Reduced APOE Expression Improves Bone Regeneration in Aged Mice

APOE, a major apolipoprotein on low‑density lipoprotein particles, has long been studied for its role in cholesterol transport and atherosclerosis. Recent epidemiological data reveal that circulating APOE concentrations rise with age, coinciding with a decline in skeletal integrity and slower fracture repair. This correlation prompted investigators to question whether APOE itself might directly interfere with the cellular programs that rebuild bone. Understanding this link is especially relevant as the global population ages and the economic burden of osteoporotic fractures continues to climb.

The open‑access study employed hepatic APOE knockout mice and a short‑acting neutralizing antibody to dissect the protein’s impact on bone healing. Both interventions reduced serum APOE, leading to a 30‑40 % increase in callus mineral density and stronger biomechanical outcomes in tibial fractures of aged mice. Mechanistically, APOE bound the Lrp4 receptor on bone‑marrow‑derived stem cells, dampening Wnt/β‑catenin signaling and blocking their differentiation into osteoblasts. Neutralizing the protein restored this pathway, allowing stem cells to mature and deposit new extracellular matrix.

These findings open a new therapeutic avenue that complements existing osteoporosis treatments, which mainly focus on bone resorption. A transient antibody could be administered shortly after injury, delivering a bone‑specific benefit without the lifelong lipid alterations seen with genetic knock‑down. Nevertheless, APOE also plays a protective role in lipid metabolism, and chronic suppression could elevate cardiovascular risk. Future work must therefore balance fracture‑healing gains against potential atherogenic effects, perhaps by refining delivery to the liver or developing bone‑targeted carriers. If safety hurdles are cleared, APOE modulation could become a cornerstone of geriatric orthopaedic care.