Targeting glioma-initiating cells via the tyrosine metabolic pathway

胶质瘤 癌症研究 医学 脑瘤 酪氨酸 肿瘤进展 病理 生物 内科学 癌症 生物化学
作者
Daisuke Yamashita,Joshua D. Bernstock,Galal Elsayed,Hirokazu Sadahiro,Ahmed Mohyeldin,Gustavo Chagoya,Adeel Ilyas,James Mooney,Dagoberto Estévez-Ordoñez,Shinobu Yamaguchi,Victoria L. Flanary,James R. Hackney,Krishna Bhat,Harley I. Kornblum,Nicola Zamboni,Sung-Hak Kim,E. Antonio Chiocca,Ichiro Nakano
出处
期刊:Journal of Neurosurgery [American Association of Neurological Surgeons]
卷期号:134 (3): 721-732 被引量:26
标识
DOI:10.3171/2019.11.jns192028
摘要

Despite an aggressive multimodal therapeutic regimen, glioblastoma (GBM) continues to portend a grave prognosis, which is driven in part by tumor heterogeneity at both the molecular and cellular levels. Accordingly, herein the authors sought to identify metabolic differences between GBM tumor core cells and edge cells and, in so doing, elucidate novel actionable therapeutic targets centered on tumor metabolism.Comprehensive metabolic analyses were performed on 20 high-grade glioma (HGG) tissues and 30 glioma-initiating cell (GIC) sphere culture models. The results of the metabolic analyses were combined with the Ivy GBM data set. Differences in tumor metabolism between GBM tumor tissue derived from within the contrast-enhancing region (i.e., tumor core) and that from the peritumoral brain lesions (i.e., tumor edge) were sought and explored. Such changes were ultimately confirmed at the protein level via immunohistochemistry.Metabolic heterogeneity in both HGG tumor tissues and GBM sphere culture models was identified, and analyses suggested that tyrosine metabolism may serve as a possible therapeutic target in GBM, particularly in the tumor core. Furthermore, activation of the enzyme tyrosine aminotransferase (TAT) within the tyrosine metabolic pathway influenced the noted therapeutic resistance of the GBM core.Selective inhibition of the tyrosine metabolism pathway may prove highly beneficial as an adjuvant to multimodal GBM therapies.

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