Diabetic Neuropathic Pain Clinical Trial
Official title:
Clinical Study on the Improvement of Diabetic Neuropathic Pain by Liraglutide
Diabetic neuropathic pain is a common clinical manifestation of diabetic neuropathy, which seriously affects the quality of life of patients. The clinical treatment is limited and the curative effect is not good. In the previous animal studies, investigators found that the change of pain threshold in diabetic rats showed a staged change, and was significantly related to the change of brain microglia activity. It was confirmed that liraglutide could regulate the activation of microglia in vitro. Then investigators found that it could intervene diabetic neuropathic pain through the intervention of liraglutide in diabetic rats. In the early stage of clinical observation, the investigators also preliminarily observed that liraglutide can intervene diabetic neuropathic pain. At present, liraglutide is a commonly used hypoglycemic drug in clinic. Therefore, on the basis of previous studies, this study intends to select diabetic neuropathic pain patients whose blood sugar is not up to the standard, and give Mecobalamin to treat diabetic neuropathy. In addition, on the basis of the original hypoglycemic treatment, participants are randomly divided into one group to give liraglutide, one group to increase or adjust insulin, with similar blood glucose level. The improvement of diabetic neuropathic pain was observed. The aim of this study was to evaluate the safety and efficacy of liraglutide in improving diabetic neuropathic pain.
1. Diabetic neuropathic pain seriously affects the quality of life, clinical problems are
difficult, and new treatment methods are urgently needed.
Diabetic neuropathy is one of the most common complications of diabetes mellitus. The study
of investigators shows that the prevalence rate of diabetic neuropathy diagnosed in downtown
Shanghai is as high as 61.8%. The most common type of diabetic peripheral neuropathy is
distal symmetric polyneuropathy, which is the main cause of diabetic neuropathic pain (DNP).
Diabetic neuropathic pain can affect about one fifth of diabetic patients, which can lead to
the decrease of daily activities, even the loss of work, severe depression, and quality of
life. The pathogenesis of diabetic neuropathic pain is complex and not yet fully clear, so
there is a lack of available and effective treatment. At present, the first-line clinical
treatment drugs include pregabalin, duloxetine, amitriptyline, gabapentin and venlafaxine,
etc., and these drugs sometimes relieve the symptoms of diabetic neuropathic pain not
obvious, and have more side effects, which has become a difficult problem in clinical
treatment. Therefore, it is urgent to explore effective drugs for diabetic neuropathic pain.
2. The clinical observation and animal study of the investigators show that the GLP-1
receptor agonist (liraglutide) can improve diabetic neuropathic pain.
1. Diabetic neuropathic pain is related to brain microglia. In the animal model of diabetes
mellitus, investigators found the phenomenon of abnormal activation of microglia.
Previous studies showed that the abnormal activation of microglia at the level of spinal
cord was closely related to diabetic neuropathic pain, and microglia at the level of
spinal cord played an important role in the transmission of pain. As the center of pain
loop, the activity of microglia in cerebral cortex and thalamus is less related to
diabetic neuropathic pain.
Therefore, investigators used STZ induced diabetic neuropathy model of SD rats. Before
STZ injection (0 week), at the 2nd, 4th, 6th and 12th week after STZ induced
hyperglycemia. The investigators monitored the changes of body weight, blood glucose
level and pain threshold of mechanical pain and thermal pain in rats. The investigators
used [18F] dpa714 specific marker transfer protein TSPO to carry out PET / CT scan of
brain to reflect microglia in each brain area. After PET / CT scan, EMG was used to
evaluate the degree of peripheral nerve injury. The results showed that after STZ
injection, compared with the control group, the blood glucose of STZ group increased
gradually, and with the increase of blood glucose, the nerve conduction velocity of
diabetic rats decreased gradually. Mechanical pain decreased significantly in 4-6 weeks,
thermal pain threshold decreased significantly in 4 weeks, and mechanical pain and
thermal pain sensitivity disappeared in 12 weeks. The results of PET / CT showed that in
cortex, hippocampus, thalamus, hypothalamus and pituitary, dpa714 standard uptake value
was significantly higher than other time points in the fourth week, and significantly
higher than that in the control group. The correlation analysis indicated that the pain
threshold of thermal pain was significantly related to the activity of microglia in
thalamus and hypothalamus. Previous studies have shown that hyperglycemia can induce
neuropathic pain. Thermal hyperalgesia occurs 4 weeks after hyperglycemia, while
mechanical hyperalgesia occurs 4-6 weeks. PET / CT study showed that the activity of
microglia in the brain of diabetic rats increased in the fourth week, and the activity
of microglia was significantly related to the occurrence of heat pain. It has not been
reported that the relationship between the activity of microglia and diabetic
neuropathic pain was directly observed by PET / CT.
2. Liraglutide can regulate the activation of microglia Glucagon like peptide 1 (GLP-1)
acts by binding to GLP-1 receptor, which is a G protein coupled receptor. A large number
of studies have shown that GLP-1 receptor agonists can improve the activation of
macrophages, microglia as macrophages in the brain, and GLP-1 receptor agonists can
improve the activation of macrophages. However, few studies have shown that in vitro
cultured astrocytes and microglia, GLP-1 analogues can change the morphology of glial
cells, reduce IL-1 β and increase cAMP level at mRNA level.
Therefore, liraglutide, the GLP-1 agonist, was selected as the intervention drug . BV2
microglia cell line was used as the following treatment methods: liraglutide was co
cultured with LPS or high glucose, and liraglutide was added after LPS and high glucose
induced activation. After treatment, the levels of IL-6 and TNF - α in the supernatant
of the cells were observed. The results showed that liraglutide was added in advance
before induction and activation. Or the level of IL-6 and TNF - α released by BV2 could
be significantly reduced by using liraglutide. Therefore, liraglutide can regulate LPS
and high glucose induced microglia activation.
3. Animal experiments show that liraglutide can improve diabetic neuropathic pain. On the
basis of previous work, the investigators further studied the effect of liraglutide on
diabetic neuropathic pain at the animal level. SD rats were divided into three groups:
normal blood glucose group, normal saline control group and 200ug / kg / dliraglutide
injection group. The latencies and thresholds of thermal and mechanical pain were
monitored weekly. It was observed that for diabetic neuropathic pain rats, the
peripheral injection of GLP-1 receptor agonist (liraglutide 200ug / kg / D)
significantly increased the thermal pain threshold at 4 weeks, the mechanical pain
threshold at 8 weeks, and the pain sensitivity disappeared at 12 weeks in both the
normal saline control group and the liraglutide injection group.
4. Observation of clinical cases In clinical work, the investigators observed some obese
patients with neuropathic pain in type 2 diabetes mellitus. In the process of using
GLP-1 receptor agonist to control blood glucose, the symptoms of pain were also
significantly improved. In addition, a clinical study showed that the use of sitagliptin
(DPP-IV inhibitor, which can inhibit the degradation of GLP-1 in vivo) can also improve
diabetic neuropathic pain. However, these observations and studies have significant
limitations, not excluding the effect of blood glucose lowering itself in the population
level, nor exploring the mechanism.
3. The clinical study of liraglutide in improving diabetic neuropathic pain has better
clinical value.
The investigators found that liraglutide can improve the activation of microglia, and it can
significantly alleviate diabetic neuropathic pain at the animal level and clinical cases. The
systematic study of liraglutide used to improve neuropathic pain in diabetic patients has not
been reported, and this subject has better clinical value.
Therefore, considering the hypoglycemic effect of liraglutide on the basis of previous
studies, the investigators plan to select diabetic neuropathic pain patients whose blood
sugar is not up to standard in this study, and give Mecobalamin (one of the commonly used
drugs recommended in the guidelines for prevention and treatment of diabetes mellitus to
treat neuropathy). At the same time, on the basis of the original hypoglycemic treatment,
participants were randomly divided into one group to be given liraglutide and the other group
to be increased/adjusted insulin. After 3 months, the improvement of diabetic neuropathic
pain in the two groups under the condition of similar blood glucose level were observed. The
purpose of this study was to evaluate the safety and efficacy of liraglutide in improving
diabetic neuropathic pain.
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