p38β-MAPK11 and its role in female cancers

被引:18
|
作者
Katopodis, Periklis [1 ,2 ]
Kerslake, Rachel [1 ]
Zikopoulos, Athanasios [3 ]
Beri, Nefeli [4 ]
Anikin, Vladimir [2 ,5 ]
机构
[1] Brunel Univ London, Coll Hlth & Life Sci, Biosci, Uxbridge, Middx, England
[2] Harefield Hosp, Royal Brompton & Harefield NHS Fdn Trust, Div Thorac Surg, London UB9 6JH, England
[3] Royal Cornwall Hosp, Royal Cornwall Hosp NHS Fdn Trust, Obstet & Gynaecol Dept, Truro TR1 3LJ, England
[4] Karolinska Inst, Dept Med, S-17177 Stockholm, Sweden
[5] Sechenov First Moscow State Med Univ, Dept Oncol & Reconstruct Surg, Moscow 119146, Russia
关键词
MAPK11; MAPK; Female cancers; Breast cancer; Ovarian cancer; Cervical cancer; Uterine carcinosarcoma; Meexress; Smartapp; Cbioportal; canSar; Methylation; p38; beta; Pan-cancer; ACTIVATED PROTEIN-KINASE; P38; MAPK; EXPRESSION; TARGET; ALPHA; CELLS; BETA; AUTOPHOSPHORYLATION; REGULATORS; INHIBITION;
D O I
10.1186/s13048-021-00834-9
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Background: The p38MAPK family of Mitogen Activated Protein Kinases are a group of signalling molecules involved in cell growth, survival, proliferation and differentiation. The widely studied p38 alpha isoform is ubiquitously expressed and is implicated in a number of cancer pathologies, as are p38 gamma and p38 delta. However, the mechanistic role of the isoform, p38 beta, remains fairly elusive. Recent studies suggest a possible role of p38 beta in both breast and endometrial cancer with research suggesting involvement in bone metastasis and cancer cell survival. Female tissue specific cancers such as breast, endometrial, uterine and ovary account for over 3,000,000 cancer related incidents annually; advancements in therapeutics and treatment however require a deeper understanding of the molecular aetiology associated with these diseases. This study provides an overview of the MAPK signalling molecule p38 beta (MAPK11) in female cancers using an in-silico approach. Methods: A detailed gene expression and methylation analysis was performed using datasets from cBioportal, CanSar and MEXPRESS. Breast, Uterine Endometrial, Cervical, Ovarian and Uterine Carcinosarcoma TCGA cancer datasets were used and analysed. Results: Data using cBioportal and CanSAR suggest that expression of p38 beta is lower in cancers: BRCA, UCEC, UCS, CESC and OV compared to normal tissue. Methylation data from SMART and MEXPRESS indicate significant probe level variation of CpG island methylation status of the gene MAPK11. Analysis of the genes' two CpG islands shows that the gene was hypermethylated in the CpG1 with increased methylation seen in BRCA, CESC and UCEC cancer data sets with a slight increase of expression recorded in cancer samples. CpG2 exhibited hypomethylation with no significant difference between samples and high levels of expression. Further analysis from MEXPRESS revealed no significance between probe methylation and altered levels of expression. In addition, no difference in the expression of BRCA oestrogen/progesterone/HER2 status was seen. Conclusion: This data provides an overview of the expression of p38 beta in female tissue specific cancers, showing a decrease in expression of the gene in BRCA, UCEC, CESC, UCS and OV, increasing the understanding of p38 beta MAPK expression and offering insight for future in-vitro investigation and therapeutic application.
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页数:12
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