Immunity

Much of critical illness may involve disturbance of the balance between systemic inflammatory responses versus compensatory antiinflammatory responses. ^{, ,} As depicted in Fig. 84.2 , cortisol biochemistry represents a key regulatory mechanism for virtually all aspects of antiinflammation.

Signaling for the antiinflammatory actions of cortisol. COX 2, cyclo-oxygenase 2; GR, glucocorticoid receptor; IL, interleukin; iNOS, inducible nitric oxide synthase; NF- κB, nuclear factor-κB; NO, nitric oxide; PLA ₂ , phospholipase A2; PO 4, phosphate; TNF, tumor necrosis factor.

(From Goodman HM. Adrenal glands. In Goodman HM, ed. Basic Medical Endocrinology . Philadelphia: Elsevier; 2009.)

In this respect, cortisol increases the synthesis of IκB, trapping nuclear factor-κB (NF-κB) in the cytoplasm and effectively thwarting synthesis of a variety of proinflammatory mediators. In addition, cortisol increases the production of annexin, which inhibits phospholipase A ₂ , resulting in modulation of both cyclooxygenase and lipoxygenase inflammatory lipid pathways. Sepsis induces widespread immunosuppression. ^, Among children with sepsis who receive corticosteroids, further repression of gene networks related to adaptive immunity has been reported.

Metabolism

A schematic summary of the effects of cortisol on metabolism is displayed in Fig. 84.3 .

Schematic overview of metabolic actions of cortisol.

(From Goodman HM. Basic Medical Endocrinology . Philadelphia: Elsevier; 2009.)

As a key mediator of the stress response, cortisol facilitates lean muscle catabolism to provide substrate for hepatic gluconeogenesis, synthesis of acute-phase reactants, and expansion of the immune system. Hypercortisolemia represents a key mediator in hyperglycemia of critical illness discussed later. Both protein catabolism and hyperglycemia, if prolonged in the ICU, can become maladaptive and associated with increased risk for adverse outcomes, including death.

Hemodynamics

Cortisol’s permissive effects on maintaining a normal hemodynamic status include augmenting cardiac contractility, maintaining vascular tone, promoting endothelial integrity, upregulating vasoactive receptors, and increasing catecholamine synthesis. ^{, ,} Specifically, cortisol suppresses inducible nitric oxide synthetase, leading to increased vascular tone and blood pressure. Additionally, high intraadrenal concentrations of cortisol during critical illness induce the cascade of enzymatic activity that produces epinephrine via methylation of norepinephrine by phenyl-ethanolamine N-methyltransferase.

Free cortisol

Although most cortisol is bound to transcortin or serum albumin, the free fraction comprising 10% to 15% of the total is actually responsible for the protean effects of cortisol. Accordingly, it has been suggested that perhaps free cortisol rather than total cortisol concentrations might be more reliable in terms of identifying a population that would most benefit from cortisol replacement therapy. For most critically ill patients, cortisol-binding globulin is typically decreased and the percent of cortisol as the free fraction increased. Moreover, with corticotropin adrenal stimulation, free cortisol increases substantially more than total cortisol. Assessing total cortisol concentrations may be especially problematic in critically ill patients with low albumin. In an investigation that measured both total and free cortisol concentrations in a general population of critically ill children, the majority exhibited low total and free cortisol concentrations. However, none of these children demonstrated clinical evidence of corticosteroid insufficiency (hypotension, hyponatremia, hypoglycemia). These results question the use of current thresholds for assigning diagnoses of AI or critical illness–related corticosteroid insufficiency in critically ill children. The results further suggest that clinicians currently are unable to reliably define adequacy of the adrenal response to the stress of critical illness either with total or free cortisol measurements.

Primary adrenal insufficiency

Primary adrenal insufficiency, or Addison disease, is more typically encountered in adult patients and is included in a group of disorders termed autoimmune adrenalitis . ^, Signs and symptoms of Addisonian crisis include intercurrent illness with a history of chronic weight loss and anorexia, dizziness, lethargy, and chronic pigmentation. Symptoms more likely to be associated with admission to the ICU include sudden hypovolemic shock, hyperkalemia, vomiting, diarrhea, abdominal pain, and coma. Other causes of primary adrenal failure include congenital adrenal hyperplasia, an autosomal recessive disorder, with approximately 90% of cases secondary to 21 hydroxylase deficiency ( CYP21A2 mutation). ^, Primary congenital adrenal failure can also occur among infants with adrenoleukodystrophy associated with a metabolic defect in metabolism of very-long-chain fatty acids. Other causes of congenital adrenal failure include Wolman disease and familial unresponsiveness to ACTH involving altered MC2R , as previously discussed.

Because of its precarious circulation associated with a subcapsular arteriolar plexus, the adrenal glands are subject to hemorrhage and infarction, particularly in the setting of septic shock. Such events, termed the Waterhouse-Friderichsen syndrome , were initially described as adrenal apoplexy. ^,

Although a variety of drugs inhibit the sequential steps in cortisol synthesis, etomidate is particularly notable, as it is increasingly being used as a sedative to facilitate endotracheal intubation without adversely affecting hemodynamics. A single bolus of etomidate suppresses 11β-hydroxylase activity, one of the critical enzymes in the cortisol synthetic pathway. ^, A meta-analysis of seven studies concluded that administration of etomidate for endotracheal intubation was associated with higher rates of AI and mortality among patients with sepsis. Further studies, however, have not confirmed consistently worse outcomes with its use. Given the known effects of etomidate on cortisol production, and until further definitive prospective studies have been performed, the authors recommend empiric administration of stress-dose hydrocortisone for 48 hours after etomidate use in patients with septic shock.

Secondary adrenal insufficiency

Secondary AI in the pediatric ICU (PICU) can be seen with pituitary disorders (e.g., among children following surgical resection of a craniopharyngioma). In addition, long-term corticosteroid administration among patients with recalcitrant asthma, patients with oncologic or rheumatologic diagnoses, or transplantation patients results in suppression of ACTH release, occasionally leading to adrenal atrophy. ^,

Probably the most controversial cause of secondary adrenal failure seen in the ICU is so-called relative adrenal insufficiency or critical illness–related corticosteroid insufficiency (CIRCI). A seemingly inadequate adrenal response relative to the magnitude of stress characterizes CIRCI. This situation is a dynamic, typically reversible state that is thought to be secondary to both decreased cortisol production and tissue resistance to cortisol, as discussed previously. Multiple pediatric observational studies, most associated with sepsis, have examined associations with random baseline serum cortisol concentrations with various outcomes. ^, These studies ascertain cortisol circadian rhythm among children with sepsis. As sepsis severity increased (e.g., sepsis → septic shock → sepsis death), proinflammatory mediator concentrations (e.g., IL-6, TNF-α) and ACTH increased, while cortisol concentrations decreased. Both serum cortisol and ACTH concentrations correlated with illness severity per the Pediatric Risk of Mortality study, organ dysfunction scores, lactate, and C-reactive protein. Pediatric observational studies have also examined corticotropin stimulation testing among children with severe sepsis. These studies in general demonstrated that, like adults, low delta cortisol is common among children with sepsis. Among children with a low delta cortisol, illness severity was higher, as was requirement for vasoactive-inotropic resuscitation. Such children also more frequently demonstrate vasoactive-inotropic resistance shock and MODS. Chronic illness and the degree of organ dysfunction at presentation, as well as low delta cortisol concentration, predicted risk of mortality.

Treatment of adrenal insufficiency

Guidelines for steroid replacement in the acute and long-term management of primary AI are well established with utilization of stress-dose hydrocortisone during times of illness and replacement of maintenance glucocorticoids and mineralocorticoids when well. ^, The 2017 American College of Critical Care Medicine Clinical Practice Parameters for Hemodynamic Support of Pediatric and Neonatal Septic Shock additionally recommend use of hydrocortisone in children with catecholamine-resistant septic shock at risk for absolute AI, such as those with purpura fulminans, chronic steroid exposure, sedation with etomidate, and congenital adrenal hyperplasia. The same group did not make recommendations for how or when to treat CIRCI. Treatment of CIRCI remains controversial, as the diagnosis of CIRCI remains controversial.

Two recent adult randomized controlled trials again looked at mortality outcomes after use of steroids in adult patients with septic shock. The ADRENAL study found no difference in mortality among intubated adults with septic shock treated with a continuous infusion of hydrocortisone compared with those who did not received hydrocortisone. The APROCCHSS trial reported lower 90-day mortality in adults with septic shock who received hydrocortisone plus fludrocortisone compared with those who received placebo. Multiple pediatric observational cohort studies have shown no benefit or possible harm with adjunctive corticosteroids used in pediatric septic shock. No large prospective pediatric randomized clinical trial has yet to examine this issue, although one is currently underway at the time of publication of this chapter.

Glucose homeostasis in health

Under normal conditions, glucose concentration is tightly regulated by the neuroendocrine system. Control of blood glucose is complex, involving interaction among the liver, pancreas, muscle, adipose tissue, pituitary, adrenals, and bone. The brain and periphery conduct a constant biochemical conversation by which the periphery informs the brain about its metabolic needs and the brain addresses these needs through its control of somatomotor, autonomic, and neurohumoral pathways involved in energy intake, expenditure, and storage. ^,

Glucose is obtained from three sources: intestinal absorption of food, glycogenolysis, and gluconeogenesis. Once transported into cells, glucose can be stored as glycogen or it can undergo glycolysis to pyruvate. Pyruvate can be reduced to lactate, transaminated to form alanine, or converted to acetyl coenzyme A (CoA). Acetyl CoA can be oxidized in the mitochondrial tricarboxylic acid cycle to carbon dioxide and water, converted to fatty acids for storage as triglyceride, or serve as substrate for ketone body or cholesterol synthesis. Although glycogenolysis can occur in most tissues in the body, only the liver and kidneys express the enzyme glucose-6-phosphatase, which is required for release of cellular glucose into the bloodstream. The liver and kidneys also contain the enzymes required for gluconeogenesis. Of the two organs, the liver is responsible for the bulk of glucose output; the kidney supplies only 10% to 20% of glucose production during fasting.

Glucose homeostasis is centered on glucose-induced secretion of insulin from pancreatic β cells and insulin effect on glucose metabolism in peripheral tissues. The switch from glycogen synthesis during and immediately after meals to glycogen breakdown and gluconeogenesis is orchestrated by hormones, of which insulin is centrally important. Plasma insulin concentrations peak after meals. This surge in insulin activates glycogen synthesis, enhances peripheral glucose uptake, and inhibits glucose production. In addition, lipogenesis is stimulated while lipolysis and ketogenesis are suppressed. During fasting, the plasma insulin level falls to less than or equal to 5 μU/mL. Hormones—including glucagon, catecholamines, cortisol, and growth hormone (GH)—counteract the effects of insulin and promote glycogenolysis, gluconeogenesis, lipolysis, and ketogenesis.

Currently, obesity is an increasingly prevalent disease in the pediatric population. Glucose metabolism in patients with obesity is altered in health with chronic inflammation and dysregulated immune pathways, leading to impaired glucose metabolism. This subset of patients may require special attention when dealing with stress hyperglycemia.

Stress hyperglycemia and outcomes

Studies in children have challenged the assertion that hyperglycemia is beneficial or inconsequential by observing that SHG is associated with worse clinical outcomes. A retrospective study from a single PICU examined 1173 admissions. Hyperglycemia was prevalent and associated with increased morbidity, as characterized by increased LOS and mortality. Association between hyperglycemia and worse outcome in children was also demonstrated in specific disease processes, such as traumatic brain injury, general trauma, severe burns, septic shock, meningococcal sepsis, and postoperative congenital heart disease. ^, Hyperglycemia is common in infants with necrotizing enterocolitis admitted to the neonatal ICU (NICU) and is associated with increased late mortality and NICU LOS. SHG is also associated with specific complications, such as increased risk of venous thromboembolism in nondiabetic children, increased risk of mortality from central catheter–associated bloodstream infections, and more frequent nosocomial infections, including surgical site infection.

While clearly prevalent in critically ill children, some studies were unable to show a clear association between hyperglycemia and worse outcomes. One retrospective study found that hyperglycemia within 24 hours of PICU admission was associated with increased rate of mechanical ventilation, ICU LOS, and mortality, but when controlled for disease severity, it was not independently associated with increased morbidity or mortality. Another retrospective study evaluated the association between blood glucose level and duration of mechanical ventilation and ICU LOS in mechanically ventilated patients with bronchiolitis. Hyperglycemia was a frequent event in this patient population, yet results failed to show an independent association with worse outcomes. Such studies support the notion that hyperglycemia may be a marker of severity of illness rather than a cause.

Preexisting nutritional status may also impact outcomes associated with hyperglycemia in the critically ill child. A prospective study from Brazil reported that malnourished patients with hyperglycemia were at greater risk of mortality independent of severity of illness. Obesity is prevalent among critically ill pediatric patients, but the available literature on the relationship between obesity and clinical outcome is limited and conflicting. A systematic review of recent observational studies showed increased mortality in obese critically ill pediatric patients, while two separate retrospective single-center analyses revealed no difference in mortality by weight status. ^,

With current knowledge, it is clear that hyperglycemia is prevalent in critically ill children and is associated with worse outcome in some disease processes but not in others. Many studies are not controlled for severity of illness, making it difficult to interpret results. Different definitions for SHG used by different authors (range of 126–250 mg/dL in nine key pediatric studies of association of SHG and mortality) make it even harder to compare results and create thresholds for treatment. Moreover, thus far, all studies have failed to establish cause-and-effect relationships, yet many suggest that aggressive maneuvers should be used to normalize plasma glucose levels. Younger patients (<1 year) are at higher risk for spontaneous hypoglycemia and require special consideration when treating hyperglycemia with insulin.

Pathophysiology of stress hyperglycemia

During stress, the normal mechanisms that counteract hyperglycemia are overwhelmed, causing a persistent unchecked state of high glucose blood levels. These changes help the body provide glucose to meet increased metabolic demands. SHG results from increased levels of counterregulatory hormones (epinephrine and norepinephrine, glucagon, cortisol, and GH) and proinflammatory cytokines (TNF-α, IL-1, and IL-6). The overall effect is increased hepatic and renal glucose production. Peripheral and hepatic insulin resistance is a well-recognized phenomenon in critically ill patients. It is characterized by organ-specific alteration in glucose utilization/production and impaired insulin-mediated uptake. Insulin concentrations may be elevated or decreased. Use of carbohydrate-based feeds, glucose-containing fluids, and drugs such as epinephrine and corticosteroids may exacerbate the situation.

High hepatic output of glucose, especially through gluconeogenesis, is the most important contributor to SHG. Glycogen stores are limited and rapidly depleted during stress. Lactate, pyruvate, and alanine are the main precursors used by the liver for gluconeogenesis. Often overlooked, renal-derived gluconeogenesis is a significant contributor (up to 40%) of glucose production during stress, mostly in response to epinephrine. The principal precursors for renal gluconeogenesis are lactate and glycerol ( Fig. 84.4 ).

Schematic overview of gluconeogenesis. Pyruvate is generated from glycolysis, lactate, or alanine through pyruvate kinase, lactate dehydrogenase (LDH), and alanine aminotransferase (ALT), respectively. Pyruvate enters the mitochondria freely and is converted into oxaloacetate, which is then converted into malate to enter the malate shuttle and cross the mitochondrial membrane into the cytoplasm. In the cytoplasm, it is again converted into oxaloacetate and, through phosphoenolpyruvate carboxykinase (PEPCK), is converted into phosphoenolpyruvate that serves as substrate for a series of enzymatic-driven reactions and is finally converted into glucose. It should be noted that the rate-limiting step of gluconeogenesis is the conversion of fructose biphosphate into fructose 6-phosphate and is regulated by the actions of glucagon (stimulates) and insulin (inhibits) on fructose 1,6-biphosphatase. Triglycerides also contribute to gluconeogenesis by their breakdown into fatty acids and glycerol 3-phosphate. The latter is then transformed into dihydroacetone phosphate and then into fructose 1,6-biphosphate to follow the rest of the gluconeogenic pathway and result in the generation of glucose.

Mechanisms underlying insulin resistance occur at several levels. Insulin receptor levels are unchanged in most short-term animal models of sepsis. However, reduction in insulin receptors is seen in longer-term models. One known mechanism for hepatic insulin resistance is associated with an increase in GH and reduction in insulin growth factor-1 (IGF-1). During critical illness, GH levels increase significantly, but there is a fall in hepatic GH receptors with disruption of downstream signaling. IGF-1 levels drop in response to proinflammatory cytokines, especially TNF-α with decreased IGF-1 synthesis. In addition, low IGF-1 may result from upregulation and increased affinity of its binding protein IGFBP-3, reducing the free active protein.

Elevated insulin levels are common in critically ill adults. The critically ill child may present with insulin deficiency due to β-cell dysfunction and impaired insulin production (direct effect of proinflammatory cytokines), which contributes to SHG. ^,

Insulin resistance ultimately promotes a catabolic state in which lipolysis is activated. Lipotoxicity, glucotoxicity, and inflammation are key components of global SHG. Hyperglycemia itself further exacerbates the inflammatory and oxidative stress response and proinflammatory cytokine storming, promoting a vicious cycle whereby SHG leads to further SHG.

During critical illness, specific interventions can mediate development of SHG. Use of vasoactive-inotropic drugs—such as epinephrine, norepinephrine, and dopamine—is frequently associated with SHG. Epinephrine stimulates β ₂ -receptors, promoting glycogenolysis and gluconeogenesis, and increases insulin resistance by release of glucagon and cortisol. It also reduces insulin secretion via stimulation of α ₂ -receptors. Effects of dopamine and norepinephrine are less prominent due to lesser activity at the β ₂ -receptors. Several medications commonly used in the ICU setting may result in development of SHG (e.g., patients frequently receive antifungal and antibiotic medications in large volumes of dextrose-containing fluids). Corticosteroids can increase the risk of SHG, especially when given in bolus doses. Thiazide diuretics are also associated with the occurrence of SHG. Calcineurin inhibitors, such as tacrolimus and cyclosporine, can result in SHG and posttransplant diabetes due to decreased insulin biosynthesis and release.

Nutritional support practices strongly influence SHG. Critically ill children are frequently prescribed parenteral nutrition (PN). Provision of excess carbohydrate calories in PN can result in SHG, which has been associated with increased risk of mortality in critically ill pediatric patients. Overfeeding is common in critically ill children, regardless of whether PN or enteral nutrition is employed. Studies have shown that commonly used predictive equations to calculate caloric needs are inferior to targeted indirect calorimetry and frequently result in overprescription of calories.

Mechanisms of stress hyperglycemia adverse outcomes

Postulated mechanisms by which SHG causes harm include direct cellular damage and alterations of essential organ function. In diabetic patients, four main molecular mechanisms have been identified in glucose-mediated complications: (1) increased polyol pathway flux, (2) increased advanced glycation end-product formation, (3) activation of protein kinase C isoforms, and (4) increased hexosamine pathway flux. Each of the four pathogenic mechanisms reflects a hyperglycemia-induced process, namely, overproduction of superoxide anion by the mitochondrial electron-transport chain. Diabetes-related injury develops over years, but some common mechanisms parallel acute stress-related hyperglycemia. During SHG, overexpression of insulin-independent transporters (glucose transporter types 1 to 3 [GLUT-1 to GLUT-3]) results in glucose overload and toxicity essentially in every organ. Cells damaged by hyperglycemia are primarily those unable to effectively control their intracellular glucose concentration—notably, neuronal, capillary endothelium, and renal mesangial cells. Glucose overload results in excessive glycolysis and oxidative phosphorylation with increased production of reactive oxygen species such as superoxide anion, the same toxic end product involved in the injury pathway for diabetic patients. Reactive oxygen species cause mitochondrial dysfunction and altered metabolism with subsequent apoptosis and cellular and organ system failure in the critically ill child. Glucose overload can also lead to glycation, the reaction of glucose with the amine group of proteins, which may impair the function of these proteins.

Hyperglycemia is a risk factor for infection in acute illness. The relative bacterial overgrowth witnessed in hyperglycemia may be partly due to altered host defenses. Acute, short-term hyperglycemia impairs macrophage activity, reduces polymorphonuclear leukocyte chemotaxis and bactericidal capacity, and alters complement fixation in critically ill patients. SHG affects all major components of innate immunity and impairs the ability of the host to combat infection. Furthermore, hyperglycemia is associated with poor gut motility, a factor that may be important in bacterial overgrowth and translocation. A raised blood glucose level is also recognized as being proinflammatory and pro-oxidant. Mononuclear cells isolated from healthy volunteers exhibited higher levels of NF-κB binding activity, raised reactive oxygen species, and increased levels of TNF-α mRNA following exposure to hyperglycemia.

Hyperglycemia also results in a hypercoagulable state partly through the increased expression of tissue factor, which is both pro-coagulant and proinflammatory. SHG is implicated in other abnormalities, such as endothelial dysfunction and alteration in vascular smooth muscle tone, commonly observed during critical illness. Likewise, hyperglycemia has been associated with deleterious effects on the nervous system. Underlying mechanisms in critical illness remain largely speculative and are often extrapolated from knowledge in diabetic patients. Hyperglycemia-induced blood-brain barrier permeability, oxidative stress, and microglia activation may play a role and compromise neurons and glial cell integrity.

Clinical trials examining management of critical illness hyperglycemia

In 2001, a single-center adult study reported reduction of hospital mortality by more than 30% using a tight glycemic control (TGC) protocol. The effect was attributed to the actual glycemic control rather than the infused insulin dose. These impressive results brought the issue of SHG to clinical attention and fostered considerable discussion. Previously seen as an aspect of a normal stress response, physicians now started viewing SHG differently, considering it to be a major cause or contributor to pathophysiology that must be aggressively addressed and treated. The appeal of such straightforward intervention was too great to resist. Subsequent studies failed to reproduce these results, yet guidelines generated by professional societies initially recommended TGC for adult critically ill patients. ^, A large international randomized multicenter study involving more than 6000 adult patients and many other smaller studies reported that TGC increased mortality and risk for severe hypoglycemia among adults in the ICU. In the setting of such consistent negative results, guidelines were revised and currently recommend using a higher glucose threshold for initiation of insulin therapy at 150 mg/dL, with the goal of keeping blood glucose <180 mg/dL, focusing on close monitoring and safety margins to avoid hypoglycemia and minimize glucose variability. While TGC became the standard of care for adults, the pediatric critical care community was hesitant to adopt any guidelines or consistent standard approach. There are, however, several prospective randomized clinical trials to guide practice.

In very-low-birth-weight neonates, a multicenter trial of insulin with continuous 20% dextrose infusion was terminated prematurely for concerns of futility and potential harm associated with hypoglycemia. This study took a proactive approach to glycemic control in that the treatment group received insulin with glucose infusion regardless of their blood glucose level before the intervention. Considering the study population and the fact that the study was not designed to treat hyperglycemia, it is difficult to compare the results with any other pediatric study.

Five randomized prospective studies have examined the association between TGC and clinical outcomes in critically ill children. The first study, published in 2009, was derived from a single center in Belgium. The study enrolled a mixed medical/surgical patient population, although 75% of the subjects had undergone cardiac surgery. The study targeted age-adjusted glycemic range for infants and children, 50 to 80 mg/dL in children less than 1 year old, and 70 to 100 mg/dL in the remainder. Results showed improved short-term outcome, including mortality, in the TGC group despite the fact that the TGC group had severe hypoglycemia (<40 mg/dL) at unacceptable rates (25% overall and 44% in neonates).

A two-center prospective randomized trial published in 2012 enrolled 980 children below age 3 years who underwent cardiac surgery with cardiopulmonary bypass. The authors reported that TGC (target range, 80–110 mg/dL) could be achieved with a low hypoglycemia rate. However, the study found no clinical benefit for TGC in terms of infection rate, mortality, LOS, or measures of organ failure when compared with standard care. A post hoc analysis of this study demonstrated that TGC may, in fact, lower the rate of infection in children older than 60 days of age at the time of cardiac surgery when compared with standard care. In a secondary analysis of this trial, insulin appeared to have no discernible impact on skeletal muscle degradation.

The concern for the impact of hypoglycemia on neurocognitive long-term outcome was addressed by both investigator teams. Four-year neurocognitive follow-up in the single-center study ascertained that insulin-induced hypoglycemia caused by TGC was not associated with worse neurocognitive outcome. However, the outcomes of both treatment groups were similar to the few patients who developed moderate or severe hypoglycemia in the two-center, cardiac-only trial. The group that had no hypoglycemia, as reported by continuous glucose monitoring, had a markedly better neurocognitive outcome than the other three groups, raising the possibility that the group in the first trial with no hypoglycemia detected may have had undetected hypoglycemia leading to the moderately impaired outcomes. Subsequent studies have confirmed the dangers of hypoglycemia in this population. Taken together, these data suggest that, in order to ensure optimal outcome, hypoglycemia should be assiduously avoided.

In 2014, a large multicenter randomized trial involving 13 centers in the United Kingdom reported that TGC in critically ill children had no significant effect on major clinical outcomes (number of days alive and free from mechanical ventilation at 30 days after enrollment), but patients in the TGC arm had lower need for renal replacement therapy and reduced 12-month healthcare costs. These effects were mostly notable in the noncardiac patient population.

In 2010, a single-center study focusing on pediatric patients with severe burns concluded that intensive insulin therapy significantly decreased infections and sepsis and improved organ function by decreasing inflammation.

After five randomized clinical trials of TGC to low versus high target ranges, this area of critical care therapeutics has become one of the most well studied in the field. The end result in general pediatric ICU and cardiac ICU patients, although initial promising findings were noted in the original single-center trial, is that low targets produce little to no benefit yet increase hypoglycemia, which is becoming increasingly associated with harm. Consensus has evolved that insulin infusion should be initiated when glucose levels reach 150 mg/dL, with the goal of keeping blood glucose less than 180 mg/dL. In the burn population, which has repeatedly been shown to be physiologically different from other critically ill children, the single-center study that has been completed stands in support of targeting a low range of 80 to 110 mg/dL.

Clinical manifestations

Diaphoresis, tremor, tachycardia, anxiety, weakness, hunger, nausea, and vomiting are all autonomic manifestations caused by the adrenergic stress response that occurs with a rapid decline in blood glucose levels. Other symptoms associated with hypoglycemia are a result of a deficiency of the brain’s primary energy substrate, which are known as neuroglycopenic symptoms. These symptoms include headache, visual disturbances, lethargy, restlessness, irritability, dysarthria, confusion, somnolence, stupor, coma, hypothermia, seizures, and motor and sensory disturbances. The glycemic ranges at which these symptoms manifest vary, as critically ill patients cannot recognize or communicate symptoms. The picture is further masked by sedation and analgesia.

Pathogenesis

Imaging studies of infants who sustained neonatal hypoglycemic brain injury display diffuse cortical and subcortical white matter damage that is most prominent in the parietal and occipital lobes. This pattern differs from the neuroimaging features of other neonatal insults, including hypoxic-ischemic encephalopathy. Interestingly, this pattern does not resemble the glucose uptake pattern of neonatal brains by positron emission tomography, which may indicate that neuronal damage is not simply due to cerebral deprivation of its primary substrate for energy production. Evidence indicates that hypoglycemia activates receptors for excitatory amino acids within the brain and causes cell depolarization, with subsequent cellular edema and apoptosis.

Fasting adaptation

Consumption of glucose is largely dependent on the brain-to-body ratio. This phenomenon explains the reduced fasting tolerance of infants whose glucose utilization rate (approximately 6 mg/kg per minute) is significantly higher than that of older children and adults (1 to 2 mg/kg per minute). This reality places younger patients at increased risk of hypoglycemia. In addition, their ability to maintain euglycemia through glycogenolysis and gluconeogenesis is reduced because glycogen stores and muscle bulk are small, thus reducing the pool of available gluconeogenic substrates. Within the brain, astrocytes, but not neurons, are capable of storing glycogen. The brain contains less than 1 mmol/kg of free glucose reserve. Fasting tolerance increases rapidly in the first days of life. Neonates may fast up to 18 hours after 1 week of age. By 1 year, a 24-hour fast is tolerated; by 5 years, a child may fast for up to 36 hours without experiencing hypoglycemia.

Understanding fasting physiology is crucial to the logic and methodologic approach required for diagnosing the etiology of hypoglycemia. Normally in the postabsorptive state, metabolism is governed primarily by counterregulatory hormones. In the first 4 hours of a fast in infants or in the first 8 hours in older children, glucagon is released and euglycemia is maintained primarily by glycogenolysis. Following glycogen store depletion, gluconeogenesis gains importance in the maintenance of normal glucose levels (see Fig. 84.4 ).

Muscle provides amino acids, particularly alanine and glutamine, as gluconeogenic substrates. Glycerol 3-phosphate derived from triglyceride hydrolysis is also a gluconeogenic precursor. Fatty acids resulting from triglyceride hydrolysis are transported to the liver, where they are oxidized to generate acetyl CoA and ketones. The latter may then be used as alternative fuel by skeletal and cardiac muscle to help ensure availability of glucose to the brain and to erythrocytes that are strictly dependent on glucose for energy production. The brain may also use ketones as an alternative fuel source, but it does so only during a prolonged fast.

Hypoglycemia that occurs early during fasting may indicate hormonal imbalance or a primary disorder of glycogenolysis. Disorders of gluconeogenesis (see also Chapter 81 ) will not manifest during early fast. They become apparent only after glycogen stores have been depleted; hence, typically, they present later in infancy once feeding intervals become increasingly prolonged. The same is true for fatty oxidation disorders. These disorders generally require a more prolonged fast to manifest, nearing 12 to 18 hours in infants and 18 to 24 hours in older children. However, the most common cause of childhood hypoglycemia is ketotic hypoglycemia. This illness most frequently occurs in toddlers and preschoolers and is uncommon after 8 to 9 years. It is typically triggered by intercurrent infection and caloric restriction, both common events in the PICU. A defect in protein catabolism, transamination, or amino acid efflux from skeletal muscle, as well as impaired autonomic regulation of epinephrine secretion, has been postulated.

Hypoglycemia has been observed in association with a variety of critical illness diagnoses, including sepsis, congestive heart failure, renal failure, liver failure, and pancreatitis, and it has been associated with increased mortality among critically ill children. ^, Critically ill patients are at risk of hypoglycemia not only because of their underlying illness but also because of factors unique to their hospitalization, such as muscular atrophy from prolonged immobilization and gluconeogenic substrate depletion, undernutrition often resulting from the limitation of caloric intake because of fluid restriction, increased glucose consumption, AI, loss of IV access or inadvertent disconnection of infusion lines, or iatrogenic factors related to drugs and therapies, including the practice of TGC.

Hypoglycemia treatment

After obtaining the “critical” blood/urine samples, administration of 2 mL/kg of 10% dextrose water solution (or an equivalent dose of dextrose) is indicated for patients with hypoglycemia. Subsequently, an IV maintenance fluid regimen should be considered to provide a glucose infusion rate of 6 to 8 mg/kg per minute. Serum glucose should be rechecked 15 minutes after the initial bolus; if hypoglycemia persists, a repeat bolus of 2 to 4 mL/kg of 10% dextrose water (or an equivalent dose of dextrose) should be administered and the glucose infusion rate increased by 25% to 50%. If the volume of fluid required to maintain glucose concentrations greater than 70 mg/dL is excessive, a higher dextrose concentration should be used. Glucagon (0.03 mg/kg for patients <30 kg, or 1 mg for patients >30 kg) can reverse hypoglycemia in patients with adequate glycogen stores and normal glycogenolytic pathways. Definitive treatment will depend on the underlying etiology.

In summary, hypoglycemia is a manifestation of iatrogenic, intentional, or accidental drug ingestion or administration or the manifestation of an underlying disorder. All critically ill patients with hypoglycemia should raise a high index of suspicion because many defects that cause hypoglycemia remain silent until an intercurrent illness or stress overwhelms the compensatory capacity of the individual. Unless certitude of the etiology of the hypoglycemia exists before therapy, a “critical” blood/urine sample should be obtained to guide diagnosis and further management. Prompt recognition and treatment are necessary to prevent neurologic injury. A multidisciplinary approach, including endocrine and/or metabolism consultation, is often necessary.

Thyroid biochemistry

Thyroid-stimulating hormone (TSH) derived from the anterior pituitary is a pleotropic hormone that modulates all aspects of thyroid hormone synthesis. TSH action within the thyroid follicular cells facilitates the sodium iodide symporter, resulting in (1) enhanced iodine concentration in the thyroid gland; (2) increased synthesis of thyroglobulin, the site of tyrosine residues destined for iodination; and (3) activated thyroid peroxidase, which catalyzes iodination of tyrosine residues as well as tyrosine coupling. It is important to note that autoantibodies may bind to TSH receptors and stimulate a response similar to TSH, resulting in a hyperthyroid state. Leptin is likely to mediate an important role in the regulation of the thyroid axis, as suggested by the close correlation between the circadian rhythm of leptin secretion and TSH.

An overview of thyroid hormone biosynthesis and secretion is provided in Fig. 84.5 . In this schematic diagram, iodide is transported into the thyroid follicular cell by the action of the sodium-iodide symporter (NIS). Subsequently, this iodide diffuses passively through the iodide channel termed pendrin (P). Thyroglobulin (TG) is synthesized within the rough endoplasmic reticulum (ER) and subsequently packaged by the Golgi apparatus into thyroglobulin secretory vesicles that are released into the follicular cell lumen. Thyroid oxidase (TO) produces hydrogen peroxide that is subsequently used by thyroid peroxidase (TPO) to oxidize iodide to iodine, which subsequently reacts with the tyrosine residues within thyroglobulin to produce monoiodotyrosine (MIT) and diiodotyrosine (DIT) residues within the thyroglobulin peptide.

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