Your search keyword '"methylation-specific PCR"' showing total 298 results

1. Methylation of the ESR1 promoters in visceral adipose tissue and its relationship with obesity.

Author

Güçlü-Geyik, Filiz, Erginel, Turgay, Güleç, Çağrı, Köseoğlu-Büyükkaya, Pınar, and Erginel-Ünaltuna, Nihan

Abstract

Background: Obesity is associated with decreased ESR1 expression level in visceral adipose tissue. However, it is unclear exactly what mechanisms are responsible for this decline. The aim of this study was to investigate the impact of aberrant methylation of the ESR1 alternative promoters on decreased ESR1 expression and its connection to obesity. Methods: Visceral adipose tissues and peripheral blood cells were obtained from 21 patients (non-obese and obese) undergoing inguinal hernia or gallbladder removal. Alternative promoter regions, C, E2 and F of the ESR1 gene, were analyzed by Methylation-Specific PCR (MSP) and mRNA levels were measured by quantitative real-time PCR (qPCR) in both visceral adipose tissue and peripheral blood cells. All statistical analyses were performed by SPSS (23.0). Results: The methylation percentage in the three promoter regions of ESR1 was not different in obese individuals compared to non-obese individuals. We observed that promoter C had the highest methylation frequency in obese patients, although it was not statistically significant. Additionally, we observed that the hypermethylation of ESR1's promoter C was significantly associated with lower mRNA expression level in obesity (p = 0.020). Conclusion: This study suggests that methylation of ESR1 promoter C may be a factor in the development of obesity or a consequence of obesity. Further studies with advanced methods and larger study groups are needed to clarify this issue. [ABSTRACT FROM AUTHOR]

Published

2024

2. Evaluation of an In-House Genetic Testing Method for Confirming Prader-Willi and Angelman Syndromes in Sri Lanka.

Author

Kugalingam, Nirosha, de Silva, Deepthi, Rathnayake, Pyara, Atapattu, Navoda, Ranaweera, Dinali M., and Chandrasekharan, Naduviladath V.

Subjects

PRADER-Willi syndrome, GENETIC testing, ANGELMAN syndrome, TEST methods, GENETIC counseling, INTERFERON beta 1b

Abstract

Background: Prader-Willi syndrome (PWS, MIM 176,270) and Angelman syndrome (AS, MIM 105,830) are caused by imprinting defects of chromosome 15q11-13, with loss of maternal gene expression causing AS and paternal gene expression causing PWS. The diagnosis, once established in most cases by using a methylation-specific PCR test, enables appropriate therapeutic interventions and avoids the need for further investigations. Genetic testing for PWS/AS is limited in Sri Lanka (and in other low- and middle-income countries), mainly because parents are unable to pay for testing as these are not funded by the health service. Methods: Ninety cases (46 female) with clinical features suggesting PWS (n = 37) and AS (n = 53), referred by a pediatric endocrinologist and a pediatric neurologist, were recruited. Clinical information and blood samples were obtained following informed consent. DNA was extracted and methylation-specific PCR (MS-PCR) was performed following bisulfite modification of DNA by using an in-house method and a kit. Results were validated using known positive controls. Parent-child trio DNA samples were used in cases with confirmed PWS and AS to determine if the disease was due to a deletion or uniparental disomy. The cost of the MS-PCR testing of the two modification methods and the microsatellite analysis was determined. Results: Among the suspected PWS cases, 19/37 were positive, while 5/53 of the suspected AS cases were positive. The lower identification rate of AS is probably related to the overlap of clinical features of this condition with other disorders. The kit-based modification method was more reliable, less time-consuming, and cost-effective in our laboratory. Conclusions: The kit-based modification followed by MS-PCR described in this study enables more affordable genetic testing of suspected PWS/AS cases, and this is likely to improve patient care by targeting appropriate therapy for the affected cases. Parental genetic counselling is made possible regarding the low recurrence risk, especially where a deletion or uniparental disomy is confirmed. In MS-PCR, negative cases with a strong clinical suspicion of AS, UBE3A mutation testing is required. In addition, imprinting center mutation/deletion testing may also be needed in strongly clinically suspected, MS-PCR negative PWS and AS cases. [ABSTRACT FROM AUTHOR]

Published

2024

3. O6‐methylguanine methyltransferase promoter methylation status of glioblastoma cell line clonal population.

Author

Anan, Mitsuhiro, Del Maestro, Rolando Fausto, Hata, Nobuhiro, and Fujiki, Minoru

Abstract

Glioblastoma (GBM) remains a treatment‐resistant malignant brain tumor in large part because of its genetic heterogeneity and epigenetic plasticity. In this study, we investigated the epigenetic heterogeneity of GBM by evaluating the methylation status of the O6‐methylguanine methyltransferase (MGMT) promoter in individual clones of a single cell derived from GBM cell lines. The U251 and U373 GBM cell lines, from the Brain Tumour Research Centre of the Montreal Neurological Institute, were used for the experiments. To evaluate the methylation status of the MGMT promoter, pyrosequencing and methylation‐specific PCR (MSP) were used. Moreover, mRNA and protein expression levels of MGMT in the individual GBM clones were evaluated. The HeLa cell line, which hyper‐expresses MGMT, was used as control. A total of 12 U251 and 12 U373 clones were isolated. The methylation status of 83 of 97 CpG sites in the MGMT promoter were evaluated by pyrosequencing, and 11 methylated CpG sites and 13 unmethylated CpG sites were evaluated by MSP. The methylation status by pyrosequencing was relatively high at CpG sites 3–8, 20–35, and 7–83, in both the U251 and U373 clones. Neither MGMT mRNA nor protein was detected in any clone. These findings demonstrate tumor heterogeneity among individual clones derived from a single GBM cell. MGMT expression may be regulated, not only by methylation of the MGMT promoter but by other factors as well. Further studies are needed to clarify the mechanisms underlying the epigenetic heterogeneity and plasticity of GBM. [ABSTRACT FROM AUTHOR]

Published

2024

4. Epigenetically Modified DNA Fragments : What They Are and How They Can Be Used as Biomarkers of Diabetes Pathogenesis and Risk

Author

Tersey, Sarah A., Mirmira, Raghavendra G., Patel, Vinood B., Series Editor, and Preedy, Victor R., Series Editor

Published

2023

5. Genome-wide DNA methylation profiles analysis in primary warm autoimmune hemolytic anemia patients.

Author

Zhao, Manjun, Zhang, Yang, Yang, Jin, Chen, Lei, Zhang, Ziying, Wang, Huaquan, Shao, Zonghong, and Xing, Limin

Subjects

*AUTOIMMUNE hemolytic anemia, *DNA methylation, *VASCULAR endothelial growth factors, *PHOSPHOLIPASE D, *B cells, *DEMETHYLATION, *EPIGENOMICS

Abstract

Autoimmune hemolytic anemia (AIHA) is caused by auto-antibodies, secreted by overactivated B cells, directed against self-red blood cells, resulting in hemolysis. It found that aberrant DNA methylation in B cells can induce the production of autoantibodies. Therefore, we attempted to explore if similar aberrant DNA methylation occur in AIHA patients. A 49-year-old female wAIHA patient and a 47-year-old female healthy control (HC) were enrolled. Peripheral blood (PB) B cells DNA was extracted. After constructing genomic libraries, bisulfite genomic sequencing (BSP) and DNA methylation profiles were analyzed. BSP was verified using PB B cells from 10 patients with hemolysis, 10 patients with hemolytic remission, and 10 healthy controls (HCs) by Methylation-specific PCR. Total DNA methylation of whole-genome C bases (4.8%) and CG type bases (76.8%) in wAIHA patient were lower than those in the HC (5.3 and 82.5%, respectively) (p = 0.022 and p < 0.001). DNA methylation of C bases and CG type bases in whole-genome regulatory elements, such as coding sequence, up2Kb and down2Kb in the patient were also lower than those in the HC (p = 0.041, p = 0.038, and p = 0.029). 30,180 DNA-methylated regions (DMRs) on all 23 chromosomes were identified. DMR-related genes were mainly involved in the Rap1, phospholipase D, HIF-1, calcium, vascular endothelial growth factor (VEGF) and Ras signaling pathways. The DNA methylation spectrum of B cells in AIHA patients is different from that of HC, and the proportion of hypo-methylation regions is higher than that of HC. DMR-related genes are mainly related to some signaling pathways. [ABSTRACT FROM AUTHOR]

Published

2023

6. Diagnostic value of molecular approach in screening for fragile X premutation cases.

Author

Refeat, Miral M., El Saied, Mostafa M., and Abdel Raouf, Ehab R.

Abstract

Background : Fragile X syndrome (FXS) is the most common form of inherited intellectual disability, caused by CGG-repeats expansion (> 200 repeats). Premutation alleles (PM) (55–200 CGG repeats) are associated with tremor ataxia syndrome (FXTAS), fragile X-associated primary ovarian insufficiency (FXPOI), and autistic problems. Aim: To screen the frequency of premutation carriers using molecular diagnostic assays, in a cohort of Egyptian males with suspected clinical features of (FXS) checking for the presence of premutation alleles. Methods: The current study comprised 192 Egyptian male children, 92 participants presented with intellectual disability, delayed language development, autistic-like features, behavioral difficulties, anxiety, seizures, and depression compared to 100 healthy males. All cases were subjected to clinical and neuroimaging assessments, when indicated as well as molecular analysis using methylation-specific PCR (MS-PCR) and quantitative real-time PCR (qRT-PCR). Results: Thirty-four premutation carriers out of 92 Egyptian males (37%) of CGG repeats (55 to 200) were illustrated with elevated FMR1 mRNA expression level (p-value < 0.001). Additionally, 2 intermediate (IM) cases (0.03%) (45–55 CGG repeats) showed poor increase in expression level (p-value = 0.02838) plus 6 full mutation (FM) patients (0.07%) with (> 200 CGG repeats) (p-value < 0.001) resulted in FMR1 gene silence. Conclusion: Molecular diagnostic assay including (MS-PCR) and (qRT-PCR) proved to be a sensitive and rapid screening tool for the detection of premutation cases. Furthermore, the presence of positive correlation between FMR1 mRNA expression levels with CGG repeats in premutation cases could serve as a potential diagnostic marker. Application of these diagnostic tools on larger number clinically suspected cases is recommended. [ABSTRACT FROM AUTHOR]

Published

2023

7. Molecular aspects of ABCB1 and ABCG2 in Gallbladder cancer and its clinical relevance.

Author

Nimisha, Saluja, Sundeep Singh, Sharma, Abhay Kumar, Nekarakanti, Phani Kumar, Apurva, Kumar, Arun, Sattar, Real Sumayya Abdul, Anjum, Hasib, Batra, Vineeta Vijay, and Husain, Syed Akhtar

Abstract

The function of ABC transporters in the body is manifold; such as maintenance of homeostasis, effect on multi-drug resistance and their role in tumor initiation & progression. Evidence pointing towards the direct or indirect role of ABC transporter genes in particular; ABCB1 and ABCG2 in cancer genesis is increasing. However, their role in gallbladder cancer is unexplored. Therefore, we investigated the methylation status and expression pattern of ABCB1 and ABCG2in gallbladder carcinogenesis. The methylation and expression study of ABCB1/MDR1 and ABCG2/BCRP was performed in tumour and normal fresh tissue samples collected from 61 histopathologically diagnosed gallbladder cancer patients. The methylation status was analysed by Methylation-Specific PCR and expression was determined by Real-Time PCR and Immunohistochemistry. Hypomethylation of ABCB1 and ABCG2 was found in 44 (72.13%) and 48 (78.6%) cases, respectively. ABCB1 hypomethylation pattern showed association with female patients (p = 0.040) and GradeII tumors (p = 0.036) while, ABCG2 hypomethylation was more frequent in early tumors (T1-T2). The mRNA expression ofABCB1 and ABCG2 was up-regulated in 33 (54.10%) and 41 (67.21%) patients with fold change of 4.7 and 5.5, respectively. The mRNA expression of both genes showed association with Grade II tumours and the increased fold change of ABCG2 was higher in (T1-T2) depth of invasion (p = 0.02) and Stage I–II disease (p = 0.08). The protein expression on IHC was strongly positive for ABCB1/MDR1and ABCG2/BCRP in 32 (52.46%) and 45 (73.77%) patients, respectively. The protein expression in ABCG2 showed association with patients age > 50 years (p = 0.04) and GradeII differentiation (p = 0.07). Interestingly, the hypomethylation of both the genes showed significant correlation with increased expression. ABCB1/MDR1 and ABCG2/BCRP hypomethylation and overexpression could have a potential role in gallbladder cancer tumorigenesis especially in early stages. The epigenetic change might be a plausible factor for altered gene expression of ABCB1 and ABCG2 in gallbladder cancer. [ABSTRACT FROM AUTHOR]

Published

2023

8. Genome-wide DNA methylation profiles analysis in primary warm autoimmune hemolytic anemia patients

Author

Manjun Zhao, Yang Zhang, Jin Yang, Lei Chen, Ziying Zhang, Huaquan Wang, Zonghong Shao, and Limin Xing

Subjects

Warm autoimmune hemolytic anemia, B lymphocytes, DNA methylation, Methylation-specific PCR, Bisulfite genomic sequence, Autoimmunity disease, Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

ABSTRACTBackground Autoimmune hemolytic anemia (AIHA) is caused by auto-antibodies, secreted by overactivated B cells, directed against self-red blood cells, resulting in hemolysis. It found that aberrant DNA methylation in B cells can induce the production of autoantibodies. Therefore, we attempted to explore if similar aberrant DNA methylation occur in AIHA patients.Methods A 49-year-old female wAIHA patient and a 47-year-old female healthy control (HC) were enrolled. Peripheral blood (PB) B cells DNA was extracted. After constructing genomic libraries, bisulfite genomic sequencing (BSP) and DNA methylation profiles were analyzed. BSP was verified using PB B cells from 10 patients with hemolysis, 10 patients with hemolytic remission, and 10 healthy controls (HCs) by Methylation-specific PCR.Results Total DNA methylation of whole-genome C bases (4.8%) and CG type bases (76.8%) in wAIHA patient were lower than those in the HC (5.3 and 82.5%, respectively) (p = 0.022 and p

Published

2023

9. BRCA1 Promoter Hypermethylation in Malignant Breast Tumors and in the Histologically Normal Adjacent Tissues to the Tumors: Exploring Its Potential as a Biomarker and Its Clinical Significance in a Translational Approach.

Author

Oubaddou, Yassire, Oukabli, Mohamed, Fenniche, Salma, Elktaibi, Abderrahim, Elochi, Mohamed Reda, Al Bouzidi, Abderrahmane, Qmichou, Zineb, Dakka, Nadia, Diorio, Caroline, Richter, Antje, Bakri, Youssef, and Ameziane El Hassani, Rabii

Subjects

*BREAST, *BRCA genes, *TUMOR suppressor genes, *BREAST tumors, *BIOMARKERS, *PROMOTERS (Genetics)

Abstract

The hypermethylation status of the promoter region of the breast cancer 1 (BRCA1), a well-known tumor suppressor gene, has been extensively investigated in the last two decades as a potential biomarker for breast cancer. In this retrospective study, we investigated the prevalence of BRCA1 promoter methylation in 84 human breast tissues, and we correlated this epigenetic silencing with the clinical and histopathological parameters of breast cancer. We used methylation-specific PCR (MSP) to analyze BRCA1 promoter hypermethylation in 48 malignant breast tumors (MBTs), 15 normal adjacent tissues (NATs), and 21 benign breast lesions (BBLs). The results showed that BRCA1 promoter hypermethylation was higher in MBTs (20/48; 41.67%) and NATs (7/15; 46.67%) compared to BBLs (4/21; 19.05%). The high percentage of BRCA1 hypermethylation in the histologically normal adjacent tissues to the tumors (NATs) suggests the involvement of this epigenetic silencing as a potential biomarker of the early genomic instability in NATs surrounding the tumors. The detection of BRCA1 promoter hypermethylation in BBLs reinforces this suggestion, knowing that a non-negligible rate of benign breast lesions was reported to evolve into cancer. Moreover, our results indicated that the BRCA1 promoter hypermethylated group of MBTs exhibited higher rates of aggressive features, as indicated by the SBR III grade (14/19; 73.68%), elevated Ki67 levels (13/16; 81.25%), and Her2 receptor overexpression (5/20; 25%). Finally, we observed a concordance (60%) in BRCA1 promoter hypermethylation status between malignant breast tumors and their paired histologically normal adjacent tissues. This study highlights the role of BRCA1 promoter hypermethylation as a potential useful biomarker of aggressiveness in MBTs and as an early marker of genomic instability in both histological NATs and BBLs. [ABSTRACT FROM AUTHOR]

Published

2023

10. Identification of DNA methylation change in TCF7L2 gene in the blood of type 2 diabetes mellitus as a predictive biomarker in Iraq Kurdistan region by using methylation-specific PCR

Author

Smail Harem Othman and Mohamad Dlnya Asaad

Subjects

type 2 diabetes mellitus, methylation-specific pcr, tcf7l2, roc curve, bisulfite-converted dna, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Objective. Nowadays, type 2 diabetes mellitus (T2D) is the most common chronic endocrine disorder affecting an estimated 5–10% of adults worldwide, and this disease also rapidly increased among the population in the Kurdistan region. This research aims to identify DNA methylation change in the TCF7L2 gene as a possible predictive T2D biomarker.

Published

2023

11. Study of the Methylation of Bovine GSTP1 Gene under the Influence of Pesticide Mospilan 20SP Alone and in Combination with Pesticide Orius 25EW.

Author

HALUŠKOVÁ, JANA, HOLEČKOVÁ, BEÁTA, LUPTÁKOVÁ, LENKA, KOŠUTH, JÁN, SCHWARZBACHEROVÁ, VIERA, GALDÍKOVÁ, MARTINA, and KOLENIČOVÁ, SIMONA

Subjects

METHYLATION, DNA methylation, BOS, GENE expression, PROMOTERS (Genetics), PESTICIDES

Abstract

DNA methylation, one of the most studied epigenetic mechanisms, when present in the promoter region of genes, causes inhibition of gene expression, and conversely, hypomethylation of these regions enables gene expression. DNA methylation is susceptible to nutritional and environmental influences, and undesirable alterations in methylation patterns manifested in changes in the expression of relevant genes can lead to pathological consequences. In the present work, we studied the methylation status of the bovine GSTP1 gene under the influence of pesticide Mospilan 20SP alone and in combination with pesticide Orius 25EW in in vitro proliferating bovine lymphocytes. We employed methylation-specific PCR, and when studying the effect of pesticide combinations, we also used its real-time version followed by a melting procedure. Our results showed that Mospilan 20SP alone at 5, 25, 50, and 100 µg.ml–1 and 5, 10, 25, and 50 µg.ml–1 for the last 4 and 24 hours of culture with in vitro proliferating bovine lymphocytes, respectively, did not induce methylation of the bovine GSTP1 gene. The same results were revealed when studying the effect of the combination of the pesticides added to the lymphocyte cultures for the last 24 hours of cultivation in the following amounts: 1.25, 2.5, 5, 10, and 25 µg.ml–1 of Mospilan 20SP and 1.5, 3, 6, 15, and 30 µg.ml–1 of Orius 25EW. We have also revealed that the less laborious real-time MSP followed by a melting procedure may replace MSP for studying the methylation status of the GSTP1 gene. [ABSTRACT FROM AUTHOR]

Published

2023

12. Detection and relevance of epigenetic markers on ctDNA: recent advances and future outlook

Author

Evi Lianidou

Subjects

cell‐free DNA, circulating tumor cells, circulating tumor DNA, DNA methylation, methylation‐specific PCR, minimal residual disease, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Liquid biopsy, a minimally invasive approach, is a highly powerful clinical tool for the real‐time follow‐up of cancer and overcomes many limitations of tissue biopsies. Epigenetic alterations have a high potential to provide a valuable source of innovative biomarkers for cancer, owing to their stability, frequency, and noninvasive accessibility in bodily fluids. Numerous DNA methylation markers are now tested in circulating tumor DNA (ctDNA) as potential biomarkers, in various types of cancer. DNA methylation in combination with liquid biopsy is very powerful in identifying circulating epigenetic biomarkers of clinical importance. Blood‐based epigenetic biomarkers have a high potential for early detection of cancer since DNA methylation in plasma can be detected early during cancer pathogenesis. In this review, we summarize the latest findings on DNA methylation markers in ctDNA for early detection, prognosis, minimal residual disease, risk of relapse, treatment selection, and resistance, for breast, prostate, lung, and colorectal cancer.

Published

2021

13. Frequent Downregulation and Promoter Hypermethylation of DLC1: Relationship with Clinical Outcome in Gallbladder Cancer.

Author

Singh, Deepika, Bharti, Amisha, Biswas, Dipanjan, Tewari, Mallika, Kar, Amrita Ghosh, Ansari, Mumtaz Ahmed, Singh, Sunita, and Narayan, Gopeshwar

Abstract

Introduction: Down regulation of DLC1 is associated with poor prognosis in many cancers, however, its role in gallbladder cancer (GBC) is still unclear. In present study, we investigated the expression profile and promoter methylation status of DLC1. Methods: Expression profiles of DLC1 in 55 GBC and their paired adjacent control samples were analyzed through real time RT-PCR and immunohistochemistry. The mRNA data was correlated with clinico-pathological parameters. Promoter hypermethylation was analyzed through MSP. Results: DLC1 shows downregulation in 76.4%, upregulation in 10.9% whereas no change in 12.7% of GBC samples. Its underexpression shows significant correlation with tumor grade and nodal spread. IHC shows cytoplasmic expression of DLC1 in normal as well as tumor samples. IHC result was concordant to mRNA result. Samples having downregulated DLC1 expression show heterozygous methylation in 83.3% of samples and homozygous methylation in 9.5% of samples whereas 7% of samples have no methylation. Kaplan–Meier analysis shows patient with decreased mRNA of DLC1 have significant low mean survival compared to patients with higher mRNA expression of DLC1. Conclusion: Our findings suggested that dysregulated expression of DLC1 and its hypermethylation may be one of the events playing roles in tumorigenesis of GBC and may serve as a potential target for development of future GBC gene therapy. [ABSTRACT FROM AUTHOR]

Published

2022

14. Principles of PCR

Author

van Pelt-Verkuil, E., te Witt, R., van Pelt-Verkuil, E., editor, van Leeuwen, W.B., editor, and te Witt, R., editor

Published

2019

15. Cohesin RAD21 Gene Promoter Methylation Correlated with Better Prognosis in Breast Cancer Patients.

Author

Cui, Rongrong, Chen, Pu, Wang, Yuanyuan, Lu, Rong, Ji, Meiju, Hou, Peng, and Qu, Yiping

Subjects

*BREAST cancer prognosis, *CANCER prognosis, *COHESINS, *BREAST, *METHYLATION, *NATURAL immunity, *PROGRESSION-free survival

Abstract

RAD21 plays multiple roles in numerous cancers. In breast cancer (BC), a high level of RAD21 correlates with poor disease outcomes and resistance to chemotherapy. However, data regarding RAD21 promoter methylation in BC tissue and its correlation with clinical outcomes in patients with BC remain limited. Here, we investigated the clinicopathological features associated with the methylation status of RAD21 in BC to figure out its possible role in pathogenesis and the formation of breast carcinogenesis. The methylation status of the RAD21 gene was significantly associated with better clinical outcomes in patients with BC. [ABSTRACT FROM AUTHOR]

Published

2022

16. Clinical Utility of Methylation-Specific Multiplex Ligation-Dependent Probe Amplification for the Diagnosis of Prader-Willi Syndrome and Angelman Syndrome.

Author

Boram Kim, Yongsook Park, Sung Im Cho, Man Jin Kim, Jong-Hee Chae, Ji Yeon Kim, Moon-Woo Seong, and Sung Sup Park

Subjects

PRADER-Willi syndrome, ANGELMAN syndrome, GENOMIC imprinting, POLYMERASE chain reaction, MOLECULAR probes, DIAGNOSIS, GENE amplification

Abstract

Background: Prader-Willi syndrome (PWS) and Angelman syndrome (AS) are genomic imprinting disorders that are mainly caused by a deletion on 15q11-q13, the uniparental disomy of chromosome 15, or an imprinting defect. We evaluated the utility of methylation-specific multiplex ligation-dependent probe amplification (MS-MLPA) as a diagnostic tool and for demonstrating the relationship between molecular mechanisms and clinical presentation. Methods: We performed MS-MLPA using DNA samples from 93 subjects (45 PWS, 24 AS, and 24 non-PWS/AS controls) who had previously undergone MS-PCR for the diagnosis of PWS/AS. We compared the results of both assays, and patients' clinical phenotypes were reviewed retrospectively. Results: MS-MLPA showed a 100% concordance rate with MS-PCR. Among the 45 PWS patients, 26 (57.8%) had a deletion of 15q11-q13, and the others (42.2%) had uniparental disomy 15 or an imprinting defect. Among the 24 AS patients, 16 (66.7%) had a deletion of 15q11-q13, 7 AS patients (29.2%) had uniparental disomy 15 or an imprinting defect, and one AS patient (4.2%) showed an imprinting center deletion. Conclusions: MS-MLPA has clinical utility for the diagnosis of PWS/AS, and it is superior to MS-PCR in that it can identify the molecular mechanism underlying the disease. [ABSTRACT FROM AUTHOR]

Published

2022

17. Stratifin in ocular surface squamous neoplasia and its association with p53.

Author

Chauhan, Sheetal, Sen, Seema, Chauhan, Shyam S., Pushker, Neelam, Tandon, Radhika, Kashyap, Seema, Vanathi, Murugesan, and Bajaj, Mandeep S.

Subjects

*REVERSE transcriptase polymerase chain reaction, *GENE expression, *TUMORS, *CELLULAR signal transduction, *P53 protein, *SUNBURN

Abstract

Purpose: Sunlight‐induced p53 mutations are known to contribute towards increased risk of ocular surface squamous neoplasia (OSSN). Stratifin (14‐3‐3σ)/HEM (human epithelial marker) is a p53‐mediated inhibitor of cell cycle progression and has been shown to be a target of epigenetic deregulation in various carcinomas. In the present study, Stratifin expression, its promoter methylation status as well as expression of mutant p53 in early and advanced AJCC stages (8th edition) of OSSN, was evaluated. Methods: Sixty‐four OSSN [20 conjunctival intraepithelial neoplasia (CIN) and 44 squamous cell carcinoma (SCC)] patients were registered for this study, and they were followed up for 36–58 months (mean 48 ± 3.6). Immunoexpression of Stratifin and mutant p53 protein, mRNA expression of Stratifin by reverse transcription polymerase chain reaction (PCR) and methylation status of Stratifin by methylation‐specific PCR, was undertaken. Results: Hypermethylation of Stratifin promoter in 63% (40/64), loss of Stratifin expression in 75% (48/64) and downregulation of Stratifin mRNA in 61% (39/64) were observed. Stratifin hypermethylation was significantly associated with reduced disease‐free survival in both early and advanced T stage SCC cases. Expression of mutant p53 expression was seen in 48% (31/64) OSSN cases. Of the 31 patients with mutant p53 expression, 87% (27/31) also demonstrated loss of Stratifin immunoexpression. A significant association was seen between mutant p53 expression and Stratifin loss (p = 0.01) in advanced T stage SCC cases. Conclusions: Hypermethylation of Stratifin gene and its reduced mRNA expression both are potential biomarkers for identifying high‐risk OSSN patients. Aberrant methylation of Stratifin and simultaneous mutant p53 expression implicates involvement of p53‐Stratifin mediated signalling pathway in the pathogenesis of OSSN. [ABSTRACT FROM AUTHOR]

Published

2021

18. Case Report: An Atypical Angelman Syndrome Case With Obesity and Fulfilled Autism Spectrum Disorder Identified by Microarray

Author

Areerat Hnoonual, Phawin Kor-anantakul, Chariyawan Charalsawadi, Juthamas Worachotekamjorn, and Pornprot Limprasert

Subjects

angelman syndrome, autism, methylation-specific PCR, microarray, uniparental disomy, Genetics, QH426-470

Abstract

Autism spectrum disorder (ASD) is a group of neurodevelopmental disorders which are etiologically heterogeneous. Chromosomal microarray is now recommended as the first-tier clinical diagnostic test for ASD. We performed chromosomal microarray in 16 Thai patients with ASD using an Illumina HumanCytoSNP-12 v2.1 array and found one case with uniparental disomy (UPD) of chromosome 15. Methylation-specific PCR showed abnormal methylation of the maternal SNRPN allele. Haplotype analysis revealed that the patient had received both chromosomes 15 from his father. These results were consistent with Angelman syndrome. However, his clinical features had no clinical significance for classic Angelman syndrome. He had first presented at the pediatric clinic with no speech, poor social interaction skills and repetitive behaviors consistent with ASD based on the DSM-IV criteria at 2 years of age and later confirmed by ADOS at 5 years of age. He was strikingly overweight but had no dysmorphic facies, seizures nor ataxia and was diagnosed as non-syndromic ASD, a diagnosis which was believed until at 10 years of age, his DNA was included for analysis in this current cohort study. Our findings suggest that ASD patients with unknown etiology should be considered for methylation-specific PCR testing for Angelman syndrome where chromosomal microarray is not available. In the study, we also review the clinical features of Angelman syndrome caused by UPD and the frequency of ASD in individuals with Angelman syndrome.

Published

2021

19. Case Report: An Atypical Angelman Syndrome Case With Obesity and Fulfilled Autism Spectrum Disorder Identified by Microarray.

Author

Hnoonual, Areerat, Kor-anantakul, Phawin, Charalsawadi, Chariyawan, Worachotekamjorn, Juthamas, and Limprasert, Pornprot

Subjects

AUTISM spectrum disorders, ANGELMAN syndrome, PEDIATRIC clinics, DIAGNOSIS, CHILDREN with autism spectrum disorders, SOCIAL skills

Abstract

Autism spectrum disorder (ASD) is a group of neurodevelopmental disorders which are etiologically heterogeneous. Chromosomal microarray is now recommended as the first-tier clinical diagnostic test for ASD. We performed chromosomal microarray in 16 Thai patients with ASD using an Illumina HumanCytoSNP-12 v2.1 array and found one case with uniparental disomy (UPD) of chromosome 15. Methylation-specific PCR showed abnormal methylation of the maternal SNRPN allele. Haplotype analysis revealed that the patient had received both chromosomes 15 from his father. These results were consistent with Angelman syndrome. However, his clinical features had no clinical significance for classic Angelman syndrome. He had first presented at the pediatric clinic with no speech, poor social interaction skills and repetitive behaviors consistent with ASD based on the DSM-IV criteria at 2 years of age and later confirmed by ADOS at 5 years of age. He was strikingly overweight but had no dysmorphic facies, seizures nor ataxia and was diagnosed as non-syndromic ASD, a diagnosis which was believed until at 10 years of age, his DNA was included for analysis in this current cohort study. Our findings suggest that ASD patients with unknown etiology should be considered for methylation-specific PCR testing for Angelman syndrome where chromosomal microarray is not available. In the study, we also review the clinical features of Angelman syndrome caused by UPD and the frequency of ASD in individuals with Angelman syndrome. [ABSTRACT FROM AUTHOR]

Published

2021

20. PCSK9 genetic (rs11591147) and epigenetic (DNA methylation) modifications associated with PCSK9 expression and serum proteins in CAD patients.

Author

Shyamala, Nivas, Gundapaneni, Kishore Kumar, Galimudi, Rajesh Kumar, Tupurani, Mohini Aiyengar, Padala, Chiranjeevi, Puranam, Kaushik, Kupsal, Keerthi, Kummari, Ramanjaneyulu, Gantala, Srilatha Reddy, Nallamala, Krishna Reddy, Sahu, Sanjib K., and Hanumanth, Surekha Rani

Abstract

Introduction: Proprotein convertase subtilisin/kexin type 9 (PCSK9) genetic polymorphisms play a significant role in cholesterol homeostasis. Therefore, we aimed to investigate the association of PCSK9 genetic variations NM_174936.3:c.137G>T (R46L, rs11591147) and NM_174936.3:c.1120G>T (D374Y, rs137852912), as well as promoter DNA methylation status, with mRNA expression and circulating serum protein levels in coronary artery disease (CAD) patients. Methods: The present study includes 300 CAD cases and 300 controls from South India. Biochemical assays were performed using commercially available kits. PCSK9 rs11591147 and rs137852912 polymorphisms were analyzed by the polymerase chain reaction (PCR)‐restriction fragment length polymorphism method, whereas promoter DNA methylation status and gene expression were determined using methylation specific PCR and quantitative PCR respectively. Results: The genotypic distribution of PCSK9 rs11591147 revealed that individuals with the TT‐genotype and T‐allele have a reduced risk for CAD. Furthermore, patients with the PCSK9 rs11591147 TT genotype have a significantly lower total cholesterol and low‐density lipoprotein‐cholesterol levels and also higher high‐density lipoprotein‐cholesterol levels than individuals with the GG genotype. Logistic regression analysis has shown that the GG and GT (p = 1.51 × 10–8, p = 1.47 × 10–9) genotypes predicted the risk for CAD with an odds ratio of 5.8 and 7.3 respectively. In addition, individuals with the TT genotype were hypermethylated at promoter DNA of PCSK9, resulting in lower mRNA expression and circulating serum proteins than in individuals with the GG genotype. In silico analyses revealed that rs11591147 T‐allele has protein destabilizing capacity. Conclusions: In conclusion, the present study indicates that the PCSK9 gene expression and circulating serum protein levels are not only associated with rs11591147 genotype, but also with promoter DNA methylation. Furthermore, the findings with respect to both single nucleotide polymorphism and promoter DNA methylation may open avenues for novel treatment possibilities targeting PCSK9 for CAD management. [ABSTRACT FROM AUTHOR]

Published

2021

21. The Preliminary Study of Pesticide Mospilan Effect on the GSTP1 Gene Methylation in Bovine Lymphocytes

Author

Halušková J., Holečková B., Staničová J., and Verebová V.

Subjects

bovine, dna methylation, gstp1, methylation-specific pcr, mospilan, pesticide exposure, Veterinary medicine, SF600-1100

Abstract

The epigenetic mechanisms represent a dynamic, reversible and heritable manner modulating gene expression during the life cycle of an animal organism. They generate the specific epigenetic marks which constitute so-called epigenome. One of the most studied epigenetic mechanisms/marks is DNA methylation which is, similarly as the whole epigenome, susceptible to environmental and nutritional influences. The aberrations of the DNA methylation profile may alter gene expression leading to pathologic consequences. Pesticides along with their pest-reducing effects may also negatively affect non-target organisms. In our preliminary study, we investigated an effect of the pesticide Mospilan on the DNA methylation of the bovine GSTP1 gene which plays an important role in the cell detoxification processes. The specific primers for the GSTP1 Methylation-specific PCR (MSP) analysis were proposed and tested with the DNA from the Mospilan-treated bovine lymphocytes. It seems that the pesticide with the concentration of 100 µg.ml−1 did not induce DNA methylation changes in GSTP1 gene in bovine lymphocytes.

Published

2019

22. Detection and relevance of epigenetic markers on ctDNA: recent advances and future outlook.

Author

Lianidou, Evi

Abstract

Liquid biopsy, a minimally invasive approach, is a highly powerful clinical tool for the real‐time follow‐up of cancer and overcomes many limitations of tissue biopsies. Epigenetic alterations have a high potential to provide a valuable source of innovative biomarkers for cancer, owing to their stability, frequency, and noninvasive accessibility in bodily fluids. Numerous DNA methylation markers are now tested in circulating tumor DNA (ctDNA) as potential biomarkers, in various types of cancer. DNA methylation in combination with liquid biopsy is very powerful in identifying circulating epigenetic biomarkers of clinical importance. Blood‐based epigenetic biomarkers have a high potential for early detection of cancer since DNA methylation in plasma can be detected early during cancer pathogenesis. In this review, we summarize the latest findings on DNA methylation markers in ctDNA for early detection, prognosis, minimal residual disease, risk of relapse, treatment selection, and resistance, for breast, prostate, lung, and colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2021

23. Prospective study to validate the clinical utility of DNA diagnosis of peritoneal fluid cytology test in gastric cancer.

Author

Harada, Hiroki, Soeno, Takafumi, Nishizawa, Nobuyuki, Washio, Marie, Sakuraya, Mikiko, Ushiku, Hideki, Niihara, Masahiro, Hosoda, Kei, Kumamoto, Yusuke, Naitoh, Takeshi, Sangai, Takafumi, Hiki, Naoki, and Yamashita, Keishi

Abstract

The clinical efficacy of DNA cytology test (CY) in gastric cancer (GC) has been retrospectively proposed using cancer‐specific methylation of cysteine dioxygenase type 1 (CDO1). We confirmed the clinical utility of DNA CY in a prospective cohort. Four hundred GC samples were prospectively collected for washing cytology (UMIN000026191), and detection of the DNA methylation of CDO1 was assessed by quantitative methylation‐specific PCR in the sediments. Endpoint was defined as the match rate between conventional CY1 and DNA CY1 (diagnostic sensitivity), and the DNA CY0 rate (diagnostic specificity) in pStage IA. DNA CY1 was detected in 45 cases (12.5%), while CY1 was seen in 31 cases (8.6%) of 361 chemotherapy‐naïve samples, where the sensitivity and specificity of the DNA CY in the peritoneal solutions were 74.2% and 96.5%, respectively. The DNA CY was positive for 3.5/0/4.9/11.4/58.8% in pStage IA/IB/II/III/IV, respectively (P <.01). In the multivariate analysis, DNA CY1 was independently correlated with pathological tumor depth (pT) (P =.0012), female gender (P =.0099), CY1 (P =.0135), P1 (P =.019), and carcinoembryonic antigen (CEA) (P =.036). The combination of DNA CY1 and P factor nearly all covered the potential peritoneal dissemination (P1 and/or CY1 and/or DNA CY1) (58/61:95.1%). DNA CY1 had a significantly poorer prognosis than DNA CY0 in GC patients (P <.0001). DNA CY1 detected by CDO1 promoter DNA methylation has a great value to detect minimal residual disease of the peritoneum in GC clinics, representing poor prognosis as a novel single DNA marker. [ABSTRACT FROM AUTHOR]

Published

2021

24. Evaluation of MGMT Gene Methylation in Neuroendocrine Neoplasms.

Author

Monica, Rosa Della, Cuomo, Mariella, Visconti, Roberta, Mauro, Annabella di, Buonaiuto, Michela, Costabile, Davide, De Riso, Giulia, Risi, Teodolinda Di, Guadagno, Elia, Tafuto, Roberto, Lamia, Sabrina, Ottaiano, Alessandro, Cappabianca, Paolo, Del Basso de Caro, Maria Laura, Tatangelo, Fabiana, Hench, Juergen, Frank, Stephan, Tafuto, Salvatore, and Chiariotti, Lorenzo

Subjects

NEUROENDOCRINE tumors, O6-Methylguanine-DNA Methyltransferase, ALKYLATING agents, METHYLATION, BRAIN tumors

Abstract

Unresectable neuroendocrine neoplasms (NENs) often poorly respond to standard therapeutic approaches. Alkylating agents, in particular temozolomide, commonly used to treat high-grade brain tumors including glioblastomas, have recently been tested in advanced or metastatic NENs, where they showed promising response rates. In glioblastomas, prediction of response to temozolomide is based on the assessment of the methylation status of the MGMT gene, as its product, O 6-methylguanine-DNA methyltransferase, may counteract the damaging effects of the alkylating agent. However, in NENs, such a biomarker has not been validated yet. Thus, we have investigated MGMT methylation in 42 NENs of different grades and from various sites of origin by two different approaches: in contrast to methylation-specific PCR (MSP), which is commonly used in glioblastoma management, amplicon bisulfite sequencing (ABS) is based on high-resolution, next-generation sequencing and interrogates several additional CpG sites compared to those covered by MSP. Overall, we found MGMT methylation in 74% (31/42) of the NENs investigated. A higher methylation degree was observed in well-differentiated tumors and in tumors originating in the gastrointestinal tract. Comparing MSP and ABS results, we demonstrate that the region analyzed by the MSP test is sufficiently informative of the MGMT methylation status in NENs, suggesting that this predictive parameter could routinely be interrogated also in NENs. [ABSTRACT FROM AUTHOR]

Published

2020

25. Promoter hypermethylation of cysteine dioxygenase type 1 in patients with non-small cell lung cancer.

Author

Yin, Wei, Wang, Xiang, Li, Yunping, Wang, Bin, Song, Mingzhe, Hulbert, Alicia, Chen, Chen, and Yu, Fenglei

Subjects

*NON-small-cell lung carcinoma

Abstract

In the present study, promoter hypermethylation of cysteine dioxygenase type 1 (CDO1) was evaluated in non-small cell lung cancer (NSCLC) tissues to assess the value of CDO1 as a novel biomarker to improve the diagnosis of NSCLC. Tumor tissue samples and corresponding normal lung tissue samples from 42 patients with NSCLC were obtained at the Department of Thoracic Surgery, The Second Xiangya Hospital (Changsha, China). Conventional methylation-specific PCR (cMSP) and methylation-on-beads followed by quantitative methylation-specific PCR (MOB-qMSP) were used to analyze the tumor and normal lung tissue samples. Using these two methods, promoter DNA hypermethylation of the CDO1 gene was detected in 59.4 and 71.0% of tumor tissues of patients with NSCLC and in 9.4 and 0% of normal lung tissue, respectively. Compared with the rate of methylation in the well-differentiated NSCLC tissues (15.4 and 55.6%, respectively), the rate of CDO1 gene promoter methylation was higher in the poorly differentiated tissues (89.5 and 92.3%, respectively). Overall, it was demonstrated that the MOB-qMSP method had a higher positive detection rate for CDO1 hypermethylation compared with the cMSP method. In conclusion, CDO1 gene promoter hypermethylation was more frequently observed in NSCLC tissues compared with in normal lung tissues, and a high methylation frequency of the CDO1 gene in biopsy specimens of NSCLC was associated with the degree of differentiation. [ABSTRACT FROM AUTHOR]

Published

2020

26. TET2 promotor methylation and TET2 protein expression in pediatric posterior fossa ependymoma.

Author

Pierscianek, Daniela, Teuber‐Hanselmann, Sarah, Ahmadipour, Yahya, Darkwah Oppong, Marvin, Unteroberdörster, Meike, Müller, Oliver, Jabbarli, Ramazan, Sure, Ulrich, Zhu, Yuan, and El Hindy, Nicolai

Subjects

*PROTEIN expression, *METHYLATION, *TUMORS in children, *ARACHNOID cysts, *P16 gene, *DNA methylation, *BRAIN tumors, *CANCER stem cells

Abstract

Pediatric posterior fossa ependymoma (PF) is one of the most common brain tumors in children. Recently, two subtypes of PF were identified. PF‐A has a dismal prognosis and shows a hypermethylation phenotype, whereas PF‐B shows a great genomic instability. The ten‐eleven translocation methylcytosine dioxygenase 2 (TET2) gene (TET2) has been linked to the regulation of DNA methylation. We analyzed TET2 promotor methylation and protein expression to assess the role of TET2 in PF. Medical records of all PF cases treated in our institution between 1993 and 2015 were evaluated regarding tumor histology, grade, tumor location, gender, age, tumor recurrence, distant metastasis, survival and time to progression. Subsequently, we analyzed TET2 promotor methylation using methylation‐specific polymerase chain reaction. TET2 protein expression was assessed using immunohistochemistry. Low TET2 expression was detected in seven of 17 cases. There was an association between low TET2 expression and tumor recurrence (P = 0.049). A TET2 promotor methylation was detected in five of 10 cases. There was no association between the TET2 promotor methylation with recurrence, tumor grade or gender. TET2 promotor methylation and low TET2 expression was detected in a subgroup of PF. Our data show an association between low TET2 expression and tumor recurrence in PF. [ABSTRACT FROM AUTHOR]

Published

2020

27. Evaluation of the Epigenetic Demethylation of NRF2, a Master Transcription Factor for Antioxidant Enzymes, in Colorectal Cancer.

Author

Taheri, Zahra, Aghdaei, Hamid Asadzadeh, Irani, Shiva, Modarressi, Mohammad Hossein, and Noormohammadi, Zahra

Subjects

*DEMETHYLATION, *COLORECTAL cancer, *DNA methyltransferases, *TRANSCRIPTION factors, *DNA demethylation, *EPIGENETICS, *FETAL hemoglobin

Abstract

Background: Epigenetic changes in CpG islands of the promoter regions of homeostasis-related genes, including nuclear factor erythroid 2-related factor 2 (NRF2), have been shown to hold a significant role in the development of colorectal cancer. Therefore, we aimed to examine the DNA demethylation pattern of the NRF2 promoter region in cancerous lesions from patients with colorectal cancer and the association of methylation status with clinicopathological features in the Iranian population. Methods: In this cross-sectional study, 114 colorectal tissue samples were collected. These samples included: 34 tumour tissue samples, 60 precancerous polyps, and 20 normal tissue samples. The promoter methylation status of the NRF2 gene was examined using methylation-specific PCR. Additionally, the relationship between the methylation status and the clinicopathological features was investigated. Results: The frequency of NRF2 demethylation in the tumour samples was significantly higher compared to the polyp tissues (p= 0.003) and normal tissue (p= 0.009), indicating that cancerous colorectal tissues exhibit increased demethylation of the NRF2 promoter. After examining the demethylation status of tissue samples, the clinicopathological features were compared to the demethylation results. No significant association was found between NRF2 promoter demethylation and the clinicopathological features of patient samples. Conclusions: Our findings suggest that the epigenetic modifications leading to NRF2 demethylation found in colorectal tumour samples may contribute to cancer progression from precancerous polyps to cancerous lesions. [ABSTRACT FROM AUTHOR]

Published

2020

28. Analysis of DNA Methylation in Clinical Samples: Methods and Applications

Author

Dobrovic, Alexander, Lakhani, Sunil R., editor, and Fox, Stephen B., editor

Published

2016

29. O 6 -methylguanine methyltransferase promoter methylation status of glioblastoma cell line clonal population.

Author

Anan M, Del Maestro RF, Hata N, and Fujiki M

Subjects

Humans, Clone Cells pathology, DNA Methylation, HeLa Cells, Methyltransferases genetics, RNA, Messenger, Brain Neoplasms genetics, DNA Modification Methylases genetics, DNA Repair Enzymes genetics, Glioblastoma genetics, Glioblastoma pathology

Abstract

Glioblastoma (GBM) remains a treatment-resistant malignant brain tumor in large part because of its genetic heterogeneity and epigenetic plasticity. In this study, we investigated the epigenetic heterogeneity of GBM by evaluating the methylation status of the O 6 -methylguanine methyltransferase (MGMT) promoter in individual clones of a single cell derived from GBM cell lines. The U251 and U373 GBM cell lines, from the Brain Tumour Research Centre of the Montreal Neurological Institute, were used for the experiments. To evaluate the methylation status of the MGMT promoter, pyrosequencing and methylation-specific PCR (MSP) were used. Moreover, mRNA and protein expression levels of MGMT in the individual GBM clones were evaluated. The HeLa cell line, which hyper-expresses MGMT, was used as control. A total of 12 U251 and 12 U373 clones were isolated. The methylation status of 83 of 97 CpG sites in the MGMT promoter were evaluated by pyrosequencing, and 11 methylated CpG sites and 13 unmethylated CpG sites were evaluated by MSP. The methylation status by pyrosequencing was relatively high at CpG sites 3-8, 20-35, and 7-83, in both the U251 and U373 clones. Neither MGMT mRNA nor protein was detected in any clone. These findings demonstrate tumor heterogeneity among individual clones derived from a single GBM cell. MGMT expression may be regulated, not only by methylation of the MGMT promoter but by other factors as well. Further studies are needed to clarify the mechanisms underlying the epigenetic heterogeneity and plasticity of GBM., (© 2023 Japanese Society of Neuropathology.)

Published

2024

30. Interrelations of Apoptotic and Cellular Senescence Genes Methylation in Inflammatory Bowel Disease Subtypes and Colorectal Carcinoma in Egyptians Patients.

Author

Salama, Ragaa H., Sayed, Zain El-Abdeen A., Ashmawy, Ahmed M., Elsewify, Wael A., Ezzat, Ghada M., Mahmoud, Mahmoud A., Alsanory, Aya A., and Alsanory, Tasneem A.

Abstract

Ras-related domain family member 1 transcript variant A (RASSF1A) controls apoptosis and cell proliferation while p14/ARF gene has a regulatory role in cellular senescence. Failure of apoptosis and cellular senescence occurs during inflammatory bowel disease (IBD) and colorectal cancer (CRC). To reveal the role of peripheral leukocyte promoter methylation of RASSF1A and p14/ARF in the pathogenesis of IBD subtypes and CRC we investigated the methylation state of the two genes by methylation-specific polymerase chain reaction (MSP-PCR) in 60 CRC patients, 60 patients with IBD; 27 with ulcerative colitis and 33 had Crohn's disease and also in 30 healthy subjects. Methylated RASSF1A and p14/ARF genes were detected in 55% and 60% of CRC, while the frequency of the methylated RASSF1A and p14/ARF genes was 23.3% and 43.3% in IBD patients and 3.3% and 13.3% in the control group (P = 0.000 each). Also, the frequency of methylated RASSF1A gene was significantly higher in ulcerative colitis than in Crohn's disease, while a non-significant frequency of methylated p14/ARF was detected between ulcerative colitis and Crohn's disease. Furthermore, methylated RASSF1A and p14/ARF were associated with the grade of CRC but not associated with the age of patients, family history, or tumor location. Results suggest that methylated RASSF1A and p14/ARF are related to CRC and IBD pathogenesis and may be used as molecular biomarkers for early detection of CRC and IBD. [ABSTRACT FROM AUTHOR]

Published

2019

31. 结肠癌组织RASGRF1蛋白表达与基因 甲基化状态变化及其临床意义.

Author

钱伟明, 王海燕, and 李可

Abstract

Objective To investigate the expression of Ras protein-specific guanosine-releasing factor-1 (RASGRF1) and the changes of gene methylation status in the colon cancer tissues and their clinical significance. Methods Eighty-one eases of colon cancer tissues excised surgically and their matched normal adjacent tissues were collected. The expression of RASGRF1 protein was detected by immunohistochemistry, and methylation-specific PCR was used to detect the methylation status of RASGRF1 gene. The expression of RASGRF1 protein and gene methylation status were analyzed, and the relationships of RASGRF1 protein and gene methylation status with the clinicopathological characteristics of patients were analyzed. Results The positive expression rate of RASGRF1 protein in the colon cancer tissues was significantly lower than that in the adjacent tissues X2=51.995, P<0.01).The positive rate of methylation of RASGRF1 gene was signifieandy higher than that of the adjacent tissues (X2 = 44. 100, P<0.01). The positive expression of RASGRF1 protein was negatively correlated with the methylation status of RASGRF1 gene (p=-0.486 . P<0.05). The positive expression of RASGRF1 protein in the colon cancer tissues was related to TNM stage and lymph node metastasis (both P<0.05), but not to sex, age, tumor diameter, or degree of tissue differentiation (all P>0.05). The methylation status of RASGRF1 gene in the colon cancer tissues was related to TNM stage and lymph node metastasis (both P<0.05), hut not to sex, age, tumor diameter, or degree of tissue differentiation (all P>0.05). Conclusion RASGRF1 protein is low expressed in the colon cancer tissues, and the methylation of RASGRF1 gene is abnormally elevated, with a negative correlation between them, and both of them are related to TNM stage and lymph node metastasis of colon cancer. [ABSTRACT FROM AUTHOR]

Published

2019

32. Hypermethylation Analysis of p16INK4a and p15INK4b Promoters in Chronic Lymphocytic Leukaemia Patients and Normal Individuals.

Author

Amira M., Sarina S., Rosline H., Azlan H., Farid J., Muhammad, and Chang K. M.

Subjects

*P16 gene, *CHRONIC lymphocytic leukemia, *LEUKEMIA, *DNA methylation, *DEMOGRAPHIC characteristics, *NUCLEOTIDE sequence

Abstract

Introduction: Chronic Lymphocytic Leukaemia (CLL) is a common type of leukaemia in persons of predominantly European descent but is rare in the Asian population. Disparities in CLL incidence among people of Asian and European descent may be related to the genetic make-up of the two different populations. Hypermethylation event might be one of the silencing mechanisms that inactivate the tumour suppressor genes in CLL. The aim of this study was to determine the hypermethylation status of p16INK4a and p15INK4b among CLL patients and normal individuals. Materials & Methods: A total of 25 CLL patients and 25 normal individuals were recruited for this study and their genomic DNA were extracted from the peripheral blood. The hypermethylation status of p16INK4a and p15INK4b were determined using Methylation Specific-PCR (MS-PCR) whereas DNA sequencing method was applied to selected samples for validation of the MS-PCR results. We also evaluated the association between hypermethylation of these genes with the clinical and demographic characteristics of each group of subjects. Results: Among the CLL patients, p15INK4b partial-methylation occurred in 6 (24%) subjects while methylation occurred in 1 (4%) subject. All the remaining patients were unmethylated at p15INK4b. All the samples showed unmethylation at p16INK4a. Statistically significant associations were found between p15INK4b hypermethylation with the presence of CLL (p=0.01) and with race (p=0.02). Conclusion: Further study using a larger sample size is warranted to explore the significance of DNA methylation incidence among the CLL patients of the Malaysian population. Hence, we suggest that hypermethylation at p15INK4b has a huge influence that kick-starts CLL disease among Malaysians and MS-PCR technique is applicable to be used in methylation study. [ABSTRACT FROM AUTHOR]

Published

2019

33. IDLN-MSP: Idiolocal normalization of real-time methylation-specific PCR for genetic imbalanced DNA specimens

Author

Simeon Santourlidis, Foued Ghanjati, Agnes Beermann, Thomas Hermanns, and Cédric Poyet

Subjects

DNA methylation, methylation-specific PCR, biomarkers, diagnosis, epigenetics, Biology (General), QH301-705.5

Abstract

Sensitive, accurate, and reliable measurements of tumor cell-specific DNA methylation changes are of fundamental importance in cancer diagnosis, prognosis, and monitoring. Real-time methylation-specific PCR (MSP) using intercalating dyes is an established method of choice for this purpose. Here we present a simple but crucial adaptation of this widely applied method that overcomes a major obstacle: genetic abnormalities in the DNA samples, such as aneuploidy or copy number variations, that could result in inaccurate results due to improper normalization if the copy numbers of the target and reference sequences are not the same. In our idiolocal normalization (IDLN) method, the locus for the normalizing, methylation-independent reference amplification is chosen close to the locus of the methylation-dependent target amplification. This ensures that the copy numbers of both the target and reference sequences will be identical in most cases if they are close enough to each other, resulting in accurate normalization and reliable comparative measurements of DNA methylation in clinical samples when using real-time MSP.

Published

2016

34. Clinical Utility of Methylation-Specific Multiplex Ligation-Dependent Probe Amplification for the Diagnosis of Prader–Willi Syndrome and Angelman Syndrome

Author

Yongsook Park, Sung Sup Park, Sung Im Cho, Boram Kim, Jong-Hee Chae, Jiyeon Kim, Man Jin Kim, and Moon Woo Seong

Subjects

Oncology, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Prader–Willi syndrome, Concordance, Clinical Biochemistry, Bisulfite sequencing, Methylation, Chromosome 15, Utility, Angelman syndrome, Internal medicine, Diagnosis, Medicine, Humans, Multiplex ligation-dependent probe amplification, Imprinting (psychology), Retrospective Studies, Chromosomes, Human, Pair 15, business.industry, Biochemistry (medical), nutritional and metabolic diseases, General Medicine, Methylation-specific multiplex ligation-dependent probe amplification, DNA Methylation, medicine.disease, Uniparental disomy, nervous system diseases, Methylation-specific PCR, Original Article, business, Genomic imprinting, Diagnostic Genetics, Multiplex Polymerase Chain Reaction, Prader-Willi Syndrome

Abstract

Background Prader-Willi syndrome (PWS) and Angelman syndrome (AS) are genomic imprinting disorders that are mainly caused by a deletion on 15q11-q13, the uniparental disomy of chromosome 15, or an imprinting defect. We evaluated the utility of methylation-specific multiplex ligation-dependent probe amplification (MS-MLPA) as a diagnostic tool and for demonstrating the relationship between molecular mechanisms and clinical presentation. Methods We performed MS-MLPA using DNA samples from 93 subjects (45 PWS, 24 AS, and 24 non-PWS/AS controls) who had previously undergone MS-PCR for the diagnosis of PWS/AS. We compared the results of both assays, and patients' clinical phenotypes were reviewed retrospectively. Results MS-MLPA showed a 100% concordance rate with MS-PCR. Among the 45 PWS patients, 26 (57.8%) had a deletion of 15q11-q13, and the others (42.2%) had uniparental disomy 15 or an imprinting defect. Among the 24 AS patients, 16 (66.7%) had a deletion of 15q11-q13, 7 AS patients (29.2%) had uniparental disomy 15 or an imprinting defect, and one AS patient (4.2%) showed an imprinting center deletion. Conclusions MS-MLPA has clinical utility for the diagnosis of PWS/AS, and it is superior to MS-PCR in that it can identify the molecular mechanism underlying the disease.

Published

2022

35. Evaluation of MGMT Gene Methylation in Neuroendocrine Neoplasms

Author

Davide Costabile, Giulia De Riso, Paolo Cappabianca, Stephan Frank, Salvatore Tafuto, Alessandro Ottaiano, Annabella Di Mauro, Roberto Tafuto, Rosa Della Monica, Lorenzo Chiariotti, Roberta Visconti, Sabrina Lamia, Fabiana Tatangelo, Marialaura Del Basso De Caro, Juergen Hench, Michela Buonaiuto, Mariella Cuomo, Elia Guadagno, and Teodolinda Di Risi

Subjects

Cancer Research, Amplicon bisulfite sequencing, Methyltransferase, Bisulfite sequencing, Biology, Article, Temozolomide, medicine, Humans, MGMT gene methylation, Promoter Regions, Genetic, Antineoplastic Agents, Alkylating, DNA Modification Methylases, neoplasms, Gastrointestinal tract, Brain Neoplasms, Tumor Suppressor Proteins, General Medicine, Methylation, DNA Methylation, Amplicon, DNA Repair Enzymes, Oncology, CpG site, Neuroendocrine neoplasms, Methylation-specific PCR, Cancer research, Biomarker (medicine), medicine.drug

Abstract

Unresectable neuroendocrine neoplasms (NENs) often poorly respond to standard therapeutic approaches. Alkylating agents, in particular temozolomide, commonly used to treat high-grade brain tumors including glioblastomas, have recently been tested in advanced or metastatic NENs, where they showed promising response rates. In glioblastomas, prediction of response to temozolomide is based on the assessment of the methylation status of the MGMT gene, as its product, O 6-methylguanine-DNA methyltransferase, may counteract the damaging effects of the alkylating agent. However, in NENs, such a biomarker has not been validated yet. Thus, we have investigated MGMT methylation in 42 NENs of different grades and from various sites of origin by two different approaches: in contrast to methylation-specific PCR (MSP), which is commonly used in glioblastoma management, amplicon bisulfite sequencing (ABS) is based on high-resolution, next-generation sequencing and interrogates several additional CpG sites compared to those covered by MSP. Overall, we found MGMT methylation in 74% (31/42) of the NENs investigated. A higher methylation degree was observed in well-differentiated tumors and in tumors originating in the gastrointestinal tract. Comparing MSP and ABS results, we demonstrate that the region analyzed by the MSP test is sufficiently informative of the MGMT methylation status in NENs, suggesting that this predictive parameter could routinely be interrogated also in NENs.

Published

2021

36. Blood Based Methylated DNA and Tumor-Specific Protein Analysis in Gastric Cancer Diagnostics

Author

Elistratova, Elena V., Shelestyuk, Petr I., Permyakova, Valentina I., Chikova, Elena D., Tuzikov, Sergey A., Vlassov, Valentin V., Laktionov, Pavel P., Rykova, Elena Y., and Gahan, Peter B., editor

Published

2011

37. Gene-Specific Hypermethylation in Aging

Author

Akintola, Adebayo D., Parrish, Alan R., and Tollefsbol, Trygve O., editor

Published

2010

38. A sample-to-answer droplet magnetofluidic assay platform for quantitative methylation-specific PCR.

Author

Stark, Alejandro, Shin, Dong Jin, and Wang, Tza-Huei

Published

2018

39. Methylation-specific PCR: four steps in primer design

Author

Davidović Radoslav, Božović Ana, Mandušić Vesna, and Krajnović Milena

Subjects

methylation-specific pcr, primer design, database, software for msp primer design, transcriptional start site, Biology (General), QH301-705.5

Published

2014

40. DNA Methylation Changes Induced by Redox-Active Compounds—Choosing the Right PCR-Based Method

Author

Patrycja Jakubek, Jovana Rajić, Monika Baranowska, Melita Vidaković, Agnieszka Bartoszek, and Jacek Namieśnik

Subjects

catechins, DNA methylation, methylation-specific PCR, methylation-sensitive high resolution melting, redox homeostasis, epigenetics, General Works

Abstract

The impact of catechins on the expression profile of redox-related genes in HT29 cell line has been studied recently by our group using Oxidative Stress RT2 Profiler PCR Array. Within the examined panel of 84 genes, the down-regulation of SRXN1 gene was unique among other up-regulated genes. We hypothesized that the observed down-regulation resulted from DNA methylation and have exploited this observation to choose the proper strategy to monitor the changes in DNA methylation patterns incurred by dietary antioxidants. The current study verified two PCR-based approaches.

Published

2019

41. Prospective study to validate the clinical utility of DNA diagnosis of peritoneal fluid cytology test in gastric cancer

Author

Naoki Hiki, Masahiro Niihara, Takafumi Sangai, Marie Washio, Nobuyuki Nishizawa, Yusuke Kumamoto, Takafumi Soeno, Mikiko Sakuraya, Hideki Ushiku, Kei Hosoda, Takeshi Naitoh, Keishi Yamashita, and Hiroki Harada

Subjects

Male, Cancer Research, medicine.medical_specialty, Cysteine dioxygenase type 1, methylation‐specific PCR, Cytodiagnosis, Bisulfite sequencing, washing cytology test, Gastroenterology, chemistry.chemical_compound, Carcinoembryonic antigen, Cell, Molecular, and Stem Cell Biology, Stomach Neoplasms, Cytology, Internal medicine, Biomarkers, Tumor, Ascitic Fluid, Humans, Medicine, Prospective Studies, Promoter Regions, Genetic, Peritoneal Neoplasms, Aged, Neoplasm Staging, biology, business.industry, gastric cancer, Cysteine Dioxygenase, peritoneal dissemination, DNA, General Medicine, DNA Methylation, Prognosis, Minimal residual disease, Oncology, chemistry, Genetic marker, DNA methylation, biology.protein, Original Article, Female, ORIGINAL ARTICLES, Peritoneum, business

Abstract

The clinical efficacy of DNA cytology test (CY) in gastric cancer (GC) has been retrospectively proposed using cancer‐specific methylation of cysteine dioxygenase type 1 (CDO1). We confirmed the clinical utility of DNA CY in a prospective cohort. Four hundred GC samples were prospectively collected for washing cytology (UMIN000026191), and detection of the DNA methylation of CDO1 was assessed by quantitative methylation‐specific PCR in the sediments. Endpoint was defined as the match rate between conventional CY1 and DNA CY1 (diagnostic sensitivity), and the DNA CY0 rate (diagnostic specificity) in pStage IA. DNA CY1 was detected in 45 cases (12.5%), while CY1 was seen in 31 cases (8.6%) of 361 chemotherapy‐naïve samples, where the sensitivity and specificity of the DNA CY in the peritoneal solutions were 74.2% and 96.5%, respectively. The DNA CY was positive for 3.5/0/4.9/11.4/58.8% in pStage IA/IB/II/III/IV, respectively (P, The bar graphs represent diagnostic sensitivity of the conventional CY1 and the DNA CY1 according to pathological factor.

Published

2021

42. Screening and identification of a tumor specific methylation phenotype in the colorectal laterally spreading tumor.

Author

NI, H.-B., WANG, F.-Y., XU, J., HE, X.-J., CHEN, J., WU, Q., WU, J.-F., and SUN, Y.-S.

Abstract

OBJECTIVE: We screened and identified the differential expression of the methylation phenotype in the whole genome of colorectal laterally spreading tumor (LSTs). MATERIALS AND METHODS: 3 tissue samples of colorectal polypoid adenomas (PAs), 3 tissue samples of LSTs and 3 tissue samples of colon cancer were analyzed with a high-density gene chip, and about 450,000 methylation sites were detected covering approximately 95% of the CpG islands. The Delta Data screening was taken through a cluster analysis of methylation phenotype differential expression. 50 tissue samples each of PAs patients, LSTs patients, and colorectal cancer patients were selected. Methylation-specific PCR (MSP) was used to detect RASSF1A and WIF-1 methylation levels. He RT-PCR method was used to detect the relative mRNA expression levels for methylation expression identification. RESULTS: The degree of LST methylation was higher than that of PAs, and 1234 genes were found to have a lower expression when compared to colorectal cancer samples. 764 genes had a higher expression when compared to colorectal cancer, and 559 genes lower expression when compared to PAs. The average methylation level of LSTs was higher than that of PAs, and lower than that of colorectal cancer. The chromosomal location was taken on these 1234 genes, which were higher than that of PAs, and lower than that of colorectal cancer; 518 genes were located on chromosome No. 2 (41.98%), 236 on No. 5 (19.12%), 357 on No. 8 (28.93%), and 123 on No. 10 (9.97%). According to clustering analysis, DNA differentially methylated sites were mainly on genes of cell adhesion molecules regulation, signaling pathways, energy transduction, cell cycle and apoptosis. The positive rate of RASSF1A and WIF-1 methylation in the tissues of LSTs patients were higher than that of PAs, and lower than that of colorectal cancer; differences were statistically significant (p<0.05). The relative expression levels of RASSF1A and WIF-1mRNA that of PAs, higher than that of colorectal cancer, and the difference was statistically significant (p<0.05). CONCLUSIONS: The administration of high-density gene chip technology has a good application value to screen the differential expression of LSTs gene methylation phenotype. Results are consistent with the identification results. [ABSTRACT FROM AUTHOR]

Published

2017

43. Promoter Hypermethylation and Its Impact on Expression of MGMT Gene in the GIT Malignant Patients of Kashmiri Origin.

Author

Bhat, Arif Akbar, Wani, Hilal Ahmad, Ishaq, Shiekh, Waza, Ajaz Ahmad, Malik, Rawoof Ahmad, Shabir, Iram, Jeelani, Showkat, Kadla, Showkat, Qureshie, Waseem, Masood, Akbar, and Majid, Sabhiya

Subjects

*GASTROINTESTINAL cancer, *DNA methylation, *GENE expression, *CANCER invasiveness, *DNA methyltransferases, *KASHMIRI (South Asian people), *DISEASES

Abstract

Epigenetic alterations, in addition to multiple gene abnormalities, are involved in the genesis and progression of human cancers. Gastrointestinal tract (GIT) cancer is a major medical and economic burden worldwide. Aberrant methylation of CpG islands within promoter regions is associated with transcriptional inactivation of various tumor suppressor genes. Although a number of cancer-associated genes have been found to be hypermethylated in GIT cancer, valuable methylation markers for early diagnosis and prognostic evaluation of this cancer remain largely unknown. O6-methyguanine DNA methyltransferase (MGMT) is a DNA-repair gene that removes mutagenic and cytotoxic adducts from the O6 position of guanine induced by alkylating agents. MGMT promoter hypermethylation and reduced expression have been found in some primary human carcinomas. We studied DNA methylation of CpG islands of the MGMT gene and its relation with MGMT protein expression in human GIT carcinomas. A total of 210 GIT tumor samples and 90 adjacent normal tissues were analyzed for MGMT promoter methylation by methylation-specific polymerase chain reaction after bisulfite modification of DNA and same samples were analyzed for MGMT protein expression by Western blotting. The methylation frequencies of MGMT gene promoter were 41.4%, 34.2%, and 44.2% in stomach, esophageal, and colorectal cancer cases while as 16.6, 13.3, and 13.3 in respective controls. MGMT protein was found downregulated in controls of all GIT. The results suggest that methylation at CpG islands of MGMT may be responsible for the downregulation of MGMT protein expression in GIT cancers. [ABSTRACT FROM AUTHOR]

Published

2017

44. Genome-wide DNA methylation profile identified a unique set of differentially methylated immune genes in oral squamous cell carcinoma patients in India.

Author

Basu, Baidehi, Chakraborty, Joyeeta, Chandra, Aditi, Katarkar, Atul, Baldevbhai, Jadav Ritesh Kumar, Chowdhury, Debjit Dhar, Ray, Jay Gopal, Chaudhuri, Keya, and Chatterjee, Raghunath

Subjects

*DNA methylation, *CARCINOMA, *IMMUNE response

Abstract

Background: Oral squamous cell carcinoma (OSCC) is one of the common malignancies in Southeast Asia. Epigenetic changes, mainly the altered DNA methylation, have been implicated in many cancers. Considering the varied environmental and genotoxic exposures among the Indian population, we conducted a genome-wide DNA methylation study on paired tumor and adjacent normal tissues of ten well-differentiated OSCC patients and validated in an additional 53 well-differentiated OSCC and adjacent normal samples. Results: Genome-wide DNA methylation analysis identified several novel differentially methylated regions associated with OSCC. Hypermethylation is primarily enriched in the CpG-rich regions, while hypomethylation is mainly in the open sea. Distinct epigenetic drifts for hypo- and hypermethylation across CpG islands suggested independent mechanisms of hypo- and hypermethylation in OSCC development. Aberrant DNA methylation in the promoter regions are concomitant with gene expression. Hypomethylation of immune genes reflect the lymphocyte infiltration into the tumor microenvironment. Comparison of methylome data with 312 TCGA HNSCC samples identified a unique set of hypomethylated promoters among the OSCC patients in India. Pathway analysis of unique hypomethylated promoters indicated that the OSCC patients in India induce an anti-tumor T cell response, with mobilization of T lymphocytes in the neoplastic environment. Survival analysis of these epigenetically regulated immune genes suggested their prominent role in OSCC progression. Conclusions: Our study identified a unique set of hypomethylated regions, enriched in the promoters of immune response genes, and indicated the presence of a strong immune component in the tumor microenvironment. These methylation changes may serve as potential molecular markers to define risk and to monitor the prognosis of OSCC patients in India. [ABSTRACT FROM AUTHOR]

Published

2017

45. Ras Association Domain Family 1A Gene Promoter Methylation as a Biomarker for Chronic Viral Hepatitis C-related Hepatocellular Carcinoma.

Author

Abou Zeid AA, El-Sayed ET, Ahdy JK, and Tawfik MR

Abstract

Background One of the most prevalent aberrant epigenetic modifications found in hepatocellular carcinoma (HCC) is abnormal DNA methylation. Our study aimed to evaluate serum Ras association domain family 1A (RASSF1A) gene promoter methylation in patients with chronic viral hepatitis C (HCV)-associated liver cirrhosis with and without HCC as a potential new marker for the early detection of HCC. Methodology The 60 participants who participated in the trial were divided into the following three groups: 20 patients with newly diagnosed primary HCC on top of HCV-related liver cirrhosis, 20 patients with HCV-related liver cirrhosis, and 20 age- and sex-matched healthy individuals as a control group. All participants underwent methylation-specific polymerase chain reaction testing to detect the blood level of the RASSF1A gene's methylated promoter. Results Methylated RASSF1A was found in 30% of patients with liver cirrhosis caused by HCV and in 65% of patients with HCC, but not in any of the controls. It was discovered that the serum methylation RASSF1A had an accuracy of 82.50% and an area under the curve (AUC) of 0.825 for separating HCC patients from healthy controls. With an AUC of 0.675 and an accuracy of 67.50%, it was able to differentiate patients with HCC from those with HCV-related liver cirrhosis. Additionally, there was no statistically significant association between RASSF1A methylation status and HCC mass size (p = 0.449). Conclusions Serum RASSF1A promoter methylation status detection could be useful for detecting HCC early, especially in high-risk individuals such as those with HCV., Competing Interests: The authors have declared that no competing interests exist., (Copyright © 2023, Abou Zeid et al.)

Published

2023

46. Effects of Methylation of FHIT Gene on it’s Protein and mRNA Expression in Non-small Cell Lung Cancer

Author

Wentong LI, Chonggao YIN, Weidong ZHANG, and Hongli LI

Subjects

Lung neoplasms, Methylation, Methylation-specific PCR, FHIT gene, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background and objective Fragile histidine triad (FHIT) is a new tumor suppressor gene, whose promoter methylation plays an important role in carcinogenesis. The aim of this study is to explore the effects of CpG island methylation on protein and mRNA expression of FHIT in non-small cell lung cancer, and the roles of FHIT gene in pathogenesis of NSCLC. Methods Methylation and protein expression and transcriptional level of FHIT gene were detected by methylationspecific PCR, Western Blot and RT-PCR in 52 tumor tissues and normal tissues of NSCLC. Results Methylation in the tumor samples was detected at 38.46%, whereas it occurred at lower frequencies (7.69%) in the corresponding normal lung tissues. Protein expression frequencies was 28.8% in the tumor samples, whereas it was 88.5% in the corresponding normal lung tissues. MRNA expression frequencies was 51.9% in the tumor samples and 100% in the corresponding normal lung tissues. Conclusion In NSCLC, FHIT gene promoter methylation frequency was significantly increased with decreased expression, suggesting that FHIT promoter methylation plays a role in lung cancer carcinogenesis.

Published

2009

47. Epigenetic Changes in Tumor Suppressor Genes, P15, P16, APC-3 and E-cadherin in Body Fluid

Author

Mei-Ling Chen, Julia Huei-Mei Chang, Kun-Tu Yeh, Ya-Sian Chang, and Jan-Gowth Chang

Subjects

body fluid, cytologist, malignant cells, methylation-specific PCR, tumor suppressor gene, Medicine (General), R5-920

Abstract

The inactivation of tumor suppressor genes by promoter methylation plays an important role in the development of cancers; it can also be used as a marker to distinguish cancerous cells from non-cancer cells. In this study, we investigated the aberrant methylation profile of the tumor suppressor genes P15, P16, APC and E-cadherin in the cells of body fluid. A methylation-specific polymerase chain reaction was performed in 31 cases of malignant effusion and 39 cases of nonmalignant effusion. Aberrant promoter methylation of P15, P16, APC and E-cadherin genes was seen in 0%, 25.8%, 35.5% and 6.5% of malignant effusion cases, respectively, whereas the frequencies were 0%, 2.6%, 2.6% and 0%, respectively, for negative control effusion. There were statistically significant differences in the aberrant methylation of P16 (p = 0.008) and APC (p = 0.018) genes between cases of malignant effusion and controls. Methylation of one of three genes (P16, E-cadherin, APC) was found in 14 out of 31 (45.2%) cases of malignant effusion, and in two out of 39 (5.1%) cases of non-malignant effusion (p = 0.000004). Concurrent methylation was found in nine out of 31 (29%) cases of malignant effusion, but in no non-malignant effusion sample. From these results, we suggest that methylation-specific polymerase chain reaction to analyze the promoters of tumor suppressor genes can distinguish between malignant effusion and benign effusion, and may help cytologists to make more accurate diagnoses.

Published

2007

48. Polycyclic aromatic hydrocarbons are associated with insulin receptor substrate 2 methylation in adipose tissues of Korean women.

Author

Kim, Young Hun, Lee, Yoon Soon, Lee, Duk Hee, and Kim, Dong Sun

Subjects

*POLYCYCLIC aromatic hydrocarbons, *INSULIN receptors, *ADIPOSE tissues, *WOMEN, *DNA methylation, *PROMOTERS (Genetics)

Abstract

Polycyclic aromatic hydrocarbons (PAHs) are highly lipid soluble and are an increasing concern for general populations given their various adverse health effects, including obesity-related metabolic dysfunction. DNA methylation can act as a downstream effector for the biological effects of environmental exposures, but whether PAHs influence DNA methylation is unclear. To test for possible adverse effects of PAHs on adipose tissue (AT), we determined the promoter methylation status of 12 genes involved in glucose and lipid metabolism ( CS, GLUT4, IR, IRS1, IRS2, LIPIN1, MCAD, PCK1, PCK2, PPARGC1 Β , SDHA, and SREBP1 ) in visceral AT of Korean women by using methylation-specific PCR (MSP). IRS2 methylation alone was significantly associated with concentrations of individual PAH chemicals. When the PAH summary measure was used, the odds ratios of IRS2 hypermethylation across quartile of the PAH summary measure were 1, 1.7, 2.0, and 11.2 (95% confidence interval: 1.5–84.0) after adjusting for age and BMI (P trend=0.02). The strength of association between PAH summary measure and IRS2 hypermethylation was as similar as that of BMI. Collectively, these results suggested that lipophilic PAHs might be contributing factors to the pathogenesis of insulin resistance through methylation-mediated suppression of the IRS2 gene. However, further studies with large sample size are needed to confirm our findings. [ABSTRACT FROM AUTHOR]

Published

2016

49. Association of the hypermethylation status of PTEN tumor suppressor gene with the risk of breast cancer among Kurdish population from Western Iran.

Author

Yari, Kheirollah, Payandeh, Mehrdad, and Rahimi, Zohreh

Abstract

Breast cancer is the most common cancer with high morbidity and mortality among women worldwide. Aberrant hypermethylation in promoter regions of the tumor suppressor genes such as PTEN gene is a key event in the progression and development of breast cancer. The aim of the present study was to evaluate an association between PTEN gene methylation status with the risk of breast cancer in an Iranian population. We studied 255 individuals, including 103 patients with breast cancer, 102 first-degree female relatives of patients (mother, sister, or daughter of patients), and 50 healthy individuals as a control group. Genomic DNA was extracted from peripheral blood leukocytes, and the PTEN promoter methylation status was detected using methylation-specific PCR (MSP) method with specific methylated and unmethylated primers. In some samples, direct DNA sequencing was used to confirm the results obtained by the MSP method. The frequency of PTEN-methylated (MM) genotype was 6 % in the healthy control group, 23.3 % in relatives of patients, and 41.7 % in patients ( χ = 24.62, p < 0.001). There were significant differences in the frequency of PTEN-methylated genotype between healthy control compared to that in patients ( χ = 15.1, p < 0.001) and also compared to that in relatives of patients ( χ = 6.9, p = 0.009). In the presence of PTEN MM genotype, there was a 3.1-fold susceptibility to breast cancer compared to the UU genotype ( p < 0.001). Also, in the presence of PTEN M allele, the risk of breast cancer was 2.71-fold compared to the presence of U allele ( p < 0.001). Our findings indicated increased frequency of hypermethylation of PTEN promoter in the studied patients and their relatives that could be considered as one of the epigenetic factors affecting the risk of breast cancer in Iranians. [ABSTRACT FROM AUTHOR]

Published

2016

50. The Preliminary Study of Pesticide Mospilan Effect on the GSTP1 Gene Methylation in Bovine Lymphocytes

Author

V. Verebová, Jana Halušková, Beáta Holečková, and Jana Staničová

Subjects

pesticide exposure, 0301 basic medicine, Genetics, bovine, mospilan, Veterinary medicine, methylation-specific pcr, GSTP1 Gene, dna methylation, General Medicine, Methylation, Biology, Pesticide, gstp1, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, SF600-1100

Abstract

The epigenetic mechanisms represent a dynamic, reversible and heritable manner modulating gene expression during the life cycle of an animal organism. They generate the specific epigenetic marks which constitute so-called epigenome. One of the most studied epigenetic mechanisms/marks is DNA methylation which is, similarly as the whole epigenome, susceptible to environmental and nutritional influences. The aberrations of the DNA methylation profile may alter gene expression leading to pathologic consequences. Pesticides along with their pest-reducing effects may also negatively affect non-target organisms. In our preliminary study, we investigated an effect of the pesticide Mospilan on the DNA methylation of the bovine GSTP1 gene which plays an important role in the cell detoxification processes. The specific primers for the GSTP1 Methylation-specific PCR (MSP) analysis were proposed and tested with the DNA from the Mospilan-treated bovine lymphocytes. It seems that the pesticide with the concentration of 100 µg.ml−1 did not induce DNA methylation changes in GSTP1 gene in bovine lymphocytes.

Published

2019