Lec 30-Cytokines

Question 1

Introduction

Answer 1

• Cytokines are immunomodualtors that act at specific receptors on target cells
• Hormone-like polypeptide molecules: IL, chemokine, TNF-a, interferons, colony stimulating factors (CSFs)
• Cytokines circulate at lower levels than hormones (10-12M and active between 10-10M -10-15M and may increase by x106 during inflammation
• Cytokines can modify cell activity through acting at several types of surface receptors -Most effects are due to changes in gene expression

Question 2

What do cytokines do

Answer 2

• Growth factors
• Differentiation factors-
• Secretion of autocoids, production of antibodies and other proteins
• Chemotaxis (for cell-cell interactions
• Cytokines exhibit redundancy and are pleiotropic (many different action)
• Cytokines e.g. TNF can activate cells that produce it (Autocrine) or other cells (paracrine)

Question 3

Receptors tyrosine kinases

Answer 3

• Receptors consist of 2 identical single-pass transmembrane protein
• Receptors have kinase binding domains at intracellular cytoplasmic ends
• Tyrosine kinases are recruited to a receptor following agonists binding
• Cause activation of intracellular signalling cascades
• One such receptor-associated tyrosine kinase in janus kinase (JAK), many of whose effects are mediated by STAT (Signal transducer and Activator of Transcription)- proteins

Question 4

JAK-STAT- SIGNALLING BY RECEPTOR ASSOCIATED WITH TYROSINE KINASE

Answer 4

• when the cytokine binds to cytokine receptor the JAK is activated, meaning its kinase activity occurs and it phosphorylates the receptors
• This attracts normally inactive protein STAT’s causing the stat to bind to the receptor
• When this occurs the JAK will the place an phosphate onto the STAT
• Once STAT is phosphorylated they release from the receptor and form dimers with another STAT molecule- this is the active form
• These enter the nucleus to act as transcription factors to allowing protein synthesis to occur

Question 5

How is JAK-STAT different to other tyrosine kinases

Answer 5

• The JAK-STAT pathways are much shorter and simpler than the pathways triggered by RTK’s and so the response of cells to these ligands tends to be much more rapid
• NB this pathways is also used by IL’s, CSF’s and interferons

Question 6

TNF (tumor necrosis factor) signalling

Answer 6

• TNF is mitogenic (causes mitosis) in normal cells but induces cell death in cancer cells
• Excess TNF activity inflammation by enhancing expression of pro-inflammatory genes
• The TNF-induced survival pathway is mediated by the transcription factor NF-kB
• Activation of NF-kB occurs via phosphorylation of IkB which dissociated and is degraded
• Active NF-kB moves into the nucleus where it alters genes and expression

Question 7

TNF-a signalling (to kill cells

Answer 7

• TNF-a receptor is a trimer and binds to another protein called DISC
• This causes mitochondrial perturbation and punches holes in the mitochondrial membrane
• Causes the release of effector caspase’s -Causing apoptosis

Question 8

TNF signalling-a in normal cells to promote survival

Answer 8

• TNF-a binds to TNFRI (receptor) and activates NF-kB
• This protein is normal inactive by being complexed with IkB (-ve regulator)
• IkB is then phosphorylated by TNFRI and falls off NFkB
• IkB is then sent to proteasome’s to be degraded
• NF-kB is then able to enter the nucleus where it can interact with the kB unit on the gene and switch on transcription

Question 9

TNF-a (the other signalling pathway)

Answer 9

• DISC is activated ]
• This activate MAP3K
• This activated JNK
• Can bind to the gene

Question 10

Induction of inflammation IL2, IL4 -we can either produce T cells or B cells (the 2 different pathways)- This is T cell

Answer 10

• Antigen is presented to T CD4+ (T cell that can develop in multiple ways)
• If IL2 predominates then this will stimulate T cells to turn into Th0 -Then Th1
• Th1 then increases release of interferon gamma (INFy) and more IL2
• This process activates macrophages, NK cells -IFN will suppress the production of Th2
• Leads to a prolonged inflammatory response (this process is associated with inflammation)

Question 11

Induction of inflammation; B cell pathway

Answer 11

• Antigen is presented to T CD4+
• If IL4 predominates
• Th0 is produced
• Then Th2 is produced
• B cells are then stimulated to develop into anti-body producing plasma cells
• IL4 and TGF-b suppress Th1 cells
• This process is associated with anti-inflammatory

Question 12

Induction of inflammation: inhibition of the pathways

Answer 12

• INFy (created in the T cell pathway) will inhibit the B cell pathway
• IL4 and TGFb will inhibit T cell pathway

Question 13

TNF; IL-1; IL-6

Answer 13

• Main pro-inflammatory cytokines
• Involved in effector phase of immune/inflammatory response -Produced by macrophages and other cells

Question 14

IL-6; IL-1; TNF increase expression of COX2

Answer 14

• Cox-2 activity is increased in inflammation
• Leads to enhanced production of PGE2
• In hypothalamus leads to a rise in body temperature
• In endothelial cells leads to increase in vascular permeability

Question 15

Effects of TNF, IL-1 and IL-6 (think of areas of the body)

Answer 15

• Acts on hypothalamus to induce fever
• Act on liver to induce production of acute-phase proteins (e.g. serum amyloid protein, CRP, complement, mannose binding protein)
• Act on vascular endothelial cells and macrophages to induce secretion of colony stimulating factor (CSF) that subsequently act on bone marrow to increase WBC
• Act on vascular endothelial cells to increase both vascular permeability (Leukocyte migration) and expression of cell adhesion molecules (for rolling and firm adhesion of leukocytes)

Question 16

Other action of TNF action in inflammation

Answer 16

• Stimulates tissue (e.g. cartilage) degradation by increasing expression of matrix metalloproteinases
• Stimulates expression of pro-inflammatory genes e.g. IL-1,6 and NOS
• Promotes fibroblast proliferation
• Promotes tissue metric deposition
• Leads to scarring

Question 17

Linking cytokine mediators to symptoms (think of cardinal signs)

Answer 17

• Heat- increased body temp due to IL-1 acting to increase PGE in hypothalamus
• Redness- increased blood flow- due to cytokine promoted NO production= vasodilation
• Swelling- increased vascular permeability due to cytokine induced PGE2 synthesis
• Pain- cytokine induced PGE promotes nerve ending sensitisation to bradykinin
• Loss of function- fibrous due to TNF-a activation of fibroblast proliferation

Question 18

Chemokine and chemotaxis

Answer 18

• Chemokines are specific class of cytokine that mediate chemotaxis between cells
• IL-8 is the only chemokine originally named an IL
• Act on GPCR’s; co-receptor for AIDS virus (IL-5)
• C-X-C chemokine e.g. (IL-8) act on neutrophils and are involved in acute inflammation
• C-C chemokine e.g.(MCP-1) act on monocytes and other cells and are involved in chronic inflammation

Question 19

Anti-inflammatory cytokines

Answer 19

• TGF-b, IL-4 and others
• Inhibit production of chemokines
• Inhibit responses by Th1 cells (and stimulate responses by Th2 cells) and so switch immune system from cell-mediated to immunity to antibodies

Question 20

Interferons IFN

Answer 20

• IFN-a and IFN-b are produced from virally infected cells
• IFN-a is used as an anti-viral agent
• IFN-y is immunoregulatory and is used in multiple sclerosis to reduce antibody production

Question 21

Colony stimulating factors

Answer 21

• Produced mainly by bone marrow stroll cells, endothelial cells and fibroblasts in a constitutive fashion
• They stimulate inflammatory cell growth
• GM-CSF. A growth factor for many progenitors and a differentiation factor acting on granulocytes, macrophages and dendritic cells-G-CSG. Stimulates neutrophils -IL e.g.3,7 can also act on CSF
• CSF’s are used in conditions where there is depletion of WBC’s

Question 22

Steroids also lead to serious side effects

Answer 22

• Decreased fibroblast function less collagen- poor healing -Decreased osteoblast and increase osteoclast activity= osteoporosis
• Decreased macrophage sensitivity to cytokines- immunosuppression

+decreased leukocyte recruitment

+decreased basctericidal activity (iNOS)

+Decreased vasodilation

Question 23

Intro to steroids

Answer 23

• 1950 Hench- RA women who became pregnant went into remission, increase glucocorticoids
• Synthetic glucocorticoids decreases inflammation
• Mineralo and glucorticoids synthesised in adrenal cortex in response to ACTH
• Glucocorticoids- homeostasis of protein and CHO metabolism, anti-inflammator , immunosuppressive -Physiological role- prevent overshoot of body defence (magnitude and duration) -exert -ve feedback via pituiatary

Question 24

Endogenous glucocorticoid metabolism

Answer 24

• 90% hydrocortisone; 10% corticosterone
• Circulate attached to albumin or corticosteroid binding protein (CBP) but not synthetic hormones
• Can enter directly or via a complex bound to CBP
• Excess corticoids leads to bushings syndrome (cataract, abdominal fat, poor wound feeling, muscle wasting, HTN)

Question 25

Mechanism of GC action

Answer 25

3000-100,000 GCRs per cell in nucleus

• GCRs and GC bind to DNA -Attach to specific sequence present in promotors of 10-100 genes (~1% of cellular genes)= GC responsive element
• Can increase or decrease levels of protein depending on the gene -Initiator- promotes mRNA production increase in levels of protein e.g. Lipocortin
• Inhibitor- (1) block RNA polymerase- inhibit protein expression or (2) bind to and inhibit other transcription factors e.g. AP1- repress transcription factor controlling collagen production- reduced healing

Question 26

Targets for glucocorticoids

Answer 26

UPREGULATION -Lipocortin- endogenous inhibitor of PLA2 (15-30 min)

-This means no arachidonic acid so no: TXA’s: PG; LT’s: -This pretty much cuts of inflammation at its source

DOWNREGULATION

• COX2 but not COX-1 -IL-1 and 6
• iNOS
• MMP (matrix metalloprotinase)
• Collagen
• Adhesion molecules

Question 27

Other inflammatory mediators reduced by steroids

Answer 27

• Complement component
• Histamine release
• Phagocyte activity
• Reduced clonal expansion of T and B cells

Question 28

Clinical effects of steroids

Answer 28

• Inhibit inflammation arsing from all types of stimuli e.g. chemical, physical and endogenous
• Inhibit early phase- redness, heat, pain, swelling
• Inhibit late phase- healing repair
• Act on endothelial and inflammatory cells and their mediator

Question 29

Kinetics

Answer 29

• Response time 6-24 hours after injection (ie. bronchodilator also required for asthma attack
• Half life 90 minutes

Question 30

Problems associated with steroids

Answer 30

• Large acute doses are tolerated well
• Chronic therapeutic corticoid - suppress production of endogenous corticoids
• Withdrawal of treatment - adrenal insufficiency- Addison’s disease- Low BP, hypoglycaemia

Question 31

Steroids also lead to serious side effects

Answer 31

• Decreased fibroblast function- less collagen- poor healing -Decreased osteoblast and increased osteoclast activity- osteoporosis (destroy bone and not remake it)
• Decreased macrophage sensitivity to cytokine - immunosuppression

+decreased leukocyte recruitment

+decreased bactericidal activity (iNOS)

+Decreased vasodilation