FB2026_01 , released March 12, 2026
FB2026_01 , released March 12, 2026
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Citation
Croy, H.E., Fuller, C.N., Giannotti, J., Robinson, P., Foley, A.V., Yamulla, R.J., Cosgriff, S., Greaves, B.D., von Kleeck, R.A., An, H.H., Powers, C.M., Tran, J.K., Tocker, A.M., Jacob, K.D., Davis, B.K., Roberts, D.M. (2016). The Poly(ADP-ribose) Polymerase Enzyme Tankyrase Antagonizes Activity of the β-Catenin Destruction Complex through ADP-ribosylation of Axin and APC2.  J. Biol. Chem. 291(24): 12747--12760.
FlyBase ID
FBrf0232585
Publication Type
Research paper
Abstract
Most colon cancer cases are initiated by truncating mutations in the tumor suppressor, adenomatous polyposis coli (APC). APC is a critical negative regulator of the Wnt signaling pathway that participates in a multi-protein "destruction complex" to target the key effector protein β-catenin for ubiquitin-mediated proteolysis. Prior work has established that the poly(ADP-ribose) polymerase (PARP) enzyme Tankyrase (TNKS) antagonizes destruction complex activity by promoting degradation of the scaffold protein Axin, and recent work suggests that TNKS inhibition is a promising cancer therapy. We performed a yeast two-hybrid (Y2H) screen and uncovered TNKS as a putative binding partner of Drosophila APC2, suggesting that TNKS may play multiple roles in destruction complex regulation. We find that TNKS binds a C-terminal RPQPSG motif in Drosophila APC2, and that this motif is conserved in human APC2, but not human APC1. In addition, we find that APC2 can recruit TNKS into the β-catenin destruction complex, placing the APC2/TNKS interaction at the correct intracellular location to regulate β-catenin proteolysis. We further show that TNKS directly PARylates both Drosophila Axin and APC2, but that PARylation does not globally regulate APC2 protein levels as it does for Axin. Moreover, TNKS inhibition in colon cancer cells decreases β-catenin signaling, which we find cannot be explained solely through Axin stabilization. Instead, our findings suggest that TNKS regulates destruction complex activity at the level of both Axin and APC2, providing further mechanistic insight into TNKS inhibition as a potential Wnt pathway cancer therapy.
PubMed ID
27068743
PubMed Central ID
PMC4933447 (PMC) (EuropePMC)
DOI
10.1074/jbc.M115.705442
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Secondary IDs
    Language of Publication
    English
    Additional Languages of Abstract
    Parent Publication
    Publication Type
    Journal
    Abbreviation
    J. Biol. Chem.
    Title
    Journal of Biological Chemistry
    Publication Year
    1905-
    ISBN/ISSN
    0021-9258
    Data From Reference
    Alleles (3)
    Gene Groups (2)
    Genes (4)
    Physical Interactions (6)
    Natural transposons (1)
    Experimental Tools (1)
    Transgenic Constructs (2)