HMGA2 Antisense Long Non-coding RNAs as New Players in the Regulation of HMGA2 Expression and Pancreatic Cancer Promotion

Ros, Gloria; Pegoraro, Silvia; Angelis, Paolo De; Sgarra, Riccardo; Zucchelli, S.; Gustincich, Stefano; Manfioletti, Guidalberto

doi:10.3389/fonc.2019.01526

Cited by 23 publications

(21 citation statements)

References 81 publications

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“…The noncoding RNA (ncRNA) gene RPSAP52 can regulate HMGA2 both posttranscriptionally by blocking HMGA2 ‐targeted miRNA activity and transcriptionally. ( 40 )…”

Section: Resultsmentioning

confidence: 99%

Prioritization of Osteoporosis‐Associated Genome‐wide Association Study (GWAS) Single‐Nucleotide Polymorphisms (SNPs) Using Epigenomics and Transcriptomics

et al. 2021

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Genetic risk factors for osteoporosis, a prevalent disease associated with aging, have been examined in many genome‐wide association studies (GWASs). A major challenge is to prioritize transcription‐regulatory GWAS‐derived variants that are likely to be functional. Given the critical role of epigenetics in gene regulation, we have used an unusual epigenetics‐based and transcription‐based approach to identify some of the credible regulatory single‐nucleotide polymorphisms (SNPs) relevant to osteoporosis from 38 reported bone mineral density (BMD) GWASs. Using Roadmap databases, we prioritized SNPs based upon their overlap with strong enhancer or promoter chromatin preferentially in osteoblasts relative to 12 heterologous cell culture types. We also required that these SNPs overlap open chromatin (Deoxyribonuclease I [DNaseI]‐hypersensitive sites) and DNA sequences predicted to bind to osteoblast‐relevant transcription factors in an allele‐specific manner. From >50,000 GWAS‐derived SNPs, we identified 14 novel and credible regulatory SNPs (Tier‐1 SNPs) for osteoporosis risk. Their associated genes, BICC1, LGR4, DAAM2, NPR3, or HMGA2, are involved in osteoblastogenesis or bone homeostasis and regulate cell signaling or enhancer function. Four of these genes are preferentially expressed in osteoblasts. BICC1, LGR4, and DAAM2 play important roles in canonical Wnt signaling, a pathway critical for bone formation and repair. The transcription factors predicted to bind to the Tier‐1 SNP‐containing DNA sequences also have bone‐related functions. We present evidence that some of the Tier‐1 SNPs exert their effects on BMD risk indirectly through little‐studied long noncoding RNA (lncRNA) genes, which may, in turn, control the nearby bone‐related protein‐encoding gene. Our study illustrates a method to identify novel BMD‐related causal regulatory SNPs for future study and to prioritize candidate regulatory GWAS‐derived SNPs, in general. © 2021 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.

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“…The noncoding RNA (ncRNA) gene RPSAP52 can regulate HMGA2 both posttranscriptionally by blocking HMGA2 ‐targeted miRNA activity and transcriptionally. ( 40 )…”

Section: Resultsmentioning

confidence: 99%

Prioritization of Osteoporosis‐Associated Genome‐wide Association Study (GWAS) Single‐Nucleotide Polymorphisms (SNPs) Using Epigenomics and Transcriptomics

et al. 2021

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“…A search using the key words of lncRNA and pancreatic cancer in PubMed on July 28, 2020 yielded 589 publications, with the most relevant one dating back in 2011 (19). Most lncRNAs have been reported to promote the proliferation of pancreatic cancer through different signaling pathways (20)(21)(22)(23). In the case of lncRNA AL161431.1, its identi ed targets include miR-1252-5p, and the pathways include MAPK signaling in endometrial carcinoma and a competing endogenous RNA network in lung squamous cell carcinoma (7,9; Table S2).…”

Section: Discussionmentioning

confidence: 99%

The role of long noncoding RNA AL161431.1 in the development and progression of pancreatic cancer

Fan

et al. 2021

Preprint

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Pancreatic cancer is known for its notorious fast progression and poor prognosis. Long noncoding RNA (lncRNA) AL161431.1 has been reported to be involved in the pathogenesis of different cancers. In this study, we explored the role of lncRNA AL161431.1 in the development and progression of pancreatic cancer by bioinformatic analysis, in vitro and in vivo experiments in pancreatic cancer BxPC-3 and SW1990 cells, as well as clinical samples. We found that lncRNA AL161431.1 was highly expressed in pancreatic cancer cells and tissues. Knock down of lncRNA AL161431.1 led to increased cancer cell death and cell cycle arrest. Xenograft growth of SW1990 cells with stable knockdown of lncRNA AL161431.1 in mice was significantly slower than that of SW1990 cells with scrambled control shRNA. Finally, we showed the involvement of lncRNA AL161431.1 in pancreatic cancer was related to its promotion of epithelial mesenchymal transition process.

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“…One of these ncRNA genes, RPSAP52, can regulate HMGA2 both post-transcriptionally by blocking HMGA2targeted miRNA activity and transcriptionally. (39) From our TFBS analysis, we predict that the three HMGA2 far-upstream Tier-1 SNPs are in DNA sequences that bind HMGA1, YY1, SATB1 or ZBTB20 specifically at their Alt alleles (Table 1). These TFs are associated with bone or cartilage biology ( Supplemental Table S6).…”

Section: Hmga2 Has Three Far-upstream Bmd-risk Tier-1 Snps Near a Novmentioning

confidence: 99%

Prioritization of osteoporosis-associated GWAS SNPs using epigenomics and transcriptomics

Zhang

Deng

Shen

et al. 2020

Preprint

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Genetic risk factors for osteoporosis, a prevalent disease associated with aging, have been examined in many genome-wide association studies (GWAS). A major challenge is to prioritize transcription-regulatory GWAS-derived variants that are likely to be functional. Given the critical role of epigenetics in gene regulation, we have used an unusual epigenetics-and transcription-based approach to identify credible regulatory SNPs relevant to osteoporosis from 38 reported BMD GWAS. Using Roadmap databases, we prioritized SNPs based upon their overlap with strong enhancer or promoter chromatin preferentially in osteoblasts relative to 11 heterologous cell culture types. The selected SNPs also had to overlap open chromatin (DNaseI-hypersensitive sites) and DNA sequences predicted to bind to osteoblast-relevant transcription factors in an allele-specific manner. From >50,000 GWAS-derived SNPs, we identified 16 novel and credible regulatory SNPs (Tier-1 SNPs) for osteoporosis risk. Their associated genes, BICC1, LGR4, DAAM2, NPR3, or HMGA2, are involved in osteoblastogenesis or bone homeostasis and regulate cell signaling or enhancer function. Four of them are preferentially expressed in osteoblasts. BICC1, LGR4, and DAAM2 play important roles in canonical Wnt signaling, a pathway critical to bone formation and repair. The transcription factors that are predicted to bind to the Tier-1 SNP-containing DNA sequences also have bone-related functions. For the seven Tier-1 SNPs near the 5' end of BICC1, examination of eQTL overlap and the distribution of BMD-increasing alleles suggests that at least one SNP in each of two clusters contributes to inherited osteoporosis risk. Our study not only illustrates a method that can be used to identify novel BMD-related causal regulatory SNPs for future study, but also reveals evidence that some of the Tier-1 SNPs exert their effects on BMD risk indirectly through little-studied noncoding RNA genes, which in turn may control the nearby bone-related proteinencoding gene.

show abstract

HMGA2 Antisense Long Non-coding RNAs as New Players in the Regulation of HMGA2 Expression and Pancreatic Cancer Promotion

Cited by 23 publications

References 81 publications

Prioritization of Osteoporosis‐Associated Genome‐wide Association Study (GWAS) Single‐Nucleotide Polymorphisms (SNPs) Using Epigenomics and Transcriptomics

Prioritization of Osteoporosis‐Associated Genome‐wide Association Study (GWAS) Single‐Nucleotide Polymorphisms (SNPs) Using Epigenomics and Transcriptomics

The role of long noncoding RNA AL161431.1 in the development and progression of pancreatic cancer

Prioritization of osteoporosis-associated GWAS SNPs using epigenomics and transcriptomics

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