Summary

This document discusses drugs affecting hemostasis, including the coagulation system, prevention of clotting, and dissolution of blood clots. It also covers the mechanism of action of different drugs and their effects on the body.

Full Transcript

Part 2 2: Dru ugs affe ecting he emostas sis █ Basiic inform mation stasis is th Hemos h...

Part 2 2: Dru ugs affe ecting he emostas sis █ Basiic inform mation stasis is th Hemos he spontan neous arresst of bleed ding from damaged d b blood vess sel. ▌The c coagulatiion syste em: It conssists of a number of plasma a proteinns (facto ors). Eac ch factorr activatees anothe er till acttivation off fibrinog gen to formm fibrin. Activation cascad de is done e through 2 systemms: the inttrinsic sys stem (can n be mon nitored by the activaated partia al throbop plastin tim me “APTT””) and the e extrinssic system m (can be monitored d by protthrombin time). Preven ntion of clo otting:  Plassma conttains a number n off protteins thatt normally y preventt clottting thro ough inhibition off clottting factors (e.g. antithrombin n III).  Hepparin activvates antith hrombin III thuss inhibits ac ctivation of factors IX, X, XI, and XII.  Oraal anticoag gulants inh hibit synthhesis of clo otting facto ors by the l iver. Dissolu ution of bllood clots s:  Theere are oth a proteinss that can dissolve blood clotts (i.e. fibrrinolytic her plasma systtem e.g. plasmin).  The ere are som me drugs that t activa ate plasmin nogen to form the acctive plasm min and thuss enhancee fibrinolysis (e.g. stre eptokinas se, urokina ase, etc.).  Amminocaproiic acid is ana inhibitorr of fibrinolysis. ▌Drug gs can afffect hemo ostasis a and throm mbosis through:  By modifying the integriity of the vvessel wall.  By modifying blood coa agulation (clot forma ation).  By modifying platelet adhesion an nd activation.  By modifying fibrinolysis. 208 █ DRU UGS THAT T PREVEN NT COAGU ULATION (ANTICOA ( AGULANTS S) Heparin Warfarin (Ora l anticoag gulant) Source e& Naatural sulfate ed polysac ccharide Synthetic cuomaarin compound chemis stry preesent in maast cells & c carries –ve chaarge Coommercial preparation p ns are de- rive ed from bovine lung o or porcine intesttinal extractts Absorp ption  No becaus se it precip pitates by  Good (bioavaailability is 100%). gastric HC Cl.  Can n cross BB BB and pla acenta. Distribttion  Cannot crross BBB o or placenta a.  Its action depends d o on the pres s-  Wa arfarin inhib bits vitamin K ence of a natural clo otting inhibb- epooxide redu uctase enz zyme itor called heparin co ofactor in the liver leaading to in nhibition (antithrom mbin III) in plasma. of formation f o of the activve form  Small quantities of h heparin can n of vitamin v K → ↓ synthes sis of Mechanism of action activate anntithrombin n III leading vita amin K-dep pendent cllotting to inhibitio on of severral clotting factors (II, VIII, IX, and X). X factors especially fac ctor X &  Thee action off warfarin could c thrombin (factor ( II). be antagonizeed by vitam min K. Onset and Immediate and a short ((2-4 hrs). Delayyed for 8-1 2 hrs (time e duratio on needeed for deple letion of clo otting factorrs & vit K) aand long (33-7 d) Pharma acol  Anticoagullant in vivo o & in vitro Antico oagulant in n vivo only y. effects s  Stimulates s lipoproteiin lipase → ↓↓ serum triglyceride t es (TGs). Therappeu-  Treatmennt of estabblished Warfa arin is givenn oral 2-10 0 tic use es thrombos sis: heparin n is given mg/daay for prevvention an nd parenteral 5000-10,0000 U i.v. treatm ment of: then 5000 U s.c./8h to maintaiin – Deeep vein thrrombosis (DVT) ( blood coagulation 2--3 times ass – Posstoperativee thrombossis. normal and preventt further – Cerrebral venoous thromb bosis. 209 extension of the thrombus. – Coronary thrombosis: treatment continued for  Prevention of thrombosis: several years. 5000 U s.c./8-12 hrs. – Acute arterial & pulmonary embolism: anticoagulation is initiated by heparin and maintained by warfarin. – AF and artificial heart valves Monitor- By activated partial thrombo- By prothrombin time (PT) or ing of plastin time (APTT). International Normalized Ratio therapy It must be kept 2-3 times as the (INR). It is the ratio of the PT in normal value. the patient to that of normal person. It must be kept 2-3 times as the normal value. Adverse  Bleeding is the most common and dangerous SE (e.g. hematuria effects & major organ bleeding). It could be treated by the following: (a) Immediate stopping of the drug. (b) Fresh frozen plasma (FFP): to provide fresh clotting factors. (c) Protamine sulfate (Protam): (c) Vitamin K1: 10 mg slowly - Protamine carries +ve charge i.v. or i.m. to enhance that combines with heparin synthesis of clotting factors. (carries -ve charge) to form stable complex. - 1 mg of protamine can bind to 100 U of heparin.  Hematoma if given IM (so, con-  Hemorrhagic skin necrosis: traindicated to give it IM). when starting warfarin, biosyn-  Thrombocytopenia: immune- thesis of protein C is reduced mediated reaction due to for- leading to temporary procoag- mation of antibodies that can ulant state. This can lead to bind to platelets. Platelet count hemorrhagic infarction of skin, should be performed regularly breast, intestine and fatty tiss-  Osteoporosis and spontaneous ue. normally avoided by conc- fractures on long-term therapy urent heparin administration.  Alopecia and dermatitis: rare  Teratogenicity: abnormal bone and transient. formation in early pregnancy (fetal warfarin syndrome).  CNS Hemorrhage in the fetus if given in late pregnancy.  Sudden withdrawal may lead to thrombotic catastrophes. 210 Low-m moleculaar-weigh ht hepari ns (LMW WH) (Enoxa aparin – Dalteparin) D )  Sta nfractionatted) heparrin is a andard (un mixxture of different d molecular m weight frac ctions (MW W 3000-30,000 Da) thhat can affe ect more th han one cooagulation n factor andd produce thromboc cytopenia (↑ risk of b bleeding).  LMW WH has a MW less than 80 000 Da thatt makes it specific for f factor X with minnimal effec cts on platelets and d other clottting factorrs. Unfra actionated d heparin LMWH H Molecu ular weightt range Wide (ranges fro om 3000 to o Less thhan 8000 Da D 30,00 00 Da) Anti-fac ctor Xa acttivity Less sspecific More sspecific Non-sppecific bind ding to High Low vascula ar endothe elium and plasma a proteins Bioavailability after s.c. Low High injectio on (due tto binding to s.c. tissue) e) Half-life e Short (given 3 tiimes/d) Long (g given once e/d) Thromb bocytopen nia Comm mon (10%)) Less ccommon (<

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