Your search keyword '"Raffaella, Sordella"' showing total 37 results

1. An epigenetic switch regulates the ontogeny of AXL-positive/EGFR-TKi-resistant cells by modulating miR-335 expression

Author

Serif Senturk, Ingrid Ibarra, Lawrence Glassman, Michael Esposito, Paul C. Lee, Madison Miller, Jiahao Huang, Kevin Hyman, Raffaella Sordella, Debjani Pal, David Zeltsman, Navya Korimerla, Gregory J. Hannon, Trine Lindsted, Polona Safaric Tepes, Vilma Jimenez Sabinina, Amaia Lujambio, Safaric Tepes, Polona [0000-0002-5833-739X], Lujambio, Amaia [0000-0002-2798-1481], Senturk, Serif [0000-0003-3963-2294], Sordella, Raffaella [0000-0001-9745-1227], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Lung Neoplasms, Cell, Epigenesis, Genetic, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Osimertinib, Biology (General), Cancer Biology, Aniline Compounds, General Neuroscience, General Medicine, ErbB Receptors, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Medicine, Intercellular Signaling Peptides and Proteins, Epigenetics, Erlotinib, Lung cancer, Research Article, medicine.drug, Human, QH301-705.5, Science, Antineoplastic Agents, Context (language use), Biology, Erlotinib-resistant, General Biochemistry, Genetics and Molecular Biology, Erlotinib Hydrochloride, 03 medical and health sciences, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Humans, RNA, Messenger, Protein Kinase Inhibitors, Acrylamides, General Immunology and Microbiology, GAS6, Receptor Protein-Tyrosine Kinases, Axl, medicine.disease, MicroRNAs, 030104 developmental biology, Drug Resistance, Neoplasm, Mutation, Cancer cell, Cancer research

Abstract

Despite current advancements in research and therapeutics, lung cancer remains the leading cause of cancer-related mortality worldwide. This is mainly due to the resistance that patients develop against chemotherapeutic agents over the course of treatment. In the context of non-small cell lung cancers (NSCLC) harboring EGFR-oncogenic mutations, augmented levels of AXL and GAS6 have been found to drive resistance to EGFR tyrosine kinase inhibitors such as Erlotinib and Osimertinib in certain tumors with mesenchymal-like features. By studying the ontogeny of AXL-positive cells, we have identified a novel non-genetic mechanism of drug resistance based on cell-state transition. We demonstrate that AXL-positive cells are already present as a subpopulation of cancer cells in Erlotinib-naïve tumors and tumor-derived cell lines and that the expression of AXL is regulated through a stochastic mechanism centered on the epigenetic regulation of miR-335. The existence of a cell-intrinsic program through which AXL-positive/Erlotinib-resistant cells emerge infers the need of treating tumors harboring EGFR-oncogenic mutations upfront with combinatorial treatments targeting both AXL-negative and AXL-positive cancer cells.

Published

2021

2. Author response: An epigenetic switch regulates the ontogeny of AXL-positive/EGFR-TKi-resistant cells by modulating miR-335 expression

Author

Gregory J. Hannon, Trine Lindsted, Serif Senturk, Polona Safaric Tepes, David Zeltsman, Madison Miller, Kevin Hyman, Debjani Pal, Raffaella Sordella, Navya Korimerla, Paul C. Lee, Ingrid Ibarra, Lawrence Glassman, Amaia Lujambio, Vilma Jimenez Sabinina, Jiahao Huang, and Michael Esposito

Subjects

Egfr tki, Ontogeny, Cancer research, Epigenetics, Biology

Published

2021

3. An epigenetic switch regulates the ontogeny of AXL-positive/EGFR-TKI resistant cells by modulating miR-335 expression

Author

Amaja Lujambio, Serif Senturk, Larry Glassman, Polona Safaric Tepes, Vilma Jimenez Sabinina, Debjani Pal, Madison Miller, David Zeltsman, Ingrid Ibarra, Michael Esposito, Gregory J. Hannon, Trine Lindsted, Jiahao Huang, Kevin Hyman, Paul C. Lee, Raffaella Sordella, and Navya Korimerla

Subjects

GAS6, Cell, Context (language use), Biology, medicine.disease, respiratory tract diseases, medicine.anatomical_structure, Cell culture, Cancer cell, medicine, Cancer research, Erlotinib, Epigenetics, Lung cancer, medicine.drug

Abstract

Lung cancer remains the leading cause of cancer-related mortality worldwide, despite current advancements in research and therapeutics. Many patients diagnosed with lung cancer will develop resistance to chemotherapeutic agents. In the context of non-small cell lung cancers (NSCLC) harboring EGFR oncogenic mutations, augmented levels of AXL and GAS6 have been found to drive Erlotinib resistance in certain tumors with mesenchymal-like features. By studying the ontogeny of AXL-positive cells, we have identified a novel non-genetic mechanism of drug resistance based on cell-state transition. We demonstrate that AXL-positive cells are already present as a sub-population of cancer cells in Erlotinib-naïve tumors and tumor-derived cell lines, and that the expression of AXL is regulated through a stochastic mechanism centered on the epigenetic regulation of miR-335. The existence of a cell-intrinsic program through which AXL-positive/Erlotinib-resistant cells emerge infers the need of treating tumors harboring EGFR-oncogenic mutations upfront with combinatorial treatments targeting both AXL-negative and AXL-positive cancer cells.

Published

2021

4. The nuclear transport receptor Importin-11 is a tumor suppressor that maintains PTEN protein

Author

Lorna Wills, Saya H. Ebbesen, Wu Zheng, Navneet Narula, Scott Powers, Kendra S. Plafker, Lloyd C. Trotman, Tali Herzka, Brian D. Robinson, Kaitlin Watrud, Vivek Mittal, Brendon M. Stiles, Nasser K. Altorki, Carlos Stahlhut, Dawid G. Nowak, John E. Wilkinson, Abu Nasar, Raffaella Sordella, Matthias Minderer, Carlos Cordon-Cardo, Mireia Castillo-Martin, Martha E. Zeeman, Alexandra Ambrico, Muhan Chen, Victoria M.-Y. Wang, and Scott M. Plafker

Subjects

0301 basic medicine, Cytoplasm, Lung Neoplasms, Phosphatase, Receptors, Cytoplasmic and Nuclear, Importin, Biology, Article, Cell Line, law.invention, Metastasis, Mice, 03 medical and health sciences, law, Cell Line, Tumor, medicine, Animals, Humans, Tensin, PTEN, Receptor, Research Articles, Cell Nucleus, Tumor Suppressor Proteins, PTEN Phosphohydrolase, Cell Biology, beta Karyopherins, medicine.disease, 3. Good health, 030104 developmental biology, Ubiquitin-Conjugating Enzymes, Cancer research, biology.protein, Suppressor, Adenocarcinoma, HeLa Cells

Abstract

Reduced PTEN protein is linked to tumorigenesis. Here, Chen et al. show that the nuclear transport receptor Importin-11 separates PTEN from degradation machinery. IPO11 mutant mice exhibit PTEN degradation, lung adenocarcinoma, and prostate neoplasia. In human prostatectomy patients, IPO11 status predicts disease recurrence and metastasis., Phosphatase and tensin homologue (PTEN) protein levels are critical for tumor suppression. However, the search for a recurrent cancer-associated gene alteration that causes PTEN degradation has remained futile. In this study, we show that Importin-11 (Ipo11) is a transport receptor for PTEN that is required to physically separate PTEN from elements of the PTEN degradation machinery. Mechanistically, we find that the E2 ubiquitin-conjugating enzyme and IPO11 cargo, UBE2E1, is a limiting factor for PTEN degradation. Using in vitro and in vivo gene-targeting methods, we show that Ipo11 loss results in degradation of Pten, lung adenocarcinoma, and neoplasia in mouse prostate with aberrantly high levels of Ube2e1 in the cytoplasm. These findings explain the correlation between loss of IPO11 and PTEN protein in human lung tumors. Furthermore, we find that IPO11 status predicts disease recurrence and progression to metastasis in patients choosing radical prostatectomy. Thus, our data introduce the IPO11 gene as a tumor-suppressor locus, which is of special importance in cancers that still retain at least one intact PTEN allele.

Published

2017

5. Rapid and tunable method to temporally control gene editing based on conditional Cas9 stabilization

Author

Alexander G. Vaughan, Serif Senturk, Justin B. Kinney, Lloyd C. Trotman, Nitin H. Shirole, Vincenzo Corbo, Debjani Pal, Raffaella Sordella, David A. Tuveson, and Dawid G. Nowak

Subjects

0301 basic medicine, Time Factors, Science, CRISPR-Associated Proteins, Protein domain, General Physics and Astronomy, Computational biology, Biology, Ligands, Article, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, Protein Domains, Genome editing, Recombinase, genome editing, Animals, Humans, CRISPR, Gene, Gene Editing, Genetics, CRISPR interference, Multidisciplinary, Integrases, Protein Stability, Cas9, Lentivirus, General Chemistry, Fibroblasts, Tamoxifen, 030104 developmental biology, A549 Cells, CRISPR-Cas Systems, Function (biology), RNA, Guide, Kinetoplastida

Abstract

The CRISPR/Cas9 system is a powerful tool for studying gene function. Here, we describe a method that allows temporal control of CRISPR/Cas9 activity based on conditional Cas9 destabilization. We demonstrate that fusing an FKBP12-derived destabilizing domain to Cas9 (DD-Cas9) enables conditional Cas9 expression and temporal control of gene editing in the presence of an FKBP12 synthetic ligand. This system can be easily adapted to co-express, from the same promoter, DD-Cas9 with any other gene of interest without co-modulation of the latter. In particular, when co-expressed with inducible Cre-ERT2, our system enables parallel, independent manipulation of alleles targeted by Cas9 and traditional recombinase with single-cell specificity. We anticipate this platform will be used for the systematic characterization and identification of essential genes, as well as the investigation of the interactions between functional genes., CRISPR/Cas9-based genome editing enables specific deletion of target genes. Here, Senturk et al. develop an inducible editing system by fusing a conditional destabilization domain to Cas9 and demonstrate temporal control of gene editing in response to a synthetic ligand.

Published

2017

6. Author response: TGF-β reduces DNA ds-break repair mechanisms to heighten genetic diversity and adaptability of CD44+/CD24− cancer cells

Author

Debjani Pal, Zhan Yao, Hilary Cox, Anja Pertot, Gary C Stone, Naishitha Anaparthy, Raffaella Sordella, James W. Hicks, Nitin H. Shirole, Jude Kendall, Tyler Garvin, Leyla Edwards, Gregory J. Hannon, Michael C. Schatz, Fred Rollins, Vijay A Singh, and Kenneth Chang

Subjects

Genetic diversity, CD24, media_common.quotation_subject, CD44, Biology, Adaptability, Cell biology, chemistry.chemical_compound, chemistry, Cancer cell, biology.protein, DNA, media_common, Transforming growth factor

Published

2016

7. Metabolic Alterations in Lung Cancer–Associated Fibroblasts Correlated with Increased Glycolytic Metabolism of the Tumor

Author

Virendra K. Chaudhri, Brendon M. Stiles, Raffaella Sordella, Melanie S. Buckman, Edward D. Karoly, Robert P. Mohney, Nasser K. Altorki, Timothy E. McGraw, Olivier Elemento, Gregory G. Salzler, and Salihah A. Dick

Subjects

Cancer Research, Lung Neoplasms, Cell Separation, Biology, Article, Metabolomics, Autophagy, medicine, Humans, Glycolysis, Fibroblast, Lung cancer, Molecular Biology, Cell Line, Transformed, Fibroblasts, medicine.disease, Cell biology, Metabolic pathway, Glucose, medicine.anatomical_structure, Oncology, Cell culture, Cancer cell, Cancer research, Microtubule-Associated Proteins

Abstract

Cancer cells undergo a metabolic reprogramming but little is known about metabolic alterations of other cells within tumors. We use mass spectrometry–based profiling and a metabolic pathway–based systems analysis to compare 21 primary human lung cancer–associated fibroblast lines (CAF) to “normal” fibroblast lines (NF) generated from adjacent nonneoplastic lung tissue. CAFs are protumorigenic, although the mechanisms by which CAFs support tumors have not been elucidated. We have identified several pathways whose metabolite abundance globally distinguished CAFs from NFs, suggesting that metabolic alterations are not limited to cancer cells. In addition, we found metabolic differences between CAFs from high and low glycolytic tumors that might reflect distinct roles of CAFs related to the tumor's glycolytic capacity. One such change was an increase of dipeptides in CAFs. Dipeptides primarily arise from the breakdown of proteins. We found in CAFs an increase in basal macroautophagy which likely accounts for the increase in dipeptides. Furthermore, we show a difference between CAFs and NFs in the induction of autophagy promoted by reduced glucose. In sum, our data suggest that increased autophagy may account for metabolic differences between CAFs and NFs and may play additional as yet undetermined roles in lung cancer. Mol Cancer Res; 11(6); 579–92. ©2013 AACR.

Published

2013

8. TP53 exon-6 truncating mutations produce separation of function isoforms with pro-tumorigenic functions

Author

Madison Miller, Joseph Boroda, Nitin H. Shirole, Debjani Pal, Paola Pisterzi, Marc Ladanyi, Raffaella Sordella, Gustavo Munoz, Scott W. Lowe, Marko Anderluh, Serif Senturk, and Edward R. Kastenhuber

Subjects

0301 basic medicine, Gene isoform, CypD, Mouse, QH301-705.5, tumor suppressor, Science, Mutant, Regulator, Biology, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Exon, medicine, cancer, metastasis, Allele, Biology (General), Cancer Biology, Genetics, General Immunology and Microbiology, General Neuroscience, Alternative splicing, General Medicine, Cell Biology, Phenotype, 3. Good health, Cell biology, mitochondria, 030104 developmental biology, TP53 truncations, Medicine, Carcinogenesis, Research Article, Human

Abstract

TP53 truncating mutations are common in human tumors and are thought to give rise to p53-null alleles. Here, we show that TP53 exon-6 truncating mutations occur at higher than expected frequencies and produce proteins that lack canonical p53 tumor suppressor activities but promote cancer cell proliferation, survival, and metastasis. Functionally and molecularly, these p53 mutants resemble the naturally occurring alternative p53 splice variant, p53-psi. Accordingly, these mutants can localize to the mitochondria where they promote tumor phenotypes by binding and activating the mitochondria inner pore permeability regulator, Cyclophilin D (CypD). Together, our studies reveal that TP53 exon-6 truncating mutations, contrary to current beliefs, act beyond p53 loss to promote tumorigenesis, and could inform the development of strategies to target cancers driven by these prevalent mutations. DOI: http://dx.doi.org/10.7554/eLife.17929.001

Published

2016

9. Transforming Big Data into cancer-relevant insight: An initial, multi-tier approach to assess reproducibility and relevance

Author

Edus H. Warren, Anna Lasorella, Hanlee P. Ji, Alykhan F. Shamji, Michael A. White, Tina Zheng, Jonathan S. Weissman, Jesse S. Boehm, Stanley R. Riddell, Michael T. McManus, Chris Sander, Adam A. Margolin, Christopher J. Kemp, Haian Fu, Michael Boettcher, Stuart L. Schreiber, Ken Chen, Justin Chen, Frank McCormick, Andrea Califano, Raffaella Sordella, Calvin J. Kuo, Fadlo R. Khuri, Olivier Gevaert, Brent R. Stockwell, Paul A. Clemons, Scott Powers, Francisca Vazquez, Bridget K. Wagner, Barbara A. Weir, Cindy S. Hon, Sourav Bandyopadhyay, Harshil Dhruv, John D. Minna, John B. MacMillan, Darren Finlay, Carla Grandori, Jessica N. Mazerik, Michael G. Roth, Allan Balmain, Trever G. Bivona, Erin F. Simonds, Olga Nikolova, Zhenyi An, Daniela S. Gerhard, Margaret A. Johns, Ozlem Aksoy, Jose M. Silva, Bruce A. Posner, Kristiina Vuori, Subhashini Jagu, Eduardo Mendez, Seungchan Kim, Matthew J. Hangauer, Kenneth L. Scott, Jeff Kiefer, Gordon B. Mills, Martin W. McIntosh, William A. Weiss, Carlos S. Moreno, Michael E. Berens, Vijayakrishna K. Gadi, Scott W. Lowe, Han Liang, Mahalaxmi Aburi, Kenneth C. Smith, William C. Hahn, Alexander Krasnitz, and Antonio Iavarone

Subjects

0301 basic medicine, Cancer Research, Biomedical Research, business.industry, Collaborative network, Big data, Reproducibility of Results, Biology, Bioinformatics, Data science, Data resources, Work environment, Article, 03 medical and health sciences, 030104 developmental biology, Oncology, Neoplasms, Key (cryptography), Cancer research, Humans, Relevance (information retrieval), Multi tier, business, Molecular Biology

Abstract

The Cancer Target Discovery and Development (CTD2) Network was established to accelerate the transformation of “Big Data” into novel pharmacologic targets, lead compounds, and biomarkers for rapid translation into improved patient outcomes. It rapidly became clear in this collaborative network that a key central issue was to define what constitutes sufficient computational or experimental evidence to support a biologically or clinically relevant finding. This article represents a first attempt to delineate the challenges of supporting and confirming discoveries arising from the systematic analysis of large-scale data resources in a collaborative work environment and to provide a framework that would begin a community discussion to resolve these challenges. The Network implemented a multi-tier framework designed to substantiate the biological and biomedical relevance as well as the reproducibility of data and insights resulting from its collaborative activities. The same approach can be used by the broad scientific community to drive development of novel therapeutic and biomarker strategies for cancer. Mol Cancer Res; 14(8); 675–82. ©2016 AACR.

Published

2016

10. Effectors and potential targets selectively upregulated in human KRAS-mutant lung adenocarcinomas

Author

Raffaella Sordella, Jinyu Li, and Scott Powers

Subjects

MAPK/ERK pathway, 0301 basic medicine, Lung Neoplasms, MAP Kinase Signaling System, Mutant, Adenocarcinoma of Lung, Adenocarcinoma, Protein Serine-Threonine Kinases, medicine.disease_cause, Article, Receptor tyrosine kinase, Proto-Oncogene Proteins p21(ras), 03 medical and health sciences, 0302 clinical medicine, PTPRM, Gene expression, medicine, Humans, Gene, PI3K/AKT/mTOR pathway, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Mutation, Multidisciplinary, biology, Sequence Analysis, RNA, Receptor-Like Protein Tyrosine Phosphatases, Class 4, Receptor-Like Protein Tyrosine Phosphatases, Class 2, Pyruvate Dehydrogenase Acetyl-Transferring Kinase, Proto-Oncogene Proteins c-met, digestive system diseases, Up-Regulation, 3. Good health, Gene Expression Regulation, Neoplastic, 030104 developmental biology, 030220 oncology & carcinogenesis, Phosphoprotein, Proteome, biology.protein, Cancer research, raf Kinases, KRAS, Tumor Suppressor Protein p53

Abstract

Genetic and proteomic analysis of human tumor samples can provide an important compliment to information obtained from model systems. Here we examined protein and gene expression from the Cancer Genome and Proteome Atlases (TCGA and TCPA) to characterize proteins and protein-coding genes that are selectively upregulated in KRAS-mutant lung adenocarcinomas. Phosphoprotein activation of several MAPK signaling components was considerably stronger in KRAS-mutants than any other group of tumors, even those with activating mutations in receptor tyrosine kinases (RTKs) and BRAF. Co-occurring mutations in KRAS-mutants were associated with differential activation of PDK1 and PKC-alpha. Genes showing strong activation in RNA-seq data included negative regulators of RTK/RAF/MAPK signaling along with potential oncogenic effectors including activators of Rac and Rho proteins and the receptor protein-tyrosine phosphatase genes PTPRM and PTPRE. These results corroborate RAF/MAPK signaling as an important therapeutic target in KRAS-mutant lung adenocarcinomas and pinpoint new potential targets.

Published

2016

11. A Rapid and Scalable System for Studying Gene Function in Mice Using Conditional RNA Interference

Author

Lukas E. Dow, Claudio Scuoppo, Kenneth R. Shroyer, Scott W. Lowe, Cornelius Miething, Ross A. Dickins, Matthew Camiolo, Prem K. Premsrirut, Colin D. Malone, Gregory J. Hannon, Johannes Zuber, Raffaella Sordella, Sang Yong Kim, and Scott C. Kogan

Subjects

Lung Neoplasms, Mice, Transgenic, Adenocarcinoma, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, General Biochemistry, Genetics and Molecular Biology, Article, Small hairpin RNA, Mice, RNA interference, microRNA, Gene Knockdown Techniques, Animals, Gene silencing, RNA Processing, Post-Transcriptional, RNA, Small Interfering, Gene, Embryonic Stem Cells, Gene knockdown, Biochemistry, Genetics and Molecular Biology(all), Wnt signaling pathway, Molecular biology, Cell biology, Wnt Proteins, MicroRNAs, RNA Interference, Signal Transduction

Abstract

Summary RNA interference is a powerful tool for studying gene function, however, the reproducible generation of RNAi transgenic mice remains a significant limitation. By combining optimized fluorescence-coupled miR30-based shRNAs with high efficiency ES cell targeting, we developed a fast, scalable pipeline for the production of shRNA transgenic mice. Using this system, we generated eight tet-regulated shRNA transgenic lines targeting Firefly and Renilla luciferases, Oct4 and tumor suppressors p53, p16 INK4a , p19 ARF and APC and demonstrate potent gene silencing and GFP-tracked knockdown in a broad range of tissues in vivo. Further, using an shRNA targeting APC, we illustrate how this approach can identify predicted phenotypes and also unknown functions for a well-studied gene. In addition, through regulated gene silencing we validate APC/Wnt and p19 ARF as potential therapeutic targets in T cell acute lymphoblastic leukemia/lymphoma and lung adenocarcinoma, respectively. This system provides a cost-effective and scalable platform for the production of RNAi transgenic mice targeting any mammalian gene. PaperClip

Published

2011

12. DLC1 is a chromosome 8p tumor suppressor whose loss promotes hepatocellular carcinoma

Author

Stephan Singer, Carlos Cordon-Cardo, Wen Xue, Lars Zender, Florian Kuehnel, Raffaella Sordella, Michael Wigler, Alexander Krasnitz, Robert Lucito, Scott Powers, Linda VanAelst, and Scott W. Lowe

Subjects

Regulation of gene expression, Gene knockdown, RHOA, Tumor suppressor gene, Biology, medicine.disease_cause, medicine.disease, law.invention, law, Hepatocellular carcinoma, Genetics, medicine, Cancer research, biology.protein, Suppressor, DLC1, Carcinogenesis, Developmental Biology

Abstract

Deletions on chromosome 8p are common in human tumors, suggesting that one or more tumor suppressor genes reside in this region. Deleted in Liver Cancer 1 (DLC1) encodes a Rho-GTPase activating protein and is a candidate 8p tumor suppressor. We show that DLC1 knockdown cooperates with Myc to promote hepatocellular carcinoma in mice, and that reintroduction of wild-type DLC1 into hepatoma cells with low DLC1 levels suppresses tumor growth in situ. Cells with reduced DLC1 protein contain increased GTP-bound RhoA, and enforced expression a constitutively activated RhoA allele mimics DLC1 loss in promoting hepatocellular carcinogenesis. Conversely, down-regulation of RhoA selectively inhibits tumor growth of hepatoma cells with disabled DLC1. Our data validate DLC1 as a potent tumor suppressor gene and suggest that its loss creates a dependence on the RhoA pathway that may be targeted therapeutically.

Published

2008

13. Epidermal Growth Factor Receptor Mutants from Human Lung Cancers Exhibit Enhanced Catalytic Activity and Increased Sensitivity to Gefitinib

Author

Daniel A. Haber, Karen S. Anderson, Jeffrey Settleman, Daphne W. Bell, Raffaella Sordella, Youngjoo Kim, Roseann Mulloy, and Audrey Ferrand

Subjects

Cancer Research, Lung Neoplasms, Antineoplastic Agents, Spodoptera, Catalysis, Substrate Specificity, T790M, Gefitinib, Growth factor receptor, Epidermal growth factor, medicine, Animals, Humans, Epidermal growth factor receptor, Kinase activity, Cells, Cultured, biology, Phosphotransferases, ErbB Receptors, Oncology, Drug Resistance, Neoplasm, Quinazolines, Cancer research, biology.protein, Cyclin-dependent kinase 8, Mutant Proteins, Erlotinib, Baculoviridae, medicine.drug

Abstract

Somatic mutations within the epidermal growth factor receptor (EGFR) kinase domain are detected in 10% to 30% of human non–small cell lung cancers and are correlated with striking clinical responses in a subset of patients treated with EGFR kinase inhibitors, such as gefitinib and erlotinib. Cell-based studies suggest that these mutant EGFRs promote increased autophosphorylating activity on a subset of EGFR COOH-terminal tyrosines and the consequent engagement of a subset of downstream effectors. Because EGFR function is regulated at multiple levels in vivo, and it is therefore difficult to assess the direct consequences of these mutations on EGFR enzyme function, we measured EGFR catalytic activity in in vitro kinase assays using purified recombinant proteins corresponding to the cytoplasmic domain of wild-type and two frequently detected EGFR mutants (DelL747-P753insS and L858R). Both mutants exhibit substantially increased autophosphorylating activity relative to wild-type EGFR, and they exhibit distinct reaction kinetics. In addition, the mutant kinases are more sensitive to kinase inhibition by gefitinib, which seems to reflect their increased drug affinity. These findings suggest that the altered signaling properties and drug sensitivity of these EGFR mutants that have been observed in vivo largely result from differences in the catalytic properties of the kinase. In addition, we find that the T790M secondary “drug resistance mutation” of EGFR, which frequently arises in relapsed patients that initially responded to treatment, confers enhanced kinase activity to primary activating EGFR alleles and may, therefore, be oncogenic in some contexts. [Cancer Res 2007;67(5):2325–30]

Published

2007

14. A rapid and tunable method to temporally control Cas9 expression enables the identification of essential genes and the interrogation of functional gene interactions in vitro and in vivo

Author

Stegmeier F, Serif Senturk, Raffaella Sordella, Lloyd C. Trotman, Adam Kepecs, Nitin H. Shirole, Alexander G. Vaughan, Nowak Dd, David A. Tuveson, and Corbo

Subjects

Genetics, Cas9, Recombinase, CRISPR, Identification (biology), Guide RNA, Computational biology, Allele, Biology, Gene, Function (biology)

Abstract

The Cas9/CRISPR system is a powerful tool for studying gene function. Here we describe a method that allows temporal control of Cas9/CRISPER activity based on conditional CAS9 destabilization. We demonstrate that fusing an FKBP12-derived destabilizing domain to Cas9 enables conditional rapid and reversible Cas9 expression in vitro and efficient gene-editing in the presence of a guide RNA. Further, we show that this strategy can be easily adapted to co-express, from the same promoter, DD-Cas9 with any other gene of interest, without the latter being co-modulated. In particular, when co-expressed with inducible Cre-ERT2, our system enables parallel, independent manipulation of alleles targeted by Cas9 and traditional recombinase with single-cell specificity. We anticipate this platform will be used for the systematic identification of essential genes and the interrogation of genes functional interactions.

Published

2015

15. Myc drives Pten/p53-deficient proliferation and metastasis due to Il6-secretion and Akt-suppression via Phlpp2

Author

Serif Senturk, Kaitlin Watrud, Victoria M.-Y. Wang, Muhan Chen, Hyejin Cho, Daniel V. DeMarco, David Ding, Raffaella Sordella, Mireia Castillo-Martin, Tumas Beinortas, David Kleinman, Brian D. Robinson, John E. Wilkinson, Dawid G. Nowak, Christof Fellmann, Carlos Cordon-Cardo, Tali Herzka, and Lloyd C. Trotman

Subjects

Male, STAT3 Transcription Factor, Lung Neoplasms, Genotype, Genes, myc, Cell Communication, Article, Epithelium, Metastasis, Mice, Neoplasms, medicine, Phosphoprotein Phosphatases, PTEN, Animals, Humans, Neoplasm Metastasis, Phosphorylation, STAT3, Protein kinase B, PI3K/AKT/mTOR pathway, Cell Proliferation, Oncogene, biology, Interleukin-6, PTEN Phosphohydrolase, Prostatic Neoplasms, medicine.disease, Oncology, Mutation, biology.protein, Cancer research, Signal transduction, Stromal Cells, Tumor Suppressor Protein p53, Proto-Oncogene Proteins c-akt, Gene Deletion, Protein Binding, Signal Transduction

Abstract

We have recently recapitulated metastasis of human PTEN/TP53–mutant prostate cancer in the mouse using the RapidCaP system. Surprisingly, we found that this metastasis is driven by MYC, and not AKT, activation. Here, we show that cell–cell communication by IL6 drives the AKT–MYC switch through activation of the AKT-suppressing phosphatase PHLPP2, when PTEN and p53 are lost together, but not separately. IL6 then communicates a downstream program of STAT3-mediated MYC activation, which drives cell proliferation. Similarly, in tissues, peak proliferation in Pten/Trp53–mutant primary and metastatic prostate cancer does not correlate with activated AKT, but with STAT3/MYC activation instead. Mechanistically, MYC strongly activates the AKT phosphatase PHLPP2 in primary cells and prostate cancer metastasis. We show genetically that Phlpp2 is essential for dictating the proliferation of MYC-mediated AKT suppression. Collectively, our data reveal competition between two proto-oncogenes, MYC and AKT, which ensnarls the Phlpp2 gene to facilitate MYC-driven prostate cancer metastasis after loss of Pten and Trp53. Significance: Our data identify IL6 detection as a potential causal biomarker for MYC-driven metastasis after loss of PTEN and p53. Second, our finding that MYC then must supersede AKT to drive cell proliferation points to MYC inhibition as a critical part of PI3K pathway therapy in lethal prostate cancer. Cancer Discov; 5(6); 636–51. ©2015 AACR. This article is highlighted in the In This Issue feature, p. 565

Published

2015

16. Amplification of MET may identify a subset of cancers with extreme sensitivity to the selective tyrosine kinase inhibitor PHA-665752

Author

Dennis C. Sgroi, Anne Barmettler, Daphne W. Bell, Ross A. Okimoto, Beth Muir, Woo J. Kim, James G. Christensen, Gromoslaw A. Smolen, Raffaella Sordella, Heidi Archibald, Daniel A. Haber, Jeffrey Settleman, and Gayatry Mohapatra

Subjects

Indoles, medicine.drug_class, medicine.medical_treatment, Antineoplastic Agents, Apoptosis, Biology, Tyrosine-kinase inhibitor, Targeted therapy, Growth factor receptor, Cell Movement, Stomach Neoplasms, Cell Line, Tumor, Proto-Oncogene Proteins, Biomarkers, Tumor, medicine, Humans, Receptors, Growth Factor, Genetic Testing, Sulfones, Multidisciplinary, Oncogene, Gene Amplification, Cancer, Biological Sciences, Protein-Tyrosine Kinases, Proto-Oncogene Proteins c-met, Oncogene Addiction, medicine.disease, Drug Resistance, Neoplasm, Cancer cell, Cancer research, Tyrosine kinase

Abstract

The success of molecular targeted therapy in cancer may depend on the selection of appropriate tumor types whose survival depends on the drug target, so-called “oncogene addiction.” Preclinical approaches to defining drug-responsive subsets are needed if initial clinical trials are to be directed at the most susceptible patient population. Here, we show that gastric cancer cells with high-level stable chromosomal amplification of the growth factor receptor MET are extraordinarily susceptible to the selective inhibitor PHA-665752. Although MET activation has primarily been linked with tumor cell migration and invasiveness, the amplified wild-type MET in these cells is constitutively activated, and its continued signaling is required for cell survival. Treatment with PHA-665752 triggers massive apoptosis in 5 of 5 gastric cancer cell lines with MET amplification but in 0 of 12 without increased gene copy numbers ( P = 0.00016). MET amplification may thus identify a subset of epithelial cancers that are uniquely sensitive to disruption of this pathway and define a patient group that is appropriate for clinical trials of targeted therapy using MET inhibitors.

Published

2006

17. Irreversible inhibitors of the EGF receptor may circumvent acquired resistance to gefitinib

Author

Brian W. Brannigan, Godin-Heymann Nadia G, Kurt J. Isselbacher, Daniel A. Haber, David R. Driscoll, Raffaella Sordella, Kwak Eunice L, Jeffrey Settleman, Thomas J. Lynch, Patricia L. Harris, Ross A. Okimoto, John P. McGinnis, Allan Wissner, Sreenath V. Sharma, Sridhar K. Rabindran, Daphne W. Bell, and Panos Fidias

Subjects

Lung Neoplasms, Receptor, ErbB-2, medicine.drug_class, Immunoblotting, Molecular Sequence Data, Drug Resistance, Tyrosine-kinase inhibitor, Erlotinib Hydrochloride, T790M, Gefitinib, Carcinoma, Non-Small-Cell Lung, Tumor Cells, Cultured, medicine, Humans, Epidermal growth factor receptor, Organic Chemicals, Phosphorylation, neoplasms, Cell Proliferation, Aniline Compounds, Multidisciplinary, Base Sequence, biology, Sequence Analysis, DNA, Biological Sciences, respiratory tract diseases, ErbB Receptors, Mutation, Aminoquinolines, Quinazolines, Quinolines, Cancer research, biology.protein, Erlotinib, Neoplasm Recurrence, Local, Signal transduction, Tyrosine kinase, Signal Transduction, medicine.drug

Abstract

Non-small cell lung cancers (NSCLCs) with activating mutations in the kinase domain of the epidermal growth factor receptor (EGFR) demonstrate dramatic, but transient, responses to the reversible tyrosine kinase inhibitors gefitinib (Iressa) and erlotinib (Tarceva). Some recurrent tumors have a common secondary mutation in the EGFR kinase domain, T790M, conferring drug resistance, but in other cases the mechanism underlying acquired resistance is unknown. In studying multiple sites of recurrent NSCLCs, we detected T790M in only a small percentage of tumor cells. To identify additional mechanisms of acquired resistance to gefitinib, we used NSCLC cells harboring an activating EGFR mutation to generate multiple resistant clonesin vitro. These drug-resistant cells demonstrate continued dependence on EGFR and ERBB2 signaling for their viability and have not acquired secondary EGFR mutations. However, they display increased internalization of ligand-activated EGFR, consistent with altered receptor trafficking. Although gefitinib-resistant clones are cross-resistant to related anilinoquinazolines, they demonstrate sensitivity to a class of irreversible inhibitors of EGFR. These inhibitors also show effective inhibition of signaling by T790M-mutant EGFR and killing of NSCLC cells with the T790M mutation. Both mechanisms of gefitinib resistance are therefore circumvented by irreversible tyrosine kinase inhibitors. Our findings suggest that one of these, HKI-272, may prove highly effective in the treatment of EGFR-mutant NSCLCs, including tumors that have become resistant to gefitinib or erlotinib.

Published

2005

18. Molecular Targeted Therapy of Lung Cancer: EGFR Mutations and Response to EGFR Inhibitors

Author

Godin-Heymann Nadia G, Raffaella Sordella, Thomas J. Lynch, Daniel A. Haber, Jeffrey Settleman, Sreenath V. Sharma, Daphne W. Bell, and E. L. Kwak

Subjects

Male, Models, Molecular, Lung Neoplasms, Antineoplastic Agents, In Vitro Techniques, Biochemistry, Gefitinib, Carcinoma, Non-Small-Cell Lung, Genetics, medicine, Humans, Epidermal growth factor receptor, Lung cancer, Molecular Biology, EGFR inhibitors, Clinical Trials as Topic, biology, business.industry, Gene Amplification, Oncogenes, Oncogene Addiction, medicine.disease, respiratory tract diseases, ErbB Receptors, Drug Resistance, Neoplasm, Mutation, Quinazolines, Cancer research, biology.protein, Female, Erlotinib, business, Tyrosine kinase, Targeted therapy of lung cancer, medicine.drug

Abstract

Somatic mutations within the kinase domain of the epidermal growth factor receptor (EGFR) are present in approximately 10% of non-small-cell lung cancer (NSCLC), with an increased frequency in adenocarcinomas arising in nonsmokers, women, and individuals of Asian ethnicity. These mutations lead to altered downstream signaling by the receptor and appear to define a subset of NSCLC characterized by "oncogene addiction" to the EGFR pathway, which displays dramatic responses to the reversible tyrosine kinase inhibitors gefitinib and erlotinib. The rapid acquisition of drug resistance in most cases, either through mutation of the "gateway" residue in the EGFR kinase domain or by alternative mechanisms, appears to limit the impact on patient survival. Irreversible inhibitors of EGFR display continued effectiveness in vitro against cells with acquired resistance and are now undergoing genotype-directed clinical trials. The molecular and clinical insights derived from targeting EGFR in NSCLC offer important lessons for the broader application of targeted therapeutic agents in solid tumors.

Published

2005

19. An FF Domain-Dependent Protein Interaction Mediates a Signaling Pathway for Growth Factor-Induced Gene Expression

Author

Shweta Hakre, Jeffrey Settleman, Raffaella Sordella, Guang-Chao Chen, Wei Jiang, and Ananda L. Roy

Subjects

GTPase-activating protein, Recombinant Fusion Proteins, Molecular Sequence Data, Active Transport, Cell Nucleus, Gene Expression, GTPase, Biology, DNA-binding protein, Cell Line, Mice, Transcription Factors, TFII, Transcriptional regulation, Animals, Guanine Nucleotide Exchange Factors, Receptors, Platelet-Derived Growth Factor, Amino Acid Sequence, Phosphorylation, Nuclear protein, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Platelet-Derived Growth Factor, Cell Cycle, GTPase-Activating Proteins, Genes, fos, Nuclear Proteins, Cell Biology, Molecular biology, Protein Structure, Tertiary, Cell biology, DNA-Binding Proteins, Repressor Proteins, Tyrosine, Guanine nucleotide exchange factor, Signal transduction, Signal Transduction

Abstract

FF domains are poorly understood protein motifs found in all eukaryotes but in a very small number of proteins. They typically occur in tandem arrays and appear predominantly in splicing and transcription factors. Curiously, they are also present in the p190 family of cytoplasmic Rho GTPase activating proteins (GAPs). We identified the serum-responsive transcriptional regulator TFII-I as a specific interactor with the p190 RhoGAP FF domains. p190 sequesters TFII-I in the cytoplasm via the FF domains, but upon PDGF receptor-mediated phosphorylation of an FF domain, TFII-I is released from p190 and translocates to the nucleus where it can activate transcription of serum-inducible genes including c-fos. These findings reveal a pathway by which mitogens promote gene transcription and indicate a role for FF domains in phosphorylation-mediated signal transduction.

Published

2005

20. Gefitinib-Sensitizing EGFR Mutations in Lung Cancer Activate Anti-Apoptotic Pathways

Author

Raffaella Sordella, Daniel A. Haber, Jeffrey Settleman, and Daphne W. Bell

Subjects

Lung Neoplasms, Cell Survival, medicine.drug_class, Cell, Mutation, Missense, Antineoplastic Agents, Apoptosis, Protein Serine-Threonine Kinases, Transfection, Tyrosine-kinase inhibitor, Cell Line, Mice, Gefitinib, Carcinoma, Non-Small-Cell Lung, Catalytic Domain, Cell Line, Tumor, Proto-Oncogene Proteins, STAT5 Transcription Factor, medicine, Animals, Humans, Epidermal growth factor receptor, Phosphorylation, RNA, Small Interfering, Lung cancer, Protein kinase B, Sequence Deletion, Multidisciplinary, biology, Milk Proteins, medicine.disease, respiratory tract diseases, DNA-Binding Proteins, Enzyme Activation, ErbB Receptors, medicine.anatomical_structure, Protein kinase domain, Mutation, Quinazolines, Trans-Activators, Cancer research, biology.protein, Tyrosine, Mitogen-Activated Protein Kinases, Signal transduction, Proto-Oncogene Proteins c-akt, Signal Transduction, medicine.drug

Abstract

Gefitinib (Iressa, Astra Zeneca Pharmaceuticals) is a tyrosine kinase inhibitor that targets the epidermal growth factor receptor (EGFR) and induces dramatic clinical responses in nonsmall cell lung cancers (NSCLCs) with activating mutations within the EGFR kinase domain. We report that these mutant EGFRs selectively activate Akt and signal transduction and activator of transcription (STAT) signaling pathways, which promote cell survival, but have no effect on extracellular signal–regulated kinase signaling, which induces proliferation. NSCLC cells expressing mutant EGFRs underwent extensive apoptosis after small interfering RNA–mediated knockdown of the mutant EGFR or treatment with pharmacological inhibitors of Akt and STAT signaling and were relatively resistant to apoptosis induced by conventional chemotherapeutic drugs. Thus, mutant EGFRs selectively transduce survival signals on which NSCLCs become dependent; inhibition of those signals by gefitinib may contribute to the drug's efficacy.

Published

2004

21. Activating Mutations in the Epidermal Growth Factor Receptor Underlying Responsiveness of Non–Small-Cell Lung Cancer to Gefitinib

Author

Patricia L. Harris, Raffaella Sordella, David C. Christiani, Frank G. Haluska, Daniel A. Haber, Sarada Gurubhagavatula, Jeffrey G. Supko, Brian W. Brannigan, Sara M. Haserlat, Daphne W. Bell, Jeff Settleman, Ross A. Okimoto, Thomas J. Lynch, and David N. Louis

Subjects

Adult, Male, Heterozygote, Lung Neoplasms, DNA Mutational Analysis, Molecular Sequence Data, Antineoplastic Agents, Adenocarcinoma, Gefitinib, Epidermal growth factor, Carcinoma, Non-Small-Cell Lung, Humans, Medicine, Osimertinib, Amino Acid Sequence, Epidermal growth factor receptor, Aged, Sequence Deletion, EGFR inhibitors, Aged, 80 and over, Base Sequence, Epidermal Growth Factor, biology, business.industry, Genes, erbB-1, General Medicine, Middle Aged, Protein-Tyrosine Kinases, EGFR Tyrosine Kinase Inhibitor Therapy, respiratory tract diseases, ErbB Receptors, Drug Resistance, Neoplasm, Mutation, Quinazolines, Cancer research, biology.protein, Female, Erlotinib, business, Tyrosine kinase, medicine.drug

Abstract

BACKGROUND Most patients with non-small-cell lung cancer have no response to the tyrosine kinase inhibitor gefitinib, which targets the epidermal growth factor receptor (EGFR). However, about 10 percent of patients have a rapid and often dramatic clinical response. The molecular mechanisms underlying sensitivity to gefitinib are unknown. METHODS We searched for mutations in the EGFR gene in primary tumors from patients with non-small-cell lung cancer who had a response to gefitinib, those who did not have a response, and those who had not been exposed to gefitinib. The functional consequences of identified mutations were evaluated after the mutant proteins were expressed in cultured cells. RESULTS Somatic mutations were identified in the tyrosine kinase domain of the EGFR gene in eight of nine patients with gefitinib-responsive lung cancer, as compared with none of the seven patients with no response (P

Published

2004

22. Modulation of CREB Activity by the Rho GTPase Regulates Cell and Organism Size during Mouse Embryonic Development

Author

Kang Quan Hu, Jeffrey Settleman, Raffaella Sordella, Le Zhang, Yoshihiko Yamada, Madeleine R. Brouns, Barry Fine, Stephen F. Matheson, Hiroya Takami, and Marie Classon

Subjects

rho GTP-Binding Proteins, GTPase-activating protein, Cell, Morphogenesis, GTPase, Biology, CREB, Models, Biological, General Biochemistry, Genetics and Molecular Biology, Embryonic and Fetal Development, Mice, medicine, Animals, Guanine Nucleotide Exchange Factors, Insulin, Phosphorylation, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Transcription factor, Cell Size, Mice, Knockout, GTPase-Activating Proteins, Nuclear Proteins, Cell Biology, Phosphoproteins, Molecular biology, Cell biology, DNA-Binding Proteins, Repressor Proteins, Phenotype, medicine.anatomical_structure, Insulin Receptor Substrate Proteins, biology.protein, Body Constitution, Mitogen-Activated Protein Kinases, Signal transduction, Signal Transduction, Developmental Biology

Abstract

Rho GTPases regulate several aspects of tissue morphogenesis during animal development. We found that mice lacking the Rho-inhibitory protein, p190-B RhoGAP, are 30% reduced in size and exhibit developmental defects strikingly similar to those seen in mice lacking the CREB transcription factor. In p190-B RhoGAP-deficient mice, CREB phosphorylation is substantially reduced in embryonic tissues. Embryo-derived cells contain abnormally high levels of active Rho protein, are reduced in size, and exhibit defects in CREB activation upon exposure to insulin or IGF-1. The cell size defect is rescued by expression of constitutively activated CREB, and in wild-type cells, expression of activated Rho or dominant-negative CREB results in reduced cell size. Together, these results suggest that activity of the Rho GTPase modulates a signal from insulin/IGFs to CREB that determines cell size and animal size during embryogenesis.

Published

2002

23. p53Ψ is a transcriptionally inactive p53 isoform able to reprogram cells toward a metastatic-like state

Author

Trushar Rathod, Matthew J. Lazzara, Matthew Camiolo, Zhan Yao, Scott W. Lowe, Alice Nemajerova, Brendon M. Stiles, Adrian R. Krainer, Nasser K. Altorki, Raffaella Sordella, Ute M. Moll, Serif Senturk, Alice M. Walsh, and Luca Cartegni

Subjects

Gene isoform, Epithelial-Mesenchymal Transition, Lung Neoplasms, Mutant, Biology, Lung injury, medicine.disease_cause, Cyclophilins, Mice, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Commentaries, medicine, Protein Isoforms, Animals, Humans, Neoplasm Metastasis, Gene, Mutation, Multidisciplinary, Alternative splicing, Intron, CD24 Antigen, Lung Injury, Cadherins, Genes, p53, Introns, Mitochondria, Alternative Splicing, Hyaluronan Receptors, PNAS Plus, RNA splicing, Cancer research, RNA Splice Sites, Tumor Suppressor Protein p53, Reactive Oxygen Species, Cyclophilin D

Abstract

Although much is known about the underlying mechanisms of p53 activity and regulation, the factors that influence the diversity and duration of p53 responses are not well understood. Here we describe a unique mode of p53 regulation involving alternative splicing of the TP53 gene. We found that the use of an alternative 3' splice site in intron 6 generates a unique p53 isoform, dubbed p53 Psi. At the molecular level, p53. is unable to bind to DNA and does not transactivate canonical p53 target genes. However, like certain p53 gain-of-function mutants, p53. attenuates the expression of E-cadherin, induces expression of markers of the epithelial-mesenchymal transition, and enhances the motility and invasive capacity of cells through a unique mechanism involving the regulation of cyclophilin D activity, a component of the mitochondrial inner pore permeability. Hence, we propose that p53. encodes a separation-of-function isoform that, although lacking canonical p53 tumor suppressor/transcriptional activities, is able to induce a prometastatic program in a transcriptionally independent manner.

Published

2014

24. TAp73 is essential for germ cell adhesion and maturation in testis

Author

Ute M. Moll, Lena Holembowski, Matthias Dobbelstein, Dietmar Riedel, Daniela Kramer, Raffaella Sordella, and Alice Nemajerova

Subjects

Male, endocrine system, Mice, 129 Strain, Transcription, Genetic, Spermiogenesis, Biology, Article, Mice, Testis, Cell Adhesion, medicine, Animals, Spermatogenesis, Cell adhesion, Cell Shape, Research Articles, Cells, Cultured, Blood–testis barrier, Mice, Knockout, Sertoli Cells, urogenital system, Nuclear Proteins, Cell Biology, Sertoli cell, Spermatozoa, Coculture Techniques, Cell biology, Mice, Inbred C57BL, Fertility, Intercellular Junctions, Seminiferous Epithelium, medicine.anatomical_structure, Seminiferous tubule, Gene Expression Regulation, Germ line development, Germ cell

Abstract

The p53 family member TAp73 is required for sperm maturation through promotion of adhesion between developing germ cells and Sertoli nurse cells., A core evolutionary function of the p53 family is to protect the genomic integrity of gametes. However, the role of p73 in the male germ line is unknown. Here, we reveal that TAp73 unexpectedly functions as an adhesion and maturation factor of the seminiferous epithelium orchestrating spermiogenesis. TAp73 knockout (TAp73KO) and p73KO mice, but not ΔNp73KO mice, display a “near-empty seminiferous tubule” phenotype due to massive premature loss of immature germ cells. The cellular basis of this phenotype is defective cell–cell adhesions of developing germ cells to Sertoli nurse cells, with likely secondary degeneration of Sertoli cells, including the blood–testis barrier, which leads to disruption of the adhesive integrity and maturation of the germ epithelium. At the molecular level, TAp73, which is produced in germ cells, controls a coordinated transcriptional program of adhesion- and migration-related proteins including peptidase inhibitors, proteases, receptors, and integrins required for germ–Sertoli cell adhesion and dynamic junctional restructuring. Thus, we propose the testis as a unique organ with strict division of labor among all family members: p63 and p53 safeguard germ line fidelity, whereas TAp73 ensures fertility by enabling sperm maturation.

Published

2014

25. Protein Interaction Mapping in C. elegans Using Proteins Involved in Vulval Development

Author

Gary F. Temple, Nicolas Thierry-Mieg, James L. Hartley, Raffaella Sordella, Marc Vidal, Michael A. Brasch, Albertha J.M. Walhout, and Xiaowei Lu

Subjects

medicine.medical_specialty, Databases, Factual, Genetic Vectors, Molecular cloning, Retinoblastoma Protein, Genome, Vulva, Open Reading Frames, Gene mapping, Two-Hybrid System Techniques, Molecular genetics, medicine, Animals, Cloning, Molecular, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Gene, Genes, Helminth, Organism, Genetics, Multidisciplinary, biology, Helminth Proteins, biology.organism_classification, Repressor Proteins, Phenotype, Mutation, Proteome, Female

Abstract

Protein interaction mapping using large-scale two-hybrid analysis has been proposed as a way to functionally annotate large numbers of uncharacterized proteins predicted by complete genome sequences. This approach was examined in Caenorhabditis elegans , starting with 27 proteins involved in vulval development. The resulting map reveals both known and new potential interactions and provides a functional annotation for approximately 100 uncharacterized gene products. A protein interaction mapping project is now feasible for C. elegans on a genome-wide scale and should contribute to the understanding of molecular mechanisms in this organism and in human diseases.

Published

2000

26. Driving Actin Dynamics under the Influence of Alcohol

Author

Raffaella Sordella and Linda Van Aelst

Subjects

N-Methylaspartate, Alcohol Drinking, Injury control, Accident prevention, Cell, Poison control, macromolecular substances, Biology, Receptors, N-Methyl-D-Aspartate, General Biochemistry, Genetics and Molecular Biology, Mice, Cognition, Actin dynamics, medicine, Animals, Humans, Cytoskeleton, Actin, Neurons, Ethanol, Biochemistry, Genetics and Molecular Biology(all), GTPase-Activating Proteins, fungi, Actin cytoskeleton, Actins, Cell biology, medicine.anatomical_structure

Abstract

The actin cytoskeleton plays a pivotal role in regulating neuronal development and activity, and dysregulation of actin dynamics has been linked to impaired cognitive function. In this issue of Cell Rothenfluh et al. (2006) , and Offenhäuser et al. (2006) show that actin dynamics can also affect the cellular and behavioral responses of flies and mice to alcohol.

Published

2006

27. TGF-beta IL-6 axis mediates selective and adaptive mechanisms of resistance to molecular targeted therapy in lung cancer

Author

Vivek Mittal, Dingcheng Gao, Michaela Schlederer, Lukas Kenner, Christopher Johns, Matthew Camiolo, Nasser K. Altorki, Raffaella Sordella, Zhan Yao, Silvia Fenoglio, Brendon M. Stiles, and Trine Lindsted

Subjects

Lung Neoplasms, medicine.drug_class, Cell Survival, medicine.medical_treatment, Mice, Nude, Biology, Tyrosine-kinase inhibitor, Targeted therapy, Cell Line, Mesoderm, Erlotinib Hydrochloride, Mice, Gefitinib, Cell Movement, Transforming Growth Factor beta, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Animals, Humans, Epidermal growth factor receptor, Protein Kinase Inhibitors, Tumor microenvironment, Multidisciplinary, Base Sequence, Interleukin-6, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Epithelial Cells, Biological Sciences, respiratory tract diseases, ErbB Receptors, Gene Expression Regulation, Neoplastic, Drug Resistance, Neoplasm, Mutation, Cancer research, biology.protein, Quinazolines, RNA Interference, Erlotinib, Tyrosine kinase, medicine.drug

Abstract

The epidermal growth-factor receptor (EGFR) tyrosine kinase inhibitor erlotinib has been proven to be highly effective in the treatment of nonsmall cell lung cancer (NSCLC) harboring oncogenic EGFR mutations. The majority of patients, however, will eventually develop resistance and succumb to the disease. Recent studies have identified secondary mutations in the EGFR (EGFR T790M) and amplification of the N-Methyl-N′-nitro-N-nitroso-guanidine (MNNG) HOS transforming gene (MET) oncogene as two principal mechanisms of acquired resistance. Although they can account for approximately 50% of acquired resistance cases together, in the remaining 50%, the mechanism remains unknown. In NSCLC-derived cell lines and early-stage tumors before erlotinib treatment, we have uncovered the existence of a subpopulation of cells that are intrinsically resistant to erlotinib and display features suggestive of epithelial-to-mesenchymal transition (EMT). We showed that activation of TGF-β–mediated signaling was sufficient to induce these phenotypes. In particular, we determined that an increased TGF-β–dependent IL-6 secretion unleashed previously addicted lung tumor cells from their EGFR dependency. Because IL-6 and TGF-β are prominently produced during inflammatory response, we used a mouse model system to determine whether inflammation might impair erlotinib sensitivity. Indeed, induction of inflammation not only stimulated IL-6 secretion but was sufficient to decrease the tumor response to erlotinib. Our data, thus, argue that both tumor cell-autonomous mechanisms and/or activation of the tumor microenvironment could contribute to primary and acquired erlotinib resistance, and as such, treatments based on EGFR inhibition may not be sufficient for the effective treatment of lung-cancer patients harboring mutant EGFR.

Published

2010

28. Increased Prevalence of EGFR-Mutant Lung Cancer in Women and in East Asian Populations: Analysis of Estrogen-Related Polymorphisms

Author

Daniel A. Haber, Dianne M. Finkelstein, Raffaella Sordella, Tetsuya Mitsudomi, Keitaro Matsuo, Jeff Settleman, Brian W. Brannigan, and Daphne W. Bell

Subjects

Male, Cancer Research, Heterozygote, Lung Neoplasms, Genotype, Biology, Article, Sex Factors, Gene Frequency, Polymorphism (computer science), Carcinoma, Non-Small-Cell Lung, medicine, Prevalence, Humans, Allele, Lung cancer, Allele frequency, Genetics, Polymorphism, Genetic, Cancer, Estrogens, medicine.disease, ErbB Receptors, Oncology, CYP17A1, Mutation, Cancer research, HSD17B1, Female

Abstract

Purpose: Somatic mutations in the epidermal growth factor receptor (EGFR) gene occur in a subset of non–small-cell lung cancer (NSCLC) and are highly predictive of the clinical response to selective EGFR kinase inhibitors. The prevalence of EGFR-mutant NSCLC is appreciably higher in females than in males and in East Asian than in Caucasian populations. We hypothesized that these disparate frequencies may be attributable to underlying genetic modifiers. Given the coincident differences in sex and ethnic origin, we tested allozymatic variants of enzymes involved in estrogen biosynthesis and metabolism, encoded by polymorphic alleles known to differ in frequency between Caucasian and Asian populations, as modifying alleles.Experimental Design: We genotyped nine polymorphisms in the CYP1A1, CYP17A1, CYP19, HSD17B1, COMT, GSTM1, and GSTT1 genes, in a series of 100 Japanese NSCLCs, selected for equal representation of EGFR wild-type (wt) and EGFR-mutant cases, as well as male and female cases. Associations between polymorphic variants and the EGFR genotype and sex of NSCLC cases were examined using Fisher's exact test of significance.Results: Only CYP1A1*2C showed a difference in allele frequency that approached statistical significance. Heterozygotes were underrepresented among EGFR-mutant cases compared with EGFR-wt cases (27% versus 47%, P = 0.08), with a concurrent trend toward overrepresentation of CYP1A1*2CIle/Ile homozygotes among EGFR-mutant cases as compared with EGFR-wt cases (69% versus 51%, P = 0.13).Conclusion: Within the power of this study, our findings suggest that the selected polymorphic variants in the estrogen biosynthesis and metabolism pathways are unlikely to be major genetic modifiers of the prevalence of EGFR-mutant NSCLC.

Published

2008

29. Dialogue between RhoA/ROCK and members of the Par complex in cell polarity

Author

Raffaella Sordella and Linda Van Aelst

Subjects

RHOA, Dendritic spine, animal structures, Polarity (physics), Dendritic Spines, Dendritic spine morphogenesis, GTPase, General Biochemistry, Genetics and Molecular Biology, Cell polarity, Animals, Humans, cdc42 GTP-Binding Protein, Molecular Biology, book, Protein Kinase C, rho-Associated Kinases, biology, Rho GTPases, Developmental cell, Cell Polarity, Cell Biology, Cell biology, Rats, biology.protein, book.journal, Carrier Proteins, Developmental Biology

Abstract

Cell polarity is essential for many biological processes and is regulated by conserved protein complexes, including the Par complex, Rho GTPases, and their regulators. In this issue of Developmental Cell, studies by Nakayama et al. and Zhang and Macara examine how interplay between Rho GTPases and the Par complex control polarized cell migration and dendritic spine morphogenesis in alternate ways.

Published

2008

30. Distinct but overlapping functions for the closely related p190 RhoGAPs in neural development

Author

Stephen F. Matheson, Madeleine R. Brouns, Kang-Quan Hu, Raffaella Sordella, Jeffrey Settleman, and John D. VanderHeide

Subjects

Telencephalon, RHOA, Neurite, Cellular differentiation, Growth Cones, Down-Regulation, GTPase, Biology, Nervous System Malformations, Lateral ventricles, Mice, Developmental Neuroscience, Cell Line, Tumor, Neurites, Animals, Growth cone, Mice, Knockout, Neurons, Stem Cells, Neurogenesis, GTPase-Activating Proteins, Brain, Gene Expression Regulation, Developmental, Cell Differentiation, Cell biology, DNA-Binding Proteins, Repressor Proteins, Neurology, biology.protein, RNA Interference, Neuroscience, Neural development, Signal Transduction

Abstract

The p190 RhoGAPs, p190A and p190B, are highly related GTPase-activating proteins for the Rho GTPases. Rho GTPases and p190A reportedly control various aspects of brain development, and we hypothesized that p190B would be likewise involved in neuronal development. We find that like p190A, p190B is prominently expressed in the developing and adult brain. Unlike p190A, p190B is not abundantly tyrosine phosphorylated. We further demonstrate, using p190B-deficient mice, that p190B is required for normal brain development. Mice lacking p190B display several major defects, including (1) deficits in the formation of major forebrain commissures, including the corpus callosum and anterior commissure, (2) dilation of the lateral ventricles, suggesting inhibition of neurogenesis and/or survival, (3) thinning of the neocortical intermediate zone, suggesting defects in neuronal differentiation and/or axonal outgrowth, and (4) impaired neuronal differentiation. These defects are similar to, but distinct from, those described in p190A-deficient mice. RNA interference-mediated knockdown of neither p190 protein results in significant inhibition of neurite outgrowth in neuroblastoma cells, despite an apparent increase in RhoA activity. We conclude that p190 RhoGAPs control pivotal aspects of neural development, including neuronal differentiation and process outgrowth, and that these effects are mediated by signaling systems that include, but are not limited to, RhoA.

Published

2006

31. Genetic Analysis of Rho Protein Function in Mice

Author

Jeffrey Settleman and Raffaella Sordella

Subjects

medicine.anatomical_structure, Transgene, Cell, Morphogenesis, medicine, Motility, Context (language use), GTPase, Biology, Actin cytoskeleton, Function (biology), Cell biology

Abstract

The Rho small GTPases regulate a variety of cellular functions, including proliferation, differentiation, vesicle trafficking, gene expression, adhesion, and motility. Among their well established essential roles is that of organizing the actin cytoskeleton, and this aspect of Rho GTPase function has led to the identification of important roles for various Rho family GTPases in a variety of actin-dependent cellular processes, including cell shape change, adhesion, and migration. As critical regulators of these actin-mediated processes, the Rho GTPases also function as essential regulators of many developmental processes. The morphogenesis of tissues in all developing multi-cellular organisms requires precise changes in cell shape and cell movements that depend on the various Rho GTPases. This has been observed in studies using sevefigureral different developmental model systems, including flies, worms, frogs, and mice. Here, we review the literature reporting functions for Rho GTPases and their associated signaling components in the context of embryonic development, adult physiology, and pathogenesis. In particular, the focus of the studies described here is on the mouse system, where transgenic and “knockout” strategies have played an especially important role in elucidating the in vivo organization and function of the various Rho signaling pathways.

Published

2005

32. SHP-2 Positively Regulates Myogenesis by Coupling to the Rho GTPase Signaling Pathway

Author

Seda Eminaga, Anton M. Bennett, Mara Fornaro, Jeffrey Settleman, Raffaella Sordella, Maria I. Kontaridis, and Christina Ivins Zito

Subjects

rho GTP-Binding Proteins, RHOA, animal structures, DNA, Complementary, GTPase-activating protein, chemical and pharmacologic phenomena, Protein Tyrosine Phosphatase, Non-Receptor Type 11, Protein tyrosine phosphatase, GTPase, Biology, MyoD, Muscle Development, Models, Biological, Cell Line, Myoblasts, Mice, Animals, Guanine Nucleotide Exchange Factors, Phosphorylation, Molecular Biology, Cell Growth and Development, Mice, Knockout, Base Sequence, Myogenesis, GTPase-Activating Proteins, Intracellular Signaling Peptides and Proteins, Gene Expression Regulation, Developmental, Nuclear Proteins, hemic and immune systems, Cell Biology, Cell biology, DNA-Binding Proteins, Repressor Proteins, embryonic structures, biology.protein, Mutagenesis, Site-Directed, Tyrosine, RNA Interference, Guanine nucleotide exchange factor, biological phenomena, cell phenomena, and immunity, Protein Tyrosine Phosphatases, rhoA GTP-Binding Protein, Signal Transduction

Abstract

Myogenesis is an intricate process that coordinately engages multiple intracellular signaling cascades. The Rho family GTPase RhoA is known to promote myogenesis, however, the mechanisms controlling its regulation in myoblasts have yet to be fully elucidated. We show here that the SH2-containing protein tyrosine phosphatase, SHP-2, functions as an early modulator of myogenesis by regulating RhoA. When MyoD was expressed in fibroblasts lacking functional SHP-2, muscle-specific gene activity was impaired and abolition of SHP-2 expression by RNA interference inhibited muscle differentiation. By using SHP-2 substrate-trapping mutants, we identified p190-B RhoGAP as a SHP-2 substrate. When dephosphorylated, p190-B RhoGAP has been shown to stimulate the activation of RhoA. During myogenesis, p190-B RhoGAP was tyrosyl dephosphorylated concomitant with the stimulation of SHP-2's phosphatase activity. Moreover, overexpression of a catalytically inactive mutant of SHP-2 inhibited p190-B RhoGAP tyrosyl dephosphorylation, RhoA activity, and myogenesis. These observations strongly suggest that SHP-2 dephosphorylates p190-B RhoGAP, leading to the activation of RhoA. Collectively, these data provide a mechanistic basis for RhoA activation in myoblasts and demonstrate that myogenesis is critically regulated by the actions of SHP-2 on the p190-B Rho GAP/RhoA pathway.

Published

2004

33. Bone Marrow Induces STAT3 Pathway Activation in a Model of Disseminated Non-Small Cell Lung Cancer Cells

Author

Brendon M. Stiles, Antonio Coppolino, Raffaella Sordella, Seongho Ryu, Esi Kajno, Christopher J. Agrusa, and Nasser K. Altorki

Subjects

biology, business.industry, medicine.disease, medicine.anatomical_structure, Cancer stem cell, Cancer research, biology.protein, Medicine, Surgery, Bone marrow, Non small cell, business, Lung cancer, STAT3

Published

2014

34. Inherited susceptibility to lung cancer may be associated with the T790M drug resistance mutation in EGFR

Author

Ira Gore, Brian W. Brannigan, Godin-Heymann Nadia G, Ross A. Okimoto, Daniel A. Haber, Daphne W. Bell, Raffaella Sordella, Gayatry Mohapatra, Jeff Settleman, Roseann Mulloy, and Sreenath V. Sharma

Subjects

Male, Threonine, Lung Neoplasms, Somatic cell, Antineoplastic Agents, Biology, medicine.disease_cause, Germline, T790M, Methionine, Germline mutation, Carcinoma, Non-Small-Cell Lung, Genetics, Genetic predisposition, medicine, Humans, Genetic Predisposition to Disease, Lung cancer, Protein Kinase Inhibitors, Germ-Line Mutation, Mutation, Middle Aged, Protein-Tyrosine Kinases, medicine.disease, Pedigree, respiratory tract diseases, ErbB Receptors, Drug Resistance, Neoplasm, Immunology, Cancer research, Female, Tyrosine kinase

Abstract

Somatic activating mutations in EGFR identify a subset of non-small cell lung cancer that respond to tyrosine kinase inhibitors. Acquisition of drug resistance is linked to a specific secondary somatic mutation, EGFR T790M. Here we describe a family with multiple cases of non-small cell lung cancer associated with germline transmission of this mutation. Four of six tumors analyzed showed a secondary somatic activating EGFR mutation, arising in cis with the germline EGFR mutation T790M. These observations implicate altered EGFR signaling in genetic susceptibility to lung cancer.

Published

2005

35. Abstract 5261: PKC alpha is implicated in epithelial to mesenchymal transition and erlotinib resistance in non-small cell lung carcinoma cells

Author

Raffaella Sordella, Mahlet B. Abera, and Marcelo G. Kazanietz

Subjects

Cancer Research, Cell, Vimentin, Biology, medicine.disease, PKC alpha, respiratory tract diseases, Cell biology, medicine.anatomical_structure, Oncology, Cell culture, medicine, Cancer research, biology.protein, Erlotinib, Epithelial–mesenchymal transition, Epidermal growth factor receptor, Lung cancer, medicine.drug

Abstract

Overexpression and mutational activation of the epidermal growth factor receptor (EGFR) play important roles in the pathogenesis of non-small-cell lung cancer (NSCLC). For patients with EGFR activating mutations, EGFR tyrosine kinase inhibitors (TKIs) are given as a primary therapy. However, the majority of these patients eventually develop resistance to TKIs. To address a potential role of PKC isozymes in the resistance to TKIs, we used an isogenic model: the NSCLC H1650 cell line and its erlotinib-resistance derivative H1650-M3. H1650-M3 cells display a mesenchymal-like morphology driven by TGF-β signaling (PNAS 107:15535-15540, 2010). Comparison of the expression of PKC isozymes by Western blot between parental and erlotinib-resistant H1650 cells revealed that the M3 derivative displays remarkably high levels of PKCα and reduced levels of PKCδ. qPCR analysis established that PKCα mRNA levels in H1650-M3 cells are ∼ 40-fold higher than in parental cells. In order to investigate a potential involvement of PKCα in TKI resistance we used RNAi. Upon PKCα depletion H1650-M3 cells display a morphology that is consistent with the epithelial phenotype. Moreover, depletion of PKCα from H1650-M3 cells led to significant changes in the expression of EMT markers. Indeed, mRNA levels of vimentin, Zeb2, SNAIL and TWIST were reduced by more than 50 % in erlotinib-resistant cells when PKCα expression was silenced. Analysis of cell viability in response to erlotinib treatment showed that pretreatment with either the pan-PKC inhibitor GF 109203X or the cPKC inhibitor Gö6976 sensitized H1650-M3 to erlotinib. Furthermore, PKCα RNAi depletion markedly sensitized H1650 cells to the TKI. Therefore, PKCα up-regulation in erlotinib-resistant cells may play an important role in driving the resistance to the drug. Our results also highlight a potential role for PKCα in EMT in lung cancer cells. Citation Format: Mahlet Abera, Raffaella Sordella, Marcelo Kazanietz. PKC alpha is implicated in epithelial to mesenchymal transition and erlotinib resistance in non-small cell lung carcinoma cells. [abstract]. In: Proceedings of the 104th Annual Meeting of the American Association for Cancer Research; 2013 Apr 6-10; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2013;73(8 Suppl):Abstract nr 5261. doi:10.1158/1538-7445.AM2013-5261

Published

2013

36. Modulation of Rho GTPase Signaling Regulates a Switch between Adipogenesis and Myogenesis

Author

Guang-Chao Chen, Jeffrey Settleman, Wei Jiang, Raffaella Sordella, and Marcello Curto

Subjects

rho GTP-Binding Proteins, Cell type, Cell signaling, Regulator, GTPase, Biology, Cell fate determination, General Biochemistry, Genetics and Molecular Biology, Dexamethasone, Receptor, IGF Type 1, Mesoderm, Mice, Fetus, Animals, Guanine Nucleotide Exchange Factors, Enzyme Inhibitors, Insulin-Like Growth Factor I, Muscle, Skeletal, Cells, Cultured, Mice, Knockout, Myogenesis, Biochemistry, Genetics and Molecular Biology(all), Stem Cells, GTPase-Activating Proteins, Nuclear Proteins, Cell Differentiation, Cell biology, Cell Compartmentation, DNA-Binding Proteins, Repressor Proteins, Protein Transport, Adipose Tissue, Adipogenesis, Mutation, Signal transduction, Signal Transduction

Abstract

Mature adipocytes and myocytes are derived from a common mesenchymal precursor. While IGF-1 promotes the differentiation of both cell types, the signaling pathways that specify the distinct cell fates are largely unknown. Here, we show that the Rho GTPase and its regulator, p190-B RhoGAP, are components of a critical switch in the adipogenesis-myogenesis “decision.” Cells derived from embryos lacking p190-B RhoGAP exhibit excessive Rho activity, are defective for adipogenesis, but undergo myogenesis in response to IGF-1 exposure. In vitro, activation of Rho-kinase by Rho inhibits adipogenesis and is required for myogenesis. The activation state of Rho following IGF-1 signaling is determined by the tyrosine-phosphorylation status of p190-B RhoGAP and its resulting subcellular relocalization. Moreover, adjusting Rho activity is sufficient to alter the differentiation program of adipocyte and myocyte precursors. Together, these results identify the Rho GTPase as an essential modulator of IGF-1 signals that direct the adipogenesis-myogenesis cell fate decision.

37. DOCK4, a GTPase Activator, Is Disrupted during Tumorigenesis

Author

Jeff Settleman, Raffaella Sordella, Daniel A. Haber, Doke C.R. Wahrer, Vijay Yajnik, Andrea I. McClatchey, Mako Saito, Robert J. Lake, Daphne W. Bell, Paul A. Reynolds, Charles Paulding, and Sander van den Heuvel

Subjects

Mutant, Molecular Sequence Data, Bone Neoplasms, GTPase, Biology, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Adherens junction, 03 medical and health sciences, Mice, 0302 clinical medicine, Sequence Homology, Nucleic Acid, Genes, Regulator, medicine, Tumor Cells, Cultured, Gene family, Animals, Humans, Gene Silencing, Caenorhabditis elegans, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Osteosarcoma, Sequence Homology, Amino Acid, Biochemistry, Genetics and Molecular Biology(all), GTPase-Activating Proteins, Homozygote, Mice, Mutant Strains, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, Eukaryotic Cells, rap GTP-Binding Proteins, Tumor progression, 030220 oncology & carcinogenesis, Mutation, Cancer research, Rap1, Carcinogenesis, Gene Deletion

Abstract

We used representational difference analysis to identify homozygous genomic deletions selected during tumor progression in the mouse NF2 and TP53 tumor model. We describe a deletion targeting DOCK4, a member of the CDM gene family encoding regulators of small GTPases. DOCK4 specifically activates Rap GTPase, enhancing the formation of adherens junctions. DOCK4 mutations are present in a subset of human cancer cell lines; a recurrent missense mutant identified in human prostate and ovarian cancers encodes a protein that is defective in Rap1 activation. The engulfment defect of C. elegans mutants lacking the CDM gene ced-5 is rescued by wild-type DOCK4, but not by the mutant allele. Expression of wild-type, but not mutant, DOCK4 in mouse osteosarcoma cells with a deletion of the endogenous gene suppresses growth in soft agar and tumor invasion in vivo. DOCK4 therefore encodes a CDM family member that regulates intercellular junctions and is disrupted during tumorigenesis.