Case 4- colon cancer, staging and screening

Question 1

Why is grading and staging important

Answer 1

Useful for evidence-based prognosis and may indicate different treatment. Helps communication between health professionals as you don’t have to describe the cancer in detail

Question 2

Cancer grading

Answer 2

Histological and is based on tissue samples from a biopsy, looking at how aggressive the cancer is. It looks at the degree of differentiation between the tumour and normal tissue. Tumours which are poorly differentiated will be very different to normal tissue and will be more aggressive.

Question 3

How can degree of differentiation be determined by

Answer 3

• Mitotic activity- more aggressive tumours will have increased mitotic activity
• Nuclear size- more aggressive tumours will have increased DNA replication meaning that the nucleus size within cells increases
• Hyperchromasia (how dark the nucleus is)- increased DNA replication in aggressive tumours causes the nucleus to appear darker when looked at under the microscope, as it contains more DNA than usual

Question 4

Bowel cancer grading

Answer 4

GX - cannot be identified - for example the tissue sample may not have been labelled correctly
G1 - well differentiated
G2 - moderately differentiated
G3 - poorly differentiated
G4 - undifferentiated (anaplastic tissue)

Question 5

Cancer staging

Answer 5

Is anatomical and is based on scans, it looks at how widespread the cancer, will also look at its size and if it entered the lymphatic system

Question 6

Most common staging method

Answer 6

TNM is the most common staging method, it stands for tumour size, nodal involvement and metastases. It will be written in the format T2N1M0

Question 7

Staging tumour size guide

Answer 7

TX- tumour size cant be assessed, no scans or imaging
T0- no tumour present
Tis- ‘tumour in situ’. The tumour has malignant potential, the biopsy shows increased mitotic activity or an enlarged nuclei, but the tumour has not yet invaded through the basement membrane.
T1- into submucosa
T2- into muscularis propria
T3- into subserosa
T4a- into visceral peritoneum
T4b- attached to other organs/structure

Question 8

Staging nodal involvement

Answer 8

NX- cant be assessed
N0- no lymph nodes involved
N1- 1 single lymph node involved or more then one lymph node is involved but they are all part of the same group of lymph nodes
N2- more then one group of lymph nodes affected

Question 9

Staging metastases involvement

Answer 9

M0- no metastases present

M1- metastases are present (either one or multiple)

Question 10

Stage 0-4 cancer

Answer 10

A stage 0 cancer is one where the tumour is in situ (has malignant potential but hasn’t invaded through the basement membrane. Stages 1, 2 and 3 show that there is local growth and spread. In stage 4 there is distant metastases.

Question 11

Screening and public health

Answer 11

Screening is a part of secondary disease prevention. It helps identify a disease at its early stage so it can be more easily managed

Question 12

Types of prevention

Answer 12

Primary prevention- reducing the risk of a disease i.e. immunisation or banning toxic substances
Secondary prevention- identification/ management of an early disease i.e. screening and self-breast examinations by women
Tertiary prevention- prevention of chronic and disabling effect of a disease i.e. chronic disease management programmes and support programmes

Question 13

Screening

Answer 13

Not a diagnostic procedure but instead identifies apparently healthy people who are at an increased risk of a disease or a condition. They can then be offered information, further tests and appropriate treatment to reduce their risk and/or any complications arising from the disease or condition.

Question 14

Fetal anomaly screening programme

Answer 14

Screens for 11 structural anomalies including down’s syndrome. Multiple tests done between 10 and 20 weeks

Question 15

Infectious diseases in pregnancy screening (IDPS) programme

Answer 15

Offers testing for hep B, HIV and syphilis. Usually done at 10 weeks

Question 16

New-born and infant physical examination (NIPE) screening programme

Answer 16

Screens new-borns within 72 hours and at 6-8 weeks after birth, including hips, eyes and hearts

Question 17

New-born blood spot (NBS) screening programme

Answer 17

Heel prick test at 5 days old. For sickle cell, CF, congenital hypothyroid, inherited metabolic diseases, e.g phenylketonuria, MCADD

Question 18

New-born hearing screening programme (NHSP)

Answer 18

Offered to all babies within 4-5 weeks to test hearing

Question 19

Sickle cell and thalassaemia (SCT) screening programme

Answer 19

All pregnant women in England are offered a blood test to find out if they carry a gene for thalassaemia. Those at high risk of being a sickle cell carrier are offered a test for sickle cell.

Question 20

Diabetic eye screen

Answer 20

Yearly retinal exam of all people with a diagnosis of diabetes over age 12

Question 21

Bowel cancer screening

Answer 21

FIT tests for all adults aged 60-74, every two years. gFOB test is also used. In the FIT test the end of a stick is dipped into a single bowel motion, replaced in a tube and returned in a prepaid envelope

Question 22

Cervical cancer screening

Answer 22

LBC test for all women. Aged 25-49, every 3 years. for those aged 50-64 it’s every 5 years

Question 23

Breast cancer screening

Answer 23

Mammogram all women aged 50-70, every 3 years, and self refer>70 years.

Question 24

NHS health check screening

Answer 24

Adults between the age of 40-74 get this test every 5 years. It checks your lifestyle and family history, height and weight, blood pressure and blood test. It uses an algorithm to provide a risk assessment for a CVD event in the next 5 years. It screens for diabetes, heart disease and stroke.

Question 25

Genetic screening

Answer 25

Done under certain circumstances to inform reproductive choice, identifies risk factors and can inform preventative action (BRCA). Can also be used in antenatal screening and IVF pre-implantation genetic testing.

Question 26

The three main categories of screening

Answer 26

Proactive screening which can be targeted, regular breast exams between 50 and 70, or untargeted, all new-borns get a physical exam. Voluntary screening is by patient request i.e. prostate cancer. Opportunistic screening is if you got a cholesterol test because you were visiting the GP.

Question 27

The 4 criteria’s for implementing a screening test

Answer 27

The disease, the screening test, diagnosis and treatment, the programme

Question 28

Screening test criteria- the disease

Answer 28

Needs to be a common and serious health problem. There needs to be a strong link between the risk factors of the disease marker you are testing and the actual disease

Question 29

Screening test criteria- the screening test

Answer 29

Test must be valid (sensitive and specific), simple, cheap, safe, acceptable and reliable. If the test is not acceptable to the patient there will be a low uptake. Sensitivity is about correctly identifying those who have the disease (true positive) whilst specificity is about identifying those who don’t have the disease (true negative).

Question 30

Screening test criteria- diagnosis and treatment

Answer 30

An agreed policy and appropriate treatment options for those who test positive. The facilities must be adequate to meet the demand of the treatment.

Question 31

Screening test criteria- the programme

Answer 31

There must be evidence that the screening programme is beneficial and reduces disease and mortality. It must be acceptable to the public and healthcare professionals whilst being cheap. There must also be the appropriate facilities in place with quality assurance.

Question 32

The principles of Cancer surveillance

Answer 32

About analysing and collecting data in order that action may be taken. There should be systematic collection of data for cases, analyses of data and stats and distribution of this data. In the UK all cases of cancer are registered on the national cancer registration

Question 33

Colonic carcinoma- inherited

Answer 33

Under 10% of colonic carcinoma cases have a true inherited disposition, 1% is FAP (inherited mutations in the APC mutation gene, they get polyps which develop into cancer at 40) and 2-5% HNPCC (Lynch syndrome- due to mutations in DNA repair genes).

Question 34

Colonic carcinoma risk factors

Answer 34

Being over 50, previous CRC (the colonic epithelium will be unstable), strong family history of CRC. Previous adenomatous polyps, longstanding IBD (inflammatory bowel disease such as Crohn’s or ulcerative colitis, the risk is proportional to how long you have had the disease and how much of the bowel is affected), inherited syndromes, type 2 diabetes and an unhealthy lifestyle. You reduce your risk by eating high fibre fruit and veg, as low fibre and red meat increase the amount of time faecal matter is in the colon. Red meat consumption, smoking and alcohol consumption increase the risk.

Question 35

Pathology of colon cancer

Answer 35

Highly proliferative epithelium, adenoma, adenocarcinoma

Question 36

Symptoms of right sided colon cancer

Answer 36

Tiredness, weight loss, anaemia, occult bleeding and RIF mass

Question 37

Symptoms of left sided colon cancer

Answer 37

Tiredness, weight loss, colicky pain, rectal bleeding, bowel obstruction, tenesmus, LIF mass and change in bowel habits

Question 38

How the gut is separated

Answer 38

The gut is split into the foregut, the midgut and the hindgut. The left side of the colon is hindgut and most of the right side is in the midgut. Right colon cancer tends to cause pain around the umbilicus and the left colon cancer causes pain in the hypogastrium/suprapubic.

Question 39

Why do cancers in the right colon tend to grow larger

Answer 39

There is lots of space for the cancer to grow into without causing obstructive symptoms, such as bloating or pain. The faecal stream is liquid so is able to move through a small space.

Question 40

Why is colon cancer associated with Iron deficient anaemia

Answer 40

As the cancer grows it is supplied by blood vessels, these vessels are very fragile and tend to bleed. The blood will mix with the fecal stream and not be visible. So cancers on the right side wont show their bleeding but will deplete the bodies iron stores leading to anaemia.

Question 41

What type of anaemia is iron deficient anaemia

Answer 41

Microcytosis with small red blood cells

Question 42

Why is colon cancer a good candidate for a screening programme

Answer 42

The earlier you pick up bowel cancer the more treatable it is, i.f you have a positive screening test a colonoscopy will be performed

Question 43

Mechanism of bowel cancer

Answer 43

Go through a pre-malignant stage before they become cancerous. They start at adenomas which are benign growths. There is a mutation in the APC gene (tumour suppressor gene) which leads to uncontrolled growth of the epithelium (Hyperproliferative epithelium). Then there is a K ras and DCC mutation which causes an adenoma. Then a p53 mutation which creates a carcinoma.

Question 44

Appearance of a non-benign adenoma

Answer 44

The cells will not be regular, some patches will be more vascular then others and the centre will be sunken suggesting the scar tissue is pulling the polyp down. The basement of the epithelium will be a lot less clear

Question 45

Treatment for colon cancer

Answer 45

At the T1 stage the tumour may be removable though endoscopy and wont require surgery. Fluid can be injected in the submucosal space, this will lift the polyp free of the bowel wall. A snare can be placed over the polyp and then it can be removed

Question 46

Testing for colon cancer

Answer 46

You can use a faecal immunochemical test (FIT) to detect blood in your stool, tests for Globin so you don’t get false positives. You will also do a blood test to detect number of red and white blood cell. You will then have a colonoscopy to confirm the cancer, take a biopsy to confirm the microscopic factors. CT colonoscopy can provide x-ray pictures.

Question 47

Polyps

Answer 47

Mass of cells that grow in the inner lining of the colon.

Question 48

Haemorrhoids

Answer 48

Swollen veins in the lower part of the rectum or anus

Question 49

Fissure

Answer 49

A cut or tear in the anus

Question 50

Diverticular disease

Answer 50

The growth of small sacs in the colon due to weakening of the lining, they protrude outwards

Question 51

Ulcerative colitis

Answer 51

Swelling of the colon and rectum

Question 52

Carcinoma

Answer 52

Cancers derived from epithelial cells

Question 53

Sarcoma

Answer 53

Cancers derived from connective tissue, originating in mesenchymal cells

Question 54

Lymphoma

Answer 54

Cancer forming from blood forming cells that tend to leave the bone marrow and mature in the lymph nodes and blood

Question 55

Blastoma’s

Answer 55

Cancers derived from immature precursor cells or embryonic tissue