human microbiome

Question 1

The microbes we are exposed to may…

Answer 1

• fail to colonize (then die)
• become short-term residents (live for short time, body prevent it from being long-term)
• become long-term residents (shape our life history)

Question 2

Do we have microbes in utero?

Answer 2

No! However after birth the residence of TRILLIONS of microbes is normal

Question 3

Microbial metagenome is much larger than
human genome?

Answer 3

True

Question 4

The presence of microbes in tissues is…

Answer 4

NOT normal.

Question 5

Tight gut barrier

Answer 5

mucin layer over tightly joined epithelial cells
* excludes microbes from the underlying tissues of our body
* mucin layer - lubricating barrier

Question 6

Parasitism

Answer 6

Partner 1 benefits - increased growth output for parasite/pathogen
Partner 2 harmed - reduced growth output for ‘host’
Host better without parasite

Question 7

Commensalism

Answer 7

Partner 1 benefits - increased growth output for commensal
Partner 2 neutral - no growth change for host
Host same with/without commensal

Question 8

Mutualism

Answer 8

Partner 1 benefits - increased growth output for mutualist
Partner 2 benefits - improved growth for host
Host needs microbe for optimal fitness

Question 9

In the absence of Microbes…

Answer 9

• Gut functions are different – reduced digestive capacity
• Immune functions are different – essentially no adaptive immunity
• Metabolic regulation is different – altered neuro-endocrine signalling pathways
• Cognitive functions & mood are different – underdeveloped ENS

Question 10

The gut microbiome develops…

Answer 10

at approximately the same time postnatal development finishes.

Question 11

factors in normal microbiome development

Answer 11

• microbe exposure (birth canal, skin)
• infant diet (breast milk)
• immune sytem development

Question 12

disturbances to microbiome development

Answer 12

cause deviations from microbial homeostasis
* antibiotics (at birth or during infancy)
* microbe exposure (C-section, infection)
* diet (breast/formula; weaning pattern)

Question 13

deviance from immune homeostasis

Answer 13

cause immune-mediated diseases in later childhood
* asthma
* atopic disease
* T1D
* Crohn’s & Colitis

Question 14

gut microbiome

Answer 14

the stable resident microbial community of a defined habitat (gut) in an individual person.

Question 15

Bacterial numbers in stomach & small/large intestine

Answer 15

• Stomach - continually exposed to microbes, but very few actually grow there.
• Distal Small intestine (mainly ileum) - site of stable occupation by microbes. Lower numbers than colon.
• Large intestine (colon) - has distinct conditions for microbial growth and far higher microbe cell density than ileum.

Question 16

Over 98% of the total microbial cells in our gut are Bacteria .

Answer 16

true!

Question 17

Bacteroidetes (10-90% of all cells)

Answer 17

• Tens to hundred of Bacteroidetes species
• Vast majority show fermentative metabolism
• Diverse growth substrates commonly polysaccharides

Question 18

Firmicutes (10-90% of all cells)

Answer 18

• Hundreds of Firmicutes species.
• Vast majority show fermentative metabolism.
• Diverse growth substrates commonly polysaccharides

Question 19

Proteobacteria (1–5% of all cells)

Answer 19

• Tens of Proteobacteria species.
• Respiratory and fermentative metabolism
• Growth substrates rarely polysaccharides, commonly small molecules (sugars, amino acids and fatty acids).

Question 20

Methanobrevibacter (1-2%)

Answer 20

• One or two species.
• One type of metabolism (methanogenesis).
• Growth on one-carbon compounds and hydrogen.

Question 21

The presence of microbes changes our food requirements

Answer 21

• Quantity - Less food is eaten by animals that are colonised.
• Quality - The diet fed to germ-free animals requires vitamin supplementation and a simple carbohydrate profile.

Question 22

Small intestine

Answer 22

Tank for further hydrolysis.
* Cells of accessory organs secrete enzymes and bile.
* Intestinal epithelial cells absorb nutrients.

Question 23

Stomach

Answer 23

• An acid hydrolysis tank.
• Gastric cells secrete acid and enzymes

Question 24

Material passing to the colon includes…

Answer 24

Indigestible - chemically inaccessible to human enzymes (e.g. fibre)
Inaccessible – particle structure prevents enzyme access (e.g. intact corn kernel)
Excess – exceeded digestion/absorption capacity of small intestine.

Question 25

Plant cell walls…

Answer 25

are digestion resistant (e.g. cellulose, xylan).
* Starch must be released to be degraded by amylases.
* Other storage polysaccharides of plants are typically also digestion-resistant (e.g. inulin, arabinogalactans).

Question 26

Ruminants Vs. Humans

Answer 26

Ruminants: up to 70% of calories via rumen microbes
Humans: 10 – 15% of calories via colon microbes

Question 27

Plant specialists

Answer 27

have complex digestive tract with a specialised fermentation chamber

Question 28

meat-specialists

Answer 28

simple digestive tract

Question 29

Short Chain Fatty Acids

Answer 29

SCFA are fermentation metabolites that are valuable energy sources for animals

Question 30

Most common metabolism is Fermentation Simple Carbs to…

Answer 30

• Acetate, CO2, H2
• Propionate, CO2, H2
• Butyrate, CO2, H2
• mixed SCFA, CO2, H2
• human energy sources : intestinal gases

Question 31

Sulphate reduction

Answer 31

A specialised respiratory metabolism
* SCFA -> CO2 + H2S
* Toxic molecules

Question 32

Other bioactive microbial metabolites include…

Answer 32

• Bile acid derivatives DCA and LCA
• Neurotransmitter production (serotonin, GABA)
• Vitamin production
• Amino acid production
• human essential nutrients

Question 33

The net effect of microbial metabolites on our health is a product of:

Answer 33

• Food items/diet
• Microbial activity
• Types of microbes
• Adaptive responses

Question 34

“Nutrient control”

Answer 34

determines population size and activity in the gut (encourages functions we need):
* Body directs bacteria to use fibre - rapidly absorbs other nutrients
* Body selects for fermentative metabolism – excludes oxygen, removes iron
* Body supports growth on fibre - adds back nitrogen ‘fertiliser (uric acid, urea)
* Body limits total bacterial biomass - poops often
* Bacteria trained to ‘do the right thing’: stay in gut, grow on fibre, release SCFA

Question 35

Immune functions contain bacterial activity within the gut (Punish activities we don’t need)

Answer 35

• Intestinal mucosal surface limits bacterial contact with epithelium
• Immune defences kill bacteria at epithelium.
• The lamina propria (adjoining intestinal tissue) is kept ‘sterile’
• Bacteria near the wrong place, or in the wrong place, are not tolerated

Question 36

Microbe interaction with immune system

Answer 36

• Immune system has functions in preventing and resolving infections at all body sites.
• Immune system is also potentially dangerous – today chronic diseases involving immune-metabolic dysfunction are the major health burden

Question 37

Key features of Pathogens

Answer 37

• Not normally present
• Presence is associated with disease consistently
• Experimental infection is sufficient to cause disease.
• “Specialist pathogens”
• EXCLUDE from body

Question 38

Key features of Commensals

Answer 38

• Normally present
• Absence leads to abnormal physiology (in experimental Germ-free animals).
• May indirectly contribute to disease
• “Potential pathogens”
• “Opportunistic pathogens”
• ENCOURAGE in some parts and EXCLUDE from others

Question 39

Defence against pathogens involves…

Answer 39

1. Colonisation resistance
2. Barrier functions
3. Immune functions

Question 40

Pathogens can colonise…

Answer 40

• on external body surface (skin, teeth etc.)
• internal cavity (gut lumen)
• internal mucosal surface (epithelium of lung etc.)

Question 41

direct effect of pathogen

Answer 41

produce toxin or tissue-destructive enzyme
OR
Obstruction

Question 42

MAMPs

Answer 42

Microbe-associated Molecular Patterns

Question 43

DAMPs

Answer 43

Damage-associated Molecular Patterns

Question 44

Immune tone

Answer 44

• Differences in immune tone are major factors in different infectious disease severity.
• Change in immune tone is a major factor in development of chronic diseases.
• The gut microbiome is a factor in modulation of immune tone.

Question 45

Dysbiosis

Answer 45

a term for diseases of a poorly functioning symbiosis

Question 46

Is our risk for infection tightly inter-related with our microbiome?

Answer 46

YES - Opportunistic pathogens typically co-occur with normal microbes in our gut and specialist pathogens can invade our gut.

Question 47

The biggest disease burdens today are characterised as…

Answer 47

chronic immuno-metabolic diseases.
* Nearly all of them are nutrition-related and microbiome-related