SciELO - Scientific Electronic Library Online

 
vol.109 número5Aplicación de la clasificación de Neff modificada en el manejo de la diverticulitis agudaHepatitis aguda virus E autóctona: Un diagnóstico en aumento. Análisis clínico-epidemiológico de nuestra experiencia índice de autoresíndice de assuntospesquisa de artigos
Home Pagelista alfabética de periódicos  

Serviços Personalizados

Journal

Artigo

Indicadores

Links relacionados

  • Em processo de indexaçãoCitado por Google
  • Não possue artigos similaresSimilares em SciELO
  • Em processo de indexaçãoSimilares em Google

Compartilhar


Revista Española de Enfermedades Digestivas

versão impressa ISSN 1130-0108

Rev. esp. enferm. dig. vol.109 no.5 Madrid Mai. 2017

https://dx.doi.org/10.17235/reed.2017.4219/2016 

ORIGINAL PAPERS

 

The utility of the macro-aggregated albumin lung perfusion scan in the diagnosis and prognosis of hepatopulmonary syndrome in cirrhotic patients candidates for liver transplantation

 

 

Israel Grilo1, Juan Manuel Pascasio2, Juan Luis Tirado3, Francisco Jesús López-Pardo4, Francisco Ortega-Ruiz5, José Manuel Sousa2, María José Rodríguez-Puras4, María Teresa Ferrer2, Miguel Ángel Gómez-Bravo6 and Antonio Grilo7

1Department of Digestive Diseases. Hospital de Alta Resolución de Écija. Sevilla, Spain.
2Department of Digestive Diseases. Hospital Virgen del Rocío. IBIS, CIBERehd. Sevilla, Spain.
3Department of Nuclear Medicine Department. Hospital Virgen del Rocío. Sevilla, Spain.
4Department of Heart Diseases. Hospital Virgen del Rocío. Sevilla, Spain.
5Department of Respiratory Diseases. Hospital Virgen del Rocío. Sevilla, Spain.
6Department of Hepato-Biliary-Pancreatic Surgery and Liver Transplantation. Hospital Virgen del Rocío. Sevilla, Spain.
7Department of Internal Medicine. Hospital Virgen de Valme. Sevilla, Spain

Author's contribution: Israel Grilo and Juan Manuel Pascasio contributed to the manuscript equally.

Ethical approval: All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Helsinki declaration and its later amendments or comparable ethical standards.

Correspondence

 

 


ABSTRACT

Background: The macro-aggregated albumin lung perfusion scan (99mTc-MAA) is a diagnostic method for hepatopulmonary syndrome (HPS).
Aim: To determine the sensitivity of 99mTc-MAA in diagnosing HPS, to establish the utility of 99mTc-MAA in determining the influence of HPS on hypoxemia in patients with concomitant pulmonary disease and to determine the correlation between 99mTc-MAA values and other respiratory parameters.
Methods: Data from 115 cirrhotic patients who were eligible for liver transplantation (LT) were prospectively analyzed. A transthoracic contrast echocardiography and 99mTc-MAA were performed in 85 patients, and 74 patients were diagnosed with HPS.
Results: The overall sensitivity of 99mTc-MAA for the diagnosis of HPS was 18.9% (14/74) in all of the HPS cases and 66.7% (4/6) in the severe to very severe cases. In HPS patients who did not have lung disease, the degree of brain uptake of 99mTc-MAA was correlated with the alveolar-arterial oxygen gradient (A-a PO2) (r = 0.32, p < 0.05) and estimated oxygen shunt (r = 0.41, p < 0.05) and inversely correlated with partial pressure of arterial oxygen (PaO2) while breathing 100% O2 (r = -0.43, p < 0.05). The 99mTc-MAA was positive in 20.6% (7/36) of the patients with HPS and lung disease. The brain uptake of 99mTc-MAA was not associated with mortality and normalized in all cases six months after LT.
Conclusions: The 99mTc-MAA is a low sensitivity test for the diagnosis of HPS that can be useful in patients who have concomitant lung disease and in severe to very severe cases of HPS. It was not related to mortality, and brain uptake normalized after LT.

Key words: Cirrhosis. Ascites. Contrast echocardiography. Pulmonary vascular diseases. Perioperative care.


 

Introduction

HPS is characterized by the presence of intrapulmonary vascular dilations (IPVD), which cause a physiologic shunt that decreases the alveolar-arterial oxygen gradient (A-a PO2) and can produce hypoxemia in patients with liver disease (1,2). Thoracic contrast echocardiography (TCE), which is a non-invasive and sensitive method for diagnosing IPVD, is considered to be the gold standard for diagnosing HPS (1,3). The 99mTc-MAA can also diagnose and quantify IPVD, but its sensitivity is lower; however, there are few studies that have compared the two techniques (4-8).

The ability of this method to quantify IPVD by determining the brain uptake of 99mTc-MAA makes it attractive for stratifying the severity of HPS. In this context, there are some studies linking the increased brain uptake of 99mTc-MAA to increased mortality among HPS patients (6-8). In an attempt to validate its ability to quantify IPVD, its correlations with different respiratory parameters that could measure HPS severity, such as the PaO2 while breathing 100% oxygen, A-a O2, estimated degree of oxygen shunt and corrected diffusing capacity for carbon monoxide (DLCOco), have been analyzed; however, the information is scarce and inconclusive (5-9).

When HPS was first defined, no existing concomitant cardiopulmonary diseases were required for its diagnosis (10). Subsequently, it was observed that HPS could be present in patients with lung disease. Because IPVD are frequent in cirrhotic patients without HPS, they are often detected by TCE, and the problem arises of determining whether hypoxemia in patients with pulmonary disease is due to IPVD or to HPS (3). It has been speculated that 99mTc-MAA may be useful for assessing the contribution of HPS to hypoxemia in patients with concomitant pulmonary disease (5).

LT is capable of reversing the HPS quickly, except for some of its parameters, such as DLCOco (11-16). There are scarce data on the changes in the uptake of 99mTc-MAA in the brain after LT (8).

The objectives of our study were the following: a) to determine the sensitivity of 99mTc-MAA for diagnosing HPS in cirrhotic patient candidates for LT; b) to establish the utility of 99mTc-MAA in determining the influence of HPS on hypoxemia in patients with concomitant pulmonary disease; and c) to examine the correlation between 99mTc-MAA values and other respiratory parameters that can define HPS severity and the influence of 99mTc-MAA values on pre- and post-LT survival.

 

Materials and methods

Selection of patients

All of the adult patients with cirrhosis who were evaluated for a first LT at the Hospital Universitario Virgen del Rocío in Seville (Spain) for a period of five years were prospectively included in the study. Candidates who were evaluated for re-transplantation were excluded. To be included in the study, patients signed an informed consent form which was in accordance with the ethical guidelines of the Declaration of Helsinki and was approved by the ethics committee of the hospital. Patients whose results from an arterial blood gas analysis in the supine position were compatible with a diagnosis of HPS were selected. These results are part of a larger study, and some of its findings have been previously published (16).

Hepatopulmonary syndrome

Blood gas studies

An arterial blood gas analysis was performed while the patients were in the supine position and breathing room air. The samples were analyzed using a gasometer (ABL-500 gasometer, Radiometer, Copenhagen, Denmark), and the A-a PO2 was calculated using the following formula: A-a PO2 = [(BP - 47) FIO2 - PaCO2/0.8] - PaO2, where BP is barometric pressure, FIO2 is the fraction of inspired O2, PaCO2 is the partial pressure of carbon dioxide, and PaO2 is the partial pressure of arterial oxygen. The intrapulmonary shunt size was determined by studying the ratio of PaO2 in the arterial blood when a second blood gas analysis was performed while the patients were breathing with FIO2 = 1 (100% O2) for 15 minutes through a face mask with a reservoir. The shunt was determined from the nomogram devised by Chiang (17).

Transthoracic contrast echocardiography

All of the patients whose blood gas analysis results were compatible with a HPS diagnosis received a TCE, which was performed by two cardiologists from our hospital. A 10 ml saline serum solution was shaken in two 10 ml syringes that were connected to a three-way valve. The solution was injected into a peripheral vein of the upper limb through a 20G catheter. An apical four-chamber image was taken with a variable-frequency transducer (2.1-4.2 MHz) that had a Philips iE-33 scanner (Royal Philips Electronics, Amsterdam, the Netherlands) to detect the presence of micro-bubbles. The presence of micro-bubbles between the fourth and sixth beat after the injection in the left chambers was considered as a positive result.

Macro-aggregated albumin lung perfusion scan

A 99mTc-MAA was performed in the patients whose blood gas analysis results were compatible with a HPS diagnosis. The scan was performed by injecting 100,000 particles (1.3 to 2.1 mCi in size) of albumin macro-aggregates labeled with Tc 99 (TechneScan LyoMAA; Tyco Healthcare, Madrid, Spain; 95% of the particles have a diameter between 10 and 100 µm) through a peripheral vein while the patient was in the sitting position. Then, the patient was placed in the supine position, and images were obtained of each half of the head and of the anterior and posterior thorax using a parallel hole collimator, with a 20% window centered at the technetium peak of 140 keV for five minutes, and a gamma camera (Apex SPX Helix, Elscint, Haifa, Israel). The regions of interest were drawn around the brain and lungs, and the radiation counts of those areas were recorded. The extrapulmonary shunt fraction, assuming that 13% of the cardiac output is delivered to the brain, was calculated using the geometric mean of technetium (GMT) counts around the brain and lung in the following formula: (GMTbrain)/(GMTbrain + GMTlung). The scan was considered to be positive when the fraction of the extrapulmonary shunt in the brain was greater than or equal to 6%; the shunt fraction was quantitatively recorded in all cases (4,5).

Hepatopulmonary syndrome and orthodeoxia criteria

HPS was defined according to the following criteria: a) PaO2 < 70 mmHg and/or A-a PO2 ≥ 20 mmHg while the patient was in a supine position (6,8,11,18,19); b) a positive TCE; and c) evidence of cirrhotic liver disease. Patients were classified into the following four degrees of HPS severity according to the level of PaO2: mild (PaO2 ≥ 80 mmHg), moderate (PaO2 < 80 mmHg and ≥ 60 mmHg), severe (PaO2 < 60 mmHg and ≥ 50 mmHg), and very severe (PaO2 < 50 mmHg) (1). Orthodeoxia occurred when arterial blood gas PaO2 in seated patients (after spending at least 20 minutes standing or seated) was reduced by ≥ 5% or ≥ 4 mmHg compared with the values for patients in the supine position.

Studies of lung function

The patients performed spirometric tests according to the Spanish Society of Pneumology and Thoracic Surgery (SEPAR) recommendations, and values from a Mediterranean population were used as a reference. A pneumotachograph spirometer (Masterlab, Erich Jaeger GmbH, Würzburg, Germany) was used for the tests. Forced vital capacity (FVC), forced expiratory volume in one second (FEV1) and the FEV1/FVC ratio were recorded. Patients were considered to have obstructive lung disease when the FEV1/FVC ratio was less than 70% or when the FEV1 was less than 80% of the reference value. Patients were diagnosed with restrictive lung disease when their FVC was less than 80% from baseline or with mixed lung disease when they had both criteria. DLCO values (expressed in mmol/min/kPa) and DLCO values adjusted for alveolar volume (expressed in mmol/min/kPa/l) and hemoglobin (DLCOco) were obtained. All lung function tests followed SEPAR recommendations and used reference values for the Mediterranean population.

Post LT follow-up

A 99mTc-MAA was performed in patients with HPS every three to six months after LT until the values returned to normal.

Survival analysis

The date of death, transplantation or last follow-up at the hospital before the end of the study was considered to be the last date of the transplant waiting list period. The date of death or last visit to the hospital before the end of the study was considered to be the last date in the post-transplant period.

Statistical analysis

Continuous variables are expressed as medians and interquartile ranges (IQRs), and categorical variables are expressed as numbers (n) and percentages (%). Comparisons between categorical variables were performed using the Chi-squared test or Fisher's exact test, and comparisons between continuous variables were performed with Student's t test or Mann-Whitney test. The relationships between variables were assessed by the Spearman correlation coefficient. Survival analyses were performed using the Kaplan-Meier method and Cox regression. The statistical analysis was performed with SSPS version 15.0 (SSPS Inc., Chicago, IL, USA).

 

Results

A total of 316 of the 367 patients examined were enrolled in the study. A total of 115 (36.4%) patients had blood gas analysis results that were compatible with HPS, and each of these patients received a TCE. A 99mTc-MAA was carried out in 85 (73.9%) patients who had alterations in their blood gas analysis that were compatible with HPS. There were no significant differences in clinical findings between the two groups except the presence of HPS was more frequent in the study sample. Figure 1 shows an outline of the study.

 

 

Patient characteristics

The study sample included 115 patients; 92 (80%) were men and 23 (20%) were women. The median age was 55 years (IQR: 49-60). The etiology of cirrhosis was alcohol in 61 (53%) patients, hepatitis C virus (HCV) in 11 (9.6%) patients, alcohol and HCV in 17 (14.8%) patients, hepatitis B virus (HBV) in 4 (3.5%) patients, HBV and alcohol in 7 (6.1%) patients, and other causes in 15 (13%) patients. The distribution of cirrhosis severity according to the Child-Pugh classification was the following: class A, 17 (14.8%) patients; class B, 47 (40.9%) patients; and class C, 51 (44.3%) patients. The median model for end-stage liver disease (MELD) index was 16 (IQR: 12-19). Eighty-one (70.4%) patients were diagnosed with HPS.

Comparative study between 99mTc-MAA and TCE for the diagnosis of HPS

A 99mTc-MAA and a TCE were performed in 85 patients who had arterial blood gas analysis results that were compatible with HPS. The time interval between the two procedures was less than one month. No adverse events were observed during either procedure. Seventy-four (87%) patients were diagnosed with HPS according to an arterial blood gas analysis (59/74) (79.7%) with only an A-a PO2 ≥ 20 mmHg without PaO2 < 70 mmHg) and a positive TCE result. The following distribution of HPS severity was observed: 29 mild cases (39.2%), 39 moderate cases (52.7%), five severe cases (6.8%), and one very severe case (1.4%). Only 14 (18.9%) patients with HPS had a positive 99mTc-MAA; thus, the overall sensitivity of the 99mTc-MAA in diagnosing HPS was 19%. The specificity was 100%, none of the 11 patients with negative TCE had a positive 99mTc-MAA. The negative predictive value was 15%, and the positive predictive value was 100%. The 99mTc-MAA was positive in 10/68 (14.7%) mild to moderate cases of HPS versus 4/6 (66.7%) severe or very severe cases; this difference was statistically significant (p = 0.01).

A statistically significant association (p < 0.05) was observed between the 99mTc-MAA and platelet count, PaCO2 in the supine position, PaO2 while breathing 100% oxygen, the degree of estimated oxygen shunt and DLCOco. 99mTc-MAA was also associated with hypersplenism and orthodeoxia; however, these associations were on the verge of statistical significance (p = 0.06). In the multivariate study, DLCOco and PaCO2 in the supine position remained independent predictors of a positive 99mTc-MAA (Table I).

 

 

Correlation of brain uptake in 99mTc-MAA with variables associated with HPS

The brain uptake of 99mTc-MAA in patients with HPS was not significantly correlated with PaO2 while breathing room air, A-a PO2, or DLCOco. However, the brain uptake of 99mTc-MAA was inversely correlated with PaO2 while breathing 100% oxygen (r = -0.42, p < 0.01) and PaCO2 (r = -0249, p < 0.05), and was positively correlated with the degree of oxygen shunt (r = 0.42, p < 0.01). When exclusively analyzing HPS patients who did not have underlying lung disease, a statistically significant weak positive correlation was observed with A-a PO2 (r = 0.32, p < 0.05) and the degree of oxygen shunt (r = 0.41, p < 0.05), and an inverse correlation was observed with PaO2 while breathing 100% O2 (r = -0.43, p < 0.05). However, the brain uptake of 99mTc-MAA was not correlated with PaO2 while breathing room air, PaCO2, or DLCOco (Fig. 2).

 

 

Correlation between the brain uptake of 99mTc-MAA and the parameters of liver function and of portal hypertension

The brain uptake of 99mTc-MAA was not correlated with the Child-Pugh classification of cirrhosis severity, MELD index or levels of total bilirubin, albumin, international normalized ratio (INR) and platelet count.

Role of 99mTc-MAA in patients with concomitant lung disease

Among the HPS patients, there were no significant differences in a positive 99mTc-MAA between the patients who had concomitant respiratory disease and those who did not (p = 0.77). 99mTc-MAA was positive in seven of the 34 (20.6%) patients who had coexisting respiratory disease and in seven of the 40 (17.5%) without respiratory disease. When stratified by the severity of HPS, the 99mTc-MAA was positive in 4/25 (13.8%) mild or moderate cases versus 3/5 (60%) severe or very severe cases (p = 0.048). 99mTc-MAA was negative in 27 of the 34 (79.4%) patients who had coexisting respiratory disease and in 33 of 40 (82.5%) without respiratory disease.

Statistically significant differences were observed between a positive 99mTc-MAA and the value of PaO2 while breathing 100% O2, degree of estimated oxygen shunt and DLCOco in patients with HPS and concomitant lung disease. These differences were not observed among patients who had HPS but did not have pulmonary disease (Table II).

 

 

Pre-LT and post-LT mortality of HPS patients

Mortality in the pre-transplantation or the post-transplantation periods was not associated with positive 99mTc-MAA results, shunt values obtained by 99mTc-MAA, PaO2 while breathing room air or 100% oxygen, A-a PO2, degree of oxygen shunt calculated, or DLCO. These associations were also negative when the two periods were jointly analyzed. Two patients with 99mTc-MAA > 20% received transplants, and one of them died.

Changes in 99mTc-MAA post- transplantation

Ten patients who had HPS and a positive 99mTc-MAA result received a transplant, and two of them died. A new 99mTc-MAA was performed during the first six months post-LT in six of the eight survivors, and the result was negative for all of them.

 

Discussion

This study prospectively analyzed the utility of the standardized 99mTc-MAA for the diagnosis and prognosis of HPS and its relationship to other respiratory parameters associated with. This makes it one of the largest collections studied to date in the literature.

99mTc-MAA sensitivity in the diagnosis of HPS

This study found that the 99mTc-MAA has a low sensitivity (19%) for diagnosing HPS compared to the sensitivity of TCE. However, the sensitivity changed with the severity of HPS; it increased to 66.7% in severe and very severe cases. The 99mTc-MAA results were never positive when the TCE results were negative. This low sensitivity is also observed in HPS patients without lung disease. In this analysis, the confusing implication of lung disease on oxygenation abnormality and possible false positive cases of HPS (hypoxemia or altered A-a PO2 caused by lung disease and positive TCE) are avoided.

Abrams et al. established the diagnostic utility of 99mTc-MAA in adults with HPS through two studies published in 1995 and 1998 (4,5). In the first study, the 99mTc-MAA was demonstrated to be negative (i.e., it established a minor shunt fraction equal to 6%) in healthy patients and in patients who had lung disease and hypoxemia without cirrhosis. Moreover, 99mTc-MAA was also negative in normoxemic cirrhotic patients who had a positive TCE result, and 99mTc-MAA was found to have a negative predictive value of 93% (4). The second study analyzed 25 patients with HPS, and 21 (84%) of them had severe or very severe HPS (10 severe and 11 very severe). The study found that the 99mTc-MAA had a sensitivity of 84%, with the four negative cases corresponding to a moderate case and three mild cases. The 99mTc-MAA was also found to be negative in hypoxemic patients who had lung disease but did not have cirrhosis. The study concluded that a positive 99mTc-MAA is specific to the presence of severe or very severe HPS (5). Krowka et al. also found that the 99mTc-MAA had a very high sensitivity of 96% in a group of 25 patients with HPS; 19 (76%) of the patients had severe or very severe HPS (6). In a sample of 25 HPS patients, in which 15 (60%) had severe or very severe HPS, Arguedas et al. obtained a sensitivity of 76% (7). Swanson et al. studied the use of 99mTc-MAA in 37 patients with HPS; although they did not specify its diagnostic sensitivity, they observed that the 99mTc-MAA was never negative if patient hypoxemia was less than or equal to 50 mmHg (8).

The sensitivity of the 99mTc-MAA in our study is significantly lower than that reported in the literature. This can be explained by a difference in the characteristics of the HPS patient populations; our sample predominantly consisted of mild to moderate HPS cases, whereas the samples in the other studies mainly consisted of severe or very severe cases. This difference can be explained by the selection of HPS patients. In our study, HPS patients were selected in a systematic way as part of the pre-transplantation evaluation. In contrast, the other studies were performed in clinical patients or the population characteristics were not specified. In our study and in the study by Abrams et al., the 99mTc-MAA was observed to be positive much more frequently in patients with severe or very severe HPS than in patients with mild to moderate HPS. However, the 99mTc-MAA was positive in 14.7% of mild to moderate cases in our study, which indicates that a positive 99mTc-MAA result is not specific to the presence of severe or very severe HPS, as had previously been indicated (5).

In our study, the low sensitivity of 99mTc-MAA and the significant number of HPS cases that were not diagnosed by 99mTc-MAA despite a positive TEC suggest against the systematic use of the 99mTc-MAA as a diagnostic tool for HPS. Another issue is its use as a prognostic measure or in assessing the role of HPS in patients with cirrhosis and concomitant lung disease; this will be discussed below.

Correlation of the brain uptake in 99mTc-MAA with respiratory function parameters associated with HPS

A weak positive correlation was observed between the degree of brain uptake of 99mTc-MAA and the A-a PO2 and calculated degree of oxygen shunt, whereas an inverse correlation was found with PaO2 while breathing 100% O2. The degree of brain uptake of 99mTc-MAA was not correlated with PaO2 while breathing room air or with DLCOco. The calculated degree of oxygen shunt and PaO2 while breathing 100% O2 were also associated with a positive 99mTc-MAA in the univariate analysis but not in the multivariate analysis.

In this sense, the results are contradictory between the different studies. Abrams et al. found a strong negative correlation with PaO2 while breathing room air but not with PaO2 while breathing 100% O2 in a sample of 21 patients (6). Krowka et al., however, observed a negative correlation with PaO2 while breathing 100% O2 but a positive correlation with A-a PO2 (similar to our study) and with PaO2 while breathing room air. There was no correlation observed with DLCO (7). Arguedas et al. observed a strong negative correlation with PaO2 while breathing room air, a positive correlation with A-a PO2 and, similar to our study, a weak correlation with PaO2 while breathing 100% O2 (8). Finally, Swanson et al. found the same correlations with PaO2 while breathing room air, A-a PO2 and PaO2 while breathing 100% O2 (9). The 99mTc-MAA was not correlated with the calculated degree of oxygen shunt in any of the studies (Table III).

 

 

One explanation of why the brain uptake of 99mTc-MAA was not correlated with PaO2 in the supine position and, to a lesser extent, with A-a PO2 in our study is, once again, the difference in the severity of HPS in our patient sample compared to that of the samples in other studies. Considering the results of these studies together, we observe that the correlation between the estimated shunt by 99mTc-MAA and PaO2 while breathing 100% oxygen is independent of HPS severity; however, A-a PO2 and PaO2 while breathing room air are dependent on the severity of HPS.

Correlation with parameters of liver function and portal hypertension

The level of brain uptake of 99mTc-MAA was not correlated with any parameters of liver function or the indirect parameters of portal hypertension. This finding is consistent with those of other studies (5,6,20).

Utility of 99mTc-MAA in patients with HPS and concurrent respiratory pathology

The 99mTc-MAA was positive in the same proportion of HPS patients with and without respiratory disease. This comparison has not been previously conducted, and it allows us to conclude that the results of the 99mTc-MAA are not influenced by the presence of concomitant lung disease, even in patients with HPS. The negative results of the 99mTc-MAA in hypoxemic and non-cirrhotic lung disease (5) patients have been previously described. This observation is important because the use of 99mTc-MAA in patients with HPS who also have lung disease is recommended to assess the degree to which HPS influences hypoxemia in these patients. We observed that the 99mTc-MAA was positive in 20% of HPS patients with coexisting lung disease and increased to 60% in severe and very severe cases. Although this observation is based on few patients, it supports the recommendation of using 99mTc-MAA to detect patients with HPS and coexisting lung disease, especially in patients with severe or very severe HPS. A positive 99mTc-MAA result supports the diagnosis of HPS. Another issue is how a negative 99mTc-MAA result in such patients should be interpreted. This may entail cirrhotic patients with mild or moderate HPS, in whom the sensitivity of 99mTc-MAA is low. Another possibility is that patients do not really have HPS, but that their hypoxemia is due to concomitant lung disease. Other studies have shown that a positive TCE result is more frequent than the actual presence of HPS; thus, patients with concomitant lung disease and hypoxemia may be misdiagnosed with HPS (8,21-23). In this sense, other parameters suggestive of HPS should be evaluated by diagnostic tests. In the group of HPS patients with concomitant lung disease, our study found statistically significant differences in the values of DLCOco, calculated shunt and PaO2 while breathing 100% oxygen, between the patients with positive and negative 99mTc-MAA. These findings suggest that hypoxemia in patients with negative 99mTc-MAA results is not associated with the presence of HPS. These differences were not observed in patients without concomitant lung disease. Krowka et al. also found significantly lower levels of PaO2 while breathing 100% oxygen in patients who had lung disease and HPS compared to those of HPS patients without lung disease; however, they did not link it to 99mTc-MAA results (6).

Pre- and post-LT mortality

We found no association between overall mortality and the levels of 99mTc-MAA, PaO2 while breathing room air or 100% oxygen, degree of calculated shunt, nor DLCOco, in HPS patients who were either on the active transplant waiting list or in the post-transplantation period. Arguedas et al. and Swanson et al. found that a lower PaO2 and higher brain uptake of 99mTc-MAA were associated with increased post-transplantation mortality (7,8). However, Gupta et al. did not observe increased post-transplantation mortality in patients with severe HPS compared to the other HPS patients (14). Iyer et al. observe that survival after LT was not associated with PaO2 levels at the time of HPS diagnosis (24). In our study, two patients who had a brain uptake of 99mTc-MAA > 20% received a transplant, and one of them died. Therefore, we can neither affirm nor deny the prognostic value of 99mTc-MAA in patients with severe or very severe HPS, but we can note that in mild and moderate HPS cases, 99mTc-MAA is not useful in determining the risk of mortality.

Changes in MAA post-transplantation

The shunt values measured with 99mTc-MAA in HPS patients who had a positive 99mTc-MAA result normalized in the first six months post-transplantation. This quick normalization of 99mTc-MAA results is consistent with previously published results from the same sample of patients, in which the symptoms of HPS were completely reversed in 100% of cases during the first 12 months after LT and in 8% of cases during the first six months. Because the 99mTc-MAA is less sensitive than TCE in detecting IPVD, it seems logical that its results normalize earlier than those of TCE. Swanson et al. also observed a normalization of the 99mTc-MAA scan in 20 patients by 12 months after LT (8).

One of the limitations of this study is that patients enrolled came from only one center, which limits the application of its findings to other populations due to possible genetic or environmental differences in the study population. Another limitation is the relatively small sample size, although it is the largest reported in the literature. It must also be highlighted that our study predominantly included mild to moderate cases, so the findings primarily apply to this group of patients. However, it is noteworthy that the results of this study are based on a standardized HPS screening in cirrhotic patients who were eligible for LT and, therefore, are of great interest in this context.

In conclusion, the 99mTc-MAA is a low sensitivity test for the diagnosis of IPVD that defines the presence of HPS compared to the TCE, and we do not advise its widespread use as a diagnostic test. However, it might be useful in the diagnosis of HPS in patients who have concomitant lung disease to determine the role of HPS in hypoxemia, especially patients with severe and very severe HPS. In cases of mild to moderate HPS, the 99mTc-MAA value was moderately correlated with PaO2 while breathing 100% oxygen and the calculated shunt but not with PaO2 while breathing room air or A-a PO2. The 99mTc-MAA values were not related to mortality in patients with mild to moderate HPS and normalized soon after LT.

 

References

1. Rodríguez-Roisin R, Krowka MJ, Herve P, et al.; ERS Task Force Pulmonary-Hepatic Vascular Disorders (PHD) Scientific Committee. Pulmonary-hepatic vascular disorders (PHD). Eur Respir J 2004; 24:861-80. DOI: 10.1183/09031936.04.00010904.         [ Links ]

2. Rodríguez Roisin R, Krowka MJ. Hepatopulmonary syndrome. A liver-induced lung vascular disorder. N Engl J Med 2008;358:2378-87. DOI: 10.1056/NEJMra0707185.         [ Links ]

3. Aller R, Moya JL, Moreira V, et al. Diagnosis of hepatopulmonary syndrome with contrast transesophageal echocariography. Advantages over contrast transthoracic echocardiography. Dig Dis Sci 1999;44:1243-8. DOI: 10.1023/A:1026657114256.         [ Links ]

4. Abrams GA, Jaffe CC, Hoffer PB, et al. Diagnostic utility of contrast echocardiography and lung perfusion scan in patients with hepatopulmonary syndrome. Gastroenterol 1995;109:1283-8.         [ Links ]

5. Abrams GA, Nanda NC, Dubovsky EV, et al. Use of macroaggregated albuming lung perfusion scan to diagnose hepatopulmonary syndrome: A new approach. Gastroenterol 1998;114:305-10. DOI: 10.1016/S0016-5085(98)70481-0.         [ Links ]

6. Krowka MJ, Wiseman GA, Burnett OL, et al. Hepatopulmonary syndrome: A prospective study of relationships between severity of liver disease, PaO2 response to 100% oxygen, and brain uptake after 99mTcMAA lung scanning. Chest 2000;118:615-24. DOI: 10.1378/chest.118.3.615.         [ Links ]

7. Arguedas MR, Abrams GA, Krowka MJ, et al. Prospective evaluation of outcomes and predictors of mortality in patients with hepatopulmonary syndrome undergoing liver transplantation. Hepatol 2003;37:192-7. DOI: 10.1053/jhep.2003.50023.         [ Links ]

8. Swanson KL, Wiesner RH, Krowka MJ. Natural history of hepatopulmonary syndrome: Impact of liver transplantation. Hepatol 2005;41:1122-9. DOI: 10.1002/hep.20658.         [ Links ]

9. Márquez E, Jara L, Ortega F, et al. Síndrome hepatopulmonar en paciente con hepatopatía avanzada: estudio de 24 casos. Med Clin 2008;130:98-102. DOI: 10.1157/13115351.         [ Links ]

10. Rodríguez-Roisin R, Roca J. Hepatopulmonary syndrome: The paradigm of liver-induced hypoxaemia. Baillieres Clin Gastroenterol 1997;11:387-406. DOI: 10.1016/S0950-3528(97)90046-4.         [ Links ]

11. Krowka MJ. Hepatopulmonary syndrome: Recent literature (1997 to 1999) and implications for liver transplantation. Liver Transpl 2000;6:S31-5.         [ Links ]

12. Kim HY, Choi MS, Lee SC, et al. Outcomes in patients with hepatopulmonary syndrome undergoing liver transplantation. Transpl Proc 2004;36:2762-3. DOI: 10.1016/j.transproceed.2004.10.002.         [ Links ]

13. Deberaldini M, Arcanjo ABB, Melo E, et al. Hepatopulmonary syndrome: Morbidity and survival after liver transplantation. Transpl Proc 2008;40:3512-6. DOI: 10.1016/j.transproceed.2008.08.134.         [ Links ]

14. Gupta S, Castel H, Rao RV, et al. Improved survival after liver transplantation in patients with hepatopulmonary syndrome. Am J Transplant 2009;9:1-10.         [ Links ]

15. Martínez-Palli G, Gómez FP, Barberá JA, et al. Sustained low diffusing capacity in hepatopulmonary syndrome after liver transplantation. World J Gastroenterol 2006;12:5878-83.         [ Links ]

16. Pascasio JM, Grilo I, López-Pardo FJ, et al. Prevalence and severity of hepatopulmonary syndrome and its influence on survival in cirrhotic patients evaluated for liver trasplantation. Am J Transplant 2014;14:1391-9. DOI: 10.1111/ajt.12713.         [ Links ]

17. Chiang ST. A nomogran for venous shunt calculation. Thorax 1968:23:563-5.         [ Links ]

18. Krowka MJ, Mandell MS, Ramsay MA, et al. Hepatopulmonary syndrome and portopulmonary hypertension: A report of the multicenter liver transplant database. Liver Transpl 2004;10:174-82. DOI: 10.1002/lt.20016.         [ Links ]

19. Taille C, Cadranel J, Bellocq A, et al. Liver transplantation for hepatopulmonary syndrome: A ten-year experience in Paris, France. Transplantation 2003;75:1482-9. DOI: 10.1097/01.TP.0000061612. 78954.6C.         [ Links ]

20. Whyte MK, Hughes JM, Peters AM, et al. Analysis of intrapulmonary right to left shunt in the hepatopulmonary syndrome. J Hepatol 1998;29:85-93. DOI: 10.1016/S0168-8278(98)80182-7.         [ Links ]

21. Aller R, Moya JL, Moreira V, et al. Diagnosis and grading of intrapulmonary vascular dilatation in cirrhotic patients with contrast transesophageal echocardiography. J Hepatol 1999;31:1044-52. DOI: 10.1016/S0168-8278(99)80317-1.         [ Links ]

22. Schenk P, Fuhrmann V, Madl C, et al. Hepatopulmonary syndrome: Prevalence and predictive value of various cut offs for arterial oxygenation and their clinical consequences. Gut 2002;51:853-9. DOI: 10.1136/gut.51.6.853.         [ Links ]

23. Lima BL, França AV, Pazin-Filho A, et al. Frequency, clinical characteristics, and respiratory parameters of hepatopulmonary syndrome. Mayo Clin Proc 2004;79:42-8. DOI: 10.4065/79.1.42.         [ Links ]

24. Iyer VN, Swanson KL, Cartin-Ceba R, et al. Hepatopulmonary syndrome: Favorable outcomes in the MELDexception era. Hepatol 2013;57:2427-35. DOI: 10.1002/hep.26070.         [ Links ]

 

 

Correspondence:
Israel Grilo Bensusan.
Department of Digestive Diseases.
Hospital de Alta Resolución de Écija
C/ Sor Cándida Sáiz, 1.
41400 Écija, Sevilla. Spain
e-mail: igrilob@telefonica.net

Received: 27-01-2016
Accepted: 08-01-2017