Cronkhite-Canada syndrome (CCS) is a rare, non-inherited polyposis syndrome, characterized by diffuse gastrointestinal (GI) hamartomatous polyposis with unique dermatologic changes including alopecia, skin hyperpigmentation, and nail dystrophy. Patients can typically present with diarrhea, weight loss, protein-losing enteropathy, and nutritional deficiency. However, it can demonstrate diverse other clinical features, usually with poor prognosis. Currently, there are no specific diagnostic criteria established yet. The etiology of CCS is still obscure, but an autoimmune process has been suggested. Here we present an 81-year-old Caucasian female who had clinical presentations, physical exam, imaging, endoscopy and pathology findings that were all consistent with the diagnosis of CCS. We also include a detailed literature review of the other gastrointestinal polyposis syndromes (hamartomatous, adenomatous, hyperplastic and inflammatory polyposis). A high index of suspicion and recognition of the characteristic clinical, endoscopic as well as histopathological findings of CCS, as well as different gastrointestinal polyposis conditions, can help clinicians with more timely and correct diagnosis.
The Cronkhite-Canada syndrome (CCS) was a rare, non-hereditary disorder that was originally described in 1955 by Leonard W. Cronkhite, and Wilma J. Canada [
An 81-year-old Caucasian female with past medical history of hypothyroidism (currently on synthroid) and colon adenocarcinoma status post right hemicolectomy (2006), presented to the GI office with new onset diarrhea and weight loss of 16 lbs over one month. The diarrhea was profuse, 7 - 8 watery stools every day, sometimes associated with fecal incontinence, but without blood, mucus, or abdominal pain. She also had loss of appetite and pruritic rash on the inner thighs. She initially went to ER for the diarrhea, but was found to have pneumonia and treated with levaquin. Her diarrhea continued. Her family history was significant for colon adenocarcinoma, affecting her father, maternal uncle, and two cousins. She lived alone, and denied alcohol, tobacco or illicit drug use. Her physical examination showed rashes on inner thighs, mild bilateral lower extremity edema, and guaiac positive brown stool.
Her blood work showed normal hemoglobin concentration with elevated MCV (107 fL), deceased serum potassium (K), total protein and albumin (K 3.1 mmol/L, serum albumin 2.4 g/dL, total protein 4.7 g/dL). Her other serum electrolytes, liver function tests (liver enzymes [ALT, AST], total bilirubin, and alkaline phosphatase), and 24-hr urine protein were all normal. Her vitamin B12 was low (128 pg/mL), TSH was elevated (8.65 uIU/mL). Her CEA was 5.3 ng/mL (nl < 5). Stool cultures, stool clostridium difficile toxin and celiac panel were all negative.
Computed tomography (CT) of the abdomen and pelvis showed gastric fold thickening, most prominent in the distal gastric body and gastric antrum (
She showed mild improvement after H. Pylori eradication treatment, and was started on B12 supplements. However, her diarrhea recurred again, resulting in a total of 25 lb weight loss, with hair thinning, loss of fingernails, and hyperpigmentation of the skin (
She subsequently had an upper GI with small bowel follow through (SBFT), which revealed diffusely thickened and nodular gastric folds and evidence of innumerable tiny nodules or polyps, particularly in the antrum with mild distal small bowel fold thickening (
once daily, tapered by 5 mg every 2 weeks). She was also given low dose Lasix for her peripheral edema, with potassium supplements.
The Cronkhite-Canada syndrome (CCS) is an uncommon, non-hereditary GI hamartomatous polyposis syndrome. Since its first description in 1955, there have been more than 500 cases reported in the literature. So far no germline mutation has been found, and there does not appear to have familial predisposition. It occurs most often in middle-aged or older adults, with a slight male predominance of male-to-female ratio of 3:2 [
The etiopathogenesis of CCS is still unclear. In the past, mental and physical stresses were reported as precipitating factors [
Patients typically present with diarrhea, weight loss, hematochezia, or abdominal pain. The diarrhea is usually 5 - 7 bowel movements a day, and the volume can be as high as 4 - 6 L/day. Hypogeusia or dysgeusia, progressive anorexia, xerostomia, or neurologic symptoms (such as seizures) has also been reported [
The unique ectodermal abnormalities of CCS include alopecia, onychodystrophy and diffuse skin hyperpigmentation. Alopecia can involve scalp, eyebrows, axillae, pubic areas, and extremities, and eventually complete hair loss in some patients. Onychodystrophic changes include thinning, splitting, spongy change, onycholysis (partial separation of nail from bed), and onychomadesis (loss of fingernails and toenails). The skin hyperpigmentation is usually manifested in the form of brown macules and plaques on the dorsal surface of the hands, palms, face, neck, and soles. This special dermatological triad is an important feature to distinguish CCS from the other hamartomatous polyposis syndromes (see below).
Radiographically or endoscopically, multiple hamartomatous polyps (varies from 5 to innumerable) are diffusely distributed throughout the GI tract, only sparing the esophagus. Histologically, they can be indistinguishable from juvenile polyposis, characterized by cystic gland dilatation, expanded edematous lamina propria, hyperplasia of foveolar epithelium and mild infiltration of inflammatory cells including eosinophils. Most of the polyps in CCS are non-neoplastic, however, it has been reports that serrated adenomas and carcinomas can arise from the CCS polyps, mostly gastric or colonic (sigmoid or rectum more common) [
Our patient presented in the paper had both upper and lower GI polyposis. Her physical examination, endoscopic findings, pathological features, and anatomic distribution of her polyps are all typical for CCS.
The disease course is usually progressive, leading to anemia, electrolyte disturbances, hypoalbuminemia, hypoproteinemia and vitamin deficiencies due to malabsorption and GI losses. The 5-year mortality rate of CCS has been reported to be 55% [
The optimal treatment of CCS has not been established because of the rarity of the disorder and the poor understanding of the etiology. Current literature favors a combination therapy including nutritional support, H2 receptor antagonist or proton pump inhibitors (PPIs), immune suppression (corticosteroids, azathioprine and cyclosporine), antibiotics, cromolyn sodium, or surgery [
The differential diagnosis includes a number of gastrointestinal polyposis syndromes (
Hamartomatous polyps are overgrowth of the normal cellular tissue of the GI tract, but have a markedly distorted architecture. CCS, along with Juvenile polyposis syndrome (JPS), Peutz-Jeghers syndrome (PJS), and Cowden syndrome (CS) all belong to the hamartomatous polyposis family. Only CCS is sporadic and nonfamilial. The remaining hamartomatous polyposis syndromes are autosomal dominant, with their own specific germline mutation, clinical manifestations, as well as intestinal and extra-intestinal malignancy risks (
Juvenile polyposis syndrome is characterized by multiple juvenile polyps in the GI tract (5 is the minimal for diagnosis, but most cases have 50 - 200). It is typically diagnosed before the age of 20. It is autosomal dominant with 3 genes, SMAD4, BMPR1A, and ENG, being implicated. JPS polyps histologically most resemble CCS polyps. The JPS polyps are pedunculated, demonstrating a villiform architecture. Histologically, the polyp demonstrates edematous lamina propria, with gland dilatation and inflammatory cell infiltration [
In addition to hamartomatous polyps being distributed throughout the GI tract, Peutz-Jeghers syndrome (PJS)
Disease | Age of onset | Gene | Mode of inheritance | # Polyps | Polyps distribution | Histology |
---|---|---|---|---|---|---|
Non-neoplastic polyps | ||||||
Inflammatory “cap” polyposis | 40 - 50 | - | Sporadic | 1 to >100 | Predominantly in distal colon, but can be throughout the colon | Hyperplastic crypts, inflammatory infiltrate and fibromuscular obliteration of the lamina propria, with a white cap of fibrinopurulent exudate |
Hyperplastic polyposis | >40 | - | Familial cluster | 5 - 100, mostly 40 - 100 | Abundance throughout the colon, sparing of stomach or small bowel | Hyperplastic polyps, sessile serrated adenomas |
Adenomatous polyposis | ||||||
Classical Familial adenomatous polyposis (FAP) | 10 - 20 | APC | AD | >100 | Colorectum (100%), gastric fundic gland polyps, duodenum, and periampullary polyps | Adenoma ( tubular adenomas identical to sporadic adenomas) |
Attenuated FAP (AFAP) | 20 - 30 | APC | AD | <100 | Colorectum, Gastroduodenum and periampullary polyps | Adenoma (same as FAP) |
MUTYH- associated polyposis (MAP) | 40 - 60 | MUTYH | AR | 20 - 100 | Colorectum Gastric and duodenal polyps | Adenoma (tubular adenomas, with a minority of tubulovillous adenomas and few hyperplastic polyps) |
Hamartomatous polyposis | ||||||
Juvenile polyposis syndrome | <20 | SMAD4, BMPR1A, ENG | AD | 5 to 200 | More common in the colorectum. The chance in the stomach and small intestine are <20% | Mucous-filled, edematous stroma, dilated glands, inflammatory cell infiltration, and absence of smooth-muscle proliferation |
Peutz-Jeghers syndrome | 10 - 30 | STK11 gene | AD | 1 - 20 | Most common in small intestine (100%), less common in colorectum and stomach (20%). Also seen extra-intestinal tract such as respiratory, uterus, or bladder | “Christmas tree” appearance at low power, Hamartomatous polyps supported by broad bands of muscularis mucosa smooth muscle |
Cowden syndrome | 9 - 20 | PTEN | AD | Multiple | Throughout the GI tract | Hamartomatous polyps, histologically, similar to the juvenile polyps, frequently containing ganglion cells |
Bannayan- Ruvalcaba- Riley syndrome | Early in life | PTEN | AD | Multiple | Majority are identified in the distal ileum and colon, though they may be seen throughout the GI tract | Hamartomatous polyps, histologically similar to the JPS-type polyp |
Cronkhite- Canada syndrome | 50 - 60 | -- | Sporadic | 5 to numerous | Predominantly in stomach and colon (90%), followed by small bowel (80%) and rectum (67%), usually spare esophagus | Hamartomatous polps exhibiting glandular hyperplasia, cystic dilation, mucosal edema |
AD: Autosomal Dominant; AR: Autosomal Recessive.
are also associated with distinctive mucocutaneous pigmented lesions (melanosis), most commonly on the lips and buccal mucosa, less frequently on the hands, feet, periorbital and genital area. These tend to fade during puberty [
Disease | Extra-colonic manifestations | Lifetime CRC or GI malignancy risks | Extra-gastrointestinal malignancy |
---|---|---|---|
Non-neoplastic Polyps | |||
Inflammatory “cap” polyposis | None | No | - |
Hyperplastic polyposis | None | Increased risk of CRC (mostly R-sided) | - |
Adenomatous polyposis | |||
Classical Familial adenomatous polyposis (FAP) | ・ Upper GI polyposis: gastric FGP, duodenum and ampullary adenomas /adenocarcinomas ・ Desmoids tumors, osteomas , epidermoid cysts, dental abnormalities, CHRPE | 100% CRC (left-sided predominance) Duodenal and periampullary cancer (4% - 12%) | Thyroid cancer (1% - 2%), hepatoblastoma (1% - 2%), medulloblastoma (<1%) |
Attenuated FAP (AFAP) | ・ Upper GI polyposis: gastric FGP, duodenum and ampullary adenomas /adenocarcinomas ・ Usually lack the extra-intestinal manifestations of classic FAP | 80% - 100% CRC (usually right-sided) Duodenal and periampullary cancer (4% - 12%) | Thyroid cancer (1% - 2%) |
MUTYH- associated polyposis (MAP) | ・ Gastric FGP, duodenal adenomas/adenocarcinomas ・ CHRPE, osteomas,and Muir-Torre phenotype with sebaceous gland tumors | 80% - 100% CRC (2/3 right sided) Duodenal cancer (4%) | Increased risk of ovarian, bladder, skin, and breast cancer |
Hamartomatous polyposis | |||
Juvenile polyposis syndrome (JPS) | ・ Pulmonary arterio-venous malformations ・ Mucocutaneous telangiectasias | CRC (68%), gastric (21%), small bowel, and pancreatic cancer | No increased risk in extra-GI site |
Peutz-Jeghers syndrome | ・ Mucocutaneous melanosis (lips, buccal mucosa) | CRC (39%), gastric (29%), small bowel (13%), pancreatic cancer (36%) | Breast (54%), lung (15%), ovarianor testicular cancer; ovarian sex-cord tumors with annular tubules (SCTAT), cervical adenoma malignum, male Sertoli-cell testicular tumors |
Cowden syndrome | ・ Mucocutaneous lesions (facial trichilemmomas, acral keratosis, papillomatous papules), LDD, macrocephaly, mental retardation ・ Glycogenic acanthosis of the esophagus | Low | Breast (50%), thyroid (10%), endometrial, ovarian or cervical cancer, renal cell carcinoma, bladder transitional carcinoma |
Cronkhite-Canada syndrome | Unique dermatologic triad: alopecia, skin hyperpigmentation, onychodystrophy | CRC (mostly left sided) Gastric cancer | - |
Both Cowden syndrome (CS) and Bannayan-Ruvalcaba-Riley syndrome (BRRS) are autosomal dominant disorders, caused by the germline mutations of the tumor suppressor gene PTEN (on chromosome 10q23). They are refered to as the PTEN hamartomatous tumor syndrome (PHTS). CS is characterized by multiple hamartomatous polyps throughout the GI tract. CS is associated with increased risk of breast, thyroid, and endometrial cancer, but not GI tract [
Adenomatous polyps are the most common type of polyps. Adenomatous polyposis syndrome includes familial adenomatous polyposis (FAP), hereditary nonpolyposis colon cancer (HNPCC, Lynch syndrome), and MUTYH-associated polyposis (MAP). Since polyposis is not common with Lynch syndrome, it is not included in this review.
Familial adenomatous polyposis (FAP) is characterized by the development of hundreds to thousands of adenomatous polyps in the colorectum starting in childhood or adolescence. It is an autosomal dominant disease, caused by a germline mutation in the adenomatous polyposis coli (APC) gene (on chromosome 5q21). Without treatment, all patients will develop colorectal cancer (CRC) by the age of 40. Attenuated FAP (AFAP) is a milder form of FAP, characterized by less number of polyps (<100) or later onset of adenoma and cancer. Although a smaller polyp burden, without treatment their risk of CRC is still high (80% - 100%).
Upper GI polyposis is common in FAP and AFAP. Gastric fundic gland polyps (FGP) are found in over 50% of FAP patients. Although, dysplasia is reported in these lesions, FGP rarely progress to cancer. Adenomatous polyps of the duodenum and periampullary region are reported in up to 90% of FAP cases [
Extra-intestinal manifestations associated with FAP include desmoid tumors, fibromas, epidermal cysts, osteomas (painless bony growth, most commonly on the skull and the mandible), and dental abnormalities (unerupted teeth, supernumerary teeth etc). Gardner first described these extra-intestinal lesions, and this phenotypic variant of FAP was later named as “Gardner syndrome”. While the benign growths are usually of little concern, desmoid tumors can be associated with significant morbidity and mortality, especially intraabdominal desmoids which can cause bowel obstruction, perforation, or intestinal hemorrhage. In some patients, benign pigmented lesions can be seen in the retina, known as congenital hypertrophy of the retinal pigment epithelium (CHRPE). It is not specific for FAP, but when multiple bilateral lesions are present, it should prompt for screening for FAP.
MUTYH-associated polyposis (MAP) is currently the only known autosomal recessive polyposis syndrome, caused by biallelic MUTYH mutation. Patients usually develop 10 - 100 adenomatous polyps and are typically diagnosed at 40 - 60 years of age. These colonic phenotypic features resemble AFAP [
Extra-colonic features include gastric fundic gland polyps, gastric and duodenal adenomas, duodenal carcinoma, carcinoid tumors, osteomas, CHRPE and Muir-Torre phenotype with sebaceous gland tumors. The extra-intestinal cancer risk is substantial in MAP, with increased risk of breast, ovarian, bladder, and skin cancer.
Hyperplastic polyps (HP) are the most common non-neoplastic type of colonic polyps. They are usually diminutive (typically <5 mm) and commonly found in rectosigmoid. Histologically, they have serrated or “sawtooth” gland outlines of elongated crypts. Hyperplastic polyposis syndrome (HPS) refers to a rare, sporadic entity, in which hyperplastic polyps are found in abundance throughout the colon, with the sparing of stomach or small bowel. It is often diagnosed over 40 years of age, and no germline mutation has been identified. In contrast to the sporadic, small, distal hyperplastic polyps, HPS is characterized by its multiplicity, increased size and extensive distribution of polyps in the colon. The World Health Organization defined HPS as: 1) more than 5 hyperplastic polyps proximal to the sigmoid, of which 2 or more are >1cm; 2) any number of hyperplastic polyps proximal to the sigmoid in a patient who has a first degree relative with HPS; or 3) >30 hyperplastic polyps of any size scattered throughout the colon. HP has traditionally been considered to have no malignant potential. However, molecular studies have identified high levels of DNA methylation in some hyperplastic polyps. These can show genetic instability and be associated with Microsatellite Instability-high (MSI-H) cancers [
Inflammatory polyps are usually associated with inflammatory bowel disease (IBD) such as Crohn’s disease or Ulcerative Colitis. However, there is a particular form of “inflammatory polyposis” that is not associated with IBD, and is called inflammatory “cap” polyposis (ICP). It is a rare nonneoplastic sporadic polyposis, usually limited to the large intestines, especially rectosigmoid colon, although they can progress proximally throughout the colon. The pathogenesis is unclear, but thought to be related to colonic dysmotility or recurrent mucosal trauma due to chronic straining. The common presentations are rectal bleeding, mucous diarrhea, or tenesmus. The number of polyps can vary from 1 to over 100 [
I declare there are no conflicts of interest.