Trials / Active Not Recruiting

Active Not RecruitingNCT02470507

Immune Function in Acute Kidney Injury

Evaluation of Immune Function in Patients With Acute Kidney Injury

Summary

The immune response to kidney damage during acute kidney injury (AKI) is an important contributor to the prolonged lack of renal function and progression of kidney injury. Most data related to intrarenal and interorgan pathways in AKI stem from animal research with sometimes conflicting results. Accurate evaluation of these processes in humans and identification of early diagnostic tools are critical for the development of strategies to prevent and attenuate AKI-related morbidity and mortality in patients. The aim of this study is to evaluate immune function and miRNA expression in hospitalised patients with and without AKI.

Detailed description

Hypothesis: An overriding pro-inflammatory immune response underlies AKI in humans which contributes to dysfunction of non-renal organs Principal research question: Is AKI in humans associated with a predominantly pro-inflammatory immune response? Secondary research questions: 1. Does AKI affect the phenotypic characterisation and function of neutrophils? 2. Does severity of AKI lead to differences in phenotypic characterisation and function of neutrophils? 3. What are the differences in cytokine profiles between AKI patients with and without systemic inflammation? 4. What are the differences in cytokine profiles between AKI patients with systemic inflammation and patients with systemic inflammation without AKI? 5. Is there a correlation between microRNA levels in patients with AKI and degree of AKI, renal recovery and patient outcome? Study design: Observational non-interventional study Study population: 30 patients with AKI stage II or III \* and systemic inflammation without sepsis 30 patients with AKI stage II or III \* and no systemic inflammation 30 patients with systemic inflammation and normal renal function 30 patients after major surgery who do not have an infection, SIRS or AKI \* AKI will be defined by the KDIGO criteria Primary outcome Detection of measurable phenotypic characteristics and function of leukocytes that are specific of patients with AKI. Secondary outcomes: 1. Differences in phenotypic characterisation and function of neutrophils between patients with AKI stage II and III. 2. Differences in phenotypic characterisation and function of neutrophils between patients with and without AKI. 3. Differences in cytokine profiles between patients with AKI and systemic inflammation and patients with AKI without systemic inflammation 4. Differences in cytokine profiles between AKI patients with systemic inflammation and patients with systemic inflammation without AKI 5. Correlation between microRNA levels in patients with AKI and renal recovery 6. Correlation between microRNA levels in patients with AKI and patient outcome 7. Differences in cytokine profiles between AKI patients without systemic inflammation and patients without AKI and without systemic inflammation / infection. Statistical analysis: For the analysis of laboratory variables that describe the immunological phenotype, standard statistical methods will be applied. 1) When the normal distribution assumption is met, groups will be compared using ANOVA and the corresponding contrasts for group by group comparisons; 2) In the absence of normality or for ordinal variables, Kruskal Wallis will be applied for multi-group comparisons, and Wilcoxon for two-groups analysis. We will apply multiple testing correction via Benjamini-Hochberg FDR control. For the analysis of miRNA array data, we will first follow the protocol quality control measures appropriate for the platform of choice, and subsequently will carry out statistical analysis using the SAMr and LIMMA packages from Bioconductor, via the R software. Similarly, for the analysis of PCR data, the package HTqPCR from bioconductor will be used for quality control. Depending on the distribution of the final data, either non-parametric statistics, or a moderated t-test will be applied for statistical comparisons, with the corresponding multiple testing corrections as above.

Conditions

• Acute Kidney Failure

Interventions

Timeline

Start date

2013-06-01

Primary completion

2022-08-01

Completion

2026-12-01

First posted

2015-06-12

Last updated

2024-01-23

Locations

1 site across 1 country: United Kingdom

Source: ClinicalTrials.gov record NCT02470507. Inclusion in this directory is not an endorsement.