Liver Cancer Clinical Trial
— IDASPHERE IIOfficial title:
Chemoembolisation of Hepatocellular Carcinomas Not Subject to Interventive Care by Idarubicin-loaded Beads - IDASPHERE II
NCT number | NCT02185768 |
Other study ID # | FFCD 1307 |
Secondary ID | |
Status | Completed |
Phase | Phase 2 |
First received | |
Last updated | |
Start date | January 2015 |
Est. completion date | May 2018 |
Verified date | March 2020 |
Source | Federation Francophone de Cancerologie Digestive |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The most frequently used products in CHE are doxorubicin (36%), cisplatin (31%), and
epirubicin (12%). But until recently, there were no obvious reasons to use one product over
another. In fact, systemic chemotherapy is considered ineffective in HCC [hepatocellular
carcinoma], which does not allow any argument in favour of the product. Moreover, 2
randomised trials comparing the molecules (doxorubicin vs. epirubicin) proved to be negative
in terms of survival.
Cytotoxicity of different anticancer agents on HCC cell lines have been compared in order to
select the best candidate for CHE. Eleven chemotherapy molecules have been tested, including
those more frequently used in CHE. Among them, idarubicin (an anthracycline) proved to be the
most effective in vitro by far. The superiority of idarubicin (as opposed to doxorubicin) was
noted especially on the SNU-449 line, which is known for its resistance to several
chemotherapy agents. The best cytotoxicity of idarubicin can be explained by 2 mechanisms: 1)
idarubicin has a better intracellular penetration than the other anthracyclines. This is
probably due to its more considerable lipophily, facilitating thus its passage through the
membrane made up of a double lipid layer, 2) idarubicin is resistant to the multidrug
resistance system (MDR). The MDR mechanism, which is often noted in HCC, consists of membrane
pumps transporting the molecule outside the cell. These two particularities could explain a
more significant accumulation of idarubicin in the HCC cells, and thus better efficacy. It is
interesting to note that orally administered idarubicin (5 mg/day for 21 days) has proved to
be less toxic and is effective in HCC. Currently, idarubicin is used to treat leukaemia. Its
toxicity profile (especially, haematological and cardiac) is known.
On these grounds, A pilot study has been conducted in order to assess the tolerance and
efficacy of lipiodol-based CHE using a 10 mg dose of idarubicin in 21 patients with
unresectable HCC. These preliminary data reveal that CHE with idarubicin is effective and
less toxic.
Idarubicin can be loaded in microbeads. A phase I study (IDASPHERE) has been conducted on DC
Beads® microbeads (300-500µm) loaded with idarubicin (dose increased from 5 to 25 mg). The
DLT [dose-limiting toxicity] and MTD [maximum tolerated dose] have been determined in 21
patients using a CRM. The MTD of idarubicin was assessed at 10 mg. In our study, the
idarubicin-loaded beads did not give rise to any specific toxicity-related problem. The 10 mg
dose is compatible with the known toxicity profile of idarubicin: cumulative cardiotoxicity
of doxorubicin is noted from 550 mg/m², whereas that of idarubicin is noted from 93 mg/m².
There is thus a 5.9:1 ratio between their cumulative toxicities. The most frequently used
dose (and also the weakest one) for the doxorubicin-based CHE is 50 mg. The equivalent of the
idarubicin dose would thus be: 50 mg (doxorubicin) / 5.9 (doxorubicin/idarubicin ratio) =
approx. 10 mg of idarubicin.
It has been already demonstrated that hepatic extraction of idarubicin is better than those
of doxorubicin and daunorubicin in an animal sarcoma model. In this study, AUC 0-48h and AUC
0-72h were 1.35 times higher with idarubicin, proving that its intra-hepatic penetration was
35% higher.
The randomised phase II PRECISION V study compared conventional CHE (cCHE) with CHE by
doxorubicin beads (DC Bead®) in patients with HCC. It is currently the largest randomised
trial on CHE published. The PRECISION V data can be thus used to compare the other studies in
terms of efficacy and tolerance.
To continue our preliminary study and the phase I IDASPHERE study, investigators wish to
assess thus the efficacy and confirm the tolerance of idarubicin-loaded beads for the CHE of
HCC according to a protocol similar to PRECISION V, as part of a single-arm phase II study.
Status | Completed |
Enrollment | 46 |
Est. completion date | May 2018 |
Est. primary completion date | May 2018 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility |
Inclusion Criteria: - - Histologically diagnosed HCC or HCC diagnosed according to the EASL criteria - Measurable targets according to the mRECIST v1.1 criterion - Preserved liver function (in case of Child-Pugh A or B7 cirrhosis) - Tumour not subject to interventive care (liver transplant, surgical resection or percutaneous destruction) - BCLC A/B without portal or extra-hepatic invasion - No prior treatment by chemotherapy, radiotherapy or transarterial embolisation (with or without chemotherapy) - Age = 18 years - WHO 0 or 1 - Laboratory test: platelets = 50,000 mm3, N = 1,000/mm3, creatininaemia = 150 µmol/L, PT = 50% - No heart failure (isotope or ultrasound VEF > 50%) Exclusion Criteria: - - Advanced tumour (vascular or extra-hepatic invasion including brain metastasis or diffuse HCC with liver invasion > 50%) - History of other type of cancer except cancer known to be in remission for more than 5 years (in this case, HCC histological proof is required), or basal-cell carcinoma or in situ cervix uteri cancer properly treated with curative treatment - Advanced liver disease (Child B8, B9 and C, bilirubinaemia > 3 mg/dL, SGOT and SGPT > 5 x ULN or 250 U/L) - Previous treatment by idarubicin and/or doxorubicin - Idarubicin contraindications (cardiopathy with myocardial failure, serious kidney or liver failure, yellow fever vaccine) - Concurrent disease or uncontrolled severe clinical condition - Uncontrolled severe infection - Patient requiring long-term anticoagulant treatment - Thrombosis of the portal vein or a 3-segment region or more - Hepatofugal portal venous flow - Presence of serious atheromatosis - Presence of collateral vascular ways potentially affecting the normal regions during embolisation - Presence of arthritis of the hepatic artery branches to be treated - Presence of arterioportal or arterial subhepatic fistula that cannot be embolised by coils - Pregnancy or breastfeeding - Absence of effective contraception (for men and women of childbearing age) - Patient who cannot be regularly monitored on account of psychological, social, family- or geography-related reasons - Concomitant participation of a patient in another study |
Country | Name | City | State |
---|---|---|---|
France | CHU Amiens | Amiens | |
France | CHU d'ANGERS | Angers | |
France | CHU - Hôpital François Mitterand | Dijon | |
France | Hôpital Edouard Herriot | Lyon | |
France | Hôpital La Croix Rousse | Lyon | |
France | CHU St Eloi | Montpellier | |
France | Hôpital de l'Archet II | Nice |
Lead Sponsor | Collaborator |
---|---|
Federation Francophone de Cancerologie Digestive |
France,
Guiu B, Chevallier P, Assenat E, Barbier E, Merle P, Bouvier A, Dumortier J, Nguyen-Khac E, Gugenheim J, Rode A, Oberti F, Valette PJ, Yzet T, Chevallier O, Barbare JC, Latournerie M, Boulin M. Idarubicin-loaded Beads for Chemoembolization of Hepatocellul — View Citation
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Rate of patients in objective response (complete or partial response) | The main judgement criterion is the rate of patients in objective response (complete or partial response) at 6 months according to the mRECIST criteria and based on the central review. | up to 6 months | |
Secondary | Rate of patients in objective response (complete or partial response) and assessed according to the investigator. | The rate of patients in objective response (complete or partial response) at 6 months according to the mRECIST criteria, and assessed according to the investigator. | up to 6 months | |
Secondary | Treatment failure date | The time interval until treatment failure This is defined by the time interval between the inclusion date and the protocol Treatment failure date. Death, progression, and any protocol treatment discontinuation (regardless of the cause) are considered as treatment failure. Surviving patients not subject to treatment failure will be withdrawn on the date of the last 6-month morphological assessment. |
up to 2 years | |
Secondary | Best response | The best response according to the mRECIST criteria | up to 6 months | |
Secondary | Survival without progression | Survival without progression: This is defined by the time interval between the inclusion date and the date of the 1st progression according to the mRECIST criteria (assessed in central review) or death (regardless of the cause). The surviving patients without progression will be withdrawn on the date of the last recorded news |
up to 2 years | |
Secondary | Overall survival | Overall survival This is defined by the time interval between the inclusion date and the date of death (regardless of the cause) or the date of the last recorded news for the surviving patients. | up to 2 years | |
Secondary | Treatment tolerance | Treatment tolerance Toxicities will be assessed using the NCI-CTC criteria v4.0. They will be described according to their degree as number of toxicities and number of patients presenting toxicity. | up to 2 years |
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