Search for: All records | NSF Public Access

Note: When clicking on a Digital Object Identifier (DOI) number, you will be taken to an external site maintained by the publisher. Some full text articles may not yet be available without a charge during the embargo (administrative interval).
What is a DOI Number?

Some links on this page may take you to non-federal websites. Their policies may differ from this site.

An ensemble of cadherin-catenin-vinculin complex employs vinculin as the major F-actin binding mode

https://doi.org/10.1016/j.bpj.2023.04.026

Shi, Bright; Matsui, Tsutomu; Qian, Shuo; Weiss, Thomas M.; Nicholl, Iain D.; Callaway, David J.E.; Bu, Zimei (May 2023, Biophysical Journal)

Full Text Available
pH-Dependent Solution Micellar Structure of Amphoteric Polypeptoid Block Copolymers with Positionally Controlled Ionizable Sites

https://doi.org/10.1021/acs.biomac.3c00407

Zhang, Meng; Liu, Yun; Zuo, Xiaobing; Qian, Shuo; Pingali, Sai Venkatesh; Gillilan, Richard E.; Huang, Qingqiu; Zhang, Donghui (July 2023, Biomacromolecules)
Structure and dynamics of lipid membranes interacting with antivirulence end-phosphorylated polyethylene glycol block copolymers

https://doi.org/10.1039/C9SM01642B

Yu, Jing; Mao, Jun; Nagao, Michihiro; Bu, Wei; Lin, Binhua; Hong, Kunlun; Jiang, Zhang; Liu, Yun; Qian, Shuo; Tirrell, Matthew; et al (January 2020, Soft Matter)

The structure and dynamics of lipid membranes in the presence of extracellular macromolecules are critical for cell membrane functions and many pharmaceutical applications. The pathogen virulence-suppressing end-phosphorylated polyethylene glycol (PEG) triblock copolymer ( Pi-ABAPEG ) markedly changes the interactions with lipid vesicle membranes and prevents PEG-induced vesicle phase separation in contrast to the unphosphorylated copolymer ( ABAPEG ). Pi-ABAPEG weakly absorbs on the surface of lipid vesicle membranes and slightly changes the structure of 1,2-dimyristoyl- sn-glycero -3-phosphocholine ( DMPC ) unilamellar vesicles at 37 °C, as evidenced by small angle neutron scattering. X-ray reflectivity measurements confirm the weak adsorption of Pi-ABAPEG on DMPC monolayer, resulting in a more compact DMPC monolayer structure. Neutron spin-echo results show that the adsorption of Pi-ABAPEG on DMPC vesicle membranes increases the membrane bending modulus κ .
more » « less
Full Text Available
An ensemble of flexible conformations underlies mechanotransduction by the cadherin–catenin adhesion complex

https://doi.org/10.1073/pnas.1911489116

Bush, Martin; Alhanshali, Bashir M.; Qian, Shuo; Stanley, Christopher B.; Heller, William T.; Matsui, Tsutomu; Weiss, Thomas M.; Nicholl, Iain D.; Walz, Thomas; Callaway, David J.; et al (October 2019, Proceedings of the National Academy of Sciences)

The cadherin–catenin adhesion complex is the central component of the cell–cell adhesion adherens junctions that transmit mechanical stress from cell to cell. We have determined the nanoscale structure of the adherens junction complex formed by the α-catenin•β-catenin•epithelial cadherin cytoplasmic domain (ABE) using negative stain electron microscopy, small-angle X-ray scattering, and selective deuteration/small-angle neutron scattering. The ABE complex is highly pliable and displays a wide spectrum of flexible structures that are facilitated by protein-domain motions in α- and β-catenin. Moreover, the 107-residue intrinsically disordered N-terminal segment of β-catenin forms a flexible “tongue” that is inserted into α-catenin and participates in the assembly of the ABE complex. The unanticipated ensemble of flexible conformations of the ABE complex suggests a dynamic mechanism for sensitivity and reversibility when transducing mechanical signals, in addition to the catch/slip bond behavior displayed by the ABE complex under mechanical tension. Our results provide mechanistic insight into the structural dynamics for the cadherin–catenin adhesion complex in mechanotransduction.
more » « less
Full Text Available