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Multiple Myeloma: Genetic and Epigenetic Biomarkers with Clinical Potential

Title:	Multiple Myeloma: Genetic and Epigenetic Biomarkers with Clinical Potential
Authors:	Yuliya A. Veryaskina; Sergei E. Titov; Natalia V. Skvortsova; Igor B. Kovynev; Oksana V. Antonenko; Sergei A. Demakov; Pavel S. Demenkov; Tatiana I. Pospelova; Mikhail K. Ivanov; Igor F. Zhimulev
Source:	International Journal of Molecular Sciences ; Volume 25 ; Issue 24 ; Pages: 13404
Publisher Information:	Multidisciplinary Digital Publishing Institute
Publication Year:	2024
Collection:	MDPI Open Access Publishing
Subject Terms:	microRNA; oncogenes; tumor suppressors; multiple myeloma; prognostic biomarkers
Subject Geographic:	agris
Description:	Multiple myeloma (MM) is characterized by the uncontrolled proliferation of monoclonal plasma cells and accounts for approximately 10% of all hematologic malignancies. The clinical outcomes of MM can exhibit considerable variability. Variability in both the genetic and epigenetic characteristics of MM undeniably contributes to tumor dynamics. The aim of the present study was to identify biomarkers with the potential to improve the accuracy of prognosis assessment in MM. Initially, miRNA sequencing was conducted on bone marrow (BM) samples from patients with MM. Subsequently, the expression levels of 27 microRNAs (miRNA) and the gene expression levels of ASF1B, CD82B, CRISP3, FN1, MEF2B, PD-L1, PPARγ, TERT, TIMP1, TOP2A, and TP53 were evaluated via real-time reverse transcription polymerase chain reaction in BM samples from patients with MM exhibiting favorable and unfavorable prognoses. Additionally, the analysis involved the bone marrow samples from patients undergoing examinations for non-cancerous blood diseases (NCBD). The findings indicate a statistically significant increase in the expression levels of miRNA-124, -138, -10a, -126, -143, -146b, -20a, -21, -29b, and let-7a and a decrease in the expression level of miRNA-96 in the MM group compared with NCBD (p < 0.05). No statistically significant differences were detected in the expression levels of the selected miRNAs between the unfavorable and favorable prognoses in MM groups. The expression levels of ASF1B, CD82B, and CRISP3 were significantly decreased, while those of FN1, MEF2B, PDL1, PPARγ, and TERT were significantly increased in the MM group compared to the NCBD group (p < 0.05). The MM group with a favorable prognosis demonstrated a statistically significant decline in TIMP1 expression and a significant increase in CD82B and CRISP3 expression compared to the MM group with an unfavorable prognosis (p < 0.05). From an empirical point of view, we have established that the complex biomarker encompassing the CRISP3/TIMP1 expression ratio holds ...
Document Type:	text
File Description:	application/pdf
Language:	English
Relation:	Biochemistry; https://dx.doi.org/10.3390/ijms252413404
DOI:	10.3390/ijms252413404
Availability:	https://doi.org/10.3390/ijms252413404
Rights:	https://creativecommons.org/licenses/by/4.0/
Accession Number:	edsbas.281648A
Database:	BASE