BMJ 2003;327:78-79 (12 July), doi:10.1136/bmj.327.7406.78
Paper
Prognosis in heart failure with preserved left ventricular systolic function: prospective cohort study
Philip A MacCarthy, consultant1,
Mark T Kearney, senior lecturer1,
James Nolan, consultant2,
Amanda J Lee, statistician3,
Robin J Prescott, statistician3,
Ajay M Shah, British Heart Foundation professor1,
W Paul Brooksby, consultant cardiologist4,
Keith A A Fox, British Heart Foundation professor5
1 Department of Cardiology, Guy's, King's, and St Thomas's School of Medicine,
London SE5 9PJ,
2 North Staffordshire Cardiac Centre, Stoke on Trent, ST4 6QG,
3 Medical Statistics Unit, University of Edinburgh, Edinburgh EH3 9YW,
4 Pontefract and Wakefield Hospitals, Pontefract WF8 1PL,
5 Department of Cardiology, University of Edinburgh
Correspondence to: M T Kearney
mark.kearney{at}kcl.ac.uk
Introduction
Chronic heart failure due to left ventricular systolic impairment
is
characterised by a poor prognosis and abnormalities of cardiac
structure,
autonomic and neurohumoral function, and fluid and
electrolyte homoeostasis,
all of which are thought to contribute
to the pathophysiology of this
condition. However, some studies
have found that 30-50% of all patients with
chronic heart failure
have preserved left ventricular systolic
function.
1 Despite
this, the natural course of the condition in these patients
is controversial,
and their pathophysiological characterisation
poor. As a result, optimum
treatment strategies are unclear.
We looked at five year mortality in patients
recruited to a
large cohort study of chronic heart failure, comparing those
having impairment of left ventricular function with those having
preserved
function.
Participants, methods, and results
We have published details of the United Kingdom heart failure
evaluation
and assessment of risk trial (UK-HEART)
previously.
2
3 Five hundred and fifty
three unselected ambulant patients
were prospectively recruited from April
1993 to December 1995.
Patients were enrolled if they had had stable,
symptomatic
chronic heart failure for at least three months (other primary
causes of symptoms were excluded). As well as symptoms of chronic
heart
failure, all patients had evidence of cardiac dysfunction
documented at the
index assessment by one or more of the following:
systolic left ventricular
dysfunction on echocardiography or
radionuclide ventriculography;
cardiothoracic ratio > 0.55;
and pulmonary venous congestion and/or upper
lobe venous diversion
on chest radiography. Left ventricular hypertrophy was
assessed
from electrocardiography (on the basis of Sokolow-Lyon criteria).
All
patients had 24 hour ambulatory monitoring for arrhythmia
analysis and
assessment of heart rate variability. A global
index of total heart rate
variabilitythe standard deviation
of all normal R-R intervals (SDNN)
(with a low value indicating
a disadvantageous neurohumoral
profile)
was derived from
this recording. All patients were
logged on the NHS Central
Register (part of the Office of Population Censuses
and Surveys),
which notified the investigators when patients died.
Most studies confirm that patients with an ejection fraction
50% can
be considered to have preserved left ventricular systolic function. We
therefore chose this value to dichotomise patients into those with preserved
(
50%) and those with impaired (< 50%)
function.4
In all, 522 patients had adequate measurements of ejection fraction, of
whom 163 (31%) had values
50% and 359 (69%) < 50%. Information on
deaths was recorded to April 2000, allowing five year survival status to be
determined for all patients. The
table shows the characteristics
of the two groups and statistical methods.
View this table:
[in this window]
[in a new window]
|
Characteristics of 522 patients with chronic heart failure and preserved or
impaired left ventricular systolic function. Values are means (standard
deviations) unless stated otherwise
|
|
Five year mortality was substantial in both groups but significantly
greater in patients with impaired left ventricular systolic function (41.5%
v 25.2%, P < 0.001). Twenty five per cent of patients with
preserved function had non-sustained ventricular tachycardia. Both groups had
similar SDNN measurements, which were lower than previously shown in age
matched healthy control
subjects.5
Comment
Mortality is significantly greater in patients with chronic
heart failure
and impaired left ventricular systolic function
than in those with preserved
systolic function. However, even
the patients with preserved systolic function
have a 25% five
year mortality. Therefore, clinical heart failure itself has
a
poor long term prognosis, irrespective of electrocardiographically
determined
left ventricular systolic function. Autonomic function
was abnormal in both
groups, and this, allied to the presence
of non-sustained ventricular
tachycardia and left ventricular
hypertrophy, may contribute to the high
mortality found in
the patients with preserved systolic function.
Our findings add to those of a recent study by Kitzman et al, who found
that patients with chronic heart failure and preserved left ventricular
systolic function have similar, but not as severe, pathophysiological
derangements to those with impaired systolic
function.4 These and
our data suggest that established treatments for systolic heart failure may
also have a role in patients with chronic heart failure and preserved left
ventricular systolic function.
A graph showing
survival curves is available on
bmj.com
Contributors: PAM and MTK conceived the original idea, did the retrieval,
analysis, and interpretation of the data, and wrote the paper. MTK helped to
collect the raw data. KAAF, JN, and WPB were responsible for the original
concept of the UK-HEART study, designed the database, and collected the data
on patients; they also reviewed and revised the current paper. AJL and RJP
helped with data acquisition and advised on statistical analysis. AJL did a
large part of the statistical analysis. AMS helped with the conception of this
project, the study design, the interpretation of data, and the revision of the
manuscript. MTK is the guarantor for the paper.
Funding: PAM was the recipient of an advanced training scholarship from the
British Heart Foundation; MTK is a British Heart Foundation (BHF) intermediate
research fellow; and AMS and KAAF hold BHF chairs in cardiology.
Competing interests: None declared.
Ethical approval: Local ethics committees at each participating hospital
approved the protocol, and informed written consent was obtained from all
patients.
References
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(Accepted April 15, 2003)

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