Clinical oncology

Question 1

Cancer definition

Answer 1

Group of diseases characterised by uncontrolled growth and spread of abnormal cells within a body

Question 2

Oncology/ oncologists

Answer 2

Specialism/ specialists in cancer

Question 3

How many cancers?

Answer 3

Around 200

Question 4

Classification of cancers

Answer 4

Type of cancer cell
-glandular e.g. adenocarcinoma
-skin/ mucosa e.g. squamous cell carcinomoma
-connective tissues e.g. sarcoma
-small cell e.g. small cell carcinoma
Grade (degree of differentiation usually G1-G3)
TNM staging
-size of tumour
-spread to lymph nodes
-spread to distal organs

Question 5

Prognostic makers to determine treatment pathways

Answer 5

E.g.

• oestrogen receptor (ER) in breast cancer
• HER2 receptor in breast cancer
• BRAF mutation in melanoma
• HPV association in head and neck cancer
• EGFR expression in lung cancer
• PSA level in prostate cancer

Question 6

How common is cancer?

Answer 6

1 in 3 lifetime risk

Increasing incidence for several types

Question 7

Incidence of oral cavity cancer

Answer 7

Males higher than females

• males ~11/100,000
• females ~7/100,000

Question 8

Risk factors for head and neck cancer

Answer 8

Smoking
Alcohol
Diet and nutrition
Viruses
-HPV
-Epstein Barr Virus
Immunosuppression
Premalignant oral conditions
-leukoplakia
-lichen sclerosis
Radiotherapy exposure

Question 9

Risk factors for colorectal cancer

Answer 9

Dietary

Genetic

Question 10

Risk factors for lung cancer

Answer 10

Smoking

Question 11

Risk factors for breast cancer

Answer 11

Genetic

Obesity

Question 12

Risk factors for skin cancer

Answer 12

Sun exposure

Question 13

Risk factors for cervical cancer

Answer 13

HPV

Question 14

Changes in incidence of oral cancer

Answer 14

Men over 80: incidence of OC more than halved since 1975
Men in 70’s: rates remained relatively stable
Large > in incidence of OC diagnosed in men in 40s & 50s: rates more than doubled

Question 15

Improved survival

Answer 15

Earlier diagnosis
- > pt awareness (media, internet)
-screening programs (colorectal, breast, prostate, ovary, cervix)
Improved treatment
-surgery
-radiotherapy
-chemotherapy

Question 16

Treatment options

Answer 16

1. Surgery
2. Radiotherapy
3. Chemotherapy
4. Hormonal therapy
5. Targeted therapies
6. Immunotherapy
7. Laser therapy
8. Cryotherapy
9. Best supportive care
10. Any combination of these

Question 17

Surgery

Answer 17

Can be curative treatment on its own for many cancers
Usually need to be fit for GA
Aims to remove tumour with clear margins
May require further treatment on review of histology
-adjuvant chemotherapy/ hormones
-adjuvant radiotherapy

Question 18

Side effects of surgery

Answer 18

Functional
Cosmetic
Risks of anaesthetic

Question 19

Chemotherapy

Answer 19

The use of cytotoxic drugs to kill malignant cells
Systemic treatment: IV, PO or IT
Can be given in more localised way for certain tumour types e.g. intravesical to treat superficial bladder cancer
Drugs which affect cell function
Drugs often used in combination in increase effect
Anti cancer action in expense of side effects

Question 20

Different mechanisms of action of chemotherapy

Answer 20

Platinum
-cisplatin/ carboplatin/ oxaliplatin
Taxanes
-docetaxel/ paclitaxel
Anti metabolites
-5 fluorouracil/ methotrexate
Alkylating agents
-dacarbazine/ temozolamide
Anthracyclines
-doxorubicin/ epirubicin

Question 21

Chemotherapy adjuvant treatment

Answer 21

High risk post op pts
Often combination of drugs - more side effects
Given chemo to < risk of recurrence
-pt may not have disease and not need it
-pt may get recurrence despite chemo
-proportion (5-10%) will be cured because of it
-need to assess risks vs benefits with pt carefully

Question 22

Chemotherapy -palliative treatment

Answer 22

Treatment to improve symptoms and maybe extend life
Often single drug
- < side effects
-lower intensity of treatment
Not usually offered until symptomatic
Stop early if not working or increasing toxicity

Question 23

Chemo side effects

Answer 23

General
-nausea and vomiting
-fatigue
-change in taste
-bowel disturbance
Skin
-rash
-hair loss
-extravasation
Nerves
-neuropathy
-hearing loss
Infertility/ premature menopause
Bone marrow
-anaemia
-neutropenia
-thrombocytopenia
Renal dysfunction
Liver dysfunction
Allergic reaction/ anaphylaxis
Lung toxicity
-fibrosis
-bleomycin
Cardiac toxicity
-cardiomyopathy
-anthycyclines

Question 24

More modern targeted agents

Answer 24

Tyrosine kinase inhibitors (oral)
-Vermurafenib (BRAF mutation melanoma)
-Gefinitinib
-Imatinib 
-Sunitinib
Monoclonal antibodies (IV infusion)
-Trastuzumab (HER2 receptor breast cancer)
-Cetuximab
-bevacuizumab

Question 25

Radiotherapy

Answer 25

Radium used until mid 1900s
-cobalt and caesium units came into use
Linear accelerators been used since late 1940s
The use of ionising radiation to treat cancer

Question 26

Radiotherapy

-therapeutic vs diagnostic

Answer 26

Energy of photos higher in therapeutic setting as opposed to diagnostic setting

• diagnostic x-rays up to 150KV
• therapeutic photons 80KV to 20MV

Question 27

How does radiotherapy work?

Answer 27

Ionising radiation interacts with water molecules –> free radicals
Free radicals cause DNA damage
Malignant and normal cells are damaged
Normal cells can repair if tolerance not exceeded

Question 28

Side effects of radiotherapy

Answer 28

Damage to normal cells
-depend on area to be treated
-divided into early or late effects
Early (acute)
-develop during or shortly after RT
-very common
-nearly always resolve
Late (chronic)
-develop months to years (>40yrs) after RT
-very rare
-irreversible and often severe

Question 29

Intention of radiotherapy

Answer 29

Radical - curative
Palliative - to improve symptoms
Adjuvant - alongside surgery
Neoadjuvant - before surgery
Alone - single modality
Combined with chemo - can sensitise tissues to radiotherapy
*Local treatment

Question 30

Dose and number of radiotherapy treatments (fractions) depends on

Answer 30

Area being treated

Intention of treatment - curative vs palliative

Question 31

Curative radiotherapy

Answer 31

Complex planning
Accurate localisation - CT
Longer course 
More early side effects
Less late side effects

Question 32

Palliative radiotherapy

Answer 32

Simple planning
Simple localisation - X-ray
Short course
Less early side effects
More late side effects

Question 33

Radiotherapy treatment modalities

Answer 33

X-rays
-superficial radiotherapy
-megavoltage radiotherapy 6-20MV
Electron treatment 6-20MeV
Bracytherapy: insertion of isotopes into tumour

Question 34

Superficial radiotherapy

Answer 34

100KV photons
Treats to depth of 6mm
Good for superficial BCC and SCC

Question 35

Megavoltage x-rays and e- treatment

Answer 35

The linear accelerator

Question 36

CT planned radiotherapy

Answer 36

Less dose to underlying structures

Less toxicity?

Question 37

Stereotactic radiosurgery

Answer 37

Brain metastasis
- <3 lesions of 3cm size
Single treatment of high dose

Question 38

Types of head and neck cancer

Answer 38

Oral cavity
-floor of mouth
-anterior 2/3 tongue
-alveolus
-retromolar trigone
-hard palate
Nasopharynx
Oropharynx
Larynx
-supraglottis/ glottis/ post cricoid
Hypopharynx
Sinuses

Question 39

Pathology of head and neck cancer

Answer 39

Squamous cell cancer 90% (arising from mucosa)
Adenocarcinoma
Small cell carcinoma
Sarcoma
Lymphoma
Skin
-SCC
-BCC
-malignant melanoma
-merkel cell tumour

Question 40

Demographics of head and neck cancer

Answer 40

Males > females 2:1
Peak incidence 60-75 years
Mortality: 3000 deaths/ year in England and Wales

Question 41

Human Papilloma Virus

Answer 41

DNA virus
72 L1 capsid proteins
Orogenital transmission
Cervical and oropharyngeal SCC type 16 most common

Question 42

HPV in head and neck cancer

Answer 42

+ve in approx 25%
Distinct disease entity
-younger pts
-40s to 50s
Often not smokers or heavy alcohol drinkers
Associated with orogenital and oroanal sex and > no. partners
HPV related cancer (particularly H&N) definitely on the rise
Improved response to chemoradiation
-28% < risk of dying
-49% < risk of local recurrence

Question 43

Patterns of spread

Answer 43

Locally
-soft tissues
-cartilage
-bone
-nerves
Lymph nodes
-very common esp. nasopharynx and oropharynx
Vascular 
-to lungs, bone and liver occurs late

Question 44

How is the decision made about treatment for an individual pt and their cancer?

Answer 44

Multidisciplinary approach
Need to know
-type of cancer
-stage of cancer
-fitness of pt
-pt's wishes
-functional outcomes for treatments/ side effects of treatments/ is it curative etc

Question 45

Decision making

Answer 45

Should happen in joint clinic

• surgeon
• oncologist
• specialist nurse
• plastic surgeon
• speech and language therapist
• dietician
• (psycology input)

Question 46

Investigations needed:

Answer 46

Clinical examination
Blood tests
Examination under anaesthesia
Biopsy
Imaging
-of primary (MRI, CT scan)
-potential sites of metastatic disease (FDG-PET scan, CT scan thorax/CXR)

Question 47

Other investigations

Answer 47

Bone scan
CT/ MRI scan of brain
Angiograms
etc

Question 48

General management principles of early stage disease

Answer 48

Can be treated with either surgery or Radiotherapy
Choice of treatment largely depends upon functional outcome and patient choice
Surgery allows review of tumour, margins and lymph node status
Cancer involving cartilage or bone is best treated with surgery

Question 49

General management principles of locally advanced disease

Answer 49

Surgery followed by Chemoradiotherapy
Chemoradiotherapy alone
Induction Chemotherapy followed by Chemoradiotherapy

Question 50

General management principles of metastatic disease

Answer 50

Palliative Radiotherapy
Palliative Chemotherapy
Best supportive care

Question 51

Non-surgical oncology for H&N cancer

Answer 51

Radiotherapy
Chemotherapy
Targeted therapy
-organ preservation: primary treatment
-used alongside surgery to > chance of cure (adjuvant treatment)
-often combined together: multimodality therapy

Question 52

Head and neck radiotherapy

Answer 52

Critical structures close e.g. spinal cord, optic chiasm, eyes & brain
Essential to keep pt v still & reproduce same position each day of treatment
Pt often needs to be immobilised using head shell
Pt then has CT scan in head shell
CT is used to mark on:
-areas to be treated
-target volumes
-organs at risk
CT used to produce radiotherapy plan: radiotherapy prescription
Verification process
Pt then goes on to have their treatment
Dose & number of treatments depends on site to be treated and treatment intent
-may be daily treatments for up to 7 weeks if curative
-may be single dose if palliative

Question 53

Verification process (radiotherapy)

Answer 53

Pt then goes to machine called simulator for verification
Treatment check
‘Simulator’ is x-ray machine which can move in same way as treatment machine
Simulates treatment
X-rays taken by simulator to check treatment can be reproduced accurately
Pt position verified

Question 54

Early side effects of head and neck radiotherapy

Answer 54

Xerostomia
Altered/loss of taste
Mucositis
Loss of hair
Fatigue
Cough 
Soreness of skin
-dry desquamation
-moist desquamation

Question 55

Late side effects of head and neck radiotherapy

Answer 55

Xerostomia
Altered taste
Osteo-radionecrosis
Alopecia
Hypothyroidism 
Sub-cutaneous fibrosis
Second malignancy
Altered pigmentation

Question 56

Effects of radiotherapy on oral cavity

Answer 56

Xerostomia accelerates dental decay
Osteo-radionecrosis of the mandible 
-associated with poor dental hygiene
Pre-treatment dental assessment essential
-for necessary treatment
-education 
-on going care
Some ps require dental clearance
-issues with treatment start date

Question 57

Radiotherapy technology

Answer 57

Developing Rapidly
More accurate delivery
Dose escalation
Less toxicity
Greater monitoring during treatment
Progress
-conformal 3D radiotherapy
-IMRT
-rotational treatment (Rapid Arc)
-robotic mounted treatment machines (Cyberknife)

Question 58

Chemotherapy in head and neck cancer

Answer 58

Concurrent Chemradiotherapy
-Cisplatin every 3 weeks during Radiotherapy
Induction Chemotherapy
-Combination Cisplatin based chemotherapy prior to Radiotherapy for fit patients with bulky tumours
-Docetaxel/ Cisplatin// 5FU (TPF) x3 every 3 weeks
Palliative chemotherapy
-Cisplatin and 5FU every 4 weeks

Question 59

Early side effects of chemotherapy

Answer 59

Alopecia
Bone marrow toxicity
-neutropenia
-thrombocytopenia
-anaemia
Mucositis
Diarrhoea
Nausea/vomiting
Peripheral Neuropathy
Ototoxicity 
Altered taste

Question 60

Late effects of chemotherapy

Answer 60

Infertility
Early menopause
Pulmonary fibrosis
Renal impairment
Cardiomyopathy
Infertility
Peripheral neuropathy
Second malignancy

Question 61

Dentists and oncology

Answer 61

Diagnosis of oral cavity tumours
Health promotion
Dental assessment pre-treatment	
-RT, chemotherapy, bisphosphonates
Pts receiving chemo may require dental work
-abscess 
-beware neutropenia & thrombocytopenia
-may need to ask oncologists opinion
Post treatment follow up
Screening for oral cancer
Maxillo-facial surgeons
Restorative dentists

Question 62

General rule for dental treatments while on chemotherapy

Answer 62

Preferably all urgent dental work to be done before commencing chemo
-above not practical for all as treatment needs to start asap to improve outcomes
If already on chemo:
-find out length of cycle
-in 3 weekly cycle (most common) max risk of immuno-suppression between 7014 days
-best to always check FBC prior to urgent dental tx to ensure not neutropenic or low platelets

Question 63

Timing for dental work while on chemo

Answer 63

General rule: avoid if not urgent
In 3 weekly cycle, counts usually are recovering in 3rd week
So just before next cycle is due
Always check FBC prior
Neutropenia is Neuts <1.0
Thrombocytopenia is platelets <100
RIsk of bleeding if platelets <20/ 30

Question 64

Dental abscess in immunocompromised pt

Answer 64

Usually on neutropenic sepsis protocol with IV antibiotics and other supportive measures
Unlikely dental abscess is only source of infection
If no other source identified and sepsis not improving with above measures
-draining of abscess recommended
-can have platelet transfusion if low with GCSF cover

Question 65

Dental work for pts on targeted treatments

Answer 65

Usually not immunosuppresed if on targeted treatments per se
Risk of infection significant
Check FBC prior to procedure and consider antibiotic cover
Always check with relevant oncologist if treatment necessary

Question 66

Immunotherapy

Answer 66

Now in use for most cancers in different settings
PDL1 inhibitors - Pembrolizumab
Immune checkpoint inhibitors - Nivolumab
Can cause ‘itis’ of any organ that can be fatal
Can also be effective in controlling cancers and in % of pts provide sustained benefit for many months/ years

Question 67

Bone treatments in cancer

Answer 67

Can be used in adjuvant or palliative setting
Either to < risk of SREs or < symptoms from SREs
Bisphosphonates
RANK ligand inhibitors
Radium 223

Question 68

Metastatic bone disease

Answer 68

> bone resorption is hallmark

• tumour cells release growth factors and cytokines
• osteoclastic resorption stimulated (peptides e.g. TGF-beta released by bone resorption, tumour cell production of factors increased)
• **

Question 69

Pharmacokinetic properties of bisphonsphonates

Answer 69

1/2 life of circulating bisphosphonate is short - around 0.5-2hrs in humans
Approx 50% of circulating bisphosphonate taken up by skeleton
Rate of uptake by bone very fast
Bisphos can remain in bone from 1-10 years in humans
Are liberated from skeleton during osteoclast resorption

Question 70

Side effects of bisphosphonates

Answer 70

Oral therapy

• upper GI inflammation
• diarrhoea and abdo pain

Question 71

Safety profile of IV bisphosphonates

Answer 71

Mild to moderate flu-like symptoms occur after initial infusions
-generally manageable with paracetamol (acetaminophren)
Dose/ infusion rate-dependent effects on renal function
-clinically relevant serum creatinine > are uncommon (<10%) and generally reversible
ONJ is uncommon event that has been reported in pts with cancer receiving complex treatment reigmens, including IV bisphonates (primarily in pts with advanced malignancies and skeletal metastases)

Question 72

ONJ

Answer 72

<1%
Probably related to potency and duration of treatment
Probably more common with IV formulations
About 1% per year of treatment on IV pamidronate/ zoledronic acid
Largely preventable with good dental care

Question 73

What do we know about ONJ and risk management?

Answer 73

Spontaneous reports primarily in pts with advanced cancer and bone mets

• freq. estimates vary but <1%
• etiology and pathogenesis poorly understood

Question 74

Recommendations for minimising ONJ risk

Answer 74

Consider dental exam with appropriate preventative dentistry before BP tx
Avoid invasive dental procedures if possible during tx
For pts requiring dental procedures, no data to suggest whether discontinuation of BPs < risk of ONJ

Question 75

In case of ONJ

Answer 75

Reassess benefit/ risk of continued BP therapy
Discuss options with pts
Manage conservatively
Note that healing of lesions has been reported in most cases

Question 76

General rule for dental treatments of pts on bisphosphonates

Answer 76

Pre-assessment prior to starting BPs or Denosumab mandatory
Prevention vital
While on BPs or Denosumab:
-at onset of symptoms suspend Rx until dental assessment to exclude any suspicion of ONJ
-if not ONJ, restart after 6 weeks of dental work
-if ONJ, suspend or stop indefinitely (discuss risk/ benefit with pt)

Question 77

Denosumab advantages

Answer 77

Given SC, more convenient than IV Zoledronate
No concerns about renal safety, so no renal monitoring required
Fewer acute-phase reactions

Question 78

ONJ zoledronic acid vs denosumab

Answer 78

Similar BUT Denosumab expensive

Question 79

Denosumab side effects

Answer 79

Back pain
Arm and leg pain
High cholesterol
Muscle pain
Bladder infection
Hypocalcaemia - prescribe calcium and vit D