ONEmreg12: The ONE Study M Reg Trial

Sponsor

University of Regensburg (Other)

Overall Status

Terminated

CT.gov ID

NCT02085629

Collaborator

(none)

Enrollment

Location

Arm

52.3

Actual Duration (Months)

0.2

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

To collect evidence of the safety of administering donor-derived regulatory macrophage (M reg) preparations to living-donor renal transplant recipients in the context of an international European Union funded consortium aimed at evaluating cellular immunotherapy in solid organ transplantation (The ONE Study). It is anticipated that immune regulation induced by M reg therapy can eventually be used to reduce the need for conventional immunosuppression in transplant recipients.

Condition or Disease	Intervention/Treatment	Phase
Renal Failure, End Stage	Biological: Donor M reg (Mreg_UKR)	Phase 1/Phase 2

Detailed Description

Decades of immunosuppressive drug development has produced an array of powerful pharmacological agents, but the various drawbacks associated with these treatments leaves considerable room for improvement. By harnessing the power of suppressive mechanisms in the human immune system, regulatory cell therapy may be able to support peripheral tolerance and induce a level of donor-specific unresponsiveness that allows for a reduction in the use of conventional immunosuppression in organ transplant recipients. Several alternative regulatory cell types have been identified as potential adjunct immunotherapies for solid organ transplantation and are now approaching a stage of development that would allow clinical testing in an early-stage trial. The EU-funded international ONE Study consortium aims to answer the question as to whether M reg treatment, or other immunoregulatory cell-based therapies, can be advanced in the clinical management of solid organ transplant recipients.

This particular M reg trial aims to explore the potential of M reg therapy as an adjunct immunosuppressive treatment in living-donor renal transplant recipients through a clinical protocol design shared by other investigators in The ONE Study group testing additional regulatory cell therapies in separate trials.

Study Design

Study Type:

Interventional

Actual Enrollment :

8 participants

Allocation:

N/A

Intervention Model:

Single Group Assignment

Masking:

None (Open Label)

Primary Purpose:

Treatment

Official Title:

The ONE Study: A Unified Approach to Evaluating Cellular Immunotherapy in Solid Organ Transplantation - M Reg Trial

Actual Study Start Date :

Jul 24, 2014

Actual Primary Completion Date :

Dec 3, 2018

Actual Study Completion Date :

Dec 3, 2018

Arms and Interventions

Arm	Intervention/Treatment
Experimental: M reg treatment Donor M reg (2.5-7.5 million cells/kg) IV infused (6-7d before Tx) into recipients of a LD renal Tx. Recipients also receive prednisolone, mycophenolate mofetil and tacrolimus, as detailed below: Prednisolone D 0: 500 mg IV D 1: 125 mg IV D 2 - 14: 20.0 mg/d (oral) Wk 3 - 4: 15.0 mg/d Wk 5 - 8: 10.0 mg/d Wk 9 - 12: 5.0 mg/d Wk 13 - 14: 2.5 mg/d Wk 15 - End: Cessation MMF (or biologic equiv.) D -7 to -2: 500 mg/d (250mg 2x/d) D -1 to 14: 2000 mg/d Wk 3 - 36: 1000 mg/d Wk 37 - 40: 750 mg/d Wk 41 - 44: 500 mg/d Wk 45 - 48: 250 mg/d Wk 49 - End: Cessation NOTE: MMF tapering will only happen if a 36-Wk biopsy shows no signs of subclinical rejection or if there is no evidence of declining renal function or if the clinician has any other concern about dose reduction. Tacrolimus (or biologic equiv.) ≤ 48 h pre-Tx to D 14: 3-12 ng/ml Wk 3 - 12: 3-10 ng/ml Wk 13 - 36: 3-8 ng/ml Wk 37 - End: 3-6 ng/ml	Biological: Donor M reg (Mreg_UKR) Experimental: M reg treatment Donor M reg (2.5-7.5 million cells/kg) IV infused (6-7d before Tx) into recipients of a living donor renal Tx. Recipients also receive prednisolone, mycophenolate mofetil and tacrolimus background immunosuppression (as described in detail in the arm description).

Arm

Intervention/Treatment

Experimental: M reg treatment

Donor M reg (2.5-7.5 million cells/kg) IV infused (6-7d before Tx) into recipients of a LD renal Tx. Recipients also receive prednisolone, mycophenolate mofetil and tacrolimus, as detailed below: Prednisolone D 0: 500 mg IV D 1: 125 mg IV D 2 - 14: 20.0 mg/d (oral) Wk 3 - 4: 15.0 mg/d Wk 5 - 8: 10.0 mg/d Wk 9 - 12: 5.0 mg/d Wk 13 - 14: 2.5 mg/d Wk 15 - End: Cessation MMF (or biologic equiv.) D -7 to -2: 500 mg/d (250mg 2x/d) D -1 to 14: 2000 mg/d Wk 3 - 36: 1000 mg/d Wk 37 - 40: 750 mg/d Wk 41 - 44: 500 mg/d Wk 45 - 48: 250 mg/d Wk 49 - End: Cessation NOTE: MMF tapering will only happen if a 36-Wk biopsy shows no signs of subclinical rejection or if there is no evidence of declining renal function or if the clinician has any other concern about dose reduction. Tacrolimus (or biologic equiv.) ≤ 48 h pre-Tx to D 14: 3-12 ng/ml Wk 3 - 12: 3-10 ng/ml Wk 13 - 36: 3-8 ng/ml Wk 37 - End: 3-6 ng/ml

Biological: Donor M reg (Mreg_UKR)

Experimental: M reg treatment Donor M reg (2.5-7.5 million cells/kg) IV infused (6-7d before Tx) into recipients of a living donor renal Tx. Recipients also receive prednisolone, mycophenolate mofetil and tacrolimus background immunosuppression (as described in detail in the arm description).

Outcome Measures

Primary Outcome Measures

biopsy-confirmed acute rejection incidence [60 weeks]

Secondary Outcome Measures

time to first acute rejection episode [60 weeks]
severity of acute rejection episodes [60 weeks]
based on response to treatment and histological scoring
total immunosuppressive burden [60 weeks]
assessed at last study visit
incidence of patients treated for subclinical acute rejection [60 weeks]
prevention of chronic graft dysfunction (chronic rejection or IF/TA) [60 weeks]
assessed by clinical (impairment of GFR) and histopathological (Banff staging) measures
incidence of post-transplant dialysis, inclusion on the transplant waiting list or re-transplantation following graft loss through rejection [60 weeks]
avoidance of drug-related complications by immunosuppressant reduction [60 weeks]
assessed by the incidence of reported adverse drug reactions
incidence of embolic pulmonary complications and other embolic events [60 weeks]
incidence of immunological reactions resulting in anaphylactoid reactions, immediate cardiovascular compromise or other acute organ failure [1 week]
biochemical disturbances caused by cell infusion [1 week]
over-suppression of the immune system assessed by the incidence of major and/or opportunistic infections, especially CMV, EBV and polyoma virus [60 weeks]
over-suppression of the immune system assessed by the incidence of neoplasia [60 weeks]
immunological condition of study patients [60 weeks]
an extensive immune monitoring program has been established in The ONE Study

Other Outcome Measures

incidence of malignancies arising directly from Mreg_UKR [60 weeks]
incidence of autoimmune disorders [60 weeks]
incidence of inflammatory pathologies [60 weeks]
incidence of anaemia, cytopaenia or biochemical disturbances unrelated to the function of the transplanted kidney [60 weeks]
A Health-Economics Subproject will evaluate the health-related quality-of-life of trial patients using patient-reported outcome measures [60 weeks]
this subproject will also calculate the cost-effectiveness of the Mreg_UKR cell product

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

RECIPEINT

Inclusion Criteria:

Chronic renal insufficiency necessitating kidney Tx
Aged at least 18 years
Able to commence the immunosuppressive regimen as specified
Willing and able to participate in The ONE Study subprojects
Signed and dated written informed consent

Exclusion Criteria:

Patient has previously received any tissue or organ Tx
Known contraindication to the protocol-specified treatments /medications
HLA 0-0-0 mismatch
PRA grade >40% within 6 mo. prior to enrolment
Previous desensitisation treatment
Concomitant malignancy or history of malignancy <5 years before study entry (excluding successfully-treated non-metastatic skin BCC or SCC)
Significant local or systemic infection
HIV-positive, EBV-negative or suffering chronic viral hepatitis
CMV negative and receiving a kidney from a CMV+ donor
Significant liver disease
Malignant or pre-malignant haematological conditions
Any uncontrolled condition that could interfere with study objectives
Any condition placing the subject at undue risk
Ongoing treatment with systemic immunosuppressive drugs at study entry
Exposure to an investigational product during the study, or within 28 days or 5 half-lives of the product before study entry
Female patients of child-bearing potential with a +pregnancy test
Female patients breast-feeding or that are of child bearing potential and unwilling to use effective birth control
Psychological, familial, sociological or geographical factors hampering compliance
Any substance abuse or psychiatric disorder
Patients unable to freely give informed consent
Known IgA or IgG deficiency
Any pro-coagulant disposition causing undue risk
Previous history of transfusion-associated disease causing undue risk
Conditions resulting in substantially reduced pulmonary vasculature or increased pulmonary vascular resistance. Diseases causing substantially elevated pulmonary arterial or right heart hypertrophy or dysfunction
Known atrial or ventricular septal defects posing a risk of embolism
Known hypersensitivity to components of the manufactured cell product

DONOR

Inclusion Criteria:

Eligible for live kidney donation
Aged at least 18 years
Willing and able to provide a blood sample for The ONE Study Subproject
Willing to provide personal and medical/biological data for the trial analysis
Eligible for leucapheresis prior to organ donation
Signed and dated written informed consent

Exclusion Criteria:

Genetically identical to the prospective organ recipient at the HLA loci (0-0-0 mismatch)
CMV-positive and donating to a CMV-negative recipient
Exposure to an investigational product during the study, or within 28 days or 5 half-lives of the product before study entry
Any form of substance abuse, psychiatric disorder, or other condition that, in the opinion of the Investigator, may invalidate communication with the investigator and/or designated study personnel
Subjects unable to freely give their informed consent

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	University Hospital Regensburg	Regensburg		Germany	93053

Sponsors and Collaborators

University of Regensburg

Investigators

Study Director: Edward K Geissler, PhD, University Hospital Regensburg, University of Regensburg
Principal Investigator: Bernhard Banas, MD, University Hospital Regensburg, University of Regensburg
Principal Investigator: James A Hutchinson, MD, PhD, University Hospital Regensburg, University of Regensburg