4.6 Article

A catenin of the plakophilin-subfamily, Pkp3, responds to canonical- Wnt pathway components and signals

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS (2021)

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Journal

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS
Volume 563, Issue -, Pages 31-39

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.bbrc.2021.05.043

Keywords

Plakophilin-3 catenin; plakophilin3-catenin; Pkp-3; Wnt signaling pathway; Destruction complex; Desmosome junction; Desmosomal junction; Nucleus; Signaling pool

Categories

Biochemistry & Molecular Biology Biophysics

Funding

  1. NIH/NIMH [R01 MH 115717]
  2. NIH/NIGMS [1 RO1 GM 107079, 3 RO1 GM107079-S]
  3. Ashbel Smith Professorship Award
  4. National Research Foundation of Korea, Ministry of Science, ICT & Future Planning [NRF-2015R1C1A1A02036506]
  5. Schissler Foundation Fellowship
  6. NIH/NCI [CA-16672]
  7. UT MDACC Department of Genetics NIH Instrumentation Grant [1S10OD024976]
  8. [K01DK092320]
  9. [R03DK118771]
  10. [R01DK115655]

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This study investigates the regulation of the plakophilin protein Pkp3 by the Wnt pathway, showing that Wnt ligands or the LRP6 receptor stabilize Pkp3 levels while destruction complex components decrease Pkp3 levels. Additionally, Pkp3 translocates into the nucleus in response to Wnt ligands, indicating that Wnt signals or pathway components can modulate Pkp3-catenin levels.
Vertebrate beta-catenin plays a key role as a transducer of canonical-Wnt signals. We earlier reported that, similar to beta-catenin, the cytoplasmic signaling pool of p120-catenin-isoform1 is stabilized in response to canonical-Wnt signals. To obtain a yet broader view of the Wnt-pathway's impact upon catenin proteins, we focused upon plakophilin3 (plakophilin-3; Pkp3) as a representative of the plakophilin-catenin subfamily. Promoting tissue integrity, the plakophilins assist in linking desmosomal cadherins to intermediate filaments at desmosome junctions, and in common with other catenins they perform additional functions including in the nucleus. In this report, we test whether canonical-Wnt pathway components modulate Pkp3 protein levels. We find that in common with beta-catenin and p120-catenin-isoform1, Pkp3 is stabilized in the presence of a Wnt-ligand or a dominant-active form of the LRP6 receptor. Pkp3's levels are conversely lowered upon expressing destruction-complex components such as GSK3b and Axin, and in further likeness to beta-catenin and p120-isoform1, Pkp3 associates with GSK3beta and Axin. Finally, we note that Pkp3-catenin trans-localizes into the nucleus in response to Wnt-ligand and its exogenous expression stimulates an accepted Wnt reporter. These findings fit an expanded model where context-dependent Wnt-signals or pathway components modulate Pkp3-catenin levels. Future studies will be needed to assess potential gene regulatory, cell adhesive, or cytoskeletal effects. (c) 2021 Elsevier Inc. All rights reserved.

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