Germinal epimutation of Fragile Histidine Triad (FHIT) gene is associated with progression to acute and chronic adult T-cell leukemia diseases

Bellon, Marcia; Bialuk, Izabela; Galli, Veronica; Bai, Xuetao; Farre, Lourdes; Bittencourt, Achiléa Lisboa; Marçais, Ambroise; Petrus, Michael; Ratner, Lee; Waldmann, Thomas A.; Asnafi, Vahid; Gessain, Antoine; Matsuoka, Masao; Franchini, Genoveffa; Hermine, Olivier; Watanabe, Toshiki; Nicot, Christophe

doi:10.1186/s12943-021-01370-2

Cited by 9 publications

(5 citation statements)

References 62 publications

(80 reference statements)

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“…From the 49 somatic SVs detected in COLO829-lifted (45 TP and 4 FN), 35 SVs overlap with 26 known genes, of which 25 are related to cancer. Some examples are FHIT (near a fragile site), tumor suppressors ITIH5, MAGI2, PTEN, WWOX, and cell-proliferation control gene TMX3 (Bellon et al 2021; Cao et al 2020; Yehia et al 2023; Husanie et al 2022; Zhang et al 2019).…”

Section: Resultsmentioning

confidence: 99%

“…B) IGV screenshot of an SV that was labeled as FN according to the benchmark by Valle-Inclan et al Our analysis calls removed thee SVs due to lack of evidence in all samples (Supplementary Table 13)Overall, the approach of incorporating alignment to CHM13-T2T followed by liftover analysis eliminated all FP somatic SV calls for COLO829. Such a reduction in FP has important impacts suppressors ITIH5, MAGI2, PTEN, WWOX, and cell-proliferation control gene TMX3(Bellon et al 2021;Cao et al 2020;Yehia et al 2023;Husanie et al 2022;Zhang et al 2019).…”

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confidence: 99%

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The benefit of a complete reference genome for cancer structural variant analysis

Paulin,

Fan,

O’Neill

et al. 2024

Preprint

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The complexities of cancer genomes are becoming more easily interpreted due to advancements in sequencing technologies and improved bioinformatic analysis. Structural variants (SVs) represent an important subset of somatic events in tumors. While detection of SVs has been markedly improved by the development of long-read sequencing, somatic variant identification and annotation remains challenging. We hypothesized that use of a completed human reference genome (CHM13-T2T) would improve somatic SV calling. Our findings in a tumour/normal matched benchmark sample and two patient samples show that the CHM13-T2T improves SV detection and prioritization accuracy compared to GRCh38, with a notable reduction in false positive calls. We also overcame the lack of annotation resources for CHM13-T2T by lifting over CHM13-T2T-aligned reads to the GRCh38 genome, therefore combining both improved alignment and advanced annotations. In this process, we assessed the current SV benchmark set for COLO829/COLO829BL across four replicates sequenced at different centers with different long-read technologies. We discovered instability of this cell line across these replicates; 346 SVs (1.13%) were only discoverable in a single replicate. We identify 49 somatic SVs, which appear to be stable as they are consistently present across the four replicates. As such, we propose this consensus set as an updated benchmark for somatic SV calling and include both GRCh38 and CHM13-T2T coordinates in our benchmark. The benchmark is available at: 10.5281/zenodo.10819636 Our work demonstrates new approaches to optimize somatic SV prioritization in cancer with potential improvements in other genetic diseases.

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Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

The benefit of a complete reference genome for cancer structural variant analysis

Paulin,

Fan,

O’Neill

et al. 2024

Preprint

View full text Add to dashboard Cite

show abstract

“…Though the exact number of HTLV-I infected individuals is likely under-estimated, it is believed that in ubiquitous, hot-spot regions, 1-2% of persons are infected, with some foci reaching 20-40% of the population over the age of 55 [3]. HTLV-I infection appears to initiate the pathway toward ATL development; however, it is unknown whether preexisting conditions or genetic defects exist before HTLV-I infection that make a host cell vulnerable to ATL development [4]. Once infected, the expression of HTLV-I proteins, specifically the viral Tax protein, instigates genome and genetic instability, allowing for T-cell transformation that culminates in the development of ATL [5].…”

Section: Adult T-cell Leukemia (Atl) Is Characterized By Clonal or Ol...mentioning

confidence: 99%

“…ATL cell lines (ATL43T, ATL55T, LM-Y1, KK1, KOB, SO4, 1185, LAF) were supplemented with 50 U/mL IL-2 and 20% FBS. Primary ATL patient samples have been used in previous studies [4,9]. ATL patient samples were obtained after informed consent.…”

Section: Cell Culture and Patient Samplesmentioning

confidence: 99%

Increased H19/miR-675 Expression in Adult T-Cell Leukemia Is Associated with a Unique Notch Signature Pathway

Bellon,

Nicot

2024

IJMS

Self Cite

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The Notch pathway is a key cancer driver and is important in tumor progression. Early research suggested that Notch activity was highly dependent on the expression of the intracellular cleaved domain of Notch-1 (NICD). However, recent insights into Notch signaling reveal the presence of Notch pathway signatures, which may vary depending on different cancer types and tumor microenvironments. Herein, we perform a comprehensive investigation of the Notch signaling pathway in adult T-cell leukemia (ATL) primary patient samples. Using gene arrays, we demonstrate that the Notch pathway is constitutively activated in ATL patient samples. Furthermore, the activation of Notch in ATL cells remains elevated irrespective of the presence of activating mutations in Notch itself or its repressor, FBXW7, and that ATL cells are dependent upon Notch-1 expression for proliferation and survival. We demonstrate that ATL cells exhibit the expression of pivotal Notch-related genes, including notch-1, hes1, c-myc, H19, and hes4, thereby defining a critical Notch signature associated with ATL disease. Finally, we demonstrate that lncRNA H19 is highly expressed in ATL patient samples and ATL cells and contributes to Notch signaling activation. Collectively, our results shed further light on the Notch pathway in ATL leukemia and reveal new therapeutic approaches to inhibit Notch activation in ATL cells.

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“…It is noteworthy that the FHIT gene also functions as a TSG. It is frequently methylated in tumor growth, although its function as a TSG is lost due to epigenetic alterations ( 108 ). Hence, the hypermethylation of the gene in CD may lead to gene suppression, leading to a loss of function in its TSG ability to suppress tumors.…”

Section: Roles Of Dnam In Ibdmentioning

confidence: 99%

Effects of DNA methylation and its application in inflammatory bowel disease (Review)

Akanyibah,

Zhu,

Wan

et al. 2024

Int J Mol Med

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Inflammatory bowel disease (IBD) is marked by persistent inflammation, and its development and progression are linked to environmental, genetic, immune system and gut microbial factors. DNA methylation (DNAm), as one of the protein modifications, is a crucial epigenetic process used by cells to control gene transcription. DNAm is one of the most common areas that has drawn increasing attention recently, with studies revealing that the interleukin (IL)-23/IL-12, wingless-related integration site, IL-6-associated signal transducer and activator of transcription 3, suppressor of cytokine signaling 3 and apoptosis signaling pathways are involved in DNAm and in the pathogenesis of IBD. It has emerged that DNAm-associated genes are involved in perpetuating the persistent inflammation that characterizes a number of diseases, including IBD, providing a novel therapeutic strategy for exploring their treatment. The present review discusses DNAm-associated genes in the pathogenesis of IBD and summarizes their application as possible diagnostic, prognostic and therapeutic biomarkers in IBD. This may provide a reference for the particular form of IBD and its related methylation genes, aiding in clinical decision-making and encouraging therapeutic alternatives.

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Germinal epimutation of Fragile Histidine Triad (FHIT) gene is associated with progression to acute and chronic adult T-cell leukemia diseases

Cited by 9 publications

References 62 publications

The benefit of a complete reference genome for cancer structural variant analysis

The benefit of a complete reference genome for cancer structural variant analysis

Increased H19/miR-675 Expression in Adult T-Cell Leukemia Is Associated with a Unique Notch Signature Pathway

Effects of DNA methylation and its application in inflammatory bowel disease (Review)

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