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NCT01639703 Clinical Trial

Hepatic Xenetix-CT Perfusion

Hepatocellular Carcinoma Clinical Trial

Official title:
Diagnostic Contribution of XENETIX® CT PERFUSION in Pre-therapeutical Assessment of Hepatocellular Carcinoma

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT01639703
Other study ID # ISO-44-013
Secondary ID
Status Completed
Phase Phase 4
First received July 6, 2012
Last updated July 11, 2017
Start date April 2012
Est. completion date October 2014

Study information
Verified date July 2017
Source Guerbet
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to prospectively determine the diagnostic value of Xenetix-CT perfusion for the discrimination between well-differentiated hepatocellular carcinomas (HCC) and poorly/moderately differentiated HCC, in histo-pathologically proven HCC, and with the aim to cover the entire liver.

Recruitment information / eligibility
Status Completed
Enrollment 96
Est. completion date October 2014
Est. primary completion date October 2014
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Subjects diagnosed for HCC and planned for surgery (lobectomy or transplantation) within a timeframe of 30 days between first imaging procedure used for the study and surgery.

Exclusion Criteria:

- Subjects who have undergone prior TACE (TransArterial Chemo Embolization), prior RFA (Radio Frequency Ablation) or prior SIRT (Selected Internal Radio Therapy) within one year before inclusion.

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
Xenetix-CT perfusion imaging
Injection of 50 ml of Xenetix

Locations
Country Name City State
Austria AKH Vienna
Germany Universitätsklinikum Erlangen Erlangen
Korea, Republic of SMC Seoul
Korea, Republic of SNUH Seoul
Switzerland Zurich University Hospital Zurich

Sponsors (1)
Lead Sponsor Collaborator
Guerbet

Countries where clinical trial is conducted

Austria,  Germany,  Korea, Republic of,  Switzerland, 

Outcome
Type Measure Description Time frame Safety issue
Primary Blood Volume (BV) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site. Within a week from CT perfusion to surgery
Primary Blood Flow (BF) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site. Within a week from CT perfusion to surgery
Primary Permeability Surface (PS) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site. Within a week from CT perfusion to surgery
Secondary Arterial Liver Perfusion (ALP) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site. Within a week from CT perfusion to surgery
Secondary Portal Venous Liver Perfusion (PVP) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site. Within a week from CT perfusion to surgery
Secondary Total Liver Perfusion (TLP) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site.
TLP = ALP + PVP		 Within a week from CT perfusion to surgery
Secondary Hepatic Perfusion Index (HPI) According to Degree of Lesions Differentiation The mean level of each CT perfusion parameter was compared between well differentiated and moderately/poorly differentiated lesions according to WHO classification evaluated off-site. Within a week from CT perfusion to surgery
Secondary Blood Volume According to Immunohistochemistry Parameter (Glutamine Synthetase) Glutamine synthetase is an immunohistochemistry parameter of hepatocellular carcinoma phenotype.
Glutamine synthetase labelling was quantified and in case of positive quantification, classified in the following categories: 1-10%, 10-50% and >50%. In case of absence of glutamine synthetase labelling, lesions were classified in the "glutamine synthetase 0%" category.		 Within a week from CT perfusion to surgery
Secondary Blood Volume According to Immunohistochemistry Parameter (CD31) CD31 is an immunohistochemistry marker of microvessel density. CD31 labelling was quantified and in case of positive quantification, classified in the following categories: 1-10%, 10-50% and >50%. In case of absence of CD31 labelling, lesions were classified in the "CD31 0%" category. Within a week from CT perfusion to surgery
Secondary Blood Flow According to Immunohistochemistry Parameter (Glutamine Synthetase) Glutamine synthetase is an immunohistochemistry parameter of hepatocellular carcinoma phenotype.
Glutamine synthetase labelling was quantified and in case of positive quantification, classified in the following categories: 1-10%, 10-50% and >50%. In case of absence of glutamine synthetase labelling, lesions were classified in the "glutamine synthetase 0%" category.		 Within a week from CT perfusion to surgery
Secondary Blood Flow According to Immunohistochemistry Parameter (CD31) CD31 is an immunohistochemistry marker of microvessel density. CD31 labelling was quantified and in case of positive quantification, classified in the following categories: 1-10%, 10-50% and >50%. In case of absence of CD31 labelling, lesions were classified in the "CD31 0%" category. Within a week from CT perfusion to surgery
Secondary Permeability Surface According to Immunohistochemistry Parameter (Glutamine Synthetase) Glutamine synthetase is an immunohistochemistry parameter of hepatocellular carcinoma phenotype.
Glutamine synthetase labelling was quantified and in case of positive quantification, classified in the following categories: 1-10%, 10-50% and >50%. In case of absence of glutamine synthetase labelling, lesions were classified in the "glutamine synthetase 0%" category.		 Within a week from CT perfusion to surgery
Secondary Permeability Surface According to Immunohistochemistry Parameter (CD31) CD31 is an immunohistochemistry marker of microvessel density. CD31 labelling was quantified and in case of positive quantification, classified in the following categories: 1-10%, 10-50% and >50%. In case of absence of CD31 labelling, lesions were classified in the "CD31 0%" category. Within a week from CT perfusion to surgery
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