SAFETY AND FEASIBILITY OF RENAL BLOOD-FLOW DETERMINATION DURING KIDNEY-TRANSPLANT SURGERY WITH PERFUSION ULTRASONOGRAPHY

Authors
ARONSON S THISTLETHWAITE RJ WALKER R FEINSTEIN SB ROIZEN MF
Citation
S. Aronson et al., SAFETY AND FEASIBILITY OF RENAL BLOOD-FLOW DETERMINATION DURING KIDNEY-TRANSPLANT SURGERY WITH PERFUSION ULTRASONOGRAPHY, Anesthesia and analgesia, 80(2), 1995, pp. 353-359
Citations number
29
Categorie Soggetti
Anesthesiology
Journal title
Anesthesia and analgesiaACNP
ISSN journal
00032999
Volume
80
Issue
2
Year of publication
1995
Pages
353 - 359
Database
ISI
SICI code
0003-2999(1995)80:2<353:SAFORB>2.0.ZU;2-Y
Abstract
Contrast-enhanced perfusion patterns of newly transplanted kidneys wer e determined in 10 patients. Albumin-stabilized sonicated microspheres were injected into the iliac-renal artery of the transplanted kidney while continuous two-dimensional ultrasound images were recorded. Dopp ler derived resistance index (RI) of the transplanted kidney's blood f low before injection of contrast (0.68 +/- 0.8) did not differ signifi cantly from RI measured immediately after injection (0.72 +/- 0.13) or RI 24 h after surgery (0.69 +/- 0.11), Heart rate, mean arterial pres sure, central venous pressure, and electrocardiogram (ECG) signs for i schemia did not change during contrast injections. Renal scintigraphy and renal biopsy revealed acute tubular necrosis and/or rejection in t wo patients at 24-48 h. Videodensitometry was used to assess the ratio of inner to outer peak pixel intensity from the recorded tomographic images in six patients. In both patients with acute rejection, the inn er to outer cortex peak pixel intensity was greater than 1, whereas it was less than 1 in the remaining four patients with normal postoperat ive renal function. Visual scores (0-3) of contrast enhancement for th ree doses of Albunex(R) were evaluated (0.5 mL, 1.0 mL, 2.0 mL). Two m illiliters always enabled perfusion assessment. In seven patients the identical dose of Albunex(R) was injected immediately before and 30 s after 2 mg of verapamil was injected directly into the renal artery at the time of surgery. The contrast enhancement score before verapamil (1.4 +/- 0.6) was significantly less than the enhancement score af ter (2.1 +/- 0.6), implying greater renal blood flow after verapamil. Eva luation of renal blood flow during kidney transplant surgery using con trast ultrasonography with sonicated albumin microspheres is feasible. Further applications for assessing regional renal blood flow changes during surgery (nontransplant) may be possible.