| URL: | http://NonStopDB.dkfz.de |
| Full name: | Nonstop Mutations in Cancer Database |
| Description: | 3,412 nonstop mutations were curated and analysed from 62 tumour entities in database NonStopDb. |
| Year founded: | 2020 |
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| Accessibility: |
Accessible
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| Country/Region: | Germany |
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| University/Institution: | University of Freiburg |
| Address: | Division of Cancer Research, Department of Thoracic Surgery, Medical Center - University of Freiburg, Faculty of Medicine, University of Freiburg, German Cancer Consortium (DKTK) Partner Site Freiburg, Freiburg, Germany. |
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| Country/Region: | Germany |
| Contact name (PI/Team): | Sven Diederichs |
| Contact email (PI/Helpdesk): | s.diederichs@dkfz.de |
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A pan-cancer analysis reveals nonstop extension mutations causing SMAD4 tumour suppressor degradation. [PMID: 32719554]
Nonstop or stop-loss mutations convert a stop into a sense codon, resulting in translation into the 3' untranslated region as a nonstop extension mutation to the next in-frame stop codon or as a readthrough mutation into the poly-A tail. Nonstop mutations have been characterized in hereditary diseases, but not in cancer genetics. In a pan-cancer analysis, we curated and analysed 3,412 nonstop mutations from 62 tumour entities, generating a comprehensive database at http://NonStopDB.dkfz.de. Six different nonstop extension mutations affected the tumour suppressor SMAD4, extending its carboxy terminus by 40 amino acids. These caused rapid degradation of the SMAD4 mutants via the ubiquitin-proteasome system. A hydrophobic degron signal sequence of ten amino acids within the carboxy-terminal extension was required to induce complete loss of the SMAD4 protein. Thus, we discovered that nonstop mutations can be functionally important in cancer and characterize their loss-of-function impact on the tumour suppressor SMAD4. |