Arhgef1 Regulates α5β1 Integrin-Mediated Matrix Metalloproteinase Expression and Is Required for Homeostatic Lung Immunity

Pulmonary immunity depends on the ability of leukocytes to neutralize potentially harmful and frequent insults to the lung, and appropriate regulation of leukocyte migration and adhesion is integral to this process. Arhgef1 is a hematopoietic-restricted signaling molecule that regulates leukocyte migration and integrin-mediated adhesion. To explore a possible regulatory role for Arhgef1 in pulmonary immunity we examined the lung and its leukocytes in wild-type and Arhgef1-deficient animals. Here we report that the lungs of Arhgef1(-/-) mice harbored significantly more leukocytes, increased expression and activity of matrix metalloproteinases (MMPs), airspace enlargement, and decreased lung elastance compared with wild-type lungs. Transfer of Arhgef1(-/-) lung leukocytes to wild-type mice led to airspace enlargement and impaired lung function, indicating that loss of Arhgef1 in leukocytes was sufficient to induce pulmonary pathology. Furthermore, we showed that Arhgef1-deficient peritoneal macrophages when either injected into the lungs of wild-type mice or cultured on fibronectin significantly increased expression and activity of MMPs relative to control macrophages, and the in vitro fibronectin induction was dependent on the alpha 5 beta 1 integrin pair. Together these data demonstrate that Arhgef1 regulates alpha 5 beta 1-mediated MMP expression by macrophages and that loss of Arhgef1 by leukocytes leads to pulmonary pathology. (Am J Pathol 2010,176:1157-1168; DOI: 10.2353/ajpath.2010.090200)