Diabetes Mellitus Clinical Trial
Official title:
Hospital Based Pilot Study: Association of Kisspeptin Levels With Insulin Secretion in Diabetes Mellitus
Since the discovery of kisspeptin as a "gate-keeper" of hypothalamo-pituitary-gonadal axis,
there has been tremendous interest in the molecule. The relevance of kisspeptin as
regulatory molecule for the reproductive system has been well documented in significant
number of trials. (1, 2) This leads to the possibility that kisspeptin could be involved in
an equally pivotal role in the other sites, where it is located, namely pancreas.
While various animal experiments have suggested that kisspeptins regulate insulin secretion,
we do not know if this is also true in humans. The investigators hypothesize that kisspeptin
levels are significantly low in individuals who have low endogenous insulin secretion.
While various animal experiments have suggested that kisspeptins regulate insulin secretion,
the investigators do not know if this is also true in humans. Investigators hypothesize that
kisspeptin levels are significantly low in individuals who have low endogenous insulin
secretion.
Thus investigators are conducting this study to understand the link between endogenous
insulin secretion and kisspeptin levels among individuals with various levels of insulin
secretory defect as seen in diabetics. Investigators believe that this will help understand
the physiologic mechanisms, and kisspeptin based insulin regulation among individuals with
diabetes mellitus.
INTRODUCTION:
Since the discovery of kisspeptin as a "gate-keeper" of hypothalamo-pituitary-gonadal axis,
there has been tremendous interest in the molecule. Kisspeptins are a group of peptides
derived from the kiss gene, which share a common C-terminal decapeptide with an
arginine-phenylalanine residue at the amino terminal.(1, 2) These peptides and their target
receptor GPR54 are highly expressed in hypothalamus, anterior pituitary, islets of
langerhans, and gonads. (2-5) The relevance of kisspeptin as regulatory molecule for the
reproductive system has been well documented in significant number of trials. (6, 7) This
leads to the possibility that kisspeptin could be involved in an equally pivotal role in the
other sites, where it is located, namely pancreas.
Investigators have demonstrated that kisspeptin plays a role in regulating beta cell
activity.(8) Despite previous conflicting results suggesting glucose mediated insulin
secretion and insulin inhibition in different studies,(9, 10) current evidence favours role
of kisspeptin in glucose mediated insulin secretion.(11) One of earliest evidence of
relation of insulin resistance with falling kisspeptin levels was demonstrated by Panidis et
al in 2006.
While various animal experiments have suggested that kisspeptins regulate insulin secretion,
we do not know if this is also true in humans. The investigators hypothesize that kisspeptin
levels are significantly low in individuals who have low endogenous insulin secretion.
Thus investigators plan this study to understand the link between endogenous insulin
secretion and kisspeptin levels among individuals with various levels of insulin secretory
defect as seen in diabetics. We believe that this will help understand the physiologic
mechanisms, and kisspeptin based insulin regulation among individuals with diabetes
mellitus.
Researchers have also noted that the mechanism of stimulating glucose induced insulin
release, is similar to the GLP1(Glucagon like peptide) action.(10) It would be interesting
to ascertain a correlation between the two peptides with potentially similar action in
insulin physiology. Leptin has been shown to alter kiss-1 expression in animal models.
Establishing a link between leptin levels with kisspeptin in humans would help us identify
further potential therapeutic targets involved in the multisystem manifestations of
diabetes.(12)
AIMS AND OBJECTIVES:
1: To explore the association between levels of fasting insulin and kisspeptin levels, in
diabetes mellitus.
2. To explore association between Obesity and Kisspeptin levels. 3. To explore the
association between kisspeptin and GLP-1 levels. 4. To explore the association of leptin and
kisspeptin levels.
RESEARCH QUESTION:
In a population of adults attending the outpatient diabetes and medicine clinic of a
tertiary care hospital, Do those with diabetes mellitus as compared to those without
diabetes mellitus, have progressively lower kisspeptin levels, and is this gradient in
Kisspeptin levels related to fasting endogenous insulin secretion. Investigators hypothesize
low Kisspeptin levels to be associated with low insulin secretion.
STUDY TYPE- STUDY DESIGN: Cross-sectional study Ethical approval for the trial protocol
obtained from the institute's ethics committee of Care Hospital, Nagpur, India
Subjects and Methods The study will be conducted in CARE Hospital, Nagpur from 1 September
2013- 31 November 2013. Patients will be selected to enter the study, in such a way that
every patient presenting to the diabetes and medicine clinic will be screened in the study
and patients fulfilling inclusion criteria will be recruited in the study.
Study population:
Total of 60 patients will be included in the study. Investigators plan to include Diabetics
without exogenous insulin supplementation, Diabetics with exogenous insulin supplementation
and normal healthy cohorts, 20 in each group.
Methods:
The investigators will screen all patients who are referred to them after fulfilling the
inclusion and exclusion criteria in the study. Written informed consent will be obtained
from all participants. The patients included in the study will be administered a
standardized questionnaire to record socio-demographic characteristics, details of diabetes
management, history of PCOD (Polycystic Ovarian Disease), history of hypogonadism or any
obvious sexual dysfunction drug history. A general examination for BMI (Body mass index),
waist hip ratio and Blood pressure would be performed. Blood samples will then be withdrawn
(8 ml : 2ml fluoride tube, 2ml EDTA (ethylenediaminetetraacetic acid ), 4 ml plain tube)
after overnight fasting for creatinine, fasting blood glucose, fasting insulin, C-peptide
levels, HbA1C (glycosylated haemoglobin), LH (luteinizing hormone), FSH (Follicle
stimulating hormone), and kisspeptin levels. In female patients samples will be collected
between day 3 to day 6 of a normal menstrual cycle. After a usual meal as regularly taken by
the patient, samples (8ml: 2ml fluoride, 4ml EDTA and 2 ml plain tube) for post-prandial
blood glucose level, insulin level, leptin level, GLP-1 level and kisspeptin levels will be
collected. The blood samples for creatinine, glucose (pre and post), insulin levels, HbA1C,
LH and FSH will be analysed immediately in the laboratory. The blood samples for kisspeptin
levels, GLP-1, leptin levels will be collected in a separate EDTA tube, centrifuged for 15
min at 4 degree and plasma will be stored separately in a deep freezer at -70 degree. The
concentration of kisspeptin will be measured using Kiss¬peptin-10 (Metastin [45-54]-Amide)
and competitive enzyme immunoassay (Kit# EK-048-56, Phoenix Pharmaceuticals, Inc.,
Burlingame, CA, USA). Leptin (Human) ELISA Kit Protocol (Cat. No.: EK-003-12, Phoenix
Pharmaceuticals) will be used for serum leptin levels. GLP-1 (7-36)-Amide (Human,Rat, Mouse)
EIA (enzymeimmunoassay) Kit (Catalog # EK-028-11, Phoenix Pharmaceuticals) will be used for
testing GLP 1 levels. The method given in the product insert will be used for the assays.
Power analyses There is no similar study done to help us predict the power of study. As the
investigators did not have previous estimates no formal power calculation was undertaken.
The investigators randomly decided to take 60 patients in the study, 20 in each arm.
Data analysis All data will be entered using MS excel. Researchers will perform a
descriptive statistical analysis of the baseline data. The analyst, who will be blinded to
the laboratory results, will compare the outcome measure using Pearsons coefficient of
correlation. All statistical analysis will be done using SPSS software (v.16.0 SPSS, Inc.,
Chicago, IL) Dissemination The results of this trial are expected to provide evidence and
clinically relevant information the relation between kisspeptin and diabetes.
Risks of participation The investigators believe there is no additional risk for the
participants included in the study.
Competing interests The authors declare that they have no competing interests.
;
Observational Model: Case Control, Time Perspective: Cross-Sectional
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