Diabetes Type 2 Clinical Trial
Glycemic control is fundamental in the management of diabetes mellitus .If lifestyle intervention and full tolerated doses of one or two oral glucose lowering drugs (OGLDs) fail to achieve or sustain glycemic goals, insulin should be initiated. New insulin analogs are generated to improve glycemic control .New insulin analogs are generated to improve glycemic control,However, the cost of these analogs is a major problem .The aim of this piggy back evaluation was to assess the effect of BIAsp 30 versus NPH plus regular human insulin on metabolic control as well as its cost-effectiveness in people with type 2 diabetes in the Iranian setting.
Study design and participants This was a randomized controlled clinical trial of 48 weeks on
subjects with T2DM between July 2011 and October 2012. Two hundred and four diabetic
subjects aged 28-65 years were included in the study. Subjects had A1C >8.0% and had
indication for starting insulin. They were randomly allocated to two groups using a simple
randomization method. Any current and prior medications were acceptable for inclusion of
participant except any type of insulin being evaluated. Demographic and anthropometric
variables were recorded. Hypoglycemia events and laboratory data including FPG, HbA1c and
lipid profiles were measured every three months. In addition, quality of life was assessed
with self-administered standard EQ-5D questionnaire (Brooks, Rabin et al. 2003).
Subjects were excluded for any of the following criteria: Alteration in insulin sensitivity
such as major surgery, infection, renal failure (Glomerular Filtration Rate < 50),
glucocorticoid treatment, recent (within 2 weeks) serious hypoglycemic episode (requires
assistance of another), simultaneous participating in another clinical study, using any type
of insulin, sight or hearing impaired, active proliferative retinopathy or maculopathy
require treatment within 6 months prior to screening, breast feeding, pregnancy or nursing
of the intention of becoming pregnant or not using adequate contraceptive measures.
The study was approved by ethics committee of Tehran University of Medical Sciences and was
recorded in IRCT (IRCT code: 201112038282N1). All eligible subjects agreed and signed
written informed consent after full explanation of the purpose and nature of all procedures
used. All patients were free to withdraw at will at any time.
Assessments and outcome measures The insulin therapies were prescribed by a single physician
in the clinic. The starting dose of BIAsp 30 (NovoMix® 30-pen, NovoNordisk) was 0.2-0.6
unit/kg per day in 2 divided doses according to level of glycemia in the intervention group.
The control group received NPH/Reg insulin (from Exir pharmaceuticals, Lorestan, Iran) in a
Ratio of 2:1 with initiation dose of 0.2-0.6 unit/kg in 2 divided doses. Two-thirds of the
dose was given before breakfast and the remainder before dinner in NPH/Reg insulin group.
Changes to oral glucose lowering drugs (OGLDs) at the time of starting the insulin analog,
or thereafter, were entirely at the discretion of the participant and physician. Para
clinical data were measured in a referral laboratory every three months. After an overnight
fast of at least 12 hours, blood samples were obtained for measurement of fasting blood
sugar (FBS) using a the glucose oxidase method, lipid profileswere determined using
enzymatic methods. These measurements were conducted using commercial Parsazmun kits
(Tehran, Iran) and a Hitachi 704 automatic analyzer (Tokyo, Japan)(Lentjes, Harff et al.
1987). HbA1c was measured using the high performance liquid chromatography
method(Esteghamati, Jamali et al. 2010). Post prandial blood glucose (PPG) was measured two
hours after breakfast using a glucose analyzer (YSI 2700 Select, YSI, Inc., Yellow Springs,
OH).
Trial visits were defined as 0, 12, 24, 36 and 48 weeks from baseline. All participants were
asked to record their 7-point blood glucose values in three consecutive days before each
visit. Seven-point self-monitoring blood glucose includes three pre-meals, three post-meals,
and bedtime blood glucose values during each day. Insulin doses were adjusted by a titration
regimen according to self-monitored blood glucose. For both groups, treatment goals were as
follows: fasting blood glucose of 80-120 mg/dl, postprandial glucose <160 mg/dl, A1C<7% and
the before dinner blood glucose target for the NPH/Reg insulin group was 100 mg/dl, with a
stepwise increase of both type of insulin depending on the pre-meal blood glucose values to
achieve targets for plasma glucose (PG)as follows: +2 IU/day where 126 mg/dl < PG < 140
mg/dl, +4 IU/day where 140 mg/dl < PG < 160 mg/dl, +6 IU/day where 160 mg/dl < PG < 180
mg/dl, +8 IU/day where 180 mg/dl < PG < 200 mg/dl and +10 IU/day where PG > 200
mg/dl(Hermansen, Davies et al. 2006; Liebl, Prager et al. 2009), unless symptoms of
hypoglycemia occurred. Hypoglycemia was defined as blood glucose <70 mg/dl. Severe
hypoglycemia was defined as an event with symptoms consistent with hypoglycemia where the
individual required the assistance of another person and was not treated with oral
carbohydrate due to confusion or unconsciousness and was associated with a blood glucose
level <40 mg/dl with recovery with intravenous glucose, or glucagon administration.
Nocturnal hypoglycemia was defined as hypoglycemia occurred at night and which commonly
known as hypoglycemia while asleep.
Data were collected from the physician's clinical notes and participants' recall and
self-monitoring blood glucose values at each visit.
Costs
Direct medical costs:
We collected medical costs of each patient by a checklist. All patients had been asked to
refer to the clinic every one month during the study. Clinical events or hospital episodes
and also all related costs were determined at each visit. Any pharmaceutical,
laboratory/diagnostic and rehabilitative care, as well as any contact with specialists,
general practitioners, nurses, opticians, and dieticians were recorded for patients
with/without complication. Finally total costs were calculated.
Direct nonmedical costs Any services such as transportation for patients and their family to
clinic and taking care of dependents were assessed for non-medical expenditures by a patient
self-estimate questionnaire.
Indirect costs The lost productivity costs due to health problems of DM were determined by
days absent from work, poor work performance, low earnings capacity from disabilities, and
mortality. We calculated number of days in each visit that the patient could not be present
in their job because of DM related health care. The average net hourly wage was asked from
each patient. For unemployed patients, we considered average wage of population who were
economically active and in employment (Javanbakht, Baradaran et al. 2011). Lost earnings
owing to premature mortality were defined as the mortality costs. Costs from the health
provider perspective, were converted from Iranian Rials (IRR) into USA dollar (USD) at an
official exchange rate of 12,260 IRR/1USD 2012 to have an international comparison (Central
Bank of Iran).
Utility calculation Utility scores were calculated with two recent well known
measurements;EQ-5D and EQ-VAS between 0-1.These are two standardized measures of health
status and quality adjusted life year (QALY), developed by the EuroQol group in order to
provide a simple, generic measure of health for clinical and economic appraisal (1990).
Cost Effectiveness Analysis Hypoglycemic events and QALYs were considered as outcomes and
the incremental cost effectiveness ratio (ICER) per patient was calculated according to the
below formula: ICER= ∆Cost/ ∆Outcome (Rasccati Karen L. 2009).The comparison of ICERs was
held afterwards per each outcome.
Analysis All data are presented as mean ± standard deviation (SD). Significant differences
in general characteristics were determined by Chi-square and Student's t-test. Change from
baseline HbA1c, FBS, PPBG, and blood lipids was analyzed using an analysis of variance
(ANOVA) model with baseline characteristics as variates. SPSS for Windows (Version 14; SPSS
Inc., Chicago, IL) was used for data analyses and P values < 0.05 were considered
statistically significant.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Subject), Primary Purpose: Treatment
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