Nelson Pediatric 22nd Edition 2024, Volume 2 PDF

Summary

This document is from the 22nd edition of Nelson Textbook of Pediatrics, Volume 2, focusing on the digestive system. It discusses normal digestive tract phenomena, clinical manifestations of gastrointestinal disease, and potential causes of gastrointestinal issues(anorexia, vomiting, and diarrhea), in children. The document includes important details about infant development and potential physiological variances.

Full Transcript

 The Digestive System PART
XVI
during a meal. Toddlers and young children also tend to eat only a lim-
Section 1 ited variety of foods. Parents should be encouraged to view nutritional
intake over several days and not be overly concerned about individ-

Clinical Manifestations
ual meals. Infancy and adolescence are periods of rapid growth; high
nutrient requirements for growth may be associated with voracious
appetites. The reduced appetite of toddlers and preschool children is
of Gastrointestinal often a worry to parents who are used to the relatively greater dietary
intake during infancy. Demonstration of age-­appropriate growth on a

Disease growth curve is reassuring.
The number, color, and consistency of stools can vary greatly in
the same infant and between infants of similar age, without apparent
explanation. The earliest stools after birth consist of meconium, a dark,
viscous material that is normally passed within the first 48 hours of
Chapter 351 life. With the onset of feeding, meconium is replaced by green-­brown
transition stools, often containing curds, and, after 4-­5 days, by yellow-­

Normal Digestive Tract brown milk stools. Stool frequency is extremely variable in normal
infants and can vary from none to seven per day. Breastfed infants can
have frequent small, loose stools early (transition stools), and then after
Phenomena 2-­3 weeks can have very infrequent soft stools. Some nursing infants
might not pass any stool for 1-­2 weeks and then have a normal soft
Asim Maqbool and Chris A. Liacouras bowel movement. The color of stool has little significance except for the
presence of blood or absence of bilirubin products (white-­gray rather
than yellow-­brown). The presence of vegetable matter, such as peas or
corn, in the stool of an older infant or toddler ingesting solids is nor-
Gastrointestinal function varies with maturity; what is a physiologic mal and suggests poor chewing and not malabsorption. A pattern of
event in a newborn or infant might be a pathologic symptom at an intermittent loose stools, known as toddler’s diarrhea, occurs com-
older age. A fetus can swallow amniotic fluid as early as 12 weeks of monly between 1 and 3 years of age. These otherwise healthy grow-
gestation, but nutritive sucking in neonates first develops at about 34 ing children often drink excessive carbohydrate-­containing beverages.
weeks of gestation. The coordinated oral and pharyngeal movements The stools typically occur during the day and not overnight. The vol-
necessary for swallowing solids develop within the first few months ume of fluid intake is often excessive; limiting sugar and unabsorbable
of life. Before this time, the tongue thrust is upward and outward to carbohydrate-­containing beverages and increasing fat in the diet often
express milk from the nipple, instead of a backward motion, which lead to resolution of the pattern of loose stools.
propels solids toward the esophageal inlet. By 1 month of age, infants A protuberant abdomen is often noted in infants and toddlers, espe-
appear to show preferences for sweet and salty foods. Infants’ inter- cially after large feedings. This can result from the combination of weak
est in solids increases at approximately 4 months of age. The recom- abdominal musculature, relatively large abdominal organs, and lordotic
mendation to begin solids at 6 months of age is based on nutritional stance. In the first year of life, it is common to palpate the liver 1-­2 cm
and cultural concepts rather than maturation of the swallowing process
(see Chapter 61). Infants swallow air during feeding, and burping is
encouraged to prevent gaseous distention of the stomach.
A number of normal anatomic variations may be noted in the
mouth. A short lingual frenulum (“tongue-­tie”) may be worrisome to
parents but only rarely interferes with nursing, bottle feeding, eating,
or speech, generally requiring no treatment. Surface furrowing of the
tongue (a geographic or scrotal tongue) is usually a normal finding. A
bifid uvula may be isolated or associated with a submucous cleft of the
soft palate (Fig. 351.1).
Regurgitation, the result of gastroesophageal reflux, occurs com-
monly in the first year of life. Effortless regurgitation can dribble out
of an infant’s mouth but also may be forceful. In an otherwise healthy
infant with regurgitation; volumes of emesis are commonly approxi-
mately 15-­30 mL but occasionally are larger. Most often, the infant
remains happy, although possibly hungry, after an episode of regurgita-
tion. Episodes can occur from one to several times per day. Regurgita-
tion gradually resolves in 80% of infants by 6 months of age and in
90% by 12 months. If complications develop or regurgitation persists,
gastroesophageal reflux is considered pathologic rather than merely
developmental and deserves further evaluation and treatment. Com- Fig. 351.1 Classic submucous cleft palate with triad of bifid uvula
(large arrow), furrow along the midline of the soft palate (arrowheads),
plications of gastroesophageal reflux include failure to thrive, pulmo- and a notch in the posterior margin of the hard palate (small arrow). The
nary disease (apnea or aspiration pneumonitis), and esophagitis with midline furrow is sometimes referred to as the zona pellucida, reflect-
its sequelae (see Chapters 369 and 370). ing the translucent nature of this area in some patients. (From Hasan A,
Infants and young children may be erratic eaters; this may be a worry Gardner A, Devlin M, Russell C. Submucous cleft palate with bifid uvula.
to parents. A toddler might eat insatiably or refuse to consume food J Pediatr. 2014;165:872.)

2223
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2224 Part XVI u The Digestive System

below the right costal margin. The normal liver is soft in consistency
and percusses to normal size for age. A Riedel lobe is a thin projection Table 352.1  Some Nondigestive Tract Causes of
of the right lobe of the liver that may be palpated low in the right lateral Gastrointestinal Symptoms in Children
abdomen. A soft spleen tip might also be palpable as a normal finding. ANOREXIA
In thin young children, the vertebral column is easily palpable, and an Systemic disease: inflammatory, neoplastic
overlying structure may be mistaken for a mass. Pulsation of the aorta Cardiorespiratory compromise
can be appreciated. Normal stool can often be palpated in the left lower Iatrogenic: drug therapy, unpalatable therapeutic diets
quadrant in the descending or sigmoid colon. Depression
Blood loss from the gastrointestinal tract is never normal, but Anorexia nervosa
swallowed blood may be misinterpreted as gastrointestinal bleeding. VOMITING
Maternal blood may be ingested at the time of birth or later by a nurs- Inborn errors of metabolism
ing infant if there is bleeding near the mother’s nipple. Nasal or oropha- Medications: erythromycin, chemotherapy, nonsteroidal
ryngeal bleeding is occasionally mistaken for gastrointestinal bleeding antiinflammatory drugs, marijuana
(see Chapter 142). Red dyes in foods or drinks can turn the stool red Increased intracranial pressure
but do not produce a positive test result for occult blood. Brain tumor
Jaundice is common in neonates, especially among premature Infection of the urinary tract
Labyrinthitis
infants, and usually results from the inability of an immature liver to Adrenal insufficiency
conjugate bilirubin, leading to an elevated indirect component (see Pregnancy
Chapter 137). Persistent elevation of indirect bilirubin levels in nurs- Psychogenic
ing infants may be a result of breast milk jaundice, which is usually Abdominal migraine
a benign entity in full-­term infants. An elevated direct bilirubin is Poisoning/toxins
not normal and suggests liver disease, although in infants it may be Renal disease
a result of extrahepatic infection (urinary tract infection). The direct DIARRHEA
bilirubin fraction should account for no more than 15–20% of the Infection: otitis media, urinary tract infection
total serum bilirubin. Elevations in direct bilirubin levels can follow Uremia
indirect hyperbilirubinemia as the liver converts excessive indirect to Medications: antibiotics, cisapride
direct bilirubin and the rate-­limiting step in bilirubin excretion shifts Tumors: neuroblastoma
from the glucuronidation of bilirubin to excretion of direct bilirubin Pericarditis
into the bile canaliculus. Indirect hyperbilirubinemia, which occurs Adrenal insufficiency
commonly in normal newborns, tends to tint the sclerae and skin CONSTIPATION
golden yellow, whereas direct hyperbilirubinemia produces a greenish Hypothyroidism
yellow hue. The degree of jaundice does not always directly correlate Spina bifida
with serum bilirubin levels. An elevated total serum bilirubin warrants Developmental delay
closer examination, fractionation of bilirubin (direct and indirect), and Dehydration: diabetes insipidus, renal tubular lesions
ongoing surveillance. Atypical elevations of unconjugated bilirubin are Medications: narcotics
Lead poisoning
associated with risk for kernicterus (see Chapter 140). Elevations in
Infant botulism
conjugated bilirubin are reviewed in the chapter on cholestasis (see
Chapter 404.1). ABDOMINAL PAIN
Pyelonephritis, hydronephrosis, renal colic
Visit Elsevier eBooks+ at eBooks.Health.Elsevier.com for Bibliography. Pneumonia (lower lobe)
Pelvic inflammatory disease
Porphyria
Fabry disease
Angioedema
Endocarditis
Abdominal migraine
Chapter 352 Familial Mediterranean fever
Sexual or physical abuse
Systemic lupus erythematosus
Major Symptoms and School phobia
Sickle cell crisis

Signs of Digestive Tract Vertebral disk inflammation
Psoas abscess
Pelvic osteomyelitis or myositis

Disorders Medications
Anterior (abdominal) cutaneous nerve entrapment syndrome (ACNES)

Asim Maqbool and Chris A. Liacouras ABDOMINAL DISTENTION OR MASS
Ascites: nephrotic syndrome, neoplasm, heart failure
Discrete mass: Wilms tumor, hydronephrosis, neuroblastoma,
mesenteric cyst, hepatoblastoma, lymphoma
Disorders of organs outside the gastrointestinal (GI) tract can produce Pregnancy
symptoms and signs that mimic digestive tract disorders and should be JAUNDICE
considered in the differential diagnosis (Table 352.1). In children with Hemolytic disease
normal growth and development, treatment may be initiated without Urinary tract infection
a formal evaluation based on a presumptive diagnosis after taking a Sepsis
history and performing a physical examination. Poor weight gain or Hypothyroidism
weight loss is often associated with a significant pathologic process and Panhypopituitarism
usually necessitates a more formal evaluation.

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 Chapter 352 u Major Symptoms and Signs of Digestive Tract Disorders 2225

DYSPHAGIA dysfunction, manifest by dysphagia with solids. The most serious com-
Difficulty in swallowing is termed dysphagia. Painful swallowing is plication of oropharyngeal dysphagia is life-­threatening aspiration.
termed odynophagia. Globus is the sensation of something stuck in A complex sequence of neuromuscular events is involved in the
the throat without a clear etiology. Swallowing is a complex process transfer of foods to the upper esophagus. Abnormalities of the muscles
that starts in the mouth with mastication and lubrication of food that involved in the ingestion process and their innervation, strength, or
is formed into a bolus. The bolus is pushed into the pharynx by the coordination are associated with transfer dysphagia in infants and chil-
tongue. The pharyngeal phase of swallowing is rapid and involves pro- dren. In such cases, an oropharyngeal problem is usually part of a more
tective mechanisms to prevent food from entering the airway. The epi- generalized neurologic or muscular problem (botulism, diphtheria,
glottis is lowered over the larynx while the soft palate is elevated against neuromuscular disease). Painful oral lesions, such as acute viral sto-
the nasopharyngeal wall; respiration is temporarily arrested while the matitis or trauma, occasionally interfere with ingestion. If the nasal air
upper esophageal sphincter opens to allow the bolus to enter the esoph- passage is seriously obstructed, the need for respiration causes severe
agus. In the esophagus, peristaltic coordinated muscular contractions distress when suckling. Although severe structural, dental, and salivary
push the food bolus toward the stomach. The lower esophageal sphinc- abnormalities would be expected to create difficulties, ingestion pro-
ter relaxes shortly after the upper esophageal sphincter, so liquids that ceeds relatively well in most affected children if they are hungry.
rapidly clear the esophagus enter the stomach without resistance. Esophageal dysphagia occurs when there is difficulty in transport-
Dysphagia is classified as oropharyngeal dysphagia and esophageal ing the food bolus down the esophagus. Esophageal dysphagia can
dysphagia. Oropharyngeal dysphagia occurs when the transfer of the result from neuromuscular disorders or mechanical obstruction (Table
food bolus from the mouth to the esophagus is impaired (also termed 352.3). Primary motility disorders causing impaired peristaltic func-
transfer dysphagia). The striated muscles of the mouth, pharynx, and tion and dysphagia are rare in children. Eosinophilic esophagitis can
upper esophageal sphincter are affected in oropharyngeal dysphagia. present with esophageal dysphagia. Achalasia is an esophageal motility
Neurologic and muscular disorders can give rise to oropharyngeal disorder with associated inability of relaxation of the lower esophageal
dysphagia (Table 352.2). Chiari malformations, Russell-­ Silver syn- sphincter; it rarely occurs in children. Motility of the distal esophagus
drome, and cri du chat may present with upper esophageal sphincter is disordered after surgical repair of tracheoesophageal fistula or acha-
lasia. Abnormal motility can accompany collagen vascular disorders.
Mechanical obstruction can be intrinsic or extrinsic. Intrinsic struc-
tural defects cause a fixed impediment to the passage of food bolus
Table 352.2  Causes of Oropharyngeal Dysphagia because of a narrowing within the esophagus, as in a stricture, web,
or tumor. Extrinsic obstruction is caused by compression from vas-
NEUROMUSCULAR DISORDERS
cular rings, mediastinal lesions, or vertebral abnormalities. Structural
Cerebral palsy
Brain tumors
defects typically cause more problems in swallowing solids than liq-
Cerebrovascular disease/stroke uids. In infants, esophageal web, tracheobronchial remnant, or vas-
Chiari malformation cular ring can cause dysphagia. An esophageal stricture secondary to
Polio and postpolio syndromes esophagitis (chronic gastroesophageal reflux, eosinophilic esophagitis,
Multiple sclerosis chronic infections) occasionally has dysphagia as the first manifesta-
Myositis tion. An esophageal foreign body or a stricture secondary to a caustic
Dermatomyositis ingestion also causes dysphagia. A Schatzki ring, a thin ring of mucosal
Myasthenia gravis tissue near the lower esophageal sphincter, is another mechanical cause
Muscular dystrophies of recurrent dysphagia, and again is rare in children.
Acquired or inherited dystonia syndrome
Dysautonomia
When dysphagia is associated with a delay in passage through the
esophagus, the patient may be able to point to the level of the chest
METABOLIC AND AUTOIMMUNE DISORDERS where the delay occurs, but esophageal symptoms are usually referred
Hyperthyroidism
Systemic lupus erythematosus
Sarcoidosis
Amyloidosis
Table 352.3  Causes of Esophageal Dysphagia
INFECTIOUS DISEASE
Meningitis NEUROMUSCULAR
Botulism Eosinophilic esophagitis
Diphtheria Achalasia cardia
Lyme disease Diffuse esophageal spasm
Neurosyphilis Scleroderma
Viral infection: polio, coxsackievirus, herpes, cytomegalovirus
GERD
STRUCTURAL LESIONS
INTRINSIC LESIONS
Inflammatory: abscess, pharyngitis
Foreign bodies including pills
Congenital web
Esophagitis: GERD, eosinophilic esophagitis, infections
Cricopharyngeal bar
Stricture: corrosive injury, pill induced, peptic
Dental problems
Esophageal webs
Bullous skin lesions
Esophageal rings
Plummer-­Vinson syndrome
Esophageal diverticula
Zenker diverticulum
Neoplasm
Extrinsic compression: osteophytes, lymph nodes, thyroid swelling,
Chagas disease
aberrant
right subclavian artery (dysphagia lusoria) EXTRINSIC LESIONS
OTHER Vascular compression
Corrosive injury Mediastinal lesion
Side effects of medications Cervical osteochondritis
After surgery Vertebral abnormalities
After radiation therapy GERD, Gastroesophageal reflux disease.
Adapted from Gasiorowska A, Faas R. Current approach to dysphagia. Gastroenterol
Adapted from Gasiorowska A, Faas R. Current approach to dysphagia. Gastroenterol
Hepatol. 2009;5(4):269–279.
Hepatol. 2009;5(4):269–279.

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2226 Part XVI u The Digestive System

to the suprasternal notch. When a patient points to the suprasternal (CTZ) are most often implicated by chemical stimuli with chemother-
notch, the impaction can be found anywhere in the esophagus. apy a prime example. Visceral stimuli can include ingestions, gastric
hyperacidity, physical stress, psychologic stressors, mechanical disten-
REGURGITATION tion of the stomach, and impaired GI motility; vagal and sympathetic
Regurgitation is the effortless movement of stomach contents into the nerves are involved in this process. Vestibular pathways are most often
esophagus and mouth. It is not associated with distress, and infants implicated in nausea related to motion sickness. Increased intracranial
with regurgitation are often hungry immediately after an episode. The pressure can also present with nausea plus or minus vomiting.
lower esophageal sphincter prevents reflux of gastric contents into the Chronic nausea is more common in adolescents and may be coinci-
esophagus. Regurgitation is a result of gastroesophageal reflux through dental with other functional GI disorders, including functional dyspep-
an incompetent or, in infants, immature lower esophageal sphincter. sia, delayed gastric emptying/gastroparesis, and constipation. There are
This is often a developmental process, and regurgitation or “spitting” gender and ethnic differences with respect to chronic nausea in adoles-
resolves with maturity. Regurgitation should be differentiated from cence, with adolescent White females with anxiety more at risk than
vomiting, which denotes an active reflex process with an extensive dif- other groups; there may be alterations in the brain gut axis coupled
ferential diagnosis (Table 352.4). with increased visceral hypersensitivity and hyperalgesia at play in the
setting (see Chapter 212). Dehydration and autonomic dysfunction
NAUSEA may also present with nausea as one facet of GI manifestations.
Nausea has been described as an unpleasant, subjective sensation of Nausea is often a clinical diagnosis, and while the differential diag-
impending/imminent vomiting, often with epigastric sensation that nosis is extensive, negative findings do not equate to the patient not
may be painless. Nausea is frequently associated with typical auto- having nausea. Nausea is often distressing, disruptive, and may be
nomic signs that accompany vomiting. Not all nausea is a prodrome disabling with respect to normal function. Table 352.5 reviews com-
to vomiting. There are multiple potential triggers to nausea, includ- mon medical conditions associated with nausea, as well as treatment
ing environmental exposures (toxins, odors), unpleasant visual stim- strategies. Hydration is important in many of these conditions. Many
uli, visceral pain, anxiety, stress, and a variety of additional etiologies of the medications used employ antihistamine, serotonergic, dopa-
(Table 352.5). minergic, and potentially even opioid pathways (although these are
The central nervous system (CNS) is frequently implicated for nau- still controversial). These agents are active at both the CNS and GI
sea. Receptors and neural pathways at the chemoreceptor trigger zone level, with significant brain-­gut axis interplay. Complementary and

Table 352.4  Differential Diagnosis of Emesis During Childhood
INFANT CHILD ADOLESCENT
COMMON
Gastroenteritis Gastroenteritis Gastroenteritis
Gastroesophageal reflux Systemic infection GERD
Overfeeding Gastritis Systemic infection
Anatomic obstruction* Toxic ingestion/poisoning Toxic ingestion/poisoning/marijuana
Systemic infection† Pertussis syndrome Gastritis
Pertussis syndrome Medication Sinusitis
Otitis media Reflux (GERD) Inflammatory bowel disease
Sinusitis Appendicitis
Otitis media Migraine
Anatomic obstruction* Pregnancy
Eosinophilic esophagitis Medications
Ipecac abuse, bulimia
Concussion
RARE
Adrenogenital syndrome Reye syndrome Reye syndrome
Inborn errors of metabolism Hepatitis Hepatitis
Brain tumor (increased intracranial pressure) Peptic ulcer Peptic ulcer
Subdural hemorrhage Pancreatitis Pancreatitis
Food poisoning Brain tumor Cholecystitis
Rumination Increased intracranial pressure Brain tumor
Renal tubular acidosis Middle ear disease/labyrinthitis Increased intracranial pressure
Ureteropelvic junction obstruction Chemotherapy Concussion
Pseudoobstruction Achalasia Middle ear disease/labyrinthitis
Cyclic vomiting (migraine) Chemotherapy
Esophageal stricture Cyclic vomiting (migraine)
Duodenal hematoma Biliary colic
Inborn error of metabolism Renal colic
Pseudoobstruction Porphyria
Gastroparesis Diabetic ketoacidosis
Adrenal insufficiency
Pseudoobstruction
Intestinal tumor
Gastroparesis
Achalasia
Superior mesentery artery syndrome
Distal intestinal obstruction syndrome
*Includes malrotation, pyloric stenosis, intussusception, Hirschsprung disease, adhesions, and hernias.
†Meningitis, sepsis.

GERD, Gastroesophageal reflux disease.

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 Chapter 352 u Major Symptoms and Signs of Digestive Tract Disorders 2227

Table 352.5  Examples of Causes and Management of Nausea
FUNCTIONAL GASTROINTESTINAL
DISORDERS TREATMENT APPROACHES
Gastroesophageal reflux Diet and lifestyle; acid reduction, refluxate management
Esophagitis (reflux related, eosinophilic, etc.) Acid reduction, identifying and restricting environmental/dietary triggers
Dyspepsia Dietary and lifestyle modification; acid reduction; cyproheptadine
Gastroparesis Smaller, more frequent meals; dietary modification; prokinetic agents (D2 antagonists such as
metoclopramide and domperidone*; low-­dose erythromycin or azithromycin)
Constipation Adequate hydration, diet and lifestyle modification, stool softeners, stimulant laxatives, additional
adjunct measures if/as indicated
Visceral hyperalgesia Tricyclic antidepressants (e.g., amitriptyline), cognitive behavioral therapy, hypnotherapy,
biofeedback, physical therapy for desensitization; biofeedback; stress reduction
OTHER GASTROINTESTINAL DISORDERS
Gastritis (medication/NSAID induced; Reduce/remove medications involved; treat the underlying cause
Helicobacter pylori)
Gastrointestinal dysmotility Adequate hydration; diet/feeding or eating modification; promotility agents
Biliary dysfunction (cholelithiasis, Treat the underlying cause
cholecystitis, biliary dyskinesia)
Fundoplication Smaller, more frequent meals; cyproheptadine to improve gastric accommodation
CENTRAL NERVOUS SYSTEM
Increased intracranial pressure Treat underlying cause
Migraines, headaches Migraine prophylactic agents, including cyproheptadine. Abortive medications including triptans.
Motion sickness/vestibular dysfunction Antihistamines (e.g., diphenhydramine, hydroxyzine) anticholinergics (e.g., scopolamine)
Autonomic dysfunction Adequate hydration, increased salt intake, diet and lifestyle modification
Chemotherapy-­induced nausea and vomiting 5-­HT3 receptor antagonists; D2 antagonists; NK-­1 antagonists; butyrophenones; benzodiazepines;
dexamethasone; synthetic cannabinoids
Postoperative nausea and vomiting 5-­HT3 receptor antagonists
NON-­GI AND NON-­CNS ETIOLOGIES OF NAUSEA
Uremia Treat the underlying disorder
Endocrine disorders [e.g., hypothyroidism] Treat the underlying disorder
*D2 receptor antagonists such as metoclopramide and domperidone have a significant side effect profile, and have a U.S. Food and Drug Administration black box warning, and
should be used with caution.
NK-­1, Neurokinin 1.

alternative medicine approaches including using ginger, peppermint, DIARRHEA
aromatherapy, and biofeedback may be helpful. Behavior psychology Diarrhea is best defined as excessive loss of fluid and electrolyte in the
and social work may be helpful in decreasing disability and enhancing stool. Acute diarrhea is defined as sudden onset of excessively loose
functionality. stools of >10 mL/kg/day in infants and >200 g/24 hr in older children,
which lasts 2 years: 1 to 1.5 mg/kg/dose PO Dimenhydrinate is available as
q6-­8h, max: 25 mg/dose 50 mg tablets, prescribe in
12.5 mg increments
Meclizine (Antivert) >2 to 12 years: 25 mg to 50 mg PO patches
1 to 4 times daily, max: Withdrawal (cholinergic
100 mg/day rebound) symptoms reported
with long-­term use, limit
duration or consider weaning
Scopolamine (Transderm-­Scop) >15 kg: 1 transdermal patch with extended use
applied behind the ear every
3 days

MISCELLANEOUS
Visceral Hypersensitivity, Feeding Cyproheptadine* 0.25 mg/kg/day PO in 1-­3 divided C onsider starting with bedtime
Intolerance doses, usual max: 4 mg/dose dose and titrating up to prevent
Antihistamine/serotonin daytime sedation
antagonist Associated with tachyphylaxis
Benefit reported in patients
with visceral hypersensitivity
Anticholinergic effects may
decrease motility

Pseudo-­obstruction Octreotide* 0.5 to 1 mcg/kg subQ once daily, M
 ay cause bradycardia,
Somatostatin analog max: 100 mcg/dose hypoglycemia

Adrenal Crisis Hydrocortisone 100 mg/m2 IV/IM x1, followed by R
 eported regimens vary, refer
25 mg/m2/dose IV/IM q6h, max: to individual protocols
100 mg/day
Taper as clinically indicated
*Limited data available

Table 352.9  Supportive and Nonpharmacologic Therapies for Vomiting Episodes
DISEASE THERAPY
All Treat cause
Obstruction: operate
Allergy: change diet (±steroids)
Metabolic error: Rx defect
Acid peptic disease: H2Ras, PPIs, etc.
COMPLICATIONS
Dehydration IV fluids, electrolytes
Hematemesis Transfuse, correct coagulopathy
Esophagitis H2Ras, PPIs
Malnutrition NG or NJ drip feeding useful for many chronic conditions
Meconium ileus Gastrografin enema
DIOS Gastrografin enema; balanced colonic lavage solution (e.g., GoLYTELY)
Intussusception Barium enema; air reduction enema
Hematemesis Endoscopic: injection sclerotherapy or banding of esophageal varices; injection therapy, fibrin sealant application,
or heater probe electrocautery for selected upper GI tract lesions
Sigmoid volvulus Colonoscopic decompression
Reflux Positioning; dietary measures (infants: rice cereal, 1 tbs/oz of formula)
Psychogenic components Psychotherapy; tricyclic antidepressants; anxiolytics (e.g., diazepam: 0.1 mg/kg PO tid-­qid)
DIOS, Distal intestinal obstruction syndrome; GI, gastrointestinal; H2RA, H2-­receptor antagonist; NG, nasogastric; NJ, nasojejunal; PPIs, proton pump inhibitors; tbs, tablespoon.
From Kliegman RM, Greenbaum LA, Lye PS, eds. Practical Strategies in Pediatric Diagnosis and Therapy. 2nd ed. Philadelphia: Elsevier; 2004: p. 319.

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2232 Part XVI u The Digestive System

Table 352.10  Mechanisms of Diarrhea
PRIMARY MECHANISM DEFECT STOOL EXAMINATION EXAMPLES COMMENT
Secretory Decreased absorption, Watery, normal Cholera, toxigenic Persists during fasting; bile
increased secretion, osmolality with ion gap Escherichia coli; carcinoid, salt malabsorption can
electrolyte transport 100 mOsm/kg laxative abuse carbohydrate
malabsorption; no stool
leukocytes
Increased motility Decreased transit time Loose to normal-­appearing Irritable bowel syndrome, Infection can also contribute
stool, stimulated by thyrotoxicosis, to increased motility
gastrocolic reflex postvagotomy dumping
syndrome
Decreased motility Defect in neuromuscular Loose to Pseudoobstruction, blind Possible bacterial
unit(s) stasis (bacterial normal-­appearing stool loop overgrowth
overgrowth)
Decreased surface area Decreased functional Watery Short bowel syndrome, Might require elemental
(osmotic, motility) capacity celiac disease, rotavirus diet plus parenteral
enteritis alimentation
Mucosal invasion Inflammation, decreased Blood and increased Salmonella, Shigella Dysentery evident in
colonic reabsorption, WBCs in stool infection; amebiasis; blood, mucus, and WBCs
increased motility Yersinia, Campylobacter
infection
VIP, Vasoactive intestinal peptide; WBC, white blood cell.
From Kliegman RM, Greenbaum LA, Lye PS. eds. Practical Strategies in Pediatric Diagnosis and Therapy. 2nd ed. Philadelphia: Elsevier; 2004: p 274.

mechanism. Diarrhea not associated with an exogenous secreta- difficulty every third day should be treated as constipation. Consti-
gogue can also have a secretory component (congenital microvillus pation can arise from defects either in filling or emptying the rectum
inclusion disease). Secretory diarrhea is usually of large volume and (Table 352.12).
persists even with fasting. The stool osmolality is predominantly A nursing infant might have very infrequent stools of normal con-
indicated by the electrolytes, and the ion gap is 100 mOsm/kg or sistency, which is usually a normal pattern. True constipation in the
less. The ion gap is calculated by subtracting the concentration of neonatal period is most likely secondary to Hirschsprung disease,
electrolytes from total osmolality: intestinal pseudoobstruction, or hypothyroidism.
Ion gap Stool osmolality  [(Stool Na  stool K) 2] Defective rectal filling occurs when colonic peristalsis is inef-
fective (in cases of hypothyroidism or opiate use and when
Osmotic diarrhea occurs after ingestion of a poorly absorbed bowel obstruction is caused either by a structural anomaly or by
solute. The solute may be one that is normally not well absorbed Hirschsprung disease). The resultant colonic stasis leads to exces-
(magnesium, phosphate, lactulose, or sorbitol) or one that is not sive drying of stool and a failure to initiate reflexes from the rectum
well absorbed because of a disorder of the small bowel (lactose with that normally trigger evacuation. Emptying the rectum by sponta-
lactase deficiency or glucose with rotavirus diarrhea). Malabsorbed neous evacuation depends on a defecation reflex initiated by pres-
carbohydrate is fermented in the colon, and short-­chain fatty acids sure receptors in the rectal muscle. Therefore stool retention can
are produced. Although short-­chain fatty acids can be absorbed in also result from lesions involving these rectal muscles, the sacral
the colon and used as an energy source, the net effect is increase in spinal cord afferent and efferent fibers, or the muscles of the abdo-
the osmotic solute load. This form of diarrhea is usually of lesser men and pelvic floor. Disorders of anal sphincter relaxation can also
volume than a secretory diarrhea and stops with fasting. The osmo- contribute to fecal retention.
lality of the stool will not be explained by the electrolyte content, Constipation tends to be self-­p erpetuating, whatever its cause.
because another osmotic component is present and so the anion Hard, large stools in the rectum become difficult and even pain-
gap is >100 mOsm. ful to evacuate; thus more retention occurs and a vicious circle
Motility disorders can be associated with rapid or delayed transit and ensues. Distention of the rectum and colon lessens the sensitivity
are not generally associated with large-­volume diarrhea. Slow motility of the defecation reflex and the effectiveness of peristalsis. Fecal
can be associated with bacterial overgrowth leading to diarrhea. The impaction is common and leads to other problems. Eventually,
differential diagnosis of common causes of acute and chronic diarrhea watery content from the proximal colon might percolate around
is noted in Table 352.11. hard retained stool and pass per rectum unperceived by the child.
This involuntary encopresis may be mistaken for diarrhea. Con-
CONSTIPATION stipation itself does not have deleterious systemic organic effects,
Any definition of constipation is relative and depends on stool but urinary tract stasis with increased risk of urinary tract infec-
consistency, stool frequency, and difficulty in passing the stool. A tions can accompany severe long-­standing cases and constipation
normal child might have a soft stool only every second or third day can generate anxiety, having a marked emotional impact on the
without difficulty; this is not constipation. A hard stool passed with patient and family.

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 Table 352.11 Differential Diagnosis of Diarrhea
INFANT CHILD ADOLESCENT
ACUTE
Common
Gastroenteritis (viral > bacterial > protozoal) Gastroenteritis (viral > bacterial > protozoal) Gastroenteritis (viral > bacterial > protozoal)
Systemic infection Food poisoning Food poisoning
Antibiotic associated Systemic infection Antibiotic associated
Overfeeding Antibiotic associated
Rare
Primary disaccharidase deficiency Toxic ingestion Hyperthyroidism
Hirschsprung toxic colitis Hemolytic uremic syndrome Appendicitis
Adrenogenital syndrome Intussusception
Neonatal opiate withdrawal
CHRONIC
Common
Postinfectious secondary lactase deficiency Postinfectious secondary lactase deficiency Irritable bowel syndrome
Cow’s milk or soy protein intolerance (allergy) Irritable bowel syndrome Inflammatory bowel disease
Chronic nonspecific diarrhea of infancy Celiac disease Lactose intolerance
Excessive fruit juice (sorbitol) ingestion Cystic fibrosis Giardiasis
Celiac disease Lactose intolerance Laxative abuse (anorexia nervosa)
Cystic fibrosis Excessive fruit juice (sorbitol) ingestion Constipation with encopresis
AIDS enteropathy Giardiasis
Inflammatory bowel disease
AIDS enteropathy
Rare
Primary immune defects Primary and acquired immune defects Secretory tumor
Autoimmune enteropathy Secretory tumors Primary bowel tumor
IPEX and IPEX-­like syndromes Pseudoobstruction Parasitic infections and venereal diseases
Glucose-­galactose malabsorption Sucrase-­isomaltase deficiency Appendiceal abscess
Microvillus inclusion disease (microvillus atrophy) Eosinophilic gastroenteritis Addison disease
Congenital transport defects (chloride, sodium) Secretory tumors
Primary bile acid malabsorption
Factitious syndrome by proxy
Hirschsprung disease
Shwachman syndrome
Secretory tumors
Acrodermatitis enteropathica
Lymphangiectasia
Abetalipoproteinemia
Eosinophilic gastroenteritis
Short bowel syndrome
IPEX, Immunodysregulation polyendocrinopathy enteropathy X-­linked.
From Kliegman RM, Greenbaum LA, Lye PS, eds. Practical Strategies in Pediatric Diagnosis and Therapy, 2nd ed. Philadelphia: Elsevier; 2004: p. 272.

Table 352.12 Causes of Constipation
NONORGANIC (FUNCTIONAL): RETENTIVE Drugs
Anatomic Anticholinergics
Anal stenosis, atresia with fistula Narcotics
Imperforate anus Methylphenidate
Anteriorly displaced anus Phenytoin
Intestinal stricture (postnecrotizing enterocolitis) Antidepressants
Anal stricture Chemotherapeutic agents (vincristine)
Pancreatic enzymes (fibrosing colonopathy)
Abnormal Musculature Lead, arsenic, mercury
Prune-­belly syndrome Vitamin D intoxication
Gastroschisis Calcium channel blocking agents
Down syndrome
Muscular dystrophy Metabolic Disorders
Hypokalemia
Intestinal Nerve or Muscle Abnormalities Hypercalcemia
Hirschsprung disease Hypothyroidism
Pseudoobstruction (visceral myopathy or neuropathy) Diabetes mellitus, diabetes insipidus
Intestinal neuronal dysplasia Porphyria
Spinal cord lesions
Tethered cord Intestinal Disorders
Autonomic neuropathy Celiac disease
Spinal cord trauma Cow’s milk protein intolerance
Spina bifida Cystic fibrosis (meconium ileus equivalent)
Chagas disease Inflammatory bowel disease (stricture)
Tumor
Connective tissue disorders
Systemic lupus erythematosus
Scleroderma
Psychiatric Diagnosis
Anorexia nervosa

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2234 Part XVI u The Digestive System

ANOREXIA ganglia, and some axons cross the midline and ascend to the medulla,
Anorexia means prolonged lack of appetite. Hunger and satiety centers midbrain, and thalamus. Pain is perceived in the cortex of the post-
are located in the hypothalamus; it seems likely that afferent nerves central gyrus, which can receive impulses arising from both sides of
from the GI tract to these brain centers are important determinants the body. In the gut, the usual stimulus provoking pain is tension or
of the anorexia that characterizes many diseases of the stomach and stretching. Inflammatory lesions can lower the pain threshold, but
intestine. Satiety is stimulated by distention of the stomach or upper the mechanisms producing pain or inflammation are not clear. Tissue
small bowel, the signal being transmitted by sensory afferents, which metabolites released near nerve endings probably account for the pain
are especially dense in the upper gut. Chemoreceptors in the intestine, caused by ischemia. Perception of these painful stimuli can be modu-
influenced by the assimilation of nutrients, also affect afferent flow to lated by input from both cerebral and peripheral sources. Psychologic
the appetite centers. Impulses reach the hypothalamus from higher factors are particularly important. Tables 352.14 and 352.15 list features
centers, possibly influenced by pain or the emotional disturbance of abdominal pain. Pain that suggests a potentially serious organic eti-
of an intestinal disease. Other regulatory factors include hormones, ology is associated with age younger than 5 years; fever; weight loss;
ghrelin, leptin, and plasma glucose, which, in turn, reflect intestinal bile-­or blood-­stained emesis; jaundice; hepatosplenomegaly; back or
function. flank pain or pain in a location other than the umbilicus; awakening
from sleep in pain; referred pain to shoulder, groin, or back; elevated
ABDOMINAL PAIN erythrocyte sedimentation rate, white blood cell count, or CRP; ane-
There is considerable variation among children in their perception mia; edema; hematochezia; or a strong family history of inflammatory
and tolerance for abdominal pain. This is one reason the evaluation of bowel disease or celiac disease (see Table 352.13).
chronic abdominal pain is difficult. A child with functional abdomi- Visceral pain tends to be dull and aching and is experienced in
nal pain (also known as centrally mediated abdominal pain syndrome the dermatome from which the affected organ receives innervations.
or brain-­gut axis dysfunction) may be as uncomfortable as one with So, most often, the pain and tenderness are not felt over the site of
an organic cause. It is very important to distinguish between organic the disease process. Painful stimuli originating in the liver, pancreas,
and nonorganic (functional) abdominal pain because the approach for biliary tree, stomach, or upper bowel are felt in the epigastrium;
the management is based on this (Table 352.13). Normal growth and pain from the distal small bowel, cecum, appendix, or proximal
physical examination (including a rectal examination) and the absence colon is felt at the umbilicus; and pain from the distal large bowel,
of anemia or hematochezia are reassuring in a child who is suspected urinary tract, or pelvic organs is usually suprapubic. The pain from
of having functional pain. the cecum, ascending colon, and descending colon sometimes is felt
A specific cause may be difficult to find, but the nature and location at the site of the lesion because of the short mesocecum and cor-
of a pain-­provoking lesion can usually be determined from the clinical responding mesocolon. The pain caused by appendicitis is initially
description. Two types of nerve fibers transmit painful stimuli in the felt in the periumbilical region, and pain from the transverse colon
abdomen. In skin and muscle, A fibers mediate sharp localized pain; is usually felt in the suprapubic region. The shifting (localization) of
C fibers from viscera, peritoneum, and muscle transmit poorly local- pain is a pointer toward diagnosis; for example, periumbilical pain
ized, dull pain. These afferent fibers have cell bodies in the dorsal root of a few hours localizing to the right lower quadrant suggests appen-
dicitis. Radiation of pain can be helpful in diagnosis; in biliary colic
the radiation of pain is toward the inferior angle of the right scapula,
Table 352.13  Red Flags and Clues to an Organic Cause pancreatic pain is radiated to the back, and the renal colic pain is
of Abdominal Pain radiated to the inguinal region on the same side.
Differentiating abdominal wall pain from visceral pain is impor-
Age 39.4°C suggests pneumonia, pyelonephritis, rib syndrome can follow overuse or even minor trauma to the ribs
dysentery, cholangitis, more than perforation or abscess) on either side. The name originates from a popping/slipping sensa-
Jaundice tion that is often reported. Slipped rib syndrome may be mistaken
Distention* for hepatobiliary, splenic, pancreatic, esophageal, or gastric etiolo-
Dysphagia
Dysuria
gies, among others. Rib fractures, costochondritis, perichondritis
Emesis (especially bilious) [Tietze syndrome], and pleuritic pain may also present as an etiol-
Anorexia ogy. Anterior (abdominal) cutaneous nerve entrapment syndrome
Weight loss, failure to thrive (ACNES) may produce acute, recurrent, or chronic unilateral local-
Positive family history (metabolic disorders, peptic ulcer disease)† ized abdominal pain. Nerve entrapment is most common at the lat-
Change in urine or stool color (blood, acholic) or frequency eral border of the rectus muscle.
Vaginal discharge Somatic pain is intense and usually well localized. When the
Menstrual abnormalities (amenorrhea) inflamed viscus comes in contact with a somatic organ such as the pari-
Sexual activity etal peritoneum or the abdominal wall, pain is localized to that site.
Delayed sexual development (chronic pain)
Anemia
Peritonitis gives rise to generalized abdominal pain with rigidity, invol-
Elevated erythrocyte sedimentation rate untary guarding, rebound tenderness, and cutaneous hyperesthesia on
Elevated stool calprotectin physical examination.
Specific physical findings (hepatomegaly, splenomegaly, absent Referred pain from extraintestinal locations, from shared central
bowel sounds, adnexal tenderness, palpable mass, involuntary projections with the sensory pathway from the abdominal wall, can
guarding, focal or diffuse tenderness, positive rectal examination give rise to abdominal pain, as in pneumonia when the parietal pleural
results, perianal disease, joint swelling, rashes) pain is referred to the abdomen (Fig. 352.1).
*Consider 5 Fs: fat, feces, flatus (aerophagia, obstruction), fluid (ascites, hydronephrosis,
cysts), and fetus (pregnancy or fetal-­like abnormal growth [e.g., tumors]). GASTROINTESTINAL HEMORRHAGE
†Family history is also positive for chronic pain syndromes (constipation, irritable bowel,
Bleeding can occur anywhere along the GI tract, and identification of
dysmenorrhea, and lactase or sucrase deficiency).
the site may be challenging (Table 352.16). Bleeding that originates
Modified from Miranda A. Abdominal pain. In: Kliegman RM, Toth H, Bordini BJ, Basel
D, eds. Nelson Pediatric Symptom-­Based Diagnosis. 2nd ed. Philadelphia: Elsevier; in the esophagus, stomach, or duodenum can cause hematemesis.
2023: Table 13.8, p. 229. When exposed to gastric or intestinal juices, blood quickly darkens to

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 Chapter 352 u Major Symptoms and Signs of Digestive Tract Disorders 2235

Table 352.14 Chronic Abdominal Pain in Children
DISORDER CHARACTERISTICS KEY EVALUATIONS
NONORGANIC
Functional abdominal pain Nonspecific pain, often periumbilical Hx and PE; tests as indicated
Irritable bowel syndrome Intermittent cramps, diarrhea, and constipation Hx and PE
Nonulcer dyspepsia Peptic ulcer–like symptoms without abnormalities on Hx; esophagogastroduodenoscopy
evaluation of the upper GI tract
GASTROINTESTINAL TRACT
Chronic constipation Hx of stool retention, evidence of constipation on Hx and PE; plain x-­ray of abdomen
examination
Lactose intolerance Symptoms may be associated with lactose ingestion; Trial of lactose-­free diet; lactose breath
bloating, gas, cramps, and diarrhea hydrogen test
Parasite infection (especially Giardia) Bloating, gas, cramps, and diarrhea Stool evaluation for O&P; specific
immunoassays for Giardia
Excess fructose or sorbitol ingestion Nonspecific abdominal pain, bloating, gas, and Large intake of apples, fruit juice, or candy
diarrhea or chewing gum sweetened with sorbitol
Crohn disease See Chapter 382.2
Peptic ulcer Burning or gnawing epigastric pain; worse on Esophagogastroduodenoscopy, upper GI
awakening or before meals; relieved with antacids contrast x-­rays, or MRI enteroscopy
Esophagitis Epigastric pain with substernal burning Esophagogastroduodenoscopy
Meckel diverticulum Periumbilical or lower abdominal pain; may have Meckel scan or enteroclysis
blood in stool (usually painless)
Recurrent intussusception Paroxysmal severe cramping abdominal pain; blood Identify intussusception during episode or
may be present in stool with episode lead point in intestine between episodes
with contrast studies of GI tract
Internal, inguinal, or abdominal wall hernia Dull abdomen or abdominal wall pain PE, CT of abdominal wall
Chronic appendicitis or appendiceal Recurrent RLQ pain; often incorrectly diagnosed, Barium enema, CT
mucocele may be rare cause of abdominal pain
GALLBLADDER AND PANCREAS
Cholelithiasis RUQ pain, might worsen with meals Ultrasound of gallbladder
Choledochal cyst RUQ pain, mass ± elevated bilirubin Ultrasound or CT of RUQ
Recurrent pancreatitis Persistent boring pain, might radiate to back, Serum amylase and lipase ± serum
vomiting trypsinogen; ultrasound, CT, or MRI-­ERCP
of pancreas
GENITOURINARY TRACT
Urinary tract infection Dull suprapubic pain, flank pain Urinalysis and urine culture; renal scan
Hydronephrosis Unilateral abdominal or flank pain Ultrasound of kidneys
Urolithiasis Progressive, severe pain; flank to inguinal region to Urinalysis, ultrasound, IVP, CT
testicle
Other genitourinary disorders Suprapubic or lower abdominal pain; genitourinary Ultrasound of kidneys and pelvis;
symptoms gynecologic evaluation
MISCELLANEOUS CAUSES
Abdominal migraine See text; nausea, family Hx migraine Hx
Abdominal epilepsy Might have seizure prodrome EEG (can require >1 study, including
sleep-­deprived EEG)
Gilbert syndrome Mild abdominal pain (causal or coincidental?); Serum bilirubin
slightly elevated unconjugated bilirubin
Familial Mediterranean fever Paroxysmal episodes of fever, severe abdominal Hx and PE during an episode, DNA
pain, and tenderness with other evidence of diagnosis
polyserositis
Sickle cell crisis Anemia Hematologic evaluation
Lead poisoning Vague abdominal pain ± constipation Serum lead level
IgA vasculitis (Henoch-Schönlein purpura) Recurrent, severe crampy abdominal pain, occult Hx, PE, urinalysis
blood in stool, characteristic rash, arthritis
Angioneurotic edema Swelling of face or airway, crampy pain Hx, PE, upper GI contrast x-­rays, serum C1
esterase inhibitor
Acute intermittent porphyria Severe pain precipitated by drugs, fasting, or Spot urine for porphyrins
infections
Anterior cutaneous nerve entrapment Exquisite localized (∼2 × 2 cm) tenderness that is Pain relief within 15 min of abdominal wall
syndrome (ACNES) replicable, most often RLQ injection of local anesthetic; may need
surgery
ERCP, Endoscopic retrograde cholangiopancreatography; EEG, electroencephalogram; GI, gastrointestinal; Hx, history; IVP, intravenous pyelography; O&P, ova and parasites; PE,
physical exam; RLQ, right lower quadrant; RUQ, right upper quadrant.

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2236 Part XVI u The Digestive System

Table 352.15  Distinguishing Features of Acute Abdominal Pain in Children
DISEASE ONSET LOCATION REFERRAL QUALITY COMMENTS
Pancreatitis Acute Epigastric, left upper quadrant Back Constant, sharp, boring Nausea, emesis,
tenderness
Intestinal obstruction Acute or Periumbilical-­lower abdomen Back Alternating cramping Distention, obstipation,
gradual (colic) and painless emesis, increased
periods bowel sounds
Appendicitis Acute (1-­3 days) Periumbilical, then localized Back or pelvis if Sharp, steady Anorexia, nausea, emesis,
to lower right quadrant; retrocecal local tenderness, fever
generalized with peritonitis with peritonitis
Intussusception Acute Periumbilical-­lower abdomen None Cramping, with Hematochezia, knees in
painless periods pulled-­up position
Urolithiasis Acute, sudden Back (unilateral) Groin Sharp, intermittent, Hematuria
cramping
Urinary tract infection Acute Back Bladder Dull to sharp Fever, costovertebral
angle tenderness,
dysuria, urinary frequency
Pelvic inflammatory Acute Pelvis, lower quadrant Upper thigh Aching, peritoneal Vaginal discharge, fever
disease signs
Small bowel Acute to Periumbilical None Cramping diffuse Emesis and obstipation
obstruction subacute
Ruptured ectopic Acute sudden Pelvis, lower quadrant None Sharp, intense, Vaginal bleeding, shock
pregnancy localized

Pancreatitis
Perforated
Heart
Liver duodenal ulcer
GERD
Peptic Penetrating
Biliary colic duodenal ulcer
ulcer
Cholecystitis,
pancreatitis,
Cholecystitis
duodenal ulcer

Small intestine Pancreatitis,
pain, appendicitis renal colic

Appendicitis
Renal
colic Rectal
Colon pain
lesions
Ureteral
colic

Fig. 352.1 Common sites of referred pain from the abdominal viscera. When a patient gives a history of referred pain from the viscera, the pain’s
location may not be directly over the impaired organ. Visceral embryologic development is the mechanism of the referred pain pattern. Pain is
referred to the site where the organ was located in fetal development.

resemble coffee grounds; massive bleeding is likely to be red. Red or lesions secondary to mucosal tears associated with emesis are causes
maroon blood in stools, hematochezia, signifies either a distal bleed- of upper intestinal bleeds. Vascular malformations are a rare cause in
ing site or massive hemorrhage above the distal ileum. Moderate to children; they are difficult to identify (Figs. 352.2 and 352.3). Upper
mild bleeding from sites above the distal ileum tends to cause black- intestinal bleeding is evaluated with esophagogastroduodenoscopy.
ened stools of tarry consistency (melena); major hemorrhages in the Evaluation of the small intestine is facilitated by capsule endoscopy.
duodenum or above can also cause melena. The capsule-­sized imaging device is swallowed in older children or
Erosive damage to the mucosa of the GI tract is the most common placed endoscopically in younger children. Lower GI bleeding is inves-
cause of bleeding, although variceal bleeding secondary to portal tigated with a colonoscopy. In brisk intestinal bleeding of unknown
hypertension occurs often enough to require consideration. Prolapse location, a tagged red blood cell scan is helpful in locating the site of the
gastropathy producing subepithelial hemorrhage and Mallory-­Weiss bleeding, although CT angiography is usually diagnostic. Occult blood

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 Chapter 352 u Major Symptoms and Signs of Digestive Tract Disorders 2237

Table 352.16  Differential Diagnosis of Gastrointestinal Bleeding in Childhood
INFANT CHILD ADOLESCENT
COMMON
Bacterial enteritis Bacterial enteritis Bacterial enteritis
Milk protein allergy intolerance Anal fissure Inflammatory bowel disease
Intussusception Colonic polyps Peptic ulcer/gastritis
Swallowed maternal blood Intussusception Prolapse (traumatic) gastropathy secondary
Anal fissure Peptic ulcer/gastritis to emesis
Lymphonodular hyperplasia Swallowed epistaxis Mallory-­Weiss syndrome
Prolapse (traumatic) gastropathy secondary to emesis Colonic polyps
Mallory-­Weiss syndrome Anal fissure

RARE
Volvulus Esophageal varices Hemorrhoids
Necrotizing enterocolitis Esophagitis Esophageal varices
Meckel diverticulum Meckel diverticulum Esophagitis
Stress ulcer, gastritis Lymphonodular hyperplasia Pill ulcer
Coagulation disorder (hemorrhagic IgA vasculitis (Henoch-Schönlein purpura) Telangiectasia-­angiodysplasia
disease of newborn) Foreign body Graft versus host disease
Esophagitis Hemangioma, arteriovenous malformation Duplication cyst
Sexual abuse Angiodysplasia
Hemolytic-­uremic syndrome Angiodysplasia with von Willebrand disease
Inflammatory bowel disease Blue rubber bleb nevus syndrome
Coagulopathy
Duplication cyst
Angiodysplasia
Angiodysplasia with von Willebrand disease
Blue rubber bleb nevus syndrome

Fig. 352.3 Operative features of blue rubber bleb nevus syndrome.
These lesions are similar to cutaneous lesions. (From Hasosah MY,
Abdul-­Wahab AA, Bin-­Yahab SA, et al. Blue rubber bled nevus syn-
drome: extensive small bowel vascular lesions responsible for gastroin-
Fig. 352.2 Intestinal angiodysplasia. A 7-­year-­old boy had tarry stool testinal bleeding. J Pediatr Child Health. 2010;46:63–65. Fig. 3.)
for days. Panendoscopy showed multiple cherry red flat spots in the
gastric mucosa, compatible with the findings of angiodysplasia in CT
angiography. (From Chuang F, Lin JS, Yeung C, et al. Intestinal angiod-
ysplasia: an uncommon cause of gastrointestinal bleeding in children.
ABDOMINAL DISTENTION AND ABDOMINAL
Pediatr Neonatol. 2011;52:214–218, Fig. 2.) MASSES
Enlargement of the abdomen can result from diminished tone of the
wall musculature or from increased content: fluid, gas, or solid. Ascites,
the accumulation of fluid in the peritoneal cavity, distends the abdo-
in stool is usually detected by using commercially available fecal occult men both in the flanks and anteriorly when it is large in volume. This
blood testing cards, which are based on a chemical reaction between fluid shifts with movement of the patient and conducts a percussion
the chemical guaiac and oxidizing action of a substrate (hemoglobin), wave. Ascitic fluid is usually a transudate with a low protein concentra-
giving a blue color. The guaiac test is very sensitive, but random testing tion resulting from reduced plasma colloid osmotic pressure of hypo-
can miss chronic blood loss, which can lead to iron-­deficiency anemia. albuminemia and/or from raised portal venous pressure. In cases of
GI hemorrhage can produce hypotension and tachycardia but rarely portal hypertension, the fluid leak probably occurs from lymphatics
causes GI symptoms; brisk duodenal or gastric bleeding can lead to on the liver surface and from visceral peritoneal capillaries, but ascites
nausea, vomiting, or diarrhea. The breakdown products of intralu- does not usually develop until the serum albumin level falls. Sodium
minal blood might tip patients into hepatic coma if liver function is excretion in the urine decreases greatly as the ascitic fluid accumu-
already compromised and can lead to elevation of serum bilirubin. lates, and thus additional dietary sodium goes directly to the peritoneal

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2238 Part XVI u The Digestive System

Benign hepatic tumors
Liver abscess
Hepatoblastoma
Hepatocellular carcinoma
Metastatic cancer Bezoar

Choledochal cyst

Splenomegaly
Splenic cyst
Intestinal obstruction

Appendiceal
abscess
Lymphoma
Intestinal
duplication

Ovarian cyst/neoplasm,
Mesenteric cyst abscess

Tuboovarian
abscess

Hydrometrocolpos

Fig. 352.4 Location of select intrabdominal tumors and masses. (From Densmore JC, Densmore EM. Abdominal masses. In Kliegman RM, Toth H,
Bordini BJ, Basel D, eds. Nelson Pediatric Symptom-­Based Diagnosis, 2nd ed. Philadelphia: Elsevier