Lowering circulating apolipoprotein E levels improves aged bone fracture healing
Rong Huang, Xiaohua Zong, Puviindran Nadesan, Janet L. Huebner, Virginia B. Kraus, James P. White, Phillip J. White, Gurpreet S. Baht
Rong Huang, Xiaohua Zong, Puviindran Nadesan, Janet L. Huebner, Virginia B. Kraus, James P. White, Phillip J. White, Gurpreet S. Baht
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Research Article Bone biology

Lowering circulating apolipoprotein E levels improves aged bone fracture healing

Abstract

Age is a well-established risk factor for impaired bone fracture healing. Here, we identify a role for apolipoprotein E (ApoE) in age-associated impairment of bone fracture healing and osteoblast differentiation, and we investigate the mechanism by which ApoE alters these processes. We identified that, in both humans and mice, circulating ApoE levels increase with age. We assessed bone healing in WT and ApoE–/– mice after performing tibial fracture surgery: bone deposition was higher within fracture calluses from ApoE–/– mice. In vitro recombinant ApoE (rApoE) treatment of differentiating osteoblasts decreased cellular differentiation and matrix mineralization. Moreover, this rApoE treatment decreased osteoblast glycolytic activity while increasing lipid uptake and fatty acid oxidation. Using parabiosis models, we determined that circulating ApoE plays a strong inhibitory role in bone repair. Using an adeno-associated virus–based siRNA system, we decreased circulating ApoE levels in 24-month-old mice and demonstrated that, as a result, fracture calluses from these aged mice displayed enhanced bone deposition and mechanical strength. Our results demonstrate that circulating ApoE as an aging factor inhibits bone fracture healing by altering osteoblast metabolism, thereby identifying ApoE as a new therapeutic target for improving bone repair in the elderly.

Authors

Rong Huang, Xiaohua Zong, Puviindran Nadesan, Janet L. Huebner, Virginia B. Kraus, James P. White, Phillip J. White, Gurpreet S. Baht

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Figure 4

Circulating ApoE inhibits bone fracture healing.

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Circulating ApoE inhibits bone fracture healing. (A) Schematic diagram: ...
(A) Schematic diagram: WT and ApoE–/– mice were anastomosed together, resulting in a shared blood supply. (B) After 4 weeks of anastomosis, ELISA was used to measure circulating ApoE levels within each mouse. (C) One WT mouse within each pairing underwent tibial fracture surgery, and fracture calluses were assessed 21 days after injury for healing. Scale bar: 1 mm. (D) Bone ratio within the callus and (E) tissue mineral density of the callus were measured using μCT and (F) histomorphometry (decalcified, paraffin embedded, Alcian blue/hematoxylin/Orange G stain) was used to quantify the amount of bone tissue deposited within the fracture callus. For both WT-WT pairs and for WT-ApoE–/– pairs, n = 5. Data are expressed as mean ± 95% confidence interval. *P < 0.05.