Summary This article provides an exam-focused overview of common and high-yield gastrointestinal tumours, covering the oesophagus, stomach, and colon/appendix.
Summary This article provides an exam-focused overview of common and high-yield gastrointestinal tumours, covering the oesophagus, stomach, and colon/appendix. It emphasizes key clinical features, risk factors, pathogenesis, histological differentiators, and genetic pathways crucial for understanding disease progression and diagnosis. Special attention is given to distinguishing features, common precursors, and prognostic indicators to aid in effective study for medical examinations. Key Points - Oesophageal Adenocarcinoma : Arises in the distal 1/3 of the oesophagus, strongly linked to Barrett oesophagus (columnar metaplasia due to chronic GERD) and TP53 mutations. Predominant in white males in Western countries. - Oesophageal Squamous Cell Carcinoma (SCC) : Typically affects the middle 1/3 of the oesophagus. Key risk factors are synergistic alcohol and tobacco use. Associated with squamous dysplasia and potentially HPV in high-risk regions. - Gastric Adenocarcinoma : Classified as intestinal or diffuse type. The diffuse type is characterized by signet ring cells and linitis plastica ("leather bottle stomach"). H. pylori infection is a major risk factor for both types. - Gastric MALT Lymphoma : A primary gastric lymphoma developing in response to chronic H. pylori gastritis. Early-stage disease often regresses with H. pylori eradication. - Carcinoid Tumours : Neuroendocrine tumours most common in the GIT, especially the small intestine (most aggressive) and appendix (almost always benign). Carcinoid syndrome occurs with liver metastases. - Gastrointestinal Stromal Tumour (GIST) : The most common mesenchymal tumour of the abdomen, primarily in the stomach. Arises from Interstitial Cells of Cajal with activating mutations in c-KIT or PDGFRA , responsive to tyrosine kinase inhibitors like Imatinib. - Colorectal Adenomas : Premalignant neoplastic polyps characterized by cytologic dysplasia. Sessile serrated adenomas lack dysplasia but are also premalignant. - Familial Adenomatous Polyposis (FAP) : Autosomal dominant condition due to an APC gene mutation, leading to 100 adenomatous polyps and near-certain colorectal cancer by age 30 if untreated. Represents the chromosomal instability pathway. - Hereditary Non-Polyposis Colorectal Cancer (HNPCC/Lynch Syndrome) : Caused by defects in DNA mismatch repair genes ( MLH1 , MSH2 ). Characterized by fewer polyps than FAP but an increased risk of colorectal and extracolonic cancers via the microsatellite instability pathway. - Colorectal Cancer Prognosis : Primarily determined by the depth of invasion (T stage) and the presence or absence of lymph node metastases (N stage). - Pseudomyxoma Peritonei : A severe complication of mucin-producing appendiceal tumours, leading to the abdomen filling with tenacious mucin, managed by debulking but ultimately fatal. Detailed Notes I. OESOPHAGUS 1. Oesophageal Adenocarcinoma This rapidly increasing cancer primarily affects white males in Western countries. Its development is a classic example of metaplasia-dysplasia-carcinoma sequence: Pathogenesis : Chronic GERD leads to Barrett oesophagus (intestinal metaplasia of squamous epithelium). Accumulation of genetic (e.g., TP53 mutation) and epigenetic changes drives progression through low-grade and high-grade dysplasia to invasive adenocarcinoma. Morphology : Typically located in the distal 1/3 of the oesophagus, often invading the gastric cardia. Microscopically, it's a mucin-producing, gland-forming tumour, frequently with adjacent Barrett oesophagus. 2. Oesophageal Squamous Cell Carcinoma (SCC) More common in adults 45, especially African Americans and in specific high-incidence regions globally. Risk Factors : Alcohol and tobacco use are synergistic . Other risks include poverty, nutritional deficiencies, caustic injury, achalasia, Plummer-Vinson syndrome, very hot beverages, and, in high-risk regions, HPV. Pathogenesis : Progression from normal squamous epithelium through squamous dysplasia (an in situ lesion) to invasive SCC. Morphology : Most often found in the middle 1/3 of the oesophagus. Early lesions are plaque-like; later stages can be polypoid, ulcerated, or diffusely infiltrative. Microscopic features include squamous differentiation. Spread : Rich submucosal lymphatics allow for widespread local and longitudinal spread, including "skip lesions." Lymph node metastasis patterns vary by location: upper 1/3 to cervical nodes, middle 1/3 to mediastinal nodes, lower 1/3 to gastric/coeliac nodes. Local invasion can lead to tracheoesophageal fistulas (aspiration pneumonia) or aortic haemorrhage. Clinical Features (Both Oesophageal Tumours) Symptoms like progressive dysphagia, odynophagia, weight loss, and haemorrhage usually indicate advanced disease. Tracheoesophageal fistulas can present with aspiration. High-Yield Differentiators: Adenocarcinoma vs SCC Feature Adenocarcinoma SCC ---------------- ---------------------- ----------------------- Location Distal 1/3 Middle 1/3 Precursor Barrett oesophagus Squamous dysplasia Key Risk GERD, obesity, tobacco Alcohol, tobacco, poverty Demographics White males, Western African Americans, rural/developing Microscopy Glands, mucin Squamous differentiation II. STOMACH 3. Gastric Polyps Inflammatory & Hyperplastic Polyps : Reactive lesions associated with chronic gastritis. Malignant risk increases with size but is generally low. Gastric Adenomas : True premalignant lesions arising in chronic gastritis with intestinal metaplasia. Require complete excision and surveillance. 4. Gastric Adenocarcinoma Incidence varies geographically and is higher in lower socioeconomic groups. Aetiology : H. pylori infection is the most common cause, along with chronic atrophic gastritis and EBV. Histologic Types : Intestinal Type : Bulky, discrete, gland-forming masses, often ulcerated. Diffuse Type : Poorly cohesive, infiltrative growth of signet ring cells (mucin-filled cells with peripherally displaced nuclei). This leads to marked thickening of the gastric wall without a discrete mass, a condition known as linitis plastica ("leather bottle stomach"). 5. Gastric MALT Lymphoma This primary gastric lymphoma originates from MALT, which is typically absent in the stomach but develops in response to chronic H. pylori gastritis . Crucially, eradication of H. pylori can lead to tumour regression in early-stage disease. 6. Carcinoid Tumours Arise from neuroendocrine cells throughout the GIT. Prognosis by Location : Small intestine carcinoids are generally the most aggressive, while appendix carcinoids are almost always benign, often discovered incidentally. Carcinoid Syndrome : A paraneoplastic syndrome occurring when vasoactive substances produced by the tumour bypass hepatic metabolism, typically due to liver metastases . Symptoms include cutaneous flushing, sweating, bronchospasm, colicky abdominal pain, diarrhea, and right-sided cardiac valvular fibrosis. 7. Gastrointestinal Stromal Tumour (GIST) The most common mesenchymal tumour of the abdomen, predominantly found in the stomach. Arises from the Interstitial Cells of Cajal (GIT pacemaker cells). Driven by activating mutations in receptor tyrosine kinases, primarily c-KIT or PDGFRA . Treatment : Responds well to tyrosine kinase inhibitors like Imatinib. III. COLON 8. Colorectal Polyps Non-Neoplastic : Hyperplastic Polyps : Benign epithelial proliferations, usually in the left colon/rectum. No malignant potential ; important to differentiate from sessile serrated adenomas. Inflammatory, Hamartomatous (e.g., Peutz-Jeghers). Neoplastic (Adenomas) : Precursors to colorectal adenocarcinoma. Hallmark is cytologic dysplasia . Sessile serrated adenomas , despite lacking overt cytologic dysplasia, are also considered premalignant. 9. Familial Adenomatous Polyposis (FAP) An autosomal dominant syndrome caused by a germline mutation in the APC gene (tumour suppressor, chromosome 5). Defined by the presence of 100 adenomatous polyps in the colon. Colorectal can