Influence of estradiol deficiency on the acute inflammatory response following a traumatic skeletal muscle injury

Abstract

Abstract Estradiol (E2) influences the inflammatory response. Research has shown that skeletal muscle chemokine mRNA expression and neutrophil infiltration after a traumatic freeze injury are blunted in ovariectomized mice treated with placebo compared to E2-treated mice. How E2 deficiency alters the acute muscle inflammatory response is unclear with potential mechanisms including alterations in the number of circulating leukocytes, leukocyte chemotaxis, and/or muscle chemokine expression. To investigate these possibilities, female C57BL/6J mice underwent a sham or ovariectomy (OVX) surgery, 21–28 d later tibialis anterior (TA) muscles were freeze injured. TA muscles and blood were collected 24 h post injury. Total white blood cell (149%) and monocytes (427%) were elevated in OVX compared to Sham mice but there was no difference in the neutrophil counts (p≥0.64). To determine if E2 deficiency impacts leukocyte chemotaxis, isolated leukocytes from bone marrow of non-injured Sham or OVX mice were placed in a transwell migration assay. OVX leukocytes had greater chemotaxis towards CXCL1 (37%), CXCL2 (43%), and CXCL5 (27%) than Sham. To examine if E2 deficiency alters muscle CXCL1 and CXCL5 protein content contributing to chemotaxis, ELISA assays were performed. Surprisingly, muscle CXCL1 and CXCL5 contents were similar between OVX and Sham. Collectively, mice lacking E2 have relatively high blood leukocytes and chemotaxis suggesting a greater acute inflammatory response which appears not to be driven by changes in muscle chemokine expression. Additional studies need to consider possible negative regulators of the acute inflammatory response in OVX muscle. Supported by DAL and GW (R01AG031743 & R01AG062899), and SLM (T32AR007612)