1 The full therapeutic potential of the main immunosuppressive drug, cyclosporin A (CsA), is limited because of its side effects, namely nephrotoxicity and hypertension. Several lines of evidence suggest that the origin of both side effects could be CsA-induced vasoconstriction. However Cyclosporin A (CsA) is currently the main immunosuppressive drug used during transplantation and autoimmune disorders. The mechanism of its immunosuppressive effect has recently been elucidated (McKeon, 1991;Schreiber & Crabtree, 1992;Swanson et al., 1992). The formation of a tertiary complex between CsA, the rotamase cyclophilin, and the protein phosphatase, calcineurin, inhibits the activity of the latter. This leads to decreased interleukin-2 (IL-2) production by lymphocyte T cells resulting in inhibition of their activation and proliferation (Cohen et al., 1984;Kunz & Hall, 1993). However, clinical use of CsA is limited due to its nephrotoxicity and ability to induce hypertension (Kahan, 1989;Mason, 1990;Textor et al., 1994). Most studies in animals as well as in CsA-treated patients suggest that CsA-induced vasoconstriction is the underlying cause of both side effects. However, the molecular mechanism of this effect is still an object of some controversy: (1) An increased sympathetic activity has been noted both in experimental models as well as in man (Moss et al., 1985;Scherrer et al., 1990;Morgan et al., 1991;Chiu et al., 1992;Lyson et al., 1993;1994). (2) Stimulation of the renin-angiotensin system has been described in hypertensive transplant recipients under CsA treatment (Julien et al., 1993) as well as in animals (Muller-Schweinitzer, 1988 British Journal of Pharmacology (1996) 118, 885-892 A. Lo Russo et al Cyclosporins and Ca2, signalling noradrenaline and AVP-induced contraction on isolated mesenteric arteries. We have also extended our previous findings to other vasoconstrictor hormones using cultured VSMC. In addition, to determine the possible role of cyclophilin or calcineurin inhibition in CsA-induced calcium potentiation, we have investigated the effect of some derivatives of CsA devoid of immunosuppressive activity.
MethodsDiameter measurement of mesenteric arteriesMale Wistar Kyoto rats (200 to 300 g) were anaesthetized by i.p. injection of a solution of pentobarbitone (200 mg kg-' body weight) and were decapitated. Resistance arteries of ca. 200 uM diameter were prepared from the mesenteric bed using segments of the third order branch. They were cleaned of adherent tissue in ice-cold Krebs-Ringer solution (KRS: see below), mounted at both ends onto glass cannulae in a chamber (Living Systems Instrumentation, Burlington, VT, U.S.A.) filled with KRS and placed on a microscope stage. The vessels were continuously superfused with oxygenated KRS at 370C.A steady pressure of 40 mmHg was created in the vessel with a pump coupled to a feed-back pressure system. Vasoconstrictor drugs were applied via the superfusate in a low [Ca2+] KRS (see Chemicals and buffers) to avoid contractions due to calcium entry throu...
