| Literature DB >> 33309780 |
Liyang Zhang1, Fangkun Liu2, Nathaniel Weygant3, Junxia Zhang4, Ping Hu5, Zailong Qin6, Jingxuan Yang7, Quan Cheng8, Fan Fan9, Yu Zeng10, Yongjian Tang11, Yusheng Li12, Anliu Tang13, Fengqiong He14, Jun Peng15, Weihua Liao16, Zhongliang Hu17, Min Li18, Zhixiong Liu19.
Abstract
A physiologically relevant glioma tumor model is important to the study of disease progression and screening drug candidates. However, current preclinical glioma models lack the brain microenvironment, and the established tumor cell lines do not represent glioma biology and cannot be used to evaluate the therapeutic effect. Here, we reported a real-time integrated system by generating 3D ex vivo cerebral organoids and in vivo xenograft tumors based on glioma patient-derived tissues and cells. Our system faithfully recapitulated the histological features, response to chemotherapy drugs, and clinical progression of their corresponding parental tumors. Additionally, our model successfully identified a case from a grade II astrocytoma patient with typical grade IV GBM features in both organoids and xenograft models, which mimicked the disease progression of this patient. Further genomic and transcriptomic characterization was associated with individual clinical features. We have demonstrated the "GBM-&Normal-like" signature to predict prognosis. In conclusion, we developed an integrated system of parallel models from patient-derived glioma cerebral organoids and xenografts for understanding the glioma biology and prediction of response to chemotherapy drugs, which might lead to a new strategy for personalized treatment for this deadly disease.Entities:
Keywords: Cerebral organoid; Disease modeling; Drug screening; GBM; Patient-derived glioma model
Year: 2020 PMID: 33309780 DOI: 10.1016/j.canlet.2020.12.013
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679