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EXPLAINS. Hypoglycemia. EX PLAINS. Exogenous Insulin . Bolus Novolg Humolog Apidra Regular Exubera(inhaled Insulin ). Basal: Lantus Levemir NPH. ex p lains. Pituitary tumor (adrenal Insuficency, GH deficency ). exp l ains. Liver disease (Cirrhosis,Tumor)
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EXPLAINS Hypoglycemia
EX PLAINS • Exogenous Insulin • Bolus • Novolg • Humolog • Apidra • Regular • Exubera(inhaled Insulin) • Basal: • Lantus • Levemir • NPH
explains • Pituitary tumor (adrenal Insuficency, GH deficency )
explains • Liver disease (Cirrhosis,Tumor) • Decresed gluconeogenesis and glycogenlysis)
explains • Adrenal insuficency(lack of steroid for sustained glycemic control)
explains • Insulin Resistance: • Most common reason for hypoglycemia • Overweight, family history of DM • Mainly postprandial:after meal ,peak in insulin secretion led to hypoglymia • Labs: high insulin level,possible hyperglycemia • TX: Metformin, TZD , precose, Glyset
Insulinomas • Incidence: 0.4/100.000 • Median age: 47 years (8-82), 59% females • Clinical Features: • Fasting hypoglycemia, but can also present as post-prandial hypoglycemia • 20% of patients misdiagnosed with a neurologic or psychiatric disorder
Insulinomas • Weight gain has been described in 18% of patients • Median duration of symptoms before diagnosis is less than 1.5 years • Tumor distribution: • 87% single benign tumor • 7% multiple benign tumors • 6% malignant insulinoma (77% males, median age 48 years)
Insulinomas • MEN-I: • 8% of inulinomas have MEN-I • median age 25 years • 53% females • All have primary hyperparathyroidism, few have prolactinomas, gastrinomas or Cushing’s • 59% have multiple islet cell tumors
Insulinomas (diagnosis) • Blood glucose<45 mg/dl • Insulin level > 6 mcu/ml (RIA) or 3 mcu/ml (ICMA) • C-Peptide > 200 pmol/l (0.6 ng/ml) • Proinsulin > 5pmol/l (ICMA) • Betahydroxybutyrate < 2.7 mmol/l • Increased BG at least 25 mg/dl after glucagon injection (10, 20, 30 min)
explains • Neoplasm: mainly pelvic tumor ,IGF-2 mediated)
explains • Secretatogue(glyburide,glipizide,amaryl, prandin, starlix) • Sepsis
Functional Hypoglycemia • Presentation:young female with spells • Etiology: rapid gastric emtying leading to peak in insulin secretion.especialy high carb meals • Treatment: low carb meal, precose , glyset.
Workup for hypoglycemia • When BG <45, draw the following labs: • Insulin(>6 indicating insulinoma) • C-peptide(>0.6 –insulinoma) • Cortisol(>20) • GH • LFT,BMP,TSH
* * * * * * * The Incretin Effect Beta-Cell Response to Oral vs IV Glucose Incretin Effect
GLP-1 Effects in HumansUnderstanding the Natural Role of Incretins
S e c t i o n 12, 12.2 Mechanism of Action of Sitagliptin Glucose dependent Insulin (GLP-1andGIP) Glucose uptake by peripheral tissue Ingestion of food Pancreas Release of active incretins GLP-1 and GIP Beta cells Alpha cells GI tract Blood glucose in fasting and postprandial states Glucose- dependent X JANUVIA (DPP-4 inhibitor) DPP-4 enzyme Hepatic glucose production Glucagon (GLP-1) Inactive GLP-1 Inactive GIP • Incretin hormones GLP-1 and GIP are released by the intestine throughout the day, and their levels in response to a meal. GLP-1=glucagon-like peptide-1; GIP=glucose-dependent insulinotropic polypeptide.
Impairedinsulin secretion Oral Antidiabetic Agents: Sites of Action SulfonylureasRepaglinide Acarbose Miglitol Pancreas Gut Adipose tissue Glucose uptake Glucose Absorption Rosiglitazone Pioglitazone Hyperglycemia HGO* Muscle Glucoseuptake Liver Rosiglitazone Pioglitazone Metformin Metformin Rosiglitazone Pioglitazone *HGO, hepatic glucose output.
Natural History of Type 2 DiabetesProgression of Complications Pre-diabetic state Onset of diabetes Environmental factors e.g. nutrition physical inactivity Complications Disability Genetic susceptibility IFG* Death Insulin resistance Hyperinsulinemia Obesity cell dysfunction Proinsulin Hypertension Dyslipidemia Atherosclerosis Hyperglycemia Retinopathy Nephropathy Neuropathy Blindness Renal failure CHD† Amputation Abnormal glucose levels Adapted from International Diabetes Center (IDC) Minneapolis, Minnesota *IFG = impaired fasting glucose †Coronary heart disease
Type 2 Diabetes is a Cardiovascular Risk Factor Diabetes and prior myocardial infarction (MI) carry the same mortality risk 45.0%* No Prior MI Prior MI Fatal or Nonfatal MI 20.2% 18.8%* 3.5% Nondiabetic Subjects (n=1373) Type 2 Diabetic Subjects (n=1059) Seven-year incidence in a Finnish-based cohort. *P<.001 Haffner SM, et al. N Engl J Med. 1998;339:229-234.
9 Conventional 8 ADA action Insulin Median HbA1c (%) Chlorpropamide Glibenclamide (glyburide) 7 ADA goal Metformin 6 Upper limit of normal range (6.2%) 0 10 3 6 9 0 Time From Randomization (years) Intensive Treatments and Increase in HbA1c Over Time United Kingdom Prospective Diabetes Study (UKPDS) UK Prospective Diabetes Study (UKPDS 34) Group. Lancet. 1998;352:854-65.
Normal Mealtime Insulin Response Breakfast Lunch Dinner Plasma insulin 4:00 8:00 12:00 16:00 20:00 24:00 4:00 8:00 Time
No hypoglycemia: TZD(Actos, Avandia) Metformin/glucophage) Alpha glucosidase inhibitor(Precose, Glyset) Combo(avandamet, actoplusmet) DPP IV inhibitor: Januvia Galvus Can Cause Hypoglycemia: SU(glyburide,Amaryl) Prandin/Starlix Combo(glucovance, avandaryl, duetact) Pills available for DM 2
Non insulin injection for DM2 GLP-1 analog(byetta) Amylin(Symlin)
Basal: Lantus Levemir NPH Bolus Novolg Humolog Apidra Regular Exubera(inhaled Insulin) Insulin treatment for DM
