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Digoxin, a drug that has been used worldwide for centuries
to treat heart disease, is associated with a significant increase
in deaths in patients with atrial fibrillation
(AF), according to results from a study published online Wednesday 28
November
2012 in the European Heart Journal.1
Foxglove flower
Digoxin, originally extracted from the foxglove plant (digitalis),
increases force of contraction of cardiomyocytes and helps maintain a
more regular rhythm. It is commonly used in AF patients,
and those with heart failure. However, it can be
problematic to use successfully, as there is a narrow dose range at
which
it is effective and beyond which, it can be
dangerous. High levels of digoxin in the blood have been correlated with
an increased
death rate in patients.
Researchers led by Samy Claude Elayi,
associate professor of medicine at the Gill Heart Institute, University
of Kentucky,
USA, analysed data from 4060 AF patients who had
enrolled in the landmark Atrial Fibrillation Follow-up Investigation of
Rhythm
Management (AFFIRM) trial, in order to determine
the relationship between digoxin and deaths in this group of patients.
They found that digoxin was associated
with a 41% increase in deaths from any cause, after controlling for
other medications
and risk factors and that an increase in deaths
occurred regardless of gender or the presence or absence of underlying
heart
failure. Digoxin was also associated with a 35%
increase in deaths from cardiovascular causes, and a 61% increase in
deaths
from arrhythmias.
Prof. Elayi said: ‘These results mean
that among AF patients taking digoxin compared to those not on digoxin
in the AFFIRM
trial, within five years one additional patient
out of six will die from any cause, one additional patient out of eight
will
die from cardiovascular causes, and one
additional patient out of 16 will die from arrhythmias.’
‘These findings call into question the widespread use of digoxin in patients with AF, particularly when used for controlling
AF rate in a similar way as in the AFFIRM trial’.
Until now, there have been limited
data on the use of digoxin in AF patients. ‘Digoxin in AF patients has
hardly been studied’,
said Prof. Elayi. ‘The main prospective
randomized controlled trials available with digoxin were performed in
patients with
heart failure and sinus rhythm, excluding AF
patients’.
As a result of these findings, the authors conclude in their paper: ‘Our study underscores the importance of reassessing the
role of digoxin in the contemporary management of AF in patients with or without HF’.
Prof. Elayi said: ‘These findings mean
that physicians should try to first control a patient's heart rate by
using alternatives
such as, beta-blockers or calcium channel
blockers; if digoxin is used, use a low dose with careful clinical
follow-up, evaluate
potential drug interactions when starting new
medications, and monitor digoxin levels. Patients should be aware of
potential
toxicity and see their physicians immediately in
specific clinical situations, for instance, if they experience
palpitations
or syncope, as these may precede arrhythmic
death’.
The researchers say that the mechanism
by which digoxin increases deaths among patients is unclear. ‘Deaths
from classic cardiovascular
causes, whether due to arrhythmia or not, can
partly but not entirely explain it. This suggests there must be some
additional
mechanism that remains to be identified’, said
Prof. Elayi.
He concluded ‘There is a need for further studies of the drug's use, particularly in systolic heart failure patients and AF
– patients that would in theory, benefit the most from digoxin’.source escardio
Andros Tofield
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