Your search keyword '"Carlos E. Zuazo"' showing total 6 results

1. Precision Medicine in a Community Cancer Center: Pan-Cancer DNA/RNA Sequencing of Tumors Reveals Clinically Relevant Gene Fusions

Author

Sourat Darabi, Carlos E. Zuazo, David R. Braxton, Burton L. Eisenberg, and Michael J. Demeure

Subjects

oncogenic fusions, structural variants, cancer genomics, tumor molecular profiling, oncology precision medicine, Biology (General), QH301-705.5

Abstract

Background: Gene fusions occur when two independent genes form a hybrid gene through genomic rearrangements, which often leads to abnormal expression and function of an encoded protein. In hematological and solid cancers, oncogenic fusions may be prognostic, diagnostic, or therapeutic biomarkers. Improved detection and understanding of the functional implications of such fusions may be beneficial for patient care. Methods: We performed a retrospective analysis of our internal genomic database to identify known and novel gene fusions in different solid tumors seen in our community cancer center. We then investigated the clinical implications of the fusions we identified. Results: We identified 420 known oncogenic fusions and 25 unclassified gene fusions across twenty-six different cancer types. Of 420 fusion-positive tumors with known fusions, there were 366 unique gene fusions. Conclusions: About 10% of tumors investigated had oncogenic fusions, which supports the notion that comprehensive molecular profiling, including RNA sequencing, should be provided for patients with advanced cancers.

Published

2023

2. Sleep is Required for Odor Exposure to Consolidate Memory and Remodel Olfactory Synapses

Author

Rashmi Chandra, Fatima Farah, Fernando Muñoz-Lobato, Anirudh Bokka, Kelli L. Benedetti, Chantal Brueggemann, Fatema Saifuddin, Julia M. Miller, Joy Li, Eric Chang, Aruna Varshney, Vanessa Jimenez, Anjana Baradwaj, Cibelle Nassif, Sara Alladin, Kristine Andersen, Veronica Bi, Sarah K. Nordquist, Raymond L. Dunn, Bryan Tsujimoto, Alan Tran, Alex Duong, Rebekka Paisner, Carlos E. Zuazo, Matthew A. Churgin, Christopher Fang-Yen, Martina Bremer, Saul Kato, Noelle Dominique L'Etoile, and Miri K. VanHoven

Subjects

History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering

Published

2022

3. Fibrin is a critical regulator of neutrophil effector function at the oral mucosal barrier

Author

Lakmali M. Silva, Andrew D. Doyle, Teresa Greenwell-Wild, Nicolas Dutzan, Collin L. Tran, Loreto Abusleme, Lih Jiin Juang, Jerry Leung, Elizabeth M. Chun, Andrew G. Lum, Cary S. Agler, Carlos E. Zuazo, Megan Sibree, Priyam Jani, Vardit Kram, Daniel Martin, Kevin Moss, Michail S. Lionakis, Francis J. Castellino, Christian J. Kastrup, Matthew J. Flick, Kimon Divaris, Thomas H. Bugge, and Niki M. Moutsopoulos

Subjects

Male, Fibrin, Multidisciplinary, Neutrophils, Fibrinolysis, Alveolar Bone Loss, Gingiva, Mouth Mucosa, Fibrinogen, Macrophage-1 Antigen, Plasminogen, Extracellular Traps, Polymorphism, Single Nucleotide, Neutrophil Activation, Gastrointestinal Microbiome, Mice, Animals, Humans, Female, Fibrinolysin, RNA-Seq, Periodontitis, Reactive Oxygen Species, Immunity, Mucosal

Abstract

Fibrin gums up the works Plasmin is an abundant plasma protease that cleaves and deactivates the clot-associated protein fibrin. Human deficiencies in plasmin and its inactive proenzyme form, plasminogen (PLG), cause severe inflammation in mucosal tissues such as the mouth and eyes. Silva et al . report that, like humans, mice lacking plasminogen accumulate extravascular fibrin and develop an oral pathology that phenocopies human ligneous periodontitis (see the Perspective by Vicanolo and Hidalgo). The excess fibrin activates neutrophils through the αMβ2 (Mac-1) integrin receptor, which triggers the production of reactive oxygen species and neutrophil extracellular traps. Additionally, certain human polymorphisms in the PLG gene were found to be associated with increased likelihood of developing periodontitis, suggesting that fibrin–neutrophil interactions may be an attractive target for future treatments of this prevalent disease. —STS

Published

2021

4. Sleep is required for odor exposure to consolidate memory and remodel olfactory synapses

Author

Rashmi Chandra, Fatima Farah, Fernando Muñoz-Lobato, Anirudh Bokka, Kelli L. Benedetti, Chantal Brueggemann, Fatema Saifuddin, Julia M. Miller, Joy Li, Eric Chang, Aruna Varshney, Vanessa Jimenez, Anjana Baradwaj, Cibelle Nassif, Sara Alladin, Kristine Andersen, Angel J. Garcia, Veronica Bi, Sarah K. Nordquist, Raymond L. Dunn, Kateryna Tokalenko, Emily Soohoo, Vanessa Garcia, Sukhdeep Kaur, Malcolm Harris, Fabiola Briseno, Brandon Fung, Andrew Bykov, Hazel Guillen, Decklin Byrd, Emma Odisho, Bryan Tsujimoto, Alan Tran, Alex Duong, Kevin C. Daigle, Rebekka Paisner, Carlos E. Zuazo, Matthew A. Churgin, Christopher Fang-Yen, Martina Bremer, Saul Kato, Noëlle D. L’Étoile, and Miri K. VanHoven

Subjects

medicine.anatomical_structure, Odor, Interneuron, Period (gene), medicine, Memory consolidation, Neuron, Biology, Inhibitory postsynaptic potential, Neuroscience, Sleep in non-human animals

Abstract

SUMMARYAnimals with complex nervous systems demand sleep for memory consolidation and synaptic remodeling. Here we show that though theCaenorhabditis elegansnervous system has a limited number of neurons, sleep is necessary for both processes. In addition, it is unclear in any system if sleep collaborates with experience to alter synapses between specific neurons and whether this ultimately affects behavior.C. elegansneurons have defined connections and well-described contributions to behavior. We show that spaced odor-training and post-training sleep induce long-term memory. Memory consolidation, but not acquisition, requires a pair of interneurons, the AIYs, which play a role in odor-seeking behavior. In worms that consolidate memory, both sleep and odor conditioning are required to diminish inhibitory synaptic connections between the AWC chemosensory neurons and the AIYs. Thus, we demonstrate in a living organism that sleep is required for events immediately after training that drive memory consolidation and alter synaptic structures.

Published

2020

5. A dysbiotic microbiome triggers T H 17 cells to mediate oral mucosal immunopathology in mice and humans

Author

Robert J. Morell, Nicolas Dutzan, Alexandra F. Freeman, T. Abe, Steven M. Holland, Carlos E. Zuazo, Teresa Greenwell-Wild, Daniel Martin, C. Hurabielle, Tetsuhiro Kajikawa, Giorgio Trinchieri, Loreto Abusleme, George Hajishengallis, Yasmine Belkaid, Vanja Lazarevic, Laurie Brenchley, Tomoko Ikeuchi, Patricia I. Diaz, and Niki M. Moutsopoulos

Subjects

0301 basic medicine, Periodontitis, business.industry, Cellular differentiation, Cell, Inflammation, 030206 dentistry, General Medicine, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Immunity, Immunopathology, Immunology, medicine, Microbiome, medicine.symptom, business, Homeostasis

Abstract

Periodontitis is one of the most common human inflammatory diseases, yet the mechanisms that drive immunopathology and could be therapeutically targeted are not well defined. Here, we demonstrate an expansion of resident memory T helper 17 (TH17) cells in human periodontitis. Phenocopying humans, TH17 cells expanded in murine experimental periodontitis through local proliferation. Unlike homeostatic oral TH17 cells, which accumulate in a commensal-independent and interleukin-6 (IL-6)-dependent manner, periodontitis-associated expansion of TH17 cells was dependent on the local dysbiotic microbiome and required both IL-6 and IL-23. TH17 cells and associated neutrophil accumulation were necessary for inflammatory tissue destruction in experimental periodontitis. Genetic or pharmacological inhibition of TH17 cell differentiation conferred protection from immunopathology. Studies in a unique patient population with a genetic defect in TH17 cell differentiation established human relevance for our murine experimental studies. In the oral cavity, human TH17 cell defects were associated with diminished periodontal inflammation and bone loss, despite increased prevalence of recurrent oral fungal infections. Our study highlights distinct functions of TH17 cells in oral immunity and inflammation and paves the way to a new targeted therapeutic approach for the treatment of periodontitis.

Published

2018

6. A dysbiotic microbiome triggers T

Author

Nicolas, Dutzan, Tetsuhiro, Kajikawa, Loreto, Abusleme, Teresa, Greenwell-Wild, Carlos E, Zuazo, Tomoko, Ikeuchi, Laurie, Brenchley, Toshiharu, Abe, Charlotte, Hurabielle, Daniel, Martin, Robert J, Morell, Alexandra F, Freeman, Vanja, Lazarevic, Giorgio, Trinchieri, Patricia I, Diaz, Steven M, Holland, Yasmine, Belkaid, George, Hajishengallis, and Niki M, Moutsopoulos

Subjects

Inflammation, Bacteria, Interleukin-6, Neutrophils, Microbiota, Mouth Mucosa, Cell Differentiation, Nuclear Receptor Subfamily 1, Group F, Member 3, Interleukin-23, Article, Mice, Animals, Dysbiosis, Humans, Th17 Cells, Bone Resorption, Periodontitis

Abstract

Periodontitis is one of the most common human inflammatory diseases, yet the mechanisms that drive immunopathology and could be therapeutically targeted are not well defined. Here, we demonstrate an expansion of resident memory Th17 cells in human periodontitis. Phenocopying humans, Th17 cells expanded in murine experimental periodontitis through local proliferation. Unlike homeostatic oral Th17 cells, which accumulate in a commensal-independent and IL-6-dependent manner, periodontitis-associated expansion of Th17 cells was dependent upon the local dysbiotic microbiome and required both IL-6 and IL-23. Importantly, Th17 cells and associated neutrophil accumulation were necessary for inflammatory tissue destruction in experimental periodontitis. Genetic or pharmacological inhibition of Th17 cell differentiation conferred protection from immunopathology. Studies in a unique patient population with a genetic defect in Th17 cell differentiation established human relevance for our murine experimental studies. Indeed, in the oral cavity, human Th17 cell defects were associated with diminished periodontal inflammation and bone loss, despite increased prevalence of recurrent oral fungal infections. Our study highlights distinct functions of Th17 cells in oral immunity and inflammation and paves the way to a new targeted therapeutic approach for the treatment of periodontitis.

Published

2018