Lecture 3 (hallmarks)

Question 1

Definition of ageing?

Answer 1

Ageing definition: Ageing is the process during which structural and functional changes
accumulate in an organism as a result of the passage of time. The
changes manifest as a decline from the organism’s peak fertility and
physiological functions until death

Question 2

Accumulation of damage:
 Partly inevitable, from the inside
 Preventable, from the outside

Examples?

Answer 2

Inside:
* Metabolism
* DNA replication damage
* Genetic predispositions

Outside:
* Exposure to toxins
* Sunlight
* Alcohol
* Smoking
* Radioactivity

Question 3

What are three criteria for the hallmarks of ageing?

Answer 3

1. Should manifest during normal ageing
2. Its experimental aggravation should accelerate ageing
3. Its experimental amelioration (improvement) should retard the ageing process and thus increase healthy lifespan

Question 4

Mention the 9 hallmarks of ageing

Answer 4

LETS MAC D, G

1. Loss of proteostasis (protein misfolding)
2. Epigenetic alterations
3. Telomere attrition
4. Stem cell exhaustion
5. Mitochondrial dysfunction
6. Altered intracellular communication
7. Cellular senescence
8. Deregulated nutrient sensing
9. Genomic instability

Question 5

What is ‘loss of proteistasis’?

Answer 5

• Stress: protein misfold
• Unfolded proteins should refold/be disposed
• If not -> aggregation

Question 6

What nutrients activate autophagy in mice and nematodes and thereby increase lifespan?

Answer 6

• spermidine
• omega-6-fatty acids

Question 7

Autophagy vs ubiquitin-proteosomal degradation: what are three differences?

Answer 7

Autophagy:
1. LARGER proteins/organelles
2. Protein aggregates
3. Under stress (nutrient depletion)

Ubiquitin-proteosomal degradation:
1. SMALLER proteins
2. Misfolded proteins
3. Always running

Question 8

Protein aggregation is a common pathogenic mechanism in what type of diseases?

Answer 8

ageing-related neurodegenerative diseases:
- Alzheimers
- Parkinson’s
- Huntington’s

Question 9

What do HSP do?

Answer 9

Regulate folding of the protein

Question 10

HSP:
- increased expression of HSP could be 1
- Does not only react to cold, but also other stressors such as 2
- 3 is linked to decreased HSP
- These things also affect HSP: 4

Answer 10

1 carcinogenic
2 cold, UV-light, exercise, alcohol, fasting
3 essential amino acid deprivation
4 pre-and probiotics, dietary restriction

Question 11

What can cause the Werner syndrome and what is it? Symptoms?

Answer 11

increased DNA damage
Werner syndrome = premature ageing syndrome
- Decreased DNA ability to repair itself
- Early hair greying, hair loss, wrinkling
- Early death (around 54 years), often due to cardiovascular disease or cancer

Question 12

What are typical sources of DNA damage (very very broadly)?

Answer 12

Endogenous DNA damage: metabolism/replication
Exogenous damage

Question 13

Explain endogenous induced DNA damage: metabolism

Answer 13

mitochondria induces ROS. Destabilize molecules around them and are unstable themselves. Disbalanced electrons.

Question 14

How to prevent mito damage by ROS?

Answer 14

 to prevent damage by this: anti-oxidants (donate electrons). Anti-oxidant will not lose its own stability after donation.

Question 15

Recall three types of anti-oxidants

Answer 15

SOD: superoxide dismutase: attacks destructive oxygen free radicals like superoxide
Catalase: detoxifies peroxide
GPx: glutathione peroxidase

Question 16

Why does ROS damage mito’s specifically?

Answer 16

ROS damages targets mitochondria quickly, as they are closest by.

Question 17

Explain endogenous induced damage: replication

Answer 17

DNA polymerase is extremely accurate, but can still make mistakes.

Question 18

Explain: exogenous damage (examples)

Answer 18

Formation of free radicals by..
- Inflammation (increased ROS)
- Smoking: breathing in ROS
- Radiation
- UV
- Air pollution

Question 19

Explain the hallmark of ageing: telomere attrition

Answer 19

Telomeres are protective caps at the ends of chromosomes
- shorten per reproduction cycle until they reach replicative senescence

Question 20

What is the Hayflick limit?

Answer 20

Normal human cell cannot replicate anymore after 40-60 cycles and will then reach replicative senescence.

Question 21

How to increase telomere length?

Answer 21

Telomerase. It is however not expressed in many cells.
In human beings, , telomere length is not a better predictor of mortality than chronological age

Question 22

What does lengthening/decreasing telomeres do in mouse models?

Answer 22

lengthening of telomeres increases lifespan, and shortening decreases lifespan

Question 23

In human beings, telomere is as good a predictor for mortality as..

Answer 23

..chronological age

Question 24

Higher paternal age =
Higher maternal age =

Longer/shorter telomeres

Answer 24

paternal: longer
MAternal: shorter

Question 25

What is the evolutionary argumant for the ‘advantage of an old father’ in terms of telomeres?

Answer 25

 Evolutionary hypothesis: descendants of males who reproduced at a later age are likely to find themselves in a harsh environment, allowing later reproduction. Longer telomeres prepares them for this.

Question 26

Altered intracellular communication: name two examples and explain them

Answer 26

• Inflammaging:
  > imflammatory cyto- and chemokines are released
  > due to dysregulated intracellular homeostasis
• Immunosenescence:
  > age-related impairments in innate and adaptive immune system

Question 27

Immunonescence and COVID: older people are more susceptible, because..

Answer 27

Suppressed immune system
Cannot cough well
Permeability in membranes
Increased risk cytokine storms etc

Question 28

When old mice get the blood of young mice, they..

Answer 28

get ‘younger’

Question 29

Explain stem cell exhaustion

Answer 29

Ageing: decline in regenerative capacity.

There is a decrease in stem cells compartments, such as:

Immune cells
Muscle fibers
Bone cells

Question 30

What is cellular senescence? What can cause it?

Answer 30

Senescence = dormant state. Arrest of the cell cycle.

o Caused by:
* Telomere shortening
* DNA damage

senescent cells make up a 2x larger part of total cells in older mice compared to younger

Question 31

Which hallmark of ageing can be used as a defence mechanism in younger people/mice?

Answer 31

Cellular senescence. In young, it promotes tissue homeostasis

Question 32

Supplement stopping cellular senescence regained …. appearance in old mice

Answer 32

youthful

Question 33

Deregulated nutrient sensing: which pathways increase ageing, which pathways decrease ageing?

Answer 33

• Overactive Insulin/IGF and mTOR increase ageing
• Overactive AMPK and SIRT decrease ageing

Question 34

What does caloric restriction do to the nutrient-sensing pathways in mice? What happened to the mice?

Answer 34

Caloric restriction: increase AMPK and decrease mTOR and Insulin/IGF in mice
- Increased lifespan, maintenance of youthful appearance, delays in age-related diseases

Question 35

What nutrient sensing pathways are there? What do they sense?

Answer 35

MAIS

mTOR
AMPK
Insulin/IGF-1
SIRT

mTOR -> senses amino acid availability
AMPK-> senses low energy states (by sensing increased AMP/ATP-ratio)
Insulin/IGF-1-> senses glucose availability
SIRT-> senses low energy states (by sensing increased NAD+-levels)

Question 36

How could calorie-restriction slow down ageing?

Answer 36

By allocating resources for repair.

All resources are divided between vital functions (growth, reproduction) on one hand, anti-ageing repair on the other

Question 37

In which types of cells can you find..
(1)Low/no turnover
(2)Medium, self-duplicating turnover
(3)High, stem cell based turnover

Answer 37

(1) Heart muscle, retina, lung, kidney
(2) Liver, pancreas, skeletal muscle, small vasculature
(3) Gut epithelium, prostate, blood cells, epidermis, epithelium

Question 38

Ageing starts around..

Answer 38

30 years old