Table 1.
Completed clinical trials of mesenchymal stem cell- and endothelial progenitor cells -based therapies in kidney diseases
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Ref.
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Condition or disease
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Trial registration
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Source
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Main findings
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| Togel et al[159], Westenfelder et al[160] | Patients with a high risk of developing AKI after undergoing cardiac surgery | NCT00733876 | Allogeneic BM-MSCs | MSC infusion was safe |
| None of the patients developed postoperative AKI or subsequent loss of kidney function | ||||
| Protection against early and late post-surgery kidney function deterioration | ||||
| Reduction in length of hospital stay | ||||
| Swaminathan et al[161] | Patients who experienced AKI 48 hr after cardiac surgery | NCT01602328 | Allogeneic BM-MSCs | No significant difference between groups in 30-d all-cause mortality or dialysis |
| No reduction in the time to recover kidney function | ||||
| No difference in adverse events between groups | ||||
| Makhlough et al[164] | CKD | NCT02195323 | Autologous BM-MSCs | MSC infusion was safe and tolerated. |
| No significant changes in eGFR and SCr | ||||
| Villanueva et al[162] | CKD | NA | Autologous AD-MSCs | MSC infusion was safe and not associated with adverse effects |
| Statistically significant improvement in urinary protein excretion but not in GFR | ||||
| Lee et al[178], Yang et al[179] | CKD at stage III or IV | NA | Autologous CD34+ EPCs | MSC infusion was safe and tolerated |
| No additional benefit from EPCs up to a follow-up period | ||||
| Significantly lower unfavourable clinical outcomes (dialysis or death) in treatment group | ||||
| Makhlough et al[163] | CKD due to autosomal dominant polycystic kidney disease | NCT02166489 | Autologous BM-MSCs | MSC infusion was safe and tolerated |
| No significant changes in eGFR and SCr | ||||
| Packham et al[180] | Diabetic nephropathy (type 2) | NCT01843387 | Allogeneic BM-MSCs | MSC infusion was safe and not associated with acute adverse events |
| Stabilisation and improvement in eGFR and mGFR | ||||
| Saad et al[181] | Atherosclerotic renovascular disease | NCT02266394 | Autologous AD-MSCs | MSC infusion was safe and well tolerated. |
| Increment in cortical perfusion and renal blood flow | ||||
| Reduction in renal tissue hypoxia within poststenotic kidney | ||||
| Sun et al[165], Liang et al[166] | Refractory SLE | NCT00698191 | Allogeneic BM-MSCs | MSC infusion was safe and tolerated |
| Improvement in disease activity | ||||
| Stabilisation in kidney function | ||||
| Sun et al[167] | Refractory SLE | NCT00698191 | Allogeneic UC-MSCs | MSC infusion was safe and tolerated |
| Improvement in disease activity | ||||
| Stabilisation in kidney function | ||||
| Wang et al[168] | Refractory SLE | NCT01741857 | Allogeneic UC-MSCs | MSC infusion was safe. |
| Reduction in proteinuria 24 hr after transplantation, with statistical differences at 9- and 12-mo follow-ups | ||||
| Deng et al[171] | LN (class III or IV) | NCT01539902 | Allogeneic UC-MSCs | No apparent additional effect over and above standard immunosuppression |
| Barbado at al[170] | Active and refractory LN | NA | Allogeneic BM-MSCs or UC-MSCs | Significant improvement in proteinuria levels during the 1st month after treatment |
| The ameliorations were sustained throughout the follow-up period | ||||
| Tan et al[177] | Kidney transplant | NCT00658073 | Autologous BM-MSCs | MSC infusion was not associated with adverse events and did not compromise kidney transplant survival |
| Lower incidence of acute rejection | ||||
| Reduction in risk of opportunistic infection, and better estimated kidney function at 1 yr | ||||
| Reinders et al[182] | Kidney transplant | NCT00734396 | Autologous BM-MSCs | MSC infusion was feasible and safe |
| Increment in incidence of opportunistic infection | ||||
| Perico et al[172,174] | Kidney transplant | NCT00752479 | Autologous BM-MSCs | MSC infusion was safe and feasible |
| Allowed enlargement of Treg in the peripheral blood | ||||
| Controlled memory CD8+ T cell function | ||||
| No major side effects during long-term follow-up | ||||
| Erpicum et al[176] | Kidney transplant | NCT01429038 | Autologous BM-MSCs | MSC infusion was safe |
| Increment in regulatory T cell proportion and with improved early allograft function | ||||
| Perico et al[172-173] | Kidney transplant | NCT02012153 | Autologous BM-MSCs | MSC infusion was safe |
| Reduction in circulating memory CD8+ T cells and donor-specific CD8+ T-cell cytolytic response | ||||
| No major side effects during long-term follow-up | ||||
| Mudrabettu et al[175] | Kidney transplant | NCT02409940 | Autologous BM-MSCs | MSC infusion was safe |
| Increment in proliferation of regulatory T cells | ||||
| Reduction in proliferation of CD4+ T cell | ||||
| Pan et al[183] | Kidney transplant | NA | Autologous BM-MSCs | None of the MSC recipients experienced immediate or long-term toxicity from the treatment |
| Comparable incidence of acute rejection and similar graft function and survival between control and study groups | ||||
| MSCs permitted the use of lower dosages of nephrotoxic calcineurin inhibitors |
MSC: Mesenchymal stem cells; EPC: Endothelial progenitor cells; BM-MSCs: Bone marrow derived- mesenchymal stem cells; AKI: Acute kidney injury; CKD: Chronic kidney disease; SCr: Serum creatinine; SLE: Systemic lupus erythematosus UC-MSCs: Umbilical cord-derived mesenchymal stem cells; NA: Not available.