Lecture 28; immunometabolism

Question 1

What was the initial discovery of immunometabolism? (involves TNFa)

Answer 1

~ 20 years ago, TNF-a administration shown to lead to hyperglycemia (cant take up blood glucose)

then

TNF-a elevated in obese rodents (Adipose Tissue Macrophages), neutralization of TNF-a improved insulin resistance and TNF-a-deficient mice had improved insulin sensitivity during diet-induced obesity

I.e overnutrition does this,

Question 2

In obese mice what is thought to be responsible for the hight TNFa?

Answer 2

Nutrient overload activates inflammation in insulin-target tissues (e.g. adipose tissue, liver, skeletal muscle, pancreas, hypothalamus)

Question 3

What basic factors does metabolism and immunity share?

Answer 3

• Sensors transduce stimuli into downstream mediators that activate effector responses to eliminate stimulus-return to homeostasis
• Metabolism and immune response organised in the same way
• A shared modular architecture

It is believed that overnutrition can alter the immune cell representation in adipose tissue and thus the inflammatory profile to a proinflam response

Question 4

Describe the immune profile of adipose tissue in a lean individual;

Answer 4

• Release of Il4,13 (antiinflam) by eosinophils
• Th2 and Tregs release IL10

Combination of these cytokines maintains an entry level macrophage state. (anti-inflam state, surveillance phenotype)

Question 5

Describe the immune profile of adipose tissue in a obese individual;

Answer 5

Obese state, immune cells recruited, recruited monocytes polarized to highly pro-inflammatory M1 state/insulin resistance
• Cytokines/chemokines stimulate inflammation in other tissues in an endocrine manner

Th1, cd4, cd 8 now present
adipokines promote M1 state of macrophages as well as pro-inflam state (promotes insulin resistance, TNFa)

Question 6

Describe the shift in adipose immune cells in an obese individual;

Answer 6

Increased;

• M1
• Mast cells
• B2
• CD8
• IFNg Th1

= Proinflam response

Decreased

• M2
• Eosinophils
• Treg

= decreased anti-inflam profile

Question 7

What diseases can result from the chronic low grade inflammation on an obese individual?

Answer 7

• Dementia (CNS inflam)
• Immune dysfunction
• Atherosclerosis (lipid uptake my macros)
• Diabetes
• Pancreatitis
• Athritis
• insulin resistance
• Gout
• Cancer

Question 8

Describe the relationship between Infection, immunity and insulin resistance;

Answer 8

• Bacterial infection activates innate immune cells-release of pro- inflammatory cytokines that mediates IR in metabolic tissues
• IR in liver-increased gluconeogenesis
• IR in muscle-decreased glucose
disposal and increased breakdown of
glycogen
• Elevated glucose can fuel immune cell
activation
• IR in adipose tissue-increased break
down of lipids and decreased
lipogenesis
• Elevated FFAs can support immune
cell metabolic demands
• Nutrients diverted to support
immunity

Question 9

What influences immune cell functional activity?

Answer 9

The mode of fuel that they use i.e FFA or glucose.

Question 10

How does IR occur?

Answer 10

• Stimulation of pro-inflammatory signalling pathways negatively regulates insulin signaling leading to insulin resistance
• TNF-a can stimulate serine kinases (IKK, JNK, S6 kinase) that leads to serine phosphorylation of insulin receptor substrate-1

Question 11

What are three pathways that can drive inflammation that can lead to IR?

Answer 11

• Saturated fatty acids can signal through TLRs to regulate pro- inflammatory gene expression
• Inflammasome activation also contributes to pro-inflammatory signalling
• Omega-3 fatty acids and IL-10 anti- inflammatory signalling, i.e. decrease IR

Question 12

Describe the M2 macrophage signalling in adipocytes in a lean state;

(signal mechanisms between the two cells)

Answer 12

• Eosinophils can release IL4,13 that act through their receptors i.e STAT6 which drives anti-inflammatory pathways
• m2 then can produce Il10 (anti) which can act on adipocytes to enhance its insulin sensitivity.
• Alternatively adiponectin or omega FA 3, can act via receptors and AMPK to inhibit pro-inflam signals. (fortifying anti-inflam signalling)

Question 13

Describe the M1 macrophage signalling in adipocytes in a obese state;

(signal mechanisms between the two cells)

Answer 13

IN the adipocyte;
- Increased adipolysis, these FFA can act via TLR on M1 and drive a pro-inflam state (TNFa)
- TNFa acts on adipocyte and up regulates more proinflam genes. (becomes a cycle perpetuating one another)
- M1 cells release CD5-like antigen, taken up by adipocyte by CD36-mediated endocytosis, promotes break down of lipids
• SFAs perpetuate M1 activation and adipocyte pro-inflammatory phenotype

Both adipocytes and M1s recruit monocytes = skewed M1 production

Question 14

Whats the evidence of autoantibody production in adipose tissue of an obese individual?

Answer 14

• When adipocytes become engorged in an obese individual, some undergo necrosis.
• These are phagocytosed and derived self antigen can be presented to TH1 cells.
• Clonal expansion of th1
• This can lead to activation of B cells producing autoantibodies

which can lead to type two hypersensitivity reaction

Question 15

What is oxidative phosphorylation?

Answer 15

OXPHOS-oxidation of nutrients in the mitochondria to produce energy (TCA cycle and electron transport chain)

Question 16

What is the TCA?

Answer 16

TCA cycle, metabolic pathway to generate ATP via the oxidization of acetate from glucose, fats, amino acids

in mitochondria, H ions pumped out into intermembrane space

Question 17

What is the primary fuel of neutrophils, M1 macros, activated DC?

Exam

Answer 17

Glucose

they ferment it to lactate (process is Warburg effect) (/aerobic glycolysis)

Question 18

Describe the warburg effect;

Exam

Answer 18

• ATP production and cellular survival dependent on glycolysis
• No OXPHOS, even in presence of oxygen
• PPP (pentose phosphate pathway) active, provides NADPH, needed for nox-dependent bactericidal activity (also being used)

Glucose -> lactate

Question 19

How do effector t cells use as fuel?

Answer 19

• Activated T cells use aerobic glycolysis and OXPHOS

* Degradation of glutamine can help replenish TCA cycle intermediates

Question 20

How do Tregs, M2 and memory t cells produce energy?

Answer 20

• Use FAO to survive and support function

i.e OXPHOS and no aerobic glycolysis

Question 21

How do mitochondria produce ROS?

Answer 21

• Energy ‘powerhouses’ of the cell
• A by-product of OXPHOS
• NADH and succinate from
the TCA cycle feed into the respiratory chain to generate ATP
• Electrons ‘leak‘ from the respiratory chain resulting in ROS (superoxide) production
• Converted to H2O2 by SODs
• mROS, a primary source of
cellular ROS

Question 22

What regulates mitochondiral ROS?

Answer 22

Immunoreceptor ligation, cytokines can augment mROS production

Question 23

How can mROS influence physiological processes?

Answer 23

mROS can influence immune cell activity, e.g. bactericidal activity and believed to help regulate expression of immune- response genes

Question 24

How does the level of mROS relate to physiological process outcomes?

Answer 24

• High levels of mROS damage proteins, lipids and nucleic acids
• Very low levels are required for cellular homeostasis
• Intermediate levels act as signalling molecules to help adapt to cellular stress (e.g. that during inflammation)

Question 25

How can mROS influence (innate immune cell) macrophage activation?

Answer 25

• mROS enhances RIG-1-like receptor/mitochondrial antiviral signalling protein signalling to induce type I IFNs/pro-inflammatory cytokines that inhibit viral replication
• ROS can oxidize specific redox- sensitive cysteine residues on target proteins

Question 26

Considering that macrophages doesnt use OXDPH then how is there an increase in ROS?

Answer 26

• When it becomes infected by a virus, there is an coupling of the ETC.
• The H in the intermembrane space dont really get pumped back by complex five so instead they are force back down complex 1. i.e when its uncoupled it reverses producing lots of ROS

Succinate (complex 2) acts as a proinflam signal.

Question 27

Describe how the mitochondrial dynamics change from a Teff to Tm cell;

Answer 27

• Round fragmented -> elongated
• loose-> tight cristae
• aerobic -> OXDPH

Question 28

Describe how the mitochondrial dynamics change from a resting macro to activated macro.

Answer 28

• Supercomplex formation -> disruption (inc. mROS)

- OXDPH -> Aerobic glycolysis