Colonic polyps in children:
From benign to serious
Edward J. Hoffenberg, MD
Polyps in the colon may be either harmless or precancerous.
In both cases, symptoms are usually frightening to patients and parents. This
review of four of the most common diagnoses in children with colonic polyps
provides a rational approach to evaluating and managing these growths.
Blood in the stool. Visible rectal mass. Abdominal pain. Anemia. Four common
pediatric conditions, each with a differential diagnosis that includes gastrointestinal
polyps.
If you have ever cared for a child who, it turns out, has colonic polyps,
you have probably supported parents as they struggled with fear stirred up by
repeated episodes of visible blood in the stool—by far the most common presenting
sign of polyps in the bowel. After diagnosis, parents continue to struggle with
guilt about transmitting a disease to their children and with ongoing anxiety
about malignancy.
To help patients and parents, pediatricians need to adopt a rational approach
to evaluating and managing colonic polyps. This article provides an update on
these growths in children and serves as a resource for delivery of care.
When to consider colonic polyps
As noted, passage of blood per rectum is the most common presenting sign of
polyps in the colon. Other common signs are visible (prolapsed) polyp and unexplained
anemia (Table 1). Less frequent manifestations include unexplained abdominal
pain (due to traction of a pedunculated polyp on the intestinal wall) and recurrent
intussusception (a complication of distal small bowel polyps). Colorectal cancer
is rarely a presentation in children, although parents may bring their child
to you because of a family history of polyps or colon cancer.
TABLE 1
When to consider colonic polyps | | Rectal bleeding or
heme-positive stools | | Prolapsed tissue | | Unexplained abdominal pain | | Unexplained anemia | | Recurrent intussusception
(usually due to small bowel polyp) | | Family history of polyps
or colon cancer before 50 years of age |
|
The blood per rectum is typically bright red, coating and mixed in with stool. It is usually visible only with defecation. Bleeding may be daily, intermittent, or quite infrequent. Large volume blood loss is extremely rare. Chronic blood loss may, however, lead to anemia and iron deficiency.
About 10% to 20% of children with polyps have a prolapsed polyp. Parents often report a strawberry-like mass that extrudes with straining but withdraws into the rectum within a few minutes.
Colonic polyps may present at any time, from the neonatal period into adulthood
(Figure 1). Most commonly, patients are about 4 years old when their condition
is diagnosed. Causes of rectal bleeding vary by age, so your evaluation should
be tailored to the individual patient (Table 2). The main disorders to consider,
in addition to polyps, are protein allergy, intussusception, fissure, infection,
Meckel's diverticulum, inflammatory bowel disease, and lymphonodular hyperplasia.
Click here to view full-size graphic
TABLE 2
Age and the changing nature of rectal bleeding | | Age
| | Causes | <1 yr | 1 to ~4 yr | >5 yr |
| | Common | Protein allergy | Fissure | Infection | | | Infection | Infection | Inflammatory bowel disease | | Fissure | Polyp | Polyp | | Ischemic bowel | Lymphonodular hyperplasia | Fissure | | (intussusception, volvulus) | Meckel’s diverticulum | Upper GI source | | Meckel’s diverticulum | | |
|
| Less common | Swallowed blood | Hemolytic uremic syndrome | Hemolytic uremic syndrome | | | Polyp | Inflammatory bowel disease | Henoch-Schönlein purpura | | Arteriovenous malformation | Henoch-Schönlein purpura | Thrombocytopenia | | Coagulopathy | Upper GI source | Other | | Other | Other | |
|
Initial assessment of rectal bleeding
In a healthy child with intermittent rectal bleeding, begin your evaluation
with a physical examination, including a digital rectal exam. Table 3 lists
key areas of the exam.
TABLE 3
Initial evaluation of suspected colonic polyps | | Physical exam | | Anorectal inspection
with digital rectal exam for palpable polyp and to evaluate other
causes of bleeding (fissure, tag, trauma) | | Examination for lumps in
muscle and bone suggestive of soft tissue tumors (familial adenomatous
polyposis/Gardner, Cowden) | | Visual examination
for mucocutaneous pigmentation/freckling (Peutz-Jeghers syndrome) | | Ophthalmologic examination
for congenital hypertrophy of retinal pigment epithelium (familial
adenomatous polyposis/Gardner) | | Laboratory tests | | Fecal occult blood
test* | | Stool culture for bacterial
pathogens and parasites | | CBC, differential, and erythrocyte
sedimentation rate | | Prothrombin time, partial
thromboplastin time | | *Perform
this test even if blood appears to be present. |
|
Always test fecal material for occult blood, even when blood appears
obvious and the stool looks normal. Other laboratory tests to consider include
a complete blood count with differential, prothrombin time, and a stool culture
for bacterial and parasitic pathogens. These tests are usually normal.
If bleeding persists beyond a few weeks, further evaluation is warranted.
Colonoscopy has largely replaced barium enema as the procedure of choice for
evaluating diseases of the colon that cause bleeding.
Most children with polyps have one of four entities (Table 4), each of which
is described in the discussion that follows. Other conditions characterized
by polyps, such as Cowden disease and lipomas, are exceedingly rare and are
not discussed here.
TABLE 4
Frequency of most common diagnoses | | | Prevalence among
all children with a polyp |
Hamartomas | | Juvenile polyps | 75%–90% | | Juvenile polyposis coli | 10% | | Peutz-Jeghers syndrome | <1% |
| | Adenomas | <1%–5% overall | Familial adenomatous polyposis
(including FAP mutations) | | Sporadic adenomas | | Other |
|
Juvenile polyps
Between 75% and 90% of children with polyps have juvenile polyps— the
most common childhood polyp. Also known as "retention," "inflammatory," or "hamartomatous"
polyps, such polyps occur singly or in clusters of two to four, typically in
the rectosigmoid colon (Figure 2). Sometimes, another juvenile polyp (JP) develops
a few years after initial diagnosis.
Click here to view full-size graphic
A JP is usually pedunculated: It has a stalk with a cap, like a mushroom (Figure
3). A polyp without a stalk is called a sessile polyp, and it may develop into
a pedunculated polyp. On histologic evaluation, a JP contains well-differentiated,
mature epithelial cells; dilated, disordered glands; and abundant acute and
chronic inflammation.
Click here to view full-size graphic
A typical JP is not considered a risk factor for colorectal cancer. However, histologic evaluation is essential to exclude other disorders, especially adenomas. As many as 5% of juvenile polyps in children have focal areas showing adenomatous changes.1 These are not adenomas, but they are worrisome because such polyps may be predisposed to malignant transformation. If smooth muscle is prominent, Peutz-Jeghers syndrome should be considered (this condition is discussed later in this article).
Juvenile polyps should be removed during colonoscopy via electrocautery. Children
with one to four juvenile polyps in the rectosigmoid colon probably do not need
follow-up after polypectomy unless rectal bleeding or another clinical manifestation
of a JP recurs. Follow-up colonoscopy in six to 12 months may be indicated if
any of the following applies:
- Family history of colon polyps.
- Five or more polyps identified at one colonoscopy or over several colonoscopies.
- Unusual features, such as a polyp in the right colon (proximal to transverse
colon) or an adenomatous change in a JP.
Juvenile polyposis coli
JPC is a condition in which more than five (some experts say more than 10) juvenile polyps develop. A first-degree relative of an index case is considered to have the syndrome even if he (or she) has only one polyp.
In JPC, polyps are limited to the colon. In the rare case in which polyps are present in the upper and lower GI tracts, the syndrome is called generalized juvenile polyposis. Persons with this generalized form of juvenile polyposis may have protein-losing enteropathy and anemia and are at high risk for malignancy.
The exact frequency of JPC is unknown. According to published reports, however, as many as 10% of children with polyps have JPC.1,2,3 Assuming that number is accurate, JPC may be the second most common polyp condition, although this is not often recognized in textbooks. Some of the difficulty distinguishing JPC from juvenile polyps arises from the fact that polyps may develop in the left colon in patients with either condition. Unless complete colonoscopy is performed in a child with one or two rectal polyps, polyps in the proximal colon may be missed and the condition misdiagnosed.
The genetic basis of JPC has been a source of confusion recently. In a study of 13 families with JPC, an association was made with mutations in chromosome 10q22-23.4 Other studies have been unable to confirm this finding, however. The 10q22-23 region is the site coding for a protein tyrosine phosphatase gene that has been linked to Cowden syndrome, a disorder associated with polyps and multiple hamartomas of skin, mucous membranes, thyroid, and breast.5 Some subjects in that study were subsequently found to have features that suggest Cowden syndrome.
Another association, this time with 18q21, was reported from a large kindred with juvenile polyps.6 This region is associated with regulation of TGF-B, a protein important in mediating growth-inhibiting signals. Whether this mutation is present in other affected families is unknown, and the genetic basis for JPC remains unclear. It is possible that different mutations may lead to the same phenotypic expression, which we call juvenile polyposis coli.
It is important to distinguish patients with juvenile polyps from those with JPC because evidence suggests that JPC increases the risk of colorectal cancer.7 My approach to managing children with JPC is to establish a surveillance program with the following goals:
- Make the correct diagnosis over time on the basis of the location, number,
and histologic features of polyps
- Prevent complications such as malignancy, bleeding, anemia, and abdominal
pain.
These goals are achieved by removing polyps as they form. For that reason, once JPC is diagnosed, I schedule another colonoscopy in six months to remove remaining polyps and monitor the rate of formation of new polyps. That is also the time to assess the rest of the GI tract with upper endoscopy and an upper GI series with small bowel follow-through.
The next colonoscopy is usually performed one year later. If no new polyps are noted, follow-up colonoscopy can be performed every two or three years. If exuberant formation of polyps continues, if adenomatous changes are observed within the polyp, or if the polyp is an adenoma, consider colectomy.
Peutz-Jeghers syndrome
PJS is characterized by the association of mucocutaneous pigmentation and
hamartomatous polyps of the GI tract. PJS may be diagnosed during childhood
or adolescence, although most patients are in their 20s when their condition
is diagnosed. The syndrome has an incidence of about 1 in 80,000. Inheritance
is thought to be autosomal dominant with variable penetrance. There is no known
gender or ethnic predominance. The melanosis is most commonly noted on the lips
(95%) and buccal mucosa (65% to 85%), and may also be evident on the nose, hands,
and feet. Look for brown to black macules, 1 to 5 mm in diameter, which may
be perceived as multiple freckles. Pigmented macules may fade around the time
of puberty.
More than 90% of patients have multiple hamartomatous polyps, most commonly
in the small bowel (65% to 95%), colon (60%), and stomach (50%). The small bowel
polyps lead to the most common presentation: intermittent colicky abdominal
pain, intussusception with intestinal obstruction, and GI bleeding and anemia.
Extraintestinal polyps are sometimes found in the bronchi and genitourinary
tract. The polyps in PJS contain smooth muscle in prominent bands, a feature
that distinguishes them from juvenile polyps. There may, however, be a significant
overlap in the histologic features of the two types of polyps.8
About 50% of persons with PJS develop extracolonic cancers, usually of the
breast, cervix, ovary, testes, or pancreas. Adenomatous changes are seen in
about 5% of PJS polyps, and the risk of colon cancer in patients with PJS is
2% to 13%.9
Guidelines for managing PJS, based on the fairly limited data available, have
recently been published.9 Beginning at the age of 10 years, surveillance
for upper GI tract lesions should be performed every two years by endoscopy
and an upper GI series with small bowel follow-through. Identified polyps may
be removed by endoscopy or enteroscopy, although surgery may be required for
symptomatic distal small bowel polyps. Also starting at age 10 in male patients,
a testicular exam should be performed yearly to detect tumors. If feminizing
features develop, testicular ultrasonography is indicated to search for Sertoli
cell tumor.
Once a patient reaches adulthood, emphasize the need for routine yearly evaluation
for breast cancer (exam, mammography), uterine cancer (pelvic exam, Pap smear,
ultrasonography), and pancreatic cancer (ultrasonography).
Familial adenomatous polyposis syndromes
The FAP syndromes, caused by mutations in the adenomatous polyposis coli (APC) gene on chromosome 5q2l-22, are the most important colonic polyps to diagnose because they almost always undergo malignant transformation. Mean age of onset of malignancy is 39 years, but cancer has been found in the first and second decades of life. In addition to adenocarcinoma of the colon, cancers of the ampulla of Vater, thyroid gland, stomach, pancreas, and brain (medulloblastoma and glioblastoma, called Turcot syndrome) and hepatoblastoma occur. Because the disease can affect areas outside the colon, "adenomatous polyposis coli" is a misnomer; I prefer "FAP syndromes."
FAP mutations occur in about 1 in 10,000 people and are usually inherited
in an autosomal dominant fashion. Approximately one third of patients have no
family history, however, and represent new germline mutations. The mean age
at which the first adenomatous polyp develops is 16 years (Figure 4). Polyps
are usually small (<5 mm diameter) and range from several to innumerable,
sometimes carpeting the entire colonic mucosa.
Click here to view full-size graphic
The term Gardner syndrome is traditionally applied to patients with FAP who also have prominent extraintestinal tumors. The prevalence of these extraintestinal manifestations depends in part on how aggressively they are sought. Many patients with FAP have minor extraintestinal lesions. Therefore, FAP and Gardner are terms that probably represent variations of the same phenotypic spectrum derived from mutations in the APC gene.
The soft-tissue lesions in patients with FAP or Gardner syndrome include sebaceous and epidermoid cysts, lipomas, and subcutaneous fibromas. Osteomas of the skull and jaw, supernumerary teeth, and congenital hypertrophy of the retinal pigment epithelium are also common. Desmoid tumors may develop after surgical colectomy or other surgery and can cause obstruction, perforation, and abscess.
Diagnosis of FAP is based either on the presence of numerous adenomatous polyps in the colon or on genetic testing; the latter identifies about 80% of mutations10 (more than 100 mutations have been identified). The index case usually undergoes evaluation for FAP by having a protein truncation test, which screens for alterations in the protein product of the APC gene. If the test is positive, then analysis for identifiable mutations can be performed. If a specific mutation is identified, family members can undergo testing for that specific mutation. If, however, the index case tests negative on the protein truncation test, all family members should undergo monitoring for FAP (see next paragraph). For persons in whom FAP is suspected but who do not have known affected family members (that is, they are a probable de novo mutation), genetic testing may be confirmatory. Remember, however, that a negative test does not exclude FAP.
In patients with FAP, surveillance for adenomas by annual colonoscopy should begin no later than 10 to 12 years of age, or 10 years before the youngest diagnosis of colorectal cancer in the family.9 Once adenomas develop, the conservative approach is to recommend total colectomy and a permanent ileostomy. Ileorectal anastomosis preserves continence but retains a small area of affected tissue that requires continued surveillance. Ileoanal anastomosis removes the entire colonic mucosa and, in recent years, has gained favor. Less invasive techniques such as laparoscopic colectomy and one-step colectomy that avoids temporary ileostomy are increasingly popular.
Medical management of FAP is also evolving. Two published short-term trials
have shown a decrease in the number and size of adenomatous polyps with sulindac
(Clinoril) 150 mg orally bid11 or celecoxib (Celebrex) 400 mg orally
bid.12 The mechanism is thought to be inhibition of the enzyme cyclooxygenase-2.
A third drug, exisulind (Aptosyn), which is thought to act by inhibiting a novel
enzyme, cGMP phosphodiesterase, is undergoing clinical trials in adults and
children (For more information, see www.cellpathways.com , the Web site of the
manufacturer of exisulind.) Until long-term data on safety and on efficacy of
medical therapy for preventing cancer are available, such therapy should
not replace colectomy and careful surveillance.
Once FAP is diagnosed, lifelong screening for extracolonic disease is required.9 Hepatoblastoma, which occurs in the first decade of life in about 1.6% of children
with FAP, merits annual examination and consideration of a-fetoprotein determination
and ultrasonography. Beginning at the age of 10 years, a thyroid exam should
be performed annually to detect thyroid cancer, which occurs in about 2% of
those with FAP. After 20 years of age, side-viewing endoscopy should be performed
every one to three years to look for gastric, duodenal, and periampullary lesions,
which can become malignant. Last, also starting at about 20 years, consider
periodic evaluation for pancreatic cancer, which develops in about 2% of affected
persons.
Spreading the word
Although polyps in children are often benign, a complete evaluation and timely
diagnosis are essential to alleviating worrisome symptoms and detecting polyps
that may become malignant. Table 5 summarizes the risk of malignancy by disease
entity.
TABLE 5
Risk of malignancy by diagnosis | | Diagnosis | Risk profile |
| | Juvenile polyp | Not thought to increase risk of colorectal
cancer. Histologic evaluation essential to exclude other disorders,
especially adenomas. | | Juvenile polyposis coli | Evidence suggests an increase in the risk
of colorectal cancer. | | Peutz-Jeghers syndrome | Increases the risk of colorectal cancer.
About half of patients develop extracolonic cancer. | | Familial adenomatous polyposis | Polyps almost always undergo malignant transformation. |
|
Pediatricians and parents can take advantage of expanding resources for education,
support, and advocacy. The box on the left lists resources selected for their
broad appeal. One example is the Hereditary Colon Cancer Association (HCCA,
www.hereditarycc.org ), a new support group that has developed an excellent
pamphlet for families and is taking a leading role in advocacy and education.
1. Hoffenberg E, Sauaia A, Maltzman T, et al: Symptomatic
colonic polyps in childhood: Not so benign. J Pediatr Gastroenterol Nutr 1999;28:175
2. Cynamon H, Milov D, Andres J: Diagnosis and
management of colonic polyps in children. J Pediatr 1989;114:593
3. Mestre J: The changing pattern of juvenile polyps.
Am J Gastroenterol 1986;81:312
4. Jacoby R, Schlack S, Cole C, et al: A juvenile
polyposis tumor suppressor locus at 10q22 is deleted from nonepithelial cells
in the lamina propria. Gastroenterology 1997;112:1398
5. Liaw D, Marsh D, Li J, et al: Germline mutations
of the PTEN gene in Cowden disease, an inherited breast and thyroid cancer syndrome.
Nat Genet 1997;16:64
6. Howe J, Ringold J, Summers R, et al: A gene
for familial juvenile polyposis maps to chromosome 18q21.1. Am J Hum Genet 1998;62:1129
7. Giardiello F, Hamilton S, Kern S, et al: Colorectal
neoplasia in juvenile polyposis or juvenile polyps. Arch Dis Child 1991;66:971
8. Fulcheri E, Baracchini P, Pagani A, et al: Significance
of the smooth muscle cell component in Peutz-Jeghers and juvenile polyps. Human
Pathology 1991;22:1136
9. Burt R: Colon cancer screening. Gastroenterology 2000;119:837
10. Powell S, Petersen G, Krush A, et al: Molecular
diagnosis of familial adenomatous polyposis. N Engl J Med 1993;329:1982
11. Giardiello F, Hamilton S, Krush A, et al: Treatment
of colonic rectal adenomas with sulindac in familial adenomatous polyposis.
N Engl J Med 1993;328:1313
12. Steinbach G, Lynch P, Phillips R, et al: The
effect of celecoxib, a cyclooxygenase-2 inhibitor, in familial adenomatous polyposis.
New Engl J Med 2000;342:1946
THE AUTHOR is associate professor of pediatrics at the University of Colorado
School of Medicine, Denver, and director, Center for Pediatric Inflammatory
Bowel Diseases, The Children's Hospital, Denver. He is a recipient of a research
grant from Cell Pathways, Inc., and a member of the scientific advisory board
for the Hereditary Colon Cancer Association.
Resources
Hereditary Colon Cancer Association
www.hereditarycc.org
A new organization dedicated to promoting awareness, education, and prevention
of hereditary colon cancer.
National Organization for Rare Disorders
www.rarediseases.org
PO Box 8923
New Fairfield, CT 06812-8923
800-999-6673
National organization of rare disorders. Diverse information on rare diseases, their support groups, treatment trials, meetings, etc.
Clinical trials, a service of the NIH
www.clinicaltrials.gov/ct/gui/clb
Provides information about clinical research studies; searchable by disease,
location, key word, treatment, and sponsor.
National Center for Biotechnology Information
Online Mendelian Inheritance in Man
www.ncbi.nlm.nih.gov/Omim
Catalog of human genetic disorders with information in text, pictures, links
to MEDLINE, and detailed references.
GeneClinics
www.geneclinics.org/profiles/fap/details.html
A resource for information on diagnosis, management, and genetic counseling for families affected with specific inherited disorders.
Kids with Gardners Syndrome
clubs.yahoo.com/clubs/kidswithgardnerssyndrome
A place for kids with Gardner syndrome, familial adenomatous polyposis, and their friends.
Association of Cancer Online Resources
listserv.acor.org/archives/(pjs.html)
listserv.acor.org/archives/(fap-gs.html)
listserv.acor.org/archives/(desmoid.html)
Finds lists of online support groups and allows you to enter your own search
terms.
Edward Hoffenberg. Colonic polyps in children: From benign to serious. Contemporary Pediatrics 2001;9:118.
