Background and Aim:
The prevalence of cardiomyopathy in cirrhotics remains unknown because of its latent
nature, characterized by blunted contractile responsiveness to stress, altered diastolic
relaxation, and electrophysiological abnormalities. Our aim was to detect early myocardial
dysfunction using new echocardiography technologies in cirrhotic patients and correlating
them to liver stiffness (LS) and severity of liver disease.
Methods:
Consecutive patients with liver cirrhosis without structural heart disease and portal
vein thrombosis were included. Conventional and speckle-tracking echocardiography
(Vendor GE, EchoPAC PC software) were performed by a single investigator (EACVI TTE
certified). Subclinical myocardial dysfunction of left ventricle was defined as average
global longitudinal strain (GLS) < -18% (Lang RM, et al. J Am Soc Echocardiogr 2015;28:1
– 39). LS was assessed by transient elastography (TE, Fibroscan®, Echosens) and share
wave elastography (SWE) from Hitachi (Arietta V70). Reliable results were defined
as median value of 10 valid measurements with an IQR/Med < 30% and expressed in kPa.
The presence of ascites, esophageal varices, splenomegaly and/or thrombocytopenia
were considered as sign of portal hypertension.
Results:
We evaluated 48 patients, but 8 did not fulfilled the inclusion criteria (1 portal
vein thrombosis, 2 coronary artery disease, 1 cor pulmonale and 4 patients with valvular
dysfunction). The final analysis included 40 patients, with mean age of 58.7 ± 11.1
years (67.5% males). Compensated cirrhosis (Child-PughA) was present in 60% of patients,
22.5% were classified as Child-PughB and 17.5% as Child-PughC. LS could be evaluated
in 77.5% of cases by TE and in all patients by HitachiSWE. Slightly reduced left ventricular
ejection fraction (EF) was observed in 10% and diastolic dysfunction in 40% of cases.
Subclinical systolic dysfunction as assessed by GLS was present in 22.5% of cases.
The presence of systolic dysfunction tends to correlate with LS (Table).
Tab. 1
|
Parameter
|
GLS < -18% or reduced EF
(n = 10)
|
GLS ≥ -18% and normal EF
(n = 30)
|
p value
|
|
LS by TE (kPa)
|
41.3 ± 25.1
|
29.1 ± 17.6
|
0.09
|
|
LS by SWE (Hitachi)(kPa)
|
10.8 ± 3.8
|
14.6 ± 6.3
|
0.006
|
|
MELD
|
9.9 ± 3.8
|
10.8 ± 4.7
|
0.48
|
|
Child-Pugh:
– compensated (A)
– decompensated (B+C)
|
7 (70%)
3 (30%)
|
18 (60%)
12 (40%)
|
0.85
0.85
|
|
Portal vein velocity (cm/s)
|
17.1 ± 3.9
|
15.9 ± 2.9
|
0.23
|
|
Signs of portal hypertension
|
6 (60%)
|
23 (57.5%)
|
0.81
|
|
Etiology:
– alcoholic
– other etiologies
|
5 (50%)
5 (50%)
|
19 (63.3%)
11 (36.7%)
|
0.71
0.71
|
|
Age (years)
|
61.5 ± 12.2
|
58.8 ± 10.6
|
0.54
|
|
Gender:
– male
– female
|
5 (50%)
5 (50%)
|
22 (73.3%)
8 (26.7%)
|
0.33
0.33
|
Conclusion:
Clinical or subclinical left ventricular dysfunction was identified in a quarter of
cirrhotic patients and this seems to correlate with LS, but not with the severity
of liver cirrhosis.
