DNA methylation in germ cell tumour aetiology: current understanding and outstanding questions

Qin

et al. 2013

Cell Physiol Biochem

Background: MiR-141 has been confirmed to be associated with various human diseases. However, whether miR-141 is involved in the pathogenesis of Hirschsprung's disease (HSCR) remains unknown. Here, we design the experiment to reveal the relationship between miR-141 and HSCR. Methods: Quantitative real-time PCR and Western blot were used to detect the expression levels of miR-141 and its potential genes in 70 tissues of HSCR compared with 60 controls. Bisulfite sequencing PCR (BSP) assay was applied to explain the possible mechanism of the aberrant expression level of miR-141. We employed a dual-luciferase reporter assay to validate the regulation relation between miR-141 and CD47/CUL3. Cell migration, proliferation, apoptosis, and cell cycle progression were examined by transwell assay, MTT assay, and flow cytometry, respectively. Results: MiR-141 was down-regulated whereas CD47 and CUL3 expression was increased in colon tissues from patients with HSCR compared with control group, The increased level of CD47 and CUL3 induced by miR-141 reduced proliferation and migration of 293T and SH-SY5Y cells. Furthermore, this suppression was reversed by reducing of CD47 and CUL3. Hypermethylation of a CpG Island in the promoter region of miR-141 gene was confirmed in HSCR tissues. Conclusion: Aberrant reduction of miR-141 may play an important role in the pathogenesis of HSCR with the inhibiting affection on cell migration and proliferation abilities. The present study demonstrates for the first time the role of miR-141 and its target genes in the occurrence of HSCR, and provides us a new direction for the study of the pathogenesis of Hirschsprung's disease.

Section: Discussionmentioning

confidence: 99%

Aberrant Reduction of MiR-141 Increased CD47/CUL3 in Hirschsprung's Disease

Qin

et al. 2013

Cell Physiol Biochem

“…5,6 GCTs are heterogeneous with regard to both tumor location and histology, which vary by sex, age at diagnosis and race/ethnicity and also impact survival. 2,[6][7][8][9][10][11][12] For example, tumors of mixed histology display a higher rate of death than other histologic subtypes in females. 12 In males diagnosed with testicular cancer at ages <40 years, nonseminoma histology is associated with a higher risk of death than seminoma.…”

Section: Introductionmentioning

confidence: 99%

“…GCTs are heterogeneous with regard to both tumor location and histology, which vary by sex, age at diagnosis and race/ethnicity and also impact survival . For example, tumors of mixed histology display a higher rate of death than other histologic subtypes in females .…”

Section: Introductionmentioning

confidence: 99%

Survival differences by race/ethnicity among children and adolescents diagnosed with germ cell tumors

Williams

Frazier

Poynter

2019

Intl Journal of Cancer

Survival differences by racial and ethnic group have been reported in children and adolescents with germ cell tumors (GCTs), but whether these differences depend on stage of disease is unclear. Using the SEER 18 registries (2000–2015), we examined GCT survival differences by race/ethnicity (non‐Hispanic white [NHW], Black, Asian/Pacific Islander [API], Hispanic) separately for males and females aged 0–19 years at diagnosis. We used Kaplan–Meier survival curves (Log‐Rank p values) to characterize survival differences. Cox proportional hazards models were used to estimate hazard ratios (HR) and 95% confidence intervals (95% CI) for the association between race/ethnicity and death. Using an inverse odds weighting mediation analysis, we estimated the association between race/ethnicity and death treating stage of disease as the mediator. There were no significant racial/ethnic survival differences among females. Male survival differed by race/ethnicity (p < 0.0001) with NHW males having the best survival. Compared to NHW, API and Hispanic males had significantly higher risks of death (API HR: 2.18; 95% CI: 1.32–3.56; Hispanic HR: 1.98; 95% CI: 1.42–2.78) (model adjusted for age and year at diagnosis, tumor histology and location, stage). This association was mediated by stage of disease only among Hispanic males with gonadal tumors (indirect HR: 1.18; 95% CI: 1.03–1.35). The increased risk of death after a testicular GCT diagnosis observed among Hispanic males was mediated by stage of disease. For API males and Hispanic males with extragonadal tumors, other unidentified factors including differences in exposures, tumor biology or treatment received may impact the observed racial/ethnic survival disparities.

“…2 Extragonadal tumours are more common in the paediatric age range compared to adolescent or young adult tumours, and are thought to arise from abnormal migration of PGCs during embryogenesis. 8,9 As germ cells undergo extensive epigenetic reprogramming during the embryonic and early developmental periods, 6,10–12 understanding differences in methylation patterns between histologic subtypes may shed light on aetiologic variation by histology as we work toward identifying important windows of exposure.…”

Section: Introductionmentioning

confidence: 99%

“…12,13 In general, paediatric tumours are less likely than adult cancers to result from the accumulation of mutations or DNA damage possibly due to the short latency period from birth to cancer diagnosis. 6,14 Therefore, other mechanisms such as aberrant DNA methylation in GCT development may play an essential role in GCT initiation and progression, particularly among paediatric GCTs.…”

Section: Introductionmentioning

confidence: 99%

Differences in DNA methylation profiles by histologic subtype of paediatric germ cell tumours: a report from the Children’s Oncology Group

et al. 2018

Background Abnormal DNA methylation may be important in germ cell tumour (GCT) aetiology, as germ cells undergo complete epigenetic reprogramming during development. GCTs show differences in global and promoter methylation patterns by histologic subtype. We conducted an epigenome-wide study to identify methylation differences by GCT histology. Methods Using the Illumina HumanMethylation450K array we measured methylation in 154 paediatric GCTs (21 germinomas/seminomas/dysgerminoma, 70 yolk sac tumours [YST], 9 teratomas, and 54 mixed histology tumours). We identified differentially methylated regions (DMRs) between GCT histologies by comparing methylation beta values. Results We identified 8,481 DMRs (FWER < 0.05). Unsupervised hierarchical clustering of individual probes within DMRs resulted in four high level clusters closely corresponding to tumour histology. Clusters corresponding to age, location, sex and FFPE status were not observed within these DMRs. Germinomas displayed lower levels of methylation across the DMRs relative to the other histologic subtypes. Pathway analysis on the top 10% of genes with differential methylation in germinomas/seminomas/dysgerminoma compared to YST suggested angiogenesis and immune cell-related pathways displayed decreased methylation in germinomas/seminomas/dysgerminoma relative to YST. Conclusions Paediatric GCT histologies have differential methylation patterns. The genes that are differentially methylated may provide insights into GCT aetiology including the timing of GCT initiation.