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Advances in Interventional Cardiology/Postępy w Kardiologii Interwencyjnej
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1/2014
vol. 10
 
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Cardiovascular imaging
Noninvasive assessment of cerebral artery stenoses from anatomic computed tomography angiography

Xiaolong Qi
,
Fangyu Zhou
,
Jun Wan
,
Lin Zhou
,
Wei Xu
,
Juan Cheng
,
Yu Mao
,
Wanrong Ma
,
Wenbin Ji
,
Changqing Yang

Postep Kardiol Inter 2014; 10, 1 (35): 18–20
Online publish date: 2014/03/23
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Introduction



Trans-stenotic pressure gradient (TSPG) and fractional flow reserve (FFR) are two well-validated functional indices to assess the ischemic severity of arterial stenoses [1–3]. They have been demonstrated as a promising tool to identify patients who would likely benefit from revascularization [4–6]. However, TSPG and FFR measurement has significant restrictions in clinical practice due to its invasiveness and high cost.

A novel noninvasive assessment of FFR from anatomic computed tomography (CT) angiography has been well validated in evaluating functional coronary stenoses [1–3].

The study aims to transplant the functional diagnosis, for the first time, to cerebral artery stenoses and develop a noninvasive assessment of cerebral TSPG (TSPGni) and FFR (FFRni).



Case report



A 65-year-old woman who had symptoms of cerebral ischemia was recruited and gave written informed consent. Approval was obtained from the ethical committees of Tongji Hospital, Tongji University. Transcranial Doppler ultrasound and CT angiography were performed according to a recognized protocol by two technicians who had at least 5 years’ vascular examination experience.

For the TSPGni and FFRni interpretation, all CT images were imported into Medical Imaging Control Software MIMICS10.0 where the posterior cerebral artery (PCA) was reconstructed. Three dimensional virtual arteries were then exported from MIMICS10.0 as a virtual reality modeling file to the developed workflow. The inlets and outlets were defined according to the position from which the physiological data were recorded. The closed surface was “meshed” into approximately 1.2 million internal tetrahedra, in preparation for the computational fluid dynamics analysis. Measured flow data and universal central venous pressure were imported, processed, and applied to the inlet and outlet as boundary conditions, and a definition file was created that fully specified the model for the computational fluid dynamics solver ANSYS13.0. This solved the unsteady momentum Navier-Stokes and continuity equations with finite element analysis. TSPGni and FFRni were then calculated. An optimization process was used to determine the microvascular resistance for the patient and we averaged the resistance to produce a generic value applicable to the whole cohort. This approach demonstrated the most effectively predictive capability of the model with minimal personalized data.

Two-dimensional models of the PCA in transverse planes were reconstructed (Figure 1 A). 3D geometric models of the PCA were separated (Figure 1 B). Finite element computational fluid dynamics of ANSYS11.0 was applied to mesh the models. Thereafter, a well-defined mathematical model was obtained (Figure 1 C).

Cerebral TSPGni and FFRni were successfully computed. The peak systolic velocity (PSV) of the PCA was 117 cm/s (left) and 92 cm/s (right). Computed tomography angiography images suggested that the level of stenoses in the PCA was 60% (left) and 15% (right). According to novel assessment, TSPGni and FFRni of the right side of the PCA were 31.6 mm Hg and 0.43. For the left side, they were 59.2 mm Hg and 0.22 (Figure 2 A). The velocity distribution in the coronal plane indicated that the velocity remained equal at the proximal and distal stenoses. However, it increased significantly from 1.5 m/s to 5.0 m/s at the site of stenoses (Figure 2 B). In addition, it showed that the rate of blood flow increased obviously and central speed shifted to the narrow (Figure 2 C).



Discussion



Digital subtraction angiography is still treated as a “gold standard” to evaluate “significant” cerebral artery stenoses. However, drawbacks, such as invasiveness and lack of lesion-specific functional diagnosis, greatly limit its clinical worth [7–9]. A large number of clinical trials have proved the great value of TSPG and FFR, which are well-defined functional indices to evaluate the ischemic significance of artery stenoses [4–6]. Recently, the results of a series of international multicenter clinical trials suggested the highly diagnostic performance of a novel noninvasive FFR assessment from anatomic CT angiography (FFRCT) [1–3]. In the study concerning 159 vessels in 103 patients, the diagnostic accuracy, sensitivity and specificity of FFRCT were 84.3%, 87.9% and 82.2%, respectively. Area under the receiver-operator characteristics curve (AUC) was 0.90 [2]. From the results of another study carried out in 252 stable patients from 17 centers in 5 countries, the diagnostic accuracy, sensitivity and specificity of FFRCT plus CT were 73%, 90% and 54%. FFRCT was associated with improved discrimination (AUC: 0.81; 95% CI: 0.75–0.86; p < 0.001) [1].

Our previous studies have successfully demonstrated a novel method computed from CT angiography to functionally evaluate the severity of vascular disease [3]. The study aims at investigating, for the first time, a noninvasive approach to evaluate functional cerebral artery stenoses by TSPGni and FFRni. The results for the left side of the PCA were 65% stenoses, PSV = 117 cm/s, TSPGni = 59.2 mm Hg, FFRni = 0.22, which suggested functional and anatomic moderate stenoses. For the right side, they were 15% stenoses, PSV = 92 cm/s, TSPGni = 31.6 mm Hg and FFRni = 0.43, respectively. From the results, the diagnostic performance of cerebral TSPGni and FFRni was generally consistent with the diagnosis of transcranial Doppler ultrasound and CT angiography.



Conclusions



This is the first study to introduce a novel noninvasive assessment of cerebral TSPGni and FFRni to evaluate “significant” cerebral artery stenoses and their hemodynamics. It is therefore believed that the novel method might be potentially useful in evaluating the functional severity of cerebral ischemia and making clinical decisions of revascularization. Although the diagnostic performance is limited due to the small sample and lack of in vivo values of TSPG and FFR, the results are encouraging and the model will now be optimized with greater patient numbers and invasive values analysis.



Acknowledgments



Xiaolong Qi and Tangyu Zhou – equal contributor.



References



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