Neuromuscular
Any developmental delay?
muscles: spasticity, contractures, hypotonia?
Seizures: controlled or not?
Medical treatment?
Airway
Difficult intubation/ventilation?
Any risk for regurgitation/inhalation? chronic lung infection?
Signs of obstructive or central sleep apnea?
Respiratory
Reactive airway?
Restrictive or obstructive syndrome?
Chronic lung infection?
Cardiovascular
Dysrhythmia?
Cardiomyopathy?
Others
Special diet?
Tolerates fasting?
Previous anesthesia?
Psychological issues?
Communication
But the child’s age should also be taken into account because, as for any pediatric case, (1) the younger the patient, the higher the risk; (2) young age has its own anatomic, physiologic, and pharmacologic specificities; and (3) because some pathologies become worse with age, for example, mucopolysaccharidosis and mitochondrial cytopathies.
The anesthesiologist should also keep in mind that a child with a metabolic disease remains a child: the “metabolic” tree should not hide the forest! The basic pediatric preoperative evaluation should be undertaken as in any child:
Personal history: previous anesthesia?
Allergies?
Bleeding problem?
Upper airway: mouth opening? retrognathia? facial asymmetry? midface hypoplasia? loose teeth? snoring during sleep?
Airway reactivity: recent infection? asthma? passive smoking?
Difficult venous access?
Cardiopulmonary examination?
The final anesthetic plan should also be adapted to the procedure for which anesthesia is needed, whether it is an emergency or not, and whether it will occur in an operating room or outside the operating theaters area. It should be borne in mind that an emergency procedure combines the risks of emergency anesthesia (full stomach) with the effects of fever, hypovolemia, and stress on the child’s metabolic equilibrium: the child’s pediatrician’s advice and the availability of a high-dependency bed for the early postoperative period are necessary in this context.
Last but not least, there are psychological issues to consider: as it grows, a child with a metabolic disease becomes a chronic medical patient with its “special needs” and phobias (mask, needle) but also with a critical eye on what is done around him/her. Moreover, compliance with treatment is often a critical issue at the time of adolescence. In short, a child with a metabolic disease is a fragile person and taking care of it, and of its family, needs a mix of science, vigilance, and compassion.
13.3 Example 1: A Urea Cycle Defect
The urea cycle is the succession of six successive enzymatic reactions to transform ammonia, the result of endogenous and exogenous protein catabolism, in urea which can be eliminated in the urine. It occurs only in the hepatocytes [5]. N-acetyl glutamate synthetase (NAGS) is one of the three mitochondrial enzyme participating to it. NAGS deficiency is transmitted as an autosomal recessive trait (NAGS gene, 17q21.31) and its prevalence is around 1/70,000. Its clinical signs vary according to the importance of the deficit and thus of the patient’s age:
Neonatal period: difficult feeding, vomiting a few hours after birth, and rapid evolution to hypotonic coma with seizures if not diagnosed and treated.
Infancy: anorexia, vomiting, and failure to thrive; these children often undergo diagnostic esophagogastroscopies before the definitive diagnosis is established.
Childhood and adolescence: episode(s) of acute decompensation presenting as a neurologic (encephalopathy, convulsions, ataxia, psychiatric problem), metabolic (coma), or hepatic (cytolysis, Reye-like syndrome) problem precipitated by a stress such as fever, postoperative period, infection, or administration of valproate acid.
The basic principle of the treatment of NAGS is avoiding protein catabolism. The children therefore need a special diet, the protein content of which is carefully adapted to the child’s age and decreased in case of infection or stress (e.g., surgery). They often also receive a daily dose of N-carbamyl glutamic acid (30–250 mg/kg/day) according to their blood urea and NH3 level. Orthotopic liver transplantation can be performed to cure the disease.
Anesthetic implications:
N: according to the child neurologic status
A: nothing specific to the disease
R: nothing specific to the disease
C: nothing specific to the disease
O
Special diet: a low-protein and hypercaloric diet should be started 1 or 2 days before elective surgery.
Preanesthetic fasting time has to be kept as short as possible; a glucose-containing solution with electrolytes should be administered at the beginning of the preanesthesia starving period.
Monitoring: NH3 (nl <50 μmol/L), glycemia.
In case of seizures, valproate should not be administered as it inhibits carbamylphosphate transferase, another enzyme of the cycle.
There is no specific contraindication to perform a regional block, which is a good way to reduce the patient’s perioperative stress response.
In case of surgery during or following which blood can enter the digestive tract (e.g., ENT, dental, or gastrointestinal surgery), the gastric content should be aspirated (nasogastric tube) because ingested blood is an important source of exogenous protein.
In case of hyperammonemia, the following should be administered in emergency: IV glucose 20 %, Na-benzoate (0.25–0.5 g/kg/day), Na-phenylbutyrate (0.5 g/kg/day), and l-arginine (0.25–0.5 g/kg/day). In case of failure or severe neurologic signs, hemodialysis or peritoneal dialysis should be performed.
13.4 Example 2: A Glycogenosis
In case of glycogenosis type III (also called Cori’s or Forbe’s disease), the absence of amylo-1, 6-glycosidase impairs complete degradation of glycogen in glucose: both a risk of hypoglycemia and accumulation of dextrin in hepatic and/or muscular cells ensue. Both the liver and the muscles are affected in type A while only muscles cells are affected in form B.
The accumulation of dextrin into the hepatocytes leads to hepatomegaly and progressively to hepatic fibrosis; in some cases, cirrhosis and hepatic adenomas develop during adolescence. These patients are often obese because they require frequent meals to avoid hypoglycemia. Cases of late hypertrophic cardiomyopathy have been described.
Anesthetic implications [6, 7]:
N: sometimes hypotonia in infancy; proximal amyotrophy with elevated CPK in adolescents and adults
A: macroglossia that may be present
R: respiratory comorbidities of obesity, asthma and obstructive sleep apnea
C: echocardiography to rule out cardiomyopathy
O
Hepatic function has to be checked; any sign of portal hypertension?
Difficult venous access and other comorbidities of obesity.
Preanesthetic fasting time has to be kept as short as possible; a glucose-containing solution with electrolytes should be administered at the beginning of the preanesthesia starving period.
Monitoring: blood glucose level.
Succinylcholine and use of a surgical tourniquet should be best avoided to prevent rhabdomyolysis (fragile muscles).
There is no specific contraindication to perform a regional block but ultrasound-guided peripheral nerve blocks could be more tricky to perform because amyotrophy modifies muscular echogenicity.
13.5 A Mitochondrial Cytopathy
The mitochondrion is the main energy provider of the cell and many metabolic reactions occur at least partly into it: metabolism of glucose (tricarboxylic or Krebs cycle), lipids (β-oxidation of fatty acids with the carnitine shuttle system), and protein (urea cycle). In addition, many neurodegenerative diseases (e.g., some forms of Parkinson or Charcot-Marie-Tooth disease) are now known to be caused by defects in what can be called the “maintenance functions” of the mitochondrion. But the term mitochondrial cytopathy refers mainly to pathologies of the respiratory chain or oxidative phosphorylation system, a succession of reactions occurring in the inner membrane of the mitochondrion: it generates an active proton (H+) and a free electron gradient leading to the production of ATP. The five protein complexes involved in the respiratory chain are encoded by genes that are present in the mitochondrial or in the nuclear DNA: their mode of transmission is complex being either maternal or autosomic dominant or recessive. Moreover, their phenotypic expression is highly variable depending on the relative distribution of wild and mutated mitochondria within each cell and on the energetic needs of the tissue wherein they are distributed (threshold effect) [8]. Mitochondrial cytopathies are usually called according to acronyms such as MERFF (myoclonus, epilepsy, ragged red fibers), MELAS (mitochondrial encephalopathy, lactic acidosis, stroke-like episodes), or their discoverer’s name (e.g., Leigh or Kearns-Sayre’s disease).
A peculiar aspect of the anesthetic care of mitochondrial cytopathies is that many anesthetic agents do interfere in vitro with the respiratory chain. Those data were obtained in vitro on wild mitochondria isolated from tissue: their relevance for clinical practice is thus difficult to define taking into account that almost all anesthetic agents have been used in patients with a mitochondrial cytopathy without observing major clinical effects. However, they should be kept in mind when planning anesthesia, for example:
Propofol inhibits complexes II and V of the respiratory chain as well as the intramitochondrial transport of free fatty acids by the carnitine system: a continuous infusion of propofol is thus considered as contraindicated because it could induce a propofol infusion syndrome (PRIS) [9]. However small case series have been published showing no untoward effect of a continuous infusion of propofol in patients with a mitochondrial cytopathy provided a glucose-containing solution was associated [10]. Recently a case of neurologic deterioration has been observed after a single dose of propofol given without glucose administration in a girl with MELAS syndrome but her clinical status was deteriorating before anesthesia: it is thus difficult to determine whether her metabolic deterioration would have occurred without propofol [11]. In any case, a glucose-containing solution (6 mg·kg−1·h−1) should always be associated with the use of propofol in patients with a known or suspected mitochondrial cytopathy, and their blood lactate level should be monitored if a continuous infusion of propofol is used.Related posts:
Pain After Surgical Correction of Congenital Chest Wall Deformities
Perioperative Care of the Pediatric Neurosurgical Patient
Acute Pain Management and Prevention
Perioperative Medicine
Long-Term Consequences of Anesthesia (and Surgery) on the Infant Brain
Perioperative Care of Children with Cerebral Palsy and Behavioral Problems
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