FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4295412654> ?p ?o ?g. }

• W4295412654 abstract "Gliomas are the most prevalent kind of malignant and severe brain cancer. Apoptosis regulating mechanisms are disturbed in malignant gliomas, as they are in added forms of malignancy. Understanding apoptosis and other associated processes are thought to be critical for understanding the origins of malignant tumors and designing anti-cancerous drugs for the treatment. The purpose of this study was to evaluate the variation in the expression level of several apoptotic proteins that are responsible for apoptosis in low to high-grade glioma. This suggests a significant change in the expression of five apoptotic proteins: Clusterin, HSP27, Catalase, Cytochrome C, and SMAC. Cytochrome C, one of the five substantially altered proteins, is a crucial component of the apoptotic cascade. The complex enzyme Cytochrome C is involved in metabolic pathways such as respiration and cell death. The results demonstrated that Cytochrome C expression levels are lower in glioma tissues than in normal tissues. What's more intriguing is that the expression level decreases with an increase in glioma grades. As a result, the discovery shows that Cytochrome C may be a target for glioma prognostic biomarkers." @default.
• W4295412654 created "2022-09-13" @default.
• W4295412654 creator A5010130353 @default.
• W4295412654 creator A5015254224 @default.
• W4295412654 creator A5020058862 @default.
• W4295412654 creator A5020250424 @default.
• W4295412654 creator A5029438224 @default.
• W4295412654 creator A5032560400 @default.
• W4295412654 creator A5048222955 @default.
• W4295412654 creator A5057111603 @default.
• W4295412654 creator A5068372503 @default.
• W4295412654 creator A5071101610 @default.
• W4295412654 creator A5082607751 @default.
• W4295412654 creator A5091838258 @default.
• W4295412654 date "2022-09-13" @default.
• W4295412654 modified "2023-09-24" @default.
• W4295412654 title "Cytochrome C as a potential clinical marker for diagnosis and treatment of glioma" @default.
• W4295412654 cites W1506642042 @default.
• W4295412654 cites W1515506492 @default.
• W4295412654 cites W1550975546 @default.
• W4295412654 cites W1618299283 @default.
• W4295412654 cites W1835909107 @default.
• W4295412654 cites W1916970793 @default.
• W4295412654 cites W1965760417 @default.
• W4295412654 cites W1970514669 @default.
• W4295412654 cites W1987126302 @default.
• W4295412654 cites W1989157196 @default.
• W4295412654 cites W1998439025 @default.
• W4295412654 cites W1999381573 @default.
• W4295412654 cites W2011993914 @default.
• W4295412654 cites W2015094489 @default.
• W4295412654 cites W2025729195 @default.
• W4295412654 cites W2032984191 @default.
• W4295412654 cites W2035660903 @default.
• W4295412654 cites W2038208489 @default.
• W4295412654 cites W2055829071 @default.
• W4295412654 cites W2057129424 @default.
• W4295412654 cites W2072841722 @default.
• W4295412654 cites W2074978845 @default.
• W4295412654 cites W2107789276 @default.
• W4295412654 cites W2124311542 @default.
• W4295412654 cites W2128951234 @default.
• W4295412654 cites W2133650808 @default.
• W4295412654 cites W2136096552 @default.
• W4295412654 cites W2139937771 @default.
• W4295412654 cites W2141565353 @default.
• W4295412654 cites W2146226667 @default.
• W4295412654 cites W2148977460 @default.
• W4295412654 cites W2149967205 @default.
• W4295412654 cites W2171317213 @default.
• W4295412654 cites W2235236654 @default.
• W4295412654 cites W2313086999 @default.
• W4295412654 cites W2366536035 @default.
• W4295412654 cites W2398656198 @default.
• W4295412654 cites W2505666614 @default.
• W4295412654 cites W2515008081 @default.
• W4295412654 cites W2515804433 @default.
• W4295412654 cites W2577310139 @default.
• W4295412654 cites W2598780850 @default.
• W4295412654 cites W2606306441 @default.
• W4295412654 cites W2766986991 @default.
• W4295412654 cites W2796968871 @default.
• W4295412654 cites W2886761670 @default.
• W4295412654 cites W2980499488 @default.
• W4295412654 cites W3023279101 @default.
• W4295412654 cites W3174246647 @default.
• W4295412654 cites W4230172521 @default.
• W4295412654 cites W2417836974 @default.
• W4295412654 doi "https://doi.org/10.3389/fonc.2022.960787" @default.
• W4295412654 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36176404" @default.
• W4295412654 hasPublicationYear "2022" @default.
• W4295412654 type Work @default.
• W4295412654 citedByCount "2" @default.
• W4295412654 countsByYear W42954126542022 @default.
• W4295412654 countsByYear W42954126542023 @default.
• W4295412654 crossrefType "journal-article" @default.
• W4295412654 hasAuthorship W4295412654A5010130353 @default.
• W4295412654 hasAuthorship W4295412654A5015254224 @default.
• W4295412654 hasAuthorship W4295412654A5020058862 @default.
• W4295412654 hasAuthorship W4295412654A5020250424 @default.
• W4295412654 hasAuthorship W4295412654A5029438224 @default.
• W4295412654 hasAuthorship W4295412654A5032560400 @default.
• W4295412654 hasAuthorship W4295412654A5048222955 @default.
• W4295412654 hasAuthorship W4295412654A5057111603 @default.
• W4295412654 hasAuthorship W4295412654A5068372503 @default.
• W4295412654 hasAuthorship W4295412654A5071101610 @default.
• W4295412654 hasAuthorship W4295412654A5082607751 @default.
• W4295412654 hasAuthorship W4295412654A5091838258 @default.
• W4295412654 hasBestOaLocation W42954126541 @default.
• W4295412654 hasConcept C123249941 @default.
• W4295412654 hasConcept C181199279 @default.
• W4295412654 hasConcept C190283241 @default.
• W4295412654 hasConcept C2778227246 @default.
• W4295412654 hasConcept C2779476363 @default.
• W4295412654 hasConcept C2780768313 @default.
• W4295412654 hasConcept C29311851 @default.
• W4295412654 hasConcept C502942594 @default.
• W4295412654 hasConcept C55493867 @default.
• W4295412654 hasConcept C86803240 @default.
• W4295412654 hasConceptScore W4295412654C123249941 @default.

• next