Non Alcoholic Fatty Liver Disease Clinical Trial
Official title:
Effect of Empagliflozin on Liver Fat Content in Patients With Type 2 Diabetes: A 12-week Randomized Clinical Study
Fatty liver disease is an increasingly recognized health problem in patients with type 2 diabetes mellitus (T2DM). Sodium glucose co-transporter type 2 (SGLT-2) inhibitors are a new class of anti-diabetic agents that cause weight loss by inducing glycosuria. The effect of SGLT-2 inhibitors on liver fat content is not evaluated. Empagliflozin is an orally active, selective inhibitor of SGLT-2. We hypothesized that Empagliflozin, when added to standard care for T2DM, would improve fatty liver disease. Therefore, the present study is planned to evaluate the effect of Empagliflozin on the liver fat content.
Fatty liver disease is an increasingly recognized health problem in patients with type 2
diabetes mellitus (T2DM). Sodium glucose co-transporter type 2 (SGLT-2) inhibitors are a new
class of anti-diabetic agents that cause weight loss by inducing glycosuria. The effect of
SGLT-2 inhibitors on liver fat content is not evaluated. Empagliflozin is an orally active,
selective inhibitor of SGLT-2. We hypothesized that Empagliflozin, when added to standard
care for T2DM, would improve fatty liver disease. Therefore, the present study is planned to
evaluate the effect of Empagliflozin on the liver fat content.
Review of literature
Empagliflozin is a selective SGLT-2 inhibitor, recently approved by the U.S. FDA for use in
patients with T2DM. Empagliflozin in patients with type 2 diabetes provided sustained
glycemic control and weight loss over 90 weeks and was generally well tolerated (1). Another
study demonstrated that Empagliflozin in patients with T2DM resulted in reductions in HbA1c
and fasting plasma glucose (FPG), and reductions in body weight compared with placebo.
Empagliflozin was well tolerated with a favorable safety profile (2). Some congeners of this
class of molecules have been seen to reduce liver fat content in rat models. However, the
effect of this drug on liver fat content in humans has not been evaluated.
Research question
Does Empagliflozin reduce liver fat content in patients with T2DM and fatty liver disease?
Aim of the study
To study the effect of Empagliflozin on liver fat content in patients with T2DM
Primary objective
1. To evaluate the change in liver fat content from baseline at week 12
Secondary objective
2. To evaluate the changes from baseline in pancreatic fat content, visceral fat and
subcutaneous fat content at 12 weeks
Material and Methods
Ethical considerations
The trial protocol will be submitted to Medanta ethics committees for approval. The trial
will be conducted in accordance with the principles of the Declaration of Helsinki and Good
Clinical Practice guidelines. All the patients will be provided with written informed consent
before participation.
Patients and study area A total of 100 patients will be enrolled for the study. Consecutive
patients attending outpatient Department of Endocrinology and Diabetes for management of
diabetes will be enrolled.
Sample Size Calculation:
Assumptions: Change in liver fat content from baseline to week 12 in Empagliflozin dose group
(m1) = 6.0 unit Change in liver fat content from baseline to week 12 in Standard dose group
(m2) = 10.0 unit
Confidence level -95%, Power - 80%, Coefficient of variation = 80% Formula for sample size
calculation: n = (Zα+Zβ)2 * (σ12 + σ22)) / (m1-m2)2, where Zα is the value of normal
distribution corresponding to desired confidence level, Zβ is the value of the Normal
distribution corresponding to desired power, σ1 and σ2 are the standard deviation of the two
groups. With these assumptions the sample size per group works out as 50.
Randomization
SPSS software will be used to generate 100 random numbers between 000 to 999. The random
numbers will be divided by 2 and the reminder noted. The reminders 0, & 1 will correspond to
Empagliflozin dose and standard dose group respectively. It will be ensured that these are
equal in number.
Opaque envelopes will be prepared with serial number on the top and the assigned group inside
the envelope.
After recruiting the subjects the envelop with corresponding serial number will be opened and
the subjects assign to the relevant groups.
Statistical Analysis Plan:
The analysis will include profiling of patients on different demographic, clinical and
laboratory parameters etc. Quantitative data will be presented in terms of means and standard
deviation and qualitative/categorical data will be presented as absolute numbers and
proportions. Cross tabulation will be generated and chi square test will be used for testing
of association. Student t test will be used for comparison of quantitative outcome parameters
and standard normal deviate test for proportions. P-value < 0.05 is considered statistically
significant. SPSS software will be used for analysis.
All patients will be randomized to one of the following intervention groups: group I (n =
50): T2DM patients receiving standard care for T2DM (metformin, sulfonylurea, DPP-4 inhibitor
or insulin, in any combination) plus 10 mg of Empagliflozin per day and group II (n = 50):
Standard care for T2DM upgraded without Empagliflozin.
Liver fat content, pancreatic fat content, visceral and subcutaneous fat content will be
assessed by magnetic resonance imaging (MRI) proton density fat Fraction (PDFF) at the
beginning of study and again after 12 weeks of intervention. PDFF is emerging as a leading
MR-based biomarker for noninvasive quantification of hepatic steatosis (3, 4). Multiple human
studies have shown that this method accurately estimates PDFF in the liver. Based on these
results, this magnitude-based PDFF estimation method now is being used to quantify liver fat
in clinical practice in several institutions in the United States and is being used as a
biomarker of drug efficacy and drug toxicity by the National Institutes of Health (NIH) and
industry in clinical trials (5, 6). This method has been shown to be both accurate, and
reproducible (7).
Fatty liver will also be assessed by ultrasonography of liver at the beginning of study and
again after 12 weeks of intervention. On ultrasonography, severity of fatty liver will be
quantitated using a scoring system (0 = no fatty liver, 1 = mild fatty liver, 2 = moderate
fatty liver and 3 = severe fatty liver). Automated body composition analyzer (BCA) will also
be used to assess body composition at 0 and 12 weeks.
Laboratory workup Biochemical parameters will include fasting and post-prandial plasma
glucose, glycosylated hemoglobin (HbA1C), lipid profile, hemogram, kidney function test
(urea, creatinine) and liver function test (total and fractionated bilirubin, alanine
transaminase (ALT), aspartate aminotransferase (AST), gamma-glutamyl transpeptidase (GGT),
total protein, albumin) before and after the intervention period.
The primary end point
1. Change in liver fat content from baseline at week 12 The secondary end points
2. Change in pancreatic fat content, visceral fat and subcutaneous fat content from
baseline at week 12
Confidentiality Precautions will be taken to ensure confidentiality. Data collection forms
will not reveal the name of the patients included in study.
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