FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4387680653> ?p ?o ?g. }

• W4387680653 endingPage "485" @default.
• W4387680653 startingPage "485" @default.
• W4387680653 abstract "Background: Beta thalassemia is a condition in which the body cannot produce the beta subunit of hemoglobin due to harmful mutations in the globin gene that cause inadequate development of adult hemoglobin (HbA). In beta-thalassemic individuals, fetal hemoglobin (HbF), consisting of two and two subunits, is a potential replacement for HbA with significant therapeutic importance. HbF increase is a powerful and essential therapeutic tool to overcome the problem of beta-thalassemia. Materials and Methods: The GEO2R statistical tool and the GSE96060 dataset from the gene expression omnibus database were used to determine the differentially expressed genes (DEGs). The search tool for the retrieval of interacting genes program was used to reveal connections between these DEGs in samples, followed by applying the molecular complex detection algorithm to identify clusters of genes within these interaction networks. Using ClueGo and CluePedia, the discovered DEGs were subjected to functional annotation, including gene ontology (GO) and enriched molecular pathway analysis. Results: We searched the top 200 DEGs that met the criteria for significance (P-value 0.05; fold two change >1 or 1). Myeloid cell differentiation, erythrocyte differentiation, cellular detoxification, and heme binding are only a few examples of the biological processes and molecular pathways the GO analysis of DEGs identified as having significant alterations. The link between the DEGs in heme biosynthesis and transcriptional dysregulation in cancer was discovered by studying enriched Kyoto encyclopedia of genes and genomes pathways. To find possible targets for beta thalassemia treatments, we looked for the genes Krüppel-like factors 1 (KLF1) and mouse double minute 2 (MDM2). By activating both beta-globin and HbF gamma-globin genes, KLF1 encourages HbF repression, which is regulated by changing myeloblastosis expression. Conclusion: This study shows that the genes KLF1 and MDM2 are related to dysregulated molecular pathways, contribute to the development of beta thalassemia, and may be exploited as a platform for the induction of fetal hemoglobin in the development of therapeutics." @default.
• W4387680653 created "2023-10-17" @default.
• W4387680653 creator A5003678403 @default.
• W4387680653 creator A5008050583 @default.
• W4387680653 creator A5072284282 @default.
• W4387680653 creator A5072566023 @default.
• W4387680653 date "2023-01-01" @default.
• W4387680653 modified "2023-10-17" @default.
• W4387680653 title "Molecular pathways and gene networks in fetal hemoglobin as a novel protein target for beta-thalassemia" @default.
• W4387680653 doi "https://doi.org/10.4103/mgmj.mgmj_44_23" @default.
• W4387680653 hasPublicationYear "2023" @default.
• W4387680653 type Work @default.
• W4387680653 citedByCount "0" @default.
• W4387680653 crossrefType "journal-article" @default.
• W4387680653 hasAuthorship W4387680653A5003678403 @default.
• W4387680653 hasAuthorship W4387680653A5008050583 @default.
• W4387680653 hasAuthorship W4387680653A5072284282 @default.
• W4387680653 hasAuthorship W4387680653A5072566023 @default.
• W4387680653 hasBestOaLocation W43876806531 @default.
• W4387680653 hasConcept C104317684 @default.
• W4387680653 hasConcept C150194340 @default.
• W4387680653 hasConcept C152724338 @default.
• W4387680653 hasConcept C172680121 @default.
• W4387680653 hasConcept C2776317666 @default.
• W4387680653 hasConcept C2777799968 @default.
• W4387680653 hasConcept C2777940137 @default.
• W4387680653 hasConcept C2779234561 @default.
• W4387680653 hasConcept C2987395477 @default.
• W4387680653 hasConcept C54355233 @default.
• W4387680653 hasConcept C60644358 @default.
• W4387680653 hasConcept C70721500 @default.
• W4387680653 hasConcept C86803240 @default.
• W4387680653 hasConceptScore W4387680653C104317684 @default.
• W4387680653 hasConceptScore W4387680653C150194340 @default.
• W4387680653 hasConceptScore W4387680653C152724338 @default.
• W4387680653 hasConceptScore W4387680653C172680121 @default.
• W4387680653 hasConceptScore W4387680653C2776317666 @default.
• W4387680653 hasConceptScore W4387680653C2777799968 @default.
• W4387680653 hasConceptScore W4387680653C2777940137 @default.
• W4387680653 hasConceptScore W4387680653C2779234561 @default.
• W4387680653 hasConceptScore W4387680653C2987395477 @default.
• W4387680653 hasConceptScore W4387680653C54355233 @default.
• W4387680653 hasConceptScore W4387680653C60644358 @default.
• W4387680653 hasConceptScore W4387680653C70721500 @default.
• W4387680653 hasConceptScore W4387680653C86803240 @default.
• W4387680653 hasIssue "3" @default.
• W4387680653 hasLocation W43876806531 @default.
• W4387680653 hasOpenAccess W4387680653 @default.
• W4387680653 hasPrimaryLocation W43876806531 @default.
• W4387680653 hasRelatedWork W1479471826 @default.
• W4387680653 hasRelatedWork W2045978612 @default.
• W4387680653 hasRelatedWork W2164932045 @default.
• W4387680653 hasRelatedWork W2394799567 @default.
• W4387680653 hasRelatedWork W2407360281 @default.
• W4387680653 hasRelatedWork W2408406049 @default.
• W4387680653 hasRelatedWork W2418032027 @default.
• W4387680653 hasRelatedWork W2464759683 @default.
• W4387680653 hasRelatedWork W3018810360 @default.
• W4387680653 hasRelatedWork W4313346160 @default.
• W4387680653 hasVolume "10" @default.
• W4387680653 isParatext "false" @default.
• W4387680653 isRetracted "false" @default.
• W4387680653 workType "article" @default.