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10 results on '"Heredia, Jose E"'

1. Eosinophils secrete IL-4 to facilitate liver regeneration

Author

Goh, YP Sharon, Henderson, Neil C, Heredia, Jose E, Eagle, Alex Red, Odegaard, Justin I, Lehwald, Nadja, Nguyen, Khoa D, Sheppard, Dean, Mukundan, Lata, Locksley, Richard M, and Chawla, Ajay

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Liver Disease, Regenerative Medicine, Digestive Diseases, Chronic Liver Disease and Cirrhosis, Oral and gastrointestinal, Animals, Cell Cycle, Cell Proliferation, Eosinophils, Gene Expression Profiling, Hepatectomy, Hepatocytes, Immunoblotting, Interleukin-4, Interleukin-4 Receptor alpha Subunit, Liver, Liver Regeneration, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Oligonucleotide Array Sequence Analysis, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction, type 2 immunity, tissue injury and repair, inflammation, parasites
Abstract

The liver is a central organ for the synthesis and storage of nutrients, production of serum proteins and hormones, and breakdown of toxins and metabolites. Because the liver is susceptible to toxin- or pathogen-mediated injury, it maintains a remarkable capacity to regenerate by compensatory growth. Specifically, in response to injury, quiescent hepatocytes enter the cell cycle and undergo DNA replication to promote liver regrowth. Despite the elucidation of a number of regenerative factors, the mechanisms by which liver injury triggers hepatocyte proliferation are incompletely understood. We demonstrate here that eosinophils stimulate liver regeneration after partial hepatectomy and toxin-mediated injury. Liver injury results in rapid recruitment of eosinophils, which secrete IL-4 to promote the proliferation of quiescent hepatocytes. Surprisingly, signaling via the IL-4Rα in macrophages, which have been implicated in tissue repair, is dispensable for hepatocyte proliferation and liver regrowth after injury. Instead, IL-4 exerts its proliferative actions via IL-4Rα in hepatocytes. Our findings thus provide a unique mechanism by which eosinophil-derived IL-4 stimulates hepatocyte proliferation in regenerating liver.

Published
2013

2. Type 2 Innate Signals Stimulate Fibro/Adipogenic Progenitors to Facilitate Muscle Regeneration

Author

Heredia, Jose E, Mukundan, Lata, Chen, Francis M, Mueller, Alisa A, Deo, Rahul C, Locksley, Richard M, Rando, Thomas A, and Chawla, Ajay

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Stem Cell Research, Regenerative Medicine, Stem Cell Research - Nonembryonic - Non-Human, Underpinning research, 1.1 Normal biological development and functioning, Musculoskeletal, Animals, Cobra Cardiotoxin Proteins, Eosinophils, Immunity, Innate, Interleukin-13, Interleukin-4, Mice, Muscle Development, Muscle, Skeletal, Myeloid Cells, Receptors, Cell Surface, Regeneration, STAT6 Transcription Factor, Signal Transduction, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

In vertebrates, activation of innate immunity is an early response to injury, implicating it in the regenerative process. However, the mechanisms by which innate signals might regulate stem cell functionality are unknown. Here, we demonstrate that type 2 innate immunity is required for regeneration of skeletal muscle after injury. Muscle damage results in rapid recruitment of eosinophils, which secrete IL-4 to activate the regenerative actions of muscle resident fibro/adipocyte progenitors (FAPs). In FAPs, IL-4/IL-13 signaling serves as a key switch to control their fate and functions. Activation of IL-4/IL-13 signaling promotes proliferation of FAPs to support myogenesis while inhibiting their differentiation into adipocytes. Surprisingly, type 2 cytokine signaling is also required in FAPs, but not in myeloid cells, for rapid clearance of necrotic debris, a process that is necessary for timely and complete regeneration of tissues.

Published
2013

3. TRB3 Links the E3 Ubiquitin Ligase C0P1 to Lipid Metabolism

Author

Qi, Ling, Heredia, Jose E., Altarejos, Judith Y., Screaton, Robert, Goebel, Naomi, Niessen, Sherry, MacLeod, Ian X., Liew, Chong Wee, Kulkarni, Rohit N., Bain, James, Newgard, Christopher, Nelson, Michael, Evans, Ronald M., Yates, John, and Montminy, Marc

Published
2006

5. IL-23 signaling is not an important driver of liver inflammation and fibrosis in murine non-alcoholic steatohepatitis models

Author

Heredia, Jose E., primary, Sorenson, Clara, additional, Flanagan, Sean, additional, Nunez, Victor, additional, Jones, Charles, additional, Martzall, Angela, additional, Leong, Laurie, additional, Martinez, Andres Paler, additional, Scherl, Alexis, additional, Brightbill, Hans D., additional, Ghilardi, Nico, additional, and Ding, Ning, additional

Published
2022
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7. PPAR-δ senses and orchestrates clearance of apoptotic cells to promote tolerance

Author

Mukundan, Lata, Odegaard, Justin I., Morel, Christine R., Heredia, Jose E., Mwangi, Julia W., Ricardo-Gonzalez, Roberto R., Goh, Y.P.Sharon, Eagle, Alex Red, Dunn, Shannon E., Awakuni, Jennifer U.H., Nguyen, Khoa D., Steinman, Lawrence, Michie, Sara A., and Chawla, Ajay

Subjects
Physiological aspects, Research, Genetic aspects, Risk factors, Cell receptors -- Physiological aspects -- Research -- Genetic aspects, Autoimmune diseases -- Risk factors -- Research -- Genetic aspects, Apoptosis -- Research -- Physiological aspects -- Genetic aspects
Abstract

In vertebrates, resident and recruited macrophages are the professional phagocytes that rapidly clear apoptotic cells (1). This functions to protect neighboring cells from the noxious contents of dying cells and [...], Macrophages rapidly engulf apoptotic cells to limit the release of noxious cellular contents and to restrict autoimmune responses against self antigens. Although factors participating in recognition and engulfment of apoptotic cells have been identified, the transcriptional basis for the sensing and the silent disposal of apoptotic cells is unknown. Here we show that peroxisome proliferator-activated receptor-δ (PPAR-δ) is induced when macrophages engulf apoptotic cells and functions as a transcriptional sensor of dying cells. Genetic deletion of PPAR-δ decreases expression of opsonins such as complement component-1qb (C1qb), resulting in impairment of apoptotic cell clearance and reduction in anti-inflammatory cytokine production. This increases autoantibody production and predisposes global and macrophage-specific [Ppard.sup.-/-] mice to autoimmune kidney disease, a phenotype resembling the human disease systemic lupus erythematosus. Thus, PPAR-δ has a pivotal role in orchestrating the timely disposal of apoptotic cells by macrophages, ensuring that tolerance to self is maintained.

Published
2009

8. A TRPA1 inhibitor suppresses neurogenic inflammation and airway contraction for asthma treatment

Author

Balestrini, Alessia, primary, Joseph, Victory, additional, Dourado, Michelle, additional, Reese, Rebecca M., additional, Shields, Shannon D., additional, Rougé, Lionel, additional, Bravo, Daniel D., additional, Chernov-Rogan, Tania, additional, Austin, Cary D., additional, Chen, Huifen, additional, Wang, Lan, additional, Villemure, Elisia, additional, Shore, Daniel G.M., additional, Verma, Vishal A., additional, Hu, Baihua, additional, Chen, Yong, additional, Leong, Laurie, additional, Bjornson, Chris, additional, Hötzel, Kathy, additional, Gogineni, Alvin, additional, Lee, Wyne P., additional, Suto, Eric, additional, Wu, Xiumin, additional, Liu, John, additional, Zhang, Juan, additional, Gandham, Vineela, additional, Wang, Jianyong, additional, Payandeh, Jian, additional, Ciferri, Claudio, additional, Estevez, Alberto, additional, Arthur, Christopher P., additional, Kortmann, Jens, additional, Wong, Ryan L., additional, Heredia, Jose E., additional, Doerr, Jonas, additional, Jung, Min, additional, Vander Heiden, Jason A., additional, Roose-Girma, Merone, additional, Tam, Lucinda, additional, Barck, Kai H., additional, Carano, Richard A.D., additional, Ding, Han Ting, additional, Brillantes, Bobby, additional, Tam, Christine, additional, Yang, Xiaoying, additional, Gao, Simon S., additional, Ly, Justin Q., additional, Liu, Liling, additional, Chen, Liuxi, additional, Liederer, Bianca M., additional, Lin, Joseph H., additional, Magnuson, Steven, additional, Chen, Jun, additional, Hackos, David H., additional, Elstrott, Justin, additional, Rohou, Alexis, additional, Safina, Brian S., additional, Volgraf, Matthew, additional, Bauer, Rebecca N., additional, and Riol-Blanco, Lorena, additional

Published
2021
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9. Eosinophils secrete IL-4 to facilitate liver regeneration.

Author

Sharon Goh, Y. P., Henderson, Neil C., Heredia, Jose E., Red Eagle, Alex, Odegaard, Justin I., Lehwald, Nadja, Nguyen, Khoa D., Sheppard, Dean, Mukundan, Lata, Locksley, Richard M., and Chawla, Ajay

Subjects
EOSINOPHILS, LIVER regeneration, METABOLITES, LIVER cells, HEPATECTOMY
Abstract

The liver is a central organ for the synthesis and storage of nutrients, production of serum proteins and hormones, and breakdown of toxins and metabolites. Because the liver is susceptible to toxin- or pathogen-mediated injury, it maintains a remarkable capacity to regenerate by compensatory growth. Specifically, in response to injury, quiescent hepatocytes enter the cell cycle and undergo DNA replication to promote liver regrowth. Despite the elucidation of a number of regenerative factors, the mechanisms by which liver injury triggers hepatocyte proliferation are incompletely understood. We demonstrate here that eosinophils stimulate liver regeneration after partial hepatectomy and toxin-mediated injury. Liver injury results in rapid recruitment of eosinophils, which secrete IL-4 to promote the proliferation of quiescent hepatocytes. Surprisingly, signaling via the IL-4Rα in macrophages, which have been implicated in tissue repair, is dispensable for hepatocyte proliferation and liver regrowth after injury. Instead, IL-4 exerts its proliferative actions via IL-4Rα in hepatocytes. Our findings thus provide a unique mechanism by which eosinophil-derived IL-4 stimulates hepatocyte proliferation in regenerating liver. [ABSTRACT FROM AUTHOR]

Published
2013
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10. TRB3 Links the E3 Ubiquitin Ligase COPI to Lipid Metabolism.

Author

Ling Qi, Heredia, Jose E., Altarejos, Judith Y., Screaton, Robert, Goebel, Naomi, Niessen, Sherry, MacLeod, Ian X., Chong Wee Liew, Kulkarni, Rohit N., Bain, James, Newgard, Christopher, Nelson, Michael, Evans, Ronald M., Yates, John, and Montminy, Marc

Subjects
*CATECHOLAMINES, *UBIQUITIN, *METABOLISM, *LIGASES, *ADIPOSE tissues, *LIPOLYSIS, *OXIDATION, *PHOSPHORYLATION, *HOMEOSTASIS
Abstract

During fasting, increased concentrations of circulating catecholamines promote the mobilization of Lipid stores from adipose tissue in part by phosphorylating and inactivating acetyl-coenzyme A carboxylase (ACC), the rate-limiting enzyme in fatty acid synthesis. Here, we describe a parallel pathway, in which the pseudokinase TribbLes 3 (TRB3), whose abundance is increased during fasting, stimulates lipolysis by triggering the degradation of ACC in adipose tissue. TRB3 promoted ACC ubiquitination through an association with the E3 ubiquitin ligase constitutive photomorphogenic protein 1 (COP1). Indeed, adipocytes deficient in TRB3 accumulated larger amounts of ACC protein than did wild-type cells. Because transgenic mice expressing TRB3 in adipose tissue are protected from diet-induced obesity due to enhanced fatty add oxidation, these results demonstrate how phosphorylation and ubiquitination pathways converge on a key regulator of lipid metabolism to maintain energy homeostasis. [ABSTRACT FROM AUTHOR]

Published
2006

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