Diabetes & The Endocannabinoid System: Prospects For Therapeutic Control
By:
Matthew Schnur
Quick Outline
• This will be a very detailed discussion, so lets put it in perspective
• First we'll discuss causes of diabetes
• Then move on to insulin receptor signaling and defects in this mechanism
• Next we will focus on the PPARγ and cannabinoid CB1 & CB2 receptors
• Finally, it will all be tied together; how cannabinoid therapy treats the symptoms of Type 1 & Type 2 Diabetes

Diabetes Background
• Over 28 million Americans have diabetes (Type 1 or 2)
• 80% of cases are diagnosed as Type 2
• The leading cause of blindness and amputations
• Diagnosed cases are rising exponentially-directly related to diet
• For every kg bodyweight over healthy BMI, a 7% increase in getting Type 2 is found
What is Diabetes?
• Type 1 (Diabetes Mellitus)

– An autoimmune disorder characterized by islet β-cell destruction 

– Plasma glucagon levels may be increased

– No detectable plasma insulin
What Is Diabetes?
• Type 2 (Diabetes Insipidus)
– Often environmentally induced in predisposed individuals
– Characterized by:
• Obesity		
• Impaired IRS phosphorylation
• Impaired PI3K activity
• Impaired GLUT-4 translocation
• Increased FFA

Common Attributes To Both
• Both Type 1 and 2 patients have;
– Hypo/hyperglycemia
– Dyslipidemia
– Decreased immune function
– Poor wound healing
– Microangiopathies
• Neuropathy, retinopathy, nephropathy
– Depression & weight gain
• Both attributable to inflamm. TNFα, IL-2, and IL-6
Causes of Diabetes
• Type 1:
– Only 30% identical twins will both have it
– MHC genes on chromosome 6
• Of 21 known DR alleles, DR3 & DR4 found in 95%
– β-cell autoantibodies
• Directed against GAD (glutamic acid decarboxylase), unique to β-cells
Causes of Diabetes
• Type 2
– A variety of theories, we'll focus on PPAR based
– Interruption of lipid homeostasis
- Leads to increased FFA
- FFAs normally decreased by PPAR activation
2.  Activation of inflammatory cytokines normally suppressed by PPAR
Insulin Receptor Signaling
1.  Insulin binds to the heterotetrameric IR (Insulin Receptor)
	- Causes autophosphorylation of tyrosine residues

2. Tyrosine autophosphorylation causes dissociation of IRS-1 (Insulin Receptor Substrate-1)
	- 4 IRS proteins;
		* IRS-1 - immediate activation 	       of PI3K
		* IRS-2 - prolonged activation of 	        PI3k
		* IRS-3 & -4 - inhibit PI3K 	  	        activation


Insulin Receptor Signaling
3.  Activation of PI3K
	- Responsible for:
	     * Activ. of Akt/PKB  (serine 	  	      phosphorylation)
	     * GLUT-4 translocation
4.  Activation of Ras/Raf
	- Both PKB mediated or directly IRS     	activated
	-Activates the MEK- ERK1/2 	pathway
5.  MEK & ERK1/2 Pathway
	- Responsible for glycolysis & 	protein synthesis
	- Activation of PPARγ
Insulin Desensitization
• Besides tyrosine autophosphorylation, the IR has;

	- Both serine & threonine residues capable of 	autophosphorylation

	- Upon excess agonist activity, serine/threonine autophosp. causes a dissociation of IRS-1 without activation

	- Results in loss of function IR, or only activation of IRS-2
		* This is why we see ͺ IRS-2 activity in both Types

 

Insulin Desensitization
• Increased Fatty Acids
- Elevated FFAs lead to accumulation of
	* DAG		*fatty acyl-CoA
	* ceramide
- These compounds are known to activate membrane bound PKCθ
- PKCθ causes serine phosphorylation of IRS-1 in lieu of IR mediated IRS-1 tyrosine phosphorylation
	* Serine phosphorylation causes a dissociation 	between IRS-1 & PI3K

Insulin Resistance
3.  TNFα and inflammatory adipokines
	- Chronic exposure to TNFα to 3T3-L1 adipocytes 	resulted in 90% " in GLUT-4 mRNA
	- TNFα has been found to:
		* Repress expression of IRS-1 & GLUT-4
		* Induce serine phosphorylation of IRS-1
		* Increase FFA plasma levels
	- TNFα levels >2.5x higher in both Type 1 & 2 than in	healthy patients

PPARγ
• Peroxisome-proliferator activated gamma (PPARγ)
• A nuclear receptor when activated dimerizes with retinoic X receptor
• A downstream mediator of IR - MEK- ERK1/2 pathway
• Both PPARγ & retinoic X receptor activation shown to enhance insulin sensitivity
• Ligands include mono- & poly-unsaturated fatty acids, PGs, the most commonly prescribed Type 2 diabetes medications thiazodolines (TZDs), and  some NSAIDs (possible breakdown to AM404)
Functions of the PPARγ
• Originally discovered to inhibit lipid peroxidation
• Agonist activity found to down regulate TNFα gene
• Stimulates adipocyte differentiation & apoptosis
– Beneficial mostly for Type 2
• Represses gene expression of chemokines involved in 	insulin resistance:
• Leptin			* Plasminogen activator-inhibitor-1
• Resistin		* IL-6 & IL-11
• Induces gene expression of insulin sensitizing factors:
• Adiponectin		* Fatty acid transport protein
• IRS-2
The Endocannabinoid System
• The CB1 & CB2 receptors are the most abundant G-protein coupled receptors in the human body
• Besides CB1 & CB2 endo- & phyto- cannabinoids also bind to the PPARγ and TRPV1 vanilloid receptor
– The vanilloid receptor is expressed both in the islet β-cells and smooth muscle cells
– Vanilloid receptor activation found to enhance insulin secretion and sensitivity
• Anandamide (arachidonylethanolamide) & 2-AG (arachidonylglycerol) are endocannabinoids
– These are under negative control of leptin

Endocann. Continued
– Leptin is a hormone secreted by adipose tissue and exerts its effects in the hypothalamus

– As previously mentioned, leptin increases insulin resistance

– Endocannabinoids are down-regulated by leptin
• Leptin causes an inhibition in the MAPK stimulated glycogen synthase activity of the CB1 receptor


The Cannabinoid Receptors
• The CB1 & CB2 receptors
– Both GPCR with Gαi/o coupling
– CB1 also has Gαs coupling ability under certain conditions
– Both coupled to activation of the PI3k-Akt/PKB pathway
– Both receptors shown to activate MAPKs via the Ras/Raf pathway
• P38 & p42/p44 MAPKs activated
• Shown to increase glycogen storage, glucose metabolism, c-fos expression
CB Receptors Continued
– Both receptors found to activate PLC
• PLC cleaves IP3
• IP3 releases Ca2+ from intracellular storage vesicles
– CB1 receptor also shown to inhibit K+ outflow & Ca2+ efflux
– CB2 not coupled to ion channels
CB & IR Interactions
CB Agonists
• Thus CB1 activation beneficial to insulin sensitivity and glucose metabolism
• CB2 is found predominantly in immune cells & adipocytes
• CB2 activation in B-cells, macrophages, T-cells, and monocytes is found to:
– Reduce TNFα, IL-2, IL-6, and IL-11; all elevated in diabetics and correlated to insulin resistance
– Balance Th1/Th2 inflammatory cell profile
• Autoimmune Type 1 diabetes has ͺ activation of TH1/TH2
• IFN-γ, IL-12, and TNFα associated with ͺ TH1, treatment with THC showed a marked decrease in mRNA levels of all
CB Receptors & β-Cells
• Insulin secretion by β-cells follows an oscillatory pattern
– Stimulated by ͺ &" pattern of intracellular Ca2+
• Receptor localization:
– CB1 found mostly on α-cells
– CB2 found on both α- & β-cells
– TRPV1 also found on β-cells
• Cannabinoids found to/may:
– Reduce insulin secretion (metabolic syndrome X)
– CB1 may reduce cAMP dependent release of glucagon
– Enhance effects of insulin signaling

CB Receptors & β-Cells
• The Evidence:

– Anandamide & 2-AG concentration in β-cells ͺ under hyperglycemic conditions and decreases under hypoglycemic conditions

– Administration of insulin " endocannabinoid levels

– Chronic activation of CB1 leads to up-regulation of PPARγ (in adipocytes)

– Personal data: 
• Smoking + insulin = ~18%> reduction in BGL
• Smoking alone = ~8% reduction
• No reduction when large quantities cannabis used + food
• Dangerous enhancement between exercise + cannabis + insulin combination can reduce insulin by 1/5

Non-CB Mediated Effects
• Both endo- & phyto- cannabinoids bind to the PPARγ receptor
• Diabetics have a marked reduction in immune function & O2 transport
- IgA glycosylation 4x ͺ in both types of diabetics w/o complications, 33% more in Type 1
- IgM glycosylation ͺeven in healthy diabetics, 8% more in Type1
- Healthy individuals have 1-3% hemoglobin glycosylation, uncontrolled diabetics 20% (diagnostic tool HbA1c)
- Poor O2 transport by Hb leads to microangiopathies
- Other long lived proteins also get glycosylated; collagen, albumin, myelin
Non-CBR Mediated Effects
– Since protein glycosylation is an oxidative process, antioxidants have proven useful
• Preventative effects of Cannabis derived antioxidants on Hb glcosylation at [.5], [5], and [10]μg
– Quercitan (flavanoid) 3%, 37%, 52%
– Kaempferol (terpenoid) 10%, 12%, 15%
– 20 other flavanoids, also THC, CBD, CBC, and CBG all have antioxidant properties
– Hb glycosylation a Fenton Reaction
• NIH published paper on cyclic voltammetry & rat focal ischemia model:  THC 20X potent the antioxidant than ascorbate
3.  Cannabinoids (CBD) protect against myelin degradation, and excessive glutamatergic firing, a cause of one type of diabetic neuropathy (sensory)
	- NMDA receptor induced intracellular Ca2+ accumulations cause neurotoxicity

Diabetic Retinopathy
• 2 Phases:

- Nonproliferative
• Neovascularization - resp. for
dev. of new blood vessels in
many tissues, especially the retina
• Growth mediated by VEGF

- Proliferative phase
• Advanced stages of retinopathy
• Neovasc. Causes optic nerve damage & macular edema
• Leading cause of blindness
• 3/4 all diabetics after 15 yrs
Retinopathy
• The VEGF Pathway
– Also actiavtes the PI3K-AKT/PKB pathway (like the CB receptors)
– Also activates the Ras/Raf dep. MAPK pathway just like the CB receptors
– Yet again, also activates the PLCγ-PKC pathway, and IP3 mediated intracellular Ca2+ release, like the CB receptors
– How then, can cannabinoids be beneficial?

Retinopathy & The CB Receptors
How Cannabinoids Benefit Retinopathy:
• Remember, 20 flavanoids + cannabinoid are antioxidants
- The eye is rich with FFAs which are subject to oxidation (COX-2), typically elevated in diabetics
- Cannabinoids prevent superoxide anion formation, and increase fatty acid metabolism
- VEGF
        -        While VEGFR2 & CB receptors share nearly identical transduction   	 	  mechanisms, cannabinoids inhibit VEGF gene transcription via other 	 	  receptors, may not share similar phosphorylation patterns
        -        TNFα increases VEGF mRNA, as does the Ils that are inhibited by CB 	  activation
- PEDF
        -        Pigment epithelial derived factor, a potent inhibitor of neovascukaarization via 	  VEGF
        -        PEDF is inhibited by oxidative stress & TNFα

Conclusions
• Diabetes is a simple disorder with complex pathways regulating insulin resistance/sensitivity and secondary pathology 
• Nearly all complications to diabetes are the result of hyperglycemia
• After reviewing the IR, PPARγ, CB1, CB2, and VEGF, we find that cannabinoid therapy for diabetes can:
• Reduce BGLs		2.  Reduce HbA1c
• ͺ insulin sensitivity	4.  ͺ glucose & lipid metabolism
• Prevent retinopathy	6.  Inhibit inflammatory chemokines
• Neuroprotection	8. Improve O2 transport 
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