhong Ma, Yuri Pekarsky, Francesca Lovat, Frank Di Caro, Esha Sharma, Lita Crichton, Britta Will, Carlo M. Croce, and Nicholas Chiorazzi

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

167. Endogenous and artificial miRNAs explore a rich variety of conformations: a potential relationship between secondary structure and biological functionality

Author

Alfredo Ferro, Giorgia Oliviero, Danilo Milardi, Nicola Borbone, Alessandro D'Urso, Alfredo Pulvirenti, Gennaro Piccialli, Chiara M. A. Gangemi, Sara García-Viñuales, Carlo M. Croce, Andrea Patrizia Falanga, Maria Elena Fragalà, Roberto Purrello, Salvatore Alaimo, Gangemi, C. M. A., Alaimo, S., Pulvirenti, A., Garcia-Vinuales, S., Milardi, D., Falanga, A. P., Fragala, M. E., Oliviero, G., Piccialli, G., Borbone, N., Ferro, A., D'Urso, A., Croce, C. M., and Purrello, R.

Subjects

0301 basic medicine, Micro RNA, Cell, lcsh:Medicine, Endogeny, Computational biology, Biology, Calorimetry, Article, 03 medical and health sciences, 0302 clinical medicine, microRNA, medicine, Gene Silencing, lcsh:Science, Gene, Protein secondary structure, Regulation of gene expression, Multidisciplinary, Base Sequence, Sequence Analysis, RNA, lcsh:R, Base Sequence, ErbB Receptors, Gene Silencing, MicroRNAs, Nucleic Acid Conformation, Proto-Oncogene Proteins c-met, Sequence Analysis, RNA, RNA, Biological activity, Proto-Oncogene Proteins c-met, ErbB Receptors, MicroRNAs, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Nucleic Acid Conformation, lcsh:Q, Sequence Analysis

Abstract

Mature microRNAs are short non-coding RNA sequences which upon incorporation into the RISC ribonucleoprotein complex, play a crucial role in regulation of gene expression. However, miRNAs can exist within the cell also as free molecules fulfilling their biological activity. Therefore, it is emerging that in addition to sequence even the structure adopted by mature miRNAs might play an important role to reach the target. Indeed, we analysed by several spectroscopic techniques the secondary structures of two artificial miRNAs selected by computational tool (miR-Synth) as best candidates to silence c-MET and EGFR genes and of two endogenous miRNAs (miR-15a and miR-15b) having the same seed region, but different biological activity. Our results demonstrate that both endogenous and artificial miRNAs can arrange in several 3D-structures which affect their activity and selectivity toward the targets.

Published

2020

168. A large fraction of trisomy 12, 17p − , and 11q − CLL cases carry unidentified microdeletions of miR-15a/16-1

Author

Felice Pepe, Laura Z. Rassenti, Yuri Pekarsky, Jadwiga Labanowska, Tatsuya Nakamura, Giovanni Nigita, Thomas J. Kipps, Veronica Balatti, and Carlo M. Croce

Subjects

Medical Sciences, DNA Copy Number Variations, Trisomy, Chromosomes, Fluorescence, Rare Diseases, trisomy 12, miR-15a/16-1, hemic and lymphatic diseases, Pair 12, Humans, Genetic Predisposition to Disease, Pair 11, Chronic, In Situ Hybridization, Genetic Association Studies, In Situ Hybridization, Fluorescence, Cancer, Leukemia, Chromosomes, Human, Pair 12, Multidisciplinary, Pair 17, Chromosomes, Human, Pair 11, B-Cell, Hematology, Biological Sciences, Leukemia, Lymphocytic, Chronic, B-Cell, Lymphocytic, MicroRNAs, Chromosome Deletion, CLL, Human, 13q deletion, Chromosomes, Human, Pair 17

Abstract

Significance 13q14.3 deletion is the most common genetic lesion identified in CLLs. This study shows that microdeletions affecting the miR-15a/16-1 cluster are more frequent than expected in all CLL cohorts and are prevalent in patients carrying a trisomy 12. Copy-number variation analysis and an experimental FISH analysis revealed that ∼34% of samples carry previously unidentified microdeletions of miR-15a/16-1. These data may have clinical relevance for the successful stratification of patients for treatment., Chronic lymphocytic leukemia (CLL) is the most common adult leukemia and is characterized by chromosomal aberrations including 13q, 11q, and 17p deletions and a trisomy of chromosome 12 (T12). 13q deletions are often associated with 11q and 17p deletions in aggressive cases. Conversely, T12 CLLs show a variable prognosis, and association with 13q deletions is uncommon. The miR-15a/16-1 cluster is the functional target of 13q deletions, leading to BCL2 overexpression. Chromosomal aberrations in CLL are associated with prognosis, and their identification is carried out by fluorescence in situ hybridization (FISH). Since standard FISH only detects large deletions, we investigated the presence of undetected microdeletions targeting miR-15a/16-1 in CLL cases. We found that ∼34% of CLL samples show an unreported loss of the miR-15a/16-1 locus regardless of their cytogenetic profile. Interestingly, 15 out of 39 (∼39%) of all CLLs with T12, carry microdeletions of miR-15a/16-1, indicating that, in patients with T12, miR-15a/16-1 are mostly inactivated by microdeletions. In addition, ∼40% of CLL cases bearing T12, 17p−, and 11q− showed unidentified microdeletions of miR-15a/16-1, suggesting that miR-15a/16-1 loss cooperates with such chromosomal alterations in CLL. These data may have clinical relevance for the successful stratification of patients for treatment.

Published

2022

169. Pathophysiology roles and translational opportunities of miRNAs in acute leukemias

Author

Francesca Lovat and Carlo M. Croce

Published

2022

170. miR-15/16 in human malignancies

Author

Yuri Pekarsky and Carlo M. Croce

Published

2022

171. Contributors

Author

Samuel Akanksha, Alessandra Allione, Juan Carlos Álvarez-Perez, Alvaro Andrades, Alberto M. Arenas, Carlos Baliñas-Gavira, Dominik A. Barth, Anna Bielowski, Roopa Biswas, Mattia Boeri, Elisabetta Broseghini, George A. Calin, Enrica Calura, Elisabetta Casalone, Vera Constâncio, Giulia Cosentino, Marina C. Costa, Carlo M. Croce, Marta Cuadros, Christine E. Cutucache, Ben Davidson, Emi Dika, Sayra Dilmac, Mihnea P. Dragomir, Rares Drula, Francisco J. Enguita, Zhaohui Feng, Manuela Ferracin, Francesca Fornari, Orazio Fortunato, André F. Gabriel, Daniel J. García, Laura Gramantieri, Rui Henrique, Wenwei Hu, Marilena V. Iorio, Carmen Jerónimo, Sakshi Kamboj, Manoj Kumar, Charles Henderson Lawrie, Ana Lúcia Leitão, Juan Liu, Francesca Lovat, Laura Masatti, Giuseppe Matullo, Pedro P. Medina, Swati Mohapatra, Vlad Moisoiu, Massimo Negrini, Vu Hong Loan Nguyen, Jacob Anderson O’Brien, Bulent Ozpolat, Barbara Pardini, Juan Rodrigo Patiño-Mercau, Laura Pazzaglia, Paola Peinado, Yuri Pekarsky, Chun Peng, George E.D. Petrescu, Martin Pichler, Ilaria Plantamura, Reuven Reich, Maria Isabel Rodriguez, Chiara Romualdi, Juan Sanjuan-Hidalgo, Katia Scotlandi, Ram C. Shankaraiah, Ondrej Slaby, Carla Solé, Dharmendra Kumar Soni, Gabriella Sozzi, Anamika Thakur, Angelo Veronese, Rosa Visone, Petra Vychytilova-Faltejskova, and Cen Zhang

Published

2022

172. Correction to: Overexpression of the HMGA2 gene in transgenic mice leads to the onset of pituitary adenomas

Author

Monica Fedele, Sabrina Battista, Lawrence Kenyon, Gustavo Baldassarre, Vincenzo Fidanza, Andres J. P. Klein-Szanto, A. F. Parlow, Rosa Visone, Giovanna M. Pierantoni, Eric Outwater, Massimo Santoro, Carlo M. Croce, and Alfredo Fusco

Subjects

Cancer Research, Genetics, Molecular Biology

Published

2022

173. Small Non-Coding RNAs in Leukemia

Author

Veronica Balatti and Carlo M. Croce

Subjects

Cancer Research, Oncology, microRNA, small non-coding RNAs, leukemia, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, miRNA, tRNA fragments

Abstract

In 2020, more than 60,500 people were diagnosed with leukemia in the USA, and more than 23,000 died. The incidence of leukemia is still rising, and drug resistance development is a serious concern for patients’ wellbeing and survival. In the past two decades, small non-coding RNAs have been studied to evaluate their functions and possible role in cancer pathogenesis. Small non-coding RNAs are short RNA molecules involved in several cellular processes by regulating the expression of genes. An increasing body of evidence collected by many independent studies shows that the expression of these molecules is tissue specific, and that their dysregulation alters the expression of genes involved in tumor development, progression and drug response. Indeed, small non-coding RNAs play a pivotal role in the onset, staging, relapse and drug response of hematological malignancies and cancers in general. These findings strongly suggest that small non-coding RNAs could function as biomarkers and possible targets for therapy. Thus, in this review, we summarize the regulatory mechanisms of small non-coding RNA expression in different types of leukemia and assess their potential clinical implications.

Published

2021

174. Newly-Discovered Neural Features Expand the Pathobiological Knowledge of Blastic Plasmacytoid Dendritic Cell Neoplasm

Author

Lorenzo Cerroni, Federica Melle, Marcello Del Corvo, Marco Paulli, Emilio Berti, Jessica Consiglio, Gaetano Ivan Dellino, Giovanna Motta, Stefano Pileri, Carlo M. Croce, Vincenzo Mazzara, Stefano Fiori, Fabio Fuligni, Giuseppe Benvenuto, Alessandro Pileri, Fabio Facchetti, Claudio Tripodo, Daniele Fanoni, Maria Rosaria Sapienza, Manuela Ferracin, Elena Sabattini, Valentina Tabanelli, Saveria Mazzara, Beatrice Belmonte, Sapienza M.R., Benvenuto G., Ferracin M., Mazzara S., Fuligni F., Tripodo C., Belmonte B., Fanoni D., Melle F., Motta G., Tabanelli V., Consiglio J., Mazzara V., Corvo M.D., Fiori S., Pileri A., Dellino G.I., Cerroni L., Facchetti F., Berti E., Sabattini E., Paulli M., Croce C.M., and Pileri S.A.

Subjects

Cancer Research, Neurogenesis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, MicroRNA Expression Profile, sequencing, Biology, Settore MED/08 - Anatomia Patologica, BPDCN, MiRNA, Network, Neurogenesis, Sequencing, BPDCN, Article, Chromatin, Gene expression profiling, MiRNA, Network, Sequencing, neurogenesis, Oncology, Downregulation and upregulation, microRNA, network, Cancer research, Immunohistochemistry, Settore MED/05 - Patologia Clinica, Neurogenesi, RC254-282, Progenitor, miRNA

Abstract

Simple Summary For the first time, neuronal features are described in blastic plasmacytoid dendritic cell neoplasm (BPDCN) by a complex array of molecular techniques, including microRNA and gene expression profiling, RNA and Chromatin immunoprecipitation sequencing, and immunohistochemistry. The discovery of unexpected neural features in BPDCN may change our vision of this disease, leading to the designing of a new BPDCN cell model and to re-thinking the relations occurring between BPDCN and nervous system. The observed findings contribute to explaining the extreme tumor aggressiveness and also to propose novel therapeutic targets. In view of this, the identification, in this work of new potential neural metastatic inducers might open the way to therapeutic approaches for BPDCN patients based on the use of anti-neurogenic agents. Abstract Blastic plasmacytoid dendritic cell neoplasm (BPDCN) is a rare and highly aggressive hematologic malignancy originating from plasmacytoid dendritic cells (pDCs). The microRNA expression profile of BPDCN was compared to that of normal pDCs and the impact of miRNA dysregulation on the BPDCN transcriptional program was assessed. MiRNA and gene expression profiling data were integrated to obtain the BPDCN miRNA-regulatory network. The biological process mainly dysregulated by this network was predicted to be neurogenesis, a phenomenon raising growing interest in solid tumors. Neurogenesis was explored in BPDCN by querying different molecular sources (RNA sequencing, Chromatin immunoprecipitation-sequencing, and immunohistochemistry). It was shown that BPDCN cells upregulated neural mitogen genes possibly critical for tumor dissemination, expressed neuronal progenitor markers involved in cell migration, exchanged acetylcholine neurotransmitter, and overexpressed multiple neural receptors that may stimulate tumor proliferation, migration and cross-talk with the nervous system. Most neural genes upregulated in BPDCN are currently investigated as therapeutic targets.

Published

2021

175. MiREDiBase, a manually curated database of validated and putative editing events in microRNAs

Author

Francesco Russo, Marina Bagnoli, Alessandro Laganà, Giovanni Nigita, Qin Ma, Rosario Distefano, Giulia Romano, Gioacchino P. Marceca, Federica Calore, Pierluigi Gasparini, Mario Acunzo, Carlo M. Croce, Luisa Tomasello, and Alfredo Ferro

Subjects

Statistics and Probability, Pan troglodytes, Science, Computational biology, Biology, Library and Information Sciences, Article, Education, Databases, microRNA, Animals, Humans, Minimum free energy, Gorilla gorilla, Extramural, Nucleic acid sequence, Macaca mulatta, Computer Science Applications, MicroRNAs, RNA editing, miRNAs, RNA Editing, Statistics, Probability and Uncertainty, Databases, Nucleic Acid, Biogenesis, Function (biology), Information Systems

Abstract

MicroRNAs (miRNAs) are regulatory small non-coding RNAs that function as translational repressors. MiRNAs are involved in most cellular processes, and their expression and function are presided by several factors. Amongst, miRNA editing is an epitranscriptional modification that alters the original nucleotide sequence of selected miRNAs, possibly influencing their biogenesis and target-binding ability. A-to-I and C-to-U RNA editing are recognized as the canonical types, with the A-to-I type being the predominant one. Albeit some bioinformatics resources have been implemented to collect RNA editing data, it still lacks a comprehensive resource explicitly dedicated to miRNA editing. Here, we present MiREDiBase, a manually curated catalog of editing events in miRNAs. The current version includes 3,059 unique validated and putative editing sites from 626 pre-miRNAs in humans and three primates. Editing events in mature human miRNAs are supplied with miRNA-target predictions and enrichment analysis, while minimum free energy structures are inferred for edited pre-miRNAs. MiREDiBase represents a valuable tool for cell biology and biomedical research and will be continuously updated and expanded at https://ncrnaome.osumc.edu/miredibase.

Published

2021

176. The MicroRNA Family Gets Wider: The IsomiRs Classification and Role

Author

Luisa Tomasello, Rosario Distefano, Carlo M. Croce, and Giovanni Nigita

Subjects

Gene isoform, variants, microRNA, QH301-705.5, Cellular differentiation, RNA, Cell Biology, Computational biology, Review, microRNA biogenesis, Biology, MicroRNA biogenesis, Cell and Developmental Biology, isomiRs, Epitranscriptomics, novel microRNA in cancer, Biology (General), Biogenesis, Developmental Biology, Epigenomics

Abstract

MicroRNAs (miRNAs or miRs) are the most characterized class of non-coding RNAs and are engaged in many cellular processes, including cell differentiation, development, and homeostasis. MicroRNA dysregulation was observed in several diseases, cancer included. Epitranscriptomics is a branch of epigenomics that embraces all RNA modifications occurring after DNA transcription and RNA synthesis and involving coding and non-coding RNAs. The development of new high-throughput technologies, especially deep RNA sequencing, has facilitated the discovery of miRNA isoforms (named isomiRs) resulting from RNA modifications mediated by enzymes, such as deaminases and exonucleases, and differing from the canonical ones in length, sequence, or both. In this review, we summarize the distinct classes of isomiRs, their regulation and biogenesis, and the active role of these newly discovered molecules in cancer and other diseases.

Published

2021

177. A negative feedback regulatory loop between miR-138 and TP53 is mediated by USP10

Author

Zhenghua Luo, Tae Jin Lee, Ri Cui, Taewan Kim, Yong Peng, Esmerina Tili, Manchao Zhang, and Carlo M. Croce

Subjects

0301 basic medicine, endocrine system diseases, miR-138, law.invention, 03 medical and health sciences, 0302 clinical medicine, Ubiquitin, stomatognathic system, law, Negative feedback, microRNA, TP53, Gene, Psychological repression, neoplasms, biology, USP10, Cell biology, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, Suppressor, Function (biology), Priority Research Paper

Abstract

TP53 is a critical tumor suppressor. In approximately 50% of human cancers the TP53 gene is either lost or mutated. The expression level of TP53 in the cells is tightly controlled by a fine-tune machinery, mainly through the Mdm2-mediated ubiquitination pathway. On the other side, the ubiquitinated TP53 could be reversed and stabilized by USP7 and USP10, to keep the amount of TP53 in check. MicroRNAs can negatively regulate TP53 expression levels through direct targeting or positively regulate TP53 function through the repression of negative regulators of TP53. Here we report that microRNA-138 controls TP53 expression by directly targeting USP10. Furthermore, TP53 represses microRNA-138 expression, forming a negative feedback regulatory loop. This finding adds another layer of complexity to the TP53 network.

Published

2019

178. MDM2 Derived from Dedifferentiated Liposarcoma Extracellular Vesicles Induces MMP2 Production from Preadipocytes

Author

Gonzalo Lopez, Abeba Zewdu, Dina Lev, Ameya Deshmukh, Danielle Braggio, Federica Calore, Paolo Fadda, Carlo M. Croce, Martin Wabitsch, Jennifer L. Leight, Lucia Casadei, Raphael E. Pollock, Chi Song, and Valerie P. Grignol

Subjects

0301 basic medicine, Cancer Research, Tumor microenvironment, MMP2, biology, Chemistry, Cancer, Matrix metalloproteinase, medicine.disease, Article, Microvesicles, Metastasis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, Cell culture, 030220 oncology & carcinogenesis, medicine, biology.protein, Cancer research, Mdm2, neoplasms

Abstract

Dedifferentiated liposarcoma (DDLPS) is frequently diagnosed late, and patients typically respond poorly to treatments. DDLPS is molecularly characterized by wild-type p53 and amplification of the MDM2 gene, which results in overexpression of MDM2 protein, a key oncogenic process in DDLPS. In this study, we demonstrate that extracellular vesicles derived from patients with DDLPS or from DDLPS cell lines are carriers of MDM2 DNA that can be transferred to preadipocytes, a major and ubiquitous cellular component of the DDLPS tumor microenvironment, leading to impaired p53 activity in preadipocytes and increased proliferation, migration, and production of matrix metalloproteinase 2; treatment with MDM2 inhibitors repressed these effects. Overall, these findings indicate that MDM2 plays a crucial role in DDLPS by enabling cross-talk between tumor cells and the surrounding microenvironment and that targeting vesicular MDM2 could represent a therapeutic option for treating DDLPS. Significance: Extracellular vesicles derived from dedifferentiated liposarcoma cells induce oncogenic properties in preadipocytes.

Published

2019

179. The combination of TPL2 knockdown and TNFα causes synthetic lethality via caspase-8 activation in human carcinoma cell lines

Author

Elia Aguado-Fraile, Carlo M. Croce, Jatin Roper, Oksana B. Serebrennikova, Keyong Du, Vasiliki Taraslia, Wenying Ren, Maria D. Paraskevopoulou, Philip N. Tsichlis, and Geeta Thapa

Subjects

Gene knockdown, RIPK1, Small interfering RNA, Multidisciplinary, Chemistry, Kinase, Tumor progression, Cancer research, Synthetic lethality, Caspase 8, Protein kinase A

Abstract

Most normal and tumor cells are protected from tumor necrosis factor α (TNFα)-induced apoptosis. Here, we identify the MAP3 kinase tumor progression locus-2 (TPL2) as a player contributing to the protection of a subset of tumor cell lines. The combination of TPL2 knockdown and TNFα gives rise to a synthetic lethality phenotype via receptor-interacting serine/threonine-protein kinase 1 (RIPK1)-dependent and -independent mechanisms. Whereas wild-type TPL2 rescues the phenotype, its kinase-dead mutant does not. Comparison of the molecular events initiated by small interfering RNA for TPL2 (siTPL2) ± TNFα in treatment-sensitive and -resistant lines revealed that the activation of caspase-8, downstream of miR-21-5p and cFLIP, is the dominant TPL2-dependent event. More important, comparison of the gene expression profiles of all of the tested cell lines results in the clustering of sensitive and resistant lines into distinct groups, providing proof of principle for the feasibility of generating a predictive tool for treatment sensitivity.

Published

2019

180. A concurrent canonical and modified miRNAome pan-cancer study on TCGA and TARGET cohorts leads to an enhanced resolution in cancer

Author

Carlo M. Croce, Rosario Distefano, Vinciguerra Glr, Marina Bagnoli, Qin Ma, Luisa Tomasello, Mario Acunzo, Gioacchino P. Marceca, Paolo Fadda, Alessandro Laganà, Yujia Xiang, Giovanni Nigita, and Pierluigi Gasparini

Subjects

Gene isoform, Pan cancer, Cancer genome, microRNA, medicine, Cancer, Computational biology, Biology, medicine.disease

Abstract

MiRNA Epitranscriptomics has placed a new layer of complexity in the cancer field. Despite the fast-growing interest in miRNA editing and shifted miRNA isoforms, a simultaneous study of both modifications in cancer is still missing. Here, we concurrently profiled multiple miRNA modifications, including A-to-I RNA editing and shifted miRNA isoforms, in >13K adult and pediatric tumor samples across 38 distinct cancer cohorts from The Cancer Genome Atlas and The Therapeutically Applicable Research to Generate Effective Treatments datasets. We investigated the differences among canonical miRNAs and the wider miRNAome in terms of expression, clustering, dysregulation, and prognostic standpoint. The combination of canonical miRNAs/miRNA isoforms boosted the quality of clustering results, outlining unique cohorts’ clinical-pathological features. We described modified miRNAs showing opposite dysregulation with respect to their canonical counterparts in cancer, potentially impacting their targetome and function. The abundance of expressed miRNA isoforms directly impacted the activation/deactivation of critical carcinogenesis pathways. Finally, we experimentally validated unique targeting for a shifted and edited miRNA isoform. Our findings outlined once more the importance of going beyond the well-established paradigm of one-mature-miRNA per miRNA arm to elucidate novel mechanisms related to cancer progression.

Published

2021

181. A novel auxin-inducible degron system for rapid, cell cycle-specific targeted proteolysis

Author

Marina Capece, Gian Luca Rampioni Vinciguerra, Carlo M. Croce, Bryan K McElwain, Dario Palmieri, Vincenzo Coppola, Chenyu Lin, Joseph Mills, Anna Tessari, and Wayne O. Miles

Subjects

chemistry.chemical_classification, education.field_of_study, medicine.diagnostic_test, Proteolysis, Cell, Population, Cell cycle, Protein degradation, Cell biology, medicine.anatomical_structure, chemistry, Auxin, medicine, Degron, education, Cell synchronization

Abstract

The OsTIR1/auxin-inducible degron (AID) system allows “on demand” selective and reversible protein degradation upon exposure to the phytohormone auxin. In the current format, this technology does not allow to study the effect of acute protein depletion selectively in one phase of the cell cycle, as auxin similarly affects all the treated cells irrespectively of their proliferation status. Therefore, the AID system requires coupling with cell synchronization techniques, which can alter the basal biological status of the studied cell population. Here, we introduce a new AID system to Regulate OsTIR1 Levels based on the Cell Cycle Status (ROLECCS system), which induces proteolysis of both exogenously transfected and endogenous gene-edited targets in specific phases of the cell cycle. This new tool paves the way to studying the differential roles that target proteins may have in specific phases of the cell cycle.

Published

2021

182. Frontiers of MicroRNA Signature in Non-small Cell Lung Cancer

Author

Xiangjie Huang, Ri Cui, Masahisa Kudo, Xinping Zhu, Haishan Tian, Carlo M. Croce, and Hehuan Sui

Subjects

Oncology, medicine.medical_specialty, miRNA dysregulation, Mini Review, Molecular Targeted Therapies, Diagnostic tools, NSCLC, Metastasis, Cell and Developmental Biology, circulatory miRNAs, Internal medicine, microRNA, medicine, Screening method, Relative survival rate, Lung cancer, neoplasms, lcsh:QH301-705.5, miRNA, business.industry, Cell Biology, miRNA therapeutics, medicine.disease, respiratory tract diseases, lcsh:Biology (General), Non small cell, business, Developmental Biology

Abstract

Lung cancer is the leading cause of cancer-related deaths worldwide and non-small cell lung cancer (NSCLC) accounts for more than 80% of all lung cancer cases. Recent advancements in diagnostic tools, surgical treatments, chemotherapies, and molecular targeted therapies that improved the therapeutic efficacy in NSCLC. However, the 5-years relative survival rate of NSCLC is only about 20% due to the inadequate screening methods and late onset of clinical symptoms. Dysregulation of microRNAs (miRNAs) was frequently observed in NSCLC and closely associated with NSCLC development, progression, and metastasis through regulating their target genes. In this review, we provide an updated overview of aberrant miRNA signature in NSCLC, and discuss the possibility of miRNAs becoming a diagnostic and therapeutic tool. We also discuss the possible causes of dysregulated miRNAs in NSCLC.

Published

2021

183. Loss of expression of both miR-15/16 loci in CML transition to blast crisis

Author

Pierluigi Gasparini, Francesca Lovat, Michael Andreeff, Carlo M. Croce, John C. Byrd, Bing Z. Carter, Giovanni Nigita, Karilyn Larkin, and Mark D. Minden

Subjects

Adult, Male, Myeloid, Blast Crisis, Receptor Tyrosine Kinase-like Orphan Receptors, Pathogenesis, hemic and lymphatic diseases, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, medicine, Humans, Chronic phase CML, Polycomb Repressive Complex 1, Multidisciplinary, Transition (genetics), business.industry, Gene Expression Regulation, Leukemic, Myeloid leukemia, Biological Sciences, Middle Aged, medicine.disease, Leukemia, MicroRNAs, medicine.anatomical_structure, Proto-Oncogene Proteins c-bcl-2, Genetic Loci, ROR1, Cancer research, Disease Progression, Female, business

Abstract

Despite advances that have improved the treatment of chronic myeloid leukemia (CML) patients in chronic phase, the mechanisms of the transition from chronic phase CML to blast crisis (BC) are not fully understood. Considering the key role of miR-15/16 loci in the pathogenesis of myeloid and lymphocytic leukemia, here we aimed to correlate the expression of miR-15a/16 and miR-15b/16 to progression of CML from chronic phase to BC. We analyzed the expression of the two miR-15/16 clusters in 17 CML patients in chronic phase and 22 patients in BC and in 11 paired chronic phase and BC CML patients. BC CMLs show a significant reduction of the expression of miR-15a/-15b/16 compared to CMLs in chronic phase. Moreover, BC CMLs showed an overexpression of miR-15/16 direct targets such as Bmi-1, ROR1, and Bcl-2 compared to CMLs in chronic phase. This study highlights the loss of both miR-15/16 clusters as a potential oncogenic driver in the transition from chronic phase to BC in CML patients.

Published

2021

184. A preliminary study of micro-RNAs as minimally invasive biomarkers for the diagnosis of prostate cancer patients

Author

Andrea Vecchione, Carlo M. Croce, Gustavo Baldassarre, Andrea Tubaro, Cosimo De Nunzio, Stefano Volinia, Roberto Cirombella, Omar Faruq, Antonella Stoppacciaro, Simona Giglio, and Hideshi Ishii

Subjects

Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, diagnosis, Diagnostic accuracy, lcsh:RC254-282, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Prostate, Multifocal disease, Internal medicine, Biopsy, Biomarkers, Tumor, medicine, Humans, Sampling (medicine), prognosis, prostate cancer, microRNAs, Aged, Aged, 80 and over, medicine.diagnostic_test, Plasma samples, business.industry, Research, Prostatic Neoplasms, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cohort, business

Abstract

Background A prostate cancer diagnosis is based on biopsy sampling that is an invasive, expensive procedure, and doesn’t accurately represent multifocal disease. Methods To establish a model using plasma miRs to distinguish Prostate cancer patients from non-cancer controls, we enrolled 600 patients histologically diagnosed as having or not prostate cancer at biopsy. Two hundred ninety patients were eligible for the analysis. Samples were randomly divided into discovery and validation cohorts. Results NGS-miR-expression profiling revealed a miRs signature able to distinguish prostate cancer from non-cancer plasma samples. Of 51 miRs selected in the discovery cohort, we successfully validated 5 miRs (4732-3p, 98-5p, let-7a-5p, 26b-5p, and 21-5p) deregulated in prostate cancer samples compared to controls (p ≤ 0.05). Multivariate and ROC analyses show miR-26b-5p as a strong predictor of PCa, with an AUC of 0.89 (CI = 0.83–0.95;p To distinguish between low and high-grade prostate cancer, we found that miR-4732-3p levels were significantly higher; instead, miR-26b-5p and miR-98-5p levels were lower in low-grade compared to the high-grade group (p ≤ 0.05). Combining miR-26b-5p and miR-4732-3p we have the highest diagnostic accuracy for high-grade prostate cancer patients, (AUC = 0.80; CI 0,69-0,873). Conclusions Noninvasive diagnostic tests may reduce the number of unnecessary prostate biopsies. The 2-miRs-diagnostic model (miR-26b-5p and miR-98-5p) and the 2-miRs-grade model (miR-26b-5p and miR-4732-3p) are promising minimally invasive tools in prostate cancer clinical management.

Published

2021

185. Detecting and Characterizing A-to-I MicroRNA Editing in Cancer

Author

Luisa Tomasello, Rosario Distefano, Giovanni Nigita, Gioacchino P. Marceca, Mario Acunzo, and Carlo M. Croce

Subjects

0301 basic medicine, Cancer Research, 010504 meteorology & atmospheric sciences, detection, Computational biology, Review, Biology, lcsh:RC254-282, 01 natural sciences, 03 medical and health sciences, 0302 clinical medicine, microRNA targeting, microRNA, medicine, Inosine, 030304 developmental biology, 0105 earth and related environmental sciences, 0303 health sciences, A-to-I RNA editing, allergology, functional characterization, RNA, Cancer, Translation (biology), Cell cycle, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Adenosine, ADAR, quantification, 3. Good health, microRNAs, 030104 developmental biology, Oncology, 030217 neurology & neurosurgery, medicine.drug

Abstract

Simple Summary Adenosine to inosine (A-to-I) editing is a type of RNA editing where individual adenosines are enzymatically converted into inosines. A-to-I RNA editing plays an important role in cancer biology. Several studies have demonstrated that A-to-I editing of microRNAs (miRNAs) very often affect miRNA function as oncosuppressors or oncogenes, hence showing clinical relevance. Hence, A-to-I miRNA editing has been suggested as a potential diagnostic and prognostic tool in the monitoring of cancer patients. Nevertheless, the process of identifying and characterizing miRNA editing events in tumor samples still presents several challenges. In this review, we outline molecular aspects linked to miRNA A-to-I editing and retrace methods and approaches dedicated to detection of editing sites and functional characterization of edited miRNAs in cancer. Abstract Adenosine to inosine (A-to-I) editing consists of an RNA modification where single adenosines along the RNA sequence are converted into inosines. Such a biochemical transformation is catalyzed by enzymes belonging to the family of adenosine deaminases acting on RNA (ADARs) and occurs either co- or post-transcriptionally. The employment of powerful, high-throughput detection methods has recently revealed that A-to-I editing widely occurs in non-coding RNAs, including microRNAs (miRNAs). MiRNAs are a class of small regulatory non-coding RNAs (ncRNAs) acting as translation inhibitors, known to exert relevant roles in controlling cell cycle, proliferation, and cancer development. Indeed, a growing number of recent researches have evidenced the importance of miRNA editing in cancer biology by exploiting various detection and validation methods. Herein, we briefly overview early and currently available A-to-I miRNA editing detection and validation methods and discuss the significance of A-to-I miRNA editing in human cancer.

Published

2021

186. Editorial: Novel Drugs Targeting the Microenvironment and the Epigenetic Changes in Hematopoietic Malignancies

Author

Diana Gulei, Ciprian Tomuleasa, Liren Qian, Cristina Bagacean, Carlo M. Croce, and Gabriel Ghiaur

Subjects

hematological malignances, epigenetic changes, lcsh:RM1-950, Methylation, Biology, tumor microenvionment, Haematopoiesis, Editorial, lcsh:Therapeutics. Pharmacology, Cancer research, Pharmacology (medical), Epigenetics, methylation, pharmacology

Published

2020

187. Holland-Frei Cancer Medicine

Author

Robert C. Bast, Jr, John C. Byrd, Carlo M. Croce, Ernest Hawk, Fadlo R. Khuri, Raphael E. Pollock, Apostolia-Maria Tsimberidou, Christopher G. Willett, Cheryl L. Willman, Robert C. Bast, Jr, John C. Byrd, Carlo M. Croce, Ernest Hawk, Fadlo R. Khuri, Raphael E. Pollock, Apostolia-Maria Tsimberidou, Christopher G. Willett, and Cheryl L. Willman

Subjects

Cancer--Treatment, Cancer--Diagnosis

Abstract

HOLLAND-FREI CANCER MEDICINE The latest edition of the gold-standard in cancer science and clinical oncology references In the newly revised Tenth Edition of Holland-Frei Cancer Medicine, a team of distinguished researchers and practitioners delivers a comprehensive and up-to-date discussion of cancer science and clinical oncology practice. The book contains timely and indispensable information on epidemiology, etiology, cancer biology, immunology, prevention, screening, clinical presentation, pathology, imaging, and therapy. Grounded in a fundamental understanding of cancer biology, Holland-Frei Cancer Medicine combines scientific principles with clinical practice. It contains hundreds of full-color illustrations and photographs, tables, graphs, and algorithms that complement and enhance the complex topics discussed within the book. This book is an invaluable clinical tool that provides readers with overview boxes, additional references, and other pedagogic features designed to make the content easy to access and comprehend. Readers will also find: A translational and integrated approach throughout the book that combines cancer biology with cancer management A strong emphasis on multidisciplinary, research-driven patient care that improves outcomes and allows for the optimal use of all clinically appropriate therapies Discussions of the most current personalized cancer care, including molecular diagnostics and therapeutics Perfect for medical oncologists, radiation oncologists, and internists, Holland-Frei Cancer Medicine, Tenth Edition will also earn a place in the libraries of allied health professionals involved in the treatment of cancer patients. This book is published in collaboration with the American Association for Cancer Research: https://www.aacr.org/

Published

2023

188. MicroRNAs in Skeletal Muscle and Hints on Their Potential Role in Muscle Wasting During Cancer Cachexia

Author

Gioacchino P. Marceca, Federica Calore, Giovanni Nigita, and Carlo M. Croce

Subjects

Cancer Research, Adipose tissue, Review, Systemic inflammation, lcsh:RC254-282, Cachexia, long non-coding RNAs, Weight loss, Medicine, Myocyte, Wasting, business.industry, Skeletal muscle, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, ADAR, microRNAs, medicine.anatomical_structure, Oncology, Cancer research, skeletal muscle wasting, medicine.symptom, extracellular vesicles, business, Myofibril, cancer cachexia

Abstract

Cancer-associated cachexia is a heterogeneous, multifactorial syndrome characterized by systemic inflammation, unintentional weight loss, and profound alteration in body composition. The main feature of cancer cachexia is represented by the loss of skeletal muscle tissue, which may or may not be accompanied by significant adipose tissue wasting. Such phenotypic alteration occurs as the result of concomitant increased myofibril breakdown and reduced muscle protein synthesis, actively contributing to fatigue, worsening of quality of life, and refractoriness to chemotherapy. According to the classical view, this condition is primarily triggered by interactions between specific tumor-induced pro-inflammatory cytokines and their cognate receptors expressed on the myocyte membrane. This causes a shift in gene expression of muscle cells, eventually leading to a pronounced catabolic condition and cell death. More recent studies, however, have shown the involvement of regulatory non-coding RNAs in the outbreak of cancer cachexia. In particular, the role exerted by microRNAs is being widely addressed, and several mechanistic studies are in progress. In this review, we discuss the most recent findings concerning the role of microRNAs in triggering or exacerbating muscle wasting in cancer cachexia, while mentioning about possible roles played by long non-coding RNAs and ADAR-mediated miRNA modifications.

Published

2020

189. MicroRNA and ER stress in cancer

Author

Carlo M. Croce and Taewan Kim

Subjects

0301 basic medicine, Cancer Research, Endoplasmic reticulum, Cancer, Cellular homeostasis, Computational biology, Biology, Cell fate determination, Proteomics, medicine.disease, Endoplasmic Reticulum Stress, Gene Expression Regulation, Neoplastic, 03 medical and health sciences, MicroRNAs, 030104 developmental biology, 0302 clinical medicine, Proteostasis, 030220 oncology & carcinogenesis, Neoplasms, microRNA, Unfolded protein response, medicine, Unfolded Protein Response, Animals, Humans

Abstract

The development of biological technologies in genomics, proteomics, and bioinformatics has led to the identification and characterization of the complete set of coding genes and their roles in various cellular pathways in cancer. Nevertheless, the cellular pathways have not been fully figured out like a jigsaw puzzle with missing pieces. The discovery of noncoding RNAs including microRNAs (miRNAs) has provided the missing pieces of the cellular pathways. Likewise, miRNAs have settled many questions of inexplicable patches in the endoplasmic reticulum (ER) stress pathways. The ER stress-caused pathways typified by the unfolded protein response (UPR) are pivotal processes for cellular homeostasis and survival, rectifying uncontrolled proteostasis and determining the cell fate. Although various factors and pathways have been studied and characterized, the understanding of the ER stress requires more wedges to fill the cracks of knowledge about the ER stress pathways. Moreover, the roles of the ER stress and UPR are still controversial in cancer despite their strong potential to promote cancer. The noncoding RNAs, in particular, miRNAs aid in a better understanding of the ER stress and its role in cancer. In this review, miRNAs that are the more-investigated subtype of noncoding RNAs are focused on the interpretation of the ER stress in cancer, following the introduction of miRNA and ER stress.

Published

2020

190. MiR-124a Regulates Extracellular Vesicle Release by Targeting GTPase Rabs in Lung Cancer

Author

Giulia Romano, Giovanni Nigita, Federica Calore, Michela Saviana, Patricia Le, Carlo M. Croce, Mario Acunzo, and Patrick Nana-Sinkam

Subjects

0301 basic medicine, Cancer Research, GTPase, Biology, lcsh:RC254-282, Rab27, 03 medical and health sciences, 0302 clinical medicine, microRNA, medicine, Secretion, Lung cancer, RAB27, Original Research, Extracellular vesicle, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell biology, miR-124a, lung cancer, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, extracellular vesicles, Rab32, Rab, Biogenesis

Abstract

Lung cancer is the leading cause of cancer mortality worldwide. Increased understanding of the molecular mechanisms of the disease has led to the development of novel therapies and improving outcomes. Recently, extracellular vesicles (EVs) have emerged as vehicles for the transfer of genetic information between tumors and their microenvironment and have been implicated in lung cancer initiation, progression, and response to therapy. However, the mechanisms that drive the biogenesis and selective packaging of EVs remain poorly understood. Rab family guanosine triphosphates (GTPases) and their regulators are important membrane trafficking organizers. In this study, we investigated the role of select Rab GTPases on the regulation of EV release. We found that microRNAs target Rab GTPases to regulate EV release from lung cancer cell lines. In particular, Rab32 is a target of miR-124a, and siRNA and miRNA mediated inhibition of Rab32 leads to impaired EV secretion. The downstream implications for microRNA-based regulation of EV release are currently under investigation.

Published

2020

191. NCL Inhibition Exerts Antineoplastic Effects against Prostate Cancer Cells by Modulating Oncogenic MicroRNAs

Author

Debra L. Zynger, Ashley Braddom, Cindy James, Dario Palmieri, Carlo M. Croce, Tasha Posid, Anna Tessari, Tyler Sheetz, Kareesma Parbhoo, Joseph Mills, Vincenzo Coppola, Valerio Embrione, Claudia Foray, and Megan Pawlikowski

Subjects

Cancer Research, business.industry, Cell, Cancer, Context (language use), lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, urologic and male genital diseases, prostate cancer, lcsh:RC254-282, Article, microRNAs, Androgen deprivation therapy, Prostate cancer, medicine.anatomical_structure, nucleolin, Oncology, DU145, LNCaP, medicine, Cancer research, castration-resistant prostate cancer, business, Nucleolin

Abstract

Prostate cancer (PCa) is the most frequently diagnosed cancer in men and second most common cause of cancer-related deaths in the United States. Androgen deprivation therapy (ADT) is only temporarily effective for advanced-stage PCa, as the disease inevitably progresses to castration-resistant prostate cancer (CRPC). The protein nucleolin (NCL) is overexpressed in several types of human tumors where it is also mislocalized to the cell surface. We previously reported the identification of a single-chain fragment variable (scFv) immuno-agent that is able to bind NCL on the surface of breast cancer cells and inhibit proliferation both in vitro and in vivo. In the present study, we evaluated whether NCL could be a valid therapeutic target for PCa, utilizing DU145, PC3 (CRPC), and LNCaP (androgen-sensitive) cell lines. First, we interrogated the publicly available databases and noted that higher NCL mRNA levels are associated with higher Gleason Scores as well as with recurrent and metastatic tumors. Then, using our anti-NCL scFv, we demonstrated that NCL is expressed on the surface of all three tested cell lines and that NCL inhibition results in reduced proliferation and migration. We also measured the inhibitory effect of NCL targeting on the biogenesis of oncogenic microRNAs such as miR-21, -221 and -222, which was cell context dependent. Taken together, our data provide evidence that NCL targeting inhibits the key hallmarks of malignancy in PCa cells and may provide a novel therapeutic option for patients with advanced-stage PCa.

Published

2020

192. Micro-RNAs as minimally invasive biomarkers for diagnosis, staging and outcome prediction in prostate cancer patients

Author

M. Pesce, Andrea Vecchione, Gustavo Baldassarre, Andrea Tubaro, C. De Nunzio, Omar Faruq, Simona Giglio, Carlo M. Croce, Roberto Cirombella, A. Stoppacciaro, and Stefano Volinia

Subjects

Oncology, medicine.medical_specialty, business.industry, Urology, medicine.disease, lcsh:Diseases of the genitourinary system. Urology, lcsh:RC870-923, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Prostate cancer, Internal medicine, medicine, Outcome prediction, business

Published

2020

193. Tumor predisposition and cancer syndromes as models to study gene X environment interactions

Author

David Malkin, Giovanni Gaudino, John H.J. Petrini, James E. Cleaver, Webster K. Cavenee, Bruce Beutler, Angela Bononi, Haining Yang, Tak W. Mak, Elizabeth P. Henske, William D. Foulkes, Carlo M. Croce, Michele Carbone, Sarah T. Arron, Paul M. Hwang, Alan D. D'Andrea, Ian D. Hickson, Richard D. Kolodner, Flavia Novelli, Raymond J. Monnat, Laura S. Schmidt, Joanna L. Groden, and Harvey I. Pass

Subjects

Cell division, DNA damage, General Mathematics, Biology, Malignancy, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Germline mutation, Neoplasms, medicine, Animals, Humans, Genetic Predisposition to Disease, Gene, Carcinogen, Germ-Line Mutation, Applied Mathematics, Cancer, medicine.disease, chemistry, 030220 oncology & carcinogenesis, Cancer research, Gene-Environment Interaction, DNA

Abstract

Cell division and organismal development are exquisitely orchestrated and regulated processes. The dysregulation of the molecular mechanisms underlying these processes may cause cancer, a consequence of cell-intrinsic and/or cell-extrinsic events. Cellular DNA can be damaged by spontaneous hydrolysis, reactive oxygen species, aberrant cellular metabolism, or other perturbations that cause DNA damage. Moreover, several environmental factors may damage the DNA, alter cellular metabolism, or affect the ability of cells to interact with their microenvironment. While some environmental factors are well established as carcinogens, there remains a large knowledge gap of others owing to the difficulty in identifying them because of the typically long interval between carcinogen exposure and cancer diagnosis. DNA damage increases in cells harboring mutations that impair their ability to correctly repair the DNA. Tumor predisposition syndromes in which cancers arise at an accelerated rate and in different organs - the equivalent of a sensitized background - provide a unique opportunity to examine how gene–environment interactions (GxE) influence cancer risk when the initiating genetic defect responsible for malignancy is known. Understanding the molecular processes that are altered by specific germline mutations, environmental exposures and related mechanisms that promote cancer, will allow the design of novel and effective preventive and therapeutic strategies.

Published

2020

194. Combined loss of function of two different loci of miR-15/16 drives the pathogenesis of acute myeloid leukemia

Author

Luca Malcovati, Michael A. Caligiuri, Mark D. Minden, Anna Gallì, Narmin Ibrahimova, Rosario Distefano, Alexey Palamarchuk, Francesca Lovat, Pierluigi Gasparini, Silvia Catricalà, Tatsuya Nakamura, Paolo Fadda, Giovanni Nigita, Carlo M. Croce, and Luisa Tomasello

Subjects

Male, Disease, Biology, Pathogenesis, Cohort Studies, hemic and lymphatic diseases, microRNA, medicine, Gene silencing, Humans, neoplasms, Loss function, Aged, Aged, 80 and over, Multidisciplinary, Gene Expression Regulation, Leukemic, Myelodysplastic syndromes, Myeloid leukemia, Methylation, Middle Aged, Biological Sciences, medicine.disease, Leukemia, Myeloid, Acute, MicroRNAs, Cancer research, Disease Progression, Female

Abstract

Double knockout of the two miR-15/16 loci in mouse resulted in the development of acute myeloid leukemia (AML). This result suggested that, at least, a fraction of human AMLs could be due to a similar mechanism. We analyzed the role of the two miR-15/16 clusters in 93 myelodysplastic syndrome (MDS) patients divided in three subgroups: patients with MDS, patients with MDS before transforming into AML (MDS-T), and patients with AML evolving from MDS (MDS-AML). Then, we tested 139 AML cases and 14 different AML cell lines by assessing microRNA (miRNA) expression, target protein expression, genetic loss, and silencing. MDS-T and MDS-AML patients show a reduction of the expression of miR-15a/-15b/-16 compared to MDS patients. Each miRNA can significantly predict MDS and MDS-T groups. Then, 79% of primary AMLs show a reduced expression of miR-15a and/or miR-15b. The expression of miR-15a/-15b/-16 significantly stratified AML patients in two prognostic classes. Furthermore, 40% of AML cell lines showed a combined loss of the expression of miR-15a/-15b and overexpression of their direct/indirect targets. As potential mechanisms involved in the silencing of the two miR-15/16 loci, we identified a genetic loss of miR-15a and miR-15b and silencing of these two loci by methylation. We identified a potential driver oncogenic role in the loss of expression of both miR-15/16 clusters in the progression of MDS into AML and in AML pathogenesis. The stratification of AML patients, based on miR-15/16 expression, can lead to targeted and combination therapies for the treatment of this incurable disease.

Published

2020

195. Synergistic apoptotic effect of miR-183-5p and Polo-Like kinase 1 inhibitor NMS-P937 in breast cancer cells

Author

Rosario Distefano, Dario Veneziano, Pierluigi Gasparini, Giovanni Nigita, Masahisa Kudo, Nicole Zalles, and Carlo M. Croce

Subjects

Apoptosis, Breast Neoplasms, Cell Cycle Proteins, Polo-like kinase, Tumor initiation, Biology, Protein Serine-Threonine Kinases, PLK1, Breast cancer, Cell Line, Tumor, Proto-Oncogene Proteins, microRNA, medicine, Humans, Molecular Biology, Mitosis, Cell Proliferation, Kinase, Cell Biology, medicine.disease, MicroRNAs, Cancer research, Quinazolines, Pyrazoles, Female

Abstract

MicroRNAs (miRNAs) are small noncoding RNAs that act as endogenous regulatory molecules targeting specific mRNAs for translational repression. Studies of breast cancer genomics indicate that breast cancer subtypes are distinguished and regulated by specific sets of miRNAs which affect activities such as tumor initiation, progression, and even drug response. Polo-like Kinase 1 (PLK1) is widely considered to be a proto-oncogene due to its increased expression in multiple tumor types, as well as its crucial role in regulating mitosis. Pharmacological inhibition of PLK1 can reduce tumor volume and induce tumor cell death in solid and hematologic malignancies. This prompted us to investigate how PLK1 inhibition with the target-specific inhibitor NMS-P937 would impact breast cancer cells, and how miRNAs may influence the overall response of these cells to this inhibition. We found that miR-183-5p targets PLK1 gene, effectively reducing its protein expression. Such miRNA-driven regulation of PLK1 expression sensitizes breast cancer cells to NMS-P937, resulting in synergistically increased apoptosis. We also show that the miRNA-regulated reduction of PLK1 influences the expression of apoptosis-related key proteins and possibly inducing further indirect PLK1 downmodulation through a DNMT1-p53 axis. These results suggest a potential biologically significant link between the expression of miR-183-5p and the efficacy of PLK1-specific inhibitors in breast cancer cells. Our work further elucidates how miR-183-5p regulates PLK1 gene while also enhancing NMS-P937 effect in breast cancer. Future studies assessing the role of miR-183-5p as a novel biomarker for anti-PLK1 chemotherapy agents are warranted.

Published

2020

196. miR-196b-5p–mediated downregulation of TSPAN12 and GATA6 promotes tumor progression in non-small cell lung cancer

Author

Xiangjie Huang, Ri Cui, Matteo Fassan, Sisi Xiao, Canwei Wang, Chengguang Zhao, Yun Yu, Carlo M. Croce, Wei Meng, Changtian Yin, Xiaokun Li, Yumin Wang, Guang Liang, Peng Zou, Masahisa Kudo, and Wangyu Zhu

Subjects

Lung Neoplasms, Tetraspanins, Down-Regulation, Mice, Nude, Biology, NSCLC, law.invention, Mice, GATA6, TSPAN12, Downregulation and upregulation, law, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, GATA6 Transcription Factor, microRNA, medicine, Animals, Humans, Lung cancer, Cell Proliferation, QKI, Multidisciplinary, miR-196b, Cell cycle, Biological Sciences, medicine.disease, Xenograft Model Antitumor Assays, respiratory tract diseases, Gene Expression Regulation, Neoplastic, MicroRNAs, Tumor progression, Cancer research, Disease Progression, Suppressor, Female

Abstract

Lung cancer is the leading cause of cancer-related deaths worldwide and non-small cell lung cancer (NSCLC) accounts for over 80% of lung cancer cases. The RNA binding protein, QKI, belongs to the STAR family and plays tumor-suppressive functions in NSCLC. QKI-5 is a major isoform of QKIs and is predominantly expressed in NSCLC. However, the underlying mechanisms of QKI-5 in NSCLC progression remain unclear. We found that QKI-5 regulated microRNA (miRNA), miR-196b-5p, and its expression was significantly up-regulated in NSCLC tissues. Up-regulated miR-196b-5p promotes lung cancer cell migration, proliferation, and cell cycle through directly targeting the tumor suppressors, GATA6 and TSPAN12. Both GATA6 and TSPAN12 expressions were down-regulated in NSCLC patient tissue samples and were negatively correlated with miR-196b-5p expression. Mouse xenograft models demonstrated that miR-196b-5p functions as a potent onco-miRNA, whereas TSPAN12 functions as a tumor suppressor in NSCLC in vivo. QKI-5 bound to miR-196b-5p and influenced its stability, resulting in up-regulated miR-196b-5p expression in NSCLC. Further analysis showed that hypomethylation in the promoter region enhanced miR-196b-5p expression in NSCLC. Our findings indicate that QKI-5 may exhibit novel anticancer mechanisms by regulating miRNA in NSCLC, and targeting the QKI5∼miR-196b-5p∼GATA6/TSPAN12 pathway may enable effectively treating some NSCLCs.

Published

2020

197. Identification of tRNA-derived small RNA (tsRNA) responsive to the tumor suppressor, RUNX1, in breast cancer

Author

Janet L. Stein, Deli Hong, Carlo M. Croce, Andrew J. Fritz, Gary S. Stein, Veronica Balatti, Dario Veneziano, Caroline E. Adams, Nicholas H. Farina, Stephanie Scalia, Jane B. Lian, and Terri L. Messier

Subjects

0301 basic medicine, Physiology, Clinical Biochemistry, Breast Neoplasms, Biology, Article, law.invention, Metastasis, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Breast cancer, Downregulation and upregulation, RNA, Transfer, law, hemic and lymphatic diseases, Cell Line, Tumor, medicine, Humans, Transcription factor, Cell Proliferation, Tumor Suppressor Proteins, Epithelial Cells, Cell Biology, medicine.disease, Non-coding RNA, Gene Expression Regulation, Neoplastic, 030104 developmental biology, RUNX1, chemistry, 030220 oncology & carcinogenesis, Core Binding Factor Alpha 2 Subunit, Cancer research, Suppressor, RNA, Ectopic expression, Female

Abstract

Despite recent advances in targeted therapies, the molecular mechanisms driving breast cancer initiation, progression, and metastasis are minimally understood. Growing evidence indicate that transfer RNA (tRNA)-derived small RNAs (tsRNA) contribute to biological control and aberrations associated with cancer development and progression. The runt-related transcription factor 1 (RUNX1) transcription factor is a tumor suppressor in the mammary epithelium whereas RUNX1 downregulation is functionally associated with breast cancer initiation and progression. We identified four tsRNA (ts-19, ts-29, ts-46, and ts-112) that are selectively responsive to expression of the RUNX1 tumor suppressor. Our finding that ts-112 and RUNX1 anticorrelate in normal-like mammary epithelial and breast cancer lines is consistent with tumor-related activity of ts-112 and tumor suppressor activity of RUNX1. Inhibition of ts-112 in MCF10CA1a aggressive breast cancer cells significantly reduced proliferation. Ectopic expression of a ts-112 mimic in normal-like mammary epithelial MCF10A cells significantly increased proliferation. These findings support an oncogenic potential for ts-112. Moreover, RUNX1 may repress ts-112 to prevent overactive proliferation in breast epithelial cells to augment its established roles in maintaining the mammary epithelium.

Published

2020

198. Pleiotropic tumor suppressor functions of WWOX antagonize metastasis

Author

Rosario Distefano, Rami I. Aqeilan, Sung-Suk Suh, Sara Oster, Tamar Geiger, Victoria L. Seewaldt, Yong Peng, Giovanni Nigita, Yoav Smith, Abed Khalaileh, Carlo M. Croce, and Saleh Khawaled

Subjects

0301 basic medicine, WWOX, Cancer Research, Epithelial-Mesenchymal Transition, Dishevelled Proteins, lcsh:Medicine, Triple Negative Breast Neoplasms, Biology, Article, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Transforming Growth Factor beta, Genetics research, microRNA, Genetics, medicine, Humans, Protein Interaction Maps, Smad3 Protein, Neoplasm Metastasis, lcsh:QH301-705.5, Wnt Signaling Pathway, Cell Proliferation, Regulation of gene expression, Tumor Suppressor Proteins, lcsh:R, Wnt signaling pathway, Cancer, Genetic Pleiotropy, medicine.disease, 3. Good health, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, lcsh:Biology (General), WW Domain-Containing Oxidoreductase, Tumor progression, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Female, Signal Transduction

Abstract

Tumor progression and metastasis are the major causes of death among cancer associated mortality. Metastatic cells acquire features of migration and invasion and usually undergo epithelia-mesenchymal transition (EMT). Acquirement of these various hallmarks rely on different cellular pathways, including TGF-β and Wnt signaling. Recently, we reported that WW domain-containing oxidoreductase (WWOX) acts as a tumor suppressor and has anti-metastatic activities involving regulation of several key microRNAs (miRNAs) in triple-negative breast cancer (TNBC). Here, we report that WWOX restoration in highly metastatic MDA-MB435S cancer cells alters mRNA expression profiles; further, WWOX interacts with various proteins to exert its tumor suppressor function. Careful alignment and analysis of gene and miRNA expression in these cells revealed profound changes in cellular pathways mediating adhesion, invasion and motility. We further demonstrate that WWOX, through regulation of miR-146a levels, regulates SMAD3, which is a member of the TGF-β signaling pathway. Moreover, proteomic analysis of WWOX partners revealed regulation of the Wnt-signaling activation through physical interaction with Disheveled. Altogether, these findings underscore a significant role for WWOX in antagonizing metastasis, further highlighting its role and therapeutic potential in suppressing tumor progression.

Published

2020

199. MicroRNA profiling of blastic plasmacytoid dendritic cell neoplasm and myeloid sarcoma

Author

Maria Antonella Laginestra, Luciano Cascione, Claudio Agostinelli, Elena Sabattini, Marco Paulli, Saveria Mazzara, Emilio Berti, Carlo M. Croce, Stefano Pileri, Giovanna Motta, Lorenzo Cerroni, Alessandro Laganà, Fabio Facchetti, Federica Melle, Alessandro Pileri, Valentina Tabanelli, Maria Rosaria Sapienza, Valentina Indio, Fabio Fuligni, Manuela Ferracin, Sapienza M.R., Fuligni F., Melle F., Tabanelli V., Indio V., Laginestra M.A., Motta G., Mazzara S., Cerroni L., Pileri A., Facchetti F., Paulli M., Cascione L., Lagana A., Berti E., Ferracin M., Agostinelli C., Sabattini E., Croce C.M., and Pileri S.A.

Subjects

Cancer Research, Biology, BPDCN, microRNA, Myeloid sarcoma, medicine, Humans, Sarcoma, Myeloid, Survival analysis, miRNA, discriminant analysis, miRNAs, MS, Hematology, General Medicine, Blastic plasmacytoid dendritic cell neoplasm, Dendritic Cells, medicine.disease, Survival Analysis, MicroRNAs, Oncology, Hematologic Neoplasms, Cancer research, Microrna profiling, Blast Crisis, discriminant analysi, Plasmacytoma

Abstract

not present

Published

2020

200. Abrogation of esophageal carcinoma development in miR-31 knockout rats

Author

Karl J. Smalley, Ruiyan Jing, Sili Fan, Carlo M. Croce, Guidantonio Malagoli Tagliazucchi, Louise Y.Y. Fong, Oliver Fiehn, Joseph Altemus, Cristian Taccioli, Kay Huebner, Alexey Palamarchuk, and John L. Farber

Subjects

Genome instability, Male, Medical Sciences, Knockout rat, Esophageal Neoplasms, Transgenic, law.invention, Transcriptome, Gene Knockout Techniques, 0302 clinical medicine, law, Neoplasms, in vivo antimiR-31 delivery, constitutive miR-31 knockout rat, zinc deficiency, In vivo antimiR-31 delivery, 2.1 Biological and endogenous factors, Aetiology, Cancer, Esophageal cancer rat model, 0303 health sciences, Multidisciplinary, Tumor, Zinc deficiency, NF-kappa B, Biological Sciences, Constitutive miR-31 knockout rat, Esophageal squamous cell carcinoma, 3. Good health, esophageal squamous cell carcinoma, Gene Expression Regulation, Neoplastic, mir-31, Zinc, 030220 oncology & carcinogenesis, Rats, Transgenic, medicine.symptom, Biotechnology, Signal Transduction, Nitrosamines, Inflammation, Biology, Cell Line, Hypoxia-Inducible Factor-Proline Dioxygenases, 03 medical and health sciences, Experimental, Rare Diseases, Esophagus, Cell Line, Tumor, Genetics, medicine, Carcinoma, Animals, Humans, neoplasms, Gene knockout, Nutrition, 030304 developmental biology, Neoplastic, esophageal cancer rat model, Human Genome, Neoplasms, Experimental, medicine.disease, digestive system diseases, Rats, MicroRNAs, Gene Expression Regulation, Dietary Supplements, Cancer research, Carcinogens, Suppressor, Digestive Diseases

Abstract

Significance ESCC is a deadly disease with few prevention or treatment options. In a dietary Zn deficiency-promoted rat ESCC model with miR-31–controlled inflammation pathway up-regulation, systemic antimiR-31 reduces miR-31 level and inflammation, suppressing ESCC development. We identified Egln3 as a direct miR-31 target and developed a constitutive miR-31 knockout rat model. Interactions of oncogenic miR-31, EGLN3 down-regulation, and inflammation occur in rat and human ESCC tissue. Since miR-31 genetic knockout prevents Zn deficiency-associated ESCC by eliminating or greatly reducing the entire miR-31-EGLN3/STK40-NF-κB–controlled inflammatory process, we conclude that miR-31 and downstream signaling proteins should be tested as prognostic and therapeutic targets and inexpensive Zn supplementation should be implemented for ESCC prevention in deficient populations., MicroRNA-31 (miR-31) is overexpressed in esophageal squamous cell carcinoma (ESCC), a deadly disease associated with dietary Zn deficiency and inflammation. In a Zn deficiency-promoted rat ESCC model with miR-31 up-regulation, cancer-associated inflammation, and a high ESCC burden following N-nitrosomethylbenzylamine (NMBA) exposure, systemic antimiR-31 delivery reduced ESCC incidence from 85 to 45% (P = 0.038) and miR-31 gene knockout abrogated development of ESCC (P = 1 × 10−6). Transcriptomics, genome sequencing, and metabolomics analyses in these Zn-deficient rats revealed the molecular basis of ESCC abrogation by miR-31 knockout. Our identification of EGLN3, a known negative regulator of nuclear factor κB (NF-κB), as a direct target of miR-31 establishes a functional link between oncomiR-31, tumor suppressor target EGLN3, and up-regulated NF-κB–controlled inflammation signaling. Interaction among oncogenic miR-31, EGLN3 down-regulation, and inflammation was also documented in human ESCCs. miR-31 deletion resulted in suppression of miR-31–associated EGLN3/NF-κB–controlled inflammatory pathways. ESCC-free, Zn-deficient miR-31−/− rat esophagus displayed no genome instability and limited metabolic activity changes vs. the pronounced mutational burden and ESCC-associated metabolic changes of Zn-deficient wild-type rats. These results provide conclusive evidence that miR-31 expression is necessary for ESCC development.

Published

2020