Non-selective α-blockers can cause a much more pronounced reflex
tachycardia than the selective
α1 blockers. Like the selective α1 blockers, phentolamine causes a relaxation of systemic vasculature, leading to
hypotension. This hypotension is sensed by the
baroreceptor reflex, which results in increased sympathetic nerve firing on the heart, releasing
norepinephrine. In response, the
β1 adrenergic receptors on the heart increase their
rate,
contractility, and
dromotropy, which help to offset the decrease in systemic blood pressure. Unlike the α1 selective blockers, phentolamine also inhibits the α2 receptors, which function predominantly as
presynapticnegative feedback for norepinephrine release. By abolishing this negative feedback phentolamine leads to even less regulated norepinephrine release, which results in a more drastic increase in heart rate.[4]
It also has usefulness in the treatment of
cocaine-induced cardiovascular complications, where one would generally avoid
β-blockers (e.g.
metoprolol), as they can cause unopposed α-adrenergic mediated
coronary vasoconstriction, worsening myocardial ischemia and hypertension.[6][7] It is important to note that phentolamine is not a first-line agent for this indication. Phentolamine should only be given to patients who do not fully respond to
benzodiazepines,
nitroglycerin, and
calcium channel blockers.[8][9]
When given by injection it causes blood vessels to
dilate, thereby increasing blood flow. When injected into the penis (intracavernosal), it increases blood flow to the penis, which results in an erection.[10]
It may be stored in
crash carts to counteract severe peripheral vasoconstriction secondary to
extravasation of peripherally placed
vasopressor infusions, typically of
norepinephrine.
Epinephrine infusions are less vasoconstrictive than norepinephrine as they primarily stimulate β receptor more than α receptors, but the effect remains dose-dependent.
Phentolamine is marketed in the dental field as a local anesthetic reversal agent. Branded as OraVerse, it is a phentolamine mesylate injection designed to reverse the local vasoconstrictor properties used in many local anesthetics to prolong anesthesia.[12]
Chemistry
Phentolamine can be synthesized by alkylation of 3-(4-methylanilino)phenol using 2-chloromethylimidazoline:[13][14]
^Jewell JR, Longworth DL, Stoller JK, Casey D (2003). The Cleveland Clinic internal medicine case reviews. Hagerstown, MD: Lippincott Williams & Wilkins. p. 32.
ISBN0-7817-4266-8.
^Shen H (2008). Illustrated Pharmacology Memory Cards: PharMnemonics. Minireview. p. 14.
ISBN978-1-59541-101-3.
^Tuncel M, Ram VC (2003). "Hypertensive emergencies. Etiology and management". American Journal of Cardiovascular Drugs: Drugs, Devices, and Other Interventions. 3 (1): 21–31.
doi:
10.2165/00129784-200303010-00003.
PMID14727943.
S2CID1993954.
^Schurr JW, Gitman B, Belchikov Y (December 2014). "Controversial therapeutics: the β-adrenergic antagonist and cocaine-associated cardiovascular complications dilemma". Pharmacotherapy. 34 (12): 1269–1281.
doi:
10.1002/phar.1486.
PMID25224512.
S2CID5282953.
^Freeman K, Feldman JA (February 2008). "Cocaine, myocardial infarction, and beta-blockers: time to rethink the equation?". Annals of Emergency Medicine. 51 (2): 130–134.
doi:
10.1016/j.annemergmed.2007.08.020.
PMID17933425.
^Hollander JE, Henry TD (February 2006). "Evaluation and management of the patient who has cocaine-associated chest pain". Cardiology Clinics. 24 (1): 103–114.
doi:
10.1016/j.ccl.2005.09.003.
PMID16326260.