⇓“The tantalizing problem of the connective link in cirrhotic patients between oxygen unsaturation and possible arteriovenous shunting in the lungs remains unsolved, and any relation between arterial unsaturation and pulmonary vasodilation remains obscure.”
Berthelot et al. 1
“Portal venous hypertension coexisted with pulmonary arterial hypertension. These observations suggested two questions: What was the origin of the pulmonary vascular changes? Was there a possible relationship between these pulmonary vascular lesions and abnormalities in the portal venous system?”
Naeye 2
Background
Owing to the success of orthotopic liver transplantation (OLT), there has been increasing recognition of the importance of pulmonary vascular complications of hepatic disease states. Such vascular complications, namely hepatopulmonary syndrome (HPS) and portopulmonary hypertension (PPHTN), are commonly present as dyspnoea and are not always easily distinguished from nonpulmonary symptoms caused by manifestations of advanced liver disease (such as anaemia, ascites and muscle wasting). More importantly, since the late 1980s, experience has taught that such complications influence survival and candidacy for OLT. Currently, OLT is the only effective treatment for improving outcome in patients with HPS, a life-threatening condition whose prevalence can approach 20% in some series of patients awaiting OLT. PPHTN, pulmonary arterial hypertension (PAH) occurring in the setting of liver disorders, another dramatic pulmonary–hepatic vascular condition, has a prevalence in the order of 5% in hepatic patients submitted to OLT. Unlike in HPS, in the moderate-to-severe stages of PPHTN, OLT is not widely recommended, even being regarded a contraindication due to its negative perioperative and postoperative impact. As a consequence, a difficult pharmacological vasodilatory strategy becomes mandatory before proceeding to OLT. Notwithstanding, it is now evident that knowledge and understanding from diagnosis to management of these two distinct entities are rudimentary, such that underdiagnosis, undertreatment and inconsistent management are common worldwide.
During the 2000 European Respiratory Society (ERS) Annual Congress held in Florence, Italy (August 2000), a symposium on these two disorders, entitled “Advances in Understanding Pulmonary Complications in Hepatic Diseases”, was organised under the auspices of the Clinical Physiology and Integrative Biology ERS Assembly. The participants in this symposium, all experts in pulmonary and hepatic diseases, unanimously agreed to apply for an ERS Task Force on Pulmonary–Hepatic Vascular Disorders (PHD), which was approved and funded by the Scientific Committee in October 2001. The recommendations in this report were essentially developed during two workshops. The first was held within the context of the European Association for the Study of the Liver (EASL) Annual Meeting, in Madrid, Spain (April 2002), and the second in Barcelona, Spain (January 2003).
This ERS Task Force on PHD had three major objectives: 1) to increase awareness of both HPS and PPHTN in the medical community in order to minimise the growing impact of their morbidity and mortality; 2) to improve diagnosis and management of HPS and PPHTN through a major concerted effort by specialists involved in all facets of their clinical care; and 3) to stimulate the minimal programme of research interest in these two disorders.
Hepatopulmonary syndrome
Definition
HPS is defined as an arterial oxygenation defect induced by intrapulmonary vascular dilatations (IPVD) associated with hepatic disease 3–6. The vascular component characteristically includes diffuse or localised dilated pulmonary capillaries and, less commonly, pleural and pulmonary arteriovenous communications. All in all, HPS encompasses a clinical triad characterised by arterial deoxygenation, IPVD and liver disorder. Although HPS is predominantly seen in middle-aged patients without sex difference, it can also occur in children 7, 8.
The most common hepatic disorder leading to HPS is liver cirrhosis, irrespective of aetiology 3–6, although HPS has also been observed in many other chronic, and even acute, hepatic conditions 3–13. The pulmonary gas exchange abnormality is characterised by arterial deoxygenation that may be mild, moderate or severe 3, 5, 13–16. There is an increased alveolar–arterial oxygen tension difference (PA–a,O2). In contrast, arterial carbon dioxide retention (arterial carbon dioxide tension (Pa,CO2) ≥6.0 kPa (≥45 mmHg)) is never present 3–5, 13, 14. On the contrary, since patients with advanced liver disease usually hyperventilate, hypocapnia (Pa,CO2 <4.7 kPa (<35 mmHg)) and respiratory alkalosis are common. Calculation of PA–a,O2 is one of the most sensitive approaches for the detection of early arterial deoxygenation 3, 5, since PA–a,O2 can increase before arterial oxygen tension (Pa,O2) itself becomes abnormally low. At sea level and while breathing room air, a resting PA–a,O2 of ≥2.0 kPa (≥15 mmHg) can be considered abnormal 15, 16, but, for patients aged >64 yrs, a PA–a,O2 of ≥2.7 kPa (≥20 mmHg) can be recommended (table 1⇓) 14. However, an increased PA–a,O2 alone is not sufficient to confirm the existence of HPS 13. IPVD must also be present and are considered to exist when pulmonary capillary diameter ranges 15–60 µm, being the major structural derangement in HPS 1. Contrast-enhanced echocardiography (CEE) and perfusion lung scanningusing technetium-99m-labelled macroaggregated albumin (99mTcMAA) are the two most well-accepted approaches for assessing IPVD 3–6. Although some imaging techniques, such as pulmonary angiography and conventional or high-resolution computed tomography (HRCT) scanning, may also provide information about the shape, appearance and distribution of pulmonary vessels 17, their diagnostic accuracy has not yet been sufficiently well established. This combination of arterial deoxygenation, IPVD and liver disease is so unique that it supports the diagnosis of HPS even in the presence of associated chronic cardiopulmonary diseases, such as chronic obstructive pulmonary disease (COPD), bronchial asthma or idiopathic pulmonary fibrosis, which can also cause (or aggravate) arterial gas exchange abnormalities, including hypoxaemia with or without hypercapnia 18.
Staging of severity
Staging of the severity of HPS is important because severity influences survival 19–22, and is useful in determining the timing and risks of OLT 5, 21–23. A classification of the severity of HPS based on oxygenation abnormalities in four stages is proposed (table 2⇓) 3–6, 13, 14. More severe HPS causes greater clinical symptoms 13, 14, probably affects quality of life and signals the need to consider specific therapeutic interventions (i.e. long-term oxygen therapy and embolotherapy) to offset the deleterious effects of tissue hypoxia 24. Assessment of the severity of IPVD is difficult by means of CEE because this technique does not provide a quantitative evaluation. Extrapulmonary uptake of 99mTcMAA can be quantified, but the procedure has not been sufficiently standardised beyond a few centres. The sensitivity of both approaches for the detection of anatomical pulmonary arteriovenous communications or diffuse or localised vascular dilatations alone is similar 25.
Natural history and outcome
Definite statements concerning the natural history of HPS have been limited by two factors. First, few HPS patients are followed in any single centre. A multicentric database for OLT candidates described 20% of HPS patients who were denied this surgical procedure due to extrapulmonary comorbid conditions, with follow-up not reported 26. In the largest single-centre-based series to date, in HPS patients (Pa,O2 cut-off of <9.3 kPa (<70 mmHg)) who did not undergo OLT until 1988 27, median survival was 41 months following diagnosis of HPS, and the longest survivor not having undergone transplantation lived >10 yrs. Mortality is usually due to complications of hepatic disease, as opposed to a primary respiratory event. A more recent prospective study demonstrated a shorter median survival (∼11 months) with similar causes of death 23.
Secondly, OLT interrupts or modulates the natural course of HPS. Not only has OLT become the treatment of choice for HPS in many centres, but successful OLT has also resulted in complete resolution of HPS in the majority of survivors of the early post-surgical period 6, 27. Preliminary data suggests, however, slow recovery of arterial hypoxaemia, but long-term survival following OLT in some HPS patients 6, 27. Sporadic cases of PPHTN after OLT-induced HPS resolution have been reported 6, 28, 29.
In patients with portal hypertension, the natural history of HPS is not sufficiently understood, since its precise pathogenic mechanisms remain unsettled 6. Moreover, the prevalence of HPS varies widely between pulmonary and liver centres. In patients with cirrhosis, the mean prevalence of subclinical HPS is 15% 3, 30, depending on the cut-off values of Pa,O2 used to define the entity 14 and/or means of calculation of PA–a,O2 to diagnose HPS (table 1⇑) 3, 5, 13, 14. In patients with unusual hepatic diseases, the prevalence of HPS is unknown, although it may be anticipated to be extremely low, given the lower incidence of these hepatic conditions compared with that of liver cirrhosis. In chronic viral hepatitis with or without cirrhosis, the prevalence of HPS is ∼10% 9. The prevalence of HPS in OLT candidates (18%) is elevated 13 and has been reported to be as high as 28% in Budd-Chiari syndrome 11. Rare cases of HPS in combination with PPHTN before OLT have also been documented (Ph. Hervé and R. Rodríguez-Roisin, personal communications) 31. The behaviour of Pa,O2 in advanced cirrhotic patients without HPS remains unknown 32, as does the outcome of HPS with coexisting cardiopulmonary comorbid conditions.
Pathophysiology
The major primary structural disturbance in HPS is dilatation of the pulmonary pre-capillary and post-capillary vessels that allows mixed venous blood to pass either very quickly or even directly into the pulmonary veins 3–6. Absent or reduced pulmonary vascular tone with impaired hypoxic vasoconstriction may also occur 33, 34. There are three well-known intrapulmonary determinants of arterial deoxygenation, namely alveolar ventilation–perfusion (V'A/Q') imbalance, increased intrapulmonary shunt (i.e. nonventilated or zero V'A/Q' units) and diffusion impairment to oxygen, essentially reflecting a diffusion–perfusion defect 35, and all may be present in advanced HPS 3–6, 33, 34, 36–40. By contrast, the role of direct portopulmonary venous communications to arterial deoxygenation is negligible 3. However, the relative contributions of the former three determinants appear to vary. Although it is agreed that V'A/Q' mismatching is the pivotal mechanism for arterial deoxygenation since it fits well with the presence of lung regions in which alveoli are normally ventilated but overperfused, the relevance of the other two factors remains somewhat speculative 41. An added conceptual difficulty is the reconciliation of the presence of elevated levels of increased intrapulmonary shunt (i.e. ≥20% of cardiac output (Q')) despite the active Pa,O2 response to 100% oxygen (i.e. Pa,O2 >40 kPa (>300 mmHg)) observed in many patients. Diffusion impairment to oxygen, as shown by a greater predicted (according to the multiple inert gas elimination technique) 42 than measured Pa,O2 40, 41 while breathing room air, is also present in advanced HPS, a mechanism also consistent, in part, with the common finding of a low diffusing capacity of the lung for carbon monoxide (DL,CO). It is of note that the presence of an elevated Q' facilitates, in part, this favourable Pa,O2 response to breathing 100% oxygen, other things being equal. Presumably, DL,CO is reduced because the distance between the alveoli and the red cells in the central stream of the dilated pulmonary microvessels is too great for complete equilibration of carbon monoxide with haemoglobin. Although capillary blood volume is likely to be increased, diffusion impairment to oxygen may be aggravated, in part, by a high Q', resulting in a shorter transit time of the red blood cell and, hence, contributing to the development of a diffusion–perfusion imbalance 35. Nevertheless, this pulmonary gas exchange status is still consistent with the coexistence of the three mechanisms of hypoxaemia mentioned previously, their individual roles varying according to HPS severity (table 2⇑) 3. Thus, early HPS stages with normoxaemia (Pa,O2 ≥10.6 kPa (≥80 mmHg)) and increased PA–a,O2 (≥2.0 kPa (≥15 mmHg)) alone or with moderate levels of hypoxaemia (Pa,O2 ≥8.0–<10.6 kPa (≥60–<80 mmHg)) may be associated with mild V'A/Q' inequality and modest intrapulmonary shunt (<10% of Q'), but rarely with diffusion impairment, whereas, in severe HPS (Pa,O2 ≥6.7–<8.0 kPa (≥50–<60 mmHg)), and also in the most severe hypoxaemic stages (Pa,O2 <6.7 kPa (<50 mmHg)), all three determinants of arterial deoxygenation can coexist. Hyperventilation, by increasing alveolar oxygen tension, and high Q', by raising mixed venous oxygen tension, may diminish the reduction in Pa,O2 43. The influence of coexisting chronic lung disorders, such as COPD or idiopathic pulmonary fibrosis, of relatively common occurrence in HPS patients, on arterial desaturation remains unsettled 18.
Pathology
Several pathological abnormalities have been documented in the pulmonary vasculature of cirrhotic patients with HPS 44. These abnormalities include diffuse or localised dilatation of alveolar pre-capillary and post-capillary vessels, pleural (surface) and pulmonary anatomical artery-to-vein communications and portopulmonary venous anastamoses 1. However, the few detailed pathological studies were carried out before the standardisation of a universal definition of HPS and prior to the availability of imaging modalities used to detect IPVD. Nonetheless, dilatation of capillary vessels in alveolar regions 1, 45 is a central prerequisite and the principal pathophysiological hallmark of arterial deoxygenation in both human and experimental HPS 46, 47. In addition, in animal models, intravascular accumulation of macrophages in the pulmonary microcirculation and increased numbers of pulmonary capillaries have been shown, suggesting a vasculogenic response 47, 48. Whether similar changes occur in humans and are important pathogenically has not been resolved.
Pathogenesis
Most clinical cases have been reported in the setting of liver cirrhosis and portal hypertension, although controversy exists over whether the frequency and severity of HPS correlate with the degree of hepatic synthetic dysfunction and portal hypertension 6, 19, 25, 49. The evidence that HPS occurs in both extrahepatic portal venous obstruction 50 and hepatic venous outflow obstruction without cirrhosis (extrinsic liver disease) 51 shows that severe hepatic dysfunction and cirrhosis are not absolutely required for HPS to develop. In addition, the finding that HPS can occur in the setting of acute 52 and chronic noncirrhotic hepatitis 7, 9 demonstrates that portal hypertension may not be present in all cases. Finally, a clinical syndrome similar to HPS is observed in congenital disorders without liver injury in which either hepatic venous blood flow does not reach the lung 53 or portal venous blood reaches the inferior vena cava without passing through the liver 54, supporting the theory that factors either produced or metabolised in the liver can modulate the pulmonary vasculature.
Enhanced pulmonary production of nitric oxide (NO) has been implicated in the development of IPVD in cirrhotic patients with HPS 55–59. Exhaled NO levels are increased in HPS patients and normalise after OLT 56–58, as HPS resolves or is minimised. However, the mechanism of increased endogenous NO production and its relationship to the presence of portal hypertension, the hyperdynamic circulation and the degree of liver injury, remains uncertain. In addition, whether other mediators might contribute to IPVD has not yet been studied.
Experimentally, chronic common bile duct ligation (CBDL) is the only identified rat model of HPS 60, 61, whereas partial portal vein ligation has been used as a control intervention in which both portal hypertension and a hyperdynamic circulation develop without hepatic injury and subsequent HPS 61. Early studies focused on the vasoconstrictor role of eicosanoids and the increased numbers of intravascular macrophage-like cells 48, 60, 62. Subsequent work identified increased pulmonary vascular endothelial (eNOS) and inducible (iNOS; in macrophages) NO synthase expression and activity as the origin of the increase in pulmonary NO production 63–68. Intravenous NG-nitro-l-arginine methyl esther (l-NAME) improved hypoxaemia in CBDL rats, thereby supporting the pathogenic role of excessive pulmonary NO release in HPS 69. Further studies have demonstrated that increased hepatic production and release of low levels of endothelin (ET)-1 is one mechanism for triggering an increase in pulmonary eNOS levels and vasodilatation after CBDL 64, 65. This is associated with a selective increase in pulmonary vascular ETB receptor expression in cirrhosis and portal hypertension, an event that appears to enhance ETB receptor-mediated ET-1-induced NO production 66. The roles of other enzymes and mediators investigated have recently refocused interest on the accumulation of intravascular macrophages. An increase in pulmonary iNOS expression 63 has been observed in CBDL 67, predominantly in intravascular macrophage-like cells, and was felt to be an important source of NO. Furthermore, treatment of CBDL with norfloxacin decreased macrophage accumulation and normalised iNOS but not eNOS levels 68, hence, supporting a role for bacterial translocation in pulmonary macrophage accumulation and its contribution to IPVD. Pentoxifylline, an inhibitor of tumour necrosis factor (TNF)-α production in macrophages 70, also prevented HPS in the rat model 71, thereby supporting its pathogenic role. Recent work suggests that ET-1 and TNF-α can both interact in the development of experimental HPS 72. More recently, the findings of increased haem oxygenase-1 expression and carbon monoxide production in CBDL support their role in the progression of IPVD 73, 74. Figure 1⇑ highlights some of these mechanisms.
Clinical diagnosis
Symptoms and physical examination
Shortness of breath is a common symptom when arterial hypoxaemia associated with HPS develops in the setting of chronic liver disease. The development of HPS does not appear to correlate uniformly with the severity of underlying liver disease, as characterised by the Child-Pugh score 19, 49. Characteristic but not pathognomic of HPS, however, is the typical complaint of platypnoea (increased dyspnoea from the supine to upright position) 5 and the associated finding of orthodeoxia (decrease in Pa,O2 ≥5% or ≥4 mmHg from the supine to upright position) 36, 75, whose mechanism has been recently clarified 75. Early exertional dyspnoea may evolve into dyspnoea at rest as hypoxaemia progresses. Fatigue resulting from anaemia and hepatic dysfunction may be difficult to distinguish from HPS-induced hypoxaemia. Spider naevi, digital clubbing, and cyanosis of the lips and nail beds are consistent findings in advanced HPS, although they are not entirely specific 5, 33, 76. Clinicians should also be aware that common chronic pulmonary comorbid conditions, in particular COPD, bronchial asthma and idiopathic pulmonary fibrosis, coexist in approximately a third of HPS patients 18, 23, 77. Extrapulmonary complications of right-to-left pulmonary communications, such as the development of a brain abscess 78, 79 or intracranial haemorrhage 80, and hypoxaemia-induced polycythaemia 81, have been reported. Information on health status is not available.
Lung function tests
Both forced spirometric results and static lung volumes (by plethysmography or helium-dilution) are characteristically within normal limits in HPS in the absence of pulmonary comorbid conditions 12, 22, 82. Although mild-to-moderate ventilatory abnormalities may be present in some patients 22, 82, a moderately to severely reduced DL,CO after adequate correction for anaemia 83 appears to be a common functional marker of HPS 3, 13. Compared to the full reversibility of all functional and clinical outcomes, a sustained low DL,CO in HPS patients 1 yr after successful OLT is an intriguing finding 84, 85, which could be related to collagen tissue deposition in pulmonary capillary and venule walls, as shown in a single post mortem study 86. Since the mechanism of low DL,CO remains unsettled, this gas exchange descriptor is not recommended for the screening evaluation of HPS (see below).
Arterial blood gas tensions, assessed at rest while breathing room air and in the sitting position by arterial puncture or through an indwelling arterial catheter, are mandatory for both the diagnosis and staging of severity of HPS, and encompass a wide spectrum of abnormalities from a simple increase in PA–a,O2 alone to very severe, life-threatening levels of hypoxaemia, usually associated with hypocapnia. During exercise, patients with HPS achieve lower peak oxygen uptakes than cirrhotics without HPS, with more hypoxaemia and an elevated dead space, hence, suggesting that abnormal pulmonary ciculation contributes to further exercise limitation in HPS 87. Pulse oximetry for the assessment of arterial oxygen saturation (Sa,O2) is useful in the follow-up of patients with moderate-to-severe HPS, particularly children, before OLT, but is not sufficiently accurate to replace the detailed information provided by routine arterial blood gas tension determination (because of the shape of the oxyhaemoglobin dissociation curve).
Haemodynamics
A hyperkinetic circulatory state, with high Q' and low systemic vascular resistance and pulmonary vascular resistance (PVR), is present in 30–50% of cirrhotic patients and generally correlates with the Child-Pugh score 88–92, especially in patients with moderate-to-severe HPS. Patients with portal hypertension show a low median PVR with a wide range 88. Systemic and pulmonary vasodilatation in cirrhosis and portal hypertension appears to be the consequence of a widespread decrease in vascular tone 92, 93 that results in impaired responsiveness to vasoconstrictors 94, 95. Hypoxic pulmonary vasoconstriction is absent or mitigated in ∼30% of patients with advanced cirrhosis, with or without associated HPS, and appears to become less evident as liver disease worsens 33, 34, 96–98. Whether or not a progressive loss of pulmonary vascular tone as liver disease deteriorates contributes to IPVD and the development of HPS remains controversial 22, 98, 99.
Biochemistry and noninvasive exhaled biomarkers
No serum test of hepatic function has been shown to be of value in the diagnosis of HPS 3–6. However, serum progesterone and oestradiol levels are generally elevated in HPS 99 and both hormones have been correlated with the appearance of spider naevi, a finding also related to haemodynamic and gas exchange abnormalities in cirrhotic patients 33. Sex hormone levels and IPVD return to normal after OLT, suggesting a pathogenic role in HPS 99. Serum nitrite/nitrate levels are increased in liver cirrhosis and this is related to endotoxaemia 100. Increased exhaled NO levels, derived from the alveolar region 101,102, are observed in patients with advanced cirrhosis with and without HPS 57, 58, 103, and correlate with the abnormally increased PA–a,O2 57 and high Q' 103. Partial or complete resolution of clinical and functional markers of HPS after using different inhibitors and/or interventions that block the effects of NO, such as methylene blue 59, 104 and l-NAME 105, or following smoking 106 and OLT 56, sporadically or anecdotally reported, support the idea that increased endogenous pulmonary NO could play a pivotal role in the development of arterial deoxygenation. Further clinical studies are needed to establish the precise utility of exhaled NO in the clinical work-up of HPS. To date, no data are available regarding exhaled gas condensates 107.
Lung imaging
Contrast-enhanced echocardiography
Transthoracic echocardiography with contrast enhancement (CE-TTE) provides a sensitive, noninvasive and qualitative screening approach for the detection of IPVD, the central defining structural characteristic of HPS 108, and is considered the gold standard for the diagnosis of HPS. It is commonly accomplished by hand agitation of 10 mL normal saline, resulting in microbubbles (≤90 µm in diameter), which are injected into an upper extremity vein. Detection of microbubbles within the left atrium is considered positive CEE. Microbubbles are physiologically trapped and absorbed by normal alveoli during the first passand should not appear in the left atrium. Following microbubble appearance in the right atrium, immediate appearance in the left atrium (within less than three cardiac cycles) suggests an intra-atrial right-to-left communication, whereas delayed appearance in the left heart cavities (within greater than three cardiac cycles) implies definite IPVD 5, 108. Although positive CE-TTE results are found in 11–47% of patients with liver disease (with or without associated HPS), only 32–59% of these patients have arterial hypoxaemia 49, 109–113. Patients with positive CE-TTE results and normal arterial oxygenation may have forme fruste (or clinically silent) HPS, but their outcome remains unknown 114. Indocyanine green solution (microbubble size ≤90 µm) 109 or a modified gelatin solution (which creates microbubbles of 10±2 µm) 115 are the alternative contrast agents used and possibly contribute to the different prevalence findings 14.
Transoesophageal echocardiography
Alternatively, transoesophageal echocardiography with contrast enhancement (CE-TEE) may be superior to CE-TTE for the diagnosis of IPVD in cirrhotic patients with HPS, being more sensitive and showing better correlation with Pa,CO2 and DL,CO than in patients without HPS 116. Further, it can definitively discern the passage of microbubbles through an interatrial pathway versus microbubble entrance into the left atrium from the pulmonary veins. However, CE-TEE is more expensive, requires sedation and poses a theoretical risk in patients with oesophageal varices, which may be present in patients with liver disease. Since CE-TTE has been shown to be more sensitive than lung perfusion scanning for the detection of IPVD 19, with the additional advantage that it can be conducted as part of routine echocardiographic screening for pulmonary hypertension by Doppler assessment of tricuspid systolic peak regurgitant jet velocity (see Portopulmonary hypertension section), it can be recommended as the best choice for screening for both HPS and PPHTN.
Perfusion lung scanning
Whole-body 99mTcMAA scanning allows for the detection of IPVD, along with their quantification, detecting areas with both low and zero V'A/Q' units 49, 117. Since macroaggregates are >20 µm in diameter, they are normally trapped in the pulmonary vascular network. In patients with intracardiac shunt or IPVD, radiolabelled particles bypass, or pass through, the pulmonary vascular bed and are transported to and retained by extrapulmonary regions, such as the brain, kidneys, spleen and liver. The major disadvantage of perfusion lung scanning relative to CE-TTE is its inability to differentiate between intracardiac communications and IPVD. In addition, the sensitivity of lung perfusion scanning is lower than that of CE-TTE in detecting HPS 49. However, the radionuclide approach allows the quantification of IPVD by assessment of systemic and pulmonary uptake, and various indices have been proposed 19, 118. In addition, increased systemic distribution of radiolabelled particles does not occur in chronic associated respiratory comorbid conditions, whereas CEE results remain positive, such that the 99mTcMAA approach may be of help in evaluating the contribution of HPS to arterial hypoxaemia in these patients. One validated perfusion (or shunting) index not, however, used routinely takes into account the 99mTcMAA activity of the liver and the brain 19, 20, 49, with a cut-off value of ≥6% of Q' when intracardiac communications or IPVD are present. The assessment of IPVD using the isotopic method provides shunt estimates that often exceed the functional estimates of shunt provided by the conventional 100% oxygen method 25. This is because IPVD may continue to participate in alveolar gas exchange, especially when the driving oxygen pressure is increased by the administration of high oxygen concentrations. Finally, the combination of quantifying the severity of arterial deoxygenation and the degree of intrapulmonary shunting indices by 99mTcMAA may offer complementary information for the stratification of HPS patients at greater risk of OLT mortality 19–21.
Pulmonary angiography
One pulmonary angiographic study in a small subset of HPS patients demonstrated two angiographic patterns: type I, or diffuse, and type II, or focal 17. The type I pattern was subdivided into a “minimal” pattern, characterised by normal vessels or fine diffuse spidery arterial vascular abnormalities, and an “advanced” pattern, with a diffuse spongy or blotchy appearance. Thetype II pattern, more infrequent, consisted of focal arteriovenous communications similar to those seen in hereditary haemorrhagic telangiectasia. Patients with “advanced” type I and type II patterns may exhibit a poor response to oxygen breathing (Pa,O2 <40 kPa (<300 mmHg)). Under these circumstances, the latter subset of patients may be considered for vascular embolisation, as type II lesions are not reversible and the patients may be at risk of cerebral embolism and/or abscess 17, 78, 79. Type I lesions can also be successfully embolised with subsequent marked increases in Pa,O2, as shown in a case report 24.
Thoracic computed tomographic scanning
There is little information regarding the use of conventional thoracic computed tomography (CT) scans for the diagnosis of HPS. In one small study, CT demonstrated that the peripheral pulmonary arteries were significantly dilated compared with controls and normoxaemic cirrhotic patients 119. However, a retrospective study did not confirm these results 120. A thoracic HRCT scan may beuseful for excluding coexistent chronic respiratory conditions when HPS is suspected 18.
Screening
The major screening steps for HPS are summarised in figure 2⇑, and are particularly recommended for all OLT candidates and for hepatic patients who have shortness of breath. Arterial blood gas levels, including calculation of PA–a,O2 using the abbreviated formula (table 1⇑), are measured, and, if an abnormally increased PA–a,O2 is confirmed, with or without coexisting hypoxaemia, both CEE and a complete set of lung function tests (forced spirometry with bronchodilator response, static lung volumes and DL,CO) are carried out. A negative CEE result excludes the diagnosis of HPS, whereas a positive CEE result establishes the diagnosis of HPS, irrespective of the presence or absence of intrinsic cardiopulmonary disease. In the event of normoxaemic HPS (increased PA–a,O2 alone with positive CEE results), arterial blood gas levels should be measured, at least once a year, to detect any abnormal Pa,O2 change, and/or if symptoms (essentially dyspnoea) appear. In addition, thoracic HRCT may be carried out, irrespective of the detection of any abnormal lung function tests, in order to rule out underlying subclinical chronic pulmonary disorders. Complementarily, the perfusion index calculated from a whole-body 99mTcMAA scan 49 can be helpful in estimating the outcome after OLT (see below).
If hypoxaemia is mild to moderate (PA–a,O2 ≥2.0 kPa (≥15 mmHg) and/or Pa,O2 ≥8.0–<10.6 kPa (≥60–<80 mmHg)), periodic follow-up is recommended, at least once a year, with assessment of lung function, including pulse oximetry and/or arterial blood gas levels if necessary (Sa,O2 <89%). If hypoxaemia progressively deteriorates in a symptomatic (breathless) patient, then OLT can be considered. Likewise, if hypoxaemia is severe (Pa,O2 ≥6.7–<8.0 kPa (≥50–<60 mmHg)), consideration of OLT is vital. If the hypoxaemia is very severe or extreme (Pa,O2 <6.7 kPa (<50 mmHg)) 21 and/or cardiopulmonary comorbid conditions exist 18, OLT needs to be considered on an individual basis after full assessment of the severity and prognosis of the associated extrahepatic disorders. Lung biopsy specimens are not required for diagnosis of HPS as IPVD are not reliably detected in tissue specimens. However, if coexisting idiopathic lung fibrosis is suspected in the face of potential OLT indication on the basis of severe HPS, then lung biopsy can be required to determine suitability for OLT.
Management
Pharmacological treatment
A number of small uncontrolled trials using various classes of drug, such as somatostatin analogue 17, β-blockers 121, 122, cyclooxygenase inhibitors 123, 124, glucocorticoids and immunosuppressors (cyclophosphamide) 125, pulmonary vasoconstrictors (almitrine) 126, 127, NO inhibitors 59, 104–106, 128, inhaled NO 129, 130, antimicrobials 68, 131 and garlic preparation 132, for the treatment of HPS have been reported. None of the studies, however, demonstrated consistent improvement in oxygenation and/or IPVD, as all were of inadequate size to test efficacy. In addition, rare spontaneous recovery has been observed in HPS 7, 133, although the mechanism remains uncertain. Future randomised placebo-controlled multicentric trials are needed in order to further investigate these and new therapeutic interventions.
Nonpharmacological treatment
Long-term oxygen therapy
HPS patients with severe hypoxaemia (Pa,O2 <8.0 kPa (<60 mmHg)) at rest are commonly seen and should receive continuous long-term low-flow oxygen therapy. No data are available, however, regarding the efficacy, compliance, tolerance and cost-effectiveness of such a therapeutic approach.
Transjugular intrahepatic portosystemic shunt
Portal hypertension appears to play a central role in the pathogenesis of HPS. Accordingly, a reduction in portal pressure might be beneficial in HPS 134–137. To date, only a few case reports using transjugular intrahepatic portosystemic shunt (TIPS) for HPS have been published, and have shown variable short-term effects on pulmonary gas exchange 134, 137. Therefore, insufficient data are available to support TIPS as a compassionate therapeutic approach in HPS 138.
Cavoplasty
This effective decompressive treatment in patients with suprahepatic inferior vena cava obstruction causing Budd-Chiari syndrome showed promise in reversing coexistent HPS 11. Similarly, venous decompression by abscess drainage resolved HPS in a single case with Budd-Chiari syndrome 11.
Embolisation
Coil embolisation (embolotherapy) in type II angiographic pattern HPS 17 has been reported to improve arterial oxygenation (as a temporary measure) in a single case report 24.
Orthotopic liver transplantation
Complete resolution of HPS following OLT has been observed in >80% of reported cases, and many centres currently view HPS as an indication for OLT 139–145, particularly in the paediatric population 146–149. Morbidity may be higher after OLT in severe HPS, based on pre-OLT severity of hypoxaemia and abnormal extrapulmonary 99mTcMAA uptake 21, 22. Such patients, depending on local surgical and post-OLT expertise facilities, might benefit from referral to highly specialised transplantation centres with significant HPS experience. Spontaneous recurrence of HPS 150, 151 and development of PPHTN before 31 or following OLT for HPS 6, 29 have been reported, but appear to be rare events. Liver transplantation from living donors for HPS has been shown to be successful in children 152, but no data are available in adults.
Task Force recommendations
The major Task Force recommendations concerning the diagnosis and treatment of HPS are summarised in table 3⇓.
Research prospects
1) Natural history, incidence and prevalence, particularly in the most advanced hepatic patients, remain controversial. All these aspects should be investigated prospectively through large multicentric studies, including the influence of long-term oxygen therapy.
2) The relevance and implications of positive CEE results suggestive of underlying IPVD, in the context of normal gas exchange, are completely ignored. There is a need for studies investigating the importance of this positive hallmark and its impact on the natural history of HPS.
3) The potential of experimental HPS models and their interplay with clinical studies need to be explored. This would facilitate greater insight into the pathogenic mechanisms of HPS. OLT is the only reliable treatment for full or partial resolution of HPS. Multicentric prospective studies of the natural history of OLT outcomes of HPS need to be developed.
4) Given the pathogenic role of some mediators, such as NO and ET, clinical trials of long-term inhaled NOS and ETB receptor antagonists, TNF-α inhibitors and antibiotics are necessary research topics that could result in new therapeutic approaches.
Portopulmonary hypertension
Definition
PPHTN can be defined as a PAH associated with portal hypertension, with or without hepatic disease 153–156. Diagnosis of PPHTN is based on pulmonary haemodynamic criteria obtained via right heart catheterisation 6, 153. Diagnostic criteria for PAH include a mean pulmonary arterial pressure (Ppa) of >25 (at rest) or >30 mmHg (during exercise), with a mean pulmonary artery occlusion pressure (mPAOP) of <15 mmHg 153, 154, 157. A moderate increase in Ppa (25–35 mmHg) is seen in up to 20% of patients with cirrhosis and portal hypertension 158. This increase in Ppa is most commonly caused by increases in Q' (despite reduced PVR) and/or in blood volume (increased mPAOP) 158, 159, without pulmonary vascular remodelling. Less commonly, moderate-to-severe PAH with extensive pulmonary vascular remodelling (increased PVR) develops 6, 153, 158, 160, 161. In order to distinguish between these two forms of PAH, criteria have evolved for the diagnosis of PPHTN (table 4⇓) 162–165. These haemodynamic criteria are consistent with the definitions and classification proposed by the 3rd World Symposium on Pulmonary Arterial Hypertension 166. Unlike HPS, arterial deoxygenation is not a major functional feature of PPHTN.
Staging of severity
A classification of severity of PPHTN is proposed (table 5⇓), based on Ppa 167. Such severity staging correlates with the increased mortality following OLT in moderate-to-severe PPHTN (pre-OLT Ppa of >35 mmHg) 164, 168.
Natural history and outcome
Initially described in 1951, the existence of portal hypertension and development of PAH are not coincidental 169. Pulmonary hypertension has been reported in 0.13% of unselected patients versus 0.73% of patients with cirrhosis and portal hypertension 170. Clinical series with biopsy-proven cirrhosis showed a prevalence of PAH ranging 0.61–2.0% 88, 97, 170. Recent studies from OLT centres have indicated a 3.1–4.7% frequency of moderate PPHTN in patients with severe liver disease 158, 171–173. Approximately 65% of patients with PAH had undergone previous portosystemic surgical shunt procedures 174. Noncirrhotic (extrahepatic) portal hypertension has been associated with up to 10% of patients with PPHTN 174, 175. In most series, the diagnosis of portal hypertension pre-dates the diagnosis of PPHTN, and the correlation between aetiology of liver disease, degree of portal hypertension (hepatic wedge pressure gradient), systemic haemodynamics and severity of PAH has been shown to be poor 88. Both the US National Institutes of Health 176 and the International Primary Pulmonary Hypertension Study (IPPHS) 177, aimed at evaluating primary pulmonary hypertension (PPH), have reported a significant proportion (7.3 and 8%, respectively) of patients as having PPHTN as opposed to PPH.
In the pre-OLT era, mean and median survivals of 15 and 6 months, respectively, were reported in a literature review of PPHTN patients (Ppa 48 mmHg) 178. A single-centre study reported that 58% died within 1 yr of the PPHTN diagnosis. Causes of death were equally distributed between liver- and lung-related problems 88. A 5-yr survival of 30% was reported in a study of PPHTN patients, not treated with i.v. epoprostenol, referred to the Mayo Clinic 179. Causes of death were equally distributed between complications of liver disease and right heart failure.
Pathology
The histopathological appearance of the pulmonary vessels in PPHTN is indistinguishable from that in other forms of PAH 2, 180–183. Intimal proliferation and/or thickening, medial smooth muscle hypertrophy and fibrosis are seen in the small pulmonary arteries 2, 156, 161. Thrombus with recanalisation may be present, which led authors to attribute PPHTN to emboli from the portal vein or other systemic sources 169. It is clear that these lesions are not embolic, as they may be seen in the absence of systemic sources of clot in many forms of pulmonary hypertension 182. This in situ thrombosis has been attributed to abnormal local endothelial thrombolytic activity and a hypercoagulable state 183. Platelet activation may also contribute 183. A characteristic (but not necessary) histological feature of PAH, including PPHTN, is the plexiform lesion, which is a dilated pulmonary artery with the normal structure replaced by an intraluminal plexus of endothelial cells and slit-like vascular channels 2, 160, 161.
Pathophysiology and pathogenesis
Vasoproliferation
The concept of a vasoproliferative process in PAH, including PPHTN, that causes increased resistance to arterial flow has been hypothesised 181. Monoclonal proliferation of the endothelium has been documented in PPH, but not in PPHTN to date 181. A decrease in prostacyclin (prostaglandin I2) expression in the pulmonary arteries of PPHTN patients has been noted 180. Proposed factors responsible for such findings are discussed as follows. Portal hypertension induces systemic inflammatory changes and increased vascular wall shear stress, which may trigger a cascade of intracellular signals 6. Activation or repression of various genes in the endothelial and/or smooth muscle cells may follow and this could lead to pulmonary vascular remodelling and/or vasculogenesis in genetically susceptible patients 184, 185. Abnormal plasma levels of vasoconstrictors (i.e. noradrenalin, rennin–angiotensin–aldosterone and arginine vasopressin) and vasodilators (i.e. NO, glucagon, vasoactive peptide and substance P) have been measured in the setting of portal hypertension 186–188. In short, investigators have hypothesised that an imbalance of vasoactive substances could reach the pulmonary circulation in abnormally high concentrations due to portosystemic shunts or defective hepatic metabolism, causing the pathological pulmonary vascular lesions seen in PPHTN 6, 153.
Genetics
Heterozygous mutations in the bone morphogenetic protein receptor type II and activin receptor-like kinase 1 genes (encoding different types of receptor member of the transforming growth factor-β signalling superfamily) were recently reported in familial, as well as sporadic, PPH and PAH associated with hereditary haemorrhagic telangiectasia, respectively 185, 189–191. Such receptors presumably control diverse cellular processes, including cell differentiation, endothelial/smooth muscle cell proliferation and apoptosis 190. These abnormalities have not been found in patients with PPHTN (M. Humbert, Hôpital A Béclère, Clamart, France; personal communication, 2002).
Inflammation
The development of portosystemic shunts and dramatic decrease in the phagocytic capacity of the liver allows circulating bacteria or bacterial endotoxins from the gastrointestinal tract to enter the pulmonary circulation 192–197. An increase in pulmonary phagocytic activity is ascribable to extensive accumulation of pulmonary intravascular macrophages that adhere to the pulmonary endothelium 6, 67, 196. Following phagocytosis, activated macrophages release numerous cytokines, including TNF-β, growth factors and NO into the extracellular milieu 67, 196–198. This pulmonary phagocytosis has been demonstrated in cirrhotic patients, suggesting that induction of pulmonary intravascular macrophages might contribute to the development of the pulmonary vascular disease, such as HPS and PPHTN, seen in these patients 196.
Neurohormones
Both serotonin and ET-1 are dual-action neurohormones that may cause vasoconstriction and mitogenesis in pulmonary arteries 199–202. Their abnormal regulation of portal hypertension makes them potentially important candidates in the pathogenesis of PPHTN. Circulating levels of serotonin, a potent pulmonary vasoconstrictor, correlate with PVR in patients with PPH 199. Serotonin predominantly originates from the enterochromaffin cells within the gastrointestinal tract wall. The lung is normally protected from high levels of free plasma serotonin by normal hepatic metabolism and the storage of serotonin in platelets 203. Portal hypertension is associated with decreased platelet levels, reduced platelet uptake and increased levels of serotonin 203–205. Compared with controls, patients with PPH more frequently carry the LL genetic variant of the serotonin transporter 206. This functional insertion/deletion polymorphism results in increased serotonin transporter expression and enhanced uptake of serotonin by pulmonary artery smooth muscle cells 206. This polymorphism has not been found in PPHTN (S. Adnot, Hôpital H Mondor, Créteuil, France; personal communication, 2003).
ET-1 is produced by the pulmonary endothelium and liver 207, 208. Binding to ETA and ETB receptors on smooth muscle cells results in vasoconstriction and mitogenesis. Circulating ET-1 also binds to ETB receptors, resulting in endothelium-dependent vasodilatation, mediated by NO and prostaglandin I2 production 208–211. Increased circulating levels of ET-1 have been documented in PPH and portal hypertension without pulmonary hypertension 67, 212, 213. Without knowing the concentration gradients across the hepatic and pulmonary circulations, it is unclear what the net effect is on the pulmonary vascular bed in the setting of advanced liver disease 208, 213.
Clinical diagnosis and screening
Symptoms and physical examination
Patients with portal hypertension who report dyspnoea, at rest or during exercise, should be assessed for the presence of PPHTN. Chest discomfort and syncope are features of advanced PPHTN. Physical examination results include elevated jugular venous pressure, an accentuated P2 component, a tricuspid regurgitation murmur, right ventricular heave or increasing lower extremity oedema (with other evidence of right-sided heart failure) 214, 215. In the setting of advanced PPHTN, chest radiography may show increased main pulmonary artery size or cardiomegaly in the absence of other pulmonary parenchymal abnormalities 216–218. Pulmonary function tests may show a reduced DL,CO. Arterial blood gas levels may show mild-to-moderate hypoxaemia, an increased PA–a,O2 and a decreased Pa,CO2 156, 179. Electrocardiography suggests right atrial enlargement, right ventricular hypertrophy or right axis deviation 215, 216. Conventional lung perfusion scanning may show “mosaic” perfusion, but other segmental perfusion abnormalities should prompt evaluation for pulmonary emboli 216, 217. Specific thoracic CT scan findings for PPHTN have not been documented. B-type natriuretic peptide may be a useful serum marker of right ventricular stress 218. To date, no data are available regarding exhaled markers 107.
Transthoracic Doppler echocardiography
Transthoracic echocardiographic findings (increased tricuspid peak regurgitant jet velocity, pulmonic valve insufficiency, paradoxical septal motion, right ventricular hypertrophy–dilatation and an increased right ventricular systolic pressure estimate (RVsys) by the Bernouilli equation) in the setting of portal hypertension suggest, but do not prove, PPHTN 175, 219–221. Accordingly, pulmonary haemodynamic measurements by right heart catheterisation must be performed in order to confirm the diagnosis 153, 156, 219. Lung biopsy is not advised due to increased risk of bleeding.
Screening for PPHTN is extremely important when OLT is considered 77, 164. A retrospective analysis showed that screening Doppler echocardiography (RVsys of >50 mmHg) identifies essentially all patients who should proceed to right heart catheterisation 219. A prospective study of OLT candidates who underwent Doppler echocardiography (RVsys of >30 mmHg) and catheterisation measurements revealed sensitivity, specificity, and positive and negative predictive values for a diagnosis of PPHTN of 100, 96, 59, and 100%, respectively 221. These studies support the value of echocardiography for screening OLT candidates for PPHTN. Therefore, transthoracic Doppler echocardiography should be the screening test of choice for OLT candidates, as recommended by the 3rd World Symposium on Pulmonary Arterial Hypertension 166. Patients who are listed for OLT without evidence of PPHTN on initial evaluation should undergo echocardiography annually; those with PPHTN may need to be followed more frequently, at least twice or three times every year.
Haemodynamics
Right heart catheterisation is the gold standard for the diagnosis of PAH, including PPHTN 6, 153, 219. The procedure measures pressures and flow and provides assessment of disease severity, right heart function and potential acute vasoreactivity. Haemodynamic measurements must include the following parameters: Ppa, mPAOP, mean right atrial pressure and Q', by either thermodilution or the Fick method, such that PVR can be calculated 6, 153.
Acute vasodilator testing
In PPH, acute vasodilator testing is usually performed with either i.v. epoprostenol or inhaled NO. Although both agents exert similar effects on Ppa, i.v. epoprostenol produces greater increases in Q' than does NO 222, 223. It is possible that patients with PPHTN could be less reactive to NO because liver cirrhosis is a condition of persistent endogenous NO overproduction 223–226. Indeed, significant acute pulmonary vasodilatation has been shown in PPHTN when using higher concentrations of NO (40 ppm) 225, 226. Accordingly, changes in selected haemodynamic parameters, such as PVR, should take into account the vasodilating agent that has been employed. Most investigators agree that acute decreases in both Ppa and PVR (>20% from baseline), with no change or increase in Q', can be considered a significant vasodilatory response 214, 215. The goal of such vasodilator testing is to determine staging severity and therapeutic expectations; there is no clinical relevance for calcium channel blockers use since they are contraindicated in portal hypertension (see below).
The acute vasodilatory effect of i.v. epoprostenol in PPHTN seems to be greater than that of NO. A significant decrease in pulmonary arterial pressure (>20%) in almost half of a small subset of patients with severe PPHTN during acute infusion of i.v. epoprostenol was reported 227, 228. In patients with PPHTN tested with both agents, the proportion of haemodynamic responders was greater when using i.v. epoprostenol than with inhaled NO (J.A. Barberà, Hospital Clínic, Barcelona, Spain; personal communication, 2003).
Pulmonary haemodynamic subsets
Unlike PPH, most patients with advanced liver disease experience a hyperdynamic circulatory state, namely increased Q' and decreased systemic vascular resistance 6, 158, 167. In addition, some patients exhibit increased pulmonary venous volume due to systemic volume or left ventricular abnormalities. It is clinically useful, therefore, to characterise the pulmonary haemodynamics that complicate liver disease into the three following subsets on the basis of measured haemodynamic outcomes, such as Ppa, Q' and mPAOP, and calculated PVR, via right heart catheterisation in the stable resting state (table 6⇓) 6, 167, 216, 229. 1) Hyperdynamic circulatory state. In this condition, the pulmonary vascular bed shows a minimal increase in pulmonary arterial pressure with increased Q', due to passive distension of compliant arterial vessels and recruitment of upper lung blood vessels 6, 167; Ppa can increase, usually by <35 mmHg, in response to high Q'. This subgroup is the most frequent finding in liver disease, including HPS 158. 2) Increased pulmonary venous volume. Volume increase reflects probable excess of volume and/or pressure increase due to limitation in pulmonary blood flow to the left atrium because of left ventricular dysfunction (systolic or diastolic). This results in increased mPAOP. This subset occurs in alcoholic cirrhosis, familial amyloidosis and combined liver–renal insufficiency 6, 167. Long-standing changes may increase PVR, but not to the degree documented in PPHTN. The transpulmonary pressure gradient (TPG=Ppa–mPAOP) can discern between excess of volume (TPG <10 mmHg) and additional pulmonary vascular abnormalities (TPG >10 mmHg) 230. 3) Vascular obstruction (i.e. PPHTN). Here, the pathological features of PPHTN include vasoconstriction and obstruction/obliteration due to endothelial proliferation, smooth muscle proliferation, fibrosis and in situ thrombosis 6, 160, 161. The pulmonary haemodynamics in early PPHTN are unique, with markedly increased Ppa, PVR and Q' 156, 163, 228. As PVR increases, right ventricular failure ensues, characterised by falling Q'.
Prognostic implications for OLT using staging of severity and pulmonary haemodynamic subsets can exist. The combination of a Ppa of <35 mmHg and a PVR of <250 dyn·s·cm−5 has been associated with an excellent post-OLT outcome 164. By contrast, a Ppa of >35 mmHg has been associated with increased mortality 164, 168. Intuitively, the measurement of right atrial pressure, right ventricular function and effects of volume loading should not be ignored 231, 232. Figure 3⇑ demonstrates the importance of right heart catheterisation relationships between Q', Ppa and PVR in the setting of advanced liver disease states. Most patients with significant increases in Ppa show reduced Q' and a PVR of >240 dyn·s·cm−5. Patients showing PVR ranging 120–240 dyn·s·cm−5 were more likely to exhibit both increased TPG and increased mPAOP.
Management
Pharmacological treatment
In patients with PPHTN, thrombocytopenia and/or an increase in prothrombin time are common events 233. Under these conditions of a high risk of gastrointestinal bleeding, oral anticoagulant therapy should not be recommended in PPHTN patients.
Nonspecific therapy
Diuretics
The goal of diuretics is to reduce both the intravascular volume and hepatic congestion that occur in patients with right-sided heart failure. Alternatively, hypovolaemia induced by an excessive amount of diuretics can reduce the Q' needed by decreasing right ventricle pre-load 233. Furosemide and/or spironolactone (up to 400 mg·day−1) should be prescribed carefully 233.
Cardiac glycosides
Digoxin has been shown to improve Q' acutely in PPH 234. Digitoxin toxicity may be enhanced if hypoxaemia and diuretic-induced hypokalaemia are also present. The efficacy of cardiac glycosides in PPHTN patients is unknown. It is of note that β-blockers could contribute to deterioration of PPHTN.
Vasodilator therapy
Pulmonary artery vasoconstriction contributes to the pathogenesis of PAH 235–237, and has been demonstrated in PPHTN 228. Although pure vasodilators reverse this component of the disease, they have little or no effect on the fibrotic and proliferative remodelling changes that predominate in PPHTN. Several agents are available (listed as follows).
Calcium channel blockers
Calcium channel blockers are not recommended in patients with portal hypertension as they may increase the hepatic venous pressure gradient 228, 238, 239.
Nitrates
A single case report described a patient who showed acute and chronic improvement in haemodynamics with isosorbide-5′-mononitrate 240.
Continuous i.v. epoprostenol infusion
Prostacyclin (prostaglandin I2 or epoprostenol) is a potent systemic and pulmonary vasodilator, powerful inhibitor of platelet aggregation, and possible inotrope 214, 215. Epoprostenol can only be administered by continuous i.v. infusion (central venous access via portable infusion pump), since its half-life in the circulation is brief (3–5 min) 214, 215. Common adverse effects attributable to epoprostenol include jaw pain, headache, diarrhoea, flush, leg pain, nausea and vomiting 239. More serious complications may occur due to the delivery system (catheter-related infections or thrombosis). The interruption of infusion may be life-threatening because of the sudden loss of vasodilatation. Ascites may be related to severe right heart failure, but also to increased permeability of the peritoneal membrane promoted by epoprostenol.
Randomised clinical trials using i.v. epoprostenol have not been performed in PPHTN, but several case series have shown substantial acute short-term and long-term improvement in pulmonary haemodynamics in New York Heart Association Functional Class III and IV patients 228, 241–244. Long-term continuous infusion of epoprostenol (up to 30 months) has resulted in significant and favourable changes in Ppa, PVR, Q' and the 6-min walking distance (6MWD) 228, 244. Regarding long-term survival and the use of epoprostenol in PPHTN, preliminary data from the Mayo Clinic (Rochester, MN, USA) suggest that i.v. epoprostenol may not result in long-term survival benefit (at 5 yrs) compared to controls with portal hypertension, unless OLT can be accomplished 179. As a cautionary note, continuous i.v. epoprostenol therapy has been followed by the development of progressive splenomegaly and worsening thrombocytopenia and leukopenia 245.
Other prostacyclin analogues (treprostinil, iloprost and beraprost)
Patients with PPHTN have been treated with long-term subcutaneous infusion of treprostinil, resulting in an improved 6MWD 246. A single patient with PPHTN was tested acutely with inhaled aerosolised iloprost, resulting in a 26% decrease in Ppa and 42% fall in PVR 247. Although oral beraprost was given to patients with portal hypertension (15% of the study population) in the Arterial Pulmonary Hypertension and Beraprost European Trial (ALPHABET), a separate data analysis was not reported 248.
Endothelin receptor antagonists (bosentan)
Bosentan is an orally available dual ET (ETA and ETB) receptor antagonist that may cause a transient increase in hepatic enzyme levels (observed in 14% of patients in two randomised trials) 249–251. Severe cases of acute hepatitis (one fatality) have been described with sitaxsentan, an ETA-receptor-selective antagonist 250. Since there are hepatic concerns, these agents should not be administered routinely to patients with PPHTN, but further studies in patients with minimal hepatic dysfunction are advised 249. ETA and ETB receptor antagonists could be considered in extrahepatic portal hypertension.
Nonpharmacological treatment
Long-term oxygen therapy
Mild-to-moderate degrees of arterial hypoxaemia at rest are a common finding in PPHTN 252. Theoretically, hypoxaemia may aggravate pulmonary hypertension by increasing pulmonary vasoconstriction, and supplemental oxygen therapy should be considered in patients with severe hypoxaemia at rest (Pa,O2 <60 mmHg). Severe hypoxaemia is, however, uncommon and should lead to investigation of the possibility of an intracardiac right-to-left shunt due to reopening of a patent foramen ovale 253, a possibility that can be suspected if the Pa,O2 response to 100% oxygen breathing is modest (<300 mmHg), or, alternatively, raise the coexistence of HPS.
Transjugular intrahepatic portosystemic shunt
There is no role for TIPS in PPHTN. In fact, the result of TIPS may acutely enhance pre-load and thus increase pulmonary arterial pressure and PVR 254, 255.
Orthotopic liver transplantation
Unlike HPS, PPHTN is not considered an indication for OLT 6, 154, 164, 256. For those with PPHTN who have undergone OLT, the survival and change in pulmonary haemodynamics has been variable, namely worsening, unchanged, improved and normalised 152, 257–277. Moderate-to-severe pulmonary hypertension (Ppa >35 mmHg) places the OLT patient at increased risk of perioperative morbidity and mortality 164, 168. Current data indicate a perioperative mortality of >50% if OLT is carried out when Ppa is 35–45 mmHg and PVR >250 dyn·s·cm−5 168. By contrast, there is no increase in mortality if Ppa is ≤35 mmHg (158, 168]. Nonetheless, there are reports of successful OLT and long-term survival in a few patients with a Ppa of >50 mmHg and elevated PVR 265.
In a recent literature review, >60% of patients with PPHTN were detected for the first time on the operating table, on induction of anaesthesia for OLT 168. When a diagnosis of moderate PAH (Ppa >35 mmHg) is made on the operating table, a careful assessment of the haemodynamic data must be undertaken. The diagnosis of PPHTN must be considered due to the major risks related to cardiac failure, particularly right ventricular failure and immediate graft failure as the result of venous congestion 163, 168. In this scenario, cardiac function is best determined by transoesophageal echocardiography 232. Indicators that would promote further therapy and cancellation of OLT surgery are poor left ventricular function, a dilated right ventricle and right atrium, and severe volume overload.
A factor to take into consideration during OLT is the 5–10% increase in Q' that may occur on reperfusion of the liver graft 232. This increase in Q' is, however, unpredictable and may reach ≥300% in a small number (up to 3.8%) of patients, precipitating right heart failure in a ventricle that is already under strain 232. The increased Q' is probably the result of the removal of the obstruction to portal blood flow by the extraction of the diseased liver, together with the systemic vasodilatation caused by washout of acid metabolites and other vasodilator substances from the new graft. Patients with a relatively fixed PVR can only react to the increased flow by an acute increase in Ppa, with subsequent right heartfailure. This unpredictable and variable response to reperfusion may be one factor explaining the different outcomes reported on patients undergoing OLT with severe PAH.
Task Force recommendations
Both PPHTN screening and haemodynamic treatment recommendations are summarised in figure 4⇑ 163, 164, 274. Despite clinical intervention, right heart failure may develop in the immediate post-OLT period 163, 164, 276. The new graft is immediately compromised and the survival of the patient may be in jeopardy. It should be noted that living-donor liver transplantation 152 and heart–double lung–liver transplantation have been accomplished in highly selected patients 278. If conventional measures fail, atrial septostomy 279 and/or the insertion of a right ventricular assist device may be life-saving 280.
The major Task Force recommendations concerning the diagnosis and treatment of PPHTN are summarised in table 7⇓. The principal differential traits between PPHTN and HPS are set out in table 8⇓. HPS is primarily a pulmonary gas exchange abnormality, whereas PPHTN is a major haemodynamic problem. Both entities can be clinically debilitating, and their diagnostic and therapeutic strategies are quite distinct 153, 281.
Research prospects
1) The genetic predisposition and mutations associated with portopulmonary hypertension and hepatopulmonary syndrome should be characterised. Similarities and distinctions as compared to the disorders of hereditary haemorrhagic telangiectasia and primary pulmonary hypertension, respectively, need to be investigated.
2) Efforts should be undertaken to identify circulating vascular mediators and their respective concentration gradients over the portal–hepatic venous and pulmonary arterial–venous circulations.
3) From a treatment perspective, further multicentric randomised trials of both the efficacy and safety of new molecules, such as oral endothelin receptor antagonists, phosphodiesterase inhibitors, serotonin transport inhibitors and inhaled prostanoids, should be considered in portopulmonary hypertension.
4) Identification of subsets of portopulmonary hypertension patients amenable to early orthotopic liver transplantation should be considered, and long-term follow-up reported.
Acknowledgments
The authors would like to express their gratitude to J. Bruix (Hospital Clínic, Barcelona, Spain) for facilitating the support of the European Association for the Study of the Liver (EASL) during the 2002 Madrid (Spain) workshop. They also thank L. Morte (Hospital Clínic, Barcelona, Spain) for administrative and expert secretarial assistance.
Footnotes
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↵ERS Task Force PHD Scientific Committee: J.A. Barberá, J.O. Cáneva, M.B. Fallon, J.C. García-Pagán, J.C. García-Valdecasas, Ph. Hervé, S. Kawut, M.J. Krowka, D. Lebrec, D. Navarro, M. Navasa, M.A.E. Ramsay, J. Rodés, R. Rodríguez-Roisin, G. Rolla, O. Sitbon, P.D. Wagner
- © ERS Journals Ltd
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