Therapeutic Implications of PPARγin Human Osteosarcoma

Author:

Wagner Eric R.1,He Bai-Cheng12,Chen Liang12,Zuo Guo-Wei12,Zhang Wenli13,Shi Qiong12,Luo Qing12,Luo Xiaoji12,Liu Bo12,Luo Jinyong12,Rastegar Farbod1,He Connie J.1,Hu Yawen1,Boody Barrett1,Luu Hue H.1,He Tong-Chuan12,Deng Zhong-Liang12,Haydon Rex C.1

Affiliation:

1. Molecular Oncology Laboratory, Department of Surgery, The University of Chicago Medical Center, Chicago, IL 60637, USA

2. Key Laboratory of Diagnostic Medicine, Chongqing Medical University, Chinese Ministry of Education, Chongqing 400016, China

3. Department of Orthopaedics, West China Hospital, Sichuan University, Sichuan 610041, China

Abstract

Osteosarcoma (OS) is the most common nonhematologic malignancy of bone in children and adults. Although dysregulation of tumor suppressor genes and oncogenes, such as Rb, p53, and the genes critical to cell cycle control, genetic stability, and apoptosis have been identified in OS, consensus genetic changes that lead to OS development are poorly understood. Disruption of the osteogenic differentiation pathway may be at least in part responsible for OS tumorigenesis. Current OS management involves chemotherapy and surgery. Peroxisome proliferator-activated receptor (PPAR) agonists and/or retinoids can inhibit OS proliferation and induce apoptosis and may inhibit OS growth by promoting osteoblastic terminal differentiation. Thus, safe and effective PPAR agonists and/or retinoid derivatives can be then used as adjuvant therapeutic drugs for OS therapy. Furthermore, these agents have the potential to be used as chemopreventive agents for the OS patients who undergo the resection of the primary bone tumors in order to prevent local recurrence and/or distal pulmonary metastasis.

Funder

Brinson Foundation

Publisher

Hindawi Limited

Subject

Pharmacology (medical),Drug Discovery

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