1 This study investigates the role of tumour necrosis factor (TNF) in the induction of nitric oxide synthase (NOS) by bacterial endotoxin (lipopolysaccharide; LPS) in a rat model of endotoxin shock. 2 In anaesthetized rats, pretreatment with a monoclonal antibody for TNF (TNFab; 20 mg kg-', s.c., at 16 h prior to LPS) ameliorated the fall in mean arterial blood pressure (MAP) in response to LPS (2 mg kg-', i.v.). For instance, endotoxaemia for 180 min resulted in a fall in MAP from 114 ± 6 (control) to 84 ± 5 mmHg (P <0.01; n = 7). In contrast, animals pretreated with TNFab prior to LPS injection maintained significantly higher MAP when compared to LPS-control (MAP at 180 min; 118± 3mmHg; P<0.01, n=5). 3 Three hours of endotoxaemia was also associated with a significant reduction of the contractile effects of noradrenaline (NA) (10-'-10-6 M) on the thoracic aorta ex vivo. This hyporeactivity to NA was partially restored by in vitro treatment of the vessels with N0-nitro-L-arginine methyl ester (L-NAME, 20 min, 3 x 10-4 M). Pretreatment of rats with TNFab (20 mg kg-'; at 16 h prior to LPS) significantly (P<0.05) attenuated the LPS-induced hyporeactivity of rat aortic rings ex vivo. L-NAME did not enhance the contractions of aortic rings obtained from TNFab pretreated LPS-rats. 4 At 180min after LPS there was a significant elevation of the induced NOS activity in the lung (5.14 ± 0.57 pmol citrulline mg-' min-', n = 8). TNFab pretreatment significantly attenuated this induction of NOS in response to LPS by 37 ± 6% (n = 5; P<0.05). 5 We conclude that the formation of endogenous TNF contributes to the induction of the calciumindependent isoform of NOS in response to LPS in vivo. Thus, the beneficial effects of agents which inhibit either the release or the action of TNF in circulatory shock may be, in part, due to inhibition of NOS induction.