The adiponectin receptor agonist AdipoAI attenuates periodontitis in diabetic rats by inhibiting gingival fibroblast‐induced macrophage migration

Abstract

Background and PurposeLow‐grade inflammation, a common feature of both diabetes and periodontitis, partly accounts for the complexity and refractoriness of diabetes‐associated periodontitis. Adiponectin (APN), the most abundant adipokine in human blood, has been widely reported to have anti‐inflammatory functions. Herein, we investigated the ability of an APN receptor agonist, AdipoAI, to alleviate diabetes‐associated periodontitis. Furthermore, we revealed the possible mechanism underlying its anti‐inflammatory effects.Experimental ApproachThe maxillary first molar of Zucker diabetic fatty (ZDF) rats was ligated to construct a diabetes‐associated periodontitis model, and rats were administered AdipoAI by gavage. We examined diabetes‐related indexes, pathological changes in insulin target organs, alveolar bone resorption and systemic and local inflammation. In vitro, transwell assays were used to evaluate monocyte/macrophage migration induced by human gingival fibroblasts (hGFs) with/without AdipoAI treatment. Additionally, we examined chemokine expression levels in hGFs and hGF‐induced monocyte/macrophage migration upon siRNA knockdown of Adiponectin receptor expression. Expression of Adipo1/Adipo2 receptors and inflammation‐related signalling pathways were examined by IHC and WB, followed by confirmation with an NF‐κB P65 inhibitor (BAY 11‐7082).Key ResultsAdipoAI lowered fasting blood glucose and serum insulin in ZDF rats and alleviated inflammation in insulin target tissues. Locally, AdipoAI reduced alveolar bone absorption and gingival inflammation. Mechanistically, AdipoAI inhibited hGF‐induced monocyte/macrophage migration by reducing CCL2 secretion. In hGFs, AdipoAI attenuated LPS‐induced activation of NF‐κB P65 and CCL2 expression, which was dependent on the Adipo receptor 1.Conclusion and ImplicationsAdipoAI, with its ability to alleviate inflammatory damage in tissues, is a candidate for diabetes‐associated periodontitis treatment.