Haemostasis and blood coagulation 2

Question 1

Describe Thromboembolic conditions.

Answer 1

Thrombi and Embolic
1. An abnormal clot that develops in blood vessel is called Thrombus (clotting without injury)

freely flowing clots (unbound) are known as embolic

Question 2

THE EMBOLIC ORIGINATING:

Answer 2

a) in left side of the heart & large arteries= can block arteries or arterioles in the brain,
kidneys, or elsewhere.

• b) in the venous system or right side of the heart = flow into lungs = pulmonary arterial
  embolism

Question 3

the causes of thromboembolic conditions.

Answer 3

Roughened endothelial surface of a vessel—due to arteriosclerosis, infection, or
trauma (likely to initiate clotting process)
b) Very slow blood flow where small quantities of thrombin and other procoagulants are
always being formed.

Question 4

THE USE OF TISSUE PLASMINOGEN ACTIVATOR IN TREATING INTRAVASCULAR CLOTS

Answer 4

• Genetically engineered tissue plasminogen activator (t-PA) is available.
• When delivered to an area with a thrombus, it is effective in activating plasminogen to
  plasmin, which in turn can dissolve some intravascular clots.

Question 5

Femoral Venous Thrombosis

Answer 5

Blood stasis (due to immobility of patients confined to bed; practice of propping theknees up with pillows) →Intravascular clotting
1. Femoral Venous Thrombosis:
* These clots grow in slow moving venous blood, full length of leg veins, even up into
common iliac vein and inferior vena cava.

Question 6

Massive pulmonary Embolism

Answer 6

A large part of the clot disengages from its attachments to the vessel wall →flows through
venous blood →right side of the heart → pulmonary arteries → massive blockage of the
pulmonary arteries.

• If both pulmonary arteries are occluded at the same time = immediate death ensues.
• If only one pulmonary artery is blocked:
  a) death may not occur, OR
  b) the embolism may lead to death a few hours to several days later due to further clot growth
• However, t-PA therapy can be a lifesaver.

Question 7

3. Disseminated Intravascular Coagulation:

Answer 7

circulation→ disseminated intravascular coagulation (DIC).
* DIC results from the presence of large amounts of traumatized or dying tissue in the body
that releases great quantities of tissue factor into the blood.

• Frequently, the clots are small but numerous, and they plug a large share of the small
  peripheral blood vessels.
• This process occurs especially in patients with widespread septicemia, in which circulating
  bacteria or bacterial toxins (esp. endotoxins), activate the clotting mechanisms.
• The plugging of small peripheral vessels greatly diminishes delivery of oxygen and other
  nutrients to the tissues→ circulatory shock.
• septicemic shock is lethal in 35% to 50% of patients.
• Effect of DIC, patients begin to bleed= due to so many of the clotting factors being removed
  by the widespread clotting → too few procoagulants remain to allow normal hemostasis of the
  remaining blood

Question 8

The delay of coagulation processes in some thromboembolic conditions is due to ———–being developed

Answer 8

anticoagulation

Question 9

Most clinically useful anticoagulants are:

Answer 9

1. Heparin—Intravenous Anticoagulant
2. Coumarins as Anticoagulants

Question 10

Heparin the intravenous anticoagulant

Answer 10

Injection of about 0.5 to 1 mg/kg of body weight→ ↑s blood-clotting time from about 6 minutes
(normal time) to 30 or more minutes.
* This change in clotting time occurs instantaneously → immediately preventing or slowing
further development of a thromboembolic condition.
Anticoagulants for Clinical Use
* The action of heparin lasts about 1.5 to 4 hours.
* The injected heparin is destroyed by an enzyme in the blood known as heparinase.

Question 11

Coumarins as Anticoagulants.

Answer 11

• Coumarin, such as warfarin, given to a patient→ ↓s active prothrombin and factors VII, IX, and
  X.
• Warfarin causes this effect by inhibiting the enzyme VKORC1.
• VKORC1 enzyme converts inactive, oxidized form of vitamin K to its active, reduced form.
• So, inhibition of VKORC1 by warfarin→ ↓s active form of vitamin K in the tissues → this
  decrease inactivates coagulation factors.
  Anticoagulants for Clinical Use
• After administration of an effective dose of warfarin, the coagulant activity of the blood
  decreases to about 50% of normal by the end of 12 hours and to about 20% of normal by the
  end of 24 hours.
• Normal coagulation usually returns 1 to 3 days after discontinuing coumarin therapy

Question 12

Prevention of Blood Coagulation Outside the Body

Answer 12

Substances that ↓ [calcium ions] in the blood → can prevent blood.
coagulation outside the body.

Example:
a) Soluble oxalate compound mixed with sample of blood →causes precipitation of
calcium oxalate from the plasma → ↓ [calcium ions] → blockage of blood
coagulation.
b) Citrate anticoagulants

Question 13

Fibrinolysis breaks up clots

Answer 13

• Cross-linked stable fibrin traps RBCs and WBCs as well as platelets in a newly
  formed thrombus.
• After plug formation, fibrinolysis (the breakdown of stable fibrin) breaks up the
  clot in a process known as thrombolysis.
• Fibrinolysis begins with the conversion of plasminogen to plasmin, catalyzed by
  tissue-plasminogen activator (t-PA) or urokinase-plasminogen activator (u-PA).
• The tissue plasminogen activator is produced by the endothelial cells.
• The presence of fibrin greatly accelerates the conversion of plasminogen to
  plasmin.

Question 14

Enzyme that breaks down both fibrin and fibrinogen?

Answer 14

Plasmin

Question 15

The system that regulates fibrinolysis at several levels using both inhibitors and enhancing mechanisms?

Answer 15

Cardiovascular system

Question 16

Name 2 serpins that reduces the activity of the plasminogen activators.

Answer 16

1.plasminogen activator inhibitor 1 produced by endothelial cells, inhibits both tPA and u-PA

2.Plasminogen activator inhibitor 2
(PAI-2): mainly inhibits u-PA.

• α2-antiplasmin (α2
  -AP) made by liver, kidney, and other tissues, target plasmin

α2-AP binds and inactivates plasmin not bound to fibrin; but when
plasmin is bound to fibrin, the inhibition by α2
-AP is greatly reduced.

Thrombin-activatable fibrinolysis inhibitor (TAFI) also inactivates plasmin

Question 17

what is Streptokinase?

Answer 17

Streptokinase (s-PA) = thrombolytic enzyme (used in MI, pulmonary
embolism etc

Question 18

A thrombolytic enzyme (used in acute ischemic strokes,
MI, pulmonary embolism, etc.

Question 19

The protein that inhibits coagulation also inhibits — and —- enhancing fibrinolysis.

Answer 19

Protein C
PAl-1
PAI-2

Question 20

Platelets inhibitors effets:

Answer 20

1. Intact endothelium serve as a barrier that shields platelets from subendothelial vWF
   and collagen.
2. Normal endothelium releases several factors that inhibit platelet activation and
   aggregation:
   a) Prostacyclin (PGI2
   ): produced by Cyclooxygenase-1, which is expressed by “healthy”
   endothelium under normal flow conditions.
   b) Nitric oxide (NO): is the product of endothelial nitric oxide synthase eNOS.
   c) Adenosine diphosphatase: degrades ADP (potent activator of platelet aggregation

Question 21

Blood coagulation tests: Bleeding time.

Answer 21

• When a sharp-pointed knife is used to pierce the tip of the finger or earlobe, bleeding
  ordinarily lasts for 1 to 6 minutes.
• This time depends mainly on the:
  a) depth of the wound
  b) degree of hyperemia in the finger or earlobe at the time of the test.
• Lack of any one of the several clotting factors can prolong the bleeding time, more especially
  the lack of platelets

Question 22

Clotting time

Answer 22

• Method mostly used for determining blood-clotting time:
  a) Collect blood in a glass test tube and then tip the tube back and forth about every 30
  seconds until the blood has clotted = normal clotting time is 6 to 10 minutes.
• However, clotting times vary widely, now measure clotting factors in blood

Question 23

Prothrombin Time and International Normalized Ratio.

Answer 23

Prothrombin time indicates the [prothrombin] in the blood.
* Method for determining prothrombin time:
* Blood removed from the patient is immediately oxalated to prevent prothrombin conversion
to thrombin.
Large excess of calcium ion and tissue factor is quickly mixed with the oxalated blood.
* Excess calcium nullifies the effect of the oxalate,
* Tissue factor activates the prothrombin to thrombin (through extrinsic clotting pathway).
* Time required for coagulation to occur = prothrombin time.
* The shortness of the time is determined mainly by the prothrombin concentration.
* The normal prothrombin time is about 12 seconds.

Question 24

Fibrin Degradation Products (FDPs)

Answer 24

• Once damaged endothelium is repaired, the fibrin thrombus must be removed to restore
  normal blood flow.
• Thrombus removal is facilitated by plasmin.
• Release of tissue plasminogen activator (t-PA) from endothelial cells leads to conversion of
  the proenzyme plasminogen into plasmin.
• Plasmin has the capacity to digest fibrin in addition to fibrinogen and a number of other
  proteins.
• Digestion of cross-linked fibrin by plasmin →formation of ‘degradation products’/ D-dimers=
  their presence in the plasma indicates that the coagulation mechanism has been activated.
• Elevated levels of fibrin degradation products, most notably fibrin-derived D-dimers, are a
  useful clinical marker of several thrombotic states.

Question 25

, clotting of plasma is initiated by the addition of negatively charged particles That activate a)———-together with b——————and
c———— and the time to fibrin clot formation is recorded

Answer 25

a. Factor xii
b. phospholipids
c. calcium