Year 12 Biology Module 8 · IQ2 ⏱ ~45 min Practice bank · 3 Short Answer Lesson 10 of 21

Cancer — Cell Cycle, Oncogenes, Tumour Suppressors and Metastasis

Every cancer begins with a normal cell that has lost the molecular brakes on its own division. Understanding cancer means understanding which genes control those brakes, how mutations disable them, and why a single cell out of tens of trillions can eventually kill an organism by producing descendants that invade and colonise other tissues.

Today's hook: Cancer is not one disease but hundreds — yet they all share a single trait: cells that forget how to stop dividing. What breaks the brakes on cell division, and why is metastasis so deadly?

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Worksheets

Practise this lesson

Four printable worksheets that build from the foundations up to exam-style questions — start at whatever level suits you.

Build Foundations & guided practice Apply Application & data response Master Mastery tasks Exam Exam-style questions

Genetic disorders — cancer-predisposing mutations context

Genetic disorders — inherited mutations (e.g. BRCA1/2) raise cancer susceptibility

THINK FIRST · CONCEPTUAL CHALLENGE

Why Can't the Body Just Stop a Cancerous Cell From Dividing?

Your immune system identifies and destroys thousands of abnormal cells every day — cells with viral infections, cells with DNA damage, cells displaying unusual surface proteins. Yet cancer still develops in roughly 1 in 2 Australians over a lifetime.

Cancer is not a failure of the body to notice the cell is abnormal. Cancer is a failure of the cell itself to follow the normal rules of division — and the mutations that cause this failure also often make the cell invisible to immune surveillance.

Before reading on:

Q1: A normal cell divides only when it receives specific growth signals and stops when it touches neighbouring cells. Cancer cells divide without growth signals and do not stop when crowded. What types of genes — accelerators or brakes — might be mutated to cause this behaviour?

Q2: A single mutation in one cell rarely causes cancer. Why do you think multiple mutations are needed? What does this suggest about how many independent control systems the cell cycle has?

Scan these before reading

vocab

CancerA disease of uncontrolled cell division caused by accumulated mutations in genes that regulate the cell cycle.

Proto-oncogeneA normal gene that promotes cell division; when mutated into an oncogene, it causes excessive, uncontrolled cell growth.

Tumour suppressor geneA gene that inhibits cell division or triggers apoptosis (e.g. p53); loss-of-function mutations remove this brake on cell growth.

MetastasisThe spread of cancer cells from the original tumour to distant tissues via the bloodstream or lymphatic system.

ApoptosisProgrammed cell death; a normal process that eliminates damaged or abnormal cells — cancer cells often evade apoptosis.

Benign vs malignantBenign tumours do not invade surrounding tissue or metastasise; malignant tumours do and are classified as cancer.

Learning Intentions

goals

Know

The distinction between proto-oncogenes and oncogenes, and between tumour suppressor genes and their mutant forms
The role of p53 and BRCA1/2 as tumour suppressor genes
The difference between benign and malignant tumours
The stages of metastasis

Understand

Why oncogenes are dominant (one mutant copy sufficient) but tumour suppressors are recessive (both copies must be lost)
Why multiple mutations are required for cancer to develop
How biological, chemical, and physical carcinogens trigger cancer through DNA damage
Why metastasis makes cancer dramatically harder to treat

Can Do

Explain cancer development using the accelerator/brake analogy
Apply the two-hit hypothesis to BRCA1/2 and inherited cancer risk
Classify carcinogens as biological, chemical, or physical with examples
Trace the full pathway from normal cell → primary tumour → metastatic cancer

Core Content

Key Point

Connect this concept back to the broader homeostasis and disease framework you have built across the course. Cancer is not random chaos — it is the predictable result of specific mutations in the genes that regulate the cell cycle.

The Cell Cycle, Checkpoints and What Goes Wrong in Cancer

+5 XP

Cancer is not random chaos — it is the predictable result of specific mutations in specific types of regulatory genes

A normal cell divides only when it receives appropriate signals, only when its DNA is intact, and only when neighbouring cells permit it to do so. Cancer is what happens when the molecular machinery enforcing these three conditions is systematically disabled — not by one mutation, but by the accumulation of multiple mutations over time.

Cancer development showing cell cycle control, oncogenes and tumour suppressors

Stages of tumour progression from normal cell to metastasis

The cell cycle consists of four phases: G1 (cell growth), S (DNA synthesis/replication), G2 (preparation for division), and M (mitosis). Three major checkpoints enforce the rules of normal division:

G1/S checkpoint: Is the cell big enough? Is DNA undamaged? Are growth signals present? p53 is a key enforcer — if DNA damage is detected, p53 halts the cycle and activates repair. If damage is irreparable, p53 triggers apoptosis.
G2/M checkpoint: Is DNA replication complete and error-free? Are there sufficient resources for mitosis?
Spindle assembly checkpoint (M phase): Are all chromosomes correctly attached to the spindle before separation?

Cancer develops when mutations accumulate in the genes that govern these checkpoints. Typically, 4–8 driver mutations are required for a fully malignant cancer to develop from a normal cell — this explains why cancer predominantly affects older people (it takes decades for this many mutations to accumulate in one cell lineage) and why cancer risk increases with any exposure that accelerates mutation rate (carcinogens, radiation).

Analogy

Think of a car with both an accelerator (proto-oncogenes — drive division) and brakes (tumour suppressors — stop division). Normal cell division requires the accelerator to be pressed AND the brakes released. Cancer requires the accelerator to be stuck ON (oncogene mutation) OR the brakes to be cut (tumour suppressor loss) — or, more commonly, both. Multiple independent safety systems must all fail for a car to crash uncontrollably — similarly, multiple mutations must accumulate for a cell to become truly malignant.

What to write in your book

Cell cycle: G1 → S → G2 → M, with checkpoints at G1/S (p53), G2/M, and spindle assembly.
p53 detects DNA damage → halts cycle for repair, or triggers apoptosis if irreparable.
Cancer needs 4–8 driver mutations accumulating in one cell lineage over time.
Accelerator (oncogene stuck ON) + brakes cut (tumour suppressor lost) = uncontrolled division.

A fully malignant cancer typically requires 4–8 _____ mutations to accumulate in a single cell lineage.

Interactive · Cell Cycle Checkpoint Simulator

Oncogenes and Tumour Suppressor Genes — Two Ways to Lose Control

+5 XP

Oncogenes = dominant gain-of-function · Tumour suppressors = recessive loss-of-function · Both must accumulate for malignancy

There are two fundamentally different ways that mutations can drive a cell toward cancer — and they follow opposite genetic logic. Oncogenes act dominantly (one mutant copy is enough); tumour suppressor loss acts recessively (both copies must be inactivated). Understanding this distinction explains why inherited cancer syndromes are often linked to tumour suppressor genes rather than oncogenes.

Proto-oncogenes → Oncogenes (Accelerator stuck ON)

Normal proto-oncogene: promotes cell division in response to growth signals — turned ON only when needed
Oncogene mutation: point mutation, gene amplification, or chromosomal translocation causes constitutive (always-on) activity
Effect: cell divides continuously without growth signals
Genetic: dominant — one mutant allele is sufficient because the overactive protein is produced regardless of the normal copy
Examples: RAS (mutated in 30% of all cancers — stuck in active GTP-bound state), HER2 (amplified in 20% of breast cancers), MYC (amplified transcription factor)
Analogy: accelerator pedal jammed down — car accelerates regardless of driver intention

Tumour Suppressor Genes (Brake cut)

Normal function: inhibit cell cycle progression, promote apoptosis, or repair DNA — turn OFF division when needed
Mutation: loss-of-function mutation inactivates the protein; second mutation ('second hit') inactivates the remaining allele
Effect: cells cannot stop dividing, cannot repair damage, cannot undergo apoptosis
Genetic: recessive — both alleles must be inactivated (two-hit hypothesis)
Examples: TP53 (p53 — mutated in ~50% of cancers), RB1 (retinoblastoma), BRCA1/2 (breast and ovarian cancer), APC (colorectal cancer), CDKN2A (p16/melanoma)
Analogy: brake cable cut — car cannot stop

The two-hit hypothesis and inherited cancer syndromes

Alfred Knudson's two-hit hypothesis explains why some cancers run in families. In sporadic (non-inherited) cancer, both alleles of a tumour suppressor must be independently mutated in the same cell — a relatively rare double event. In inherited cancer syndromes (e.g. hereditary breast cancer from BRCA1 mutation), every cell in the body already carries one non-functional allele inherited from a parent. Only one additional somatic mutation ('second hit') is needed in any cell to lose both copies — dramatically increasing lifetime cancer risk.

This explains why people with inherited BRCA1 mutations have ~70% lifetime risk of breast cancer (vs ~12% population risk) — not because the mutation causes cancer directly, but because they start with one brake already cut. One additional mutation in any breast cell is all that is needed to lose tumour suppressor function entirely.

Common Error

Students write "oncogenes cause cancer by producing too much of a protein." More precisely: proto-oncogene mutations produce a protein that is constitutively active (always switched on regardless of normal growth signals). The problem is not quantity but regulation — a RAS protein stuck in its active form drives division continuously whether growth factors are present or not. The protein is not necessarily overproduced; it is simply unable to switch off.

L07 Link

Connect to L07 (Huntington's disease): Huntington's is a gain-of-function dominant mutation — one mutant allele produces a toxic protein. Oncogenes are also gain-of-function dominant mutations — one mutant allele produces an overactive protein that drives division. Both contrast with recessive loss-of-function conditions (CF, tumour suppressor loss) where both alleles must be mutated before the phenotype appears.

What to write in your book

Proto-oncogene → oncogene: gain-of-function, dominant (1 copy). E.g. RAS, HER2, MYC stuck ON.
Tumour suppressor: loss-of-function, recessive (both copies lost). E.g. p53, RB1, BRCA1/2, APC, CDKN2A.
Two-hit hypothesis: inherited 1st hit (all cells) + somatic 2nd hit → cancer susceptibility.
Oncogene problem = unregulated activity (always-on), not overproduction.

Why is one mutant copy of an oncogene sufficient to drive division, but a tumour suppressor needs both copies lost?

Interactive · Cancer Development Stepper

Carcinogens — Biological, Chemical and Physical Agents That Drive Mutation

+5 XP

Every carcinogen causes cancer by the same final pathway — accumulation of mutations in cell cycle regulatory genes

Carcinogens are agents that increase cancer risk by increasing the rate of DNA mutation. They act through different mechanisms but converge on the same endpoint: mutations that activate oncogenes or inactivate tumour suppressors. The three categories — biological, chemical, and physical — each have characteristic mechanisms and associated cancers.

Category	Examples	Mechanism of DNA damage	Associated cancers
Chemical	PAHs in tobacco smoke, nitrosamines, benzene, aflatoxin B1 (mould toxin)	Reactive metabolites form covalent adducts with DNA bases → G→T transversion or other mutations during replication	Lung (tobacco), bladder (aniline dyes), liver (aflatoxin), leukaemia (benzene)
Physical	UV radiation (UVB), ionising radiation (X-rays, gamma rays, radon), asbestos fibres	UV: thymine dimers → C→T mutations; Ionising radiation: double-strand DNA breaks; Asbestos: ROS from frustrated macrophages → oxidative DNA damage	Melanoma, BCC, SCC (UV); leukaemia, thyroid cancer (ionising radiation); mesothelioma (asbestos)
Biological	Human papillomavirus (HPV strains 16/18), Hepatitis B and C viruses, Helicobacter pylori, Epstein-Barr virus	HPV: viral E6 protein binds and degrades p53; E7 protein inactivates RB1 tumour suppressor. H. pylori: chronic inflammation → ROS → DNA damage in gastric epithelium	Cervical cancer (HPV), liver cancer (Hep B/C), gastric cancer (H. pylori), Burkitt's lymphoma (EBV)

HPV and cervical cancer — a biological carcinogen in detail

HPV strains 16 and 18 are responsible for approximately 70% of cervical cancers. The virus integrates its DNA into the host cell genome and produces two oncoproteins: E6 (which binds p53 and targets it for degradation) and E7 (which binds and inactivates the RB1 tumour suppressor protein). By simultaneously disabling p53 and RB1, HPV infection effectively removes two of the most critical brakes on cell cycle progression. Cells cannot respond to DNA damage (p53 gone) and cannot halt at the G1/S checkpoint (RB1 gone) — accumulating further mutations and progressing toward cervical cancer.

This is why HPV vaccination (Gardasil — targeting HPV 6, 11, 16, 18) is the primary prevention strategy for cervical cancer in Australia. Australia's national HPV vaccination program, introduced in 2007 and extended to boys in 2013, has produced dramatic reductions in HPV-related precancerous lesions and is on track to effectively eliminate cervical cancer as a public health problem in Australia.

Australian Context

Australia has the most comprehensive HPV vaccination program in the world and is projected to be the first country to eliminate cervical cancer (defined as fewer than 4 cases per 100,000 women per year) — a milestone expected around 2028. This is entirely the result of three combined public health interventions: HPV vaccination (targeting the biological carcinogen), cervical screening (catching precancerous changes early), and accessible treatment. It is one of the clearest examples in medicine of understanding the mechanism of a cancer's cause directly enabling its elimination.

What to write in your book

Chemical: PAHs, nitrosamines → DNA adducts → G→T mutation.
Physical: UV → thymine dimers → C→T; ionising radiation → strand breaks; asbestos → ROS.
Biological: HPV → E6 degrades p53, E7 inactivates RB1; H. pylori → chronic inflammation.
All carcinogens converge on one endpoint: mutations in cell-cycle regulatory genes.

How does HPV act as a biological carcinogen?

Benign vs Malignant Tumours — and the Process of Metastasis

+5 XP

The difference between a nuisance and a killer — and how cancer cells leave their origin and colonise other organs

Not all tumours are cancer. A benign tumour is a localised mass of abnormally dividing cells that respects tissue boundaries and does not spread. A malignant tumour invades surrounding tissue and, once cells enter the bloodstream or lymph, can establish secondary tumours throughout the body — a process called metastasis. It is metastasis, not the primary tumour, that kills most cancer patients.

Feature	Benign Tumour	Malignant Tumour (Cancer)
Growth pattern	Slow, well-defined, often encapsulated	Rapid, irregular, infiltrating
Tissue invasion	No — remains localised	Yes — invades surrounding tissue
Metastasis	No — does not spread to distant sites	Yes — can spread via blood or lymph
Cell appearance	Similar to normal cells (differentiated)	Abnormal, poorly differentiated (anaplastic)
Treatment	Surgical removal usually curative	May require surgery + chemotherapy + radiation; metastatic disease rarely curable
Example	Uterine fibroid, lipoma, most skin moles	Melanoma, lung cancer, breast cancer, leukaemia

The stages of metastasis

Local invasion: Cancer cells in the primary tumour develop mutations in cell adhesion molecules (e.g. E-cadherin) and proteases (e.g. matrix metalloproteinases) that allow them to break away from the tumour mass and digest the surrounding extracellular matrix.

Intravasation: Cells penetrate the walls of nearby blood vessels or lymphatic vessels and enter the circulation — a process requiring further mutations enabling survival in a non-adherent state (normally, cells that lose contact with surfaces undergo apoptosis — 'anoikis').

Circulation and survival: Most cancer cells in circulation are destroyed by shear forces or immune cells. A small fraction survive — often by forming clusters with platelets that shield them from immune attack.

Extravasation: Surviving cells arrest in small capillaries of distant organs, then squeeze through the vessel wall into surrounding tissue.

Secondary tumour formation: Cells that successfully colonise a new tissue proliferate, inducing new blood vessel formation (angiogenesis) to supply the growing secondary tumour. Not all cancer cells can complete all five steps — metastasis is highly inefficient, but even rare successful events are life-threatening.

Common metastatic destinations reflect patterns of blood flow and lymphatic drainage: bowel cancer commonly metastasises to the liver (via portal circulation); lung cancer to the brain and adrenal glands; breast cancer to bone, liver, lung, and brain. The clinical consequence of metastasis is that treatment must address multiple sites simultaneously rather than a single localised tumour.

Common Error

Students write "cancer spreads because it grows too large." Metastasis is not a passive overflow — it is an active multi-step process requiring specific additional mutations (in cell adhesion molecules, proteases, anoikis resistance). Cells must acquire the molecular machinery to detach, survive in circulation, extravasate, and proliferate in a foreign tissue environment. A large primary tumour does not automatically metastasise — it requires these specific additional mutations.

What to write in your book

Benign: localised, encapsulated, no invasion, no metastasis. Malignant: invasive, can metastasise.
Metastasis (5 steps): local invasion → intravasation → circulation/survival → extravasation → secondary tumour + angiogenesis.
Metastasis needs specific extra mutations (E-cadherin loss, proteases, anoikis resistance) — not just large size.
Metastasis, not the primary tumour, kills most cancer patients.

Metastasis happens simply because a tumour grows too large and overflows into surrounding tissue.

Oncogenes are mutated versions of proto-oncogenes that promote uncontrolled cell division.

Metastasis occurs when cancer cells remain localised at the primary tumour site and do not spread.

Activity 1

ApplyBand 4

Oncogene or Tumour Suppressor? Dominant or Recessive?

For each scenario or gene description, classify it as an oncogene mutation or tumour suppressor mutation, state whether it acts dominantly or recessively, and explain what the mutation does to cell cycle control.

A mutation in the RAS gene causes the RAS protein to remain permanently bound to GTP (its active form) regardless of whether growth factor receptors are stimulated. One allele is mutated; the other is normal.
A woman inherits one non-functional BRCA1 allele from her mother. At age 42, a somatic mutation inactivates her remaining functional BRCA1 allele in a breast epithelial cell.
HPV E6 protein binds to p53 and targets it for ubiquitin-mediated degradation. HPV E7 protein binds to RB1 and prevents it from blocking S-phase entry.
Retinoblastoma is a childhood eye cancer. Children with inherited retinoblastoma have one non-functional RB1 allele in every cell from birth and develop tumours in multiple spots in both eyes. Children with non-inherited retinoblastoma develop a single tumour in one eye, usually later in childhood. Explain why using the two-hit hypothesis.

Activity 2

AnalyseBand 5

Applying Cancer Concepts to Clinical Scenarios

Read each scenario and answer all parts using precise biological terminology.

A 58-year-old man is diagnosed with metastatic bowel cancer. His oncologist explains that surgery to remove the primary bowel tumour was successful, but CT scans show secondary tumours in the liver and lungs. The patient asks: "If they removed the original tumour, why am I not cured?" Explain the answer using your knowledge of metastasis, including what would have been required at the molecular level for cells to have established the liver and lung metastases.
A researcher compares two groups: (a) people with a BRCA1 inherited mutation; (b) people without. Group (a) has a ~70% lifetime breast cancer risk vs ~12% for group (b). A cancer biologist argues that BRCA1 mutations do not cause cancer directly — rather, they dramatically increase cancer susceptibility. Explain this distinction using the two-hit hypothesis and what BRCA1 normally does.

Why Australia Has the World's Highest Skin Cancer Rate — and What Is Being Done About It

Australia has the highest incidence of skin cancer in the world — approximately 2 in 3 Australians will develop some form of skin cancer by age 70. Each year, Australia records approximately 16,000 new melanoma diagnoses and over 800,000 diagnoses of non-melanoma skin cancer (BCC and SCC combined). The primary cause is UV radiation from sunlight, which causes thymine dimers in keratinocyte and melanocyte DNA — particularly UVB-induced C→T mutations in tumour suppressor genes including CDKN2A (encoding p16, which regulates the G1/S checkpoint) and TP53.

Melanoma illustrates the multi-hit model perfectly. The sequence of mutations in melanoma progression is well characterised: an activating mutation in BRAF (V600E — an oncogene mutation present in ~50% of melanomas) is typically the first driver mutation, often caused by intermittent intense UV exposure. Additional mutations in CDKN2A (tumour suppressor), PTEN (tumour suppressor), and other genes progressively disable more checkpoints, eventually producing a cell capable of invasion and metastasis.

Treatment has been revolutionised by targeted therapy: BRAF inhibitors (vemurafenib, dabrafenib) specifically inhibit the mutant BRAF V600E protein, producing dramatic initial responses in metastatic melanoma. Immune checkpoint inhibitors (pembrolizumab, nivolumab) block the PD-1 pathway that metastatic melanoma cells use to evade immune attack, producing durable responses in a subset of patients. Five-year survival for metastatic melanoma improved from under 10% in 2010 to approximately 50% in 2023 — driven entirely by understanding the molecular mechanisms of oncogene activation and immune evasion.

PRIORITY MISCONCEPTIONS — CANCER BIOLOGY

Priority Misconceptions — Cancer Biology

✗ "Cancer is caused by a single mutation."

✓ Cancer requires accumulation of multiple driver mutations — typically 4–8 — in a single cell lineage over time. Each mutation provides a growth advantage; selection enriches for cells that have acquired the most mutations. This is why cancer takes years to decades to develop and primarily affects older people.

✗ "Oncogenes produce too much protein."

✓ Oncogene mutations typically produce a protein that is constitutively active (permanently switched on), not necessarily overproduced. A single amino acid change in RAS can lock it in the active GTP-bound state regardless of growth signals. The issue is unregulated activity, not quantity.

✗ "Benign tumours are harmless."

✓ Benign tumours are generally less dangerous than malignant tumours, but they are not harmless. A benign tumour in the brain can compress vital structures and be life-threatening. Some benign tumours produce hormones that disrupt physiology. And benign tumours can transition to malignancy over time if additional mutations accumulate.

✗ "Metastasis happens because the tumour grows too large."

✓ Metastasis is an active multi-step process requiring specific additional mutations — in cell adhesion molecules, extracellular matrix proteases, anoikis resistance pathways, and angiogenesis factors. Large size alone does not cause metastasis. A large benign tumour never metastasises.

✗ "Tumour suppressor genes suppress tumours by killing cancer cells."

✓ Tumour suppressor genes do not detect and kill cancer cells. They enforce normal cell cycle regulation in every dividing cell — halting the cycle when DNA is damaged (p53), preventing entry into S phase before conditions are right (RB1), or repairing DNA breaks (BRCA1/2). When inactivated, the brakes fail and division becomes uncontrolled. They are regulatory genes in normal cells, not cancer-killing genes.

Oncogenes vs Tumour Suppressors

Proto-oncogene → oncogene: gain-of-function, dominant (1 copy)
RAS, HER2, MYC — stuck ON, drive division without signals
Tumour suppressor: loss-of-function, recessive (2 copies must be lost)
p53, RB1, BRCA1/2, APC, CDKN2A; two-hit hypothesis

Carcinogens (3 types)

Chemical: PAHs, nitrosamines → DNA adducts → G→T mutation
Physical: UV → thymine dimers → C→T; ionising radiation → strand breaks
Biological: HPV → E6 degrades p53, E7 inactivates RB1; H. pylori → ROS

Benign vs Malignant

Benign: localised, encapsulated, no invasion, no metastasis
Malignant: invasive, can metastasise, poorly differentiated
Metastasis = spread via blood/lymph to secondary sites

Metastasis Steps

1. Local invasion (lose E-cadherin, gain proteases)
2. Intravasation (enter blood/lymph vessel)
3. Survive in circulation
4. Extravasation (exit vessel)
5. Secondary tumour + angiogenesis

Interactive Tool — Homeostasis Feedback Loops Open fullscreen ↗

The Homeostasis tool shows negative feedback. When temperature rises above set point, the effector response that brings it back is called…

Multiple Choice

+5 XP

A fresh set drawn from this lesson's question bank — feedback shown immediately. +5 XP per correct · +25 XP all correct

Pick your answer, then rate your confidence — that tells the system what to drill next.

Short Answer — 15 marks

+5 XP

ApplyBand 4(4 marks) 1. Explain the role of p53 in normal cell cycle regulation and describe what happens when both copies of the TP53 gene are mutated in a cell. Include: what p53 normally detects, what it does in response, and why loss of both copies contributes to cancer development.

AnalyseBand 4–5(5 marks) 2. Compare the mechanisms by which a chemical carcinogen (tobacco smoke PAHs) and a biological carcinogen (HPV) cause cancer. For each, describe (a) how they interact with DNA or cell cycle regulatory proteins; (b) which specific genes or proteins are affected; (c) why their combined effect (in a person who both smokes and has HPV) would be greater than either alone.

EvaluateBand 5–6(6 marks) 3. Using melanoma as a case study, explain how cancer develops through the accumulation of multiple mutations. Describe the specific mutations involved in melanoma progression, explain why melanoma illustrates the multi-hit model of cancer, and evaluate why early detection is critical given what you know about the metastatic process.

Show all answers

Multiple choice

MC answers and full explanations are shown inline as you complete each question. Use the retry button to attempt a fresh set from the lesson bank.

Activity 1 — Classify Oncogene or Tumour Suppressor

1. RAS mutation — oncogene, dominant. RAS is a proto-oncogene encoding a GTPase that normally cycles between active (GTP-bound) and inactive (GDP-bound) states, active only transiently when growth factors stimulate it. The mutation locks RAS in its GTP-bound active state (the GTPase activity that hydrolyses GTP→GDP is abolished). One mutant allele is sufficient (dominant) because the permanently active RAS signals for division continuously regardless of the other allele. The cell receives a constant growth signal even without growth factors. Gain-of-function, dominant.

2. BRCA1 — tumour suppressor, two-hit. BRCA1 encodes a protein involved in DNA double-strand break repair (homologous recombination). The inherited non-functional allele is the first hit (present in every cell since birth); the somatic mutation in the breast cell is the second hit, inactivating the remaining allele. With no functional BRCA1, double-strand breaks cannot be repaired accurately → mutations accumulate → cancer. Loss-of-function, recessive (both alleles must be inactivated).

3. HPV — biological carcinogen, dual tumour suppressor inactivation. E6 binds p53 and recruits a ubiquitin ligase that marks p53 for proteasomal degradation — the cell loses the G1/S checkpoint and apoptosis response. E7 binds and inactivates RB1, releasing the transcription factor E2F so cells continuously enter S phase. HPV is biological because it is a living organism promoting cancer via its proteins rather than direct chemical/physical DNA damage.

4. Retinoblastoma — two-hit hypothesis. Inherited form: every cell already has one inactivated RB1 allele (first hit inherited); cancer develops once any retinal cell acquires a second somatic mutation. With millions of retinal cells each needing only one more mutation, multiple bilateral tumours arise early. Sporadic form: both RB1 alleles start functional; cancer requires two independent somatic mutations in the same cell — a much rarer double event → single, unilateral, later-onset tumour.

Activity 2 — Clinical Scenarios

1. Metastatic bowel cancer — why surgery alone is not curative. Before the primary tumour was removed, cells had already completed the early steps of metastasis — acquiring mutations enabling detachment (E-cadherin loss, matrix metalloproteinase activity), intravasation, survival in circulation, and extravasation into liver and lung tissue. These cells were circulating or already established at secondary sites before surgery. Removing the primary tumour does not eliminate cells established elsewhere. Molecular requirements: (1) cell adhesion molecule loss (detachment); (2) ECM proteases (invasion); (3) anoikis resistance (survival without attachment); (4) immune evasion in circulation; (5) angiogenic factors (VEGF) for secondary tumour blood supply. Metastatic cancer needs systemic treatment (chemotherapy, immunotherapy, targeted therapy) addressing multiple sites, not just localised surgery.

2. BRCA1 — cause vs susceptibility. BRCA1 normally repairs DNA double-strand breaks via homologous recombination, maintaining genome stability. When lost, breaks are repaired by error-prone pathways → genomic instability → accelerated mutation accumulation. The inherited mutation does not directly cause cancer: every cell has one non-functional allele, but cancer only develops when a second somatic mutation inactivates the remaining allele in a breast/ovarian cell — most cells never acquire this. Risk rises dramatically because only one further hit is needed (instead of two independent hits in the same cell). Cause = necessary and sufficient; susceptibility = greatly increased probability but not certainty. BRCA1 mutation lowers the mutational barrier to tumour suppressor loss without being sufficient alone.

Short Answer Model Answers

SA1 (4 marks): Normal p53 function: p53 (encoded by TP53) is a tumour suppressor transcription factor — the cell's primary guardian against DNA damage. It detects DNA damage signals and responds by (1) halting the cell cycle at the G1/S checkpoint via p21 (which inhibits cyclin-dependent kinases) to allow repair before replication, or (2) if damage is irreparable, activating pro-apoptotic genes (e.g. BAX) to trigger programmed cell death [2]. When both TP53 alleles are mutated: the cell loses the ability to detect DNA damage and halt the cycle; cells with damaged DNA continue dividing, replicating damaged DNA and passing mutations to daughter cells; further mutations accumulate in other regulatory genes, and without p53-mediated apoptosis heavily mutated cells survive — progressively driving the cell toward malignancy [2].

SA2 (5 marks): PAHs (tobacco): (a) metabolically activated to reactive diol epoxides that form covalent adducts with guanine in DNA. (b) cause G→T transversions, mutating TP53 (e.g. codons 157, 248, 273) → non-functional p53 [1]. HPV: (a) E6 binds p53 and recruits E6AP ubiquitin ligase, degrading p53 post-translationally; E7 binds RB1, releasing E2F for continuous S-phase entry. (b) p53 and RB1 inactivated simultaneously [1.5]. Combined effect: p53 is disabled by BOTH a direct TP53 mutation (PAH) AND protein degradation (HPV E6) — robust, near-total loss. With p53 gone and RB1 inactivated, PAH-induced DNA damage cannot be detected, repaired, or eliminated by apoptosis, while E7-released E2F drives cells into DNA synthesis copying unrepaired damage — a multiplicative increase in mutation accumulation and cancer risk [1.5]. p53 is the critical shared node whose loss enables both insults to produce maximal risk [1].

SA3 (6 marks): Mutations: UVB → thymine dimers → C→T mutations. The earliest driver is usually BRAF V600E (oncogene, ~50% of melanomas) — a constitutively active kinase signalling continuous proliferation. This alone is insufficient — benign moles often carry BRAF V600E. Additional mutations accumulate: CDKN2A deletion (loses p16, the G1/S brake), PTEN loss (pro-survival PI3K signalling), TP53 mutation (loses apoptosis), plus adhesion/protease mutations for invasion [2]. Why multi-hit: each mutation gives a growth advantage but is individually insufficient — only accumulation of 4–8+ driver mutations across multiple checkpoints produces a malignant, invasive, metastatic cell. This explains why melanoma takes years to develop despite lifelong UV exposure and predominates in older individuals [2]. Why early detection is critical: before metastasis, melanoma is confined to the epidermis/superficial dermis and surgical excision with clear margins is curative (stage I ~98% 5-year survival). Once cells acquire the metastatic mutation set (detachment, invasion, intravasation, circulation survival, extravasation, secondary growth) and establish secondary tumours, treatment must address multiple sites; stage IV 5-year survival remains ~30–50% even with immunotherapy. Early detection intercepts the disease while it is still a localised, surgically addressable problem [2].

Test yourself against the clock

boss

Five timed questions on the cell cycle, oncogenes, tumour suppressors and metastasis. Beat the boss to bank a tier — gold (perfect + fast), silver (80%+), or bronze (cleared).

⚔ Enter the arena

BOSS BATTLE · CANCER SHOWDOWN

Defeat the Boss — Cancer Showdown!

Defeat the boss using your knowledge of the cell cycle, oncogenes, tumour suppressors and metastasis. Pool: lessons 1–10.

How did your thinking change?

Return to your Think First responses at the start of this lesson.

Q1 — accelerator or brake genes: Cancer involves both — oncogenes are the mutated accelerators (stuck ON), tumour suppressors are the cut brakes (both copies lost). Can you now name one specific gene in each category and describe its mechanism?
Q2 — why multiple mutations are needed: Multiple cell cycle checkpoints (G1/S, G2/M, spindle) are enforced by different proteins; each must be individually disabled. Cells also acquire further mutations enabling metastasis (E-cadherin loss, proteases).
Write the cancer development sequence from memory: normal cell → first mutation → … → metastatic cancer, naming at least three specific genes mutated along the way.

I have completed this lesson

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