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2. Reversal of malignant ADAR1 splice isoform switching with Rebecsinib

Author

Crews, Leslie A, Ma, Wenxue, Ladel, Luisa, Pham, Jessica, Balaian, Larisa, Steel, S Kathleen, Mondala, Phoebe K, Diep, Raymond H, Wu, Christina N, Mason, Cayla N, van der Werf, Inge, Oliver, Isabelle, Reynoso, Eduardo, Pineda, Gabriel, Whisenant, Thomas C, Wentworth, Peggy, La Clair, James J, Jiang, Qingfei, Burkart, Michael D, and Jamieson, Catriona HM

Subjects
Medical Biotechnology, Biomedical and Clinical Sciences, Stem Cell Research - Nonembryonic - Non-Human, Clinical Research, Rare Diseases, Cancer, Stem Cell Research, Biotechnology, Stem Cell Research - Nonembryonic - Human, Orphan Drug, Genetics, 5.1 Pharmaceuticals, Mice, Animals, Protein Isoforms, Hematopoietic Stem Cells, Adenosine Deaminase, ADAR1, RNA editing, cancer stem cells, cancer therapy, hematopoiesis, leukemia stem cells, myelofibrosis, myeloproliferative neoplasms, secondary AML, splicing, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

Adenosine deaminase acting on RNA1 (ADAR1) preserves genomic integrity by preventing retroviral integration and retrotransposition during stress responses. However, inflammatory-microenvironment-induced ADAR1p110 to p150 splice isoform switching drives cancer stem cell (CSC) generation and therapeutic resistance in 20 malignancies. Previously, predicting and preventing ADAR1p150-mediated malignant RNA editing represented a significant challenge. Thus, we developed lentiviral ADAR1 and splicing reporters for non-invasive detection of splicing-mediated ADAR1 adenosine-to-inosine (A-to-I) RNA editing activation; a quantitative ADAR1p150 intracellular flow cytometric assay; a selective small-molecule inhibitor of splicing-mediated ADAR1 activation, Rebecsinib, which inhibits leukemia stem cell (LSC) self-renewal and prolongs humanized LSC mouse model survival at doses that spare normal hematopoietic stem and progenitor cells (HSPCs); and pre-IND studies showing favorable Rebecsinib toxicokinetic and pharmacodynamic (TK/PD) properties. Together, these results lay the foundation for developing Rebecsinib as a clinical ADAR1p150 antagonist aimed at obviating malignant microenvironment-driven LSC generation.

Published
2023

3. Novel Dormancy Mechanism of Castration Resistance in Bone Metastatic Prostate Cancer Organoids

Author

Lee, Sanghee, Mendoza, Theresa R, Burner, Danielle N, Muldong, Michelle T, Wu, Christina CN, Arreola-Villanueva, Catalina, Zuniga, Abril, Greenburg, Olga, Zhu, William Y, Murtadha, Jamillah, Koutouan, Evodie, Pineda, Naomi, Pham, Hao, Kang, Sung-Gu, Kim, Hyun Tae, Pineda, Gabriel, Lennon, Kathleen M, Cacalano, Nicholas A, Jamieson, Catriona HM, Kane, Christopher J, Kulidjian, Anna A, Gaasterland, Terry, and Jamieson, Christina AM

Subjects
Biochemistry and Cell Biology, Biological Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Microbiology, Stem Cell Research, Prostate Cancer, Urologic Diseases, Genetics, Cancer, Aging, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Good Health and Well Being, Androgens, Angiotensin-Converting Enzyme 2, Animals, Benzamides, Bone Neoplasms, COVID-19, Drug Resistance, Neoplasm, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Humans, Male, Mice, Nitriles, Organoids, Phenylthiohydantoin, Prostatic Neoplasms, Prostatic Neoplasms, Castration-Resistant, Receptors, Virus, SARS-CoV-2, Serine Endopeptidases, Transplantation, Heterologous, Virus Internalization, androgen pathway directed therapy, angiotensin-converting enzyme 2, basal-luminal-like hybrid, bone metastatic prostate cancer, dormant, enzalutamide, patient-derived organoids, patient-derived xenograft, prostate cancer San Diego 1, transmembrane protease serine 2, Other Chemical Sciences, Other Biological Sciences, Chemical Physics, Biochemistry and cell biology, Medicinal and biomolecular chemistry
Abstract

Advanced prostate cancer (PCa) patients with bone metastases are treated with androgen pathway directed therapy (APDT). However, this treatment invariably fails and the cancer becomes castration resistant. To elucidate resistance mechanisms and to provide a more predictive pre-clinical research platform reflecting tumor heterogeneity, we established organoids from a patient-derived xenograft (PDX) model of bone metastatic prostate cancer, PCSD1. APDT-resistant PDX-derived organoids (PDOs) emerged when cultured without androgen or with the anti-androgen, enzalutamide. Transcriptomics revealed up-regulation of neurogenic and steroidogenic genes and down-regulation of DNA repair, cell cycle, circadian pathways and the severe acute respiratory syndrome (SARS)-CoV-2 host viral entry factors, ACE2 and TMPRSS2. Time course analysis of the cell cycle in live cells revealed that enzalutamide induced a gradual transition into a reversible dormant state as shown here for the first time at the single cell level in the context of multi-cellular, 3D living organoids using the Fucci2BL fluorescent live cell cycle tracker system. We show here a new mechanism of castration resistance in which enzalutamide induced dormancy and novel basal-luminal-like cells in bone metastatic prostate cancer organoids. These PDX organoids can be used to develop therapies targeting dormant APDT-resistant cells and host factors required for SARS-CoV-2 viral entry.

Published
2022

4. Inflammation-driven deaminase deregulation fuels human pre-leukemia stem cell evolution

Author

Jiang, Qingfei, Isquith, Jane, Ladel, Luisa, Mark, Adam, Holm, Frida, Mason, Cayla, He, Yudou, Mondala, Phoebe, Oliver, Isabelle, Pham, Jessica, Ma, Wenxue, Reynoso, Eduardo, Ali, Shawn, Morris, Isabella Jamieson, Diep, Raymond, Nasamran, Chanond, Xu, Guorong, Sasik, Roman, Rosenthal, Sara Brin, Birmingham, Amanda, Coso, Sanja, Pineda, Gabriel, Crews, Leslie, Donohoe, Mary E, Venter, J Craig, Whisenant, Thomas, Mesa, Ruben A, Alexandrov, Ludmil B, Fisch, Kathleen M, and Jamieson, Catriona

Subjects
Biological Sciences, Rare Diseases, Genetics, Stem Cell Research - Nonembryonic - Non-Human, Cancer, Stem Cell Research - Nonembryonic - Human, Stem Cell Research, Human Genome, Orphan Drug, Hematology, 2.1 Biological and endogenous factors, Cell Proliferation, Humans, Inflammation, Leukemia, Myeloid, Acute, Neoplastic Stem Cells, Enter keywords here, Biochemistry and Cell Biology, Medical Physiology, Biological sciences
Abstract

Inflammation-dependent base deaminases promote therapeutic resistance in many malignancies. However, their roles in human pre-leukemia stem cell (pre-LSC) evolution to acute myeloid leukemia stem cells (LSCs) had not been elucidated. Comparative whole-genome and whole-transcriptome sequencing analyses of FACS-purified pre-LSCs from myeloproliferative neoplasm (MPN) patients reveal APOBEC3C upregulation, an increased C-to-T mutational burden, and hematopoietic stem and progenitor cell (HSPC) proliferation during progression, which can be recapitulated by lentiviral APOBEC3C overexpression. In pre-LSCs, inflammatory splice isoform overexpression coincides with APOBEC3C upregulation and ADAR1p150-induced A-to-I RNA hyper-editing. Pre-LSC evolution to LSCs is marked by STAT3 editing, STAT3β isoform switching, elevated phospho-STAT3, and increased ADAR1p150 expression, which can be prevented by JAK2/STAT3 inhibition with ruxolitinib or fedratinib or lentiviral ADAR1 shRNA knockdown. Conversely, lentiviral ADAR1p150 expression enhances pre-LSC replating and STAT3 splice isoform switching. Thus, pre-LSC evolution to LSCs is fueled by primate-specific APOBEC3C-induced pre-LSC proliferation and ADAR1-mediated splicing deregulation.

Published
2021

5. Coccidioidomycosis Seroincidence and Risk among Military Personnel, Naval Air Station Lemoore, San Joaquin Valley, California, USA

Author

Ellis, Graham C., Lanteri, Charlotte A., Hsieh, Hsing-Chuan, Graf, Paul C.F., Pineda, Gabriel, Crum-Cianflone, Nancy F., Berjohn, Catherine M., Sanders, Terrel, Maves, Ryan C., and Deiss, Robert

Subjects
San Joaquin Valley -- Health aspects, Statistics, Risk factors, Health aspects, Air bases -- Statistics -- Health aspects, Military personnel -- Statistics -- Health aspects, Coccidioidomycosis -- Statistics -- Risk factors
Abstract

Coccidioidomycosis is an endemic mycosis caused by inhalation of Coccidioides immitis or C. posadasii spores (1). Severe disease is infrequent, and extrapulmonary dissemination occurs in only 1% of diagnosed cases [...]

Published
2022
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6. Hyper-Editing of Cell-Cycle Regulatory and Tumor Suppressor RNA Promotes Malignant Progenitor Propagation

Author

Jiang, Qingfei, Isquith, Jane, Zipeto, Maria Anna, Diep, Raymond H, Pham, Jessica, Santos, Nathan Delos, Reynoso, Eduardo, Chau, Julisia, Leu, Heather, Lazzari, Elisa, Melese, Etienne, Ma, Wenxue, Fang, Rongxin, Minden, Mark, Morris, Sheldon, Ren, Bing, Pineda, Gabriel, Holm, Frida, and Jamieson, Catriona

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biotechnology, Genetics, Stem Cell Research, Hematology, Cancer, Stem Cell Research - Nonembryonic - Non-Human, Rare Diseases, 2.1 Biological and endogenous factors, 3' Untranslated Regions, Adenosine Deaminase, Animals, Blast Crisis, Cell Cycle, Cyclin-Dependent Kinase Inhibitor p21, Enhancer of Zeste Homolog 2 Protein, Female, Gene Editing, Gene Expression Regulation, Neoplastic, Gene Regulatory Networks, HEK293 Cells, Humans, K562 Cells, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Male, Mice, MicroRNAs, Neoplasm Transplantation, Proto-Oncogene Proteins c-mdm2, RNA-Binding Proteins, 3′ UTR, ADAR1, RNA hyper-editing, cancer stem cell, cell cycle, chronic myeloid leukemia, epitranscriptome, leukemia, microRNAs, progenitors, self-renewal, Neurosciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

Adenosine deaminase associated with RNA1 (ADAR1) deregulation contributes to therapeutic resistance in many malignancies. Here we show that ADAR1-induced hyper-editing in normal human hematopoietic progenitors impairs miR-26a maturation, which represses CDKN1A expression indirectly via EZH2, thereby accelerating cell-cycle transit. However, in blast crisis chronic myeloid leukemia progenitors, loss of EZH2 expression and increased CDKN1A oppose cell-cycle transit. Moreover, A-to-I editing of both the MDM2 regulatory microRNA and its binding site within the 3' UTR region stabilizes MDM2 transcripts, thereby enhancing blast crisis progenitor propagation. These data reveal a dual mechanism governing malignant transformation of progenitors that is predicated on hyper-editing of cell-cycle-regulatory miRNAs and the 3' UTR binding site of tumor suppressor miRNAs.

Published
2019

7. Alu-dependent RNA editing of GLI1 promotes malignant regeneration in multiple myeloma.

Author

Lazzari, Elisa, Mondala, Phoebe K, Santos, Nathaniel Delos, Miller, Amber C, Pineda, Gabriel, Jiang, Qingfei, Leu, Heather, Ali, Shawn A, Ganesan, Anusha-Preethi, Wu, Christina N, Costello, Caitlin, Minden, Mark, Chiaramonte, Raffaella, Stewart, A Keith, Crews, Leslie A, and Jamieson, Catriona HM

Subjects
Animals, Humans, Mice, Multiple Myeloma, Neoplasm Recurrence, Local, Disease Progression, Adenosine Deaminase, RNA-Binding Proteins, RNA, Messenger, Prognosis, Case-Control Studies, Neoplasm Transplantation, RNA Editing, Drug Resistance, Neoplasm, Adult, Aged, Middle Aged, Female, Male, Gene Knockdown Techniques, In Vitro Techniques, Zinc Finger Protein GLI1, Neoplasm Recurrence, Local, RNA, Messenger, Drug Resistance, Neoplasm
Abstract

Despite novel therapies, relapse of multiple myeloma (MM) is virtually inevitable. Amplification of chromosome 1q, which harbors the inflammation-responsive RNA editase adenosine deaminase acting on RNA (ADAR)1 gene, occurs in 30-50% of MM patients and portends a poor prognosis. Since adenosine-to-inosine RNA editing has recently emerged as a driver of cancer progression, genomic amplification combined with inflammatory cytokine activation of ADAR1 could stimulate MM progression and therapeutic resistance. Here, we report that high ADAR1 RNA expression correlates with reduced patient survival rates in the MMRF CoMMpass data set. Expression of wild-type, but not mutant, ADAR1 enhances Alu-dependent editing and transcriptional activity of GLI1, a Hedgehog (Hh) pathway transcriptional activator and self-renewal agonist, and promotes immunomodulatory drug resistance in vitro. Finally, ADAR1 knockdown reduces regeneration of high-risk MM in serially transplantable patient-derived xenografts. These data demonstrate that ADAR1 promotes malignant regeneration of MM and if selectively inhibited may obviate progression and relapse.

Published
2017

8. ADAR1 Activation Drives Leukemia Stem Cell Self-Renewal by Impairing Let-7 Biogenesis

Author

Zipeto, Maria Anna, Court, Angela C, Sadarangani, Anil, Santos, Nathaniel P Delos, Balaian, Larisa, Chun, Hye-Jung, Pineda, Gabriel, Morris, Sheldon R, Mason, Cayla N, Geron, Ifat, Barrett, Christian, Goff, Daniel J, Wall, Russell, Pellecchia, Maurizio, Minden, Mark, Frazer, Kelly A, Marra, Marco A, Crews, Leslie A, Jiang, Qingfei, and Jamieson, Catriona HM

Subjects
Medical Biotechnology, Biomedical and Clinical Sciences, Hematology, Biotechnology, Stem Cell Research - Nonembryonic - Human, Stem Cell Research - Nonembryonic - Non-Human, Cancer, Rare Diseases, Stem Cell Research, Genetics, 2.1 Biological and endogenous factors, Adenosine Deaminase, Animals, Base Sequence, Cell Self Renewal, Fusion Proteins, bcr-abl, Gene Expression Regulation, Leukemic, Janus Kinase 2, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Mice, MicroRNAs, Neoplastic Stem Cells, RNA Editing, RNA-Binding Proteins, Signal Transduction, Biological Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

Post-transcriptional adenosine-to-inosine RNA editing mediated by adenosine deaminase acting on RNA1 (ADAR1) promotes cancer progression and therapeutic resistance. However, ADAR1 editase-dependent mechanisms governing leukemia stem cell (LSC) generation have not been elucidated. In blast crisis chronic myeloid leukemia (BC CML), we show that increased JAK2 signaling and BCR-ABL1 amplification activate ADAR1. In a humanized BC CML mouse model, combined JAK2 and BCR-ABL1 inhibition prevents LSC self-renewal commensurate with ADAR1 downregulation. Lentiviral ADAR1 wild-type, but not an editing-defective ADAR1(E912A) mutant, induces self-renewal gene expression and impairs biogenesis of stem cell regulatory let-7 microRNAs. Combined RNA sequencing, qRT-PCR, CLIP-ADAR1, and pri-let-7 mutagenesis data suggest that ADAR1 promotes LSC generation via let-7 pri-microRNA editing and LIN28B upregulation. A small-molecule tool compound antagonizes ADAR1's effect on LSC self-renewal in stromal co-cultures and restores let-7 biogenesis. Thus, ADAR1 activation represents a unique therapeutic vulnerability in LSCs with active JAK2 signaling.

Published
2016

9. Tracking of Normal and Malignant Progenitor Cell Cycle Transit in a Defined Niche.

Author

Pineda, Gabriel, Lennon, Kathleen M, Delos Santos, Nathaniel P, Lambert-Fliszar, Florence, Riso, Gennarina L, Lazzari, Elisa, Marra, Marco A, Morris, Sheldon, Sakaue-Sawano, Asako, Miyawaki, Atsushi, and Jamieson, Catriona HM

Subjects
Cell Line, Humans, Microscopy, Confocal, Coculture Techniques, Gene Expression Profiling, Sequence Analysis, RNA, Cell Cycle, Gene Expression Regulation, Neoplastic, Drug Resistance, Neoplasm, Kinetics, Neoplastic Stem Cells, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Stem Cell Niche, Time-Lapse Imaging, Microscopy, Confocal, Sequence Analysis, RNA, Gene Expression Regulation, Neoplastic, Drug Resistance, Neoplasm, Leukemia, Myelogenous, Chronic, BCR-ABL Positive
Abstract

While implicated in therapeutic resistance, malignant progenitor cell cycle kinetics have been difficult to quantify in real-time. We developed an efficient lentiviral bicistronic fluorescent, ubiquitination-based cell cycle indicator reporter (Fucci2BL) to image live single progenitors on a defined niche coupled with cell cycle gene expression analysis. We have identified key differences in cell cycle regulatory gene expression and transit times between normal and chronic myeloid leukemia progenitors that may inform cancer stem cell eradication strategies.

Published
2016

10. Proteomics studies of the interactome of RNA polymerase II C-terminal repeated domain

Author

Pineda, Gabriel, Shen, Zhouxin, de Albuquerque, Claudio Ponte, Reynoso, Eduardo, Chen, Jeffrey, Tu, Chi-Chiang, Tang, Wingchung, Briggs, Steve, Zhou, Huilin, and Wang, Jean YJ

Subjects
Biomedical and Clinical Sciences, 1.1 Normal biological development and functioning, Generic health relevance, Amino Acid Sequence, Binding Sites, Cell Cycle Proteins, Gamma Rays, Gene Expression Regulation, HeLa Cells, Humans, Models, Molecular, Molecular Sequence Data, Mutation, Neoplasm Proteins, Peptides, Phosphorylation, Protein Binding, Protein Interaction Domains and Motifs, Protein Structure, Secondary, Proteomics, RNA Polymerase II, Sequence Alignment, Serine, Signal Transduction, Tyrosine, Hela Cells, Biochemistry and Cell Biology, Other Medical and Health Sciences, Bioinformatics, Biomedical and clinical sciences
Abstract

BackgroundEukaryotic RNA polymerase II contains a C-terminal repeated domain (CTD) consisting of 52 consensus heptad repeats of Y1S2P3T4S5P6S7 that mediate interactions with many cellular proteins to regulate transcription elongation, RNA processing and chromatin structure. A number of CTD-binding proteins have been identified and the crystal structures of several protein-CTD complexes have demonstrated considerable conformational flexibility of the heptad repeats in those interactions. Furthermore, phosphorylation of the CTD at tyrosine, serine and threonine residues can regulate the CTD-protein interactions. Although the interactions of CTD with specific proteins have been elucidated at the atomic level, the capacity and specificity of the CTD-interactome in mammalian cells is not yet determined.ResultsA proteomic study was conducted to examine the mammalian CTD-interactome. We utilized six synthetic peptides each consisting of four consensus CTD-repeats with different combinations of serine and tyrosine phosphorylation as affinity-probes to pull-down nuclear proteins from HeLa cells. The pull-down fractions were then analyzed by MUDPIT mass spectrometry, which identified 100 proteins with the majority from the phospho-CTD pull-downs. Proteins pulled-down by serine-phosphorylated CTD-peptides included those containing the previously defined CTD-interacting domain (CID). Using SILAC mass spectrometry, we showed that the in vivo interaction of RNA polymerase II with the mammalian CID-containing RPRD1B is disrupted by CID mutation. We also showed that the CID from four mammalian proteins interacted with pS2-phosphorylated but not pY1pS2-doubly phosphorylated CTD-peptides. However, we also found proteins that were preferentially pulled-down by pY1pS2- or pY1pS5-doubly phosphorylated CTD-peptides. We prepared an antibody against tyrosine phosphorylated CTD and showed that ionizing radiation (IR) induced a transient increase in CTD tyrosine phosphorylation by immunoblotting. Combining SILAC and IMAC purification of phospho-peptides, we found that IR regulated the phosphorylation at four CTD tyrosine sites in different ways.ConclusionUpon phosphorylation, the 52 repeats of the CTD have the capacity to generate a large number of binding sites for cellular proteins. This study confirms previous findings that serine phosphorylation stimulates whereas tyrosine phosphorylation inhibits the protein-binding activity of the CTD. However, tyrosine phosphorylation of the CTD can also stimulate other CTD-protein interactions. The CTD-peptide affinity pull-down method described here can be adopted to survey the mammalian CTD-interactome in various cell types and under different biological conditions.

Published
2015

11. GLI2 inhibition abrogates human leukemia stem cell dormancy

Author

Sadarangani, Anil, Pineda, Gabriel, Lennon, Kathleen M, Chun, Hye-Jung, Shih, Alice, Schairer, Annelie E, Court, Angela C, Goff, Daniel J, Prashad, Sacha L, Geron, Ifat, Wall, Russell, McPherson, John D, Moore, Richard A, Pu, Minya, Bao, Lei, Jackson-Fisher, Amy, Munchhof, Michael, VanArsdale, Todd, Reya, Tannishtha, Morris, Sheldon R, Minden, Mark D, Messer, Karen, Mikkola, Hanna KA, Marra, Marco A, Hudson, Thomas J, and Jamieson, Catriona HM

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Genetics, Stem Cell Research, Orphan Drug, Biotechnology, Cancer, Regenerative Medicine, Hematology, Stem Cell Research - Nonembryonic - Human, Stem Cell Research - Nonembryonic - Non-Human, Rare Diseases, 2.1 Biological and endogenous factors, Animals, Base Sequence, Coculture Techniques, DNA Primers, Fetal Blood, Hedgehog Proteins, Humans, Kruppel-Like Transcription Factors, Leukemia, Mice, Mice, Knockout, Neoplastic Stem Cells, Nuclear Proteins, Reverse Transcriptase Polymerase Chain Reaction, Transcriptome, Zinc Finger Protein Gli2, Leukemia stem cells, Cell cycle, PF-04449913, Sonic hedgehog, Smoothened SMO, GLI2, Medical and Health Sciences, Immunology, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundDormant leukemia stem cells (LSC) promote therapeutic resistance and leukemic progression as a result of unbridled activation of stem cell gene expression programs. Thus, we hypothesized that 1) deregulation of the hedgehog (Hh) stem cell self-renewal and cell cycle regulatory pathway would promote dormant human LSC generation and 2) that PF-04449913, a clinical antagonist of the GLI2 transcriptional activator, smoothened (SMO), would enhance dormant human LSC eradication.MethodsTo test these postulates, whole transcriptome RNA sequencing (RNA-seq), microarray, qRT-PCR, stromal co-culture, confocal fluorescence microscopic, nanoproteomic, serial transplantation and cell cycle analyses were performed on FACS purified normal, chronic phase (CP) chronic myeloid leukemia (CML), blast crisis (BC) phase CML progenitors with or without PF-04449913 treatment.ResultsNotably, RNA-seq analyses revealed that Hh pathway and cell cycle regulatory gene overexpression correlated with leukemic progression. While lentivirally enforced GLI2 expression enhanced leukemic progenitor dormancy in stromal co-cultures, this was not observed with a mutant GLI2 lacking a transactivation domain, suggesting that GLI2 expression prevented cell cycle transit. Selective SMO inhibition with PF-04449913 in humanized stromal co-cultures and LSC xenografts reduced downstream GLI2 protein and cell cycle regulatory gene expression. Moreover, SMO inhibition enhanced cell cycle transit and sensitized BC LSC to tyrosine kinase inhibition in vivo at doses that spare normal HSC.ConclusionIn summary, while GLI2, forms part of a core HH pathway transcriptional regulatory network that promotes human myeloid leukemic progression and dormant LSC generation, selective inhibition with PF-04449913 reduces the dormant LSC burden thereby providing a strong rationale for clinical trials predicated on SMO inhibition in combination with TKIs or chemotherapeutic agents with the ultimate aim of obviating leukemic therapeutic resistance, persistence and progression.

Published
2015

12. Abstract 1789: Pre-clinical studies to advance anti-ROR1 CAR-T cell therapy for metastatic prostate cancer

Author

Jamieson, Christina A.M., primary, Murtadha, Jamillah, additional, Oh, Christopher S., additional, Muldong, Michelle, additional, Koutouan, Evodie, additional, Kim, JOngwook, additional, Etemadfard, Niloofar, additional, Choo, Hae Soo, additional, Sinha, Navyaa, additional, Lee, Sanghee, additional, Wu, Christina, additional, Pineda, Gabriel, additional, Lennon, Kathleen, additional, Willert, Karl, additional, Jamieson, Catriona H., additional, Gaasterland, Terry, additional, Mckay, Rana, additional, Kane, Christopher J., additional, Kipps, Thomas J., additional, Kulidjian, Anna A., additional, Cacalano, Nicholas A., additional, and Prussak, Charles, additional

Published
2023
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13. PD04-10 PRE-CLINICAL STUDIES TO ADVANCE ZILOVERTAMAB-BASED ANTI-ROR1 DUAL SPECIFICITY CAR T-CELL THERAPY FOR METASTATIC PROSTATE CANCER.

Author

Jamieson, Christina, primary, Murtadha, Jamillah, additional, Oh, Christopher S., additional, Muldong, Michelle, additional, Koutouan, Evodie, additional, Kim, JongWook, additional, Etemadfard, Niloofar, additional, Choo, Hae Soo, additional, Sinha, Navyaa, additional, Pineda, Gabriel, additional, Lennon, Kathleen, additional, Wu, Christina N., additional, Kipps, Thomas J., additional, Jamieson, Catriona, additional, Kane, Christopher, additional, Mckay, Rana, additional, Gaasterland, Terry, additional, Kulidjian, Anna, additional, Prussak, Charles, additional, and Cacalano, Nicholas, additional

Published
2023
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14. Supplementary Figure 7 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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15. Supplementary Figure 5 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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16. Supplementary Figure 6 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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17. Supplementary Figure 2 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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18. Supplementary Figure 3 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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19. Table S1 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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20. Data from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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21. Supplementary Figure 1 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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22. Supplementary Figure 4 from Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, primary, Stramucci, Lorenzo, primary, Ellis, Justin J., primary, Harb, Jason G., primary, Neviani, Paolo, primary, Wang, Shuzhen, primary, Eisfeld, Ann-Kathrin, primary, Walker, Christopher J., primary, Zhang, Bin, primary, Srutova, Klara, primary, Gambacorti-Passerini, Carlo, primary, Pineda, Gabriel, primary, Jamieson, Catriona H. M., primary, Stagno, Fabio, primary, Vigneri, Paolo, primary, Nteliopoulos, Georgios, primary, May, Philippa C., primary, Reid, Alistair G., primary, Garzon, Ramiro, primary, Roy, Denis-Claude, primary, Moutuou, Moutuaata M., primary, Guimond, Martin, primary, Hokland, Peter, primary, Deininger, Michael W., primary, Fitzgerald, Garrett, primary, Harman, Christopher, primary, Dazzi, Francesco, primary, Milojkovic, Dragana, primary, Apperley, Jane F., primary, Marcucci, Guido, primary, Qi, Jianfei, primary, Polakova, Katerina Machova, primary, Zou, Ying, primary, Fan, Xiaoxuan, primary, Baer, Maria R., primary, Calabretta, Bruno, primary, and Perrotti, Danilo, primary

Published
2023
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23. Ubiquitination and TRAF signaling

Author

Pineda, Gabriel, Ea, Chee-Kwee, Chen, Zhijian J., Back, Nathan, editor, Cohen, Irun R., editor, Lajtha, Abel, editor, Lambris, John D., editor, Paoletti, Rodolfo, editor, and Wu, Hao, editor

Published
2007
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24. PD07-04 PRE-CLINICAL STUDIES FOR ADVANCING CIRMTUZUMAB-BASED ANTI-ROR1 THERAPIES IN METASTATIC PROSTATE CANCER

Author

Muldong, Michelle, primary, Lee, Sanghee, additional, Mendoza, Theresa, additional, Burner, Danielle, additional, Wu, Christina, additional, Murtadha, Jamillah, additional, Koutouan, Evodie, additional, Pineda, Naomi, additional, Pineda, Gabriel, additional, Lennon, Kathleen, additional, Pham, Hao, additional, Willert, Karl, additional, Cacalano, Nicholas, additional, Jamieson, Catriona, additional, Gaasterland, Terry, additional, Kane, Christopher, additional, Kulidjian, Anna, additional, and Jamieson, Christina, additional

Published
2022
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25. MP33-03 DORMANT CASTRATION-RESISTANT PROSTATE CANCER ORGANOIDS WITH HYBRID BASAL-LUMINAL CELLS AND LOSS OF SARS-COV-2 HOST FACTORS EMERGED UNDER ANDROGEN DEPRIVATION

Author

Jamieson, Christina, primary, Lee, Sanghee, additional, Mendoza, Theresa, additional, Burner, Danielle, additional, Muldong, Michelle, additional, Wu, Christina, additional, Arreola, Catalina, additional, Zuniga, Abril, additional, Murtadha, Jamillah, additional, Pineda, Naomi, additional, Pham, Hao, additional, Koutouan, Evodie, additional, Pineda, Gabriel, additional, Lennon, Kathleen, additional, Cacalano, Nicholas, additional, Jamieson, Catriona, additional, Kane, Christopher, additional, Kulidjian, Anna, additional, and Gaasterland, Terry, additional

Published
2021
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27. Leveraging Synthetic Data to Create Autonomous Driving Perception Systems

Author

Villalonga Pineda, Gabriel and López Peña, Antonio M. (Antonio Manuel)

Subjects
Domain adaptation, Tecnologies, Conducció autónoma, Conducción autónoma, Autonomous driving, Computer vision, Adaptació de domini, Adaptación de dominio, Visión por computador
Abstract

L’anotació manual d’imatges per desenvolupar sistemes basats en visió per computador ha estat un dels punts més problemàtics des que s’utilitza aprenentatge automàtic per a això. Aquesta tesi es centra en aprofitar les dades sintètiques per alleujar el cost de les anotacions manuals en tres tasques de percepció relacionades amb l’assistència a la conducció i la conducció autònoma. En tot moment assumim l’ús de xarxes neuronals convolucionals per al desenvolupament dels nostres models profunds de percepció. La primera tasca planteja el reconeixement de senyals de trànsit, un problema de classificació d’imatges. Assumim que el nombre de classes de senyals de trànsit a reconèixer s’ha d’incrementar sense haver pogut anotar noves imatges amb què realitzar el corresponent reentrenament. Demostrem que aprofitant les dades sintètiques de les noves classes i transformant-les amb una xarxa adversària-generativa (GAN, de les seves sigles en anglès) entrenada amb les classes conegudes (sense usar mostres de les noves classes), és possible reentrenar la xarxa neuronal per classificar tots els senyals en una proporció ~1/4 entre classes noves i conegudes. La segona tasca consisteix en la detecció de vehicles i vianants (objectes) en imatges. En aquest cas, assumim la recepció d’un conjunt d’imatges sense anotar. L’objectiu és anotar automàticament aquestes imatges perquè així es puguin utilitzar posteriorment en l’entrenament del detector d’objectes que desitgem. Per assolir aquest objectiu, vam partir de dades sintètiques anotades i proposem un mètode d’aprenentatge semi-supervisat basat en la idea del co-aprenentatge. A més, utilitzem una GAN per reduir la distància entre els dominis sintètic i real abans d’aplicar el co-aprenentatge. Els nostres resultats quantitatius mostren que el procediment desenvolupat permet anotar el conjunt d’imatges d’entrada amb la precisió suficient per entrenar detectors d’objectes de forma efectiva; és a dir, tan precisos com si les imatges s’haguessin anotat manualment. A la tercera tasca deixem enrere l’espai 2D de les imatges, i ens centrem en processar núvols de punts 3D provinents de sensors LiDAR. El nostre objectiu inicial era desenvolupar un detector d’objectes 3D (vehicles, vianants, ciclistes) entrenat en núvols de punts sintètics estil LiDAR. En el cas de les imatges es podia esperar el problema de canvi de domini degut a les diferències visuals entre les imatges sintètiques i reals. Però, a priori, no esperàvem el mateix en treballar amb núvols de punts LiDAR, ja que es tracta d’informació geomètrica provinent del mostreig actiu del món, sense que l’aparença visual influeixi. No obstant això, a la pràctica, hem vist que també apareixen els problemes d’adaptació de domini. Factors com els paràmetres de mostreig del LiDAR, la configuració dels sensors a bord del vehicle autònom, i l’anotació manual dels objectes 3D, indueixen diferències de domini. A la tesi demostrem aquesta observació mitjançant un exhaustiu conjunt d’experiments amb diferents bases de dades públiques i detectors 3D disponibles. Per tant, en relació amb la tercera tasca, el treball s’ha centrat finalment en el disseny d’una GAN capaç de transformar núvols de punts 3D per portar-los d’un domini a un altre, un tema relativament inexplorat.Finalment, cal esmentar que tots els conjunts de dades sintètiques usats en aquestes tres tasques han estat dissenyats i generats en el context d’aquesta tesi doctoral i es faran públics. En general, considerem que aquesta tesi presenta un avanç en el foment de la utilització de dades sintètiques per al desenvolupament de models profunds de percepció, essencials en el camp de la conducció autònoma. La anotación manual de imágenes para desarrollar sistemas basados en visión por computador ha sido uno de los puntos más problemáticos desde que se utiliza aprendizaje automático para ello. Esta tesis se centra en aprovechar los datos sintéticos para aliviar el coste de las anotaciones manuales en tres tareas de percepción relacionadas con la asistencia a la conducción y la conducción autónoma. En todo momento asumimos el uso de redes neuronales convolucionales para el desarrollo de nuestros modelos profundos de percepción. La primera tarea plantea el reconocimiento de señales de tráfico, un problema de clasificación de imágenes. Asumimos que el número de clases de señales de tráfico a reconocer se debe incrementar sin haber podido anotar nuevas imágenes con las que realizar el correspondiente reentrenamiento. Demostramos que aprovechando los datos sintéticos de las nuevas clases y transformándolas con una red adversaria-generativa (GAN, de sus siglas en inglés) entrenada con las clases conocidas (sin usar muestras de las nuevas clases), es posible reentrenar la red neuronal para clasificar todas las señales en una proporción de ~1/4 entre clases nuevas y conocidas. La segunda tarea consiste en la detección de vehículos y peatones (objetos) en imágenes. En este caso, asumimos la recepción de un conjunto de imágenes sin anotar. El objetivo es anotar automáticamente esas imágenes para que así se puedan utilizar posteriormente en el entrenamiento del detector de objetos que deseemos. Para alcanzar este objetivo, partimos de datos sintéticos anotados y proponemos un método de aprendizaje semi-supervisado basado en la idea del co-aprendizaje. Además, utilizamos una GAN para reducir la distancia entre los dominios sintético y real antes de aplicar el co-aprendizaje. Nuestros resultados cuantitativos muestran que el procedimiento desarrollado permite anotar el conjunto de imágenes de entrada con la precisión suficiente para entrenar detectores de objetos de forma efectiva; es decir, tan precisos como si las imágenes se hubiesen anotado manualmente. En la tercera tarea dejamos atrás el espacio 2D de las imágenes, y nos centramos en procesar nubes de puntos 3D provenientes de sensores LiDAR. Nuestro objetivo inicial era desarrollar un detector de objetos 3D (vehículos, peatones, ciclistas) entrenado en nubes de puntos sintéticos estilo LiDAR. En el caso de las imágenes cabía esperar el problema de cambio de dominio debido a las diferencias visuales entre las imágenes sintéticas y reales. Pero, a priori, no esperábamos lo mismo al trabajar con nubes de puntos LiDAR, ya que se trata de información geométrica proveniente del muestreo activo del mundo, sin que la apariencia visual influya. Sin embargo, en la práctica, hemos visto que también aparecen los problemas de adaptación de dominio. Factores como los parámetros de muestreo del LiDAR, la configuración de los sensores a bordo del vehículo autónomo, y la anotación manual de los objetos 3D, inducen diferencias de dominio. En la tesis demostramos esta observación mediante un exhaustivo conjunto de experimentos con diferentes bases de datos públicas y detectores 3D disponibles. Por tanto, en relación a la tercera tarea, el trabajo se ha centrado finalmente en el diseño de una GAN capaz de transformar nubes de puntos 3D para llevarlas de un dominio a otro, un tema relativamente inexplorado. Finalmente, cabe mencionar que todos los conjuntos de datos sintéticos usados en estas tres tareas han sido diseñados y generados en el contexto de esta tesis doctoral y se harán públicos. En general, consideramos que esta tesis presenta un avance en el fomento de la utilización de datos sintéticos para el desarrollo de modelos profundos de percepción, esenciales en el campo de la conducción autónoma. Manually annotating images to develop vision models has been a major bottleneck since computer vision and machine learning started to walk together. This thesis focuses on leveraging synthetic data to alleviate manual annotation for three perception tasks related to driving assistance and autonomous driving. In all cases, we assume the use of deep convolutional neural networks (CNNs) to develop our perception models. The first task addresses traffic sign recognition (TSR), a kind of multi-class classification problem. We assume that the number of sign classes to be recognized must be suddenly increased without having annotated samples to perform the corresponding TSR CNN re-training. We show that leveraging synthetic samples of such new classes and transforming them by a generative adversarial network (GAN) trained on the known classes (i.e., without using samples from the new classes), it is possible to re-train the TSR CNN to properly classify all the signs for a ~1/4 ratio of new/known sign classes. The second task addresses on-board 2D object detection, focusing on vehicles and pedestrians. In this case, we assume that we receive a set of images without the annotations required to train an object detector, i.e., without object bounding boxes. Therefore, our goal is to self-annotate these images so that they can later be used to train the desired object detector. In order to reach this goal, we leverage from synthetic data and propose a semi-supervised learning approach based on the co-training idea. In fact, we use a GAN to reduce the synth-to-real domain shift before applying co-training. Our quantitative results show that co-training and GAN-based image-to-image translation complement each other up to allow the training of object detectors without manual annotation, and still almost reaching the upper-bound performances of the detectors trained from human annotations. While in previous tasks we focus on vision-based perception, the third task we address focuses on LiDAR pointclouds. Our initial goal was to develop a 3D object detector trained on synthetic LiDAR-style pointclouds. While for images we may expect synth/real-to-real domain shift due to differences in their appearance (e.g. when source and target images come from different camera sensors), we did not expect so for LiDAR pointclouds since these active sensors factor out appearance and provide sampled shapes. However, in practice, we have seen that it can be domain shift even among real-world LiDAR pointclouds. Factors such as the sampling parameters of the LiDARs, the sensor suite configuration on-board the ego-vehicle, and the human annotation of 3D bounding boxes, do induce a domain shift. We show it through comprehensive experiments with different publicly available datasets and 3D detectors. This redirected our goal towards the design of a GAN for pointcloud-to-pointcloud translation, a relatively unexplored topic. Finally, it is worth to mention that all the synthetic datasets used for these three tasks, have been designed and generated in the context of this PhD work and will be publicly released. Overall, we think this PhD presents several steps forward to encourage leveraging synthetic data for developing deep perception models in the field of driving assistance and autonomous driving. Universitat Autònoma de Barcelona. Programa de Doctorat en Informàtica

Published
2021

29. Coccidioidomycosis Seroincidence and Risk among Military Personnel, Naval Air Station Lemoore, San Joaquin Valley, California, USA1.

Author

Ellis, Graham C., Lanteri, Charlotte A., Hsieh, Hsing-Chuan, Graf, Paul C. F., Pineda, Gabriel, Crum-Cianflone, Nancy F., Berjohn, Catherine M., Sanders, Terrel, Maves, Ryan C., and Deiss, Robert

Subjects
COCCIDIOIDOMYCOSIS, DISEASE incidence, RETROSPECTIVE studies, FUNGI, RESEARCH funding, MILITARY personnel
Abstract

We conducted a retrospective cohort study that tested 2,000 US military personnel for Coccidioides antibodies in a disease-endemic region. The overall incidence of seroconversion was 0.5 cases/100 person-years; 12.5% of persons who seroconverted had illnesses requiring medical care. No significant association was found between demographic characteristics and seroconversion or disease. [ABSTRACT FROM AUTHOR]

Published
2022
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30. Hepatitis C virus protease NS3/4A cleaves mitochondrial antiviral signaling protein off the mitochondria to evade innate immunity

Author

Li, Xiao-Dong, Sun, Lijun, Seth, Rashu B., Pineda, Gabriel, and Chen, Zhijian J.

Subjects
Hepatitis C virus -- Diagnosis, Hepatitis C virus -- Development and progression, Tretinoin -- Research, Proteases -- Research, Science and technology
Abstract

Hepatitis C virus (HCV) is a global epidemic manifested mainly by chronic infection. One strategy that HCV employs to establish chronic infection is to use the viral Ser protease NS3/4A to cleave some unknown cellular targets involved in innate immunity. Here we show that the target of NS3/4A is the mitochondrial antiviral signaling protein, MAVS, that activates NF-[kappa]B and IFN regulatory factor 3 to induce type-I interferons. NS3/4A cleaves MAVS at Cys-508, resulting in the dislocation of the N-terminal fragment of MAVS from the mitochondria. Remarkably, a point mutation of MAVS at Cys-508 renders MAVS resistant to cleavage by NS3/4A, thus maintaining the ability of MAVS to induce interferons in HCV replicon cells. NS3/4A binds to and colocalizes with MAVS in the mitochondrial membrane, and it can cleave MAVS directly in vitro. These results provide an example of host-pathogen interaction in which the virus evades innate immunity by dislodging a pivotal antiviral protein from the mitochondria and suggest that blocking the cleavage of MAVS by NS3/4A may be applied to the prevention and treatment of HCV. IFN regulatory factor 3 | NF-[kappa]B | retinoic acid-induced gene / | I[kappa]B kinase

Published
2005

33. Basal-Luminal Hybrid Cells Emerge as a New Dormant, Androgen Pathway Directed Therapy-Resistant Population in Patient-Derived Prostate Cancer Organoids

Author

Lee, Sanghee, primary, Mendoza, Theresa R., additional, Burner, Danielle N., additional, Muldong, Michelle T., additional, Wu, Christina N., additional, Arreola, Catalina, additional, Zuniga, Abril, additional, Miakicheva-Greenburg, Olga, additional, Zhu, William Y., additional, Pineda, Gabriel, additional, Lennon, Kathleen M., additional, Cacalano, Nicholas A., additional, Jamieson, Catriona H.M, additional, Kane, Christopher J., additional, Kulidjian, Anna A., additional, Gaasterland, Terry, additional, and Jamieson, Christina A.M., additional

Published
2021
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34. Abstract 5726: A-to-I RNA deaminase deregulation in pre-leukemia stem cell evolution

Author

Jiang, Qingfei, primary, Holm, Frida, additional, Isquith, Jane, additional, Mark, Adam, additional, Mason, Cayla, additional, Reynoso, Eduardo, additional, Morris, Isabella, additional, Ma, Wenxue, additional, Diep, Raymond, additional, Pham, Jessica, additional, Nasamran, Chanond, additional, Xu, Guorong, additional, Sasik, Roman, additional, Rosenthal, Sara Brin, additional, Birmingham, Amanda, additional, Crews, Leslie, additional, Pineda, Gabriel, additional, Whisenant, Thomas, additional, Fisch, Kathleen, additional, and Jamieson, Catriona, additional

Published
2020
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35. Persistence of Drug-Resistant Leukemic Stem Cells and Impaired NK Cell Immunity in CML Patients Depend on MIR300 Antiproliferative and PP2A-Activating Functions

Author

Silvestri, Giovannino, primary, Trotta, Rossana, additional, Stramucci, Lorenzo, additional, Ellis, Justin J., additional, Harb, Jason G., additional, Neviani, Paolo, additional, Wang, Shuzhen, additional, Eisfeld, Ann-Kathrin, additional, Walker, Christopher J., additional, Zhang, Bin, additional, Srutova, Klara, additional, Gambacorti-Passerini, Carlo, additional, Pineda, Gabriel, additional, Jamieson, Catriona H. M., additional, Stagno, Fabio, additional, Vigneri, Paolo, additional, Nteliopoulos, Georgios, additional, May, Philippa C., additional, Reid, Alistair G., additional, Garzon, Ramiro, additional, Roy, Denis-Claude, additional, Moutuou, Moutuaata M., additional, Guimond, Martin, additional, Hokland, Peter, additional, Deininger, Michael W., additional, Fitzgerald, Garrett, additional, Harman, Christopher, additional, Dazzi, Francesco, additional, Milojkovic, Dragana, additional, Apperley, Jane F., additional, Marcucci, Guido, additional, Qi, Jianfei, additional, Polakova, Katerina Machova, additional, Zou, Ying, additional, Fan, Xiaoxuan, additional, Baer, Maria R., additional, Calabretta, Bruno, additional, and Perrotti, Danilo, additional

Published
2020
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36. BREAKING: SDCCD announces candidates for chancellor (with updates)

Author

Pineda, Gabriel SchneiderVicky

Subjects
College presidents, Community colleges, News, opinion and commentary, Sports and fitness, San Diego Mesa College
Abstract

Byline: Gabriel SchneiderVicky Pineda 11:37 a.m.: Story updated to include quote from Pamela Luster. The San Diego Community College District has chosen its four finalists to replace Constance Carroll as [...]

Published
2021

39. Iconography of the main pre-hispanic deity of death in central Mexico

Author

Espinosa Pineda, Gabriel and Camacho Ángeles, María Montserrat

Subjects
Iconography, Mictlantecuhtli, Death god, Dios de la muerte, Iconografía
Abstract

El dios Mictlantecuhtli es representado con una imagen compuesta por una serie de atributos bien identificados. Sin embargo varios de ellos no han sido satisfactoriamente explicados. En este artículo proponemos una nueva interpretación para algunos de ellos, y subrayamos la corrección de un antiguo error que ha sido reiterado a través de generaciones de investigadores. The death god, Mictlantecuhtli has been pictured as a complex set of very well-known atributes or symbols. Yet, several of them have not been satisfactorily explained. In this paper we propose a new interpretation for some of them, and we stress the correction of an old mistake that has been repeatedly reproduced through generations of researchers.

Published
2018

40. A 14q32.31 Genomic-Imprinted DLK1-DIO3 microrna promotes Leukemogenesis By Inducing Stem Cell Quiescence and Inhibiting NK Cell Anti-Cancer Immunity

Author

Silvestri, Giovannino, primary, Trotta, Rossana, additional, Stramucci, Lorenzo, additional, Wang, Shuzhen, additional, Eisfeld, Ann-Kathrin, additional, Zhang, Bin, additional, Srutova, Klara, additional, Pineda, Gabriel, additional, Jamieson, Catriona, additional, Stagno, Fabio, additional, Vigneri, Paolo, additional, Nteliopoulos, Georgios, additional, Guimond, Martin, additional, Hokland, Peter, additional, Deininger, Michael W., additional, Dazzi, Francesco, additional, Milojkovic, Dragana, additional, Apperley, Jane, additional, Marcucci, Guido, additional, Fan, Xiaoxuan, additional, Baer, Maria R., additional, Calabretta, Bruno, additional, and Perrotti, Danilo, additional

Published
2019
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41. Inflammatory Cytokine Responsive Enzymatic Mutagenesis Fuels Myeloproliferative Neoplasm Pre-Leukemia Stem Cell Evolution

Author

Jamieson, Catriona, primary, Jiang, Qingfei, additional, Holm, Frida, additional, Isquith, Jane, additional, Mark, Adam, additional, Mason, Cayla, additional, Ma, Wenxue, additional, Diep, Raymond H, additional, Pham, Jessica, additional, Reynoso Moreno, Eduardo, additional, Nasamran, Chanond A, additional, Guorong, Xu, additional, Birmingham, Amanda, additional, Crews, Leslie A, additional, Alexandrov, Ludmil, additional, Pineda, Gabriel, additional, Whisenant, Thomas, additional, and Fisch, Kathleen M, additional

Published
2019
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42. The 14q32.31DLK1-DIO3 MIR300 tumor suppressorpromotes leukemogenesis by inducing cancer stem cell quiescence and inhibiting NK cell anti-cancer immunity

Author

Silvestri, Giovannino, primary, Trotta, Rossana, additional, Stramucci, Lorenzo, additional, Ellis, Justin J., additional, Harb, Jason G., additional, Neviani, Paolo, additional, Wang, Shuzhen, additional, Eisfeld, Ann-Kathrin, additional, Walker, Christopher, additional, Zhang, Bin, additional, Srutova, Klara, additional, Gambacorti-Passerini, Carlo, additional, Pineda, Gabriel, additional, Jamieson, Catriona H. M., additional, Stagno, Fabio, additional, Vigneri, Paolo, additional, Nteliopoulos, Georgios, additional, May, Philippa, additional, Reid, Alistair, additional, Garzon, Ramiro, additional, Roy, Denis C., additional, Moutuou, Moutua-Mohamed, additional, Guimond, Martin, additional, Hokland, Peter, additional, Deininger, Michael, additional, Fitzgerald, Garrett, additional, Harman, Christopher, additional, Dazzi, Francesco, additional, Milojkovic, Dragana, additional, Apperley, Jane F., additional, Marcucci, Guido, additional, Qi, Janfei, additional, Machova-Polakova, Katerina, additional, Zou, Ying, additional, Fan, Xiaoxuan, additional, Baer, Maria R., additional, Calabretta, Bruno, additional, and Perrotti, Danilo, additional

Published
2019
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43. El arte funerario en el periodo clásico tardío maya : una interpretación del destino de las entidades anímicas después de la muerte

Author

Solanilla i Demestre, Victòria, Espinosa Pineda, Gabriel, González Austria Noguez, Liliana, Universitat Autònoma de Barcelona. Departament d'Art i de Musicologia., Solanilla i Demestre, Victòria, Espinosa Pineda, Gabriel, González Austria Noguez, Liliana, and Universitat Autònoma de Barcelona. Departament d'Art i de Musicologia.

Abstract

Departament responsable de la tesi: Departament d'Art i de Musicologia., La presente investigación es acerca del arte funerario relacionado con dos tumbas de gobernantes mayas del periodo Clásico Tardío, es decir, entre el 600 y 900 d.C. Los gobernantes son K'ihnich Janaab' Pakal de Palenque en Chiapas y el otro es Yuhkno'm Yihch'aak K'ahk' de Calakmul, en Campeche, ambos sitios en México. El marco teórico de esta investigación es la cosmovisión, es decir, la manera en que una cultura aprehende y explica el universo en un momento determinado y en un lugar determinado de Mesoamérica. La metodología es la integración plástica de todo el arte funerario relacionado con sus tumbas, es decir, la arquitectura, escultura, cerámica, pintura, escritura, joyería, etc. También se aplica el paradigma del Monte Sagrado a cada una de las pirámides que contienen las tumbas de cada uno de los dos estudios de caso. El objetivo principal es entender el concepto de la vida y de la composición de la persona y a partir de ellos acercarnos a comprender el concepto de muerte y qué pasa con las partes intangibles que conformaron a esos gobernantes después de su fallecimiento. Se plantea que las diferentes almas son encapsuladas por los descendientes en objetos que le son afines tanto en sentido material como formal., The present investigation is about the funerary art related with two tombs of Maya rulers of the Late Classic period, that is, between 600 to 900 AD. The rulers are K'ihnich Janaab' Pakal de Palenque in Chiapas and the other is Yuhkno'm Yihch'aak K'ahk' from Calakmul, in Campeche, both sites in Mexico. The theoretical framework of this research is cosmovision, this mean, the way in which a culture apprehends and explains the universe at a specific moment and in a specific place at Mesoamerica, in this case, in maya culture. The methodology is the 'plastic integration' of all the funerary art related to the tombs of two maya rulers: architecture, sculpture, ceramics, painting, writing, jewelry, etc. In this investigation is applied the paradigm of the Sacred Mount to each of the two pyramids that contain the tombs: Temple of the Inscripcions at Palenque and the Structure II at Calakmul. The main objective is to understand the concept of life and the definition of the person and, from there, to get closer to understand the concept of the death and what happens to the intangible parts of the body. It is stated that the different souls are encapsulated by the descendants in objects that are very similar physically and materially.

Published
2019

45. Abstract 4437: Down-modulation of ADAR1-mediated GLI1 editing alters extracellular and immune response genes in multiple myeloma

Author

Crews, Leslie A., primary, Lazzari, Elisa, additional, Mondala, Phoebe K., additional, Santos, Nathaniel Delos, additional, Miller, Amber, additional, Pineda, Gabriel, additional, Jiang, Qingfei, additional, Ganesan, Anusha-Preethi, additional, Wu, Christina, additional, Costello, Caitlin, additional, Minden, Mark, additional, Chiaramonte, Raffaella, additional, Stewart, A. Keith, additional, and Jamieson, Catriona H. M., additional

Published
2018
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46. Abstract 1134: The tumor suppressor activity of miR-300 is detrimental for leukemia development but required for leukemia stem cell maintenance

Author

Silvestri, Giovannino, primary, Stramucci, Lorenzo, additional, Ellis, Justin, additional, Harb, Jason, additional, Neviani, Paolo, additional, Zhang, Bin, additional, Srutova, Klara, additional, Pineda, Gabriel, additional, Jamieson, Catriona, additional, Calabretta, Bruno, additional, Stagno, Fabio, additional, Vigneri, Paolo, additional, Nteliopoulos, Georgios, additional, May, Philippa, additional, Reid, Alistar, additional, Garzon, Ramiro, additional, Roy, Denis-Claude, additional, Guimond, Martin, additional, Hokland, Peter, additional, Deininger, Michael, additional, Fitzgerald, Garrett, additional, Harman, Chris, additional, Dazzi, Francesco, additional, Milojkovic, Dragana, additional, Apperley, Jane, additional, Marcucci, Guido, additional, Qi, Jianfei, additional, Machova-Polakova, Katerina, additional, Fan, Xiaoxuan, additional, Baer, Maria, additional, Trotta, Rossana, additional, and Perrotti, Danilo, additional

Published
2018
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47. Iconografía de la principal deidad prehispánica de la muerte en el centro de México

Author

Espinosa Pineda, Gabriel, Camacho Ángeles, María Montserrat, Espinosa Pineda, Gabriel, and Camacho Ángeles, María Montserrat

Abstract

El dios Mictlantecuhtli es representado con una imagen compuesta por una serie de atributos bien identificados. Sin embargo varios de ellos no han sido satisfactoriamente explicados. En este artículo proponemos una nueva interpretación para algunos de ellos, y subrayamos la corrección de un antiguo error que ha sido reiterado a través de generaciones de investigadores., The death god, Mictlantecuhtli has been pictured as a complex set of very well-known atributes or symbols. Yet, several of them have not been satisfactorily explained. In this paper we propose a new interpretation for some of them, and we stress the correction of an old mistake that has been repeatedly reproduced through generations of researchers.

Published
2018

48. Van der Waals-like isotherms in a confined electrolyte by spherical and cylindrical nanopores

Author

Aguilar-Pineda, Gabriel, Jimenez-Angeles, Felipe, and Lozada-Cassou, Marcelo

Subjects
Electrolytes -- Chemical properties, Liquids -- Density, Liquids -- Research, Chemicals, plastics and rubber industries
Abstract

The article discusses the ionic distribution profiles and the van der Waals-like isotherms present in the electrolytes that are confined by the spherical and cylindrical nanopores. The discussed system is shown to exhibit negative compressibility, where in the pressure behaves in a non-monotonic way on increasing the confinement.

Published
2007

50. Tracking Normal and Chronic Myeloid Leukemia Progenitor Cell Cycle Kinetics in a Defined Niche Using Live Time Lapse Confocal Imaging with Fucci2BL a Novel Lentiviral Bicistronic Reporter

Author

Pineda, Gabriel, primary, Lennon, Kathleen M, additional, Delos-Santos, Nathaniel P, additional, Lambert-Fliszar, Florence, additional, Riso, Gennarina L, additional, Marra, Marco A, additional, Morris, Sheldon, additional, Sakaue-Sawano, Asako, additional, Miyawaki, Atsushi, additional, and Jamieson, Catriona HM, additional

Published
2015
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