prostaglandins - lecture Flashcards
arachidonic acid
omega 6 FA that eicosinoids are made from
things that stimulate eicosinoid release
injury (exposed collagen, thrombin, damaged cells)
heat (thermal injury)
hormones (bradykinin, angiotensin, vasopressin,cytokines)
Ag-Ab complex, activated complement
bacteria, LPS
all activate phospholipase that act on phospholipid that act on arachidonic acid
PG synthesis and action in platelets
TxA2 is released from platelets via COX-1
TxS makes TxA2
leaves via PGT channel
acts on VSMC TPbeta receptor => vasoconstriction
acts on platelets TPalpha receptor => aggregation
PG synthesis and action in endothelium
PGalphaS makes PGI2
leaves via transporter?
acts on vascular SMC via IP receptor => vasodilation
acts on platelets via IP receptor => clumping
PG synthesis and action in uterus
- PGF2 and PGE2
- Production stimulated by LH
- Stimulate follicle release, cervical ripening, uterine contractions, and penile erection
- So, NSAIDs can be used to prolong gestation and may block premature birth
PGFS makes PGF2alpha
transported out by PGT
acts on uterine smooth muscle by FP receptor => contraction and parturition
PG synthesis and action in mast cells
PGDS makes PGD2
leaves via PGT
acts on Th2 lymphocyte via DP2 receptor => chemotaxis
acts on lung epithelial cells via DP1 receptor => allergic asthma
PG synthesis and action in most cells
PGES make PGE2
transported through PGT
acts on osteoclasts via EP4 receptor => bone resorption
acts on neurons of OVLT in POA via EP3 receptor => fever generation
acts on ovarian CO cells via EP2 receptor => maturation for ovulation and fertilization
acts on spinal neurons via EP1 receptor => pain response
nsaids
- inhibit release of arachinoic acid and also cox1 and cox2 - make it more available to leukotriene pathway?
- They IRREVERSIBLY block COX-1 and COX-2. Since platelets (COX-1) are anucleate, that means no more COX-1 until new platelets are made, versus endothelial cells which can make new COX-2 later.
- They do not block and may even stimulate leukotriene synthesis
- They cause GI damage due to blockage of PG E2 production by COX-1
- They are anti-thrombotic by blocking COX-1, which blocks thromboxane production
- They also reduce risk of colon polyp and adenoma (possibly related to COX-1 blockage)
why need cox2 specific inhibitors?
selectively inhibit pg production at inflamatory sites via cox2 but don’t inhibit cytoprotective e pg that are produced by gut epi cells via cox 1
aspirin
irreversibly inhibits cox1
acetylates PG synthase => inactivation
given to patients after coronary bypass surgery
can reduce colorectal cancer death because of mutant PI3-kinase in cancer patients
vioxx
- very selective for cox 2
- so it’s less GI-damaging than NSAIDs because it doesn’t block COX-1 and its product, PG E2 (gut protective)
- However, this also means selectively blocking prostacyclin production in endothelium (via cox 2) but not blocking thromboxane A2 production via cox 1 - get clots
COX1
- Platelets (so NSAID inhibition is long lasting as platelets cannot synthesize new COX-1)
- Blocked by NSAIDs, but not Coxibs or GCs
- Produces PGE2 (gut protective), thromboxane A2 (bad – promotes atherogenesis and vasoconstriction), and PG I (opposite of TxA2)
- Its lack of inhibition by Coxibs is why they promoted vascular diseases
COX-2
- Endothelial cells (so NSAID inhibition is is removed once the cells synthesize new COX-2)
- Blocked by NSAIDs, GCs and Coxibs (specific)
- Produces inflammation, , and PG I2 (opposite of TxA2)
