Nama : Sintia
Widyo Wati
NPM : 2A214304
Kelas : 3EB24
NPM : 2A214304
Kelas : 3EB24
The
Pharmacology of Autonomic Failure: From Hypotension to Hypertension
Italo
Biaggioni
Stephanie
W. Watts, ASSOCIATE EDITOR
Pharmacological Reviews January 2017, 69 (1) 53-62;
DOI: https://doi.org/10.1124/pr.115.012161
ArticleInfo
& MetricseLetters PDF
Abstract
Primary
neurodegenerative autonomic disorders are characterized clinically by loss of
autonomic regulation of blood pressure. The clinical picture is dominated by
orthostatic hypotension, but supine hypertension is also a significant problem.
Autonomic failure can result from impairment of central autonomic pathways
(multiple system atrophy) or neurodegeneration of peripheral postganglionic
autonomic fibers (pure autonomic failure, Parkinson’s disease). Pharmacologic
probes such as the ganglionic blocker trimethaphan can help us in the
understanding of the underlying pathophysiology and diagnosis of these
disorders. Conversely, understanding the pathophysiology is crucial in the
development of effective pharmacotherapy for these patients. Autonomic failure
patients provide us with an unfortunate but unique research model characterized
by loss of baroreflex buffering. This greatly magnifies the effect of stimuli
that would not be apparent in normal subjects. An example of this is the discovery
of the osmopressor reflex: ingestion of water increases blood pressure by 30–40
mm Hg in autonomic failure patients. Animal studies indicate that the trigger
of this reflex is related to hypo-osmolality in the portal circulation
involving transient receptor potential vanilloid 4 receptors. Studies in
autonomic failure patients have also revealed that angiotensin II can be
generated through noncanonical pathways independent of plasma renin activity to
contribute to hypertension. Similarly, the mineralocorticoid receptor
antagonist eplerenone produces acute hypotensive effects, highlighting the
presence of non-nuclear mineralocorticoid receptor pathways. These are examples
of careful clinical research that integrates pathophysiology and pharmacology to
advance our knowledge of human disease.
Footnotes
This
work was supported by National Institutes of Health Grants PO1 HL056693, RO1
HL122847, and U54 NS065736
sumber :
http://pharmrev.aspetjournals.org/content/69/1/53
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