Cancers, 2020-03, Vol.12 (3), p.752
- Tran, Huy Minh
- Wu, Kuo-Sheng
- Sung, Shian-Ying
- Changou, Chun Austin
- Hsieh, Tsung-Han
- Liu, Yun-Ru
- Liu, Yen-Lin
- Tsai, Min-Lan
- Lee, Hsin-Lun
- Hsieh, Kevin Li-Chun
- Huang, Wen-Chang
- Liang, Muh-Lii
- Chen, Hsin-Hung
- Lee, Yi-Yen
- Lin, Shih-Chieh
- Ho, Donald Ming-Tak
- Chang, Feng-Chi
- Chao, Meng-En
- Chen, Wan
- Chu, Shing-Shung
- Yu, Alice L
- Yen, Yun
- Chang, Che-Chang
- Wong, Tai-Tong
2020
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Details
- Autor(en) / Beteiligte
- Tran, Huy Minh
- Wu, Kuo-Sheng
- Sung, Shian-Ying
- Changou, Chun Austin
- Hsieh, Tsung-Han
- Liu, Yun-Ru
- Liu, Yen-Lin
- Tsai, Min-Lan
- Lee, Hsin-Lun
- Hsieh, Kevin Li-Chun
- Huang, Wen-Chang
- Liang, Muh-Lii
- Chen, Hsin-Hung
- Lee, Yi-Yen
- Lin, Shih-Chieh
- Ho, Donald Ming-Tak
- Chang, Feng-Chi
- Chao, Meng-En
- Chen, Wan
- Chu, Shing-Shung
- Yu, Alice L
- Yen, Yun
- Chang, Che-Chang
- Wong, Tai-Tong
- Titel
- Upregulation of Protein Synthesis and Proteasome Degradation Confers Sensitivity to Proteasome Inhibitor Bortezomib in Myc-Atypical Teratoid/Rhabdoid Tumors
- Ist Teil von
- Cancers, 2020-03, Vol.12 (3), p.752
- Ort / Verlag
- Switzerland: MDPI AG
- Erscheinungsjahr
- 2020
- Quelle
- EZB Electronic Journals Library
- Beschreibungen/Notizen
- Atypical teratoid rhabdoid tumors (ATRTs) are among the most malignant brain tumors in early childhood and remain incurable. Myc-ATRT is driven by the oncogene, which directly controls the intracellular protein synthesis rate. Proteasome inhibitor bortezomib (BTZ) was approved by the Food and Drug Administration as a primary treatment for multiple myeloma. This study aimed to determine whether the upregulation of protein synthesis and proteasome degradation in Myc-ATRTs increases tumor cell sensitivity to BTZ. We performed differential gene expression and gene set enrichment analysis on matched primary and recurrent patient-derived xenograft (PDX) samples from an infant with ATRT. Concomitant upregulation of the Myc pathway, protein synthesis and proteasome degradation were identified in recurrent ATRTs. Additionally, we found the proteasome-encoding genes were highly expressed in ATRTs compared with in normal brain tissues, correlated with the malignancy of tumor cells and were essential for tumor cell survival. BTZ inhibited proliferation and induced apoptosis through the accumulation of p53 in three human Myc-ATRT cell lines (PDX-derived tumor cell line Re1-P6, BT-12 and CHLA-266). Furthermore, BTZ inhibited tumor growth and prolonged survival in Myc-ATRT orthotopic xenograft mice. Our findings suggest that BTZ may be a promising targeted therapy for Myc-ATRTs.
- Sprache
- Englisch
- Identifikatoren
- ISSN: 2072-6694eISSN: 2072-6694DOI: 10.3390/cancers12030752Titel-ID: cdi_doaj_primary_oai_doaj_org_article_411a987e292840b0b81b4f4c3b2d08cf
- Format
- –
- Schlagworte
- Apoptosis, Bortezomib, Brain tumors, Cancer therapies, Cell proliferation, Cell survival, Chemotherapy, Children, Gene expression, Gene set enrichment analysis, Malignancy, Medical prognosis, Multiple myeloma, Myc protein, myc-atrts, p53, p53 Protein, Principal components analysis, proteasome degradation, Proteasome inhibitors, Protein biosynthesis, Protein synthesis, Proteins, Tumor cell lines, Tumor cells, Tumors, Up-regulation, Xenografts