Vasopressors: Difference between revisions

Revision as of 04:11, 3 December 2014

Background

The goal of vasopressor use is to reach critical organ perfusion pressure. Estimated required mean arterial pressures (MAP) are listed below. It is generally safe to aim for a goal map of 65 mmHg. Vasopressors also promote increased venous return.

Brain: MAP of 50 mmHg ^[1]
Heart: MAP of 65 mmHg^[2]
Kidneys: MAP 65-75 mmHg^[3]

IV Vasopressor have not been shown to be unsafe when used peripherally^[4]

Norepinephrine

Indication

Septic shock (1st line)
Cardiogenic shock:
- If marked hypotension (SBP <70)
- If used with dobutamine

Primary Receptor

α1 >> β1

Relative Effects

↑↑↑SVR
↑HR
↑SV

Dosing

Start 2mcg/min
- Incr by 1-2mcg/min
- Max dose is 40mcg/min
Replace volume before starting

Rate of Titration

Q2-5 min

Adverse Effects

If extravasation occurs use phentolamine 0.1 to 0.2 mg/kg (maximum dose 10 mg) subcutaneous in affected site^[5]^[6]
- Consult plastic/general surgery service to follow the patient and eval for need for intervention^[7]

Notes

More potent vasoconstrictor than dopamine and phenylephrine.

Dopamine

Indication

Hypotension caused by:
- Septic shock
- MI
- Trauma/spinal shock
- Heart failure

Primary Receptor

Low dose: DA, β1
High dose: DA, α1 >> β1

Relative Effects

Low dose: Natriuresis, ↑↑HR, ↑↑SV
High dose: ↑SVR and ↑SV

Contraindication

Tachyarrhythmias

Dosing

Low dose:
- 1-5 mcg/kg/min - Vasodilation (renal, mesenteric, coronary)
- 5-10 mcg/kg/min - predominant β1
High dose: 10-20 mcg/kg/min - predominant α1
Titrate to clinical effect
- Use lowest dose possible (prevent tachyphylaxis)
May use in peripheral IV temporarily
- Avoid using in same line as alkaline infusions

Rate of Titration

Q2-5 min

Adverse Effects

Low doses:
- Hypotension
High doses:
- Hypertension, ectopic beats
Tissue necrosis (if extravasates)
- If occurs use phentolamine 5-10mg in affected area

Dobutamine

Indication

Cardiogenic shock
Low-output heart failure
Tricyclic overdose

Primary Receptor

β1
β2

Relative Effects

↑↑↑SV
↑↑HR
↓SVR (transient, from β2 agonism)

Dosing

2-20mcg/kg/min
- 10mcg works for most
May use in peripheral IV

Rate of Titration

Q2-5 min

Adverse Effects

Tachyarrhythmias
Myocardial ischemia
Hypotension as β2 effect may result in vasodilation
- Caution if SBP <90

Phenylephrine

Indication

Neurogenic Shock

Primary Receptor

α1

Relative Effects

↑SVR
↓HR (reflex bradycardia)

Dosing

Start 100-200mcg/min then taper down
- 40-60mcg/min works for most

Adverse Effects

Baroreceptor-mediated reflex bradycardia
If extravasates use phentolamine

Notes

Use with caution in pts with spinal cord injury-related bradycardia
Useful for treatment of vasodilatory shock when norepinephrine or dopamine have precipitated tachyarrhythmias
In pts with ↓LV function, unopposed α1 may lead to decreased CO or myocardial ischemia
- However clinical trials do not support these effects when used in clinically appropriate dose range

Vasopressin

Indication

Adjunct for septic shock

Primary Receptor

V1

Relative Effects

↑SVR
↓HR

Dosing

0.04 units/min

Rate of Titration

Fixed dose (do not titrate)

Adverse Effects

Bradycardia
Limb ischemia
Myocardial ischemia
Splanchnic ischemia

Notes

Adverse effects are dose-dependent
Acts on V1 receptors leading to ↑vasoconstriction and

↑sensitivity to catecholamines in pts with shock

Epinephrine

Indication

Anaphylaxis

Primary Receptor

β1
α1
β2

Relative Effects

↑↑↑HR
↑↑↑SV
↑↑↑SVR
Bronchodilation (β2)

Dosing

Dose-dependent effects:
1-10 mcg/min - increase HR and SV
10-20 mcg/min - increase SVR

Rate of Titration

Q2-5 min

Adverse Effects

Tachyarrhythmias
Myocardial ischemia
↑Serum lactate
Splanchnic ischemia

Notes

↑lactate occurs primarily from ↑glycolysis/glycogenolysis within skeletal muscles not tissue hypoperfusion
Use with caution in pts with CAD
- However clinical trials have not demonstrated worsened outcomes

Milrinone

Indication

Primary Receptor

PDE-3 inhibitor

Relative Effects

↑HR
↑↑↑SV
↓SVR

Dosing

Normal renal function:

0.25 - 0.75 mcg/kg/min

Creatinine clearance < 50mL/min, reduce infusion rate

Rate of Titration

Q2H; slower titration rate if renal insufficiency

Adverse Effects

Tachyarrhythmias
Hypotension
Myocardial ischemia

Notes

Can use as alternative to dobutamine in pts with cardiogenic shock and on b-blockers
Causes pulmonary vasodilation, may be good choice in pts with RV failure
↑cAMP in cardiac myocytes and vascular smooth muscle, thereby ↑HR and ↑SV while decreasing ↓SVR
Use with caution in pt with renal failure and hypovolemia

Push Dose Pressors

Use when need temporary BP or CO boost
- Post-intubation hypotension
- Propofol-induced hypotension
- A-fib w/ hypotension
  - Easier to convert well-perfused heart

Epinephrine

Mix 9mL of NS with 1mL of 1:10,000 epi
- Now have 10mL of 10mcg/mL
  - Use 0.5-2mL q2-5min (similar to epi drip)
  - Same as 2% lido with epi
    - Ok to give peripherally
Onset - 1min
Duration - 5-10min

Phenylephrine

Pure alpha (no effect on heart)
Place 1mL of 10mg/mL vial in 100mL NS
- Now have 100mcg/mL
- Draw up 10mL
- Use 0.5-2mL q2-5min (50-200mcg)
Onset - 1min
Duration - 20min

Source

↑ Plöchl, W, D J Cook, T A Orszulak, and R C Daly. 1998. Critical cerebral perfusion pressure during tepid heart operations in dogs. The Annals of thoracic surgery, no. 1. http://www.ncbi.nlm.nih.gov/pubmed/9692450
↑ Emcrit Vasopressor basics http://emcrit.org/podcasts/vasopressor-basics/
↑ Bellomo, Rinaldo, Li Wan, and Clive May. 2008. Vasoactive drugs and acute kidney injury. Critical care medicine, no. 4 Suppl. doi:10.1097/CCM.0b013e318169167f. http://www.ncbi.nlm.nih.gov/pubmed/18382191.
↑ Ricard JD. et al. Central or peripheral catheters for initial venous access of ICU patients: a randomized controlled trial. Crit Care Med. 2013 Sep;41(9):2108-15
↑ ZUCKER G. et al. Treatment of shock and prevention of ischemic necrosis with levarterenol-phentolamine mixtures. Circulation. 1960 Nov;22:935-7.
↑ PELNER L. et al. The problem of levarterenol (levophed) extravasation an experimental study.. Am J Med Sci. 1958 Dec;236(6):755-66
↑ Emcrit peripheral vasopressors http://emcrit.org/podcasts/peripheral-vasopressors-extravasation/

EmCrit Podcast 6

Authors:

[1] Plöchl, W, D J Cook, T A Orszulak, and R C Daly. 1998. Critical cerebral perfusion pressure during tepid heart operations in dogs. The Annals of thoracic surgery, no. 1. http://www.ncbi.nlm.nih.gov/pubmed/9692450

[2] Emcrit Vasopressor basics http://emcrit.org/podcasts/vasopressor-basics/

[3] Bellomo, Rinaldo, Li Wan, and Clive May. 2008. Vasoactive drugs and acute kidney injury. Critical care medicine, no. 4 Suppl. doi:10.1097/CCM.0b013e318169167f. http://www.ncbi.nlm.nih.gov/pubmed/18382191.

[4] Ricard JD. et al. Central or peripheral catheters for initial venous access of ICU patients: a randomized controlled trial. Crit Care Med. 2013 Sep;41(9):2108-15

[5] ZUCKER G. et al. Treatment of shock and prevention of ischemic necrosis with levarterenol-phentolamine mixtures. Circulation. 1960 Nov;22:935-7.

[6] PELNER L. et al. The problem of levarterenol (levophed) extravasation an experimental study.. Am J Med Sci. 1958 Dec;236(6):755-66

[7] Emcrit peripheral vasopressors http://emcrit.org/podcasts/peripheral-vasopressors-extravasation/

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@@ Line 4: / Line 4: @@
 *Heart: MAP of 65 mmHg<ref>Emcrit Vasopressor basics http://emcrit.org/podcasts/vasopressor-basics/</ref>
 *Kidneys: MAP 65-75 mmHg<ref>Bellomo, Rinaldo, Li Wan, and Clive May. 2008. Vasoactive drugs and acute kidney injury. Critical care medicine, no. 4 Suppl. doi:10.1097/CCM.0b013e318169167f. http://www.ncbi.nlm.nih.gov/pubmed/18382191.</ref>
+IV Vasopressor have not been shown to be unsafe when used peripherally<ref>Ricard JD. et al. Central or peripheral catheters for initial venous access of ICU patients: a randomized controlled trial. Crit Care Med. 2013 Sep;41(9):2108-15</ref>
 ==Norepinephrine==