GI Polyps & Neoplasms

Question 1

Sessile vs. Pedunculated Polyp

Answer 1

• sessile = no stalk
• pedunculated = stalk

Question 2

Tubular vs. Villous polyp

Answer 2

• tubular = smooth-ish borders
• villous = borders look like villi
  
  • villous = “villanous” (worse prognosis)

Question 3

Types of non-neoplastic polyps + key association

Answer 3

• non-neoplastic type polyps are frequently “syndromic”, i.e. associated with a genetic syndrome that overall predisposes to cancer development
• inflammatory polyps
• hamartomatous
  
  • juvenile
  • peutz-jeghers
• hyperplastic

Question 4

Characteristics of inflammatory polyps

Answer 4

• Often present with bleeding
• Often due to mucosal prolapse (very common in the rectum)
• Cycles of injury and healing result in “polyp” formation
  
  • inflamed colonic mucosa ==> ulceration/erosion ==> epithelial hyperplasia

Question 5

Characteristics of hamartomatous polyps

Answer 5

• most occur during childhood
• Hamartoma: “tumor-like” over-growth / mature tissue / developing where it is normally present (e.g. colonic tissue developing in the colon)
• Associations: Juvenile (sporadic and syndromic) and Peutz-Jeghers (syndromic)
• benign features on histo, but often have foci of dysplasia
• ==> increase risk for future GI carcinoma

Question 6

Characteristics of hyperplastic polyps

Answer 6

Smooth, nodular lesion with flat base (sessile)

• (1) The lesion abuts muscularis mucosa (arrow) and does not have a stalk.
• (2) It is composed of crowded, mixed absorptive and goblet cells
• (3) A serrated architecture results
• (4) This is a benign, usually non-neoplastic lesion to be distinguished from SSPs

Question 7

hyperplastic vs. sessile serrated polyps/adenomas

Answer 7

• hyperplastic
  
  • NOT pre-malignant
  • common @ L side of colon
  • not dysplastic epithelium
• Sessile serrated/adenoma
  
  • pre-malignant
    
    • CAN progress to adenocarcinoma
  • common @ R side of colon
  • +/- dysplastic epithelium

Question 8

Characteristics (general) of adenomas

Answer 8

• Size is variable – range from a few mm to several cm (10 cm or more)
• Present in nearly 50% of Western adults by age 50
• Present throughout the colon
• origin: epithelial cells
• gland-forming masses

Question 9

Risk factors (related to adenomas) for malignancy

Answer 9

• Have epithelial cytologic dysplasia ranging from low grade to high grade (carcinoma in situ)
• Villous adenomas contain foci of invasion more frequently than tubular adenomas
• SIZE MATTERS
  
  • most important characteristic that correlates with risk of malignancy overall in the patient
• Presence of high grade dysplasia increases risk of malignant transformation in that polyp but not in the rest of the colon

Question 10

Histologic features of adenomas

Answer 10

1. Cells
   
   1. Piling up on each other (no respect!)
2. Nuclei
   
   1. Darker (hyperchromasia)
   2. Progressive loss of basal-orientation
3. Cytoplasm
   
   1. Reduced compared to nucleus (increased N:C ratio)
   2. Reduced mucin production
4. Mitotic Figures
   
   1. Increased mitotic activity

Question 11

Risk factors for colorectal cancer

Answer 11

• Increase Risk
  
  • Body fatness
  • Abdominal fatness
  • Red/processed meat
  • Alcoholic drinks
  • Smoking
  • Genetic predisposition
• Decrease Risk
  
  • Physical Activity
  • Foods with High Fiber

Question 12

Major genetic syndromes that increase colorectal cancer risk

Answer 12

• Sporadic (65-85%)
• Familial Adenomatous Polyposis (FAP) (<1%)
• Hereditary Nonpolyposis Colorectal Cancer (HNPCC) (2-3%)

Question 13

Main molecular pathways to colorectal cancer

Answer 13

• WNT/APC/beta-catenin – classical adenoma-carcinoma sequence
• K-Ras/MAP kinase/PI3 kinase signaling pathways—activating mutations
• Microsatellite Instability – defects in mismatch repair proteins

Question 14

Characteristics of WNT/APC pathway to colorectal cancer

Answer 14

• Wnt protein ligands are critical for development
  
  • drive proliferation of their target tissues/organs
• Wnt pathway regulates the levels of cytoplasmic b-catenin
  
  • WNT binds to receptor ==> disruption of APC/beta-catenin complex (normally, this complex leads to destruction of beta-catenin/low levels of b-c) ==> elevated beta-catenin levels @ cytosol
  • b-catenin translocates to nucleus ==> cell cycle initiation w/TCF (transcription factor)
• mutated/absent APC ==> cells behave as if under constant stimulation by WNT

Question 15

Characteristics Familial Adenomatous Polyposis

Answer 15

• APC mutations can run in families, producing Familial Adenomatous Polyposis (FAP)
  
  • AD mutation @ APC gene ==> increased risk of colon cancer,
  • Most people who acquire colon cancer without FAP acquire spontaneous somatic mutations in APC

Question 16

Characteristics of Hereditary Non-Polyposis Colorectal Cancer Lynch Syndrome

Answer 16

• Develop colon cancer at an earlier age than sporadic forms
• Tend to be right-sided
• Inherit mutation of mismatch repair gene allele
  
  • _​_acquire the second allele mutation over time leading to microsatellite instability

Question 17

Common presentation of early colon carcinoma

Answer 17

–No symptoms most often
–Nonspecific findings
•Fatigue
•Weight loss
•Anemia

Question 18

Common presentation of advancing colon carcinoma

Answer 18

• Change in bowel habits and indicators
  
  • Constipation
  • Urgency
• Narrowing of stool
• Cramping / pain
• Blood Loss
  
  • Blood in stool or bleeding from rectum (BBBPR)
  • Anemia (iron-deficiency)
• Unexplained weight loss

Question 19

Common methods of screening/detection of colorectal neoplasm

Answer 19

• visualization +/- biopsy
  
  • colonoscopy
  • barium enema
• blood detection @ stool
  
  • HemOccult of Fit test
  • looking for hemorrhage of ulcerated lesion
• DNA/mutation detection in stool
  
  • looking for shedded neoplastic cells

Question 20

Histologic features of invasive adenocarcinoma

Answer 20

• gland formation
• variable - scant mucin production
• invade muscularis propria ==> desmoplastic (fibrotic) response
• “dirty necrosis” w/in some glands

Question 21

Important prognostic factors in colorectal cancer

Answer 21

1. depth of invasion
2. presence/absence of lymph node metastasis
3. distant metastasis

Question 22

Sporadic colon cancer (majority): Molecular defect, target gene, predominant side, histology

Answer 22

• molecular = APC/WNT pathway
• gene = APC
• side = left
• histo =
  
  • tubular, villous
  • typical adenocarcinoma

Question 23

Sporadic colon cancer (minority): Molecular defect, target gene, predominant side, histology

Answer 23

• moceluar = DNA mismatch repair
• gene =
  
  • MSH2
  • MLH1
• side = right
• histo =
  
  • sessile serrated adenoma
  • mucinous adenocarcinoma

Question 24

FAP (majority): Molecular defect, target gene, transmission, histology

Answer 24

• molecular = APC/WNT
• gene = APC
• transmission = AD
• histo =
  
  • tubular, villouis
  • typical adenocarcinoma

Question 25

HNPCC : Molecular defect, target gene, transmission, predominant site, histology

Answer 25

• molecular = DNA mismatch
• gene =
  
  • MSH2
  • MLH1
• transmission = autosomal
• side = right
• histo =
  
  • sessile serrated adenoma
  • mucinous adenocarcinoma