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Dynamic interactions between E-cadherin and Ankyrin-G mediate epithelial cell polarity maintenance

Author

Listed:
  • Chao Kong

    (University of Science and Technology of China
    University of Science and Technology of China)

  • Xiaozhan Qu

    (University of Science and Technology of China
    University of Science and Technology of China)

  • Mingming Liu

    (University of Science and Technology of China)

  • Weiya Xu

    (University of Science and Technology of China
    University of Science and Technology of China)

  • Da Chen

    (University of Science and Technology of China
    University of Science and Technology of China)

  • Yanshen Zhang

    (University of Science and Technology of China)

  • Shan Zhang

    (University of Science and Technology of China)

  • Feng Zhu

    (University of Science and Technology of China)

  • Zhenbang Liu

    (University of Science and Technology of China)

  • Jianchao Li

    (South China University of Technology)

  • Chengdong Huang

    (University of Science and Technology of China
    University of Science and Technology of China)

  • Chao Wang

    (University of Science and Technology of China
    University of Science and Technology of China)

Abstract

E-cadherin is an essential cell‒cell adhesion protein that mediates canonical cadherin-catenin complex formation in epithelial lateral membranes. Ankyrin-G (AnkG), a scaffold protein linking membrane proteins to the spectrin-based cytoskeleton, coordinates with E-cadherin to maintain epithelial cell polarity. However, the molecular mechanisms governing this complex formation and its relationships with the cadherin-catenin complex remain elusive. Here, we report that AnkG employs a promiscuous manner to encapsulate three discrete sites of E-cadherin by the same region, a dynamic mechanism that is distinct from the canonical 1:1 molar ratio previously described for other AnkG or E-cadherin-mediated complexes. Moreover, we demonstrate that AnkG-binding-deficient E-cadherin exhibited defective accumulation at the lateral membranes and show that disruption of interactions resulted in cell polarity malfunction. Finally, we demonstrate that E-cadherin is capable of simultaneously anchoring to AnkG and β-catenin, providing mechanistic insights into the functional orchestration of the ankyrin-spectrin complex with the cadherin-catenin complex. Collectively, our results show that complex formation between E-cadherin and AnkG is dynamic, which enables the maintenance of epithelial cell polarity by ensuring faithful targeting of the adhesion molecule-scaffold protein complex, thus providing molecular mechanisms for essential E-cadherin-mediated complex assembly at cell‒cell junctions.

Suggested Citation

  • Chao Kong & Xiaozhan Qu & Mingming Liu & Weiya Xu & Da Chen & Yanshen Zhang & Shan Zhang & Feng Zhu & Zhenbang Liu & Jianchao Li & Chengdong Huang & Chao Wang, 2023. "Dynamic interactions between E-cadherin and Ankyrin-G mediate epithelial cell polarity maintenance," Nature Communications, Nature, vol. 14(1), pages 1-15, December.
    • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-42628-1
    DOI: 10.1038/s41467-023-42628-1
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    References listed on IDEAS

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    1. Chun Tang & Charles D. Schwieters & G. Marius Clore, 2007. "Open-to-closed transition in apo maltose-binding protein observed by paramagnetic NMR," Nature, Nature, vol. 449(7165), pages 1078-1082, October.
    2. Chengdong Huang & Paolo Rossi & Tomohide Saio & Charalampos G. Kalodimos, 2016. "Structural basis for the antifolding activity of a molecular chaperone," Nature, Nature, vol. 537(7619), pages 202-206, September.
    3. W. James Nelson, 2003. "Adaptation of core mechanisms to generate cell polarity," Nature, Nature, vol. 422(6933), pages 766-774, April.
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