Show pageBacklinksCite current pageExport to PDFBack to top This page is read only. You can view the source, but not change it. Ask your administrator if you think this is wrong. ====== MCT1 ====== High Expression in GBM: MCT1 and [[MCT4]] are significantly overexpressed in IDH-wildtype [[glioblastoma]]s compared to IDH-mutant gliomas (grades 2–4), both at the [[protein]] (IHC) and [[mRNA]] levels. Endothelial Proliferation Specificity: Loss of MCT1 expression was noted in areas of endothelial proliferation within grade 4 gliomas, contrasting with its presence in non-proliferating endothelium—suggesting a specific microenvironmental regulation. Prognostic Implications: High MCT1/4 expression correlates with shorter overall survival when analyzing all [[glioma]]s together, although this correlation was not significant in GBM alone. Therapeutic Insight – [[Syrosingopine]]: Syrosingopine, a dual MCT1/4 inhibitor and old antihypertensive drug with good CNS penetration, showed dose-dependent anti-tumor effects in vitro on U87MG and LN229 glioma cell lines: Increased cytotoxicity Enhanced apoptosis Reduced migration/invasion Clinical Relevance: MCT1/4 may serve as diagnostic immunohistochemical markers. [[Syrosingopine]], a dual [[MCT1]]/4 inhibitor and old antihypertensive drug with good CNS penetration, showed dose-dependent anti-tumor effects in vitro on [[U87]]MG and [[LN229]] glioma cell lines: Increased cytotoxicity Enhanced apoptosis Reduced migration/invasion Clinical Relevance: MCT1/4 may serve as diagnostic immunohistochemical markers. Syrosingopine may represent a promising adjunctive therapy for GBM ((Behera MM, Purkait S, Ghosh A, Sable MN, Sahu RN, Chhabra G. The [[Monocarboxylate Transporter]]s [[MCT1]] and [[MCT4]] Are Highly Expressed in [[Glioblastoma]] and Crucially Implicated in the [[Pathobiology]]. Neuropathology. 2025 Mar 27. doi: 10.1111/neup.70006. Epub ahead of print. PMID: 40145253.)) mct1.txt Last modified: 2025/03/27 10:42by 127.0.0.1