Hepatic vein transit time of SonoVue: a comparative study with Levovist

Adrian K P Lim; Nayna Patel; Robert J Eckersley; Robert D Goldin; Howard C Thomas; David O Cosgrove; Simon D Taylor-Robinson; Martin J K Blomley

doi:10.1148/radiol.2401041517

Hepatic vein transit time of SonoVue: a comparative study with Levovist

Radiology. 2006 Jul;240(1):130-5. doi: 10.1148/radiol.2401041517. Epub 2006 May 23.

Authors

Adrian K P Lim¹, Nayna Patel, Robert J Eckersley, Robert D Goldin, Howard C Thomas, David O Cosgrove, Simon D Taylor-Robinson, Martin J K Blomley

Affiliation

¹ Imaging Sciences Department, Medical Research Council Clinical Sciences Centre, Faculty of Medicine, Imperial College London, Hammersmith Hospital, Du Cane Rd, London W12 0HS, England. a.lim@imperial.ac.uk

PMID: 16720867
DOI: 10.1148/radiol.2401041517

Abstract

Purpose: To prospectively compare transit times of Levovist and SonoVue in healthy volunteers and patients with biopsy-proved hepatitis C-related liver disease.

Materials and methods: Institutional review board approval and informed consent were obtained. Forty patients and 25 healthy volunteers were examined. Subjects fasted, a bolus of SonoVue (0.6 mL) was injected into a cubital fossa vein, and hepatic venous time-intensity profiles were measured with spectral Doppler tracing. This was repeated with two injections of Levovist (2 g) and another injection of SonoVue. Time-intensity curves of spectral Doppler signals of right and middle hepatic veins were analyzed. A sustained signal intensity increase of 10% above baseline levels indicated hepatic vein transit time (HVTT). Carotid artery audio intensity was measured in volunteers. Analysis of variance and t tests were used for statistical analysis.

Results: Twelve patients had mild hepatitis; 18, moderate or severe hepatitis; and 10, cirrhosis. Mean HVTTs in control, mild hepatitis, moderate or severe hepatitis, and cirrhosis groups were 38.3 seconds +/- 2.4 (standard error), 47.5 seconds +/- 6.5, 29.5 seconds +/- 10.8, and 17.6 seconds +/- 5.0, respectively, with Levovist (P < .001) and 29.4 seconds +/- 6.9, 27.4 seconds +/- 9.3, 22.9 seconds +/- 4.7, and 16.4 seconds +/- 4.9, respectively, with SonoVue (P < .001). HVTT decreased as severity increased at imaging with both contrast agents. There was no significant difference in HVTT between mild and moderate hepatitis groups with SonoVue; however, there were significant differences in HVTT between all patient groups with Levovist. HVTT of SonoVue was shorter than that of Levovist in all groups (P < .001) except the cirrhosis group; in this group, HVTT of the two contrast agents was similar (P = .05). No difference was observed in mean cardiopulmonary transit time for SonoVue or Levovist (9.1 seconds +/- 2.4 [standard error] and 8.4 seconds +/- 2.5, respectively, P = .18).

Conclusion: HVTT was significantly shorter with SonoVue than with Levovist; there was no significant difference in cardiopulmonary transit time.

RSNA, 2006

Publication types

Comparative Study
Research Support, Non-U.S. Gov't

MeSH terms

Contrast Media / pharmacokinetics*
Female
Hepatic Veins / diagnostic imaging*
Hepatitis C / classification
Hepatitis C / diagnostic imaging*
Humans
Male
Microbubbles
Middle Aged
Phospholipids / pharmacokinetics*
Polysaccharides / pharmacokinetics*
Reference Values
Sulfur Hexafluoride / pharmacokinetics*
Ultrasonography, Doppler

Substances

Contrast Media
Phospholipids
Polysaccharides
contrast agent BR1
SHU 508
Sulfur Hexafluoride