| Literature DB >> 25273088 |
Takatsune Shimizu1, Eiji Sugihara2, Sayaka Yamaguchi-Iwai3, Sakura Tamaki4, Yuko Koyama4, Walied Kamel5, Arisa Ueki6, Tomoki Ishikawa7, Tatsuyuki Chiyoda6, Satoru Osuka6, Nobuyuki Onishi6, Hiroko Ikeda8, Junzo Kamei8, Koichi Matsuo9, Yumi Fukuchi10, Toshihiro Nagai11, Junya Toguchida12, Yoshiaki Toyama13, Akihiro Muto10, Hideyuki Saya14.
Abstract
Osteosarcoma is a malignant bone tumor in children and adolescents characterized by intrinsic therapeutic resistance. The IGF2 is expressed at elevated levels in osteosarcoma after treatment with chemotherapy, prompting an examination of its functional contributions to resistance. We found that continuous exposure to IGF2 or insulin in the absence of serum created a dormant growth state in osteosarcoma cells that conferred resistance to various chemotherapeutic drugs in vitro. Mechanistic investigations revealed that this dormant state correlated with downregulation of downstream signaling by the IGF1 receptor, heightened cell survival, enhanced autophagy, and the presence of extracellular glutamine. Notably, inhibiting autophagy or depleting glutamine was sufficient to increase chemotherapeutic sensitivity in osteosarcoma xenografts in mice. Clinically, we confirmed that IGF expression levels were elevated in human osteosarcoma specimens from patients who received chemotherapy. Together, our results suggest that activation of IGF or insulin signaling preserves the survival of osteosarcoma cells under chemotherapeutic stress, providing a drug-resistant population that may engender minimal residual disease. Attenuating this survival mechanism may help overcome therapeutic resistance in osteosarcoma. ©2014 American Association for Cancer Research.Entities:
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Year: 2014 PMID: 25273088 DOI: 10.1158/0008-5472.CAN-14-0914
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701