Abstract
Pulmonary hypertension (PH) is a major complication of several haematological disorders. Chronic myeloproliferative diseases (CMPDs) associated with pulmonary hypertension have been included in group five of the clinical classification for pulmonary hypertension, corresponding to pulmonary hypertension for which the aetiology is unclear and/or multifactorial. The aim of this review is to discuss the epidemiology, pathogenic mechanism and treatment approaches of the more common forms of pulmonary hypertension in the context of CMPD's: chronic thromboembolic pulmonary hypertension, precapillary pulmonary hypertension and drug-induced PH.
Abstract
Epidemiology, pathogenic mechanism and treatment approach of PH in patients with chronic myeloproliferative diseases http://ow.ly/Q1QX4
Introduction
Pulmonary hypertension (PH), which is defined as an elevated mean pulmonary artery pressure ≥25 mmHg at rest [1–3], is a major complication of several haematological disorders. Chronic myeloproliferative diseases (CMPDs) associated with PH are included in group five of the most recent clinical classification (from the fifth World Symposium on PH, Nice, 2013), corresponding to PH with an unclear and/or multifactorial aetiology (table 1) [3]. An improvement in the characterisation of this group of diseases should be encouraged in order to support clinicians in the management of these patients with severe comorbidities, as emphasised by Simonneau et al. [2].
The haematopoietic pluripotent stem cell is capable of both self-renewal and a stepwise differentiation, after a stochastic determination, into either the lymphoid or myeloid lineage. An operational classification of haematological malignancies separates lymphoid from myeloid processes and divides them into acute or chronic according to rate of progression. The chronic myeloid disorders encompass several clinical–pathological entities including the myelodysplastic syndromes and myeloproliferative disorders, which are gathered into seven disorders in the World Health Organization (WHO) classification of the CMPDs (table 2) [5].
The pathogenesis of CMPDs involves a multipotent haemopoietic progenitor cell overproducing one or more of the elements that form the blood without significant dysplasia. CMPDs are a heterogeneous group of disorders with a different genetic basis. Disorders with primary expression of a myeloid phenotype include chronic neutrophilic leukaemia (CNL), chronic eosinophilic leukaemia (CEL) and chronic myelogenous leukaemia (CML), as they are the consequence of the balanced translocation between chromosomes 9 and 22 (the Philadelphia chromosome) [6]. By contrast, in essential thrombocytosis, polycythaemia vera and idiopathic myelofibrosis erythroid or megakaryocytic hyperplasia predominates with a different rate of expression of a JAK2 (Janus kinase 2) mutation, V617F [7]. The difference between the two groups is also reflected in the natural history of the diseases. CML, CNL and CEL have a high rate of transformation into acute leukaemia, while polycythaemia vera, idiopathic myelofibrosis and essential thrombocytosis have relatively indolent clinical courses even though they may show recurrent thrombo-haemorrhagic complications. The annual incidence of CMPDs is estimated at 6–9 new cases per 100 000 population, occurring most commonly between 40 and 60 years of age. The most frequent pulmonary complications are caused either by infection or by venous thromboembolic events. Pulmonary or pleural extramedullary haematopoiesis is a rare complication that may be associated with myelofibrosis [8, 9].
Epidemiology
The possible association between PH and CMPDs has been suggested by several case reports and small case series. However, the prevalence and incidence of PH in the context of CMPDs may be underestimated since the clinical signs of disease appear at an advanced stage of the disease and, in some cases, the diagnosis of CMPDs is difficult to establish in the context of chronic hypoxaemia.
To evaluate cardiac involvement in CMPDs, Reisner et al. [10] performed two-dimensional and Doppler echocardiographic studies in 30 patients (18 women and 12 men): 18 patients had polycythaemia vera, eight had essential thrombocytosis and four had angiogenic myeloid metaplasia. Four (13%) out of 30 were diagnosed with PH unrelated to valvular disease [10]. In another study, a cohort of 24 patients, the majority of whom were affected by essential thrombocytosis (14 out of 24), underwent an echocardiographic study [11]. PH, defined by right ventricular systolic pressure (RVSP >35 mmHg), was found in 10 (41.7%) patients, four males and six females, with a mean RVSP of 42 mmHg (range 37–70 mmHg). Age, sex, presence of splenomegaly, type of CMPD, duration of CMPD, age at diagnosis of CMPD, presence of symptoms, haemoglobin levels, and white blood cell or platelet count were not predictive of the presence of PH [11]. Altintas et al. [12] found PH in 22 (47.8%) patients out of 46 affected by essential thrombocytosis in an echocardiographic study (PH was defined as RVSP >35 mmHg). In this group of patients significantly higher platelets counts were observed. Another group [13], without confirmation of right heart catheterisation, described PH in 12 (48%) out of 25 patients with CMPDs. No relationship between PH and age at diagnosis, duration of disease, platelet count and haematocrit level was described.
The association between PH and primary myelofibrosis, since angiogenesis is believed to contribute to the pathogenesis of both conditions, was investigated in a group of 36 patients, of whom 22 were affected by primary myelofibrosis, seven by myelofibrosis developing from polycythaemia vera and seven by myelofibrosis progressing from essential thrombocytosis [14]. PH, in this case evaluated by means of transthoracic echocardiography, was found in 13 (36%) patients.
Roach et al. [15] evaluated cardiac function by means of echocardiography in 19 patients with myelofibrosis, 30 patients with aplastic anaemia and 82 patients with chronic myelogenous leukaemia. They found a higher level of estimated RVSP in patients with myelofibrosis when compared with the other patients [15].
Unpublished data from our group at the Carmel Medical Center (Haifa, Israel) showed that 22 out of 49 patients had PH, as determined by a RVSP>35 mmHg (mean 55.23±12.29 mmHg) in an echocardiographic study. In 13 out of the 22 patients, the elevated pulmonary artery pressure related to heart disease. No obvious reason for the increased pulmonary artery pressure was found in only nine (18.4%) out of the 49 patients. None of the clinical characteristics of the patients was able to identify those at risk for the development of PH. A recent, larger study by Chebrek et al. [16] evaluated 103 patients with CMPDs (including 32 patients with CML, 27 patients with essential thrombocytosis and 15 patients with myelofibrosis) and found rather a low prevalence of PH. Only five patients were found to have increased pulmonary artery pressure (<5%). Again, PH in this study was defined by echocardiography (RVSP >35 mmHg) [16].
Increased pulmonary artery pressure in patients with CMPDs may result from various mechanisms including anaemia, and a hypermetabolic state with high cardiac output and left ventricular dysfunction. Therefore, transthoracic Doppler echocardiography can only be used as a screening tool and may overestimate the prevalence of PH. This implies that a right heart study with full haemodynamic evaluation is mandatory for the correct diagnosis of PH [17–19].
Three major distinct clinical forms of PH have been described in patients with CMPDs: chronic thromboembolic PH (CTEPH), precapillary PH and drug-induced PH. Although a thrombophilic state is common in CMPDs, the clinical data on CTEPH and CMPDs is scarce. A previous clinical series described six patients with CTEPH (five presented with polycythaemia vera and one with essential thrombocytosis) [20]. Interestingly the diagnosis of CTEPH and CMPD was made simultaneously in all patients, suggesting that CTEPH could be the first manifestation of myeloproliferative disease. By contrast, precapillary PH associated with CMPD is diagnosed late in the course of the disease [20–22]. In the report by Dingli et al. [20], precapillary PH was diagnosed on average 8 years after recognition of the myeloproliferative disorder (range: 0–26 years); while in the study by Guilpain et al. [21], precapillary PH occurred later in the evolution of the CMPDs, at a median of 162 months (13.5 years), and was associated with myeloid metaplasia.
Chronic thromboembolic pulmonary hypertension
Aetiology
CMPDs, particularly polycythaemia vera and essential thrombocytosis, are characterised by a thrombophilic state, which may lead to microcirculatory disturbances, and arterial and venous thrombosis [23] (fig. 1). In polycythaemia vera the majority of the thrombotic events are arterial, in fact only about one third correspond to venous thrombosis, while in essential thrombocytosis there is a predominance of the arterial ones [24].
Unfortunately the incidence of thrombosis in polycythaemia vera and essential thrombocytosis has been difficult to establish; however, at presentation the reported incidence of thrombosis in essential thrombocytosis and polycythaemia vera varied from 11% to 25% and from 12% to 39%, respectively [23–27]. More recent series tend to describe lower incidence figures that are probably a result of both a lead time bias in diagnosis and improved therapy. The incidence of thrombotic events during follow up remains substantial. Cortelazzo et al. [28] reported that the overall risk of thrombosis in essential thrombocytosis was 6.6% per patient-year versus 1.2% per patient-year in a controlled population. The risk factors for thrombotic events include elevated red blood cell counts, higher haemoglobin levels, an increased percentage of nucleated neutrophils at the time of diagnosis, older age and a history of thrombosis.
The pathogenesis of thrombotic events in these diseases is multifactorial. Increased blood hyperviscosity, due to high haematocrit values in polycythaemia vera, causes a major disturbance to blood flow, increasing platelet activation and platelet–platelet interactions with an higher risk of thrombosis [29]. In addition, the formation of red blood cell aggregates, induced by the red blood cell abnormalities occurring in polycythaemia vera and essential thrombocytosis, directly contribute to flow disturbance, thrombosis and platelet activation, especially in small vessels [23, 30, 31].
Erythropoietin-independent erythroid colony (EEC) formation, which is considered to be among the criteria for polycythaemia vera diagnosis, is also considered to be a surrogate marker for increased thrombotic risk. Spontaneous EEC formation may be associated with thrombosis, particularly of hepatic veins, in the absence of other peripheral blood abnormalities. The presence of EEC formation leads to the diagnosis of a primary myeloproliferative disorder in 78% of cases with apparent idiopathic Budd–Chiari syndrome and in about half of patients with portal, splenic and/or mesenteric venous thrombosis [32, 33]. It seems that the EEC formation test might be of interest in order to unmask as yet unrecognised CMPDs in CTEPH patients. The platelet count per se has not been significantly correlated with thrombosis risk in either polycythaemia vera or essential thrombocytosis. However, in high-risk patients, lowering the platelet count to below 400×109 L−1 might reduce the incidence of thrombotic events [23, 25, 34, 35].
Patients with CMPDs manifest abnormal in vivo platelet activation with resultant granule release and shortened platelet survival [24]. In polycythaemia vera associated with thrombocythaemia, hyperviscosity aggravates the platelet-mediated microvascular disturbances of thrombocythaemia and may cause major arterial and venous thrombotic complications. Thrombocythaemia persists even after correction of hyperviscosity by phlebotomy [23, 36]. However, no correlation was found in other studies between the degree of thrombocytosis, the presence of platelet dysfunction and the risk of thrombosis in polycythaemia vera [26, 35].
As they are disorders of haematopoietic stem cells, the potential role of clonal leukocytes in the pathogenesis of thrombosis in polycythaemia vera and essential thrombocytosis is supported by several studies and would be consistent with the well-established anti-thrombotic effect of myelosuppressive therapy. An ongoing state of polymorphonuclear leukocyte (PMN) activation, related to increased plasma level markers of clotting activation, has been demonstrated [23, 27, 37].
The presence of the acquired gain-of-function V617F mutation in the tyrosine kinase JAK2 gene has been demonstrated in PMNs and platelets of patients with CMPDs [37, 38]. Furthermore, patients affected by essential thrombocytosis harbouring a JAK2 mutation show a “polycythaemia vera-like” phenotype with an increased rate of venous thrombosis [39]. In addition, the association between JAK2 mutation and thrombosis at uncommon sites with no relation to the CMPD has been described in several studies. Patients with the JAK2 mutation have increased PMN activation, with platelet aggregation and activation, contributing to the increase in the susceptibility to thrombotic events in patients with CMPDs [23, 40, 41].
Splenectomy is considered a risk factor for the development of CTEPH. Thromboembolic complications following splenectomy for haematological diseases occur in up to 10% of patients and may range from portal vein thrombosis to pulmonary embolism and deep vein thrombosis [42–44]. However, Bonderman et al. [45] conducted a prospective case–control study of 109 patients and did not find any relationship between splenectomy and CTEPH.
Thrombocytosis per se, following splenectomy, is not thought to be the major factor predisposing patients to thrombosis. Loss of the filtering function of the spleen, which allows abnormal red cells to remain in the peripheral circulation, may lead to activation of the coagulation system.
A worsening extramedullary haematopoiesis is seen in patients with CMPDs after splenectomy, with the potential for pulmonary infiltration. In addition, the functional abnormal platelets in CMPDs, together with the marked elevations in their counts, may explain the difference in the interval before the development of PH, which is shorter in patients with CMPDs [23]. In a case series of 10 patients with CMPDs and PH, the platelet count was not different between patients with CTEPH and pulmonary arterial hypertension (PAH) associated with CMPDs [21]. Elevated haematocrit was significantly associated with CTEPH compared with the four patients with precapillary PH, suggesting that elevated haematocrit may contribute to the development of pulmonary artery thrombosis. Interestingly, none of the patients with CTEPH had undergone a splenectomy.
Treatment
The management of arterial and venous thrombosis in polycythaemia vera and essential thrombocytosis patients should be the same as that recommended in the general population [46, 47].
Pulmonary endarterectomy is the first choice treatment in patients with CTEPH [47]. However, in inoperable cases, due to a personal choice, the anatomic distribution of their disease, the extent of their disease or their comorbidities, medical therapy including diuretics, anticoagulants and specific PAH therapy should be considered. Several small studies in patients with CTEPH have shown that the endothelin receptor antagonists, particularly oral bosentan, improve symptoms and exercise capacity [48]. In the only randomised placebo-controlled trial (BENEFIT trial), 157 patients (WHO functional class II–IV, mild to severe disease) with inoperable CTEPH (or persistent CTEPH after thromboendarterectomy) were randomly assigned to receive oral placebo or bosentan for 16 weeks. Compared with placebo, bosentan therapy was associated with improved pulmonary vascular resistance and cardiac index. However, bosentan therapy did not improve exercise capacity in this population [49].
Recently, in patients with inoperable CTEPH (WHO functional class II–III, mild to moderate disease) riociguat, a guanylate cyclase stimulator, was shown to improve exercise capacity and pulmonary haemodynamics [50]. In a multicentre, randomised placebo-controlled trial of 261 patients with either inoperable CTEPH (189 patients) or persistent PH (72 patients) following pulmonary thromboendarterectomy (CHEST-1 trial) riociguat improved 6-min walking distance and pulmonary vascular resistance [51]. Currently, no data specific to CTEPH-associated with CMPDs are available.
Hydroxyurea has been found to reduce the risk of thrombosis in high risk patients [23], possibly due to its effect on leukocyte count and leukocyte activation [52]. For this reason cytoreductive therapy with hydroxyurea is recommended [53, 54]. The effectiveness of antiplatelet agents in reducing the incidence of vascular events is of value in patients with polycythaemia vera [54], while the use of aspirin in essential thrombocytosis is controversial and there is a potential increased risk of bleeding [23, 56].
Precapillary pulmonary hypertension
Aetiology
Precapillary PH in patients affected by CMPDs may be caused by several factors. First, portal hypertension, a well-known complication of myeloid metaplasia with myelofibrosis, may cause PAH [57, 58]. However, although portal hypertension is seen in up to 17% of patients with myeloid metaplasia and myelofibrosis, the coexistence of both PH and portal hypertension is rare [20, 21].
Another cause of PH during cytotoxic chemotherapy and haematopoietic stem cell transplantation is pulmonary veno-occlusive disease (fig. 2) [59]. Willems et al. [60] have described a case of veno-occlusive disease, diagnosed by means of a biopsy, as a cause of severe PH in a patient suffering from a CMPD. In this case, the use of anagrelide several weeks before the manifestation of the symptoms may suggest this treatment has a role in the pathogenesis of a pulmonary veno-occlusive disease. Moreover, in six patients with CMPDs and echocardiographic findings of PH [61], the presence of clinical signs, such as the presence of low oxygen saturation at rest and a low diffusing capacity of the lung for carbon monoxide, as well as radiological manifestations, such as centrilobular ground-glass opacities, septal lines and lymph node enlargement on high-resolution computed tomography of the chest, suggested the diagnosis of pulmonary veno-occlusive disease with a high probability. However, the diagnosis of pulmonary veno-occlusive disease was achieved late in the course of the disease with a poor prognosis [62].
Another explanation for the pathogenesis of PH during the course of a myeloproliferative disorder may be the presence of a tumour microembolism, as found in various tumours. In patients affected by progressive myeloproliferative syndrome, translocation of megakaryocytes from the bone marrow, spleen or liver to the lungs may produce megakaryocyte embolism of pulmonary vessels, eventually leading to PH [63]. In fact, an increase in circulating megakaryocytes and myeloid progenitor cells, which are poorly deformable and larger than the alveolar capillary diameter, was observed in myelofibrosis and myeloid metaplasia. As a consequence, these cells may occlude the pulmonary microvasculature and secrete vasoactive cytokines, leading to the development of PH. The case of a patient with myeloid metaplasia, PH and right heart failure, with thrombocytosis and circulating megakaryocytes after splenectomy has been described [64]. The obstruction caused by megakaryocytes with stasis and secondary microthrombosis was thought to lead to the PH. Furthermore, many cases of CMPDs and PH have been described. Histological examination of the lung showed the presence of an obstruction of the small vessels by conglomerates of megakaryocytes [62, 63, 65].
A causal relationship between pulmonary myeloid infiltration during the chronic phase of agnogenic myeloid metaplasia and leukaemic infiltration during the acute transformation of the disease and the development of PH has been suggested. Steensma et al. [66] described four patients with myelofibrosis with myeloid metaplasia who developed severe PH. Technetium-99m sulfur colloid scintigraphy demonstrated diffuse pulmonary uptake, showing extramedullary haematopoiesis. Furthermore, in another case report an open lung biopsy demonstrated the presence of extramedullary haematopoiesis in an elderly woman with myelofibrosis and PH [67].
Although no clear association was found between platelet count and the risk of thrombosis, a correlation between elevated pulmonary artery pressure and platelet count was reported in patients with myeloid metaplasia and essential thrombocytosis, and with haemoglobin levels in patients with polycythaemia vera. Platelets seem to play a central role in the aetiology of PH; in fact, platelet-derived growth factor released from activated platelets is a strong stimulus for smooth muscle hyperplasia [68, 69] and in an animal model of PH the control of the platelet count delays the development of PH [70].
Marvin and Spellberg [64] reported that cytoreductive therapy, by decreasing the platelet count, reversed PH and right heart failure in a 72-year-old patient with myeloid metaplasia; however, the effect of the cytoreductive therapy may have been related to its effect on white blood cells. In a study by Dingli et al. [20], 12 out of 26 patients were treated with aspirin before PH was diagnosed suggesting that antiaggregant agents, as opposed to cytoreductive therapy, probably have no effect in preventing or reversing PH.
Finally, a possible pathogenic link between CMPDs and PH has been found in the peripheral blood and bone marrow, because of an enhanced angiogenesis. In this study, patients with primary myelofibrosis and PH had higher bone marrow microvessel density and vascular endothelial growth factor levels, suggesting the presence of a pro-angiogenic phenomenon [14, 71]. Other studies demonstrated that distinctive features of myelofibrosis associated with PH include normal or low circulating CD34 cell count, polyclonal platelets and granulocytes, the absence of peripheral blood dacrocytes and the JAK2 1849G>T(V617F) mutation [72, 73].
Treatment
Currently there is no effective treatment for PH associated with CMPDs. Cytoreductive therapy may have a role but the evidence is anecdotal. A previous study reported that, despite good CMPD control, there was no improvement in PH over time [20], while another case study described reversibility of PH with cytoreductive therapy and reduction of platelet counts, or due to therapeutic phlebotomies [64].
A treatment trial using whole-lung low-dose external beam radiotherapy has been suggested for patients with CMPDs and PH and evidence of extramedullar myelofibrosis as a palliative measure [66, 67]. There is no data on the role of anticoagulation and antiaggregants in patients with precapillary PH associated with CMPDs.
Dysregulation of JAK family kinases, specifically JAK1 and JAK2, contributes to the pathogenesis of myelofibrosis. Ruxolitinib, an oral JAK1/JAK2 inhibitor, is used for the treatment of intermediate-to-high risk myelofibrosis patients. Tabarroki et al. [74] described 15 patients with myelofibrosis and PH treated with ruxolitinib, in 66% of the patients an improvement of pulmonary artery pressure and right ventricle function measured by echocardiography was observed. Furthermore, ruxolitinib also decreased plasma levels of N-terminal pro-brain natriuretic peptide, von Willebrand antigen, ristocetin-cofactor activity and uric acid, and increased nitric oxide levels. This study suggests that aberrant JAK signal transducer and activator of transcription signalling in myelofibrosis may mediate PH through dysregulation of nitric oxide and cytokine levels, which can be restored by therapy with JAK inhibitors [74].
However, recently an association between worsening PAH and ruxolitinib, with improvement on withdrawal of the drug on two separate occasions, has been described in a 57-year-old woman with progressive myelofibrosis, testing positive for the JAK2 V617F mutation [75].
The effectiveness of pulmonary vasodilators used for PAH, including endothelin receptor antagonists, prostacyclin analogues and phosphodiesterase-type 5 inhibitors, should be further studied.
Drug-induced PH
Tyrosine kinase inhibitors (TKIs), such as imatinib, dasatinib and nilotinib, have recently being used as a therapy for CML with improved prognosis. Although TKIs are usually well tolerated, these agents are nevertheless associated with certain systemic side-effects such as oedema, musculoskeletal pain, diarrhoea, rash and cardiac toxicity, especially with imatinib. Pulmonary complications and specifically pleural effusions have been reported more frequently with dasatinib.
Several case reports have suggested that PH may be a potential specific complication of dasatinib use [76, 77]. The evaluation of the French registry data suggests that the lowest estimated incidence of dasatinib-associated PAH is 0.45% and dasatinib is considered a probable cause of PAH in the last updated PH classification [78]. Symptoms generally appear after 8–48 months of therapy and reported mean pulmonary artery pressures by right heart catheterization are 25–50 mmHg. Although a few patients have experienced full clinical and haemodynamic recovery, the majority have not recovered completely after a follow-up that ranges from 3 to 36 months (median 9 months) [76–78]. Montani et al. [78] described subsequent administration of an endothelin receptor antagonist in two patients and a calcium channel blocker to a third patient; it is not clear whether any subsequent improvement was related to these therapies, dasatinib discontinuation, or both.
No other PH cases were reported with the use of other TKIs at the time of PH diagnosis. Interestingly, clinical and haemodynamic improvements have been reported with imatinib therapy in two patients with CML and coexistent severe precapillary PH. It was suggested that this effect could be due to inhibition of tyrosine kinase targets of imatinib such as platelet-derived growth factor receptors and c-kit. In those patients with PH probably induced by dasatinib, clinical, functional and haemodynamic improvements were observed within 4 months of dasatinib discontinuation in all but one patient. However, after a median follow-up of 9 months, most patients did not demonstrate complete recovery and two patients died [78].
Prognosis
The prognosis of patients with precapillary PH associated with CMPDs is poor [21–23]. Precapillary PH occurs late in the course of the disease and the median survival is up to several months after diagnosis. In the study by Dingli et al. [20], the median survival time was 18 months and death was mainly related to cardiopulmonary failure. Garcia-Manero et al. [22] reported that the interval between the development of dyspnoea (leading to the diagnosis of PH) and death was <7 months in five out of six patients. In patients with CTEPH, pulmonary endarterectomy, if suitable, may reverse PH and improve prognosis. Data about the use of specific therapies in this group of patients are still not available.
Conclusion
To sum up, the exact incidence and prevalence of PH in patients with CMPDs is poorly defined. Three distinct clinical forms of PH have been described in patients with CMPDs: CTEPH, precapillary PH and drug-induced PAH. Precapillary PH is usually diagnosed late in the course of the haematological disease, while CTEPH is usually diagnosed earlier and may even be concurrent with the haematological diagnosis. Dasatinib, which is used for the treatment of CML, is considered to be a probable cause of PAH. High haematocrit levels with hyperviscosity, thrombocytosis and splenectomy may contribute, among other mechanisms, to the increased rate of thrombotic events in patients with CMPDs, especially polycythaemia vera. PAH-like disease associated with CMPD was found to be related to myeloid metaplasia, suggesting that pulmonary myeloid infiltration and pulmonary capillary obstruction by megakaryocytes with stasis and secondary microthrombosis may contribute to the pulmonary vascular disease. When PH is diagnosed, secondary causes which may contribute to the elevated pulmonary pressure, such as anaemia and heart failure, should be recognised and treated. However, when PH persists, treatment is not yet established. Anticoagulant drugs should be administered carefully because of the potential risk of haemorrhagic complications. Cytoreductive treatment should be used in association with symptomatic treatment of PH, such as oxygen and diuretics. There are no data on the effectiveness of specific PAH therapies in these patients and randomised control trials are needed. The prognosis of PH associated with CMPDs remains poor. However, pulmonary endarterectomy is the treatment of choice in eligible patients with proximal CTEPH.
Footnotes
Conflict of interest: Disclosures can be found alongside the online version of this article at err.ersjournals.com
Provenance: Publication of this peer-reviewed article was sponsored by F. Hoffman-La Roche Ltd, Basel, Switzerland (principal sponsor, European Respiratory Review issue 137).
- Received May 14, 2015.
- Accepted July 23, 2015.
- Copyright ©ERS 2015.
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