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369 results on '"Leto, Thomas L."'

1. Immunogenetics associated with severe coccidioidomycosis

Author

Hsu, Amy P, Korzeniowska, Agnieszka, Aguilar, Cynthia C, Gu, Jingwen, Karlins, Eric, Oler, Andrew J, Chen, Gang, Reynoso, Glennys V, Davis, Joie, Chaput, Alexandria, Peng, Tao, Sun, Ling, Lack, Justin B, Bays, Derek J, Stewart, Ethan R, Waldman, Sarah E, Powell, Daniel A, Donovan, Fariba M, Desai, Jigar V, Pouladi, Nima, Priel, Debra A Long, Yamanaka, Daisuke, Rosenzweig, Sergio D, Niemela, Julie E, Stoddard, Jennifer, Freeman, Alexandra F, Zerbe, Christa S, Kuhns, Douglas B, Lussier, Yves A, Olivier, Kenneth N, Boucher, Richard C, Hickman, Heather D, Frelinger, Jeffrey, Fierer, Joshua, Shubitz, Lisa F, Leto, Thomas L, Thompson, George R, Galgiani, John N, Lionakis, Michail S, and Holland, Steven M

Subjects
Rare Diseases, Prevention, Vaccine Related, Biodefense, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Humans, Tumor Necrosis Factor-alpha, Hydrogen Peroxide, Coccidioidomycosis, Coccidioides, beta-Glucans, Fungal infections, Genetics, Infectious disease, Innate immunity, Population genetics
Abstract

Disseminated coccidioidomycosis (DCM) is caused by Coccidioides, pathogenic fungi endemic to the southwestern United States and Mexico. Illness occurs in approximately 30% of those infected, less than 1% of whom develop disseminated disease. To address why some individuals allow dissemination, we enrolled patients with DCM and performed whole-exome sequencing. In an exploratory set of 67 patients with DCM, 2 had haploinsufficient STAT3 mutations, and defects in β-glucan sensing and response were seen in 34 of 67 cases. Damaging CLEC7A and PLCG2 variants were associated with impaired production of β-glucan-stimulated TNF-α from PBMCs compared with healthy controls. Using ancestry-matched controls, damaging CLEC7A and PLCG2 variants were overrepresented in DCM, including CLEC7A Y238* and PLCG2 R268W. A validation cohort of 111 patients with DCM confirmed the PLCG2 R268W, CLEC7A I223S, and CLEC7A Y238* variants. Stimulation with a DECTIN-1 agonist induced DUOX1/DUOXA1-derived hydrogen peroxide [H2O2] in transfected cells. Heterozygous DUOX1 or DUOXA1 variants that impaired H2O2 production were overrepresented in discovery and validation cohorts. Patients with DCM have impaired β-glucan sensing or response affecting TNF-α and H2O2 production. Impaired Coccidioides recognition and decreased cellular response are associated with disseminated coccidioidomycosis.

Published
2022

2. BTK drives neutrophil activation for sterilizing antifungal immunity

Author

Desai, Jigar V., Zarakas, Marissa A., Wishart, Andrew L., Roschewski, Mark, Aufiero, Mariano A., Donko, Agnes, Wigerblad, Gustaf, Shlezinger, Neta, Plate, Markus, James, Matthew R., Lim, Jean K., Uzel, Gulbu, Bergerson, Jenna R.E., Fuss, Ivan, Cramer, Robert A., Franco, Luis M., Clark, Emily S., Khan, Wasif N., Yamanaka, Daisuke, Chamilos, Georgios, El-Benna, Jamel, Kaplan, Mariana J., Staudt, Louis M., Leto, Thomas L., Holland, Steven M., Wilson, Wyndham H., Hohl, Tobias M., and Lionakis, Michail S.

Subjects
Immune response -- Research, Pharmacology, Experimental, Neutrophils -- Health aspects, Protein tyrosine kinase -- Health aspects, Cellular signal transduction -- Research, Aspergillosis -- Development and progression -- Drug therapy -- Risk factors, Health care industry
Abstract

We describe a previously unappreciated role for Bruton's tyrosine kinase (BTK) in fungal immune surveillance against aspergillosis, an unforeseen complication of BTK inhibitors (BTKi) used for treating B cell lymphoid malignancies. We studied BTK-dependent fungal responses in neutrophils from diverse populations, including healthy donors, patients who were treated with BTKi, and X-linked agammaglobulinemia patients. Upon fungal exposure, BTK was activated in human neutrophils in a TLR2-, Dectin-1-, and Fc[gamma]R-dependent manner, triggering the oxidative burst. BTK inhibition selectively impeded neutrophil-mediated damage to Aspergillus hyphae, primary granule release, and the fungus-induced oxidative burst by abrogating NADPH oxidase subunit [p40.sup.phox] and GTPase RAC2 activation. Moreover, neutrophil-specific Btk deletion in mice enhanced aspergillosis susceptibility by impairing neutrophil function, not recruitment or lifespan. Conversely, GM-CSF partially mitigated these deficits by enhancing [p47.sup.phox] activation. Our findings underline the crucial role of BTK signaling in neutrophils for antifungal immunity and provide a rationale for GM-CSF use to offset these deficits in patients who are susceptible., Introduction Invasive aspergillosis (IA), most often caused by the ubiquitous inhaled mold Aspergillus fumigatus, is an opportunistic fungal infection that exploits numeric or functional neutrophil defects (1-3). IA affects over [...]

Published
2024
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3. Clinical and functional spectrum of RAC2-related immunodeficiency

Author

Donkó, Ágnes, Sharapova, Svetlana O., Kabat, Juraj, Ganesan, Sundar, Hauck, Fabian H., Bergerson, Jenna R. E., Marois, Louis, Abbott, Jordan, Moshous, Despina, Williams, Kelli W., Campbell, Nicholas, Martin, Paul L., Lagresle-Peyrou, Chantal, Trojan, Timothy, Kuzmenko, Natalia B., Deordieva, Ekaterina A., Raykina, Elena V., Abers, Michael S., Abolhassani, Hassan, Barlogis, Vincent, Milla, Carlos, Hall, Geoffrey, Mousallem, Talal, Church, Joseph, Kapoor, Neena, Cros, Guilhem, Chapdelaine, Hugo, Franco-Jarava, Clara, Lopez-Lerma, Ingrid, Miano, Maurizio, Leiding, Jennifer W., Klein, Christoph, Stasia, Marie José, Fischer, Alain, Hsiao, Kuang-Chih, Martelius, Timi, Sepännen, Mikko R. J., Barmettler, Sara, Walter, Jolan, Masmas, Tania N., Mukhina, Anna A., Falcone, Emilia Liana, Kracker, Sven, Shcherbina, Anna, Holland, Steven M., Leto, Thomas L., and Hsu, Amy P.

Published
2024
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6. Development of an improved and specific inhibitor of NADPH oxidase 2 to treat traumatic brain injury

Author

Mason, Hannah, Rai, Ganesha, Kozyr, Arina, De Jonge, Nathaniel, Gliniewicz, Emily, Berg, Lars J., Wald, Gal, Dorrier, Cayce, Henderson, Mark J., Zakharov, Alexey, Dyson, Tristan, Audley, John, Pettinato, Anthony M., Padilha, Elias Carvalho, Shah, Pranav, Xu, Xin, Leto, Thomas L., Simeonov, Anton, Zarember, Kol A., McGavern, Dorian B., and Gallin, John I.

Published
2023
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9. Case Report: Profound newborn leukopenia related to a novel RAC2 variant

Author

Hall, Geoffrey, primary, Donkó, Ágnes, additional, Pratt, Cristina, additional, Kim-Chang, Julie J., additional, Martin, Paul L., additional, Stallings, Amy P., additional, Sleasman, John W., additional, Holland, Steven M., additional, Hsu, Amy P., additional, Leto, Thomas L., additional, and Mousallem, Talal, additional

Published
2024
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13. Dominant activating RAC2 mutation with lymphopenia, immunodeficiency, and cytoskeletal defects

Author

Hsu, Amy P., Donkó, Agnes, Arrington, Megan E., Swamydas, Muthulekha, Fink, Danielle, Das, Arundhoti, Escobedo, Omar, Bonagura, Vincent, Szabolcs, Paul, Steinberg, Harry N., Bergerson, Jenna, Skoskiewicz, Amanda, Makhija, Melanie, Davis, Joie, Foruraghi, Ladan, Palmer, Cindy, Fuleihan, Ramsay L., Church, Joseph A., Bhandoola, Avinash, Lionakis, Michail S., Campbell, Sharon, Leto, Thomas L., Kuhns, Douglas B., and Holland, Steven M.

Published
2019
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14. Spectrin Genes

Author

Winkelmann, John C., primary, Leto, Thomas L., additional, and Forget, Bernard G., additional

Published
2020
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22. Analysis of novel RAC2 variants associated with neutrophil dysfunction, lymphopenia, and primary immunodeficiency

Author

Donko, Agnes P, primary, Sharapova, Svetlana O, additional, Marois, Louis, additional, Winterbourn, Christine, additional, Ashby, Louisa, additional, Martelius, Timi, additional, Seppänen, Mikko, additional, Andreae, Doerthe A., additional, Leiding, Jennifer W., additional, Gauthier, Amélie, additional, Campbell, Nicholas, additional, Ganesan, Sundar, additional, Hsiao, Kuang-Chih, additional, Holland, Steven M., additional, Falcone, Emilia L., additional, Hsu, Amy P., additional, and Leto, Thomas L., additional

Published
2023
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25. Loss of PRDX6 aborts proliferative and migratory signaling in hepatocarcinoma cell lines

Author

Lagal, Daniel J., López-Grueso, María José, Pedrajas, J.R., Leto, Thomas L., Bárcena, José Antonio, and Requejo Aguilar, Raquel

Subjects
Redoxins, Lipid peroxidation, GSK3β, Mitochondrial dysfunction, Epithelial–mesenchymal transition (EMT)
Abstract

Peroxiredoxin 6 (PRDX6), the only mammalian 1-Cys member of the peroxiredoxin family, has peroxidase, phospholipase A2 (PLA2), and lysophosphatidylcholine (LPC) acyltransferase (LPCAT) activities. It has been associated with tumor progression and cancer metastasis, but the mechanisms involved are not clear. We constructed an SNU475 hepatocarcinoma cell line knockout for PRDX6 to study the processes of migration and invasiveness in these mesenchymal cells. They showed lipid peroxidation but inhibition of the NRF2 transcriptional regulator, mitochondrial dysfunction, metabolic reprogramming, an altered cytoskeleton, down-regulation of PCNA, and a diminished growth rate. LPC regulatory action was inhibited, indicating that loss of both the peroxidase and PLA2 activities of PRDX6 are involved. Upstream regulators MYC, ATF4, HNF4A, and HNF4G were activated. Despite AKT activation and GSK3β inhibition, the prosurvival pathway and the SNAI1-induced EMT program were aborted in the absence of PRDX6, as indicated by diminished migration and invasiveness, down-regulation of bottom-line markers of the EMT program, MMP2, cytoskeletal proteins, and triggering of the “cadherin switch”. These changes point to a role for PRDX6 in tumor development and metastasis, so it can be considered a candidate for antitumoral therapies.

Published
2023

50. Unique targeting of cytosolic phospholipase [A.sub.2] to plasma membranes mediated by the NADPH oxidase in phagocytes

Author

Shmelzer, Zeev, Haddad, Nurit, Admon, Ester, Pessach, Itai, Leto, Thomas L., Eitan-Hazan, Zahit, Hershfinkel, Michal, and Levy, Rachel

Subjects
Phospholipases -- Research, Phospholipases -- Physiological aspects, Cytology -- Research, Biological sciences
Abstract

Cytosolic phospholipase [A.sub.2] (cPL[A.sub.2])-generated arachidonic acid (AA) has been shown to be an essential requirement for the activation of NADPH oxidase, in addition to its being the major enzyme involved in the formation of eicosanoid at the nuclear membranes. The mechanism by which cPL[A.sub.2] regulates NADPH oxidase activity is not known, particularly since the NADPH oxidase complex is localized in the plasma membranes of stimulated cells. The present study is the first to demonstrate that upon stimulation cPL[A.sub.2] is transiently recruited to the plasma membranes by a functional NADPH oxidase in neutrophils and in granulocyte-like PLB-985 cells. Coimmunoprecipitation experiments and double labeling immunofluorescence analysis demonstrated the unique colocalization of cPL[A.sub.2] and the NADPH oxidase in plasma membranes of stimulated cells, in correlation with the kinetic burst of superoxide production. A specific affinity in vitro binding was detected between GST-[p47.sup.phox] or GST-[p67.sup.phox] and cPL[A.sub.2] in lysates of stimulated cells. The association between these two enzymes provides the molecular basis for AA released by cPL[A.sub.2] to activate the assembled NADPH oxidase. The ability of cPL[A.sub.2] to regulate two different functions in the same cells (superoxide generation and eicosanoid production) is achieved by a novel dual subcellular localization of cPL[A.sub.2] to different targets.

Published
2003

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