ELMO1 signaling is a promoter of osteoclast function and bone loss

Osteoporosis affects millions worldwide and is often caused by osteoclast induced bone loss. Here, we identify the cytoplasmic protein ELMO1 as an important 'signaling node' in osteoclasts. We note that ELMO1 SNPs associate with bone abnormalities in humans, and that ELMO1 deletion in mice reduces bone loss in four in vivo models: osteoprotegerin deficiency, ovariectomy, and two types of inflammatory arthritis. Our transcriptomic analyses coupled with CRISPR/Cas9 genetic deletion identify Elmo1 associated regulators of osteoclast function, including cathepsin G and myeloperoxidase. Further, we define the 'ELMO1 interactome' in osteoclasts via proteomics and reveal proteins required for bone degradation. ELMO1 also contributes to osteoclast sealing zone on bone-like surfaces and distribution of osteoclast-specific proteases. Finally, a 3D structure-based ELMO1 inhibitory peptide reduces bone resorption in wild type osteoclasts. Collectively, we identify ELMO1 as a signaling hub that regulates osteoclast function and bone loss, with relevance to osteoporosis and arthritis. Osteoporosis and bone fractures affect millions of patients worldwide and are often due to increased bone resorption. Here the authors identify the cytoplasmic protein ELMO1 as an important 'signaling node' promoting the bone resorption function of osteoclasts.

Automated summary

The study identified ELMO1 as a key signaling node in regulating osteoclast function and bone loss, demonstrating its association with bone abnormalities in both human SNPs and in vivo mouse models. ELMO1 is also found to be involved in the regulation of osteoclast-associated factors and proteins required for bone degradation, as well as contributing to the formation of sealing zones and distribution of proteases on bone surfaces in osteoclasts. Additionally, an ELMO1 inhibitory peptide based on 3D structure was shown to reduce bone resorption in wild type osteoclasts.