The severe inflammation observed during sepsis is thought to cause diaphragm dysfunction, which is associated with poor patient prognosis. Cerium oxide (CeO<
sub>
2<
/sub>
) nanoparticles have been posited to exhibit anti-inflammatory and antioxidative activities suggesting that these particles may be of potential use for the treatment of inflammatory disorders. To investigate this possibility, Sprague Dawley rats were randomly assigned to the following groups: sham control, CeO<
sub>
2<
/sub>
nanoparticle treatment only (0.5 mg/kg iv), sepsis, and sepsis+CeO2 nanoparticles. Sepsis was induced by the introduction of cecal material (600 mg/kg) directly into the peritoneal cavity. Nanoparticle treatment decreased sepsis-associated impairments in diaphragmatic contractile (P<
sub>
o<
/sub>
) function (sham: 25.6 � 1.6 N/ cm<
sup>
2<
/sup>
vs CeO<
sub>
2<
/sub>
: 23.4 � 0.8 N/ cm<
sup>
2<
/sup>
, vs Sep: 15.9 � 1.0 N/ cm<
sup>
2<
/sup>
vs Sep+CeO<
sub>
2<
/sub>
: 20.0 � 1.0 N/ cm<
sup>
2<
/sup>
, P<
0.05). These improvements in diaphragm contractile function were accompanied by a normalization of protein translation signaling (Akt, FOXO-1, and 4EBP1), diminished proteolysis (caspase 8 and ubiquitin levels), and decreased inflammatory signaling (Stat3 and iNOS). Histological analysis suggested that nanoparticle treatment was associated with diminished sarcolemma damage and diminished inflammatory cell infiltration. These data indicate CeO<
sub>
2<
/sub>
nanoparticles may improve diaphragmatic function in the septic laboratory rat.