Long-read transcriptome sequencing reveals abundant promoter diversity in distinct molecular subtypes of gastric cancer

Huang, Kie Kyon; Huang, Jiawen; Wu, Jeanie; Lee, Ming‐Hui; Tay, Su Ting; Kumar, Vikrant; Kalpana, R.; Padmanabhan, Nisha; Xu, Chong; Tan, Angie Lay Keng; Chan, Charlene; Kappei, Dennis; Göke, Jonathan; Tan, Patrick

doi:10.1186/s13059-021-02261-x

Cited by 51 publications

(44 citation statements)

References 65 publications

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“…A recent study of ten gastric cancer cell lines using PacBio's Iso-Seq technology identified approximately 39,000 novel isoforms, including for the known oncogenes ERBB2 and CD44. Alternative promoters were frequently used in gastric cancer cells which often resulted in altered downstream CDS and 3′ UTRs (Huang et al, 2021). Full-length transcripts, using both ONT and PacBio reads, have also been sequenced to identify variants involved in treatment resistance in triple negative breast and lung cancer cell lines (Lian et al, 2019;Seki et al, 2019;Oka et al, 2021).…”

Section: Long Read Profiling Of Splicing In Diseasementioning

confidence: 99%

Isoform Age - Splice Isoform Profiling Using Long-Read Technologies

Paoli-Iseppi

Gleeson

Clark

2021

Front. Mol. Biosci.

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Alternative splicing (AS) of RNA is a key mechanism that results in the expression of multiple transcript isoforms from single genes and leads to an increase in the complexity of both the transcriptome and proteome. Regulation of AS is critical for the correct functioning of many biological pathways, while disruption of AS can be directly pathogenic in diseases such as cancer or cause risk for complex disorders. Current short-read sequencing technologies achieve high read depth but are limited in their ability to resolve complex isoforms. In this review we examine how long-read sequencing (LRS) technologies can address this challenge by covering the entire RNA sequence in a single read and thereby distinguish isoform changes that could impact RNA regulation or protein function. Coupling LRS with technologies such as single cell sequencing, targeted sequencing and spatial transcriptomics is producing a rapidly expanding suite of technological approaches to profile alternative splicing at the isoform level with unprecedented detail. In addition, integrating LRS with genotype now allows the impact of genetic variation on isoform expression to be determined. Recent results demonstrate the potential of these techniques to elucidate the landscape of splicing, including in tissues such as the brain where AS is particularly prevalent. Finally, we also discuss how AS can impact protein function, potentially leading to novel therapeutic targets for a range of diseases.

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Section: Long Read Profiling Of Splicing In Diseasementioning

confidence: 99%

Isoform Age - Splice Isoform Profiling Using Long-Read Technologies

Paoli-Iseppi

Gleeson

Clark

2021

Front. Mol. Biosci.

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“…The abnormally upregulated promoter activities in HCC may lead to the changes of the CDS region and produce new protein subtypes, as reported (12). For example, the upregulated prmtr.14927 in MET may lead to the accumulation of a 960-aa protein isoform that lacks the SEMA domain in HCC (Supplementary Figure 2B).…”

Section: Identification Of Alternative Promoters In Hccmentioning

confidence: 67%

A Genome-Wide Investigation of Effects of Aberrant DNA Methylation on the Usage of Alternative Promoters in Hepatocellular Carcinoma

et al. 2022

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BackgroundThe alternative usage of promoters provides a way to regulate gene expression, has a significant influence on the transcriptome, and contributes to the cellular transformation of cancer. However, the function of alternative promoters (APs) in hepatocellular carcinoma (HCC) has not been systematically studied yet. In addition, the potential mechanism of regulation to the usage of APs remains unclear. DNA methylation, one of the most aberrant epigenetic modifications in cancers, is known to regulate transcriptional activity. Whether DNA methylation regulates the usage of APs needs to be explored. Here, we aim to investigate the effects of DNA methylation on usage of APs in HCC.MethodsPromoter activities were calculated based on RNA-seq data. Functional enrichment analysis was implemented to conduct GO terms. Correlation tests were used to detect the correlation between promoter activity and methylation status. The LASSO regression model was used to generate a diagnostic model. Kaplan–Meier analysis was used to compare the overall survival between high and low methylation groups. RNA-seq and whole-genome bisulfite sequencing (WGBS) in HCC samples were performed to validate the correlation of promoter activity and methylation.ResultsWe identified 855 APs in total, which could be well used to distinguish cancer from normal samples. The correlation of promoter activity and DNA methylation in APs was observed, and the APs with negative correlation were defined as methylation-regulated APs (mrAPs). Six mrAPs were identified to generate a diagnostic model with good performance (AUC = 0.97). Notably, the majority of mrAPs had CpG sites that could be used to predict clinical outcomes by methylation status. Finally, we verified 85.6% of promoter activity variation and 92.3% of methylation changes in our paired RNA-seq and WGBS samples, respectively. The negative correlation between promoter activity and methylation status was further confirmed in our HCC samples.ConclusionThe aberrant methylation status plays a critical role in the precision usage of APs in HCC, which sheds light on the mechanism of cancer development and provides a new insight into cancer screening and treatment.

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“…Subgrouping of patients based on molecular characteristics has considerably affected the selection of therapeutic regimens and the forecasting of therapeutic responses and prognoses [44]. The establishment of tumor molecular subtypes has advanced our understanding of tumor genotypes and phenotypes, presenting a potential application in therapeutics and prognosis estimation [61,62]. At present, the ConMC divides MIBC into six molecular subtypes and systematically exposes specific differentiation patterns, mutation genes, histology, and overall survival rates in the six molecular subtypes [45].…”

Section: Discussionmentioning

confidence: 99%

Single-Cell Proteomic Analysis Dissects the Complexity of Tumor Microenvironment in Muscle Invasive Bladder Cancer

Feng

Wang

Tao

et al. 2021

Cancers

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Muscle invasive bladder cancer (MIBC) is a malignancy with considerable heterogeneity. The MIBC tumor microenvironment (TME) is highly complex, comprising diverse phenotypes and spatial architectures. The complexity of the MIBC TME must be characterized to provide potential targets for precision therapy. Herein, an integrated combination of mass cytometry and imaging mass cytometry was used to analyze tumor cells, immune cells, and TME spatial characteristics of 44 MIBC patients. We detected tumor and immune cell clusters with abnormal phenotypes. In particular, we identified a previously overlooked cancer stem-like cell cluster (ALDH+PD-L1+ER-β−) that was strongly associated with poor prognosis. We elucidated the different spatial architectures of immune cells (excluded, infiltrated, and deserted) and tumor-associated collagens (curved, stretched, directionally distributed, and chaotic) in the MIBC TME. The present study is the first to provide in-depth insight into the complexity of the MIBC TME at the single-cell level. Our results will improve the general understanding of the heterogeneous characteristics of MIBC, potentially facilitating patient stratification and personalized therapy.

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Long-read transcriptome sequencing reveals abundant promoter diversity in distinct molecular subtypes of gastric cancer

Cited by 51 publications

References 65 publications

Isoform Age - Splice Isoform Profiling Using Long-Read Technologies

Isoform Age - Splice Isoform Profiling Using Long-Read Technologies

A Genome-Wide Investigation of Effects of Aberrant DNA Methylation on the Usage of Alternative Promoters in Hepatocellular Carcinoma

Single-Cell Proteomic Analysis Dissects the Complexity of Tumor Microenvironment in Muscle Invasive Bladder Cancer

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