Angiotensin II exacerbates lipopolysaccharide-induced contractile depression in rabbit cardiac myocytes

In sepsis, lipopolysaccharide (LPS) depresses cardiac function by inducing production of nitric oxide (NO) and its second messenger cGMP. LPS also sti mulates ANG II production. We hypothesized that ANG II modulates the cardia c response to LPS. Adult rabbit cardiac myocytes incubated with LPS (10 ng/ ml) had increased cardiac cGMP after 6 h (but not within 1 h) [527 +/- 43 v s. 316 +/- 27 (SE) fmol/mg protein in controls, n = 16 each group, P < 0.05 ]. This was associated with depressed cell shortening with no alterations i n Ca2+ transients (indo 1 fluorescence), indicating a decreased myofilament responsiveness to Ca2+. ANG II (100 nM) alone had no effect. However, ANG II with LPS produced higher cGMP levels (1,025 +/- 113 fmol/mg protein, n = 16, P < 0.05 vs. LPS alone), more severe contractile depression, impaired Ca2+ handling, and decreased mitochondrial activity (MTS assay). We conclud e that ANG II and LPS have synergistic effects on the activation of NO-cGMP pathways to induce dose-dependent impairments in excitation-contraction co upling in cardiac myocytes.