Anabolic Effects of a Novel Simvastatin Derivative on Treating Rat Bone Defects

Author:

Lee Tien-ChingORCID,Chen Hui-Ting,Tai I-Chun,Kao Li-TingORCID,Hung Ming-Hsin,Chen Chung-HwanORCID,Fu Yin-Chih,Wang Yan-Hsiung,Kao Chih-Ming,Chang Je-KenORCID,Ho Mei-Ling

Abstract

Large bone defects may develop fracture nonunion, leading to disability and psychosocial burdens. Bone grafting with anabolic agents is a good autografting alternative. Simvastatin, as a cholesterol-lowering agent worldwide, is proven to enhance osteogenesis. Considering its dose-dependent adverse effects, we developed a simvastatin derivative, named KMUHC-01, which has bone anabolic capacity and lower cytotoxicity than simvastatin. We hypothesize that KMUHC-01 could help bone formation in bone-defect animal models. We used rat models of critical calvarial and long-bone defects to evaluate the effects of KMUHC-01 and simvastatin on biological changes at the bone defect through histology, immunohistology, and mechanical testing using three-point bending and evaluated the new bone formation microstructure through microcomputed tomography analysis. The newly formed bone microstructure at the calvarial defect site showed a significantly improved trabecular bone volume in the KMUHC-01 1-μM group compared with that in the control and simvastatin groups. The biomechanical study revealed a significantly increased maximal strength in the KMUHC-01 1-μM group compared with that in the control group. KUMHC-01, as a simvastatin derivative, showed a great anabolic effect in promoting bone defect healing. However, further studies will be conducted to prove the bioavailability and bone-forming efficacy of KMUHC-01 via systemic administration.

Funder

Ministry of Science and Technology

Kaohsiung Municipal Ta-Tung Hospital

Regenerative Medicine and Cell Therapy Research Center

Publisher

MDPI AG

Subject

General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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