Type 2 Diabetes Mellitus Clinical Trial
Official title:
Modulation of Insulin Secretion and Insulin Sensitivity in Bangladeshi Type 2 Diabetic Subjects by an Insulin Sensitizer Pioglitazone and T2DM Association With PPARG Gene Polymorphism.
- The present study was undertaken to assess the efficacy and safety of two different
insulin sensitizers (namely Pioglitazone and Metformin) among subjects with type 2
diabetes mellitus (T2DM) in Bangladesh.
- A prospective, double-blind, single group, 'within-subject' designed clinical trial of
77 diagnosed T2DM patients out of 130 patients with glycosylated haemoglobin (HbA1c)
≥7.2±1.5%, aged 46±6.4 years and registered for diabetes treatment in Bangladesh
Institute of Research and Rehabilitation in Diabetes Endocrine and Metabolic Disorders
(BIRDEM) was carried out.
- The study was conducted between November 2008 and September 2010.
- Baseline data, included case history of the patients,anthropometric measurement,
biomedical parameters psychosocial factors, were collected from each subject and then
enrolled to receive treatment with 001 drug once daily for three months, then the
patients were left for wash out with metformin 850mg once daily for one month; then
they received 002 drug once daily for further three months.
- Dietary chart was remained as before.
- DNA was isolated by Chelex method using the primers and control DNA,restriction
Digestion Enzyme Endonuclease Hae 111 for genotyping PPARγ-(Peroxisome Proliferator
Activated Receptor gamma)Pro12Pro
- (Proline12Proline)/Pro12Ala-(Proline12 Alanine))/Ala12Ala-(Alanine12Alanine).
- The blinded drugs were decoded after analyzing results, 001 tablet was pioglitazone (30
mg once daily) and 002 tablets was metformin (850mg once daily). Bio-medical outcomes
were measured to assess the efficacy of both the drugs each month. After finishing the
treatment period the effects of two drugs were compared using SPSS.And the association
between the pioglitazone drug effects and genetic polymorphism was also assessed.
- The metformin effects was assessed also using the response rate of HbA1c <7.0% after 3
months treatment to the patients.
1. Introduction Thiazolidinediones and metformin are known drugs and especially metformin
is widely used medicine to treat people with T2DM. Though pioglitazone has been
suspended in many countries, its safety and efficacy is a matter of research for the
drug investigators. Thiazolidinediones had been introduced in 1997 as an oral
anti-diabetic drug (OAD). Metformin has been used as the key compound to treat T2DM for
many years and is the most prescribed OAD worldwide. Both metformin and
thiazolidinediones are considered as "insulin sensitizer". The ß-cell dysfunction and
insulin resistance are the core defects in the progression of T2DM with associated
metabolic syndrome. Evidence suggests that pioglitazone lowers glucose in blood by
increasing glucose uptake into cell and metformin by decreasing glucose production.
However, there are many controversies in clinical study specially about the improvement
of insulin action of metformin. In contrast, a research recommended pioglitazone as the
most appropriate OAD for the South Asian population. The key to this argument is that
since pioglitazone is a proliferator-activated receptor gamma (PPAR-γ or PPARG) [a
group of nuclear receptor proteins that function as transcription factors regulating
the expression of genes] agonist and decreases insulin resistance, overall glycemic
control seems to be better with this thiazolidinedione. However, there are very few
published documents on the efficacy and safety of these drugs in South Asians. To the
best of our knowledge, there is no published paper that examined and compared the
efficacy and safety of these two drugs in Bangladeshi patients T2DM. This double-blind
trail therefore examined the efficacy and safety of pioglitazone and metformin in T2DM
individuals and also the association of the effects of pioglitazone and the variants of
PPARG. We have compared the effects of pioglitazone with metformin on biomedical
variables in T2DM patients who were eligible for oral hypoglycaemic therapy and then we
also analyzed the association among the effects of pioglitazone and PPARG variants.
2. Methodology
1. Study Setting:
The study was conducted between November 2008 and September 2010. The participants
for this study were recruited from the outdoor, BIRDEM Hospital in
Dhaka,Bangladesh.
2. Subjects I.Individuals who had been diagnosed with T2DM treating with
diet/exercise or Metformin 850 mg or Pioglitazone 30mg once daily, and were
attending Outdoor Patient Department (OPD) of BIRDEM for consultation were
approached by the researcher and invited to participate in the study. The patients
were diagnosed already and registered in BIRDEM. T2DM was ascertained based on
World Health Organization recommended criteria two repeated measures of fasting
(plasma glucose ≥7.0 mmol ⁄ l or 2-h plasma glucose ≥11.1 mmol ⁄ l.)
II.We screened a total of 130 patients for eligibility and selected 80 patients
for enrollment based of our inclusion and exclusion criteria. But 77 T2DM patients
with HbA1c level < 7.5 %, BMI kg/m2 ≥ 25, SGPT≤ 100 IU/L , creatinine ≤ 1.2 mg/dl)
of both sexes, aged between 40-50, treated by monotherapy of pioglitazone or
metformin received the drug for the trial according to inclusion and exclusion
criteria. 53 patients were screening failure as some did not match eligibility
criteria (n=39), some refused to take part(n=11)and some were unable to take part
(n=03)due to unknown cause.
3. Patient Preparation:
I.Written informed consent was obtained from all participants before study entry.
Patients were instructed to follow adhere to a disease- and weight-orientated diet
throughout the study as before.
II.Each case history was documented in the case report form. The study was
approved by the National Medical Ethics Review Boards (NMERB) of Bangladesh
Medical Research Council (BMRC).The investigations were carried out in accordance
with the principles of the Declaration of Helsinki as revised in 2000.
4. Treatment:
The patients were to receive treatment pioglitazone tablet 001 (30mg once per day)
for 3 months followed by one month "metformin wash-out period", then to the
alternative treatment regimen for further 3 months with metformin tablet 002
(850mg once per day). The drugs were supplied by the Aristopharma Pharmaceutical
Ltd., Bangladesh.
5. Anthropometric Measurements I.Height: Standing height was measured using
appropriate scales (Detect-Medic, Detect scales INC, USA) without shoes.
II.Weight: Weight was measured with the balance was placed on a hard flat surface
and checked for zero balance before measurement. The subjects were in the center
of the platform wearing light cloths without shoes.
III.BMI: Body mass indexes (BMI) of the subjects were calculated using standard
formula: BMI= Weight (kg)/[Height (m)] 2.
IV.Blood Pressure: Systemic and Diastolic pressure was measured according to
WHO-IHS.
6. Blood Sample Collection for Biochemical analysis :
I. During the appointed date the patients came in the fasting condition. Fasting
blood samples (10 ml) were drawn from the antecubital vein. The time was mentioned
as 0 hour. Then the patients received drug. They were requested to swallow the
tablet and have their breakfast according to their diet charts. Next blood sample
had been drawn at 30 min and 2 hour and then they were provided the drugs for the
whole month.
II.The patients were requested to take the drug just before the breakfast every
day for 29 days.
III.From the fasting blood sample 1ml of blood was transferred in an EDTA
containing tube for measurement of HbA1C and the rest of the blood was taken in an
EDTA containing tube and centrifuged immediately.
IV.Samples after processing were divided into two aliquots under sterile
condition;one aliquot was sent for biochemical analysis for Fasting glucose, Lipid
profile, Cholesterol, ALT, Insulin, Creatinine and another one was stored at -80
0C for further verification of results in case of any necessity.
7. Biochemical Test Methods:
I. Serum glucose (fasting, 1 and 2 hours) by Glucose Oxidase (GOD-PAP) method
(Randox Laboratories Ltd., UK).
II.Serum triglyceride by enzymatic colorimetric (GPO-PAP) method (Randox
Laboratories Ltd., UK).
III.Serum total cholesterol by enzymatic endpoint (Cholesterol Oxidase/
Peroxidase) method (Randox Laboratories Ltd., UK).
IV.Serum HDL cholesterol by enzymatic colorimetric (Cholesterol CHOD-PAP) method
(Randox Laboratories Ltd., UK) using micro-plate reader (Bio-Tec, ELISA).
V.Serum creatinine by enzymatic colorimetric (GPO-PAP) method (Randox Laboratories
Ltd., UK).
VI.Serum alanine amino transferase (ALT) by UV method using ALT (GPT) opt.kit
(Randox Laboratories Ltd., UK).
VII.Serum insulin by enzyme linked immunosorbent assay (ELISA) method (Linco
Research Inc., USA).
VIII.Glycosylated Haemoglobin (HbA1c) by High Performance Liquid Chromatographic
(HPLC) method.
8. Blood sample collection for DNA analysis (PPARG gene):
I.At the end of 3rd month of each treatment 1.5 ml of blood was taken in EDTA
containing tube for genetic analysis and the whole blood specimen was collected in the
vacuum collection tube containing EDTA, stored at -20 0C to - 80 0C.
II.DNA was isolated by Chelex method, identified by electrophoresis method and
amplified by using primers. We used a published document to select the primers for
genotyping PPARγ Pro12Ala/Pro12Pro. The primers for the Pro12Ala SNP genotype, we
amplified exon B using the reverse primer 5' CTG GAA GAC AAA CTA CAA GAG 3' and the
forward primer 5' ACT CTG GGA GAT TCT CCT ATT GGC 3'. (Sigma product, Order No. SIGMA
03/11/09 4152936-F/185 PPARG-R 8006875247-1).
III.Control DNA: Professor Colin Palmer Laboratory, Biomedical Research Institute
,University of Dundee Medical School, University of Dundee, Scotland, UK sent six
control samples of 3 types control DNA genotyped for PPARG SNP rs 1801282 (Pro12Ala).
IV.Restriction Digestion Enzyme Endonuclease Hae 111 was used to identify the cutting
site(Sigma Product No. R 5628).
3. Response Rate:
1. The response rate was defined by the decrease of ≥10% FBG or by the decrease of ≥1% HbA1c
from the baseline values.
ll.There was another response group was defined by the the HbA1c rate <7.0% after 3 months
treatment with metformin only to find out the secondary failure rate of metformin.
4) Statistical Analysis: I.Statistical analysis was performed using SPSS (Statistical
Package for Social Science) software for Windows version 18 (SPSS Inc, Chicago, Illinois,
USA). Data were expressed as mean + SD (Standard Deviation).
II. Effects of drugs after 3 months treatment were analyzed using t pair tests. The groups
were compared using one way ANOVA. If the p value was <0.05, the groups were compared using
the student's t test for unpaired samples or χ2 test through univariate analysis for further
verification. Correlation coefficient among the variables was tested using Pearson's test.
Multivariate logistic regression analysis was performed to obtain the odds ratios and
independent influencing factor for finding possible association between PPARγ genotypes and
drug response in case of genetic analysis.
III.A p value <0.05 was considered significant for all tests. lv. The statistical analysis
for within group study like PPARG response group and metformin secondary failure group has
not been displayed here.
5) List of Abbreviations
AEs Adverse Events
ALT Alanine aminotransferase
BMI Body Mass Index
BMRC Bangladesh Medical Research Council
BIRDEM Bangladesh Institute of Research and Rehabilitation in Diabetes,Endocrine and
Metabolic Disorder
BP Blood Pressure
DNA Deoxynucleic Acid
DBP Diastolic Blood Pressure
DM Diabetes Mellitus
EASD European Association for the Study of Diabetes
EDTA Ethylene Diamine Tetra Acetic acid
ELISA Enzyme Linked Immunosorbent Assay
FBG/FSG Fasting Blood Glucose/Fasting Serum Glucose
FSI Fasting Serum Insulin
2hBG 2 hours Blood Glucose
HbA1c Glycosylated Haemoglobin
HOMA percent B Homeostasis Model Assessment percentage of beta cell function HOMA percent S
Homeostasis Model Assessment percentage of sensitivity
HOMA IR Homeostasis Model Assessment Insulin Resistance
HDL-C High Density Lipid Cholesterol
IU/L International Unit/Litre
LDL-C Low Density Lipid Cholesterol
ml millilitre
mm millimetre
mg/dl milligram/ decilitre
MLR Multiple Logistic Regression
OPD Outdoor Patient Department
OMIM Online Mendelian Inheritance in Man
OR Odds Ratio
PPARγ Peroxisome Proliferator Activated Receptor gamma
Pro12Pro Proline12Proline
Pro12Ala Proline 12 Alanine
Ala12Ala Alanine12Alanine
PCR Polymerase Chain Reaction
QUICKI Quantitative Insulin sensitivity Check Index
SD Standard Deviation
SPSS Statistical Package for Social Science
SBP Systolic Blood Pressure
TC Total Cholesterol
TG Triglyceride
T2DM Type 2 Diabetes Mellitus
TZD Thiazolidinedione
µl Microliter
WHO World Health Organization
;
Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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