Multi-omics characterization of molecular features of gastric cancer correlated with response to neoadjuvant chemotherapy

Li, Ziyu; Gao, Xiangyu; Peng, Xinxin; Chen, Mei-Ju May; Li, Zhe; Wei, Bin; Xi, Wen; Wei, Baoye; Yu, Dong; Bu, Zhaode; Wu, Aiwen; Wu, Qi; Tang, Lei; Li, Zhongwu; Liu, Yiqiang; Zhang, Li; Jia, Shuqin; Zhang, Lianhai; Shan, Fei; Zhang, Ji; Wu, Xiaojiang; Ji, Xin; Ji, Ke; Wu, Xiaolong; Shi, Jinyao; Xing, Xiaofang; Wu, Jianmin; Lv, Guorong; Shen, Lin; Ji, Xuwo; Liang, Han; Ji, Jiafu

doi:10.1126/sciadv.aay4211

Cited by 65 publications

(76 citation statements)

References 48 publications

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“…Patient stratification based on molecular information promises a great value for guiding diagnosis and treatment choice, particularly in genetically heterogeneous diseases such as gastric cancer. Till date, a number of studies attempted for the molecular classification of patients for this purpose, most of which are based on gene expression profiling utilizing microarray data (3)(4)(5)(7)(8)(9). With the broader availability and better quality of next-generation sequencing data, now it became possible to reliably study other molecular features than gene expression.…”

Section: Discussionmentioning

confidence: 99%

“…However, an important question is whether we can improve the selection of patients with advanced GC for chemotherapy in order to achieve greater benefit from the treatment. To address this, different groups have put much effort in stratifying patients with GC into molecular subtypes (3)(4)(5)(6)(7)(8)(9); however, these studies heavily focused on gene expression and/or mutation profiling, often with the limitations of microarray-based platforms or small sample sizes, thus novel molecular data types and approaches are needed for better guiding the chemotherapy treatment for this class of patients. Here, we demonstrate A-to-I RNA editing as a novel epigenetic classifier to reliably identify responders to chemotherapy.…”

Section: Introductionmentioning

confidence: 99%

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“3G” Trial: An RNA Editing Signature to Guide Gastric Cancer Chemotherapy

Song

et al. 2021

Cancer Research

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Gastric cancer (GC) cases are often diagnosed at an advanced stage with poor prognosis. Platinum-based chemotherapy has been internationally accepted as first-line therapy for inoperable or metastatic GC. To achieve greater benefits, selection of patients eligible for this treatment is critical. Although gene expression profiling has been widely used as a genomic classifier to identify molecular subtypes of GC and to stratify patients for different chemotherapy regimens, its prediction accuracy can be improved. Adenosine-to-inosine (A-to-I) RNA editing has emerged as a new player contributing to GC development and progression, offering potential clinical utility for diagnosis and treatment. Using a systematic computational approach followed by both in vitro validations and in silico validations in TCGA, we conducted a transcriptomewide RNA editing analysis of a cohort of 104 patients with advanced GC and identified an RNA editing (GCRE) signature to guide GC chemotherapy. RNA editing events stood as a prognostic and predictive biomarker in advanced GC. A GCRE score based on the GCRE signature consisted of 50 editing sites associated with 29 genes, predicting response to chemotherapy with a high accuracy (84%). Of note, patients demonstrating higher editing levels of this panel of sites presented a better overall response. Consistently, GC cell lines with higher editing levels showed higher chemosensitivity. Applying the GCRE score on TCGA dataset confirmed that responders had significantly higher levels of editing in advanced GC. Overall, this newly defined GCRE signature reliably stratifies patients with advanced GC and predicts response from chemotherapy. Research.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

“3G” Trial: An RNA Editing Signature to Guide Gastric Cancer Chemotherapy

Song

et al. 2021

Cancer Research

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“…Interestingly, these results showed that the subtypes could be as predictors for survival and response to adjuvant chemotherapy (Sohn et al, 2017). Moreover, a recent study characterized key mutational features, copy number alternations and gene expression changes associated with responses to neoadjuvant chemotherapy with multi-omics data of tumor samples from patients responding to neoadjuvant chemotherapy or not (Li et al, 2020). Compared the responders with non-responders tumors and pre-with post-treatment samples, the C10orf71 mutations were found to be associated with treatment resistance by statistical models (Li et al, 2020).…”

Section: Machine Learning In Gastric Cancer Researchmentioning

confidence: 99%

“…Moreover, a recent study characterized key mutational features, copy number alternations and gene expression changes associated with responses to neoadjuvant chemotherapy with multi-omics data of tumor samples from patients responding to neoadjuvant chemotherapy or not (Li et al, 2020). Compared the responders with non-responders tumors and pre-with post-treatment samples, the C10orf71 mutations were found to be associated with treatment resistance by statistical models (Li et al, 2020). Taken together, such machine learning based approach integrates multi-omics data, providing efficient ways to predict the treatment outcome based on the host genetic information.…”

Section: Machine Learning In Gastric Cancer Researchmentioning

confidence: 99%

Systems Biology of Gastric Cancer: Perspectives on the Omics-Based Diagnosis and Treatment

Shi

Wei

2020

Front. Mol. Biosci.

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Gastric cancer is the fifth most diagnosed cancer in the world, affecting more than a million people and causing nearly 783,000 deaths each year. The prognosis of advanced gastric cancer remains extremely poor despite the use of surgery and adjuvant therapy. Therefore, understanding the mechanism of gastric cancer development, and the discovery of novel diagnostic biomarkers and therapeutics are major goals in gastric cancer research. Here, we review recent progress in application of omics technologies in gastric cancer research, with special focus on the utilization of systems biology approaches to integrate multi-omics data. In addition, the association between gastrointestinal microbiota and gastric cancer are discussed, which may offer insights in exploring the novel microbiota-targeted therapeutics. Finally, the application of datadriven systems biology and machine learning approaches could provide a predictive understanding of gastric cancer, and pave the way to the development of novel biomarkers and rational design of cancer therapeutics.

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“…A consequence of the increased use of neoadjuvant protocols is the availability for research purposes of matched samples of primary tumour tissue taken before systemic therapy, usually in the form of a diagnostic biopsy, and after therapy from the resection. These matched samples present a powerful resource for study of the molecular response of tumours to therapy, and thereby to identify pathways associated with relative therapy resistance or sensitivity [ 5 – 7 ]. The hypothesis behind such analyses is that tumour cells that remain after therapy include characteristics associated with therapy resistance, while characteristics present before therapy but lost in the matched post-treatment sample include molecular events associated with relative therapy sensitivity.…”

Section: Introductionmentioning

confidence: 99%

Identification of candidate mediators of chemoresponse in breast cancer through therapy-driven selection of somatic variants

Amri

Baxter

Hanby

et al. 2020

Breast Cancer Res Treat

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Purpose More than a third of primary breast cancer patients are treated with cytotoxic chemotherapy, typically without guidance from predictive markers. Increased use of neoadjuvant chemotherapy provides opportunities for identification of molecules associated with treatment response, by comparing matched tumour samples before and after therapy. Our hypothesis was that somatic variants of increased prevalence after therapy promote resistance, while variants with reduced prevalence cause sensitivity. Methods We performed systematic analyses of matched pairs of cancer exomes from primary oestrogen receptor-positive/HER2-negative breast cancers (n = 6) treated with neoadjuvant epirubicin/cyclophosphamide. We identified candidate genes as mediators of chemotherapy response by consistent subclonal changes in somatic variant prevalence through therapy, predicted variant impact on gene function, and enrichment of specific functional pathways. Influence of candidate genes on breast cancer outcome was tested using publicly available breast cancer expression data (n = 1903). Results We identified 14 genes as the strongest candidate mediators of chemoresponse: TCHH, MUC17, ARAP2, FLG2, ABL1, CENPF, COL6A3, DMBT1, ITGA7, PLXNA1, S100PBP, SYNE1, ZFHX4, and CACNA1C. Genes contained somatic variants showing prevalence changes in up to 4 patients, with up to 3 being predicted as damaging. Genes coding for extra-cellular matrix components or related signalling pathways were significantly over-represented among variants showing prevalence changes. Expression of 5 genes (TCHH, ABL1, CENPF, S100PBP, and ZFHX4) was significantly associated with patient survival. Conclusions Genomic analysis of paired pre- and post-therapy samples resulting from neoadjuvant therapy provides a powerful method for identification of mediators of response. Genes we identified should be assessed as predictive markers or targets in chemo-sensitization.

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Multi-omics characterization of molecular features of gastric cancer correlated with response to neoadjuvant chemotherapy

Cited by 65 publications

References 48 publications

“3G” Trial: An RNA Editing Signature to Guide Gastric Cancer Chemotherapy

“3G” Trial: An RNA Editing Signature to Guide Gastric Cancer Chemotherapy

Systems Biology of Gastric Cancer: Perspectives on the Omics-Based Diagnosis and Treatment

Identification of candidate mediators of chemoresponse in breast cancer through therapy-driven selection of somatic variants

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