Your search keyword '"Yu, Anan"' showing total 6 results

1. Structural Analysis of the Interaction between Dishevelled2 and Clathrin AP-2 Adaptor, A Critical Step in Noncanonical Wnt Signaling

Author

Yu, Anan, Xing, Yi, Harrison, Stephen C., and Kirchhausen, Tomas

Subjects

*MOLECULAR structure, *WNT proteins, *CELLULAR signal transduction, *PROTEINS, *CELL receptors, *ENDOCYTOSIS, *TYROSINE

Abstract

Summary: Wnt association with its receptor, Frizzled (Fz), and recruitment by the latter of an adaptor, Dishevelled (Dvl), initiates signaling through at least two distinct pathways (“canonical” and “noncanonical”). Endocytosis and compartmentalization help determine the signaling outcome. Our previous work has shown that Dvl2 links at least one Frizzled family member (Fz4) to clathrin-mediated endocytosis by interacting with the μ2 subunit of the AP-2 clathrin adaptor, through both a classical endocytic tyrosine motif and a so-called “DEP domain.” We report here the crystal structure of a chimeric protein that mimics the Dvl2-μ2 complex. The DEP domain binds at one end of the elongated, C-terminal domain of μ2. This domain:domain interface shows that parts of the μ2 surface distinct from the tyrosine-motif site can help recruit specific receptors or adaptors into a clathrin coated pit. Mutation of residues at the DEP-μ2 contact or in the tyrosine motif reduce affinity of Dvl2 for μ2 and block efficient internalization of Fz4 in response to ligation by Wnt5a. The crystal structure has thus allowed us to identify the specific interaction that leads to Frizzled uptake and to downstream, noncanonical signaling events. [ABSTRACT FROM AUTHOR]

Published

2010

2. Association of Dishevelled with the Clathrin AP-2 Adaptor Is Required for Frizzled Endocytosis and Planar Cell Polarity Signaling

Author

Yu, Anan, Rual, Jean-François, Tamai, Keiko, Harada, Yuko, Vidal, Marc, He, Xi, and Kirchhausen, Tomas

Subjects

*WNT genes, *CELL receptors, *PEPTIDES, *XENOPUS, *GASTRULATION

Abstract

Summary: Upon activation by Wnt, the Frizzled receptor is internalized in a process that requires the recruitment of Dishevelled. We describe a novel interaction between Dishevelled2 (Dvl2) and μ2-adaptin, a subunit of the clathrin adaptor AP-2; this interaction is required to engage activated Frizzled4 with the endocytic machinery and for its internalization. The interaction of Dvl2 with AP-2 requires simultaneous association of the DEP domain and a peptide YHEL motif within Dvl2 with the C terminus of μ2. Dvl2 mutants in the YHEL motif fail to associate with μ2 and AP-2, and prevent Frizzled4 internalization. Corresponding Xenopus Dishevelled mutants show compromised ability to interfere with gastrulation mediated by the planar cell polarity (PCP) pathway. Conversely, a Dvl2 mutant in its DEP domain impaired in PCP signaling exhibits defective AP-2 interaction and prevents the internalization of Frizzled4. We suggest that the direct interaction of Dvl2 with AP-2 is important for Frizzled internalization and Frizzled/PCP signaling. [Copyright &y& Elsevier]

Published

2007

3. HaloTag as a substrate-based macroautophagy reporter.

Author

Qiang Xiao, Cruz, Gabrielle, Botham, Rachel, Fox, Susan G., Yu, Anan, Allen, Seth, Morimoto, Richard I., and Kelly, Jeffery W.

Subjects

*CELL survival, *FLUORESCENCE microscopy, *CELLULAR control mechanisms, *LYSOSOMES, *AUTOPHAGY

Abstract

Macroautophagy is a conserved cellular degradation pathway that, upon upregulation, confers resilience toward various stress conditions, including protection against proteotoxicity associated with neurodegenerative diseases, leading to cell survival. Monitoring autophagy regulation in living cells is important to understand its role in physiology and pathology, which remains challenging. Here, we report that when HaloTag is expressed within a cell of interest and reacts with tetramethylrhodamine (TMR; its ligand attached to a fluorophore), the rate of fluorescent TMR-HaloTag conjugate accumulation in autophagosomes and lysosomes, observed by fluorescence microscopy, reflects the rate of autophagy. Notably, we found that TMR-HaloTag conjugates were mainly degraded by the proteasome (~95%) under basal conditions, while lysosomal degradation (~10% upon pharmacological autophagy activation) was slow and incomplete, forming a degraded product that remained fluorescent within a SDS-PAGE gel, in agreement with previous reports that HaloTag is resistant to lysosomal degradation when fused to proteins of interest. Autophagy activation is distinguished from autophagy inhibition by the increased production of the degraded TMR-HaloTag band relative to the full-length TMR-HaloTag band as assessed by SDS-PAGE and by a faster rate of TMR-HaloTag conjugate lysosomal puncta accumulation as observed by fluorescence microscopy. Pharmacological proteasome inhibition leads to accumulation of TMR-HaloTag in lysosomes, indicating possible cross talk between autophagy and proteasomal degradation. [ABSTRACT FROM AUTHOR]

Published

2024

4. The efficacy of nimodipine drug delivery using mPEG-PLA micelles and mPEG-PLA/TPGS mixed micelles.

Author

Huang, Shuling, Yu, Xiaohong, Yang, Linlin, Song, Fenglan, Chen, Gang, Lv, Zhufen, Li, Tiao, Chen, De, Zhu, Wanhua, Yu, Anan, Zhang, Yongming, and Yang, Fan

Subjects

*DRUG efficacy, *NIMODIPINE, *DRUG delivery systems, *POLYETHYLENE glycol, *POLYLACTIC acid, *EXCIPIENTS, *DRUG development, *THERAPEUTICS

Abstract

Objective In order to develop and compare mPEG-PLA micelles and mPEG-PLA/TPGS mixed micelles, with the intention to develop a highly efficient formulation for nimodipine (NIM), NIM-loaded micelles and mixed micelles were made and their pharmacokinetics were studied. Methods Single factor experiments and orthogonal experiments were designed to optimize the final preparation process, characterizations and drug release behaviors were studied. Pharmacokinetics of NIM micelles, NIM mixed micelles were researched and were compared to NIM solution. Results Micelles and mixed micelles were prepared by solvent evaporation method, with relatively high drug loading efficiency and within nano-particle size range. The CMC value of mPEG-PLA was lower than that of mPEG-PLA/TPGS. The results of FTIR and TEM confirmed the spherical core–shell structure of micelles as well as mixed micelles, and the encapsulation of NIM inside the cores. In vitro release showed that micelles and mixed micelles had sustained release effect in the forms of passive diffusion and dissolution process, respectively. Following intraperitoneal administration (5 mg/kg), micelles and mixed micelles were absorbed faster than solution, and with larger MRT (0 – t ) , smaller CL z and larger AUC (0 – t ) as compared to that of solution, which showed micelles and mixed micelles had higher retention, slower elimination and higher bioavailability. This experiment also showed that mixed micelles released NIM more stably than micelles. By evaluate the bioequivalence, NIM micelles and NIM mixed micelles were testified non-bioequivalent to NIM solution. Conclusion Micelles and mixed micelles could sustain the NIM concentrations more efficiently in plasma as compared to solution. Mixed micelles were the best ones since they had high loading content and released more stably. Thus, apprehending micelles and mixed micelles were suited as poor aqueous solubility drug carriers, and mixed micelles were better due to their high loading content and more stable release. [ABSTRACT FROM AUTHOR]

Published

2014

5. Key Interactions for Clathrin Coat Stability.

Author

Böcking, Till, Aguet, François, Rapoport, Iris, Banzhaf, Manuel, Yu, Anan, Zeeh, Jean?Christophe, and Kirchhausen, Tom

Subjects

*PROTEIN-protein interactions, *COATED vesicles, *EUKARYOTIC cells, *GENETIC mutation, *HYDROGEN-ion concentration, *AUXILINS

Abstract

Summary: Clathrin-coated vesicles are major carriers of vesicular traffic in eukaryotic cells. This endocytic pathway relies on cycles of clathrin coat assembly and Hsc70-mediated disassembly. Here we identify histidine residues as major determinants of lattice assembly and stability. They are located at the invariant interface between the proximal and distal segments of clathrin heavy chains, in triskelions centered on two adjacent vertices of the coated-vesicle lattice. Mutation of these histidine residues to glutamine alters the pH dependence of coat stability. We then describe single-particle fluorescence imaging experiments in which we follow the effect of these histidine mutations on susceptibility to Hsc70-dependent uncoating. Coats destabilized by these mutations require fewer Hsc70 molecules to initiate disassembly, as predicted by a model in which Hsc70 traps conformational distortions during the auxilin- and Hsc70:ATP-mediated uncoating reaction. [Copyright &y& Elsevier]

Published

2014

6. Dry Gel Conversion Methodfor the Synthesis of Organic–InorganicHybrid MOR Zeolites with Modifiable Catalytic Activities.

Author

Zhou, Dan, Lu, Xinhuan, Xu, Jun, Yu, Anan, Li, Jiyang, Deng, Feng, and Xia, Qinghua

Subjects

*CHEMICAL synthesis, *ZEOLITES, *COLLOIDS, *CATALYTIC activity, *ALUMINUM silicates, *FOURIER transform infrared spectroscopy, *ALKENES, *EPOXIDATION

Abstract

Dry gel conversion (DGC) technique is first applied inthe synthesisof organic–inorganic hybrid aluminosilicate zeolites. By usingthe DGC method, methylene-bridged organic–inorganic hybridzeolites with an MOR topology are synthesized without organic additive,which are structurally characterized by powder XRD, FTIR, solid-state 29Si, 13C, 27Al MAS NMR, SEM, elementalanalysis, XRF, XPS, and N2adsorption techniques. Thiswork first reports that thus-synthesized methylene-bridged hybridzeolites can be successfully bestowed with excellent catalytic activitiesthrough different modification treatments. Co2+-exchangedhybrid zeolites are applied in the epoxidation of alkenes with airto achieve good conversions and selectivities. Especially, methylene-bridgedhybrid zeolites can be sulfonated with fuming sulfuric acid to formacidic MOR-SO3H catalyst, which exhibits highly catalyticactivity for the acid-catalyzed condensation reaction of cyclohexanoneand glycol. This method will be one potential route for the fabricationof organic–inorganic hybrid zeolite or related molecular sievecatalysts. [ABSTRACT FROM AUTHOR]

Published

2012