MAPK7 variants related to prognosis and chemotherapy response in osteosarcoma
Osteosarcoma (OS) is a class of cancer originating from the bone, affecting mainly children and young adults. Our previous study showed that MAPK7 gene overexpression was significantly associated with tumor progression, poor treatment response, and worse overall survival, suggesting that MAPK7 could...
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Veröffentlicht in: | Annals of diagnostic pathology 2020-06, Vol.46, p.151482-151482, Article 151482 |
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Sprache: | eng |
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Zusammenfassung: | Osteosarcoma (OS) is a class of cancer originating from the bone, affecting mainly children and young adults. Our previous study showed that MAPK7 gene overexpression was significantly associated with tumor progression, poor treatment response, and worse overall survival, suggesting that MAPK7 could play an important role in OS tumorigenesis. We have investigated if MAPK7 overexpression was a result of any genomic changes in OS tumor specimens. We identified five SNPs (Single Nucleotide Polymorphism) previously described in databases, dbSNP and COSMIC, and identified two single nucleotide substitution not yet described. We found, in prechemotherapy specimens, a significant association of MAPK7 rs2233072G allele variant with metastasis at diagnosis and relapse (0.0909 and 0.0455, respectively). In post-chemotherapy, rs1054206GG specimen's genotype was associated with osteoblastic histological type (P= 0.0249) and presented decreased MAPK7 gene expression when compared with pre-chemotherapy specimens of same patients (P = 0.0095). Interestingly, it was observed some SNPs genotype exchange after chemotherapy. Our data indicated that MAPK7 gene expression associated with genotype exchange after chemotherapy, and these SNPs associated with important clinical parameters might be a valuable indicator for predicting in OS.
•First study to investigate MAPK7 gene sequencing in OS•MAP K7 SNPs exchange genotype after chemotherapy.•MAP K7 SNPs were correlated with clinical parameters in OS.•MAP K7 plays an important role in OS tumorigenesis. |
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ISSN: | 1092-9134 1532-8198 |
DOI: | 10.1016/j.anndiagpath.2020.151482 |