Activation of PARP-1 by snoRNAs Controls Ribosome Biogenesis and Cell Growth via the RNA Helicase DDX21

Kim, Dae Seok; Camacho, Cristel V.; Nagari, Anusha; Malladi, Venkat S.; Challa, Sridevi; Kraus, W. Lee

doi:10.1016/j.molcel.2019.06.020

Cited by 160 publications

(177 citation statements)

References 65 publications

(97 reference statements)

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“…48,49 Therefore, we inferred that USP34 or SNORA70B might bind WNT pathway-related protein to activate it. 48,49 Therefore, we inferred that USP34 or SNORA70B might bind WNT pathway-related protein to activate it.…”

Section: Discussionmentioning

confidence: 97%

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Expression signature of six‐snoRNA serves as novel non‐invasive biomarker for diagnosis and prognosis prediction of renal clear cell carcinoma

Zhao

Yan

et al. 2020

J Cellular Molecular Medi

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Increasing evidence has verified that small nucleolar RNAs (snoRNAs) play significant roles in tumorigenesis and exhibit prognostic value in clinical practice. In the study, we analysed the expression profile and clinical relevance of snoRNAs from TCGA database including 530 ccRCC (clear cell renal cell carcinoma) and 72 control cases. By using univariate and multivariate Cox analysis, we established a six-snoRNA signature and divided patients into high-risk or low-risk groups. We found patients in highrisk group had significantly shorter overall survival and recurrence-free survival than those in low-risk group in test series, validation series and entire series by Kaplan-Meier analysis. We also confirmed this signature had a great accuracy and specificity in 64 clinical tissue cases and 50 serum samples. Then, depending on receiver operating characteristic curve analysis we found the six-snoRNA signature was an superior indicator better than conventional clinical factors (AUC = 0.732). Furthermore, combining the signature with TNM stage or Fuhrman grade were the optimal indicators (AUC = 0.792; AUC = 0.800) and processed the clinical applied value for ccRCC. Finally, we found the SNORA70B and its hose gene USP34 might directly regulate Wnt signalling pathway to promote tumorigenesis in ccRCC. In general, our study established a six-snoRNA signature as an independent and superior diagnosis and prognosis indicator for ccRCC. K E Y W O R D S biomarker, clear cell renal cell carcinoma, overall survival, prognostic, recurrence-free survival, snoRNAs S U PP O RTI N G I N FO R M ATI O N Additional supporting information may be found online in the Supporting Information section. How to cite this article: Zhao Y, Yan Y, Ma R, et al. Expression signature of six-snoRNA serves as novel non-invasive biomarker for diagnosis and prognosis prediction of renal clear cell carcinoma.

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Section: Discussionmentioning

confidence: 97%

“…Lasted studies have reported that snoRNAs could directly bind to functional protein to promote tumorigenesis. 48,49 Therefore, we inferred that USP34 or SNORA70B might bind WNT pathway-related protein to activate it.…”

Section: Discussionmentioning

confidence: 97%

Expression signature of six‐snoRNA serves as novel non‐invasive biomarker for diagnosis and prognosis prediction of renal clear cell carcinoma

Zhao

Yan

et al. 2020

J Cellular Molecular Medi

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“…PARP inhibitors are also effective in Ewing's sarcomas by blocking, on the one hand, PARP1-dependent transcriptional activation effects of ETS gene fusions such as EWS-FLI-1, and by exacerbating DNA damage on the other (Brenner et al 2012). Furthermore, PARP inhibitors reduce rDNA transcription and ribosome biogenesis in BRCA1/2-proficient cancer cells by preventing DDX21 ADP-ribosylation, and thereby reduce breast cancer growth (Kim et al 2019).…”

Section: Targeting Transcription Rna Metabolism and Ribosome Biogenmentioning

confidence: 99%

PARP and PARG inhibitors in cancer treatment

2020

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Oxidative and replication stress underlie genomic instability of cancer cells. Amplifying genomic instability through radiotherapy and chemotherapy has been a powerful but nonselective means of killing cancer cells. Precision medicine has revolutionized cancer therapy by putting forth the concept of selective targeting of cancer cells. Poly(ADP-ribose) polymerase (PARP) inhibitors represent a successful example of precision medicine as the first drugs targeting DNA damage response to have entered the clinic. PARP inhibitors act through synthetic lethality with mutations in DNA repair genes and were approved for the treatment of BRCA mutated ovarian and breast cancer. PARP inhibitors destabilize replication forks through PARP DNA entrapment and induce cell death through replication stress-induced mitotic catastrophe. Inhibitors of poly(ADP-ribose) glycohydrolase (PARG) exploit and exacerbate replication deficiencies of cancer cells and may complement PARP inhibitors in targeting a broad range of cancer types with different sources of genomic instability. Here I provide an overview of the molecular mechanisms and cellular consequences of PARP and PARG inhibition. I highlight clinical performance of four PARP inhibitors used in cancer therapy (olaparib, rucaparib, niraparib, and talazoparib) and discuss the predictive biomarkers of inhibitor sensitivity, mechanisms of resistance as well as the means of overcoming them through combination therapy.

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“…ASO-mediated knockdown of SNORA74A engendered a substantial decrease in DDX21 ADPRylation and cell proliferation, confirming that snoRNAs can activate PARP-1 in the absence of DNA damage. It was also shown that DDX21 can bind snoRNAs such as SCARNA2 on its C-terminal RNA-binding domain [74]. These snoRNAs were suggested to compete with the PARP-1 and DDX21 interactions.…”

Section: Binding Competition Protein Activation and Protein Trappingmentioning

confidence: 99%

“…The inhibition of PARP-1 is helpful in the treatment of cancers because it causes accumulation of DNA damage and synthetic lethality of cancer cells presenting defects in homologous recombination (HR)-mediated DNA repair machinery [72]. However, even tumors with non-mutated HR machinery were recently shown to be affected by PARP inhibitors [73], and Kim et al [74] discovered a mechanism that can explain this. Indeed, several mature H/ACA box snoRNAs (notably SNORA73A, SNORA73B and SNORA74A) can bind to PARP-1, leading to the activation of its ADPRylation (PAR) function.…”

Section: Binding Competition Protein Activation and Protein Trappingmentioning

confidence: 99%

Small nucleolar RNAs: continuing identification of novel members and increasing diversity of their molecular mechanisms of action

Bergeron

Fafard-Couture

Scott

2020

Biochemical Society Transactions

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Identified five decades ago amongst the most abundant cellular RNAs, small nucleolar RNAs (snoRNAs) were initially described as serving as guides for the methylation and pseudouridylation of ribosomal RNA through direct base pairing. In recent years, however, increasingly powerful high-throughput genomic approaches and strategies have led to the discovery of many new members of the family and surprising diversity in snoRNA functionality and mechanisms of action. SnoRNAs are now known to target RNAs of many biotypes for a wider range of modifications, interact with diverse binding partners, compete with other binders for functional interactions, recruit diverse players to targets and affect protein function and accessibility through direct interaction. This minireview presents the continuing characterization of the snoRNome through the identification of new snoRNA members and the discovery of their mechanisms of action, revealing a highly versatile noncoding family playing central regulatory roles and connecting the main cellular processes.

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Activation of PARP-1 by snoRNAs Controls Ribosome Biogenesis and Cell Growth via the RNA Helicase DDX21

Cited by 160 publications

References 65 publications

Expression signature of six‐snoRNA serves as novel non‐invasive biomarker for diagnosis and prognosis prediction of renal clear cell carcinoma

Expression signature of six‐snoRNA serves as novel non‐invasive biomarker for diagnosis and prognosis prediction of renal clear cell carcinoma

PARP and PARG inhibitors in cancer treatment

Small nucleolar RNAs: continuing identification of novel members and increasing diversity of their molecular mechanisms of action

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