Colorectal Cancer

Hereditary Colorectal Cancer Syndromes

Hereditary Colorectal Cancer Syndromes

Hereditary Colorectal Cancer Syndromes

What are the indicators of possible presence of cancer predisposing mutations for colorectal cancer?

  • Multiple cases of cancer in a family
  • Earlier age of onset
  • 2 or more cancers in a single individual
  • Presence of non-cancerous extracolonic features, that are a feature of some associated syndrome. Like Congenital Hypertrophy of Retinal Pigment Epithelium (CHRPE) and desmoids may be seen in Familial Adenomatous Polyposis (FAP)
  • Presence of uncommon tumors, like Adenoid Cystic Carcinoma (ACC), Sebaceous carcinoma, ampullary and small bowel carcinoma.
  • Multiple polyps in colon or rectum

What are the major genetic abnormalities and syndromes in Hereditary Colorectal Cancer?

  • Somatic mutations in oncogenes
  • Tumor suppressor genes: Familial Adenomatous Polyposis (FAP) and Peutz Jeghers Syndrome (PJS)
  • Mismatch repair genes: Hereditary Non=Polyposis Colon Cancer (HNPCC)
  • MYH gene: defective Base Excision Repair

Gene

Syndrome

TSG

APC

FAP

TP53

Li Fraumeni

STK11

PJS

PTEN

Cowden

BMPR1A

JPS

SMAD4

JPS

DNA Repair Genes

MLH1, MSH2, MSH6, PMS2

LS

EPCAM

LS

MYH

MYH-associated polyposis

POLD1, POLE

Oligopolposis

What is the absolute risk of colorectal cancer in mutation carriers?

Syndrome

Absolute Risk In Mutation Carriers

FAP

90% by age 45y

AFAP

69% by age 80y

LS

40-80% by age 75y

MYH-associated polyposis

35-53%

PJS

39% by age 70y

JPS

17-68% by age 60y

What is Familial Adenomatous Polyposis Syndrome?

It is an autosomal dominant disorder, characterised by multiple (>100) adenomatous polyps in colon and rectum developing after the first decade of life. Other features that may be seen are polyps in upper GI tract, CHRPE, Osteomas, epidermoid cysts, supernumerary teeth, desmoid formation, papillary thyroid cancer, small bowel ca, hepatoblastoma, medulloblastoma, etc.

APC gene is a tumor suppressor gene located on chromosome 5q21. Loss of APC is the earliest event in chromosomal instability of colorectal cancer pathway. By age of 10 years 15%, by 20 years 75%, and by 30 years 90% of FAP gene carriers have colonic adenomas. Without any intervention, most persons with FAP will develop colon or rectal cancer by fourth decade of life.

What are the extra-colonic manifestations of FAP syndrome?

Duodenal adenomas may be seen in 80-100% of FAP patients, most common site being D1 and D2, ie, first and second part of duodenum, especially in the periampullary region. UGI endoscopy including side-viewing duodenoscopy should be performed between 25 and 30 years of age in FAP patients to detect duodenal adenomas, followed by subsequent scopy based on Spigelman stage, that takes into account polyp size, polyp number, histology, and dysplasia.

Most common stomach tumors are fundic gland polyps. These are often diffuse and not amenable to endoscopic removal, and are not considered precancerous. If high-grade dysplasia is seen, polypectomy is done and repeat endoscopic surveillance in 3-6 months. Along with that, daily proton pump inhibitors are usually prescribed.

Next extracolonic tumors are gastric adenomas that may be seen in 2-12% of patients with FAP. They are usually treated with endoscopic polypectomy.

How is the genetic testing and screening done for FAP?

Genetic diagnosis of FAP requires <10cc of blood in which lymphocyte DNA is tested for APC mutation, which detects the mutation in approximately 80%.

In individuals with an APC gene mutation positive, screening should be initiated at 10-15 years of age.

It should be done annually with flexible sigmoidoscopy or colonoscopy

At-risk individuals who are mutation-negative should undergo at least one flexible colonoscopy at 18-25 years of age. MYH testing should be considered if APC is negative and history is compatible with recessive inheritance.

What is the treatment if polyps are detected in an individual?

Upon the manifestation of polyposis, colectomy (surgical removal of colon) is the only effective management. The various options available for surgical resection are-

  • Restorative proctocolectomy with IPAA, after which annual surveillance of the ileal pouch is required as the cumulative risk of developing adenomas in the pouch is 75% at 15 years.
  • Subtotal colectomy with Ileo-rectal anastomosis for <1000 colonic adenomas and <20 rectal polyps,
  • Total proctocolectomy with ileostomy in low rectal cancer in whom sphincter cannot be spared.

What are the chemoprevention strategies for FAP syndrome?

Celecoxib – Specific COX-2 inhibitor
Sulindac – Non-specific COX-2 inhibitor
Omega-3-PUFA (Eicosapentaenoic acid): reduce rectal poly number and size

What is Lynch or Hereditary Non-Polyposis Colon Cancer (HNPCC) Syndrome?

It is characterized by Microsatellite instability or defect in DNA Mismatch repair genes, MSH2, MLH1, MSH6, and PMS2. It accounts for 1-3% of all colorectal cancers, and is an Autosomal Dominant disorder with an early age of onset. Right sided colon tumors are more commonly seen. There may be presence of synchromous and metachronous colorectal neoplasms.

What are the extra-colonic tumors seen in HNPCC?

Most common extra-colonic malignancy is endometrial carcinoma, with a risk of occurrence of 71% risk in MSH2 carriers and 44% in MLH1 carriers. It is most commonly seen at lower uterine segment, with common histologies being endometrial, clear cell, uterine papillary serous, and malignant mixed Mullerian tumors.

What are the criteria for defining HNPCC or Lynch Syndrome (LS)?

Revised Bethesda guidelines – One criterion must be met to consider the tumor for MSI testing.

  • Colorectal cancer diagnosed in an individual <50 years of age.
  • Presence of synchronous, metachronous colorectal or other LS-associated tumor
  • Colorectal cancer with MSI-H pathology in an individual <60y of age (presence of Tumor-infiltrating lymphocytes, Crohn-like lymphocytic reaction, mucinous/signet-ring differentiation, medullary growth pattern)
  • Colorectal cancer or LS associated tumor diagnosed in at least one first degree relative <50 years of age
  • At any age in 2 first degree relatives or second degree relatives.

What is the difference between MSI high, low and stable?

% Of Unstable Loci

MSI-H (High)

>30% of tumor markers are unstable

MSI-L (Low)

Atleast 1, but fewer than 30% of markers are unstable

MSS (Stable)

No loci are unstable

How is the surveillance/screening for HNPCC or Lynch Syndrome done?

Colonoscopy is recommended every 1-2 years starting at ages 20-25 years (age 30 years for those with MSH6 mutations), or 10 years younger than the youngest age of the patient diagnosed in the family.

Also recommended annually:

Endometrial Sampling And TVS Of Uterus And Ovaries

Ages 30-35 Y

Urinalysis with cytology

Ages 25-35y

history, examination, education, genetic counselling regarding Lynch syndrome

Age 21 y

What is the role of chemoprevention?

CAPP2 trial has shown that 600mg aspirin/day for a mean of 25 months substantially reduced cancer incidence in LS.

What is the surgical management of HNPCC or Lynch Syndrome?

Extended colectomy (total or subtotal) is done as the incidence of metachronous colorectal cancer is 16% at 10 years, 41% at 20 years, and 63% at 30 years after segmental colectomy. It gives a survival advantage of around 4 years, with a 12% risk of developing cancer in the rectal remnant at 12 years post-colectomy.