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ACKGROUND: The development of new molecular techniques, in recent years, has increasing the knowledge of the composition and functionality of the intestinal microbiota. In the area of kidney transplantation, observational studies have described a change in the intestinal microbiota during the immediate post-transplantation period that seems to be related to the appearance of clinical outcomes such as diarrhea, repeated urinary tract infections, the need for adjustment of immunosuppressive treatment or acute rejection. However, intervention studies on this subject are necessary to determine how far the microbiota can influence in the development of these events.
OBJECTIVE: To clarify the influence of maintaining the composition and functionality of the intestinal microbiota on post-transplant clinical outcomes such as diarrhea, urinary tract infections, kidney graft rejection and the need for dose adjustment of immunosuppressive therapy.
MATERIALS AND METHODS: single-center, randomized, interventional pilot study with 50 deceased kidney donor transplant patients at low immunological risk. Each patient will be randomized at the time of inclusion in the study to one of the 2 branches of the study: 1) Intervention group: 25 patients who will receive a autologous fecal matter transfer during the first 6 months post-transplantation, 2) Control group: 25 renal transplant patients with the same characteristics who will not receive any type of intervention in addition to the immunosuppressive treatment indicated according to hospital protocol.
ACKGROUND: The development of new molecular techniques, in recent years, has increasing the knowledge of the composition and functionality of the intestinal microbiota. In the area of kidney transplantation, observational studies have described a change in the intestinal microbiota during the immediate post-transplantation period that seems to be related to the appearance of clinical outcomes such as diarrhea, repeated urinary tract infections, the need for adjustment of immunosuppressive treatment or acute rejection. However, intervention studies on this subject are necessary to determine how far the microbiota can influence in the development of these events.
OBJECTIVE: To clarify the influence of maintaining the composition and functionality of the intestinal microbiota on post-transplant clinical outcomes such as diarrhea, urinary tract infections, kidney graft rejection and the need for dose adjustment of immunosuppressive therapy.
MATERIALS AND METHODS: single-center, randomized, interventional pilot study with 50 deceased kidney donor transplant patients at low immunological risk. Each patient will be randomized at the time of inclusion in the study to one of the 2 branches of the study: 1) Intervention group: 25 patients who will receive a autologous fecal matter transfer during the first 6 months post-transplantation, 2) Control group: 25 renal transplant patients with the same characteristics who will not receive any type of intervention in addition to the immunosuppressive treatment indicated according to hospital protocol.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Control | Active Comparator | Patients of this branch will not have autotransplantation of gut microbiota in capsules and will follow their usual post-transplant treatment |
|
| Microbiota autotransplantation | Active Comparator | Patients in this branch will receive autotransplantation of intestinal microbiota in capsules for 6 months post-transplantation |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Microbiota autotransplantation | Dietary Supplement | Patients received microbiota autotransplantation in capsules (1g per day) for 6 months |
|
| Measure | Description | Time Frame |
|---|---|---|
| Evaluate the occurrence of diarrhea | Evaluate the occurrence of diarrhea regardless of its cause, between the intervention and control groups. Diarrhea will be defined as three or more bowel movements per day (or more frequently than normal for the individual), and presence of loose or liquid stools, following WHO definition | 6 months after transplantation |
| Measure | Description | Time Frame |
|---|---|---|
| Occurrence of post-transplant urinary tract infections | Evaluate the occurrence of post-transplant urinary tract infections (UTI), defined as positive urine culture with associated voiding symptoms or fever, as well as positive urine cultures until removal of the double J catheter, given that they will receive antibiotic treatment as if it were a UTI. Positive urine cultures or asymptomatic bacteriuria after removal of the double J catheter (usually at one-month post-transplantation) will not be included in the definition. |
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Inclusion Criteria:
Exclusion Criteria:
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Esmeralda Castillo Rodríguez, MD | Contact | 913368018 | esmeralda.castle@gmail.com | |
| Andrea Collado Alsina, PhD | Contact | 913368018 | macolladoalsina@gmail.com |
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Hospital Ramón y Cajal | Recruiting | Madrid | 28034 | Spain |
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Single-center, randomized, intervention pilot study with a sample size of 50 patients (25 patients in intervention group who will receive gut microbiota autotransplantation and 25 group in control group without intervention) for a follow-up time of 6 months
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| Control | Dietary Supplement | Patients will not received microbiota autotransplantation in capsules and will received usual medical care |
|
| 6 months after transplantation |
| Evaluate the dose/level ratio of immunosuppressive drugs | Evaluate the dose/level ratio of immunosuppressive drugs (tacrolimus or everolimus) administered in the intervention groups with respect to the control group | 6 months after transplantation |
| Evaluate the proportion of acute rejection episodes | Evaluate the proportion of acute rejection episodes between the two groups in the follow-up period | 6 months after transplantation |
| Determined Treg lymphocyte populations | Evaluate whether there are differences between the Treg lymphocyte populations in peripheral blood by flow cytometry between the two groups | 6 months after transplantation compared to pre transplant situation |
| Systemic inflammation | Measurement of inflammatory markers in serum by automated systems, such as C-reactive protein | 6 months after transplantation |
| Production of bacterial metabolites | Determination of the short-chain fatty acids (SCFA) concentration as bacterial metabolites in feces and urine by LC-MS/MS as indicators of the functionality of the microbiota | 6 months after transplantation compared to pre transplant situation |
| Analysis of the bacteria composing the microbiota | Analysis of the bacteria composing the microbiota by massive sequencing of the 16S rDNA gene | 6 months after transplantation compared to pre transplant situation |