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Background: Glioblastoma is an aggressive brain tumor linked to significant angiogenesis and poor prognosis. Anti-angiogenic therapies with vascular endothelial growth factor receptor 2 (VEGFR2) inhibition have been investigated as an alternative glioblastoma treatment. However, little is known about the effect of VEGFR2 blockade on glioblastoma cells per se.

Methods: VEGFR2 expression data in glioma patients were retrieved from the public database TCGA. VEGFR2 intervention was implemented by using its selective inhibitor Ki8751 or shRNA. Mitochondrial biogenesis of glioblastoma cells was assessed by immunofluorescence imaging, mass spectrometry, and western blot analysis.

Results: VEGFR2 expression was higher in glioma patients with higher malignancy (grade III and IV). VEGFR2 inhibition hampered glioblastoma cell proliferation and induced cell apoptosis. Mass spectrometry and immunofluorescence imaging showed that the anti-glioblastoma effects of VEGFR2 blockade involved mitochondrial biogenesis, as evidenced by the increases of mitochondrial protein expression, mitochondria mass, mitochondrial oxidative phosphorylation (OXPHOS), and reactive oxygen species (ROS) production, all of which play important roles in tumor cell apoptosis, growth inhibition, cell cycle arrest and cell senescence. Furthermore, VEGFR2 inhibition exaggerated mitochondrial biogenesis by decreased phosphorylation of AKT and peroxisome proliferator-activated receptor gamma coactivator 1-alpha (PGC1α), which mobilized PGC1α into the nucleus, increased mitochondrial transcription factor A (TFAM) expression, and subsequently enhanced mitochondrial biogenesis.

Conclusions: VEGFR2 blockade inhibits glioblastoma progression via AKT-PGC1α-TFAM-mitochondria biogenesis signaling cascade, suggesting that VEGFR2 intervention might bring additive therapeutic values to anti-glioblastoma therapy.

Titel:	VEGFR2 blockade inhibits glioblastoma cell proliferation by enhancing mitochondrial biogenesis.
Autor/in / Beteiligte Person:	Guo, M ; Zhang, J ; Han, J ; Hu, Y ; Ni, H ; Yuan, J ; Sun, Y ; Liu, M ; Gao, L ; Liao, W ; Ma, C ; Liu, Y ; Li, S ; Li, N
Link:	Full Text Finder (Volltext)
Zeitschrift:	Journal of translational medicine, Jg. 22 (2024-05-03), Heft 1, S. 419
Veröffentlichung:	[London] : BioMed Central, 2003-, 2024
Medientyp:	academicJournal
ISSN:	1479-5876 (electronic)
DOI:	10.1186/s12967-024-05155-1
Schlagwort:	Humans Cell Line, Tumor Reactive Oxygen Species metabolism Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha metabolism Brain Neoplasms pathology Brain Neoplasms metabolism Brain Neoplasms drug therapy Proto-Oncogene Proteins c-akt metabolism Signal Transduction drug effects Glioblastoma pathology Glioblastoma metabolism Glioblastoma drug therapy Vascular Endothelial Growth Factor Receptor-2 metabolism Cell Proliferation drug effects Mitochondria metabolism Mitochondria drug effects Organelle Biogenesis Apoptosis drug effects
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, Non-U.S. Gov't Language: English [J Transl Med] 2024 May 03; Vol. 22 (1), pp. 419. <i>Date of Electronic Publication: </i>2024 May 03. MeSH Terms: Glioblastoma* / pathology ; Glioblastoma* / metabolism ; Glioblastoma* / drug therapy ; Vascular Endothelial Growth Factor Receptor-2* / metabolism ; Cell Proliferation* / drug effects ; Mitochondria* / metabolism ; Mitochondria* / drug effects ; Organelle Biogenesis* ; Apoptosis* / drug effects ; Humans ; Cell Line, Tumor ; Reactive Oxygen Species / metabolism ; Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha / metabolism ; Brain Neoplasms / pathology ; Brain Neoplasms / metabolism ; Brain Neoplasms / drug therapy ; Proto-Oncogene Proteins c-akt / metabolism ; Signal Transduction / drug effects References: Nature. 2011 Oct 19;478(7369):399-403. (PMID: 22012397) ; Cell Oncol (Dordr). 2019 Oct;42(5):679-690. (PMID: 31325096) ; J Exp Clin Cancer Res. 2020 Oct 7;39(1):208. (PMID: 33028364) ; Cancer Commun (Lond). 2022 Mar;42(3):245-265. (PMID: 35234370) ; Cancer Biol Med. 2021 Feb 15;18(1):139-154. (PMID: 33628590) ; Cancer Cell. 2003 Oct;4(4):257-62. (PMID: 14585353) ; Aging Cell. 2008 Jan;7(1):101-11. (PMID: 18031569) ; Nature. 2016 Sep 15;537(7620):422-426. (PMID: 27580028) ; Clin Cancer Res. 2009 Feb 1;15(3):887-97. (PMID: 19188159) ; Vascul Pharmacol. 2016 Nov;86:14-17. (PMID: 27268035) ; Neurochem Res. 2017 Mar;42(3):918-924. (PMID: 27568206) ; Clin Immunol. 2023 Jun;251:109333. (PMID: 37088298) ; Int J Cancer. 2011 Nov 1;129(9):2115-23. (PMID: 21618508) ; Brain Tumor Pathol. 2011 Oct;28(4):291-6. (PMID: 21691733) ; Nature. 2010 Dec 9;468(7325):829-33. (PMID: 21102433) ; Int J Mol Sci. 2018 Dec 12;19(12):. (PMID: 30545129) ; Cancer Res. 2023 Apr 4;83(7):1094-1110. (PMID: 36696363) ; PLoS One. 2011;6(12):e28947. (PMID: 22174934) ; Cancer Res. 2018 Feb 1;78(3):731-741. (PMID: 29229602) ; Chemother Res Pract. 2011;2011:878912. (PMID: 22295207) ; Cell Res. 2018 Mar;28(3):265-280. (PMID: 29219147) ; Neuro Oncol. 2018 Oct 1;20(suppl_4):iv1-iv86. (PMID: 30445539) ; Biomolecules. 2020 Jan 06;10(1):. (PMID: 31935965) ; N Engl J Med. 2017 Nov 16;377(20):1954-1963. (PMID: 29141164) ; Oncogenesis. 2022 Oct 4;11(1):59. (PMID: 36195584) ; Gastroenterology. 2015 Jul;149(1):177-189.e10. (PMID: 25797700) ; N Engl J Med. 2014 Feb 20;370(8):699-708. (PMID: 24552317) ; Nat Cell Biol. 2016 Jun;18(6):645-656. (PMID: 27214280) ; PLoS Med. 2007 Jun;4(6):e186. (PMID: 17550303) ; Cell Rep. 2021 Apr 27;35(4):109024. (PMID: 33910005) ; Oncogene. 2006 Aug 10;25(35):4913-22. (PMID: 16547494) ; Neurooncol Adv. 2020 May 27;2(1):vdaa061. (PMID: 32642713) ; J Cancer. 2023 Jun 19;14(10):1781-1793. (PMID: 37476183) ; J Cell Mol Med. 2022 Feb;26(3):893-912. (PMID: 34964241) ; Neuro Oncol. 2016 May;18(5):667-78. (PMID: 26420897) ; J Radiat Res. 2010;51(3):343-8. (PMID: 20410674) ; J Exp Med. 2012 Mar 12;209(3):507-20. (PMID: 22393126) ; Int J Radiat Biol. 2019 Jul;95(7):912-919. (PMID: 30822194) ; Oncogene. 2021 Aug;40(32):5066-5080. (PMID: 34021259) ; Front Pharmacol. 2019 Jul 10;10:772. (PMID: 31354487) ; N Engl J Med. 2014 Feb 20;370(8):709-22. (PMID: 24552318) ; Cancer Cell. 2013 Mar 18;23(3):287-301. (PMID: 23416000) Grant Information: STINT the Swedish Foundation for Internationalisation of Higher Education and Research; CH2017-7179 the Swedish Foundation for Internationalisation of Higher Education and Research; 82273244 the National Science Foundation of China; No.7244328 Natural Science Foundation of Beijing Municipality; No.PYZ22122 the Capital Medical University Scientific Research Cultivation Fund; No.PYZ23112 the Capital Medical University Scientific Research Cultivation Fund Contributed Indexing: Keywords: Glioblastoma; Mitochondria; Mitochondrial transcription factor A; Peroxisome proliferator-activated receptor gamma coactivator 1-α/PGC1α; Reactive oxygen species; Vascular endothelial growth factor receptor 2 Substance Nomenclature: EC 2.7.10.1 (Vascular Endothelial Growth Factor Receptor-2) ; 0 (Reactive Oxygen Species) ; 0 (Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha) ; EC 2.7.11.1 (Proto-Oncogene Proteins c-akt) ; EC 2.7.10.1 (KDR protein, human) Entry Date(s): Date Created: 20240503 Date Completed: 20240504 Latest Revision: 20240520 Update Code: 20240520 PubMed Central ID: PMC11067099

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VEGFR2 blockade inhibits glioblastoma cell proliferation by enhancing mitochondrial biogenesis.