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CardioPul 2 > thrombolytic therapy > Flashcards

thrombolytic therapy Flashcards

1
Q

clotting vs clearing

A
  • Both are necessary, both must be controlled
  • Prevent formation and growth of clots

–> warfarin, ASA, NOACs

  • Breakdown already formed clots

–> plasmin (native agent) is the direct lytic

–> thrombolytics are not lytics per se; activated plasmin

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2
Q

describe Streptokinase

A
  • Derived from Group C streptococci
  • DIRECT PLASMINOGEN ACTIVOTR (activates plasmin to break up clots)
  • Antigenic, generic
  • Efficacy in MI time-dependent, drip dosing
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3
Q

Urokinase

A
  • Human neonatal kidney cells
  • DIRECT PLASMIOGEN ACTIVATOR
  • non-antigenic
  • used to clear lines, Pulmonary embolus, direct arterial infusion
  • Limited use in coronary thrombosis (expense limited original studies)
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4
Q

Tissue Plasminogen Activator

A
  • ALTEPLASE
  • recombinant molecule
  • occurs naturally in blood
  • DIRECT PLASMINOGEN ACTIVATOR
  • Was drug of choice for acute MI
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5
Q

describe the Thrombolysis goals in MI

A
  • Disease oriented:
  • Good blood flow in infarct vessel

–> TIMI risk: risk increases with number (0 = less risk)

–> TIMI flow: Flow increaes with number (0 = no blood flow)

  • Reduce in infarct size measured by DECREASE markers
  • patient oriented
  • improved survival rates
  • Reduce LV failure, ventricular dysrhythmias, direct complications of MI
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6
Q

Describe the effects of mortality

A
  • HIGH RISK GROUPS
  • More to gain as risk higher
  • Hypotension
  • diabetes
  • Mortality improves across all groups
  • some risk/reward balance
  • younger patients have decreased acute mortality (may not benefit as much)
  • Older patients may have more head bleeds
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7
Q

describe complications of thrombolytics

A
  • Bleeding (lytics don’t know what to lyse)

–> intercranial bleeds (higher risk if you less than 70kg, over age of 65 or have poorly controled hypertension

  • allergic reactions (rare) with SK and congeners
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8
Q

describe the Acute MI protocols

A
  • Less than 120 mins from FIRST CONTACT: go to cath lab
  • aspirin, nitro, morphine/fentanyl
  • maybe oxygen
  • local choice: anticoagulants (hemaprin, enoxaparin, ticagrelor)
  • more than 120 mins: thrombolysis
  • TNKase recommended by AHA
  • aspirin, nitro, morphine/fentanyl
  • Heparin or enoxaparin
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9
Q

describe Acute MI, late presentation

A
  • 4 to 12 hours

–> consider using lytics (steptokinase-maybe lower risk of intercranial bleeds)

  • lytic therapy >12 hours after onset

–> maybe with ongoing symtpoms/necrosis (must have low stroke risk)

–> use only with large MI (AW), low CVA risk

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10
Q

Points to ponder

A
  • Thrombolytics are not anticoagulants (thrombolytics are tx only!!! not prevention)
  • thrombolytics activate a natural process (plasmin breaks up fibrin clots)
  • thrombolytics use the benefit and risk; they usually go bi-directionally (patients with most at risk benefit the most so may tolerate harm)
  • Most newer lytics have no great patient-level benefit
  • Administering lytics in acute MI when PCI is delayed will save lives
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CardioPul 2 (16 decks)

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