Whither digitalis? What we can still learn from cardiotonic steroids about heart failure and hypertension.
Mordecai P BlausteinStephen S GottliebJohn M HamlynFrans H H LeenenPublished in: American journal of physiology. Heart and circulatory physiology (2022)
Cloning of the "Na + pump" (Na + ,K + -ATPase or NKA) and identification of a circulating ligand, endogenous ouabain (EO), a cardiotonic steroid (CTS), triggered seminal discoveries regarding EO and its NKA receptor in cardiovascular function and the pathophysiology of heart failure (HF) and hypertension. Cardiotonic digitalis preparations were a preferred treatment for HF for two centuries, but digoxin was only marginally effective in a large clinical trial (1997). This led to diminished digoxin use. Missing from the trial, however, was any consideration that endogenous CTS might influence digitalis' efficacy. Digoxin, at therapeutic concentrations, acutely inhibits NKA but, remarkably, antagonizes ouabain's action. Prolonged treatment with ouabain, but not digoxin, causes hypertension in rodents; in this model, digoxin lowers blood pressure (BP). Furthermore, NKA-bound ouabain and digoxin modulate different protein kinase signaling pathways and have disparate long-term cardiovascular effects. Reports of "brain ouabain" led to the elucidation of a new, slow neuromodulatory pathway in the brain; locally generated EO and the α2 NKA isoform help regulate sympathetic drive to the heart and vasculature. The roles of EO and α2 NKA have been studied by EO assay, ouabain-resistant mutation of α2 NKA, and immunoneutralization of EO with ouabain-binding Fab fragments. The NKA α2 CTS binding site and its endogenous ligand are required for BP elevation in many common hypertension models and full expression of cardiac remodeling and dysfunction following pressure overload or myocardial infarction. Understanding how endogenous CTS impact hypertension and HF pathophysiology and therapy should foster reconsideration of digoxin's therapeutic utility.
Keyphrases
- blood pressure
- heart failure
- clinical trial
- hypertensive patients
- acute heart failure
- left ventricular
- heart rate
- signaling pathway
- protein kinase
- white matter
- poor prognosis
- resting state
- oxidative stress
- type diabetes
- high throughput
- cardiac resynchronization therapy
- cerebral ischemia
- skeletal muscle
- randomized controlled trial
- transcription factor
- blood glucose
- replacement therapy
- open label
- pi k akt
- brain injury
- electronic health record
- combination therapy
- adverse drug
- double blind