Cancer 3

Question 1

benign tumour characteristics

Answer 1

Generally self contained and localised

well defined periphery

slow growing

expands outwards from central mass

Question 2

Malignant tumour characteristics

Answer 2

Not self contained or localised

presence of invading cells at periphery

able to spread

have capacity for rapid growth

Question 3

metastic tumors

Answer 3

Hard to treat surgically

impair organ function

chemo resistant

Question 4

How do cancer metastases

Answer 4

Lymphatic system is a common pathway for the initial spread of solid tumour

pattern of lymph nodes involvement follows natural route of drainage

can also spread through the body wall into abdominal and chest cavities

involvement of lining of cavities results in inflammatory response, accumulation of fluid and inflammatory cells

Question 5

Metastasis: Cell-cell adhesion

Answer 5

E-cadherin plays a critical role and functions as a tumour suppressor

Reduced expression of E-cadherin increases invasiveness of Tumour cells

E-cadherin loss enables disaggregation of cancer cells

Loss of E-cadherin expression correlates with poor prognosis

Question 6

Metastasis: Invasion into surrounding tissue

Answer 6

Malignant tumour secrete proteases that target the basement membrane

Facilitates local tissue penetration and entry into circulatory system

Question 7

metastasis: Angiogenesis

Answer 7

Formation of new blood vessels from pre-existing ones

Blood supply needed for tumour growth

Facilitates tumour metastasis

Question 8

Angiogenesis

Answer 8

1. Release of angiogenic factors and proteases by tumour cells
2. Degradation of basement membrane and proliferation of endothelial cells
3. Migration of endothelial cells in direction of tumour
4. Formation of tubular structures which anastomose with existing vasculature

Question 9

sustained proliferative signaling

Answer 9

1. Normal tissue carefully controls the production and release of growth promoting signals that instruct entry/progression through the cycle
2. Cancer cells dysregulate these signals to become masters of their own destiny
3. Cancer cells acquire capability for sustained proliferation in many ways
4. They produce growth factor ligands themselves and respond via expression of cognate receptors
5. They send signals to stimulate normal cells within the tumour associated stroma -> which then deliver various growth factors to the cancer cells
6. Receptor signalling can also be dysregulated by elevating the number of protein receptors on the cancer cell surface -> rendering cells hype responsive to limiting amounts of growth factor
7. Growth factor independent can also be derived from constitute activation of components of signalling pathway operating downstream of receptors -> no need for ligand mediated activation

Question 10

Disruptions of Negative Feedback mechanisms

Answer 10

1. Negative Feedback loops normally dampen down activity and regulate proliferative signals
2. Defects in feedback can enhance proliferative signals -> RAS mutation
3. Oncogenic effects of RAS are not seen in the hyperactivation of signalling, instead it affects RAS GTPASE activity which normally ensures the active signal transmission is transitory

Question 11

EGFR inhbitors

Answer 11

When EGFR is active it triggers a cascade of signalling events that promotes proliferation

Sustained proliferative signalling occurs when aberrantly activated EGFR continuously stimulates cell proliferation (even in absence of GF)

EGFR inhibitors disrupts sustained proliferative signalling, slowing down cell division and potentially reducing tumour growth

Small molecule tyrosine kinase inhibitors (gefitinib) block the ATP binding site of the EGFR tyrosine kinase domain, inhibiting enzymatic activity and downstream signalling

Question 12

Epidermal growth factor receptor

Answer 12

Inhibitors target the hallmark sustained proliferative signalling

EFGR is overexpressed in cancer cells -> uncontrolled proliferation and tumour development

the 4-Aniloquinazoline is important pharmacophore for EFGR tyrosine kinase inhibition

SAR shows electron groups are needed at the 6,7 positions and a small lipophilic group at 3’

Gefitnib

Question 13

Pharmacophore

Answer 13

The portion of a molecule that determines the biological effects of a drug

Question 14

Enediynes

Answer 14

Calicheamicin

1. Targets DNA by binding to the major groove
2. Polysaccharide chain containing aromatic ring and iodine atom binds to TCCT. TCTC, TTT regions
3. Cellular activation produces a nucleophilic S
4. Formation of new S ring causes the enediyne ring to shrink
5. Cycloaromatization generates reactive benzene diradical
6. Diradical cleaves both strands of DNA = CELL DEATH

Question 15

DNA Repair - PARP

Answer 15

1. Many enzymes repair DNA including PARP and BRCA1/2
2. Ovarian and breast cancers are often deficient in BRCA1/2 which are the tumour supressors
3. If PARP is inhibited in the cells, DNA repair is not possible and the cancer cells die
4. PARP uses NAD+, nicotinamide region binds to the active site
5. The adenine dinucleotide portion forms protein bound polymer - cellular signals for repair