The cancer-associated microprotein CASIMO1 controls cell proliferation and interacts with squalene epoxidase modulating lipid droplet formation

Polycarpou‐Schwarz, Maria; Groß, Matthias; Mestdagh, Pieter; Schott, Johanna; Grund, Stefanie; Hildenbrand, Catherina; Rom, Joachim; Aulmann, Sebastian; Sinn, Hans‐Peter; Vandesompele, Jo; Diederichs, Sven

doi:10.1038/s41388-018-0281-5

Cited by 128 publications

(109 citation statements)

References 72 publications

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“…The lncRNA profile of HCC was analyzed by a microarray‐based analysis of 32 primary tumor samples compared to seven normal liver tissue samples (Supporting Table ). To derive a broader set of cancer‐associated lncRNAs and to design a library of siRNAs against these candidates as a versatile tool to dissect lncRNAs in cancer, this data set was merged with results from two other cancer entities, breast ductal carcinoma and lung adenocarcinoma (all data deposited in the National Center for Biotechnology Information’s Gene Expression Omnibus). The analysis of this integrated data set yielded a total of 638 significantly dysregulated lncRNAs, mostly up‐regulated, which were used for the siRNA library design as described .…”

Section: Resultsmentioning

confidence: 99%

The Long Noncoding RNA Cancer Susceptibility 9 and RNA Binding Protein Heterogeneous Nuclear Ribonucleoprotein L Form a Complex and Coregulate Genes Linked to AKT Signaling

et al. 2018

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The identification of viability-associated long noncoding RNAs (lncRNAs) might be a promising rationale for new therapeutic approaches in liver cancer. Here, we applied an RNA interference screening approach in hepatocellular carcinoma (HCC) cell lines to find viability-associated lncRNAs. Among the multiple identified lncRNAs with a significant impact on HCC cell viability, we selected cancer susceptibility 9 (CASC9) due to the strength of its phenotype, expression, and up-regulation in HCC versus normal liver. CASC9 regulated viability across multiple HCC cell lines as shown by clustered regularly interspaced short palindromic repeats interference and single small interfering RNA (siRNA)-mediated and siRNA pool-mediated depletion of CASC9. Further, CASC9 depletion caused an increase in apoptosis and a decrease of proliferation. We identified the RNA binding protein heterogeneous nuclear ribonucleoprotein L (HNRNPL) as a CASC9 interacting protein by RNA affinity purification and validated it by native RNA immunoprecipitation. Knockdown of HNRNPL mimicked the loss-of-viability phenotype observed upon CASC9 depletion. Analysis of the proteome (stable isotope labeling with amino acids in cell culture) of CASC9-depleted and HNRNPL-depleted cells revealed a set of coregulated genes which implied a role of the CASC9:HNRNPL complex in AKT signaling and DNA damage sensing. CASC9 expression levels were elevated in patient-derived tumor samples compared to normal control tissue and had a significant association with overall survival of HCC patients. In a xenograft chicken chorioallantoic membrane model, we measured decreased tumor size after knockdown of CASC9. Conclusion: Taken together, we provide a comprehensive list of viability-associated lncRNAs in HCC; we identified the CASC9:HNRNPL complex as a clinically relevant viability-associated lncRNA/protein complex which affects AKT signaling and DNA damage sensing in HCC.

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Section: Resultsmentioning

confidence: 99%

The Long Noncoding RNA Cancer Susceptibility 9 and RNA Binding Protein Heterogeneous Nuclear Ribonucleoprotein L Form a Complex and Coregulate Genes Linked to AKT Signaling

et al. 2018

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“…It is increasingly being accepted that a large proportion of transcripts annotated as lncRNAs harbor smORFs and express micropeptides which may be stable enough to be functional [63][64][65]. Majority of the lncRNA products from the bifunctional or hybrid genes could be of this category and may express micropeptides which are functionally related to their canonical mRNA encoded proteins.…”

Section: Examples For Functionally Characterized Hybrid Genes Transcrmentioning

confidence: 99%

Non-coding transcript variants of protein-coding genes – what are they good for?

Dhamija

Menon

2018

RNA Biology

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The total number of protein-coding genes in the human genome is not significantly higher than those in much simpler eukaryotes, despite a general increase in genome size proportionate to the organismal complexity. The large non-coding transcriptome and extensive differential splicing, are increasingly being accepted as the factors contributing to the complex mammalian physiology and architecture. Recent studies reveal additional layers of functional complexity: some long non-coding RNAs have been re-defined as micropeptide or microprotein encoding transcripts, and in turn some protein-coding RNAs are bifunctional and display also non-coding functions. Moreover, several protein-coding genes express long non-coding RNA splice-forms and generate circular RNAs in addition to their canonical mRNA transcripts, revoking the strict definition of a gene as coding or non-coding. In this mini review, we discuss the current understanding of these hybrid genes and their possible roles and relevance.

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“…In our present study, our findings reveal that the lncRNA LINC00266-1 participates in the m 6 A recognition by m 6 A readers and the lncRNA LINC00266-1 exerts its m 6 A recognition regulation by encoding an oncopeptide instead of an RNA molecule. Our and previous studies showed that a limited number of lncRNAs and circRNAs could encode proteins/peptides to regulate tumorigenesis [37][38][39][40] . Our findings further confirmed that some peptides are hidden in some previously annotated lncRNAs.…”

Section: Resultsmentioning

confidence: 58%

An oncopeptide regulates m6A recognition by the m6A reader IGF2BP1 and tumorigenesis

et al. 2020

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N 6-methyladenosine (m 6 A) is the most prevalent modification in eukaryotic RNAs. The biological importance of m 6 A relies on m 6 A readers, which control mRNA fate and function. However, it remains unexplored whether additional regulatory subunits of m 6 A readers are involved in the m 6 A recognition on RNAs. Here we discover that the long noncoding RNA (lncRNA) LINC00266-1 encodes a 71-amino acid peptide. The peptide mainly interacts with the RNA-binding proteins, including the m 6 A reader IGF2BP1, and is thus named "RNAbinding regulatory peptide" (RBRP). RBRP binds to IGF2BP1 and strengthens m 6 A recognition by IGF2BP1 on RNAs, such as c-Myc mRNA, to increase the mRNA stability and expression of c-Myc, thereby promoting tumorigenesis. Cancer patients with RBRP high have a poor prognosis. Thus, the oncopeptide RBRP encoded by LINC00266-1 is a regulatory subunit of m 6 A readers and strengthens m 6 A recognition on the target RNAs by the m 6 A reader to exert its oncogenic functions.

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The cancer-associated microprotein CASIMO1 controls cell proliferation and interacts with squalene epoxidase modulating lipid droplet formation

Cited by 128 publications

References 72 publications

The Long Noncoding RNA Cancer Susceptibility 9 and RNA Binding Protein Heterogeneous Nuclear Ribonucleoprotein L Form a Complex and Coregulate Genes Linked to AKT Signaling

The Long Noncoding RNA Cancer Susceptibility 9 and RNA Binding Protein Heterogeneous Nuclear Ribonucleoprotein L Form a Complex and Coregulate Genes Linked to AKT Signaling

Non-coding transcript variants of protein-coding genes – what are they good for?

An oncopeptide regulates m6A recognition by the m6A reader IGF2BP1 and tumorigenesis

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