Efficacy, Safety and Response Predictors of Adjuvant Astragalus Therapy for Diabetic Kidney Disease

Last updated: December 3, 2020
Sponsor: The University of Hong Kong
Overall Status: Active - Recruiting

Phase

2/3

Condition

Diabetic Kidney Disease

Treatment

N/A

Clinical Study ID

NCT03535935
RE-02
  • Ages 35-80
  • All Genders

Study Summary

This add-on open-label randomised controlled pragmatic trial aims to:

  1. evaluate the effect of add-on astragalus treatment on type 2 diabetic patients with stage 2 to 3 chronic kidney disease and macroalbuminuria.

  2. estimate treatment effect, variance, recruitment rate, attrition rate and change in clinical manifestation including Chinese medicine syndrome for parameters optimisation and feasibility assessment for a subsequent phase III randomised controlled trial.

  3. assess response predictors for efficacy and safety among type 2 diabetic patients with stage 2 to 3 chronic kidney disease and macroalbuminuria receiving add-on astragalus treatment

Eligibility Criteria

Inclusion

Inclusion Criteria:

  • diagnosed with type 2 diabetes for at least 5 years;
  • with an estimated glomerular filtration rate (GFR) ≥30 ˂90 mL/min/1.73m2 confirmedwith repeat testing over three or more months calculated by the abbreviated MDRD studyequation;
  • persistent macroalbuminuria with spot urine albumin-to-creatinine ratio (UACR) ≥ 300mg/g confirmed by at least 2 out of 3 consecutive first morning void urine samples;
  • on stable dose of anti-diabetic drug including insulin for 12 weeks;
  • on stable dose of angiotensin-converting-enzyme inhibitor or angiotensin receptorblocker for 12 weeks; and
  • willing and able to give written informed consent

Exclusion

Exclusion Criteria:

  • with known history of glomerulonephritis, polycystic kidney disease, systemic lupuserythematosus, any suggestive evidence of nondiabetic glomerulopathy;
  • with known history of kidney transplant;
  • with concurrent severe disorders of heart, brain, liver, and hematopoietic system,tumor and mental disorder;
  • with deranged liver function;
  • poorly controlled blood pressure;
  • with known history of intolerance or malabsorption of oral medications;
  • with uncontrollable urinary infection;
  • experiencing pregnancy; or
  • participating in other clinical trial within 30 days

Study Design

Total Participants: 118
Study Start date:
July 01, 2018
Estimated Completion Date:
December 31, 2022

Study Description

This add-on open-label randomised controlled pragmatic trial.

Sample size is calculated based on planned regression analysis. We believe an annual GFR benefit of 5 ml/min/1.73m2 is deemed significant clinically. 118 patients are therefore needed to offer a power of 70% to detect a GFR difference of 5 ml/min/1.73m2 over 48-week allowing 15% attrition rate for this study with a significance level of alpha equals to 0.05.

A trial management committee (TMC) formed by PA, Co-As and RA will centralise all the data of the trial. Co-As and RA will collect, clean and send the data of patients to TMC on a weekly basis. All data will be double entered to computer and cleaned before analysis to prevent data entry errors. All data transfer will be encrypted to protect patients' confidentiality. TMC will have regular meetings monthly with experts to discuss the progress of the trial. An independent Data Monitoring Board (DMB) will be invited to monitor the progress of the trial. DMB will advise ethics committee to terminate the trial if data is showing extreme benefits or harm. Detailed guidelines will be discussed and set by DMB.

Missing values will be imputed with last observation carried forward. Patient without a postrandomisation assessment for a particular efficacy endpoint will be excluded from the analysis of that endpoint.

Regression analysis will be used to compare the adjusted mean of eGFR, UACR, HbA1c, FBG, and other biomarkers at week 48 between groups and statistical significance. The adverse events will be analysed in a narrative manner. The percentage of all adverse events and the rate of attrition due to adverse events will be compared between intervention groups and control groups.

To minimise Type I error inflation, the analysis will follow a hierarchical approach in the order of 1) comparison of baseline to end of treatment on eGFR and UACR; 2) comparison of baseline to end of treatment on other outcome measurements; 3) comparison of baseline to treatment midpoints on eGFR and UACR and 4) comparison of baseline to treatment midpoints on other outcome measurements.

Subgroup analysis will be performed for different age groups, gender chronic kidney disease stage and severity of albuminuria.

The dependent variable is the treatment response which is categorised into:

  1. Improved or stabilised renal function, defined as eGFR after 48-week treatment being higher or equal to baseline.

  2. Non-responder, defined as patients having eGFR decreased at a rate of less than 5 mL/min/1.73m2 after 48-week treatment compared to baseline.

  3. Rapid deteriorating renal function, defined as eGFR of more than 5 mL/min/1.73m2 after 48-week treatment compared to baseline.

Potential prognostic variables (baseline values) include:

  1. Demographics and past medical history: Age, gender, body mass index (BMI), systolic blood pressure, history and duration of smoking and alcohol consumption and others

  2. Chinese medicine diagnosis: presence of Chinese medicine syndromes (e.g. spleen and kidney qi deficiency) based on the presentation of standardised and commonly documented signs and symptoms

  3. Biochemical profile

Connect with a study center

  • Queen Mary Hospital

    Hong Kong,
    Hong Kong

    Active - Recruiting

  • School of Chinese Medicine

    Hong Kong,
    Hong Kong

    Site Not Available

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