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AUTHOR AND EDITOR INFORMATION

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Author: Hilarie Cranmer, MD, MPH, FACEP, Director, Global Women's Health Fellowship, Associate Director, Harvard International Emergency Medicine Fellowship, Department of Emergency Medicine, Brigham and Women's Hospital; Director, Humanitarian Studies Initiative for Residents, Harvard Humanitarian Initiative; Assistant Professor, Harvard University School of Medicine

Hilarie Cranmer is a member of the following medical societies: American College of Emergency Physicians, American Institute of Ultrasound in Medicine, American Medical Association, Massachusetts Medical Society, Physicians for Human Rights, and Society for Academic Emergency Medicine

Coauthor(s): Michael Shannon, MD, MPH, Professor, Department of Pediatrics, Harvard Medical School; Chief and CHB Chair, Division of Emergency Medicine, Children's Hospital

Editors: Debra Slapper, MD, Consulting Staff, Department of Emergency Medicine, St Anthony's Hospital; Mary L Windle, PharmD, Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy, Pharmacy Editor, eMedicine.com, Inc; Wayne Wolfram, MD, MPH, Clinical Associate Professor, Departments of Pediatrics, Children's Hospital and University of Cincinnati; John Halamka, MD, Chief Information Officer, CareGroup Healthcare System, Assistant Professor of Medicine, Department of Emergency Medicine, Beth Israel Deaconess Medical Center; Assistant Professor of Medicine, Harvard Medical School; Richard G Bachur, MD, Assistant Professor of Pediatrics, Harvard Medical School; Associate Chief and Fellowship Director, Attending Physician, Division of Emergency Medicine, Children's Hospital of Boston

Author and Editor Disclosure

Synonyms and related keywords: low blood sugar in children, low blood sugar in newborns, hypoglycemia in infancy, persistent hyperinsulinemic hypoglycemia of infancy, PHHI

INTRODUCTION

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Background

Hypoglycemia is the most common metabolic problem in neonates. In children, a blood glucose value below 40 mg/dL (2.2 mmol/L) represents hypoglycemia. A plasma glucose level of less than 30 mg/dL (1.65 mmol/L) in the first 24 hours of life and less than 45 mg/dL (2.5 mmol/L) thereafter constitutes hypoglycemia in the newborn.  

Patients with hypoglycemia may be asymptomatic or may present with severe central nervous system (CNS) and cardiopulmonary disturbances. The most common clinical manifestations can include altered level of consciousness, seizure, vomiting, unresponsiveness, and lethargy. Any acutely ill child should be evaluated for hypoglycemia, especially when history reveals diminished oral intake.

Sustained or repetitive hypoglycemia in infants and children has a major impact on normal brain development and function. There is evidence that hypoxemia and ischemia potentiate hypoglycemia, causing brain damage that may permanently impair neurologic development.

Causes of hypoglycemia in neonates differ slightly from the causes of hypoglycemia in older infants and children. Hyperinsulinism, or persistent hyperinsulinemic hypoglycemia of infancy (PHHI), is the most common cause of hypoglycemia in the first 3 months of life. It is well recognized in infants of mothers with diabetes. Other causes in all ages include gram-negative sepsis; endotoxin shock; and ingestions, including salicylates, alcohol, hypoglycemic agents, and beta-adrenergic blocking agents.

Excluding insulin therapy, almost all hypoglycemia in childhood occurs during fasting. Postprandial hypoglycemia is rare in children in the absence of prior gastrointestinal (GI) surgery. Management efforts are directed to immediate normalization of glucose levels and identification and treatment of the various causes.

Pathophysiology

Normal blood glucose is regulated very narrowly, usually from 80-90 mg/dL (4.4-5 mmol/L).

Glucose levels increase transiently after meals to 120-140 mg/dL (6.6-7.7 mmol/L). Feedback systems return the glucose concentration rapidly back to the preprandial level, usually within 2 hours after the last absorption of carbohydrates.

Insulin and glucagon are the important hormones in the immediate feedback control system of glucose. When blood glucose increases after a meal, the rate of insulin secretion increases and stimulates the liver to store glucose as glycogen. When cells (primarily liver and muscle) are saturated with glycogen, additional glucose is stored as fat.

When blood glucose levels fall, glucagon secretion functions to increase blood glucose levels by stimulating the liver to undergo glycogenolysis and release glucose back into the blood.

In starvation, the liver maintains the glucose level via gluconeogenesis. Gluconeogenesis is the formation of glucose from amino acids and the glycerol portion of fat. Muscle provides a store of glycogen and muscle protein breaks down to amino acids, which are substrates utilized in gluconeogenesis in the liver. Circulating fatty acids are catabolized to ketones, acetoacetate, and B-hydroxybutyrate and can be used as auxiliary fuel by most tissues, including the brain.

The hypothalamus stimulates the sympathetic nervous system, and epinephrine is secreted by the adrenals causing the further release of glucose from the liver. Over a period of hours to days of prolonged hypoglycemia, growth hormone and cortisol are secreted and decrease the rate of glucose utilization by most cells of the body.

In the newborn, serum glucose levels decline after birth until age 1-3 hours, then they spontaneously increase. Liver glycogen stores become rapidly depleted within hours of birth, and gluconeogenesis, primarily from alanine, can account for 10% of glucose turnover in the newborn infant by several hours of age.

Neonatal hypoglycemia

  • Inappropriate changes in hormone secretion
  • Inadequate substrate reserve in the form of hepatic glycogen
  • Inadequate muscle stores as a source of amino acids for gluconeogenesis
  • Inadequate lipid stores for the release of fatty acids

Hypoglycemia in older infants and children

  • The pathophysiology of hypoglycemia is analogous to that in adults.
  • Glucose homeostasis is maintained by glycogenolysis in the immediate postfeeding periods and by gluconeogenesis several hours after meals.

Frequency

United States

The overall incidence of symptomatic hypoglycemia in newborns varies from 1.3-3 per 1000 live births. Incidence varies with the definition, population, method and timing of feeding, and the type of glucose assay. Serum glucose levels are higher than whole blood values. The incidence of hypoglycemia is greater in high-risk neonatal groups. Early feeding decreases the incidence of hypoglycemia. Prematurity, hypothermia, hypoxia, maternal diabetes (1 in 1000 pregnant women has insulin-dependent diabetes), maternal glucose infusion in labor (gestational diabetes occurs in 2% of pregnant women), and intrauterine growth retardation increase the incidence of hypoglycemia. The incidence of inborn errors of metabolism that lead to neonatal hypoglycemia are rare but can be screened in infancy:

  • Carbohydrate metabolism disorders (>1:10,000)
  • Fatty acid oxidation disorders (1:10,000)
  • Hereditary fructose intolerance (1:20,000 to 1:50,000)
  • Glycogen storage diseases (1:25,000)
  • Galactosemia (1:40,000)
  • Organic acidemias (1:50,000)
  • Phosphoenolpyruvate carboxykinase deficiency (rare)
  • Primary lactic acidosis (rare)

Mortality/Morbidity

Hypoglycemia is the most common metabolic problem in neonates. Still, the level or duration of hypoglycemia that is harmful to an infant's developing brain is not known. Major long-term sequelae include neurologic damage resulting in mental retardation, recurrent seizure activity, developmental delay, and personality disorders. Some evidence suggests that severe hypoglycemia may impair cardiovascular function.


CLINICAL

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History

  • The clinical presentation of hypoglycemia reflects decreased availability of glucose for the CNS as well as adrenergic stimulation caused by a decreasing or low blood sugar level.
  • During the first or second day of life, symptoms vary from asymptomatic to CNS and cardiopulmonary disturbances.
  • Hyperinsulinemia
    • The onset is from birth to 18 months.
    • Insulin concentrations are inappropriately elevated at the time of documented hypoglycemia.
    • Transient neonatal hyperinsulinism occurs in macrosomic infants of diabetic mothers (who have diminished glucagon secretion and endogenous glucose production is significantly inhibited). Clinically, these infants are macrosomic and have increasing demands for feeding, intermittent lethargy, jitteriness, and frank seizures.
    • Infants with prolonged neonatal hyperinsulinism can be described by the following:
      • Small for gestational age (SGA)
      • Patients with perinatal asphyxia
      • Neonates born to mothers with toxemia
      • Have high rates of glucose utilization and often require dextrose infusion for a prolonged period of time
  • Ketotic hypoglycemia is an uncommon but dramatic illness. It is observed in children younger than 5 years who usually become symptomatic after an overnight or prolonged fast, especially with illness and poor oral intake. Children often present inexplicably lethargic or frankly comatose, having only marked hypoglycemia with ketonuria.

Physical

Clinical manifestations are broad and can be from a combination of adrenergic stimulation or from decreased availability of glucose for the CNS. Unlike older children, infants are not able to verbalize their symptoms and are particularly vulnerable to hypoglycemia.

  • Infants in the first or second day of life may be asymptomatic or have life-threatening CNS and cardiopulmonary disturbances.
    • Hypotonia
    • Lethargy, apathy
    • Poor feeding
    • Jitteriness, seizures
    • Congestive heart failure
    • Cyanosis
    • Apnea
    • Hypothermia
  • Clinical manifestations associated with activation of the autonomic nervous system
    • Anxiety, tremulousness
    • Diaphoresis
    • Tachycardia
    • Pallor
    • Hunger, nausea, and vomiting
  • Clinical manifestations of hypoglycorrhachia or neuroglycopenia
    • Headache
    • Mental confusion, staring, behavioral changes, difficulty concentrating
    • Visual disturbances (eg, decreased acuity, diplopia)
    • Dysarthria
    • Seizures
    • Ataxia, somnolence, coma
    • Stroke (hemiplegia, aphasia), paresthesias, dizziness, amnesia, decerebrate or decorticate posturing

Causes

  • Cause of neonatal hypoglycemia
    • Hyperinsulinism, or PHHI
    • Limited glycogen stores (eg, prematurity, intrauterine growth retardation)
    • Depleted glycogen stores (eg, asphyxia-perinatal stress, starvation): In ketotic hypoglycemia, easily depleted glycogen stores, in combination with inadequate production of glucose through gluconeogenesis, contribute to hypoglycemia. Thus, fatty acid oxygenation is required to provide substrate for gluconeogenesis and ketogenesis. Ketones, the byproduct of fatty acid metabolism, are found in urine and represent the starved state.
    • Increased glucose utilization (eg, hyperthermia, polycythemia, sepsis, growth hormone deficiency)
    • Decreased glycogenolysis, gluconeogenesis, or utilization of alternate fuels (eg, inborn errors of metabolism, adrenal insufficiency)
  • Causes of hypoglycemia in older infants, children, and teenagers
    • Poisonings/drugs (eg, ethanol, isoniazid, insulin, propranolol, salicylates, oral hypoglycemics, pentamidine, quinine, disopyramide, unripe ackee fruit, Vacor [rat poison]).
    • Liver disease (eg, Reye syndrome, hepatitis, cirrhosis, hepatoma)
    • Amino acid and organic acid disorders (eg, maple syrup urine disease, propionic acidemia, methylmalonic acidemia, tyrosinosis, glutaric aciduria, 3-hydroxy-3-methylglutaric aciduria)
    • Systemic disease (eg, sepsis, burns, cardiogenic shock, respiratory distress syndrome)
  • Causes of hyperinsulinemia
    • Congenital hyperinsulinism most commonly is associated with an abnormality of beta-cell regulation throughout the pancreas. A focal disease, such as isolated islet adenoma, occasionally causes congenital hyperinsulinism.
    • Recently identified genetic defects have been delineated and now replace the older terms, such as nesidioblastosis, leucine-sensitive hypoglycemia, persistent hyperinsulinemic hypoglycemia of infancy, and islet dysregulation syndrome. These defects are in the sulfonylurea receptor (SUR) and the beta-cell potassium adenosine triphosphate (ATP) channel gene located on the short arm of chromosome 11.
    • Drug-induced hyperinsulinism is secondary to surreptitious insulin administration or oral hypoglycemic drugs. Exogenous administration of insulin is diagnosed with low serum levels of C-peptide. The sulfonylureas are commonly prescribed for adults, thus, are available to children as unintentional ingestions. In these cases, hypoglycemia may persist for more than 24 hours. Diazoxide administration may be helpful by suppressing insulin secretion in severe cases.


DIFFERENTIALS

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Adrenal Insufficiency and Adrenal Crisis
Hypopituitarism
Hypothyroidism and Myxedema Coma
Munchausen Syndrome
Pediatrics, Reye Syndrome
Plant Poisoning, Hypoglycemics
Shock, Septic
Toxicity, Alcohols
Toxicity, Salicylate

Other Problems to be Considered

Fasting
Malnutrition
Diarrhea
Enzymatic defects of glycogen synthetic pathways
Enzymatic defects of glycogenolytic pathways
Enzymatic defects of gluconeogenic pathways
Glucagon deficiency
Congenital hyperinsulinism (eg, nesidioblastosis, leucine sensitive hypoglycemia)
Defects of beta cell regulation
Large tumors
Decreased or absent fat stores
Enzymatic defects in fatty acid oxidation


WORKUP

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Lab Studies

  • Fingerstick glucose levels or bedside testing may lead to overtreatment because the primary error with the chemically treated strips is an underestimation of the serum glucose value.
  • Serum or plasma glucose levels
    • Serum glucose level is higher than whole blood glucose level. Whole blood measurements of glucose may underestimate the plasma glucose concentration by approximately 10-15% because red blood cells contain relatively low concentrations of glucose. Arterial and capillary samples may overestimate the plasma glucose concentration by 10% in nonfasting patients.
    • Hold an extra tube of serum or plasma and refrigerate until laboratory glucose is known.
  • Serum insulin: When blood glucose is less than 40 mg/dL, plasma insulin concentration should be less than 5 and no higher than 10 microunits/mL.
  • Urine
    • Obtain first voided urine dipstick for ketones.
    • Failure to find large ketones with hypoglycemia suggests that fat is not being metabolized from adipose tissue (hyperinsulinism) or that fat cannot be used for ketone body formation (enzymatic defects in fatty acid oxidation).
    • Send urine for organic acid analysis.
  • Newborn screening: Electrospray ionization-tandem mass spectrometry in asymptomatic persons allows earlier identification of clearly defined inborn errors of metabolism. These include aminoacidemias, urea cycle disorders, organic acidurias, and fatty acid oxidation disorders. Earlier recognition of these inborn errors of metabolism has the potential to reduce morbidity and mortality rates in these infants.

Imaging Studies

  • The detection of adenomas by celiac angiography has limited success.
  • The chance of detecting a tumor blush must be balanced by the potential risk of causing vascular trauma in infants younger than 2 years.


TREATMENT

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Prehospital Care

Stabilize acute life-threatening conditions and initiate supportive therapy. If a patient is alert and has intact airway protective reflexes, oral liquids containing sugar (eg, orange juice) can be administered.

Emergency Department Care

Supportive therapy includes oxygen, establishing IV, and monitoring.

  • Seizures unresponsive to correction of hypoglycemia should be managed with appropriate anticonvulsants.
  • Marked acidosis (pH <7.10) suggests shock or serious underlying disease and should be treated appropriately.
  • Treatment goal is to maintain a blood glucose level of at least 45 mg/dL (2.5 mmol/L).
  • For the infant or child who will not drink but has intact airway protective reflexes, orogastric or nasogastric administration of oral liquids containing sugar may be performed.

Consultations

  • If hypoglycemia is diagnosed in an infant younger than 3 months, surgical intervention may be necessary. Surgical exploration usually is undertaken in severely affected neonates who are unresponsive to glucose and somatostatin therapy.
    • Near total resection of 85-90% of the pancreas is recommended.
    • Risks include the development of diabetes.
    • If hypoglycemia first becomes manifest in infants aged 3-6 months, a therapeutic trial of octreotide, diazoxide, steroids, and frequent feedings can be attempted for as long as 2-4 weeks.


MEDICATION

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Hypoglycemia should be treated as soon as possible to prevent complications of neurologic damage.

Mainstays of therapy for patients that are alert with intact airway protection is orange juice, 20 mL/kg. For those who cannot protect their airway or are unable to drink, NG, IM, IO, or IV routes can be used for the following drugs: dextrose, glucagon, diazoxide, and octreotide.

Case reports have shown that nifedipine may help maintain normoglycemia in children with PHHI.

Cortisol should not be used because it has minimal acute benefit and may delay the diagnosis of the cause of hypoglycemia. Cortisol stimulates gluconeogenesis and causes decreased utilization of glucose, which leads to overall elevated blood glucose and may mask the true cause of hypoglycemia.

Drug Category: Anti-hypoglycemic agents

These agents elevate blood glucose levels.

Drug NameDextrose
DescriptionTreatment of choice. Absorbed from the intestine resulting in rapid increase in blood glucose concentration when administered PO. Give IV dextrose to infants of diabetic mothers with transient neonatal hyperinsulinemia for several days until hyperinsulinemia abates. Avoid hyperglycemia evoking prompt insulin release, which may produce rebound hypoglycemia. SGA infants and those with maternal toxemia or perinatal asphyxia require dextrose IV infusion rates >20 mg/kg/min to control levels. Treatment may be necessary for 2-4 wk.
Pediatric DoseInitial bolus: 0.25 g/kg (2.5 mL/kg of 10% dextrose or 1 mL/kg of 25% dextrose) IV
Maintenance: Provide dextrose at 6-8 mg/kg/min IV by giving 10% dextrose at 1.5 times maintenance rate
ContraindicationsDocumented hypersensitivity; not to be administered SC or IM; patients in diabetic coma if blood sugar levels extremely high (avoid in severely dehydrated patients); glucose-galactose malabsorption syndrome
InteractionsCaution when administering parenteral fluids to patients receiving corticosteroids or corticotropin, especially if the solution contains sodium ions
PregnancyC - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
PrecautionsMay induce diuresis; may cause nausea, which may also occur with hypoglycemia; IV dextrose solutions may result in dilution of serum electrolyte concentrations, or overhydration when there is fluid overload; caution in patients suffering from congested states or pulmonary edema; hypertonic dextrose given peripherally may cause thrombosis (administer instead through central venous catheter); caution in subclinical diabetes mellitus or carbohydrate intolerance; there is increased risk of inducing significant hyperglycemia or hyperosmolar syndrome if solution is administered rapidly, especially in patients with chronic uremia or carbohydrate intolerance; concentrated solutions should not be administered SC or IM; rates of dextrose infusion higher than 0.5 g/kg/h may produce glycosuria; at infusion rates of 0.8 g/kg/h the incidence of glycosuria is 5%; monitor fluid balance, electrolyte concentrations and acid-base balance closely; dextrose administration may produce vitamin B-complex deficiency

Drug NameDiazoxide (Hyperstat)
DescriptionIncreases blood glucose by inhibiting pancreatic insulin release, and possibly through an extrapancreatic effect. Hyperglycemic effect starts within an hour and usually lasts a maximum of 8 h with normal renal function. Reportedly effective in SGA infants and those with maternal toxemia or perinatal asphyxia.
Pediatric Dose3-8 mg/kg/d IV divided bid/tid
ContraindicationsDocumented hypersensitivity; aortic coarctation; pheochromocytoma; arteriovenous shunts; aortic aneurysm
InteractionsMay decrease serum hydantoins, possibly resulting in decreased anticonvulsant effects; thiazide diuretics may potentiate hyperuricemic and antihypertensive effects
PregnancyC - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
PrecautionsPatients with diabetes mellitus may require treatment for hyperglycemia; when given prior to delivery, may produce fetal or neonatal hyperbilirubinemia, thrombocytopenia, altered carbohydrate metabolism, and other adverse reactions; adverse effects include hypertrichosis, salt and water retention, acute hyperglycemia (rare); may require additional diuretic; monitor blood pressure for hypotension

Drug NameOctreotide (Sandostatin)
DescriptionLong-acting analog of somatostatin that suppresses insulin secretion for short-term management of hypoglycemia.
Pediatric Dose2-10 mcg/kg/d SC divided tid/qid or continuous IV infusion
ContraindicationsDocumented hypersensitivity
InteractionsMay reduce effects of cyclosporine; patients on insulin, oral hypoglycemics, beta-blockers, and calcium channel blockers may need dosage adjustments
PregnancyB - Fetal risk not confirmed in studies in humans but has been shown in some studies in animals
PrecautionsAdverse effects primarily related to altered GI motility, and include nausea, abdominal pain, diarrhea, and increased incidence of gallstones and biliary sludge; because of alteration in counter-regulatory hormones, (insulin, glucagon, GH) hypoglycemia or hyperglycemia may occur; bradycardia, cardiac conduction abnormalities, and arrhythmias have been reported; because of inhibition of TSH secretion, hypothyroidism may occur; exercise caution in patients with renal impairment; cholelithiasis may occur

Drug NameGlucagon (Glucagon Emergency Kit)
DescriptionMay be used to treat hypoglycemia secondary to hyperinsulinemia and administered to patients without initial IV access. Each mL contains 1 mg (ie, 1 unit). Maximal glucose concentration occurs between 5-20 min for IV administration and about 30 min for IM administration.
Pediatric Dose0.03-0.1 mg/kg/dose IV/IM q20min prn; not to exceed 0.5 mg/dose; not to be administered at concentrations >1 mg/mL
ContraindicationsDocumented hypersensitivity; pheochromocytoma
InteractionsEffects of anticoagulants may be enhanced by glucagon (although onset may be delayed); monitor prothrombin activity and for signs of bleeding in patients receiving anticoagulants; adjust dose accordingly
PregnancyB - Fetal risk not confirmed in studies in humans but has been shown in some studies in animals
PrecautionsMonitor blood glucose levels in patients with hypoglycemia until they are asymptomatic; glucagon is effective in treating hypoglycemia only if sufficient liver glycogen is present; because liver glycogen availability is necessary to treat patients with hypoglycemia, glucagon has virtually no effects on patients in states of starvation, adrenal insufficiency, or chronic hypoglycemia


FOLLOW-UP

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Further Inpatient Care

  • Any child with documented hypoglycemia not secondary to insulin therapy should be hospitalized for careful monitoring and diagnostic testing.

Prognosis

  • Remission of congenital hyperinsulinism generally does not occur, but the severity of the disease may decrease with time.

Patient Education

  • Provide genetic counseling for families with affected children, including information about a possible 25% risk of recurrence.


MISCELLANEOUS

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Medical/Legal Pitfalls

  • Lack of vigilance with recurrent hypoglycemia in the ED
  • Failure to do a sepsis workup
  • Failure to consider the diagnosis of hypoglycemia, especially in a patient with sustained or repetitive episodes of hypoglycemia with resulting seizures and mental retardation
  • Failure to start 5% or 10% dextrose drip when hypoglycemia is recurrent


REFERENCES

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  • Fleisher G, ed. Pediatric hypoglycemia. In: Textbook of Pediatric Emergency Medicine. Lippincott Williams & Wilkins; 2000.
  • Halamek LP, Benaron DA, Stevenson DK. Neonatal hypoglycemia, Part I: Background and definition. Clin Pediatr (Phila). Dec 1997;36(12):675-80. [Medline].
  • Losek JD. Hypoglycemia and the ABC'S (sugar) of pediatric resuscitation. Ann Emerg Med. Jan 2000;35(1):43-6. [Medline].
  • Lteif AN, Schwenk WF. Hypoglycemia in infants and children. Endocrinol Metab Clin North Am. Sep 1999;28(3):619-46, vii. [Medline].
  • Muller D, Zimmering M, Roehr CC. Should nifedipine be used to counter low blood sugar levels in children with persistent hyperinsulinaemic hypoglycaemia?. Arch Dis Child. Jan 2004;89(1):83-5. [Medline].
  • Raghuveer TS, Garg U, Graf WD. Inborn errors of metabolism in infancy and early childhood: an update. Am Fam Physician. Jun 1 2006;73(11):1981-90. [Medline].
  • Reid SR, Losek JD, Gideon Bosker, ed. Hypoglycemia in infants and children. In: The Textbook of Primary and Acute Care Medicine. 2003.
  • Sperling MA, Behrman RE, Kliegman RM, et al, eds. Hypoglycemia. In: Nelson Textbook of Pediatrics. 15th ed. 1996.
  • Stanley CA. Hyperinsulinism in infants and children. Pediatr Clin North Am. Apr 1997;44(2):363-74. [Medline].
  • Boluyt N, van Kempen A, Offringa M. Neurodevelopment after neonatal hypoglycemia: a systematic review and design of an optimal future study. Pediatrics. Jun 2006;117(6):2231-2243. [Medline].

Pediatrics, Hypoglycemia excerpt

Article Last Updated: Oct 11, 2007