BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. T cell differentiation, Hepatitis, Intestine, Human chorionic gonadotropin, Prozac)
Bookmark Forward

The NESH/Abi-3-based WAVE2 complex is functionally distinct from the Abi-1-based WAVE2 complex.

Saki Sekino, Yuriko Kashiwagi, Hitoshi Kanazawa, Kazuki Takada, Takashi Baba, Seiichi Sato, Hiroki Inoue, Masaki Kojima, Katsuko Tani

Cell communication and signaling : CCS 2015


filter terms:
  • Abi 1 (10)
  • Abi 2 (4)
  • Abi1 protein (2)
  • abi3 protein, human (1)
  • Abl (31)
  • actin (1)
  • actin cytoskeleton (1)
  • binds (1)
  • c Abl (7)
  • cell movement (1)
  • cells (7)
  • did (1)
  • extracellular matrix (1)
  • family (1)
  • fibronectin (1)
  • help (1)
  • human (2)
  • imatinib (1)
  • mice (1)
  • NESH (13)
  • NESH protein (1)
  • plasma membrane (1)
  • protein family (2)
  • protein human (2)
  • protein transport (1)
  • pseudopodia (1)
  • region rich (1)
  • regions (1)
  • sh3 domain (1)
  • signal (2)
  • vein (1)
  • WAVE2 (11)
    • Sizes of these terms reflect their relevance to your search.

    Abl interactor (Abi) family proteins play significant roles in actin cytoskeleton organization through participation in the WAVE complex. Mammals possess three Abi proteins: Abi-1, Abi-2, and NESH/Abi-3. Abi-1 and Abi-2 were originally identified as Abl tyrosine kinase-binding proteins. It has been disclosed that Abi-1 acts as a bridge between c-Abl and WAVE2, and c-Abl-mediated WAVE2 phosphorylation promotes actin remodeling. We showed previously that NESH/Abi-3 is present in the WAVE2 complex, but neither binds to c-Abl nor promotes c-Abl-mediated phosphorylation of WAVE2. In this study, we characterized NESH/Abi-3 in more detail, and compared its properties with those of Abi-1 and Abi-2. NESH/Abi-3 was ectopically expressed in NIH3T3 cells, in which Abi-1, but not NESH/Abi-3, is expressed. The expression of NESH/Abi-3 caused degradation of endogenous Abi-1, which led to the formation of a NESH/Abi-3-based WAVE2 complex. When these cells were plated on fibronectin-coated dishes, the translocation of WAVE2 to the plasma membrane was significantly reduced and the formation of peripheral lamellipodial structures was disturbed, suggesting that the NESH/Abi-3-based WAVE2 complex was unable to help produce lamellipodial protrusions. Next, Abi-1, Abi-2, or NESH/Abi-3 was expressed in v-src-transformed NIH3T3 cells. Only in NESH/Abi-3-expressed cells did treatment with an Abl kinase inhibitor, imatinib mesylate, or siRNA-mediated knockdown of c-Abl promote the formation of invadopodia, which are ventral membrane protrusions with extracellular matrix degradation activity. Structural studies showed that a linker region between the proline-rich regions and the Src homology 3 (SH3) domain of Abi-1 is crucial for its interaction with c-Abl and c-Abl-mediated phosphorylation of WAVE2. The NESH/Abi-3-based WAVE2 complex is functionally distinct from the Abi-1-based one, and NESH/Abi-3 may be involved in the formation of ventral protrusions under certain conditions.

    Citation

    Saki Sekino, Yuriko Kashiwagi, Hitoshi Kanazawa, Kazuki Takada, Takashi Baba, Seiichi Sato, Hiroki Inoue, Masaki Kojima, Katsuko Tani. The NESH/Abi-3-based WAVE2 complex is functionally distinct from the Abi-1-based WAVE2 complex. Cell communication and signaling : CCS. 2015;13:41

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 26428302

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.