STACEY R. ROSE

DEFINITION

Jaundice is the yellow discoloration of the skin, mucous membranes, and sclerae caused by elevated serum levels of bilirubin, a by-product of heme breakdown. Bilirubin is a lipophilic pigment and must bind to plasma albumin to be transported to the liver. It is then taken up by hepatocytes for conjugation with solubilizing sugars to form bilirubin diglucuronides (and, less commonly, monoglucuronides), which can be excreted into bile. Several factors can cause jaundice. While many of these processes are pathologic, physiologic jaundice in neonates, a benign process, accounts for the vast majority of clinically encountered jaundice in pediatrics.

CAUSE AND FREQUENCY

Jaundice may be secondary to an unconjugated or conjugated hyperbilirubinemia (Table 15-1). In general, unconjugated hyperbilirubinemia results from overproduction of bilirubin, impaired uptake of bilirubin by hepatocytes, or impaired conjugation. A primary cause of overproduction is hemolysis, which is usually associated with other laboratory abnormalities including anemia, elevated LDH, low haptoglobin, and increased reticulocyte count. Reduced uptake of bilirubin can be due to poor blood flow to the liver, certain drugs, and various inherited diseases. Impaired bilirubin conjugation is usually due to various inherited disorders, such as Gilbert syndrome or Crigler-Najjar, where the enzymes needed for conjugation are deficient.

Conjugated hyperbilirubinemia occurs secondary to cholestatic conditions or direct hepatocellular injury. Cholestasis results from intra- or extrahepatic impairments in bile flow, and is accompanied by elevations in alkaline phosphatase and/or gamma-glutamyl transpeptidase (GGT). The differential diagnosis of cholestatic jaundice in the older child differs from diseases that present early in life. Young infants are more likely to have congenital anatomic anomalies, such as biliary atresia, or inborn metabolic disorders such as galactosemia. In contrast, older children are more likely to experience acquired or secondary liver diseases, such as cholelithiasis or sclerosing cholangitis. There is often an overlap between syndromes causing cholestasis and those resulting in hepatocellular injury. Generally, hepatocellular injury is accompanied by elevations in the transaminases (AST and ALT). Additionally, synthetic liver dysfunction, evidenced by hypoalbuminemia as well as prolonged coagulation measurements, may also be present. There are many causes of hepatocellular injury including infectious, autoimmune or toxic hepatitis, or metabolic processes such as alpha-1 antitrypsin deficiency.

QUESTIONS TO ASK AND WHY

• Is the elevated bilirubin level all unconjugated? Is the process a conjugated hyperbilirubinemia?

—Separating a total bilirubin measurement into its conjugated and unconjugated components is a critical step in the evaluation of hyperbilirubinemia in a child. Conjugated hyperbilirubinemia is present when the conjugated fraction is at least 1.5 mg/dL or accounts for greater than 15% of the total bilirubin measurement. Conjugated hyperbilirubinemia is abnormal and merits prompt evaluation, particularly in infants, since diseases like biliary atresia require urgent therapy. An increased unconjugated bilirubin level suggests a very different differential diagnosis and may also be a medical emergency when levels are very high since unconjugated bilirubin is able to cross the blood-brain barrier and directly injures the brain.

Sometimes the terms “direct” and “indirect” bilirubin are used interchangeably with the terms “conjugated” and “unconjugated.” The former terms derive from the van den Bergh reaction in which the conjugated bilirubin component is measured directly (by colorimetric analysis after reaction with a diazo compound). In the van den Bergh assay’s next step, the addition of methanol allows for a measurement of total bilirubin; the unconjugated fraction is then determined—indirectly—by subtracting the conjugated bilirubin level from the total bilirubin level. Of note, measurement of the direct bilirubin fraction detects not only bilirubin di- and mono-glucuronides, but also “delta” bilirubin, which forms when conjugated bilirubin seeps retrograde into the serum and binds covalently to albumin. Because of the delta component’s long half-life, the “direct fraction” can remain deceptively elevated even as a conjugated hyperbilirubinemia improves.

• Does the jaundiced baby have other concerning physical findings?

—A significant unconjugated hyperbilirubinemia can result from the accelerated breakdown of red blood cells secondary to a cephalohematoma or extensive bruising. A newborn afflicted with a TORCH infection might have microcephaly, growth retardation, hepatosplenomegaly, chorioretinitis, or rash. A heart murmur is often heard in children with Alagille syndrome, while a baby with Zellweger syndrome will be hypotonic and dysmorphic. Additionally, the presence of hypotonia, opsithotonus (backward arching of the trunk), or retrocollis (backward arching of the neck) on neurologic examination should raise immediate concerns for acute bilirubin encephalopathy or kernicterus.

• Is there a family history of jaundice?

—Many of the disorders that present with jaundice are heritable. Alpha-1-antitrypsin deficiency, Crigler-Najjar syndromes type I and II, galactosemia, and tyrosinemia are just a few of the auto-somal recessive diseases associated with neonatal jaundice. However, Alagille syndrome is an autosomal dominant disorder (but with variable reentrance and expressivity). The inheritance of glucose-6-phosphate (G6PD) deficiency is X-linked but so highly polymorphic that it should be considered in the evaluation of boys and girls alike.

• Were there changes in the child’s diet, or other new “exposures,” that preceded the onset of jaundice?

—Deficiencies in the metabolism of galactose or fructose can lead to jaundice in infants. Likewise, children with G6PD deficiency can have hemolytic crises triggered by certain foods (e.g., fava beans), medications (e.g., sulfa drugs), and other compounds (e.g., mothballs).

• Does the baby have risk factors for severe neonatal hyperbilirubinemia?

—Risk factors for neonatal jaundice include intrauterine and perinatal complications such as gestational diabetes, prematurity, blood group incompatibility, or birth trauma resulting in extra-vascular blood collections. Other independent risk factors for the infant include ethnicity (East Asian, Native American, and others), polycythemia, acidosis, hypoalbuminemia, exclusive breastfeeding, urinary tract infection or sepsis, and a long, heterogeneous list of genetic disorders.

SUGGESTED READINGS

1. Abrams SH, Shulman RJ. Causes of neonatal cholestasis. UpToDate. www.uptodate.com/contents/causes-of-neonatal-cholestasis. Updated September 1, 2010. Accessed September 22, 2011.

2. American Academy of Pediatrics Subcommittee on Hyperbilirubinemia. American Academy of Pediatrics Clinical Practice Guideline: Management of hyperbilirubinemia in the newborn infant 35 or more weeks of gestation. Pediatrics. 2004;114:297-316.

3. Dennery PA, Seidman DS, Stevenson DK. Neonatal hyperbilirubinemia. N Engl J Med. 2001;344:581-590.

4. Maisels MJ. Neonatal jaundice. Pediatr Rev. 2006;27:443-453.

5. Maisels MJ, McDonagh AF. Phototherapy for neonatal jaundice. N Engl J Med. 2008;358:920-928.

CASE 15-1

One-Day-Old Girl

STACEY R. ROSE

HISTORY OF PRESENT ILLNESS

The patient is a 1-day-old girl in the newborn nursery. The baby was born the previous night at term by vaginal delivery. This morning, the nurses noted that she appeared jaundiced. She has some nasal congestion since birth but is otherwise doing well. She is bottle-feeding, taking 1-2 oz of formula every 2-3 hours with normal urine and stool patterns. She is afebrile.

MEDICAL HISTORY

The baby was born at 37 2/7 weeks by a precipitous vaginal delivery to a 20-year-old G5P3 mother. Apgar scores at 1 and 5 minutes were 9 and 9, respectively. The patient’s mother did not receive any prenatal care and all prenatal laboratories are unknown, except for her blood type which is A+. There were no known complications during pregnancy. Since the delivery was precipitous, she did not receive antibiotics prior to giving birth. She was afebrile at delivery and rupture of membranes occurred 4 hours prior.

PHYSICAL EXAMINATION

T 36.7°C; HR 146 bpm; RR 42/min; BP 89/46 mmHg; Pulse oximetry 100%; Weight 2.77 kg (10th percentile); Length 47 cm (10th percentile); Head Circumference 32 cm (5th percentile)

The patient is awake and alert. On HEENT examination, she has a flat, open anterior fontanelle, scleral icterus, and clear rhinorrhea. Her cardiac and lung examinations are within normal limits. Abdominal examination reveals a liver edge palpable 3 cm below the costal margin and a spleen palpable 1 cm below the costal margin. Her abdomen is otherwise soft, nontender, and nondis-tended with normoactive bowel sounds. The skin examination is significant for jaundice and erythematous peeling skin at her palms and soles but no other rash or petechiae. She has prominent axillary lymphadenopathy. While examining her extremities, she becomes irritable during palpation of her right arm and that she has little spontaneous movement of her arms or legs. However, there is no swelling or bruising along the extremities and she has full range of motion of all joints.

DIAGNOSTIC STUDIES

Complete blood count: WBCs, 29 000/mm³ (neutrophils 37%, bands 15%, lymphocytes 37%); hemoglobin, 12.7 g/dL; platelets, 48 000/mm³. Serum electrolytes: sodium, 136 mEq/L; potassium, 3.5 mEq/L; chloride, 105 mEq/L; bicarbonate, 22 mEq/L; blood urea nitrogen, 20 mg/dL; creatinine, 0.7 mg/dL; glucose, 72 mg/dL; calcium, 9.6 mg/dL. Liver function tests: total bilirubin, 4.1 mg/dL; direct bilirubin, 1.1 mg/dL; total protein, 7.1 mg/dL; albumin, 3.5 mg/dL; AST, 14 U/L; ALT, 47 U/L; alkaline phosphatase, 316 U/L.

COURSE OF ILLNESS

During the assessment, a rash noted on the mothers hands strongly suggested the infant’s diagnosis (Figure 15-1). Radiographs of the infant’s humerus (Figure 15-2) and femur (Figure 15-3) were also consistent with the diagnosis. The infant was admitted to the neonatal intensive care unit for additional diagnostic testing and treatment.

DISCUSSION CASE 15-1

DIFFERENTIAL DIAGNOSIS

The patient had an unconjugated hyperbilirubinemia with otherwise normal liver function tests. While many term infants develop physiologic jaundice within the first 24 hours of life, the presence of hepatosplenomegaly and thrombocytopenia should raise immediate concern for a pathologic process. Jaundice, hepatomegaly, and splenomegaly may be caused by congenital infections, often referred to as the TORCH infections; these infections can be acquired either in utero or during birth (Table 15-2). Given the lack of prenatal care, this patient is at particular risk for some of these conditions such as syphilis, HIV, and viral hepatitis. Sepsis and urinary tract infections can also cause an unconjugated hyperbilirubinemia, hepatomegaly, and thrombocytopenia and should be considered. Since the patient did not have a conjugated hyperbilirubinemia, anatomical or obstructive causes of hepatosplenomegaly, like biliary atresia, and metabolic processes, such as galactosemia, are less likely.

DIAGNOSIS

The mothers’ hand revealed a pink, elliptical macules (Figure 15-1); the central area was darker than the periphery, which blended into the surrounding skin. The reddish hue, due to localized hyperemia, is characteristic of early secondary syphilis. Laboratory testing was significant for an RPR of 1:8 in the mother and 1:64 in the baby. These positive tests were confirmed with a positive Treponema pallidum particle agglutination (TP-PA) assay. The infant received a lumbar puncture to evaluate for neurosyphilis. CSF protein and cell count were normal and CSF Venereal Disease Research Laboratory (VDRL) test was 1:8. She had a liver ultrasound that showed a homogenous enlarged liver and spleen with a normal gallbladder. The chest radiograph was normal. However, long-bone radiographs revealed metaphyseal lucencies involving the proximal humerus (Figure 15-2) and femur (Figure 15-3) that were consistent with the diagnosis of congenital syphilis. Testing for other TORCH infections as well as hepatitis B and C and HIV was negative. Given the presence of a positive RPR and TP-PA in both the mother and baby, in conjunction with the clinical findings of lymphadenopathy, jaundice, hepatosplenomegaly, and metaphyseal dystrophy, the patient was diagnosed with congenital syphilis.

INCIDENCE AND EPIDEMIOLOGY

Syphilis is a sexually transmitted infection caused by the spirochete Treponema pallidum. Syphilis in children may be either acquired, usually due to sexual abuse, or congenital, resulting from trans-placental transmission of the organism from an infected mother to her child. Rates of fetal transmission may occur at any stage of the disease and at any time during pregnancy but are highest when the mother is in the first and second stages of syphilis (60% to 90%) and lowest in late latent syphilis (<10%).

Rates of congenital syphilis parallel rates of syphilis in the adult population. There was a steep rise in the incidence of syphilis throughout the 1980s with a peak in congenital syphilis cases in 1991. Due in large part to enhanced screening, improved education for providers and increased awareness in communities with high rates of infection, syphilis rates fell precipitously through the 1990s, reaching a nadir in 2000, increasing again until 2008 with a slight decrease between 2009 and 2011. In 2011, there were 8.5 cases of congenital syphilis per 100 000 live births, resulting in 360 reported cases of congenital syphilis. Three states (Texas, California, and Florida) accounted for nearly one-half of all cases of congenital syphilis. Maternal risk factors associated with congenital syphilis include lack of, or poor prenatal care, unprotected sexual contact, trading of sex for drugs and cocaine abuse.

CLINICAL PRESENTATION

Transmission of syphilis during pregnancy can result in fetal or perinatal death, hydrops fetalis, intrauterine growth retardation, prematurity, or congenital abnormalities, which may occur early or late. Infants may be asymptomatic at birth but signs of early congenital syphilis usually present within the first few weeks of life. Late congenital syphilis results from chronic inflammation involving the bones, teeth, and CNS and appears after 2 years of age (Table 15-3).

The infant displayed many of the clinical features consistent with early congenital syphilis, including jaundice, hepatosplenomegaly, thrombocytopenia, rash, “snuffles,” pseudoparalysis, and metaphyseal dystrophy of the humerus and femur.

DIAGNOSTIC APPROACH

Darkfield microscopy. Identification of spiro-chetes from moist lesions by darkfield microscopy is the quickest and most definitive way to diagnosis syphilis. However, this method requires special equipment, reagents, and trained personnel that may not be available in all clinical settings. As a result, serologic testing is much more widely used.

Treponemal and nontreponemal serologic testing. Two forms of serologic testing are available; nontreponemal and treponemal tests. Because each of these tests has several limitations with significant false-positive and false-negative result rates, a combination of tests is needed to establish the diagnosis of syphilis. Generally, a nontreponemal test, such as a VDRL or rapid plasma reagin (RPR), is used to screen for the disease and to follow response to treatment. If either of these tests is reactive, a confirmatory treponemal test, such as the fluorescent treponemal antibody absorption (FTA-ABS) or T pallidum particle agglutination (TP-PA), is performed.

Since maternal antibody may be passively transmitted to the fetus even after adequate treatment of syphilis in the mother, interpretation of serologic testing in the infant may be difficult. As in this case, congenital syphilis is confirmed when the infant’s nontreponemal titers are at least four times greater than those of the mother. However, infants with titers less than fourfold their mothers’ values may still be diagnosed with congenital syphilis based on the presence of other features. These include certain physical examination findings, serum and CSF laboratory values, radiologic studies, the presence of treponemes in the umbilical cord or placenta, and the treatment status of the mother. Given the complex algorithm used to diagnose and treat syphilis, please refer to the Centers for Disease Control and Prevention or the American Academy of Pediatrics for specific diagnostic and treatment algorithms and additional information.

Additional testing. The serologic status of the mother must be established before any newborn infant is discharged from the hospital. If maternal screening is positive and inadequately treated or untreated syphilis is suspected, or if the baby has any signs of congenital syphilis, the infant should undergo a (1) complete physical examination; (2) quantitative serum nontreponemal test; (3) complete blood count, including platelet count; (4) lumbar puncture with testing for CSF cell count, protein concentration, and a VDRL of the CSF; and (5) long-bone radiographs. Among infected infants, the CSF is abnormal in 50% of those with symptoms and 10% of those without symptoms. Additional testing such as a chest radiograph, liver function tests, ultrasonography, ophthalmologic examination and auditory brainstem response testing should be considered in the appropriate clinical setting. Infants evaluated for congenital syphilis should also be evaluated for other congenital infections.

TREATMENT

Infants with proven or highly probably congenital syphilis should be treated with aqueous crystalline penicillin G or penicillin G procaine for 10 days. Nontreponemal titers should be followed closely to monitor response to treatment. If the initial CSF examination is abnormal, repeat lumbar punctures are recommended every 6 months until values normalize. Treatment failures are uncommon but treatment with an additional 10-day course of penicillin may be necessary if serum nontreponemal titers continue to rise or remain elevated, or, if the CSF evaluation remains abnormal. Infants with congenital syphilis should be examined and have quantitative nontreponemal tests every 2-3 months until nonreactivity is documented.

SUGGESTED READINGS

1. Azimi P. Syphilis (Treponema pallidum). In: Behrman RE, Kliegman RM, Arvin AR, eds. Nelson’s Textbook of Pediatrics. 17th ed. Philadelphia, PA: WB Saunders Co.; 2004:978-982.

2. Centers for Disease Control and Prevention: 2011 sexually transmitted diseases surveillance. http://www.cdc. gov/std/stats11/syphilis.htm. Updated December 13, 2012. Accessed December 26, 2012.

3. Hyman EL: Syphilis. Pediat Rev. 2006;27:37-39.

4. Johnson KE. Overview of TORCH infections. UpToDate. www.uptodate.com/content/overview-of-torch-infections. Updated March 15, 2011. Accessed September 29, 2011.

5. Michelow IC, Wendel GD, Norgard MV, et al. Central nervous system infection in congenital syphilis. New Eng J Med. 2002;346:1792-1798.

6. American Academy of Pediatrics. Syphilis. In: Pickering LK, Baker CJ, Long SS, McMillan JA, eds. Red Book: 2009 Report of the Committee on Infectious Diseases. 28th ed. Elk Grove Village, IL: American Academy of Pediatrics; 2009:638-651.

CASE 15-2

Six-Week-Old Boy

STACEY R. ROSE

HISTORY OF PRESENT ILLNESS

A 6-week-old full-term boy was referred by his pediatrician for persistent jaundice and poor weight gain. The infant was seen by his pediatrician during the first week of life after the mother noted that he “looked yellow.” At that time, he was otherwise doing well and the pediatrician diagnosed physiologic jaundice. He was brought to the pediatrician today for a well visit and it was noted that the patient was still jaundiced. Additionally, the patient has not gained any weight since his first visit at week 1 of life.

The infant is being fed a cow milk-based formula. The patient’s mother reports that he has frequent episodes of emesis. She also reports that the infant has been increasingly fussy during feeds. She denies that the infant has had any diarrhea, fever, bleeding, or bruising.

MEDICAL HISTORY

The infant was born at 38 weeks gestation by vacuum-assisted vaginal delivery. His birth weight was 3.2 kg. Maternal prenatal labs were normal. His hospital stay was unremarkable and he was discharged home with her mother on his second day of life.

The infant has a healthy 3-year-old brother. There was no family history of jaundice, liver disease, anemia, or familial blood disorders.

PHYSICAL EXAMINATION

T 37.0°C; HR 136 bpm; RR 32/min; BP 88/60 mmHg; Weight 3.25 kg (<5th percentile); Length 52 cm (10th-25th percentile); Head Circumference 37 cm (10th-25th percentile)

On examination, the patient was fussy but consolable by his mother. He was jaundiced with an open, flat fontanelle. He did not have any dysmorphic features. Scleral icterus was present. The lung and cardiac examinations were normal. His abdomen was soft and nondistended with normoactive bowel sounds. A smooth, firm liver edge was palpable 2 cm below the costal margin. Additionally, there was a 4 cm soft, mobile nontender mass noted in the right upper quadrant. The genitourinary, extremity, and neurologic examinations were all normal.

DIAGNOSTIC STUDIES

Complete blood count: WBC, 6900/mm³ (neutrophils: 43%, lymphocytes: 48%); hemoglobin, 11.2 g/dL; platelets, 332 000/mm³. Liver function tests: total bilirubin, 9.5 mg/dL; direct bilirubin; 8.4 mg/dL; albumin, 3.2 mg/dL; ALT, 167 U/L; AST, 188 U/L; alkaline phosphatase, 641 U/L; gamma glutamyl transferase, 524 U/L. Serum electrolytes: normal. Urinalysis: normal.

COURSE OF ILLNESS

The patient underwent several imaging studies and was admitted for urgent evaluation of his abdominal mass and cholestatic jaundice. A contrast gastrointestinal series suggested the diagnosis (Figure 15-4).

DISCUSSION CASE 15-2

DIFFERENTIAL DIAGNOSIS

The presence of an abdominal mass requires urgent evaluation. Most abdominal masses in the neonatal period are renal in origin and include hydronephrosis, multicystic dysplastic kidneys, polycystic kidneys, or Wilm tumor. Other common causes include neuroblastomas, hepatomas, choledochal cysts, GI duplication cysts, pyloric stenosis (the “olive” of pyloric hypertrophy), ovarian cysts, or teratomas. Because this patient’s mass was soft and mobile, it is most consistent with a nonretroperitoneal cystic structure.

Additionally, the patient has a persistent conjugated hyperbilirubinemia with elevations in alkaline phosphatase and gamma-glutamyl transferase consistent with neonatal cholestasis, a condition that results from accumulation of bile components in the blood due to impaired bile flow or excretion. There are a wide variety of causes, several of which require immediate intervention and hence prompt diagnosis and treatment are crucial.

Causes of neonatal cholestasis may be subdivided into various categories. Obstructive causes include biliary atresia, choledochal cyst, cholelithiasis, and paucity of intrahepatic bile ducts (Alagille syndrome). Though less common, some of the abdominal masses listed above, such as neuroblastomas, teratomas, or GI duplication cysts, can also cause cholestasis by compressing the biliary tree. Infectious, metabolic, or iatrogenic conditions may also be present, as outlined below (Table 15-4).

DIAGNOSIS

The patient had an abdominal ultrasound to assess the mass and hepatomegaly which revealed a 3.8 cm × 1.9 cm × 2.5 cm cystic structure inferior to the liver and adjacent to the right kidney, consistent with a choledochal cyst . Ultrasound also revealed a mildly enlarged liver and normal gallbladder. He had a hepatobiliary scan that failed to show tracer excretion into the small intestine. The gastrointestinal series showed a cystic structure in the right upper quadrant compressing the transverse colon (Figure 15-4). The structure was later identified as a choledochal cyst.

INCIDENCE AND ETIOLOGY

Choledochal, or biliary, cysts are cystic dilations in the biliary tree involving both intrahepatic and extrahepatic structures. They are a rare disorder, with an estimated incidence of 1:13 000 to 1 in 2 million. There is a 3:1 girl to boy predominance and some reports of familial occurrence. Incidence is highest in Asian countries, particularly Japan where more than half of the reported cases arise. Most cysts are thought to be congenital but some may be acquired. The pathophysiology remains unclear but leading theories suggest that they form due to the reflux of pancreatic enzymes into the common bile duct, which causes inflammation, weakness, and dilation of the duct. Other theories suggest an infectious cause related to fetal viral infection or abnormal in utero proliferation of biliary epithelial cells.

Biliary cysts have been divided into five sub-types (Table 15-5). Type I and IV cysts are the most common.

CLINICAL PRESENTATION

While choledochal cysts are most commonly seen in infants and children; an increasing number of patients are now diagnosed in adulthood. The classic pediatric presentation is a triad of abdominal pain, jaundice, and a palpable mass, though few patients present with all three symptoms in practice. Other common features in infants include failure to thrive, vomiting, and fever. Symptoms differ in older children and adults. An abdominal mass is rare and instead, many present with recurrent cholangitis, intermittent jaundice, and pancreatitis. If undetected, severe liver dysfunction, ascites, and coagulopathy may develop. Furthermore, there is a strong association between choledochal cysts and biliary malignancy, particularly in adult patients.

DIAGNOSTIC APPROACH

Abdominal ultrasound. Abdominal ultrasound is very effective in diagnosing choledochal cysts, particularly in infants or children and in adults if there is a high index of suspicion. Many cysts are now detected by prenatal ultrasound.

Direct cholangiography. The best method for definitive diagnosis of choledochal cyst or for delineating the precise cyst type and anatomy is by magnetic resonance cholangiopancreatography (MRCP) which has largely supplanted endoscopic retrograde cholangiopancreatography (ERCP) as the diagnostic test of choice because MRCP offers higher resolution of relevant anatomy. Less commonly used diagnostic options include percutaneous transhepatic cholangiography and intraoperative cholangiography. These techniques allow direct visualization of the involved biliary structures and help identify the presence of an anomalous pancreaticobiliary junction.

Other modalities. CT scanning may be used to delineate the cyst and its relationship to surrounding structures. Gastrointestinal contrast series, though performed in this case, are no longer routinely performed to diagnose choledochal cysts.

TREATMENT

The preferred treatment is surgical excision of the cyst and a roux-en-Y choledochojejunostomy. Complications from untreated cysts include recurrent cholangitis, pancreatitis, and biliary malignancy.

The infant was taken immediately to the operating room where he underwent direct cholangiography that revealed a choledochal cyst with dilation of the intrahepatic bile ducts and passage of contrast into the duodenum. The cyst was resected and a roux-en-Y hepatic jejunostomy was performed. The patient initially required parenteral nutrition but enteral feeds were slowly reintroduced as he recovered. One week after surgery, he was tolerating full feeds. His conjugated hyperbilirubinemia gradually improved and his direct bilirubin at the time of discharge had decreased to 2.6 mg/dL.

SUGGESTED READINGS

1. Lipsett PA, Pitt HA, Colombani PM, et al. Choledochal cyst disease: A changing pattern of presentation. Ann Surg. 1994;220:644-652.

2. Lipsett PA, Henry AP. Surgical treatment of choledochal cysts. J Hepatobiliary Pancreat Sci. 2003;10:352-359.

3. Suchy FJ. Cystic diseases of the biliary tract and liver. In: Behrman RE, Kliegman RM, Arvin AR, eds. Nelson’s Textbook of Pediatrics. 17th ed. Philadelphia, PA: WB Saunders Co.; 2004:1343-1345.

4. Topazian M. Biliary cysts. UpToDate. http://www.uptodate.com/contents/biliary-cysts. Updated September 24, 2010. Accessed September 1, 2010.

CASE 15-3

Eight-Year-Old Girl

STACEY R. ROSE

HISTORY OF PRESENT ILLNESS

An 8-year-old girl presents with history of 2 days of headache, abdominal pain, vomiting, diarrhea, and 1 day of fever. Two days prior to admission, the patient developed a frontal headache that was relieved with acetaminophen. Shortly after, she started to complain of bilateral lower abdominal pain that soon spread to her left upper quadrant. The abdominal pain became more severe throughout the day and woke her from sleep. Overnight, she started having episodes of nonbloody, nonbilious emesis and non-bloody watery diarrhea. On the day of admission, she developed fever to 104°F and her parents noted that her eyes looked yellow so they brought her to the emergency room for evaluation.

The patient also reports recent fatigue and occasional chills but denies cough, rhinorrhea, congestion, sore throat, neck stiffness, joint pain, myalgias, or rash.

MEDICAL HISTORY

The patient was a full-term baby born in Malaysia with no complications. She moved to the U.S. at the age of 5 months. She has always been well and has had no prior hospitalizations or surgical procedures. She is up-to-date on all immunizations. She does not have any known allergies and was not taking any medications recently, other than acetaminophen for the headache. There is no family history of sickle cell disease, bleeding disorders, or liver disease. She lives at home with her parents and younger brother and is in second grade. The patient and her family report that they recently traveled to Pakistan to visit grandparents. They spent about 6 months there and returned about 2 weeks prior. They did not receive any specific vaccinations or medications prior to or during their travel.

PHYSICAL EXAMINATION

T 38.9°C; HR 96 bpm; RR 18/min; BP 97/65 mmHg; Weight 27.2 kg (50th-75th percentile)

On physical examination, the patient was awake, alert, smiling, and in no significant distress. HEENT examination was significant for mild scleral icterus and conjunctival pallor. Her oropharynx was clear, her neck was supple, and she had no cervical lymphadenopathy. Her lungs were clear to auscultation bilaterally. Cardiac examination revealed a regular rate and rhythm with a II/VI systolic ejection murmur at the right upper sternal border. On abdominal examination she was found to have a soft abdomen with normoactive bowel sounds. She was diffusely tender to palpation without guarding or rebound. Her liver was palpable about 2 cm below the costal margin and she had splenomegaly with the tip palpable about 3 cm below the left costal margin. The remainder of her examination was within normal limits.

DIAGNOSTIC STUDIES

Complete blood count: WBCs, 5800/mm³ (neutrophils: 43%, lymphocytes: 45%, eosinophils: 5%); hemoglobin, 7.8 g/dL; mean corpuscular volume, 81.3 fL; platelets, 192 000/mm³. Serum electrolytes: sodium, 140 mEq/L; potassium, 3.2 mEq/L; chloride, 103 mEq/L; bicarbonate, 19 mEq/L; blood urea nitrogen, 14 mg/dL; creatinine, 0.6 mg/dL; glucose, 112 mg/dL. Liver function tests: total bilirubin, 3.5 mg/dL; unconjugated bilirubin, 3.4 mg/dL; conjugated, 0.1 mg/dL; albumin, 4.4 mg/dL; ALT, 71 U/L; AST, 80 U/L; alkaline phosphatase, 240 U/L; GGT, 75 U/L. LDH, 410 U/L (elevated). Reticulocyte count, 3.1%. Urinalysis, small bilirubin, negative for RBCs or WBCs. CRP, 3.8 mg/dL; ESR, 98 mm/h; PT, 14.3 sec; PTT, 29.3 sec; INR, 1.22.

COURSE OF ILLNESS

The patient was admitted to the hospital where a blood smear revealed the diagnosis (Figure 15-5).

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