Percutaneous embolization of pulmonary arteriovenous fistulae in patients with hereditary hemorrhagic telangiectasia

Erudilho, Eduardo; Marchini, Júlio Flavio Meirelles; Ghandour, Mohamad Said; Carnieto, Nádia Mendonça; Cristovão, Salvador André Bavaresco; Mangione, José Armando

doi:10.1590/S2179-83972013000100018

Abstracts

Most cases of pulmonary arteriovenous malformations occur in patients with hereditary hemorrhagic telangiectasia. It is a rare disease that may present with stroke-like symptoms in young patients. With the development of occlusion devices, percutaneous embolization has become the treatment of choice. We report a case of a 33 year-old man with a history of multiple strokes, cyanosis, dyspnea, recurrent epistaxis and high flow pulmonary fistulae who was submitted to percutaneous embolization. The patient improved clinically and has had no recurring symptoms in the 30-month follow-up.

Embolization, therapeutic; Arteriovenous fistula; Telangiectasis; Arteriovenous malformations; Pulmonary artery

A maioria dos casos de malformações arteriovenosas pulmonares ocorre em pacientes portadores de telangiectasia hemorrágica hereditária. É uma doença incomum, que pode se apresentar com acidentes vasculares encefálicos em pacientes jovens. Com o surgimento de dispositivos de oclusão, a embolização percutânea tornou-se o tratamento de escolha. Relatamos o caso de um paciente de 33 anos de idade, com história de múltiplos acidentes vasculares encefálicos, cianose, dispneia, epistaxes recorrentes e presença de fístulas pulmonares de alto fluxo, submetido a embolização por via percutânea. O paciente apresentou melhora clínica, encontrando-se em acompanhamento há 30 meses, sem sintomas recorrentes.

Embolização terapêutica; Fístula arteriovenosa; Telangiectasia; Malformações arteriovenosas; Artéria pulmonar

CASE REPORT

^IInterventionist cardiologist physician. Assistant of the team Ariê Cardiologia Intervencionista do Hospital Beneficência Portuguesa de São Paulo. São Paulo, SP, Brazil

^IICardiologist physician. Trainee at the team Ariê Cardiologia Intervencionista do Hospital Beneficência Portuguesa de São Paulo. São Paulo, SP, Brazil

^IIIInterventionist cardiologist physician. Assistant of the team Ariê Cardiologia Intervencionista do Hospital Beneficência Portuguesa de São Paulo. São Paulo, SP, Brazil

^IVInterventionist cardiologist physician. Assistant of the team Ariê Cardiologia Intervencionista do Hospital Beneficência Portuguesa de São Paulo. São Paulo, SP, Brazil

^VInterventionist cardiologist physician. Holder of the team Ariê Cardiologia Intervencionista do Hospital Beneficência Portuguesa de São Paulo. São Paulo, SP, Brazil

^VIDoctor. Interventionist cardiologist physician. Director of the team Ariê Cardiologia Intervencionista do Hospital Beneficência Portuguesa de São Paulo. São Paulo, SP, Brazil

Correspondence to

ABSTRACT

Most cases of pulmonary arteriovenous malformations occur in patients with hereditary hemorrhagic telangiectasia. It is a rare disease that may present with stroke-like symptoms in young patients. With the development of occlusion devices, percutaneous embolization has become the treatment of choice. We report a case of a 33 year-old man with a history of multiple strokes, cyanosis, dyspnea, recurrent epistaxis and high flow pulmonary fistulae who was submitted to percutaneous embolization. The patient improved clinically and has had no recurring symptoms in the 30-month follow-up.

Descriptors: Embolization, therapeutic. Arteriovenous fistula. Telangiectasis. Arteriovenous malformations. Pulmonary artery.

Hereditary hemorrhagic telangiectasia, also known as Rendu-Osler-Weber syndrome, is an autosomal dominant disorder described in the 19^th century. It is classically diagnosed by the association of the four Curaçao criteria: recurrent epistaxis, multiple telangiectasias in characteristic sites (lips, oral cavity, fingers, and nose), visceral arteriovenous malformations, and family history.¹ There are two main types related to mutations of genes involved in the signalling of the transforming growth factor-beta (TGF-b) superfamily.² Patients with hereditary haemorrhagic telangiectasia type 1 (endoglin) have epistaxis in 50% of cases at approximately the age of 10 years, and higher frequency of symptomatic pulmonary arteriovenous malformations and brain abscesses,³ while patients with hereditary haemorrhagic telangiectasia type 2 (ACVRL1) have epistaxis ten years later than type 1, and only this type has symptomatic hepatic involvement.

There is marked variation in disease penetration and presentation; it is believed that external factors, such as tissue damage and wounds, are required for neoangiogenesis activation and telangiectasia appearance. The presence of pulmonary arteriovenous malformations allows for the passage of non-oxygenated blood into the left atrium, leading to cyanosis, and the occurrence of cerebrovascular accident is often the initial manifestation.

The present study reports the case of a patient with cyanosis, progressive dyspnoea, recurrent episodes of epistaxis, and four previous cerebrovascular accident episodes.

CASE REPORT

Male patient, 33 years old, was admitted to the emergency room with reduced level of consciousness, diversion of lip commissure to the right, right dysarthria, and paresthesia, with onset 24 hours earlier. At the consultation, he reported dyspnoea on exertion accompanied by cyanosis, epistaxis episodes since age 15, two episodes of upper gastrointestinal bleeding, and four ischemic cerebrovascular accidents. Since the patient had epilepsy, neurological monitoring was performed in order to investigate the hypotesis of central nervous system vasculitis. He reported a history of type 1 diabetes mellitus, hypothyroidism, and positive serology for human immunodeficiency virus (HIV), stage A1, with no indication of antiretrovirals. He had an uncle who had frequent episodes of epistaxis and intestinal bleeding. He regularly used NPH insulin, valproic acid, and levothyroxine.

Physical examination showed finger clubbing and telangiectasias on the palate. Laboratory tests showed hemoglobin of 17.3 g/dL. Magnetic resonance imaging of the brain showed multiple ischemic areas of various ages, consistent with acute, sub-acute, and old lesions. There were no cerebral arteriovenous malformations.

The cardioembolic etiology was investigated through echocardiography with microbubbles by transesophageal route, which showed passage of microbubbles in the left circulation, suggesting the presence of a patent foramen ovale or pulmonary arteriovenous malformations. Transcranial Doppler infused with microbubbles showed presence of large amounts of microbubbles at rest, accentuated during the Valsalva maneuver, strongly indicative of the presence of right-to-left shunt of high conductance.

Based on the clinical manifestations, personal and family history, and laboratory tests, the patient presented the four Curaçao criteria for the definitive diagnosis of hereditary hemorrhagic telangiectasia.⁴

The patient was then submitted to angiography through the right femoral artery and vein, which showed no coronary lesions, preserved left ventricular function, and presence of pulmonary arteriovenous malformations of high flow at the base (large fistulous sac with two adductor arteries, with diameters of 8 mm and 10 mm) and middle third of the right lung (small fistula with an adductor artery of 3.5 mm in diameter), and patent foramen ovale (Figure 1). There was no hypertension in left and right chambers, arterial saturation was low (84.2%), and the calculated flow through the fistula was 0.89 L/min, with a flow ratio Qp/Qs of 0.83.

Percutaneous treatment was chosen, which was performed under local anaesthesia and mild sedation (Figures 2 A, B, and ^C ). The patent foramen ovale was occluded using a 25-mm Intrasept^TM prosthesis (Cardia - Burnsville, United States) without complications. After that, adductor artery embolisation of the large pulmonary arteriovenous fistula was performed using 10-mm and 16-mm diameter Amplatzer^TM Vascular Plug prostheses (St. Jude Medical - St. Paul, United States). Despite the proper positioning of the plugs, significant residual flow was observed, and a reassessment after a few days was scheduled.

In a new study performed after five days, only partial thrombosis of the vascular plugs was observed, as well as persistence of high flow through the fistula. A new embolisation was performed using two MWCE-35-14-10-Nester coils, one MWCE-35-14-8-Nester coil, three MWCE-35-8-4-Tornado coils, and two MWCE-35-8-5-Tornado coils (Cook Medical - Bloomington, United States). These fibrous coils were positioned using the support provided by vascular plugs (^{Figure 2 D} ). Additionally, a small fistula was embolised in the middle lobe with one MWCE-38-8-5-Nester coil (Figures 2 E and F). The procedure resulted in complete interruption of flow through the shunts, with immediate improvement of arterial saturation in room air.

The patient was discharged in good clinical condition, on clopidogrel 75 mg/day for six months, and acetylsalicylic acid 200 mg/day for continuous use.

After 12 months, the patient returned to the hospital complaining of headache, nausea, and dizziness. He was hospitalized with suspected meningitis, but the diagnosis was ruled out. A new transcranial Doppler showed the passage of microbubbles, suggesting the appearance of new arteriovenous malformation. Catheterization was performed and the results showed that previously occluded shunts had remained occluded; however, there was a new pulmonary arteriovenous malformation (small fistulous sac with 4-mm adductor artery) in the right lung (Figures 3A and 3B), which was successfully embolized using a MWCE-38-5-5-Stainless Steel coil (Figure 3C).

The patient has now been followed-up for 30 months after the initial surgery, and did not have further episodes of cerebral embolism, showing improved physical capacity, although with complaints of sporadic episodes of epistaxis.

DISCUSSION

The rate of development of pulmonary arteriovenous malformations in patients with hereditary hemorrhagic telangiectasia ranges between 20% to 40% per year. These fistulas are classified as simple, characterized by a small fistulous sac with one artery and one vein representing 80% of cases, and complex, with the presence of a more developed fistulous sac with multiple septa and more than one artery and vein.⁵ The present study reported on a case with the presence of simple fistulas in the right upper and lower lobes, as well as a large complex fistula in the right lower lobe, with two adductor arteries and a large vein, resulting in high right-to-left flow.

These patients are at increased risk of paradoxical embolism due to venous thromboembolism or thrombus originating from the arteriovenous malformation itself, which may lead to severe cerebrovascular accident or brain abscess. Percutaneous closure is indicated in all symptomatic patients (cyanosis, hemoptysis, and recurrent cerebrovascular accidents) and in all who have fistulas with arteries > 3 mm in diameter, who have a higher risk of paradoxical embolism.⁶

There are no randomized studies demonstrating the best treatment option between occlusion or clinical treatment. However, there is ample evidence favouring occlusion regarding the decrease in the likelihood of cerebral embolization. Until 1977, the only available treatment was surgical, with morbidity and mortality of up to 4% to 5%; since then, percutaneous treatment has emerged as the preferred option, since it is safer and more effective.

The main complications of this procedure include device embolization, pleuritic pain, low fever and pleural effusion (10% to 35%), infection, and pulmonary infarction. The contraindications are pulmonary hypertension (moderate and severe) or pulmonary infection. To prevent device displacement, devices should be chosen with a diameter 2-mm greater than the diameter of the vessel to be occluded when using coils, or with a diameter 20% to 30% larger than the vessel when employing plugs.⁷

In this case, there was no difficulty in effectively treating simple fistulas with only one coil, but the complex fistula had large-calibre adductor arteries, poorly defined septa in the fistulous sac, and a large-calibre vein, which are predictors of high risk of coil embolization, with dire consequences for the systemic circulation. For this reason, it was chosen to use the Amplatzer^TM Vascular plug with larger dimensions than that of adductor vessels, preventing the risk of embolization. These were important for the posterior positioning of multiple coils due to the persistent flow through the fistula, after five days of follow-up, a technique succesfully used by Pereira et al.⁸

The concomitant presence of patent foramen ovale increased the chance of paradoxical thromboembolism, and, therefore, it was occluded with a 25-mm Cardia prosthesis, guided by transesophageal echocardiography. Although the patent foramen ovale was small, had a short tunnel, and did not present interatrial septal aneurysm, the decision to occlude it was based on the presence of right-to-left shunt through the interatrial septum in a patient with multiple previous episodes of cerebrovascular accident.

The physiopathology of arteriovenous malformation development appears to involve not only the lack of inhibition of the neoangiogenesis pathway due to lack of activation of components of the TGF-b receptor superfamily, but also tissue injury.⁹ Within this model, it is expected that new arteriovenous malformations will be established in the future, due to new episodes of injury to which biological tissues are subject. In fact, the recurrence rate is 3% a year.¹⁰

Despite the technical difficulty and high risk of occluder device embolization in complex pulmonary arteriovenous malformation, the initial choice of the vascular plug, complemented by fibrous coils, made the percutaneous treatment feasible and safe in this case. It is believed that concomitant treatment of patent foramen ovale was also important for an evolution free of embolic events at the 30-month follow-up.

CONFLICTS OF INTEREST

The authors declare to have no conflicts of interest.

REFERENCES

1. Richards-Yutz J, Grant K, Chao EC, Walther SE, Ganguly A. Update on molecular diagnosis of hereditary hemorrhagic telangiectasia. Hum Genet. 2010;128(1):61-77.
2. Dupuis-Girod S, Bailly S, Plauchu H. Hereditary hemorrhagic telangiectasia: From molecular biology to patient care. J Thromb Haemost. 2010;8(7):1447-56.
3. Lesca G, Olivieri C, Burnichon N, Pagella F, Carette MF, Gilbert-Dussardier B, et al. Genotype-phenotype correlations in hereditary hemorrhagic telangiectasia: data from the French-Italian HHT network. Genet Med. 2007;9(1):14-22.
4. Shovlin CL, Guttmacher AE, Buscarini E, Faughnan ME, Hyland RH, Westermann CJ, et al. Diagnostic criteria for hereditary hemorrhagic telangiectasia (Rendu-Osler-Weber syndrome). Am J Med Genet. 2000;91(1):66-7.
5. Reidy JF. Pulmonary arterio-venous fistulas. In: Sievert H, Qureshi S, Wilson N, Hijazi Z, editors. Percutaneous interventions for congenital heart disease. Abingdon: Informa UK; 2007. p. 419-22.
6. Abdel-Aal AK, Saddekni S, Underwood E, Oser RF, Vattoth S. Innumerable bilateral pulmonary arteriovenous malformations: percutaneous transcatheter embolization using Amplatzer vascular plug. Vasc Endovascular Surg. 2012;46(6):475-9.
7. Bertog SC, Steinberg DH, Frankie J, Wunderlich N, Sievert H, Ruygrok PN. Closure of arteriovenous fistulae and malformations. In: Eeckhout E, Serruys PW, Williams W, Vahanian A, Van Sambeek M, De Palma R, editors. Percutaneous interventional cardiovascular medicine. Spain: PCR; 2012. p. 446-8.
8. Pereira FL, Ribeiro MS, Costa RN, Braga SLN, Fontes VF, Pedra CAC. Experiência clínica com a utilização de plugs vasculares Amplatzer^® Rev Bras Cardiol Invasiva. 2010;18(3):327-36.
9. Park SO, Wankhede M, Lee YJ, Choi EJ, Fliess N, Choe SW, et al. Real-time imaging of de novo arteriovenous malformation in a mouse model of hereditary hemorrhagic telangiectasia. J Clin Invest. 2009;119(11):3487-96.
10. White RI Jr. Pulmonary arteriovenous malformations: how do I embolize? Tech Vasc Interv Radiol. 2007;10(4):283-90.

Percutaneous embolisation of pulmonary arteriovenous fistulae in patients with hereditary haemorrhagic telangiectasia

Eduardo Erudilho^I; Júlio Flavio Meirelles Marchini^II; Mohamad Said Ghandour^III; Nádia Mendonça Carnieto^IV; Salvador André Bavaresco Cristovão^V; José Armando Mangione^VI

Publication Dates

Publication in this collection
09 May 2013
Date of issue
Mar 2013

History

Received
18 Dec 2012
Accepted
21 Feb 2013

This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

[1] 1. Richards-Yutz J, Grant K, Chao EC, Walther SE, Ganguly A. Update on molecular diagnosis of hereditary hemorrhagic telangiectasia. Hum Genet. 2010;128(1):61-77.

[2] 2. Dupuis-Girod S, Bailly S, Plauchu H. Hereditary hemorrhagic telangiectasia: From molecular biology to patient care. J Thromb Haemost. 2010;8(7):1447-56.

[3] 3. Lesca G, Olivieri C, Burnichon N, Pagella F, Carette MF, Gilbert-Dussardier B, et al. Genotype-phenotype correlations in hereditary hemorrhagic telangiectasia: data from the French-Italian HHT network. Genet Med. 2007;9(1):14-22.

[4] 4. Shovlin CL, Guttmacher AE, Buscarini E, Faughnan ME, Hyland RH, Westermann CJ, et al. Diagnostic criteria for hereditary hemorrhagic telangiectasia (Rendu-Osler-Weber syndrome). Am J Med Genet. 2000;91(1):66-7.

[5] 5. Reidy JF. Pulmonary arterio-venous fistulas. In: Sievert H, Qureshi S, Wilson N, Hijazi Z, editors. Percutaneous interventions for congenital heart disease. Abingdon: Informa UK; 2007. p. 419-22.

[6] 6. Abdel-Aal AK, Saddekni S, Underwood E, Oser RF, Vattoth S. Innumerable bilateral pulmonary arteriovenous malformations: percutaneous transcatheter embolization using Amplatzer vascular plug. Vasc Endovascular Surg. 2012;46(6):475-9.

[7] 7. Bertog SC, Steinberg DH, Frankie J, Wunderlich N, Sievert H, Ruygrok PN. Closure of arteriovenous fistulae and malformations. In: Eeckhout E, Serruys PW, Williams W, Vahanian A, Van Sambeek M, De Palma R, editors. Percutaneous interventional cardiovascular medicine. Spain: PCR; 2012. p. 446-8.

[8] 8. Pereira FL, Ribeiro MS, Costa RN, Braga SLN, Fontes VF, Pedra CAC. Experiência clínica com a utilização de plugs vasculares Amplatzer^® Rev Bras Cardiol Invasiva. 2010;18(3):327-36.

[9] 9. Park SO, Wankhede M, Lee YJ, Choi EJ, Fliess N, Choe SW, et al. Real-time imaging of de novo arteriovenous malformation in a mouse model of hereditary hemorrhagic telangiectasia. J Clin Invest. 2009;119(11):3487-96.

[10] 10. White RI Jr. Pulmonary arteriovenous malformations: how do I embolize? Tech Vasc Interv Radiol. 2007;10(4):283-90.

Brasil