Antidiabetic drug-1

Antidiabetic Drug 2019

ANTIDIABETIC DRUG
1 Introduction:
Anti-diabetic drug, any drug that works to lower abnormally high glucose (sugar) levels in
the blood, which are characteristic of the endocrine system disorder known as diabetes mellitus.
Diabetes is caused by the body’s inability to produce or respond to the pancreatic
hormone insulin. One of the important physiological actions of insulin is to control blood
glucose levels. Glucose is an important nutrient for cellular metabolism, and cells must receive
neither too little nor too much. A deficiency in the pancreatic secretion of insulin, or lack of
tissue sensitivity to the hormone, leads to diabetes, the primary feature of which is elevated
blood glucose levels (hyperglycemia).
There are a number of different types of antidiabetic drug including:
1) Insulin
2) Pramlintide (Amylin)
3) GLP-1 receptor agonists (such as Byetta and Victoza)
4) Oral hypoglycemics (tablets)
2 Classification:
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2.1 Overview of Antidiabetic drug:
Class Mechanism of action Side effects Contraindications
Biguanide (metformin) Enhances
the effect of insulin
Lactic acidosis
Weight loss
Gastrointestinal
complaints are
common (e.g. diar
rhea, abdominal
cramps)
Reduced vitamin
B12absorption
Chronic kidney disease
Liver failure
Metformin must be
paused before
administration of
iodinated contrast
medium and major
surgery.
Sulfonylureas (e.g., glyburid
e, glimepiride)
Increase insulin secr
etion
from pancreaticβ-cel
ls
Risk
of hypoglycemia
Weight gain
Hematological
changes: agranulo
cytosis, hemolysis
Severe cardiovascular
comorbidity
Obesity
Sulfonamide allergy (par
ticularly long-acting sub
stances)
Meglitinides (nateglinide, rep
aglinide)
Increase insulin secr
etion
from pancreaticβ-cel
ls
Risk
of hypoglycemia
Weight gain
Severe renal
or liver failure
DPP-4
inhibitors (saxagliptin, sitagli
ptin)
Inhibit GLP-1 degra
dation →
promotes glucose-de
pendent insulin secre
tion
Gastrointestinal
complaints
Pancreatitis
Headache,
dizziness
Arthralgia
Liver failure
Moderate to severe renal
failure
GLP-1 agonists (incretin
mimetic
drugs: exenatide, liraglutide,
albiglutide)
Direct stimulation of
the GLP-1 receptor
Nausea
Increased risk
of pancreatitisand
possibly pancreati
c cancer
Preexisting,
symptomatic gastrointest
inal motility disorders
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SGLT-2
inhibitors(canagliflozin, dapa
gliflozin, empagliflozin)
Increased glucosuria
through the
inhibition
of SGLT-2 in the
kidney
Genital yeast infe
ctions and urinary
tract infections
Polyuria and dehy
dration
Diabetic
ketoacidosis
Chronic kidney disease
Recurrent urinary tract
infections
Alpha-glucosidase
inhibitors(acarbose)
Reduce intestinal
glucose absorption
Gastrointestinal
complaints
(flatulence, diarrh
ea, feeling of
satiety)
Any preexisting
intestinal conditions
(e.g., inflammatory
bowel disease)
Severe renal failure
Thiazolidinediones(pioglitaz
one)
Reduce insulin
resistance through
the stimulation of
PPARs (peroxisome
proliferator-activated
receptors)
Increase transcriptio
n of adipokines
Weight gain
Edema
Cardiac failure
Increased risk of
bone fractures (os
teoporosis)
Congestive heart failure
Liver failure
Amylin
analogs (pramlintide)
Reduce glucagon rel
ease
Reduce gastric
emptying
Increase satiety
Risk
of hypoglycemia
Nausea
Gastroparesis
3 Common contraindications of antidiabetic agents
● Type 1 diabetes mellitus: Patients require insulin therapy (see principles of insulin
therapy).
● Pregnancy and breastfeeding (also see gestational diabetes): All antidiabetic agents are
contraindicated. Antidiabetic drugs should be substituted with human insulin as early as
possible (ideally prior to the pregnancy).
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● Renal failure : Antidiabetic drugs that may be administered if GFR < 30
mL/min include DPP-4 inhibitors, incretin mimetic drugs, meglitinides,
and thiazolidinediones.
● Morbidity and surgery.
● Pause antidiabetic treatment in the following cases:
● Major surgery performed under general anesthesia.
● Acute conditions requiring hospitalization (infections, organ failure).
● Elective procedures associated with an increased risk of hypoglycemia (periods of
fasting, irregular food intake).
4 Insulinotropic agents
● Mechanism: stimulate the secretion of insulin from pancreatic β-cells.
● Glucose-independent: Insulin is secreted regardless of the blood glucose level, even if
blood glucose levels are low → risk of hypoglycemia.
● Sulfonylurea, meglitinides.
● Glucose-dependent: Insulin secretion is stimulated by elevated blood glucose levels
(postprandially). These antidiabetic agents depend on residual β-cellfunction.
● GLP-1 agonists, DPP-4 inhibitors.
5 Non-insulinotropic agents
● Mechanism:These agents do not depend on residual insulin production.
● Effective in patients with nonfunctional endocrine pancreatic β-cells..
● Biguanides (metformin), SGLT-2 inhibitor, thiazolidinediones, alpha-glucosidase
inhibitors.
5.1 Biguanides (Metformin)
5.1.1 Mechanism of action:
● enhances the effect of insulin.
● Reduction in insulin resistance via modification of glucose metabolic pathways.
● Inhibits mitochondrial glycerophosphate dehydrogenase (mGPD)..
● Decreases hepatic gluconeogenesis and intestinal glucose absorption.
● Increases peripheral insulin sensitivity.
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● Lowers postprandial and fasting blood glucose levels.
● Reduces LDL, increases HDL.
5.1.2 Indications: drug of choice in all patients with type 2 diabetes.
5.1.3 Clinical characteristics:
● Glycemic efficacy: lowers HbA1c by 1.2–2% over 3 months.
● Weight loss or weight stabilization.
● No risk of hypoglycemia.
● Beneficial effect on dyslipidemia.
● Studies show metformin reduces the risk of macroangiopathic complications in diabetic
patients.
● Cost-effective.
5.1.4 Important side effects:
● Metformin-associated lactic acidosis.
● Incidence: ∼ 8 cases/100,000 patient years.
● Clinical features: frequently nonspecific.
● Gastrointestinal prodromal symptoms: nausea, vomiting, diarrhea, abdominal pain.
● Severe symptoms: muscle cramps, hyperventilation, apathy, disorientation, coma.
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● High-risk groups.
● Elderly individuals.
● Patients with cardiac or renal insufficiency.
● Diagnostics.
● Arterial blood gas (ABG): metabolic acidosis and anion gap.
● ↑ Serum lactate.
● Treatment: discontinue metformin and treat acidosis.
● Gastrointestinal complaints are common: nausea, diarrhea, flatulence.
● Vitamin B12 deficiency.
● Metallic taste in the mouth (dysgeusia).
5.1.5 Contraindications:
● Renal failure (if creatinine clearance < 30 mL/min).
● Severe liver failure.
● Intravenous iodinated contrast medium.
● Pause metformin prior to surgery.
● Chronic pancreatitis, starvation ketosis, ketoacidosis, sepsis.
● Heart failure (NYHA III and IV), respiratory failure, shock, sepsis.
● Alcoholism.
5.1.6 Important interactions: sulfonylureas
5.2 Thiazolidinediones (glitazones, insulin sensitizers)
5.2.1 Active agents:
● Pioglitazone
● Rosiglitazone
● Activation of the transcription
factor PPARγ (peroxisome proliferator-activated receptor of gamma type).
● ↑ Transcription of genesinvolved in glucose and lipid metabolism.
● ↑ levels of adipokines such as adiponectin.
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● ↑ Storage of triglycerides and subsequent reduction of products of lipid metabolism (e.g.,
free fatty acids) that enhance insulin resistance .
● Glucose utilization is increased and hepatic glucose production reduced.
5.2.3 Indications:
May be considered as a monotherapy in patients with severe renal failure and/or
contraindications for insulin therapy.
● Glycemic efficacy: lowers HbA1c by 1% in 3 months.
● Favorable effect on lipid metabolism: ↓ triglyceride, ↓ LDL, ↑ HDL.
● Fluid retention and edema.
● Weight gain.
● Increased risk of heart failure.
● Increased risk of bone fractures (osteoporosis!).
● Congestive heart failure (NYHA III or IV).
● Liver failure.
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● Pioglitazone: history of bladder cancer or active bladder
cancer; macrohematuria of unknown origin.
5.3 Sulfonylureas
● Glyburide: the standard substance of this class with a relatively long half-life.
● Glipizide: a short-acting agent.
● Sulfonylureas block ATP-sensitive potassium channels of the pancreatic β-cells.
● Depolarization of the cell membrane.
● Calcium influx.
● Insulinsecretion.
● Extrapancreatic effect: decreases hepatic gluconeogenesis and increases
peripheral insulin sensitivity.
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5.3.3 Indications:
Particularly suitable for patients who are not overweight, do not consume alcohol, and adhere to
a consistent dietary routine.
● Glycemic efficacy: lowers HbA1c by 1.2% over 3 months.
● Long-term experience.
● Low-cost.
● Life-threatening hypoglycemia.
● Increased risk in patients with renal failure.
● Weight gain.
● Hematological changes: granulocytopenia, hemolytic anemia.
● Allergic skin reactions.
● Alcohol intolerance.
● Compared to metformin, sulfonylureas are associated with more cardiovascular
(macrovascular) complications.
● Severe cardiovascular comorbidity.
● Obesity.
● Sulfonamide allergy (particularly long-acting substances).
● Severe kidney failure.
5.4 Meglitinides (sulfonylurea analogue)
● Repaglinide: the leading agent in the class of meglitinides, which is well tolerated by
patients with chronic kidney disease
● Nateglinide
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● Enhances insulin secretion (similar mechanism of action to that of
the sulfonylureas).
● Meglitinides should be taken shortly before meals.
5.4.3 Indications: particularly suitable for patients with postprandial peaks in blood glucose
levels.
● More expensive than sulfonylureas.
● Life-threatening hypoglycemia (less risky than sulfonylureas).
● Increased risk in patients with renal failure.
● Weight gain.
● Hepatotoxicity (rare).
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● Severe renal failure.
5.4.7 Interactions: Sulfonylureas.
5.5 Incretinmimetics (GLP-1 receptor agonists)
● Exenatide.
● Liraglutide: rapid-release formula that is administered daily.
● Albiglutide: extended-release formula that is administered once weekly.
● Dulaglutide.
● Incretin effect:
1. Food intake.
2. Activation of enteroendocrine cells in the gastrointestinal tract.
3. Release of GLP-1.
4. GLP-1 degradation via the enzyme DPP-4.
5. End of the GLP-1 effect.
● Incretin mimetic drugs bind to the GLP-1 receptors and are resistant to
degradation by DPP-4 enzyme
● Increase insulin secretion, decrease glucagonsecretion, slow gastric emptying (↑
feeling of satiety, ↓ weight)
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● Glycemic efficacy: lowers HbA1c by 0.5–1.5% over 3 months
● Subcutaneous injection
● Weight loss
● No risk of hypoglycemia
5.5.4 Side effects:
● Gastrointestinal complaints (particularly impaired gastric emptying!)
● Increased risk of pancreatitis and potentially pancreatic cancer :
● Preexisting symptomatic gastrointestinal motility disorders
● Chronic pancreatitis or a family history of pancreatic tumors
5.6 Dipeptidyl peptidase-4 inhibitors (gliptins)
● Sitagliptin
● Saxagliptin
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● Gliptins indirectly increase the endogenous incretin effect by inhibiting the dipeptidyl
peptidase.
● 4 enzyme that breaks down glucagon-like peptide 1.
● Increased insulin secretion, decreased glucagon secretion, delayed gastric emptying.
5.6.3 Indications: Antihyperglycemic therapy algorithm for type 2 diabetes.
● Glycemic efficacy: lowers HbA1c by 0.5–0.75% over 3 months.No risk of
hypoglycemia unless insulin and/or insulinotropic drugs are used simultaneously.
● Gastrointestinal complaints: diarrhea, constipation (milder than
in GLP-1 agonist exposure).
● Nasopharyngitis and upper respiratory tract infection.
● Arthralgia.
● Headaches, dizziness.
● Urinary infections (mild).
● Increased risk of pancreatitis.
● Acute renal failure.
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● Hypersensitivity.
● Liver failure.
5.7 SGLT-2 inhibitors (gliflozins)
● Dapagliflozin
● Empagliflozin
● Canagliflozin
● Reversible inhibition of the sodium-dependent glucose co-transporter (SGLT-2) in
the proximal tubule of the kidney.
● reduced glucose reabsorption in the kidney.
● glycosuria and polyuria.
5.7.3Indications: A treatment option used especially in young patients
with treatment-compliant type 2 DM without significant renal failure.
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● Promotes weight loss.
● Reduces blood pressure.
● Urinary tract infections, genital infections (vulvovaginitis, balanitis).
● Dehydration as a result of polyuria.
● Severe diabetic ketoacidosis.
● Chronic kidney disease.
● Recurrent urinary tract infections (e.g., in patients with anatomical or functional
anomalies of the urinary tract).
5.8 Alpha-glucosidase inhibitors
● Acarbose
● Miglitol
● Inhibits alpha-glucosidase.
● Decreased intestinal glucose absorption.
● The drug is particularly effective in controlling postprandial blood glucose levels.
● The undigested carbohydrates reach the colon, where they are degraded by
intestinal bacteria, resulting in the production of intestinal gas.
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5.8.4 Important side effects: gastrointestinal complaints (flatulence, abdominal
discomfort, diarrhea).
5.8.5 Contraindications
● Inflammatory bowel disease.
● Conditions associated with malabsorption.
● Severe renal failure.
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References:
1. https://www.amboss.com/us/knowledge/Antidiabetic_drugs
2. American Diabetes Association. Diabetes Basics. Accessed 11/5/2018
3. MIMS. 2013. [12 December 2013]. Available from: http://www.mims.co.uk/
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