Colorectal cancer
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2024
2023
2022
2021
Adenomas
colorectal p. 396
Anemia
colorectal cancer p. 395
APC gene p. 220
colorectal cancer and p. 396
Carcinomas
colorectal p. 396
Colon cancer
5-fluorouracil for p. 444
irinotecan/topotecan for p. 444
labs/findings p. 726
metastases of p. 202
oncogenes and p. 220
Staphylococcus gallolyticus and p. 135
tumor suppressor genes and p. 220
Colorectal cancer p. 395
adenomatous polyposis and p. 394
bevacizumab for p. 446
cetuximab for p. 446
incidence/mortality in p. 202
labs/findings p. 727
Lynch syndrome p. 37
molecular pathogenesis of p. 396
therapeutic antibodies p. 120
tumor suppressor genes and p. 220
Exophytic mass (colorectal cancer) p. 395
Geriatric patients
colorectal cancer p. 395
Hematochezia
colorectal cancer p. 395
Inflammatory bowel disease (IBD) p. 389
colorectal cancer and p. 395
Iron deficiency anemia p. 423
colorectal cancer p. 395
KRAS gene p. 220
colorectal cancer and p. 396
Nonsteroidal anti-inflammatory drugs (NSAIDs) p. 495
colorectal cancer chemopreventative p. 396
Smoking
colorectal cancer and p. 395
Streptococcus bovis p. , 135
colon cancer p. 726
colorectal cancer and p. 395
Tumor markers
colorectal cancer p. 395
Weight loss
colorectal cancer p. 395
Transcript
Content Reviewers
Colorectal carcinoma, also known as colon cancer, is when malignant or cancerous cells arise in the large intestines, which includes the colon and rectum.
It is the most common type of cancer of the gastrointestinal tract, and a major cause of death and disease around the world.
The large intestine is found in the abdominal cavity, which can be thought of as having two spaces - the intraperitoneal space and the retroperitoneal space.
The intraperitoneal space contains the first part of the duodenum, all of the small intestines, the transverse colon, sigmoid colon, and the rectum; the retroperitoneal space contains the distal duodenum, ascending colon, descending colon, and anal canal.
So the large intestines essentially weave back and forth between the intraperitoneal and retroperitoneal spaces.
Now, the walls of the gastrointestinal tract are composed of four layers. The outermost layer is the called serosa for the intraperitoneal parts, and the adventitia for the retroperitoneal parts.
Next is the muscular layer, which contracts to move food through the bowel.
After that is the submucosa, which consists of a dense layer of tissue that contains blood vessels, lymphatics, and nerves.
And finally, there’s the inner lining of the intestine called the mucosa; which surrounds the lumen of the gastrointestinal tract, and comes into direct contact with digested food.
The mucosa has invaginations called intestinal glands or colonic crypts, and it’s lined with large cells that are specialized in absorption.
Most colorectal carcinomas are adenocarcinomas, meaning that they arise from the cells lining the intestinal glands.
Most cases of colorectal tumors happen because of sporadic mutations, but a small number are caused by known genetic mutations that run in a person’s family.
An example of this is the adenomatous polyposis coli gene, or APC gene, which is a tumor suppressor gene.
Normally, the APC protein identifies when a cell is accumulating a lot of mutations and forces it to undergo apoptosis, or programmed cell death.
But when the APC gene is mutated, the mutated bowel cells don’t die, and instead some start dividing uncontrollably, giving rise to polyps.
Over time, these polyps might accumulate more mutations in other tumor suppressor genes like the K-ras gene or the p53 gene, and ultimately it might might become a malignant tumor - meaning that the cells might be able to invade neighboring tissues.
Another well known example are genetic mutations in DNA repair genes which help fix up mutations in cellular DNA.
When they’re out of action - cells accumulate mutations and over time can develop into polyps and eventually adenocarcinomas.
So, broadly speaking, adenocarcinomas are the malignant evolution of polyps, and polyps arise when cells start dividing faster than usual.
There are many different types of polyps, and some are more prone to become malignant; those are called pre-malignant or neoplastic polyps.
These pre-malignant polyps can be classified into adenomatous and serrated, according to how they look under the microscope.
Typically, adenomatous polyps have an APC mutation and the cells look like normal colonic mucosa cells, whereas serrated polyps have defects in DNA repair genes and have a saw-tooth appearance.
When tumors become cancerous, they can be categorized into stages.
Stage 0 is carcinoma in situ, meaning that the tumor has not grown beyond the mucosa.
Stage 1 is when the tumor has grown beyond the mucosa, but has not spread to lymph nodes or distant organs.
Stage 2 is when the tumor has invaded the whole colonic or rectal wall, and may have reached nearby organs or tissues, but still hasn’t spread to lymph nodes or distant organs.
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- "Robbins Basic Pathology" Elsevier (2017)
- "Pathophysiology of Disease: An Introduction to Clinical Medicine 8E" McGraw-Hill Education / Medical (2018)
- "CURRENT Medical Diagnosis and Treatment 2020" McGraw-Hill Education / Medical (2019)
- "Current and future role of genetic screening in gynecologic malignancies" American Journal of Obstetrics and Gynecology (2017)
- "Metastatic Carcinoma Occurring in a Gastric Hyperplastic Polyp Mimicking Primary Gastric Cancer: The First Reported Case" Case Reports in Pathology (2014)
- "Mutation Rate in Human Microsatellites: Influence of the Structure and Length of the Tandem Repeat" The American Journal of Human Genetics (1998)