Establishment of a Colorectal Cancer-Related MicroRNA-mRNA Regulatory Network by Microarray and Bioinformatics

Jiang, Dan; Xie, Xiaoliang; Lu, Zhenhui; Liu, Liyuan; Qu, Yuliang; Wu, Shan; Li, Yanning; Li, Guangqi; Wang, Hongxia; Xu, Guofeng

doi:10.3389/fgene.2020.560186

Cited by 20 publications

(14 citation statements)

References 41 publications

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“…The study thus provides a glimpse of possible effects that can be mediated by GPR15 in colon cancer beyond its classical function as a T-cell trafficking protein. Another study on mRNA and miRNA signatures in human COAD patient samples also reported reduced GPR15 expression in tumors and potential miRNA mediated regulation of GPR15 levels in COAD 40 .…”

Section: Discussionmentioning

confidence: 88%

GPR15 in colon cancer development and anti-tumor immune responses

Namkoong

Swaminathan

Koh

et al. 2021

Preprint

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G protein-coupled receptor 15 (GPR15) is a chemoattractant receptor which in response to its ligand, C10orf99/GPR15L, promotes colon homing of T cells in health and colitis. The functional role of GPR15 in colon cancer is largely unexplored, motivating our current studies using murine colon cancer models and human colorectal cancer (CRC) tissues. Our initial analysis of human CRC specimen revealed significant reduction in GPR15 expression and frequency of GPR15+ immune cells in tumors compared to ′tumor-free′ surgical margins. In the AOM/DSS murine model of colitis associated colon cancer (CAC), we observed increased colonic polyps/tumor burden and lower survival rate in Gpr15-deficient (KO) compared to Gpr15-sufficient (Het) mice. Analysis of immune cell infiltrates in the colonic polyps showed significantly decreased CD8+ T cells and increased IL-17+ CD4+ and IL-17+ CD8+ T cells in Gpr15-KO than in Het mice. GPR15 deficiency thus alters the immune environment in colonic polyps to mitigate T cell-mediated anti-tumor responses resulting in severe disease. Consistent with a protective role of GPR15, administration of GPR15L to established tumors in the MC38 CRC mouse model increased CD45+ cell infiltration, enhanced TNFα expression on CD4+ and CD8+ T cells at the tumor site and dramatically reduced tumor burden. Our findings highlight an important, unidentified role of the GPR15-GPR15L axis in promoting a tumor-suppressive immune microenvironment and unveils a novel, colon-specific therapeutic target for CRC.

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Section: Discussionmentioning

confidence: 88%

GPR15 in colon cancer development and anti-tumor immune responses

Namkoong

Swaminathan

Koh

et al. 2021

Preprint

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“…In cancer investigations, PNOC was related to high inflammatory status and oxidative stress in C6 glioma cells, which also was highly up-regulated in pediatric brainstem ganglioglioma tissues and epithelial ovarian cancer, and in analysis of high-risk gastrointestinal stromal tumor, PNOC was reported as a prognostic biomarker ( 45 – 48 ). In a study of mRNA and microRNA network in colorectal cancer, PNOC and its targeting microRNAs were also prognostic markers for evaluation of patients ( 49 ). In our analysis, PNOC was up-regulated in cholangiocarcinoma samples, though the difference didn’t achieve significance.…”

Section: Discussionmentioning

confidence: 99%

PNOC Expressed by B Cells in Cholangiocarcinoma Was Survival Related and LAIR2 Could Be a T Cell Exhaustion Biomarker in Tumor Microenvironment: Characterization of Immune Microenvironment Combining Single-Cell and Bulk Sequencing Technology

Chen

Yan

et al. 2021

Front. Immunol.

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BackgroundCholangiocarcinoma was a highly malignant liver cancer with poor prognosis, and immune infiltration status was considered an important factor in response to immunotherapy. In this investigation, we tried to locate immune infiltration related genes of cholangiocarcinoma through combination of bulk-sequencing and single-cell sequencing technology.MethodsSingle sample gene set enrichment analysis was used to annotate immune infiltration status in datasets of TCGA CHOL, GSE32225, and GSE26566. Differentially expressed genes between high- and low-infiltrated groups in TCGA dataset were yielded and further compressed in other two datasets through backward stepwise regression in R environment. Single-cell sequencing data of GSE138709 was loaded by Seurat software and was used to examined the expression of infiltration-related gene set. Pathway changes in malignant cell populations were analyzed through scTPA web tool.ResultsThere were 43 genes differentially expressed between high- and low-immune infiltrated patients, and after further compression, PNOC and LAIR2 were significantly correlated with high immune infiltration status in cholangiocarcinoma. Through analysis of single-cell sequencing data, PNOC was mainly expressed by infiltrated B cells in tumor microenvironment, while LAIR2 was expressed by Treg cells and partial GZMB+ CD8 T cells, which were survival related and increased in tumor tissues. High B cell infiltration levels were related to better overall survival. Also, malignant cell populations demonstrated functionally different roles in tumor progression.ConclusionPNOC and LAIR2 were biomarkers for immune infiltration evaluation in cholangiocarcinoma. PNOC, expressed by B cells, could predict better survival of patients, while LAIR2 was a potential marker for exhaustive T cell populations, correlating with worse survival of patients.

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“…First, we used a relaxed cutoff threshold (adjusted p < 0.25), which could include more false positives compared to a stricter cutoff. In contrast, it is well known that a small sample size generally yields higher adjusted p -values [ 83 , 84 , 85 , 86 ]. However, the results of downstream functional analyses and data from previous publications further confirmed the validity of our methodology and findings.…”

Section: Discussionmentioning

confidence: 99%

Long-Term Effects of Very Low Dose Particle Radiation on Gene Expression in the Heart: Degenerative Disease Risks

Garikipati

Arakelyan

Blakely

et al. 2021

Cells

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Compared to low doses of gamma irradiation (γ-IR), high-charge-and-energy (HZE) particle IR may have different biological response thresholds in cardiac tissue at lower doses, and these effects may be IR type and dose dependent. Three- to four-month-old female CB6F1/Hsd mice were exposed once to one of four different doses of the following types of radiation: γ-IR 137Cs (40-160 cGy, 0.662 MeV), 14Si-IR (4-32 cGy, 260 MeV/n), or 22Ti-IR (3-26 cGy, 1 GeV/n). At 16 months post-exposure, animals were sacrificed and hearts were harvested and archived as part of the NASA Space Radiation Tissue Sharing Forum. These heart tissue samples were used in our study for RNA isolation and microarray hybridization. Functional annotation of twofold up/down differentially expressed genes (DEGs) and bioinformatics analyses revealed the following: (i) there were no clear lower IR thresholds for HZE- or γ-IR; (ii) there were 12 common DEGs across all 3 IR types; (iii) these 12 overlapping genes predicted various degrees of cardiovascular, pulmonary, and metabolic diseases, cancer, and aging; and (iv) these 12 genes revealed an exclusive non-linear DEG pattern in 14Si- and 22Ti-IR-exposed hearts, whereas two-thirds of γ-IR-exposed hearts revealed a linear pattern of DEGs. Thus, our study may provide experimental evidence of excess relative risk (ERR) quantification of low/very low doses of full-body space-type IR-associated degenerative disease development.

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Establishment of a Colorectal Cancer-Related MicroRNA-mRNA Regulatory Network by Microarray and Bioinformatics

Cited by 20 publications

References 41 publications

GPR15 in colon cancer development and anti-tumor immune responses

GPR15 in colon cancer development and anti-tumor immune responses

PNOC Expressed by B Cells in Cholangiocarcinoma Was Survival Related and LAIR2 Could Be a T Cell Exhaustion Biomarker in Tumor Microenvironment: Characterization of Immune Microenvironment Combining Single-Cell and Bulk Sequencing Technology

Long-Term Effects of Very Low Dose Particle Radiation on Gene Expression in the Heart: Degenerative Disease Risks

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