Sm. Greenstein et al., PROLONGED USE OF CYCLOSPORINE (CSA) PRODUCES REVERSIBLE HEMODYNAMIC AND ABSORPTIVE ALTERATIONS IN THE TRANSPLANTED RAT SMALL-INTESTINE, The Journal of surgical research, 56(6), 1994, pp. 518-523
Cyclosporine (CsA)-induced alterations in organ blood flow (BF) and fu
nction have been studied in kidney and pancreatic transplants. In this
study, we assessed the effect of prolonged CsA administration on graf
t tissue BF and absorption from transplanted rat small intestine (SI).
Isogeneic SI transplantation was performed in Lewis rats. Animals wer
e grouped based upon the following treatment schedules: no treatment f
or 1 week in group 1; 0.15 ml/kg/day im olive oil for 1 week in group
2; 0.15 ml/kg/day olive oil for 1 week and then 0.1 ml/kg/day for 5 we
eks in group 3; 15 mg/ kg/day im CsA for 1 week in group 4; and 15 mg/
kg/day CsA for 1 week and then 10 mg/kg/day for 5 weeks in group 5. Gr
oup 6 was the same as group 5 but CsA was withdrawn for 1 week prior t
o assessment. Maltose absorption was measured to evaluate graft absorp
tive function. BF and its intramural distribution to mucosal and seros
al/muscularis layers were determined using the radioactive microsphere
technique. Perfusion pressure was measured to calculate vascular resi
stance (VR). One week of CsA of administration in group 4 resulted in
a significant increase in mucosal VR (68.4 +/- 15.5 versus 46.9 +/- 8.
7 U/g, P < 0.01) and significant decreases in mucosal BF (1.21 +/- 0.2
5 versus 1.80 +/- 0.38 ml/g/min, P < 0.01) and maltose absorption 30 m
in after loading (168.9 +/- 21.1 versus 214.4 +/- 28.4 glucose mg/dl,
P < 0.01). Prolonged CsA treatment up to 6 weeks in group 5 resulted i
n further increases in whole intestinal VR (88.6 +/- 19.1 versus 70.1
+/- 12.4 U/g, P ( 0.05) and decreases in whole intestinal BF (0.93 +/-
0.18 versus 1.16 +/- 0.18 ml/g/min, P < 0.05) and maltose absorption
30 min after loading (137.4 +/- 21.3 versus 168.9 +/- 21.1 glucose mg/
dl) when compared with 1 week of CsA treatment in group 4. Withdrawal
of CsA for 1 week after prolonged CsA treatment in group 6 resulted in
restorations of VR in both mucosal and serosal/muscularis layers, BF
in serosal/muscularis layer, and absorptive function to the normal ran
ges as shown in group 3 (P = NS). We concluded that CsA administration
causes hemodynamic alterations in the intestinal vascular system and
dose-dependent functional impairment which are reversible when CsA is
discontinued. (C) 1994 Academic Press, Inc.