Liver Cirrhosis Clinical Trial
Official title:
Phase 1 Study of Intrahepatic Reinfusion of Highly Purified CD133+ Stem Cells in Patients With End-Stage Liver Disease
OBJECTIVE(S): Primary:
To assess the safety of the intrahepatic reinfusion of increasing numbers of autologous
highly purified CD133+ stem cells (SCs) to patients with end-stage liver disease. Safety
will be evaluated as the incidence of adverse event (graded according to WHO) and clinically
significant abnormal laboratory value following reinfusion of SCs.
Secondary:
To assess the feasibility of the immunomagnetic selection of autologous CD133+ cells
collected with leukapheresis from the peripheral blood (PB) of patients with end-stage liver
disease, previously mobilized with G-CSF. To assess the effects of the intrahepatic
reinfusion of highly purified CD133+ cells on residual hepatic function of the patients.
STUDY DESIGN:
Twelve patients will be enrolled. At first, G-CSF at 7.5µg/Kg/b.i.d. will be administered
subcutaneously (sc) from day 1 until the completion of peripheral blood stem cells (PBSC)
collection. Harvest of bone marrow (BM)-derived PBSC will begin on day + 4 only if the
concentration of CD133+ cells is > 8/uL and will be continued until the collection of the
target cell dose: 0.5 x 106 CD133+ cells/Kg for the first 2 cohorts of patients; 1 x 106
CD133+ cells/Kg for cohort 3 and 2 x 106 CD133+ cells/Kg for cohort 4 (see below for
definitions). PB mononuclear cells obtained from mobilized standard-volume leukapheresis
will be incubated with Macs colloidal superparamagnetic CD133 microbeads and CliniMacs
device will be used for the positive selection of CD133+ cells under good manufacturing
practice (GMP) conditions. Cryopreservation and storage in liquid nitrogen will be performed
according to standard procedures. At least 4 weeks after SC mobilization and collection, up
to 40 mL of single cell suspension of highly purified autologous CD133+ cells, obtained
after rapid thawing, will be infused through the hepatic artery by transfemoral or
transbrachial arteriography. Infusion time will be lower than 15ml/min to avoid thrombi
formation. The entire procedure will be performed under anesthesiological control. According
to modified Fibonacci's increment rule, highly purified G-CSF-mobilized CD133+ cells will be
administered to patients starting from 5x104/Kg patient's body weight and increased every 3
patients. The maximum infused cell dose will be 1x106/kg. G-CSF at 5µg/Kg/day will be
administered sc for 3 days after the reinfusion of SCs (day 0 to day +2).
TITLE: Phase I study of intrahepatic reinfusion of highly purified CD133+ stem cells in
patients with end-stage liver disease.
PRINCIPAL INVESTIGATOR: Roberto M. Lemoli, MD CO-INVESTIGATORS: Pietro Andreone, MD,
Francesca Bonifazi, MD; Lucia Catani, BS; Antonia D'Errico, MD; Michelangelo Fiorentino, MD;
Valeria Giudice, MD; Annagiulia Gramenzi, MD; Elisabetta Loggi, BS; Stefania Lorenzini, MD;
Francesco Losinno, MD; Maria Rosa Motta, BS; Simonetta Rizzi, BS; Cristina Rossi, MD.
STUDY CENTER: Azienda Ospedaliero-Universitaria di Bologna, Policlinico S.Orsola-Malpighi,
Bologna - Italia, Unità Operativa di Ematologia in collaboration with:
Unità Operativa di Semeiotica Medica Unità Operativa di Anatomia e Istologia Patologica
Unità Operativa di Immunoematologia e Trasfusionale Unità Operativa di Radiologia
CLINICAL PHASE: Phase I
OBJECTIVE(S): Primary:
To assess the safety of the intrahepatic reinfusion of increasing numbers of autologous
highly purified CD133+ stem cells (SCs) to patients with end-stage liver disease. CD133+ SCs
will be previously collected and cryopreserved after mobilization with granulocyte-colony
stimulating factor (G-CSF) and leukapheresis. Safety will be evaluated as the incidence of
adverse event (graded according to WHO) and clinically significant abnormal laboratory value
following reinfusion of SCs.
Secondary:
To assess the feasibility of the immunomagnetic selection of autologous CD133+ cells
collected with leukapheresis from the peripheral blood (PB) of patients with end-stage liver
disease, previously mobilized with G-CSF.
To assess the effects of the intrahepatic reinfusion of highly purified CD133+ cells on
residual hepatic function of the patients. In particular, the following values will be
monitored: synthesis of proteins (albumin), synthesis of factors of the coagulation
(prothrombin time, INR, fibrinogen, antithrombin III, thromboplastin time), bilirubinemia,
proliferative activity, biosynthetic capacity (cholesterol, pseudocholinesterase).
To assess the effects of the treatment on the production of selected cytokines during the
administration of G-CSF and after the intrahepatic reinfusion of highly purified CD133+ SCs
to patients with end-stage liver disease.
STUDY DESIGN:
Twelve patients will be enrolled within 18-24 months in the dose-finding phase. The study
has been designed as follows: at first, G-CSF (Lenograstim, Aventis Pharma or Filgrastim,
Amgen) at 7.5µg/Kg/b.i.d. will be administered subcutaneously (sc) from day 1 until the
completion of peripheral blood stem cells (PBSC) collection. Harvest of bone marrow
(BM)-derived PBSC will begin on day + 4 only if the concentration of CD133+ cells is > 8/uL
and will be continued until the collection of the target cell dose: 0.5 x 106 CD133+
cells/Kg for the first 2 cohorts of patients; 1 x 106 CD133+ cells/Kg for cohort 3 and 2 x
106 CD133+ cells/Kg for cohort 4 (see below for definitions). PB mononuclear cells obtained
from mobilized standard-volume leukapheresis will be incubated with Macs colloidal
superparamagnetic CD133 microbeads (Miltenyi Biotec, Bergisch Gladbach, Germany) and
CliniMacs device will be used for the positive selection of CD133+ cells under good
manufacturing practice (GMP) conditions (see attachments). Cryopreservation and storage in
liquid nitrogen will be performed according to standard procedures (see attachments).
At least 4 weeks after SC mobilization and collection, up to 40 mL of single cell suspension
of highly purified autologous CD133+ cells, obtained after rapid thawing, will be infused
through the hepatic artery by transfemoral or transbrachial arteriography. Infusion time
will be lower than 15ml/min to avoid thrombi formation. The entire procedure will be
performed under anesthesiological control. The intrahepatic route of administration is
deemed necessary to avoid the potential massive spleen trapping of CD133+ cells after
conventional intravenous reinfusion in cirrhotic patients. Within 24 hours from the
procedure, a doppler ultrasonography of the celiac trunk will be performed to exclude
thrombotic events of the mesenteric district.
According to modified Fibonacci's increment rule, highly purified G-CSF-mobilized CD133+
cells will be administered to patients starting from 5x104/Kg patient's body weight and
increased every 3 patients. The maximum infused cell dose will be 1x106/kg (see below).
Lenograstim or Filgrastim at 5µg/Kg/day will be administered sc for 3 days after the
reinfusion of SCs (day 0 to day +2) for their expansion and to induce a selective
proliferative advantage of reinfused cells in vivo.
NUMBER OF PATIENTS AND TIME FRAME: Twelve patients will be enrolled within 18-24 months in
the dose-finding phase.
DIAGNOSIS AND INCLUSION CRITERIA: Signed informed consent. Age >18. Karnofsky score > 70% or
WHO <1. Adequate renal (serum creatinine < 2 mg/dl) and pulmonary (Sat O2 > 96%) function.
Diagnosis of advanced, end-stage liver disease defined by a Mayo Model for End Stage Liver
Disease (MELD) score between 17 and 25.
Patients with the following liver disease etiologies will be enrolled in the study: chronic
viral hepatitis B, chronic viral hepatitis C, chronic viral hepatitis D, alcoholic
cirrhosis, primary sclerosing cholangitis, primary biliary cirrhosis, Wilson's disease,
genetic haemochromatosis or iron over-load cirrhosis, cirrhosis due to non alcoholic
steato-hepatitis. Patients with alcoholic liver cirrhosis should have withdrawn alcohol
active consumption to be enrolled in the study.
Eligibility for orthotopic liver transplantation (OLT) is not a contraindication to enter in
the clinical study. Patients in waiting list for OLT transplantation will not be withdrawn
and will be transplanted as soon as a suitable donor will become available. Their MELD score
will remain that recorded prior SCs infusion in case of improvement following the
experimental procedure.
The presence of cirrhosis related symptoms, like ascites, peripheral edema, recurrent
gastrointestinal tract bleeding, recurrent encephalopathy do not represent major
contraindications to be enrolled into the study. The patients may be considered eligible
when clinically stable.
EXCLUSION CRITERIA: HIV positivity. Pregnant or nursing females. Current uncontrolled
infection. Intercurrent organ damage. Diagnosis of hepatocarcinoma. Complete portal
thrombosis. Severe impairment of coagulative function (PT< 30%, INR>2.5, Platelets <
40x109/L) that would contraindicate artheriography. Grade IV splenomegaly.
Budd-Chiari Syndrome with sovrahepatic vein thrombosis and cirrhosis of unknown origin will
not be included in the study.
;
Endpoint Classification: Safety Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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