Institute of Diagnostic and Interventional
Radiology/Neuroradiology, Westkuestenklinikum – Academic
Teaching Hospital of the Universities of Kiel, Lübeck and
Hamburg, Heide, Germany
Objective. To evaluate, in a retrospective study, the clinical efficacy and safety of the self-expanding Nitinol stent in the superior vena cava to alleviate upper venous congestion.
Method. In 22 patients (15 men, 7 women), a tumour-related compression of the superior vena cava was diagnosed by spiral CT after intravenous application of contrast medium. Clinically, acute superior vena cava syndrome was found in all patients. Histologically, a bronchial carcinoma was present in 14/22, a lymphoma in 6/22, and mediastinal lymphnode metastases (1 breast carcinoma, 1 malignant melanoma) in 2/22. After a transfemoral approach, cavography was initially performed. The degree of stenosis was classified according to the Stanford classification. In accordance with the degree of stenosis, a self-expanding Nitinol stent was placed.
Results. Endovascular stent implantation was conducted without complications in all patients. A marked improvement in acute symptoms was observed clinically within 24 hours in all patients. In the follow-up period of up to 2 years, there were no cases of stent migration. In 7/22 patients, the CT follow-ups revealed tumour progression (3/7 after 3 months, 2/7 after 6 months, and 2/7 after 12 months) with evidence of residual stenosis caused by tumour growth through the stent mesh. During the follow-up period, 15/22 patients died (mean survival 6.4 months).
Conclusion. Self-expanding Nitinol stents
provide endovascular therapy for superior vena cava syndrome,
having a high radial expansive force and the facility to be
placed precisely, and alleviating acute, life-threatening
symptoms in the palliative situation.
S
Afr J Rad
2013;17(4):123-127. DOI:10.7196/SAJR.864
Superior vena cava syndrome (SVCS) is characterised by venous congestion and increased pressure resulting from displacement or compression of the superior vena cava (SVC). Venous congestion leads to swelling of the soft tissues of the face and neck, dyspnoea and dysphagia, extending to glottal and laryngeal oedema and the development of cerebral oedema with headache and clouded consciousness. The evolving life-threatening situation generally takes a slow and progressive course, and is rarely acute.1
The cause of the obstruction can be a thrombosis or an invasion or external compression of the SVC by topographically adjacent pathological processes, especially originating in the right lung, lymph nodes and other mediastinal structures. In rare cases, a combination of external compression and cava thrombosis is present.2 In 74 - 95% of cases, malignant tumours are the primary cause of upper venous congestion, which typically results from an advanced lung carcinoma (about 80%), more rarely from a lymphoma (about 15%) or metastasis of an extrathoracic tumour (about 5%). Up to 5% of patients with a lung carcinoma develop upper venous congestion during their illness.3 As a result of the usually rapidly advancing central tumour growth, small cell lung carcinomas (SCLCs) lead to compression of the SVC more often than do non-small cell lung carcinomas (NSCLCs).
The increasing use of central venous catheters or the implantation of cardiac pacemakers can lead to thromboses or central nervous obstructions and thus also, in rare cases, result in SVCS.4
In the case of life-threatening SVCS, rapid assistance is required to alleviate the acute symptoms and improve quality of life. Endovascular therapy by stent implantation has proved to be an effective treatment method here. Self-expanding metal stents, such as the Wallstent (Boston Scientific, Nastrick MA, USA) have been used till now.6
This retrospective study (2009
-2013) assessed the clinical efficacy and safety of
self-expanding Nitinol stents (Sinus XL, Optimed, Ettlingen,
Germany) in the treatment of acute, tumour-related SVCS. These
stents have been authorised for the treatment of cava
obstructions and for vena cava syndrome.
The indication for intervention was previously
established by an interdisciplinary tumour board, consisting of
internists/oncologists, surgeons, gynaecologists, neurosurgeons,
radio-oncologists and radiologists. Pre-interventionally,
patients were advised by the treating interventionalist about
the course of the procedure, risks and expected outcome. Written
consent was obtained from all patients before the intervention
was performed.
In 22 patients (15 men, 7 women, average age
65.9 years), a tumour-related compression of the SVC was
diagnosed by multidetector computed tomography (MDCT) of the
chest (Table 1). After injecting 100 ml Imeron 350 via an
antecubital vein in the left arm at a rate of 3 ml/s and a delay
of 30 s, CT was performed, with a 3 mm slice thickness and 3 mm
reconstruction interval. Clinically, acute SVCS was found in all
patients.
Acute or rapidly progressive dyspnoea and a swelling of the soft tissues of the face and neck led to inpatient admission in all cases (22/22). All patients were also characterised by dilatation of the jugular veins. Dilated veins of the chest wall were also found in 7/22 patients. Histologically, 14/22 had a lung carcinoma (9 SCLC, 5 NSCLC), 6/22 a lymphoma (non-Hodgkin lymphoma) and 2/22 mediastinal lymph node metastases (1 breast carcinoma, 1 malignant melanoma).
At the time of endovascular therapy, a
definitive histological diagnosis was known in 18/22 patients. A
CT-assisted biopsy was conducted in 4/22 over the further
course. If the tumour entity was known, intensive therapy
(radiochemotherapy) was started or continued. In planning the
procedure, the chest CT was evaluated to determine the extent
and cause of the occlusion, and thrombotic substrate was
searched for. In addition, cavography was performed immediately
before stent implantation for an exact assessment of the venous
system.
Under sterile conditions, after local anaesthesia with Mecain 2%, the Seldinger technique was used to puncture the right common femoral vein just below the inguinal ligament. A 10-French sheath (Terumo, Tokyo, Japan) was then inserted, followed by wire probing (Terumo Stiff guide wire 0.035 inch) of the SVC and insertion of a 4-French pigtail catheter. To prepare serial angiograms in different planes, an automated contrast medium application system (10 - 15 ml/s, total of 20 - 25 ml per series) was used for the cavography. Examinations were conducted on a digital flat detector angiography system (AlluraXper FD 20, Philips Healthcare, Best, the Netherlands) by means of pulsed fluoroscopy (image frequency 15/s).
After
cavography (Fig. 1), the stenosis was classified according to
the Stanford classification7 system into 4 types: (i)
type I describes a partial obstruction of the SVC (up to 90%)
with remaining patency and antegrade perfusion of the azygos
vein; (ii) type II shows increasing
obstruction (90 - 100%); (iii) type III is complete
obstruction with reverse circulation in the azygos vein; and (iv)
type IV is characterised by complete obstruction of the SVC
and the azygos vein, with the development of collateral
circulations via the chest wall and the internal mammary
veins.
Corresponding to
the stenosis, a self-expanding Nitinol stent was placed. Despite
the high radial expansion force of the stent, residual
tumour-related constrictions were subsequently dilated with a
balloon (Zelos, Optimed, Ettlingen, Germany) in all patients for
optimisation in the area of the stenosis. A non-compliant
balloon was used, which was chosen to be slightly smaller in
relation to the stent diameter and with a length of 40 mm.
A stent with a diameter of 20 mm was subsequently dilated with
the aid of a balloon with a diameter of 18 mm, without exceeding
the working pressure of 4 bar. Accordingly, a 20 mm balloon was
used for a 22 mm stent. The stent length and the diameter were
determined on the basis of the CT and cavography. The stent
length was chosen according to the stenosis. The stent diameter
was determined on the basis of the diameter of the SVC in the
normal calibre range, taking into account respiratory
variability (Fig. 2).
Before stent implantation, each patient
received an intravenous bolus of 5 000 IU heparin. Serial
angiograms in 2 planes (AP and 45° oblique projections) were
then prepared to check for adequate recanalisation of the SVC.
The treatment was considered to have been completed successfully
if the stent was in the correct position and showed a normal
contrast medium outflow in the cavogram, and the collaterals had
markedly receded (Fig. 3). After removal of the sheath from the
common femoral vein, the puncture site was manually compressed
until haemostasis was achieved, and a light compression bandage
was applied for at least 6 h. Bed rest was recommended for at
least 12 h. On the following day, a renewed chest CT was
conducted to check the post-interventional outcome.
The follow-up period included presentation in
the oncological outpatient department with a clinical
examination and radiological diagnostics (chest CT). The
follow-ups were after 3 months up to 24 months, and were carried
out in those patients who had survived the course. In the event
of renewed clinical deterioration, the algorithm was departed
from. Restenosis was defined as >50% lumen reduction. The
indication for re-intervention was discussed by an
interdisciplinary team only if clinical symptoms recurred.
The cavography performed before stent placement revealed a partial obstruction of the SVC in 4/22 (18.2%, type I) and in 11/22 (50%, type II) of the patients. A complete obstruction of the SVC (type III) was seen in 7/22 (31.8%) of the patients. No cases of complete obstruction of the SVC and the azygos vein (type IV) were detected. Additional cava thrombosis was not found. Stenosis lengths averaging 3.8 cm (2.5 - 5 cm) were measured. Stents with a length of 60 mm were used in all patients, with sufficient cover of the stenosis. A stent with a diameter of 20 mm was chosen for 2 patients. In 20 patients, stents of 22 mm diameter were used.
A self-expanding Nitinol stent was implanted in all cases. The technical success rate was 100%, with optimal cover of the stenosis. In all (22/22) cases, the stenosis was successfully bridged with a single stent. There were no stent-related complications such as stent migration. Complications relating to the procedure, especially in the area of the stenosis or the puncture site, were not observed. In the follow-up period of up to 2 years, no stent migration was found. An improvement in clinical symptoms was observed within 24 h after stent implantation in all cases. Of subjective importance for the patients was the improvement in dyspnoea, which meant that they could assume a lying position without difficulty, and oxygen substitution could be discontinued. Objective signs of improvement were the decline in facial and neck oedema and regression of the venous cervical and thoracic dilatation.
Patients with known tumour disease continued their intensive therapy (radio-chemotherapy). Patients with newly discovered tumour disease (3 SCLC and 1 non-Hodgkin lymphoma) were able to start oncological treatment shortly after histological clarification.
In the follow-up CT, tumour progression was
found in 7/22 patients (3/7 after 3 months, 2/7 after 6 months,
and 2/7 after 12 months), with evidence of restenosis caused by
tumour growth through the stent mesh (Fig. 4). This resulted in
a renewed SVCS. CT detected a restenosis <50% in 4/7 and a
stenosis >50% in 3/7 of the patients. For the primary patency
rate, a value of 86.4% was obtained. During the follow-up
period, 15/22 (68.2%) of the patients died, yielding a mean
survival of 6.4 months. Only one patient has so far survived a
period of 2 years after stent implantation, and continues to be
followed along with the remaining patients.
Rapid diagnostics and effective therapy are
necessary to correct tumour-related compression of the SVC
within the context of acute life-limiting symptoms.
In conventional projection radiography of the chest, the majority of patients with SVCS show pathologies that present mainly as a mediastinal broadening, and to a lesser extent also with accompanying pleural effusions.
MDCT is the method of choice; it clarifies the extent of venous obstruction, identifies the venous collateral system and enables an estimation of the cause of the SVCS. In practice, obstruction of the SVC is often diagnosed on routine contrast-enhanced chest CT via an antecubital vein in the left arm.8 To avoid lack of opacification or streak artefacts, Qanadli et al.9 recommend a simultaneous bilateral antecubital vein injection; Sheth et al.8 prefer a delay of 60 s, instead of 30 s. In the literature, typically 120 ml (up to 180 ml) of contrast medium was injected.8 , 9 Our experience with a unilateral injection of 100 ml contrast medium and a delay of 30 s has been good.
In our study, CT also served as a basis for further therapy planning within the context of an interdisciplinary therapeutic decision. MRI is another method that can be used to image the central venous system, supplying valuable information for therapy planning,10 but this was not conducted in our patient population.
Based on
the CT findings, conventional imaging of the veins was
performed within the context of the procedure for stent
implantation in our study. Cavography enables assessment of
the obstruction and visualisation of the collateral
circulations.7 Partial obstructions (types I
and II; up to 68%) and complete obstruction (type III; 32%) of
the SVC were detected most frequently in our study. Complete
obstructions including the azygos vein were not found. In
their patient population with 27 venographies performed,
Stanford et al.7 most often described type IV
obstructions (37%), followed by type II and III (26% each),
while type I (11%) occurred less frequently. Lanciego et al.11 showed a similar distribution
of the obstruction types (type I: 9%; type II: 40%; type III:
28%; type IV: 23%).
Various therapeutic options are available, with the aim of rapidly alleviating the acute symptoms and improving the quality of the remaining time available to the patient in the palliative situation. General and pharmacotherapeutic treatments (e.g. bed rest and raised upper body, diuretics, cortisone anticoagulation) can alleviate symptoms, but only show limited clinical success. Standard tumour treatment procedures are radiotherapy and chemotherapy, or a combination of the two, which create relief by reducing the tumour mass. An improvement in symptoms is achieved in 80% of patients with these treatment methods. In the case of NSCLC, a decline in symptoms of 46 - 63% is seen with radiotherapy, and of 59% with chemotherapy. In the case of SCLC, success rates of 62 - 80% with chemotherapy and 83% with combined radiochemotherapy have been achieved.3 However, these therapeutic options take 7 - 14 days before symptoms improve, and in some studies up to 4 weeks.. Aggressive radiotherapy (8Gy 3 times a week for 3 weeks) achieved a response of up to 90%, but this treatment also leads to an increase in radiation-related complications, such as tumour necrosis with fever attacks, the risk of bleeding and even perforation of the SVC. In addition, side-effects such as nausea and vomiting, skin irritations and oesophagitis have been observed.
In the light of morbidity, mortality and
limited life expectancy, surgical resection with vascular
reconstruction is performed in only the rarest of cases in this
patient population with acute symptoms. In contrast, surgical
interventions are effective in benign causes of upper venous
congestion and show relatively few complications. If, in the
case of a malignant cause of upper venous congestion, a mean
life expectancy of 6 months is assumed, which is analogous to
the 6.4 months observed in our patient population, the remaining
time should comprise alleviating the symptoms and maintaining
quality of life.
In the event of severe symptoms, endovascular stent implantation represents the method of choice for acute treatment and is characterised by its capability of providing rapid relief from the acute symptoms (within 24 h) in up to 90% of cases. The technical success rate is around 95 - 100%. In our patient population, an improvement in dyspnoea and facial swelling in particular, was observed within 24 h, with a technical success rate of 100%.
The transfemoral approach proved effective for placing the stent. The right common femoral vein is preferred, while other venous approaches such as the internal jugular vein or the peripheral veins of the upper arm are used in special cases only.6 Based on this experience, we also used a right-sided transfemoral approach, after previous skin disinfection and local anaesthesia, in all cases in our study. In none of the cases was it necessary to puncture a different vein region. When selecting the stent size, the stent length should exceed the measured obstruction cranially and caudally by 1 cm each way, while the stent diameter should be adapted to the SVC in its unobstructed state.6 Regarding efficacy, no significant difference is found in the literature between the 3 most commonly used stents (Gianturco Z-stent, Cook Medical Inc., Bloomington, USA; Palmaz stent, Johnson & Johnson, Warren, USA; Wallstent, Boston Scientific, Natrick, USA). In the past, the Gianturco Z-stent has been described as having an increased rate of stent migration and stent malpositioning. These stents are self-expanding and characterised by largely resistance-free stenosis passage and a wide range of lengths and widths. Compared with the standard metal stents, more recent self-expanding stents made of a nickel-titanium alloy (Nitinol) have a higher precision in stent placement within the stenosis, an only minimal stent shortening, lower thrombogenicity and a higher radial expansion force, while remaining highly flexible.12 , 13 In our study, a 10-F Nitinol stent system authorised for SVCS was used and is available in various widths (16 - 34 mm) and lengths (30 - 100 mm). At stenosis lengths of 2.5 - 5 cm, 6 cm stents were applied with a diameter of 2.0 and 2.2 cm. Overlapping stent implantations were not necessary in our study, as the available stent sizes enabled complete coverage of the obstruction with one stent in each case.
If both brachiocephalic veins are involved in the obstruction, the patients may benefit from a unilateral stent implantation. Unilateral treatment is sufficient; on the one hand, blood flow is also possible from the contralateral side through the stent mesh; on the other, blood circulation takes place via cervicothoracic collateral channels.6 Bilateral recanalisation does not improve the outcome. In the case of parallel positioning of the stents in the SVC, the stents may not expand fully, which may be accompanied by increased recurrence of SVCS.11 , 14
If a central venous catheter is in place, various options present. If chemotherapy has been concluded, removal of the catheter may be considered prior to stent placement. If it is still required, an attempt can be made to move the catheter tip temporarily into another position before implantation of the stent, e.g. into the cervical or brachial veins, and move it back afterwards. If this is not possible, the central venous catheter can be overstented. 6 Balloon dilatation may be necessary before stent implantation. Though desirable in cases of benign SVC obstruction, it is not always required in malignant stenoses, but may be necessary for total obstructions.6 After stent implantation, balloon dilatation is recommended to optimise an eccentric stent position and remove residual stenoses. If a thrombus is additionally present, it can be pushed back further by angioplasty in the case of incomplete stent expansion.6 So-called noncompliant balloons were exclusively used in our study; they are characterised by the fact that they only change their diameter minimally upon dilatational pressure and therefore minimise the risk of overexpansion. Complications of stent placement are seen in 3 - 7 % of patients.1 The early complications include pulmonary artery embolism, stent migrations, haematomas and bleeding, ranging up to the rare perforation or rupture of the SVC.15 No such complications were observed in our study.
Failures after stent implantation may be linked to tumour invasion into the SVC through the stent mesh and thrombus formation. Lanciego et al.11 described such re-occlusion as a result of tumour growth in 16/149 patients (~10%) and in only 2 cases as a result of a thrombus in their patient population. In our study, tumour-related restenoses were seen in about 30% of patients over a period up to 12 months, the high tumour burden and deterioration of the overall situation meaning that renewed intervention was no longer indicated. If a relevant stenosis is defined as a lumen constriction >50%, 3 restenoses were present in our patient population, thus yielding a primary patency rate of 86.4%. This value is slightly higher than that achieved by Da Ines et al.,6 using Wallstents, of about 81%.
In the case of re-obstruction, re-intervention should fundamentally be discussed.3 , 11 In such cases, the use of covered stents is conceivable, but possible thrombogenicity and potential risk of blocking afferent vessels must be borne in mind.6 At present, only individual case reports are available16 but they demonstrate that tumour growth through the stent mesh, or stent migration with vascular rupture, can be treated with a covered stent. Covered stents were not used in our study.
Within the context of treatment of SVCS,
clear recommendations are not available for anticoagulation
and platelet aggregation inhibition. While most
interventionalists routinely use a heparin bolus of 5 000 IU,6 opinion
is divided about follow-up treatment and its duration. For
example, the interdisciplinary S3 guideline of the German
Respiratory Society and the German Cancer Society says that
anticoagulation is generally not necessary. Therefore, after
stent implantation, a middle way must be found between the risk
of early re-occlusion and haemorrhagic complications. To avoid
thrombus formation, platelet aggregation inhibition with
acetylsalicylic acid and/or clopidogrel is to be recommended. If
a thrombus is present, anticoagulation with heparin is necessary
for the duration of tumour treatment.6 The duration of
anticoagulation is dependent on therapy-related factors, and
side-effects and should be discussed in conjunction with
attending oncologists on an individual basis.
Self-expanding Nitinol stents provide endovascular therapy for SVCS with a tool that can be placed precisely and that alleviates the patient’s acute, life-threatening symptoms quickly and effectively in the palliative setting. As a result of post-interventional clinical improvement, it is then possible to pass on the patient for further targeted oncological therapy.
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2. García Mónaco R, Bertoni H, Pallota G, et al. Use of self-expanding vascular endoprostheses in superior vena cava syndrome. Eur J Cardiothorac Surg 2003;24(2):208-211. [http://dx.doi.org/10.1016/S1010-7940(03)00293-8]
3. Rowell NP, Gleeson FV. Steroids, radiotherapy, chemotherapy and stents for superior vena caval obstruction in carcinoma of the bronchus: A systematic review. Clin Oncol (R Coll Radiol) 2002;14(5): 338-351.
4. Qanadli SD, El Hajjam M, Mignon F, et al. Subacute and chronic benign superior vena cava obstructions: Endovascular treatment with self-expanding metallic stents. Am J Roentgenol 1999;173(1):159-164. [http://dx.doi.org/10.2214/ajr.173.1.10397119]
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7. Stanford W, Jolles H, Ell S, et al. Superior vena cava obstruction: A venographic classification. Am J Roentgenol 1987;148(2): 259-262. [http://dx.doi.org/10.2214/ajr.148.2.259]
8. Sheth S, Ebert MD, Fishman EK. Superior vena cava obstruction evaluation with MDCT. Am J Roentgenol 2010;194(4): 336-346. [http://dx.doi.org/10.2214/AJR.09.2894]
9. Qanadli SA, El Hajjam M, Bruckert F, et al. Helical CT phlebography of the superior vena cava: Diagnosis and evaluation of venous obstruction. Am J Roentgenol 1999;172(5):1327-1333. [http://dx.doi.org/10.2214/ajr.172.5.10227511]
10. Thornton MJ, Ryan R, Varghese JC, et al. A three-dimensional gadolinium-enhanced MR venography technique for imaging central veins. Am J Roentgenol 1999;173(4):999-1003. [http://dx.doi.org/10.2214/ajr.173.4.10511166]
11. Lanciego C, Chacón JL, Julián A, et al. Stenting as first option for endovascular treatment of malignant superior vena cava syndrome. Am J Roentgenol 2001;177(3):585-593. [http://dx.doi.org/10.2214/ajr.177.3.1770585]
12. Thierry B, Merhi Y, Bilodeau L, et al. Nitinol versus stainless steel stents: Acute thrombogenicity study in an ex vivo porcine model. Biomaterials 2002;23(14):2997-3005.
13. Schmidt W, Wissgott C, Andresen R, et al. Performance characteristics of modern self-expanding nitinol stents indicated for SFA. Fortschr Röntgenstr 2011;183(9):818-825. [http://dx.doi.org/10.1055/s-0031-1273445]
14. Dinkel HP, Mettke B, Schmid F, et al. Endovascular treatment of malignant superior vena cava syndrome: Is bilateral Wallstent placement superior to unilateral placement? J Endovasc Ther 2003;10(4):788-797.
15. Smith SL, Manhire AR, Clark DM. Delayed spontaneous superior vena cava perforation associated with a SVC wallstent. Cardiovasc Intervent Radiol 2001;24(4):286-287.
16. Jean-Baptiste R, Williams DM, Gemmete JJ. Successful treatment of superior vena cava rupture with placement of a covered stent: A report of two cases. Cardiovasc Intervent Radiol 2011;4(3):667-671. [http://dx.doi.org/10.1007/s00270-011-0128-8]