整理了單個(gè)基因的DNA甲基化探針的部分可視化分析圖。

甲基化差異

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用來自5個(gè)受感染個(gè)體(F1-11, F1-12, S2, S3, S4)和100個(gè)健康個(gè)體的LRS數(shù)據(jù)，測定了全血DNA中GIPC1中擴(kuò)展GGC重復(fù)區(qū)甲基化狀態(tài);甲基化在opdm患者和對照組之間沒有顯著差異。【@Deng.2020】

甲基化差異

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CXCL12和IL7R基因區(qū)域的DNA甲基化位點(diǎn)。

這個(gè)使用的是在線工具：http://maplab.imppc.org/wanderer/

Ref：Diez-Villanueva A, Mallona I, Peinado MA. Wanderer, an interactive viewer to explore DNA methylation and gene expression data in human cancer. Epigenet Chromatin (2015) 8:22. doi: 10.1186/s13072-015-0014-8

甲基化差異

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Figure 3. Differential DNA methylation uniquely associated to SLE or to pSS. (A) Box plots showing DNA methylation levels at unique DMCs in SLE compared to controls at FADD and HIF3A.

分析方法：minfi包。

文中還有提高EWASs的統(tǒng)計(jì)分析方法。

Ref: Shared and Unique Patterns of DNA Methylation in Systemic Lupus Erythematosus and Primary Sj?gren's Syndrome . Frontiers in Immunology, 2019.

URL=https://www.frontiersin.org/article/10.3389/fimmu.2019.01686

DOI=10.3389/fimmu.2019.01686

甲基化差異

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Fig. 3 Detailed DNA methylation map of the CHRNE gene. a (i) Boxplot and dot-plot of DNA methylation for individual neonatal control and ART samples at the two probes within the CHRNE gene that showed a significant difference between groups (adjusted p-value <0.05 (Bayesian levene’s test)). n =207 biologically independent birth samples, n =233 biologically independent adult samples. (ii) Boxplot and dot-plot of the same two probes in individual adult control and ART samples. The change is no longer significant in adult samples after correction for multiple testing, but the direction of methylation change persists. Boxplot elements are: center line-median; box limits-upper (Q3) and lower (Q1) quartiles; whiskers–smallest and largest non-outlier; points-outliers. b. Map of the CHRNE gene in hg19, showing EPIC probe locations. c Mean DNA methylation level at CHRNE for neonatal and adult non-ART and ART groups. Error bars are 95% confidence intervals. DMR1 is split into two: DMR1a that shows both ART and age specific DNA methylation differences and DMR1b that only shows ART-specific DNA methylation change. In addition, an age-specific DMR (DMR2) and a DMP are highlighted

方法：MissMethyl and minfi packages；文章里面還有講到DMR和DMP的分析。

Ref：NOVAKOVIC B, LEWIS S, HALLIDAY J, et al. Assisted reproductive technologies are associated with limited epigenetic variation at birth that largely resolves by adulthood[J]. Nature communications, 2019, 10(1):3922. DOI: 10.1038/s41467-019-11929-9.

甲基化和基因表達(dá)的相關(guān)性

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Matched methylation and gene expression data from The Cancer Genome Atlas were plotted to illustrate the correlation for selected cancer testis antigens (CTAs): (A) MAGEA1, (B) PAGE2, (C) CT83, and (D) SMC1B. The x axes give the β value of the region of the CTA 200 bp upstream of the transcription start site (TSS200) as a degree of methylation. The y axes give the gene expression as log2 transformed 1+ reads per kilobase of transcript per million mapped reads values of RNAseq.

這里用到的是TSS200，而不是單個(gè)probe。
Ref: [1] DJUREINOVIC D, HALLSTR?M B M, HORIE M, et al. Profiling cancer testis antigens in non-small-cell lung cancer[J]. JCI Insight, 2016, 1(10):e86837. DOI: 10.1172/jci.insight.86837.

甲基化和基因表達(dá)的相關(guān)性

Graphical representation of correlation of DNA methylation and gene expression of DMP-DEG pairs.

Graphical representation of correlation of DNA methylation and gene expression of DMP-DEG pairs. Red and blue dots represent SSc and HD individuals, respectively.

基因表達(dá)用Z-score的數(shù)據(jù)，甲基化也用normalized的數(shù)據(jù)。

Ref：[1] LI T, ORTIZ-FERNáNDEZ L, ANDRéS-LEóN E, et al. Epigenomics and transcriptomics of systemic sclerosis CD4+ T cells reveal long-range dysregulation of key inflammatory pathways mediated by disease-associated susceptibility loci[J]. Genome medicine, 2020, 12(1):81. DOI: 10.1186/s13073-020-00779-6.

甲基化和基因表達(dá)的相關(guān)性

Figure 2. Negative correlation of *USP44* gene expression and DNA methylation across 12 cancer types.

這個(gè)來自O(shè)ncotarget的一篇文章，

Ref：Wang XX, Xiao FH, Li QG, Liu J, He YH, Kong QP. Large-scale DNA methylation expression analysis across 12 solid cancers reveals hypermethylation in the calcium-signaling pathway. Oncotarget. 2017 Feb 14;8(7):11868-11876. doi: 10.18632/oncotarget.14417