Your search keyword '"Jiujiu Yu"' showing total 5 results

1. Class A scavenger receptor-1/2 facilitates the uptake of bovine milk exosomes in murine bone marrow-derived macrophages and C57BL/6J mice.

Author

Khanam, Afsana, Jiujiu Yu, and Zempleni, Janos

Subjects

*LABORATORY mice, *MACROPHAGES, *EXOSOMES, *BOS, *NONPARAMETRIC statistics, *KNOCKOUT mice

Abstract

Bovine milk exosomes (BMEs) are being explored in drug delivery despite their rapid elimination by macrophages. We aimed at identifying the BME transporter in murine bone marrow-derived macrophages (BMDMs). Fluorophore-labeled BMEs were used in transport studies in BMDMs from C57BL/6J and class A scavenger receptor type 1/2 (CASR-1/2) knockout mice and tissue accumulation in macrophage-depleted C57BL/6J mice. Parametric and nonparametric statistics tests for pairwise and multiple comparisons were used. Chemical inhibitors of phagocytosis by cytochalasin D led to a 69 ± 18% decrease in BME uptake compared with controls (P < 0.05), whereas inhibitors of endocytic pathways other than phagocytosis had a modest effect on uptake (P > 0.05). Inhibitors of class A scavenger receptors (CASRs) including CASR-1/2 caused a 70% decrease in BME uptake (P < 0.05). The uptake of BMEs by BMDMs from CASR-1/2 knockout mice was smaller by 58 ± 23% compared with wild-type controls (P < 0.05). Macrophage depletion by clodronate caused a more than 44% decrease in BME uptake in the spleen and lungs (P < 0.05), whereas the decrease observed in liver was not statistically significant. In conclusion, CASR-1/2 facilitates the uptake of BMEs in BMDMs and C57BL/6J mice. [ABSTRACT FROM AUTHOR]

Published

2021

2. Inflammasome activation leads to Caspase-1–dependent mitochondrial damage and block of mitophagy.

Author

Jiujiu Yu, Nagasu, Hajime, Murakami, Tomohiko, Hoang, Hai, Broderick, Lori, Hoffman, Hal M., and Horng, Tiffany

Subjects

*CELL death, *OLIGOMERIZATION, *REACTIVE oxygen species, *PATHOGENIC microorganisms, *CASPASES, *MELANOMA, *PROTEIN binding

Abstract

Inflammasomes are intracellular sensors that couple detection of pathogens and cellular stress to activation of Caspase-1, and consequent IL-1β and IL-18 maturation and pyroptotic cell death. Here, we show that the absent in melanoma 2 (AIM2) and nucleotide-binding oligomerization domain-like receptor pyrin domain-containing protein 3 (NLRP3) inflammasomes trigger Caspase-1–dependent mitochondrial damage. Caspase-1 activates multiple pathways to precipitate mitochondrial disassembly, resulting in mitochondrial reactive oxygen species (ROS) production, dissipation of mitochondrial membrane potential, mitochondrial permeabilization, and fragmentation of the mitochondrial network. Moreover, Caspase-1 inhibits mitophagy to amplify mitochondrial damage, mediated in part by cleavage of the key mitophagy regulator Parkin. In the absence of Parkin activity, increased mitochondrial damage augments pyroptosis, as indicated by enhanced plasma membrane permeabilization and release of danger-associated molecular patterns (DAMPs). Therefore, like other initiator caspases, Caspase-1 activation by inflammasomes results in mitochondrial damage. [ABSTRACT FROM AUTHOR]

Published

2014

3. Metabolic Characterization of a Sirt5 deficient mouse model.

Author

Jiujiu Yu, Sadhukhan, Sushabhan, Noriega, Lilia G., Moullan, Norman, He, Bin, Weiss, Robert S., Hening Lin, Schoonjans, Kristina, and Auwerx, Johan

Subjects

*MITOCHONDRIA, *DEACETYLASES, *CARBAMOYL compounds, *HOMEOSTASIS, *GERM cells

Abstract

Sirt5, localized in the mitochondria, is a member of sirtuin family of NAD+-dependent deacetylases. Sirt5 was shown to deacetylate and activate carbamoyl phosphate synthase 1. Most recently, Sirt5 was reported to be the predominant protein desuccinylase and demalonylase in the mitochondria because the ablation of Sirt5 enhanced the global succinylation and malonylation of mitochondrial proteins, including many metabolic enzymes. In order to determine the physiological role of Sirt5 in metabolic homeostasis, we generated a germline Sirt5 deficient (Sirt5-/-) mouse model and performed a thorough metabolic characterization of this mouse line. Although a global protein hypersuccinylation and elevated serum ammonia during fasting were observed in our Sirt5-/- mouse model, Sirt5 deficiency did not lead to any overt metabolic abnormalities under either chow or high fat diet conditions. These observations suggest that Sirt5 is likely to be dispensable for the metabolic homeostasis under the basal conditions [ABSTRACT FROM AUTHOR]

Published

2013

4. Akt-mTORC1 signaling regulates Acly to integrate metabolic input to control of macrophage activation.

Author

Covarrubias, Anthony J., Aksoylar, Halil Ibrahim, Jiujiu Yu, Snyder, Nathaniel W., Worth, Andrew J., Iyer, Shankar S., Jiawei Wang, Ben-Sahra, Issam, Byles, Vanessa, Polynne-Stapornkul, Tiffany, Espinosa, Erika C., Lamming, Dudley, Manning, Brendan D., Yijing Zhang, Blair, Ian A., and Horng, Tiffany

Subjects

*MACROPHAGE activation, *MACROPHAGES, *MULTINUCLEATED giant cells, *ACETYLATION, *ELONGATOR complex

Abstract

Macrophage activation/polarization to distinct functional states is critically supported by metabolic shifts. How polarizing signals coordinate metabolic and functional reprogramming, and the potential implications for control of macrophage activation, remains poorly understood. Here we show that IL-4 signaling co-opts the Akt-mTORC1 pathway to regulate Acly, a key enzyme in Ac-CoA synthesis, leading to increased histone acetylation and M2 gene induction. Only a subset of M2 genes is controlled in this way, including those regulating cellular proliferation and chemokine production. Moreover, metabolic signals impinge on the Akt-mTORC1 axis for such control of M2 activation. We propose that Akt-mTORC1 signaling calibrates metabolic state to energetically demanding aspects of M2 activation, which may define a new role for metabolism in supporting macrophage activation. [ABSTRACT FROM AUTHOR]

Published

2016

5. Human THAP7 Is a Chromatin-associated, Histone Tail-binding Protein That Represses Transcription via Recruitment of HDAC3 and Nuclear Hormone Receptor Corepressor.

Author

Macfarlan, Todd, Kutney, Sara, Altman, Brian, Montross, Rebecca, Jiujiu Yu, and Chakravarti, Debabrata

Subjects

*CHROMATIN, *NUCLEOPROTEINS, *HISTONES, *ACYLATION, *HORMONE receptors, *BINDING sites, *BIOCHEMISTRY, *MEDICAL sciences

Abstract

The identities of signal transducer proteins that integrate histone hypoacetylation and transcriptional repression are largely unknown. Here we demonstrate that THAP7, an uncharacterized member of the recently identified THAP (Thanatos-associated protein) family of proteins, is ubiquitously expressed, associates with chromatin, and represses transcription. THAP7 binds preferentially to hypoacetylated (un-, mono-, and diacetylated) histone H4 tails in vitro via its C-terminal 77 amino acids. Deletion of this domain, or treatment of cells with the histone deacetylase inhibitor TSA, which leads to histone hyperacetylation, partially disrupts THAP7/chromatin association in living cells. THAP7 coimmunoprecipitates with histone deacetylase 3 (HDAC3) and the nuclear hormone receptor corepressor (NCoR) and represses transcription as a Gal4 fusion protein. Chromatin immunoprecipitation assays demonstrate that these corepressors are recruited to promoters in a THAP7 dependent manner and promote histone H3 hypoacetylation. The conserved THAP domain is a key determinant for full HDAC3 association in vitro, and both the THAP domain and the histone interaction domain are important for the repressive properties of THAP7. Full repression mediated by THAP7 is also dependent on NCoR expression. We hypothesize that THAP7 is a dual function repressor protein that actively targets deacetylation of histone H3 necessary to establish transcriptional repression and functions as a signal transducer of the repressive mark of hypoacetylated histone H4. This is the first demonstration of the transcriptional regulatory properties of a human THAP domain protein, and a critical identification of a potential transducer of the repressive signal of hypoacetylated histone H4 in higher eukaryotes. [ABSTRACT FROM AUTHOR]

Published

2005