Please use this identifier to cite or link to this item: https://biore.bio.bg.ac.rs/handle/123456789/5067
Title:  LTBP4, SPP1, and CD40 Variants: Genetic Modifiers of Duchenne Muscular Dystrophy Analyzed in Serbian Patients
Authors: Kosac Ana
Pešović, Jovan 
Radenković, Lana 
Brkušanin, Miloš 
Radovanović, Nemanja 
Đurišić, Marina
Radivojević, Danijela
Mladenović, Jelena
Ostojić, Slavica
Kovačević, Gordana
Kravljanac, Ružica
Savić-Pavićević, Dušanka 
Milić Rašić, Vedrana
Keywords: Duchenne muscular dystrophy;single-nucleotide polymorphisms;LTBP4;SPP1;CD40
Issue Date: 4-Aug-2022
Rank: M22
Publisher: MDPI
Citation: Kosac, Ana, Jovan Pesovic, Lana Radenkovic, Milos Brkusanin, Nemanja Radovanovic, Marina Djurisic, Danijela Radivojevic, Jelena Mladenovic, Slavica Ostojic, Gordana Kovacevic, Ruzica Kravljanac, Dusanka Savic Pavicevic, and Vedrana Milic Rasic. 2022. "LTBP4, SPP1, and CD40 Variants: Genetic Modifiers of Duchenne Muscular Dystrophy Analyzed in Serbian Patients" Genes 13, no. 8: 1385. https://doi.org/10.3390/genes13081385
Journal: Genes
Abstract: 
Background: Clinical course variability in Duchenne muscular dystrophy (DMD) is partially explained by the mutation location in the DMD gene and variants in modifier genes. We assessed the effect of the SPP1, CD40, and LTBP4 genes and DMD mutation location on loss of ambulation (LoA). Methods: SNPs in SPP1-rs28357094, LTBP4-rs2303729, rs1131620, rs1051303, rs10880, and CD40-rs1883832 were genotyped, and their effect was assessed by survival and hierarchical cluster analysis. Results: Patients on glucocorticoid corticosteroid (GC) therapy experienced LoA one year later (p = 0.04). The modifying effect of SPP1 and CD40 variants, as well as LTBP4 haplotypes, was not observed using a log-rank test and multivariant Cox regression analysis. Cluster analysis revealed two subgroups with statistical trends in differences in age at LoA. Almost all patients in the cluster with later LoA had the protective IAAM LTBP4 haplotype and statistically significantly fewer CD40 genotypes with harmful T allele and “distal” DMD mutations. Conclusions: The modifying effect of SPP1, CD40, and LTBP4 was not replicated in Serbian patients, although our cohort was comparable in terms of its DMD mutation type distribution, SNP allele frequencies, and GC-positive effect with other European cohorts. Cluster analysis may be able to identify patient subgroups carrying a combinatio
URI: https://biore.bio.bg.ac.rs/handle/123456789/5067
ISSN: 2073-4425
DOI: 10.3390/genes13081385
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