4.8 Article

Transglutaminase 2 promotes tumorigenicity of colon cancer cells by inactivation of the tumor suppressor p53

ONCOGENE (2021)

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Journal

ONCOGENE
Volume 40, Issue 25, Pages 4352-4367

Publisher

SPRINGERNATURE
DOI: 10.1038/s41388-021-01847-w

Keywords

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Categories

Biochemistry & Molecular Biology Oncology Cell Biology Genetics & Heredity

Funding

  1. Else Kroner Fresenius-Stiftung
  2. Deutsche Krebshilfe
  3. LOEWE Centers Cell and Gene Therapy Frankfurt (Hessen State Ministry for Higher Education, Research and the Arts) [III L 4-518/17.004 [2014]]
  4. Frankfurt Cancer Institute (Hessen State Ministry for Higher Education, Research and the Arts) [III L 5 - 519/03/03.001 - [0015]]
  5. Projekt DEAL

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TGM2 plays a crucial role in colorectal cancer, with its transamidation activity being essential for promoting cell survival. By binding to the tumor suppressor gene p53, TGM2 inactivates it, affecting apoptosis induction in cancer cells.
Despite a high clinical need for the treatment of colorectal carcinoma (CRC) as the second leading cause of cancer-related deaths, targeted therapies are still limited. The multifunctional enzyme Transglutaminase 2 (TGM2), which harbors transamidation and GTPase activity, has been implicated in the development and progression of different types of human cancers. However, the mechanism and role of TGM2 in colorectal cancer are poorly understood. Here, we present TGM2 as a promising drug target. In primary patient material of CRC patients, we detected an increased expression and enzymatic activity of TGM2 in colon cancer tissue in comparison to matched normal colon mucosa cells. The genetic ablation of TGM2 in CRC cell lines using shRNAs or CRISPR/Cas9 inhibited cell expansion and tumorsphere formation. In vivo, tumor initiation and growth were reduced upon genetic knockdown of TGM2 in xenotransplantations. TGM2 ablation led to the induction of Caspase-3-driven apoptosis in CRC cells. Functional rescue experiments with TGM2 variants revealed that the transamidation activity is critical for the pro-survival function of TGM2. Transcriptomic and protein-protein interaction analyses applying various methods including super-resolution and time-lapse microscopy showed that TGM2 directly binds to the tumor suppressor p53, leading to its inactivation and escape of apoptosis induction. We demonstrate here that TGM2 is an essential survival factor in CRC, highlighting the therapeutic potential of TGM2 inhibitors in CRC patients with high TGM2 expression. The inactivation of p53 by TGM2 binding indicates a general anti-apoptotic function, which may be relevant in cancers beyond CRC.

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