Endovascular Embolization of a Ruptured Distal Lenticulostriate Artery Aneurysm in Patients with Moyamoya Disease
Article information
Abstract
A ruptured distal lenticulostriate artery (LSA) aneurysm is detected occasionally in moyamoya disease (MMD) patients presented with intracerebral hemorrhage. If the aneurysm is detected in hemorrhage site on angiographic evaluation, its obliteration could be considered, because it rebleeds frequently, and is associated with poorer outcome and mortality in MMD related hemorrhage. In this case report, the authors present two MMD cases with ruptured distal LSA aneurysm treated by endovascular embolization.
INTRODUCTION
A ruptured aneurysm on collateral vessels is detected occasionally in patients with moyamoya disease (MMD) who present with intracerebral hemorrhage. This aneurysm is usually located in the anterior or posterior choroidal artery, but some can be detected in the distal lenticulostriate artery (LSA). In MMD related hemorrhage, rebleeding is known to be more frequent than spontaneous one6), and associated with poorer outcome and mortality7,9). Therefore, obliteration of this aneurysm which is detected in the center of hematoma could be considered.
Herein, we describe technique and follow-up results of two MMD cases with ruptured distal LSA aneurysms treated by embolization using n-butyl-cyanoacrylate (NBCA) for prevention of its rebleeding.
CASE REPORT
Case 1
A 53-year-old woman presented with sudden stuporous mentality. Brain CT scan showed a hemorrhage in the left basal ganglia, which was extended into the lateral ventricle. She was diagnosed with MMD 2 years ago on MRI performed for evaluation of chronic headache. Based on her past history and CT findings, diagnostic angiography was performed to detect any bleeders, and revealed a ruptured aneurysm in the left medial LSA, supplying the frontal cortex via medullary vessels (Fig. 1A). The aneurysm was located in a branch of this LSA, which was another medullary vessel connected with the insular branch of the M2 segment (Fig. 1B).
Because the patient was uncooperative, the procedure was performed under general anesthesia. Echelon-14 microcatheter (EV3, Irvine, CA, USA) was positioned directly at the target branch with the aneurysm using Synchro-14 wire (Stryker, Fremont, CA, USA) in order to save medullary vessels from this LSA. Selective angiogram showed that delayed filling defect in the M2 branch, which was connected with the LSA. This finding confirmed another collaterals to this lesion (Fig. 1B). The target branch was perfectly wedged by the microcatheter. To prevent a retrograde filling of the aneurysm from the M2 branch, the target branch of the LSA was embolized with a 33% NBCA mixture with lipiodol up to the point connecting with the insular branch of the M2 (Fig. 1C). Postembolization angiogram showed no aneurysmal filling. Patent distal vessels of the LSA and M2 branches were also confirmed (Fig. 1D).
Follow-up CT scan showed the aneurysm and target branch filled with NBCA (Fig. 1E). No infarction in the adjacent structure and cortex area was detected on diffusion weighted imaging (DWI). The patient fully recovered and no rebleeding occurred for 1 year after embolization. Aneurysm recurrence was not detected on 1-year follow-up angiography.
Case 2
A 44-year-old woman presented with stuporous mental status. Brain CT scan revealed intraventricular hemorrhage extended from a focal hemorrhage in the left caudate nucleus. The patient had a history of intracerebral hemorrhage in the right temporal lobe 8 years ago and had been diagnosed with MMD. Diagnostic angiography showed a ruptured aneurysm on medullary vessel from the LSA connected with cortical branches supplying frontal area. Additional aneurysmal dilatation was noted in these cortical branches, but its location was not in the hemorrhage site (Fig. 2A).
Under general anesthesia, Echelon-14 microcatheter was navigated into the target LSA using Synchro-14 wire. To avoid a reflux of NBCA into M1 and another vessels, the microcatheter was inserted up to proximal segment of the target LSA over its origin. Selective angiogram showed the aneurysm and cortical branches via medullary vessels (Fig. 2B). These cortical branches were found to disappear after brief opacification on selective angiogram, suggesting collateral vessels from other LSA. Occlusion of the target LSA with wedging microcatheter into the LSA induce no perfusion defect and branch loss on repeated angiograms. A 25% NBCA mixture with lipiodol was slowly injected via the microcatheter up to the aneurysm (Fig. 2C). Postembolization angiogram revealed complete obliteration of the aneurysm and patent cortical braches (Fig. 2D). No retrograde filling of the aneurysm was noted on venous phase of angiogram.
CT scan taken 3 days after embolization showed the aneurysm and LSA filled with NBCA (Fig. 2E). No infarction was detected on DWI. The patient also fully recovered without neurologic deficit. One-year follow-up angiography did not reveal the aneurysmal recurrence. No rebleeding developed during 2 years after embolization.
DISCUSSION
In MMD, LSAs serve as important transmedullary collateral vessels supplying cortex areas as well as original vascular territories, instead occluded major arteries. Fragile nature of these collateral vessels and hemodynamic stress have been considered as a cause of hemorrhage in MMD. Although aneurysmal lesion on collateral vessels is not frequently encountered in MMD patients with hemorrhage, if it is detected on angiography and well correlated with bleeding site, endovascular treatment for aneurysmal lesion could be considered as an option for prevention of rebleeding3,4).
In our experience of ruptured aneurysms in choroidal arteries in MMD patients, these arteries are usually straight, because of their subependymal location covered by ependymal layer along with ventricular wall4). Therefore, microcatheter can be easily advanced near the aneurysm. However, because LSAs have originally tortuous course and relatively small diameter, an access to the distal LSA aneurysm with microcatheter can be limited. In this situation, occlusion of long segment of the LSA can make large infarction beginning from its proximal territory and additional infarctions in cortex area supplied by its distal medullary vessels2). The easy way to avoid infarction and consequent aggravation of neurological status is the selective embolization for the target branch with the aneurysm limited within hemorrhage site and saving other collateral vessel. Although, we were able to perform the selective embolization in Case 1, it is not always possible.
When embolization of long segment of the LSA is inevitable, pre-embolization provoking test such as amobarbital test can be used3). However, in uncooperative MMD patients with hemorrhage, because this type of test was unavailable, we used careful inspection of repeated angiogram findings after wedging microcatheter into the target LSA as a simulation test, in Case 2. Although some collateral flows were confirmed, fine and complex collateral networks all of which could not be traced were found to make reverse flows, leading to no perfusion defect and branch loss on the repeated angiograms. Other reports described no detailed angiographic information on collateral flows, but reported no infarction and its related sequelae, as our cases1,5). Consequently, these cases suggest that collateral networks which develop extensively in MMD would be critical determinant for successful outcomes and a background for endovascular embolization of ruptured distal LSA aneurysm in MMD patients.
Although these collateral networks prevent infarction, they could make a retrograde filling into the aneurysm and even rebleeding, unless obliteration of the aneurysm itself is achieved. However, the LSA was usually wedged without antergrade flow after placing the microcatheter in our practice. This permitted fine control of NBCA without its reflux. Therefore, after adequate injection volume, pressure, and speed were confirmed by several test injection with contrast, we were able to penetrate NBCA up to the aneurysm or target point, avoiding occlusion of collateral vessels beyond the target. Compared with Onyx (EV3, Irvine, CA, USA), NBCA has a tendency to go straight to a target. In our cases, therefore, because embolic material had to be injected at a point far from the target lesion, we selected NBCA as adequate embolic material.
Although more long-term follow-up is necessary, aneurysm recurrence and rebleeding were not detected in our and other reports3,5,8). This may indicate that endovascular embolization is effective for prevention of rebleeding from the distal LSA aneurysm in MMD, if successful. However, because of limited cases, more investigation is necessary for proving the benefit of endovascular embolization.
CONCLUSION
A ruptured distal LSA aneurysm is not frequent in patients with MMD who present hemorrhage. However, if it is detected on angiographic evaluation and can be accessed, endovascular embolization could be considered for prevention of rebleeding. Special consideration of collateral network is mandatory.
Acknowledgements
This study was supported by grants of the Korea Healthcare Technology R&D Project, Ministry of Health and Welfare, Republic of Korea (HI10C2020), the Seoul National University Bundang Hospital research fund (02-2013-122), and a contribution from Jinyoung TBX Co., LTD (06-2013-080).