Kidney Transplantation Clinical Trial
— RituxiCAN-C4Official title:
Randomised Trial of Anti-Cd20 in C4d+ Chronic Allograft Nephropathy
| Verified date | March 2020 |
| Source | King's College London |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
Purpose of clinical trial; Evaluate the effectiveness of rituximab in C4d+ CAN
Primary objective; To determine whether anti-CD20 therapy can stabilize or improve renal
function and/or proteinuria in patients with C4d+, chronic (humoral) rejection in whom
standard therapeutic approaches have failed.
Secondary objective (s);
- To compare patient and graft survival between control and rituximab-treated groups
- To evaluate the adverse effect profile of rituximab in this group
- To correlate changes in circulating B cell numbers, anti-HLA and non-HLA Ab profiles and
titre with responses to standard therapy and / or rituximab
- To correlate changes in T cell responsiveness to alloantigens with responses to standard
therapy and / or rituximab
Study Design; Prospective, randomised, two arm, open-labeled
Study Endpoints; Primary
- Rate of deterioration in renal function, defined by slope of reciprocal creatinine plot,
on samples taken 3-5 months post-randomisation.
- Change in degree of proteinuria, where present, at 3-5 months post-randomisation 2˚
endpoints, determined at 3-5 months post-randomisation and at 1, 2 and 3 years
post-recruitment are;
- Rate of deterioration in renal function, defined by slope of reciprocal creatinine plot,
determined by analysis of samples taken since previous assessment.
- Patient survival
- Graft survival
- Incidence of culture positive infection
- Incidence of malignancy
- Degree of proteinuria
- Changes in circulating CD20+ cells in peripheral blood
- Changes in anti-graft Ab titres, (measured every 3 months)
- Changes in T cell responsiveness to alloantigens (measured every 3 months).
Sample Size; 15 patients to be randomised to each arm (i.e. 30 patients randomised). Up to
120 patients will need to be enrolled into the study. In addition, in those participants that
received a living donor kidney, these donors will be approached to provide up to 5 samples of
blood to help with the in vitro analyses.
Summary of eligibility criteria;
- Male or female renal allograft recipients 18-70 years of age
- more than 6/12 post-transplantation
- Either deteriorating allograft function on reciprocal creatinine plot or significant
proteinuria or both.
- C4d+/- CAN on renal allograft biopsy
Investigational medicinal product and dosage; Rituximab, 1g on day 0 and 1g on day 14
Active comparator product(s); None
Route(s) of administration; Intravenous infusion
Maximum duration of treatment of a subject; 14 days with rituximab. The treatment arms of the
study, including optimisation period, formal run-in and post-randomisation phase lasts for 10
months post-recruitment.
Procedures; Screening & enrollment. Potentially eligible patients will be identified by
screening renal allograft biopsies performed for 'creeping creatinine' and/or proteinuria.
Recruitment by informed consent prior to enrollment.
Procedures; Baseline. In addition to routine tests, blood for anti-HLA and non-HLA antibody
analysis and for peripheral blood mononuclear cell (PBMC) purification.
Procedures; Treatment period. 3 month run-in period on optimal conventional immunosuppressive
therapy, preceded by up to 2 months to allow tailored-optimization. Patients will be reviewed
at least six times in their normal transplant clinic appointments for routine blood
biochemistry, full blood count and urine analysis. At the end of the run-in period, further
blood will be taken for anti-graft antibody analysis and PBMC purification. Those patients in
whom allograft function stabilises and/or proteinuria improves will have normal transplant
clinic follow-up appointments and have blood taken for further anti-graft antibody and PBMC
purification up to every 3 months for 3 years. Those with continued deterioration in either
allograft function or persisting or worsening proteinuria will be randomised. These patients
will be reviewed during their normal transplant clinic appointments until the primary
end-point and will need to have at least 6 routine blood biochemistry, full blood count and
urine analysis during the final 3 months of this period, post-randomisation. At the primary
end-point, further blood will be taken for anti-graft antibody analysis and PBMC.
Procedures; End of Study. •Follow up will continue for 3 years, with blood taken for
anti-graft antibody analysis and PBMC purification every three months
Procedures for safety monitoring during trial; Regular patient interviews and examination,
routine haematological and biochemical analyses. Serious adverse events will be reported and
forwarded to the sponsor, MHRA, LREC and Roche as appropriate The WLRATC transplant research
committee will discuss the trial and any safety concerns at their regular three monthly
meetings. Data will be reviewed after 30 and also after 60 people have been enrolled.
Criteria for withdrawal of patients on safety grounds; Serious adverse effects related to
rituximab infusion
| Status | Completed |
| Enrollment | 62 |
| Est. completion date | April 2017 |
| Est. primary completion date | May 2015 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years to 70 Years |
| Eligibility |
Inclusion Criteria: - Functioning kidney allograft (with estimated (e) GFR by MDRD >20) and be >6/12 post-transplantation - Deteriorating allograft function as defined by linear regression of reciprocal creatinine plot. Deterioration will be defined as a negative slope over at least the preceding 3 months (with at least 6 creatinines included) with an adjusted r2 >0.35 and a p value of =0.05 compared to horizontal baseline. Deterioration will be confirmed by reduction in Cockcroft-Gault (CG) eGFR over the same period (to exclude increases in body mass as a cause of a negative slope on reciprocal creatinine plots) OR significant proteinuria as assessed by a urine protein/creatinine ratio of =50 - CAN, by Banff '97 criteria, and/or transplant glomerulopathy on renal allograft biopsy performed within 6/12 of enrolment - Diffuse, linear C4d deposition on at least 25% of peritubular capillary (PTC) and/or glomerular EC of renal transplant biopsy when assessed by immunoperoxidase or >50% of PTC (alone) when assessed by immunofluorescence OR PTCitis OR glomerulitis with combined PTC/g score of =2. Exclusion Criteria: - Ages below 18 years of age - Suspicion of pregnancy confirmed by positive HCG pregnancy test - Untreated ureteric obstruction on ultrasound of allograft - History of acute allograft rejection in preceding 3/12 - History of MI in preceding 3/12 - History of malignancy in previous 5 years (excluding tumours limited to skin) - Symptomatic IHD - Recipient of simultaneous pancreas/kidney transplant - Recipient of ABO-incompatible kidney - Recipient who underwent an HLA desensitisation procedure prior to transplantation - Evidence, on examination of renal allograft biopsy specimen, of recurrent or de-novo disease (except IgA deposition in absence of mesangial proliferation) - Evidence, on examination of renal allograft biopsy specimen, of CNI toxicity IF ACCOMPANIED by mostly supra-therapeutic CNI trough levels in the 6 month period preceding biopsy. - Documented allergy to mouse or chimeric human/mouse proteins - HepBsAg+, HepBcAb+, HCV Ab+ or HIV+. |
| Country | Name | City | State |
|---|---|---|---|
| United Kingdom | University Hospital Birmingham | Birmingham | |
| United Kingdom | East Kent Hospitals University NHS Foundation Trust | Canterbury | |
| United Kingdom | Univeristy Hospital of Wales | Cardiff | |
| United Kingdom | Epsom & St Helier University Hospitals Trust | Carshalton | |
| United Kingdom | Western Infirmary | Glasgow | |
| United Kingdom | Hull Royal Infirmary | Hull | |
| United Kingdom | St Jame's University Hospital | Leeds | |
| United Kingdom | Imperial College London and West London Renal & Transplantation Centre | London | |
| United Kingdom | King's College London, Guy's Hospital | London | |
| United Kingdom | The Royal Free Hospital | London | |
| United Kingdom | Manchester Royal Infirmary | Manchester |
| Lead Sponsor | Collaborator |
|---|---|
| King's College London | Medical Research Council, Roche Pharma AG |
United Kingdom,
Shiu KY, Stringer D, McLaughlin L, Shaw O, Brookes P, Burton H, Wilkinson H, Douthwaite H, Tsui TL, Mclean A, Hilton R, Griffin S, Geddes C, Ball S, Baker R, Roufosse C, Horsfield C, Dorling A. Effect of Optimized Immunosuppression (Including Rituximab) o — View Citation
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Rate of deterioration in renal function, defined by slope of reciprocal creatinine plot | 3-5 months post-randomisation | ||
| Primary | Change in degree of proteinuria, where present | 3-5 months post-randomisation | ||
| Secondary | Rate of deterioration in renal function, defined by slope of reciprocal creatinine plot, determined by analysis of samples taken since previous assessment | 1, 2 and 3 years post-recruitment | ||
| Secondary | Patient survival | 5 months post-randomisation and at 1, 2 and 3 years post-recruitment | ||
| Secondary | Graft survival | 5 months post-randomisation and at 1, 2 and 3 years post-recruitment | ||
| Secondary | Incidence of culture positive infection | 5 months post-randomisation and at 1, 2 and 3 years post-recruitment | ||
| Secondary | Incidence of malignancy | 5 months post-randomisation and at 1, 2 and 3 years post-recruitment | ||
| Secondary | Degree of proteinuria | 1, 2 and 3 years post-recruitment | ||
| Secondary | Changes in circulating CD20+ cells in peripheral blood | 5 months post-randomisation and at 1, 2 and 3 years post-recruitment | ||
| Secondary | Changes in anti-graft Ab titres | 3 monthly to 3 years post-recruitment | ||
| Secondary | Changes in T cell responsiveness to alloantigens | 3 monthly to 3 years post-recruitment |
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