Intra-arterial idarubicin_lipiodol without embolisation in hepatocellular carcinoma: The LIDA-B phase I trial

[Display omitted] •The maximum-tolerated dose (MTD) of idarubicin was 20 mg after two chemolipiodolisation sessions.•Intra-arterial idarubicin_lipiodol was well tolerated.•Intra-arterial idarubicin_lipiodol showed encouraging responses and survival.•Health-related quality of life results confirmed t...

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Published inJournal of hepatology Vol. 68; no. 6; pp. 1163 - 1171
Main Authors Guiu, Boris, Jouve, Jean-Louis, Schmitt, Antonin, Minello, Anne, Bonnetain, Franck, Cassinotto, Christophe, Piron, Lauranne, Cercueil, Jean-Pierre, Loffroy, Romaric, Latournerie, Marianne, Wendremaire, Maëva, Lepage, Côme, Boulin, Mathieu
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier B.V 01.06.2018
Elsevier Science Ltd
Subjects
Chemolipiodolisation
Clinical trials
Cytotoxicity
Drug therapy
Embolisms
Hepatocellular carcinoma
Idarubicin
Intravenous administration
Liver cancer
Pain
Patients
Pharmacokinetics
Phase I
Quality of life
Safety
Solid tumors
Chemolipiodolisation
Hepatocellular carcinoma
Idarubicin
Phase I
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Abstract [Display omitted] •The maximum-tolerated dose (MTD) of idarubicin was 20 mg after two chemolipiodolisation sessions.•Intra-arterial idarubicin_lipiodol was well tolerated.•Intra-arterial idarubicin_lipiodol showed encouraging responses and survival.•Health-related quality of life results confirmed the good safety results. Idarubicin shows high cytotoxicity against hepatocellular carcinoma (HCC) cells, a high hepatic extraction ratio, and high lipophilicity leading to stable emulsions with lipiodol. A dose-escalation phase I trial of idarubicin_lipiodol (without embolisation) was conducted in patients with cirrhotic HCC to estimate the maximum-tolerated dose (MTD) and to assess the safety, efficacy, and pharmacokinetics of the drug, and the health-related quality of life achieved by patients. Patients underwent two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation. The idarubicin dose was escalated according to a modified continuous reassessment method. The MTD was defined as the dose closest to that causing dose-limiting toxicity (DLT) in 20% of patients. A group of 15 patients were enrolled, including one patient at 10 mg, four patients at 15 mg, seven patients at 20 mg, and three patients at 25 mg. Only two patients experienced DLT: oedematous ascitic decompensation and abdominal pain at 20 and 25 mg, respectively. The calculated MTD of idarubicin was 20 mg. The most frequent grade ≥3 adverse events were biological. One month after the second session, the objective response rate was 29% (complete response, 0%; partial response, 29%) based on modified Response Evaluation Criteria In Solid Tumours. The median time to progression was 5.4 months [95% confidence limit (CI) 3.0–14.6 months] and median overall survival was 20.6 months (95% CI 5.7–28.7 months). Pharmacokinetic analysis of idarubicin showed that the mean Cmax of idarubicin after intra-arterial injection of the idarubicin-lipiodol emulsion is approximately half the Cmax after intravenous administration. Health-related quality of life results confirmed the good safety results associated with use of the drug. The MTD of idarubicin was 20 mg after two chemolipiodolisation sessions. Encouraging safety results, and patient responses and survival were observed. A phase II trial has been scheduled. There is a need for transarterial regimens that improve the responses and survival of patients with unresectable HCC. In this phase I trial, we showed that two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation was well tolerated and gave promising efficacy in terms of tumour control and patient survival.
AbstractList Background & Aims Idarubicin shows high cytotoxicity against hepatocellular carcinoma (HCC) cells, a high hepatic extraction ratio, and high lipophilicity leading to stable emulsions with lipiodol. A dose-escalation phase I trial of idarubicin_lipiodol (without embolisation) was conducted in patients with cirrhotic HCC to estimate the maximum-tolerated dose (MTD) and to assess the safety, efficacy, and pharmacokinetics of the drug, and the health-related quality of life achieved by patients. Methods Patients underwent two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation. The idarubicin dose was escalated according to a modified continuous reassessment method. The MTD was defined as the dose closest to that causing dose-limiting toxicity (DLT) in 20% of patients. Results A group of 15 patients were enrolled, including one patient at 10 mg, four patients at 15 mg, seven patients at 20 mg, and three patients at 25 mg. Only two patients experienced DLT: oedematous ascitic decompensation and abdominal pain at 20 and 25 mg, respectively. The calculated MTD of idarubicin was 20 mg. The most frequent grade ≥3 adverse events were biological. One month after the second session, the objective response rate was 29% (complete response, 0%; partial response, 29%) based on modified Response Evaluation Criteria In Solid Tumours. The median time to progression was 5.4 months [95% confidence limit (CI) 3.0–14.6 months] and median overall survival was 20.6 months (95% CI 5.7–28.7 months). Pharmacokinetic analysis of idarubicin showed that the mean Cmax of idarubicin after intra-arterial injection of the idarubicin-lipiodol emulsion is approximately half the Cmax after intravenous administration. Health-related quality of life results confirmed the good safety results associated with use of the drug. Conclusions The MTD of idarubicin was 20 mg after two chemolipiodolisation sessions. Encouraging safety results, and patient responses and survival were observed. A phase II trial has been scheduled. Lay summary There is a need for transarterial regimens that improve the responses and survival of patients with unresectable HCC. In this phase I trial, we showed that two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation was well tolerated and gave promising efficacy in terms of tumour control and patient survival.
Idarubicin shows high cytotoxicity against hepatocellular carcinoma (HCC) cells, a high hepatic extraction ratio, and high lipophilicity leading to stable emulsions with lipiodol. A dose-escalation phase I trial of idarubicin_lipiodol (without embolisation) was conducted in patients with cirrhotic HCC to estimate the maximum-tolerated dose (MTD) and to assess the safety, efficacy, and pharmacokinetics of the drug, and the health-related quality of life achieved by patients. Patients underwent two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation. The idarubicin dose was escalated according to a modified continuous reassessment method. The MTD was defined as the dose closest to that causing dose-limiting toxicity (DLT) in 20% of patients. A group of 15 patients were enrolled, including one patient at 10 mg, four patients at 15 mg, seven patients at 20 mg, and three patients at 25 mg. Only two patients experienced DLT: oedematous ascitic decompensation and abdominal pain at 20 and 25 mg, respectively. The calculated MTD of idarubicin was 20 mg. The most frequent grade ≥3 adverse events were biological. One month after the second session, the objective response rate was 29% (complete response, 0%; partial response, 29%) based on modified Response Evaluation Criteria In Solid Tumours. The median time to progression was 5.4 months [95% confidence limit (CI) 3.0-14.6 months] and median overall survival was 20.6 months (95% CI 5.7-28.7 months). Pharmacokinetic analysis of idarubicin showed that the mean C of idarubicin after intra-arterial injection of the idarubicin-lipiodol emulsion is approximately half the C after intravenous administration. Health-related quality of life results confirmed the good safety results associated with use of the drug. The MTD of idarubicin was 20 mg after two chemolipiodolisation sessions. Encouraging safety results, and patient responses and survival were observed. A phase II trial has been scheduled. There is a need for transarterial regimens that improve the responses and survival of patients with unresectable HCC. In this phase I trial, we showed that two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation was well tolerated and gave promising efficacy in terms of tumour control and patient survival.
[Display omitted] •The maximum-tolerated dose (MTD) of idarubicin was 20 mg after two chemolipiodolisation sessions.•Intra-arterial idarubicin_lipiodol was well tolerated.•Intra-arterial idarubicin_lipiodol showed encouraging responses and survival.•Health-related quality of life results confirmed the good safety results. Idarubicin shows high cytotoxicity against hepatocellular carcinoma (HCC) cells, a high hepatic extraction ratio, and high lipophilicity leading to stable emulsions with lipiodol. A dose-escalation phase I trial of idarubicin_lipiodol (without embolisation) was conducted in patients with cirrhotic HCC to estimate the maximum-tolerated dose (MTD) and to assess the safety, efficacy, and pharmacokinetics of the drug, and the health-related quality of life achieved by patients. Patients underwent two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation. The idarubicin dose was escalated according to a modified continuous reassessment method. The MTD was defined as the dose closest to that causing dose-limiting toxicity (DLT) in 20% of patients. A group of 15 patients were enrolled, including one patient at 10 mg, four patients at 15 mg, seven patients at 20 mg, and three patients at 25 mg. Only two patients experienced DLT: oedematous ascitic decompensation and abdominal pain at 20 and 25 mg, respectively. The calculated MTD of idarubicin was 20 mg. The most frequent grade ≥3 adverse events were biological. One month after the second session, the objective response rate was 29% (complete response, 0%; partial response, 29%) based on modified Response Evaluation Criteria In Solid Tumours. The median time to progression was 5.4 months [95% confidence limit (CI) 3.0–14.6 months] and median overall survival was 20.6 months (95% CI 5.7–28.7 months). Pharmacokinetic analysis of idarubicin showed that the mean Cmax of idarubicin after intra-arterial injection of the idarubicin-lipiodol emulsion is approximately half the Cmax after intravenous administration. Health-related quality of life results confirmed the good safety results associated with use of the drug. The MTD of idarubicin was 20 mg after two chemolipiodolisation sessions. Encouraging safety results, and patient responses and survival were observed. A phase II trial has been scheduled. There is a need for transarterial regimens that improve the responses and survival of patients with unresectable HCC. In this phase I trial, we showed that two sessions of treatment with a transarterial idarubicin_lipiodol emulsion without embolisation was well tolerated and gave promising efficacy in terms of tumour control and patient survival.
Author Piron, Lauranne
Lepage, Côme
Latournerie, Marianne
Loffroy, Romaric
Schmitt, Antonin
Cercueil, Jean-Pierre
Wendremaire, Maëva
Jouve, Jean-Louis
Minello, Anne
Boulin, Mathieu
Guiu, Boris
Cassinotto, Christophe
Bonnetain, Franck
Author_xml – sequence: 1
  givenname: Boris
  surname: Guiu
  fullname: Guiu, Boris
  email: b-guiu@chu-montpellier.fr
  organization: Department of Interventional Radiology, INSERM U1194, St-Eloi University Hospital, Montpellier School of Medicine, 80 Avenue Augustin Fliche, 34295 Montpellier, France
– sequence: 2
  givenname: Jean-Louis
  surname: Jouve
  fullname: Jouve, Jean-Louis
  organization: Department of Hepatogastroenterology, Dijon University Hospital and EPICAD LNC-UMR1231, Burgundy & Franche Comté University, BP 87900, 21079 Dijon, France
– sequence: 3
  givenname: Antonin
  orcidid: 0000-0002-3132-7730
  surname: Schmitt
  fullname: Schmitt, Antonin
  organization: Department of Pharmacy, Georges-François Leclerc Anticancer Centre and LNC-UMR1231, Burgundy & Franche Comté University, BP 87900, 21079 Dijon, France
– sequence: 4
  givenname: Anne
  surname: Minello
  fullname: Minello, Anne
  organization: Department of Hepatogastroenterology, Dijon University Hospital and EPICAD LNC-UMR1231, Burgundy & Franche Comté University, BP 87900, 21079 Dijon, France
– sequence: 5
  givenname: Franck
  surname: Bonnetain
  fullname: Bonnetain, Franck
  organization: Methodology and Quality of Life in Oncology Unit (EA 3181) and Quality of Life and Cancer Clinical Research Platform, University Hospital Besançon, 2 Place Saint Jacques, 25000 Besançon, France
– sequence: 6
  givenname: Christophe
  surname: Cassinotto
  fullname: Cassinotto, Christophe
  organization: Department of Interventional Radiology, INSERM U1194, St-Eloi University Hospital, Montpellier School of Medicine, 80 Avenue Augustin Fliche, 34295 Montpellier, France
– sequence: 7
  givenname: Lauranne
  surname: Piron
  fullname: Piron, Lauranne
  organization: Department of Interventional Radiology, INSERM U1194, St-Eloi University Hospital, Montpellier School of Medicine, 80 Avenue Augustin Fliche, 34295 Montpellier, France
– sequence: 8
  givenname: Jean-Pierre
  surname: Cercueil
  fullname: Cercueil, Jean-Pierre
  organization: Department of Interventional Radiology, University Hospital, 14 rue Gaffarel, 21000 Dijon, France
– sequence: 9
  givenname: Romaric
  surname: Loffroy
  fullname: Loffroy, Romaric
  organization: Department of Interventional Radiology, University Hospital, 14 rue Gaffarel, 21000 Dijon, France
– sequence: 10
  givenname: Marianne
  surname: Latournerie
  fullname: Latournerie, Marianne
  organization: Department of Hepatogastroenterology, Dijon University Hospital and EPICAD LNC-UMR1231, Burgundy & Franche Comté University, BP 87900, 21079 Dijon, France
– sequence: 11
  givenname: Maëva
  surname: Wendremaire
  fullname: Wendremaire, Maëva
  organization: Department of Pharmacology-Toxicology, University Hospital, 2 rue Angélique Ducoudray, 21000 Dijon, France
– sequence: 12
  givenname: Côme
  surname: Lepage
  fullname: Lepage, Côme
  organization: Department of Hepatogastroenterology, Dijon University Hospital and EPICAD LNC-UMR1231, Burgundy & Franche Comté University, BP 87900, 21079 Dijon, France
– sequence: 13
  givenname: Mathieu
  surname: Boulin
  fullname: Boulin, Mathieu
  organization: Department of Pharmacy, Dijon University Hospital and EPICAD LNC-UMR1231, Burgundy & Franche Comté University, BP 87900, 21079 Dijon, France
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Keywords Chemolipiodolisation
Hepatocellular carcinoma
Idarubicin
Phase I
Language English
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Snippet [Display omitted] •The maximum-tolerated dose (MTD) of idarubicin was 20 mg after two chemolipiodolisation sessions.•Intra-arterial idarubicin_lipiodol was...
Idarubicin shows high cytotoxicity against hepatocellular carcinoma (HCC) cells, a high hepatic extraction ratio, and high lipophilicity leading to stable...
Background & Aims Idarubicin shows high cytotoxicity against hepatocellular carcinoma (HCC) cells, a high hepatic extraction ratio, and high lipophilicity...
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SubjectTerms Chemolipiodolisation
Clinical trials
Cytotoxicity
Drug therapy
Embolisms
Hepatocellular carcinoma
Idarubicin
Intravenous administration
Liver cancer
Pain
Patients
Pharmacokinetics
Phase I
Quality of life
Safety
Solid tumors
Title Intra-arterial idarubicin_lipiodol without embolisation in hepatocellular carcinoma: The LIDA-B phase I trial
URI https://dx.doi.org/10.1016/j.jhep.2018.01.022
https://www.ncbi.nlm.nih.gov/pubmed/29427728
https://www.proquest.com/docview/2083800257
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