Table 1.
Author, year | Trial design | Inclusion criteria | Treatment | Patients | Immunosuppression | Follow‐up | Major EP | Major results |
---|---|---|---|---|---|---|---|---|
Kulkarni, 2017 16 | Single centre nonblinded RCT | HLA‐DSA+, 20% eGFR decline upon 12 months | Eculizumab, 600 mg/week for 4 weeks; 900 mg every 2 weeks for 26 weeks |
Treatment: n = 10 Control: n = 5 |
Not specified | 1 year |
Primary EP: eGFR decline Secondary EP: acute rejection; treatment failure (death, graft loss, loss to follow‐up or withdrawal from trial); biopsies at 3, 6 and 12 months, DSA MFI and C1q fixation |
Marginal improvement of eGFR trajectory (P = 0.09); no effect on morphological and molecular biopsy results |
Moreso, 2018 35 | Multicentre placebo‐controlled RCTa | HLA‐DSA+, chronic ABMR (cg > 0) |
IVIGx4 (0.5 g/kg) every 3 weeks RTX (375 mg/m2) 1 week after the last IVIG infusion |
Treatment: n = 13 Placebo: n = 12 |
Tac/MMF Tac C0: 5–10 ng/ml |
1 year |
Primary EP: eGFR decline Secondary EP: proteinuria, biopsies at 12 months, DSA MFI |
No effect on eGFR decline, biopsy results and DSA‐MFI; no differences in adverse events |
Eskandary, 2018 34 | Single centre placebo‐controlled RCT | HLA‐DSA+, late ABMR after >180 days | Bortezomib (two cycles; each four injections, 1.3 mg/m2; 3‐month interval) |
Treatment: n = 21 Placebo: n = 23 |
Triple immunosuppression Tac C0: 7–10 ng/ml CyA C0: 80–120 ng/ml |
2 years |
Primary EP: eGFR slope Secondary EP: proteinuria; biopsies at 24 months, DSA MFI |
No effect on eGFR decline, biopsy results and DSA MFI Higher rate of SAEs |
ABMR, antibody‐mediated rejection; DSA, donor‐specific antibody; eGFR, estimated glomerular filtration rate; EP, endpoint; MMF, mycophenolate mofetil; MFI, mean fluorescence intensity; RCT, randomized controlled trial; SAE, severe adverse event; Tac, tacrolimus.
Planned sample size: 25 patients per group (not achieved because of budgetary constraints and slow patient recruitment).