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Ultrasound Int Open 2015; 01(02): E53-E57
DOI: 10.1055/s-0035-1565130
Original Article
© Georg Thieme Verlag KG Stuttgart · New York

The Posterior Cerebral Artery and its Main Cortical Branches Identified with Noninvasive Transcranial Color-Coded Duplex Sonography

P. E. Frid
1   Department of Neurology, Institute for Clinical Sciences, Malmö, Sweden
,
S. J. Schreiber
2   Neurology, Charité Berlin, Berlin, Germany
,
O. Pade
3   Department of Neurology and Neurophysiology, AMEOS Klinikum Neustadt, Neustadt i. H., Germany
,
F. Doepp
4   Department of Neurology, Charité Campus Virchow, Berlin, Germany
,
J. Valdueza
5   Neurologie, Neurologisches Zentrum der Segeberger Kliniken, Bad Segeberg, Germany
› Author Affiliations
Further Information

Correspondence

Dr. Petrea E Frid, MD
Department of Neurology
Institute for Clinical Sciences
Skåne University Hospital
Malmö
Sweden S-20502   
Phone: +46/731/500 943   
Fax: +46/403/33 055   

Publication History

received 24 June 2015

accepted 12 October 2015

Publication Date:
06 November 2015 (online)

Also available ateRefMedOne
 
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Abstract

Purpose: To differentiate PCA segments and cortical branches by means of transcranial color-coded duplex sonography (TCCD) and to measure flow parameters at rest and during visual stimulation.

Materials and Methods: 60 healthy subjects with a good acoustic temporal bone window were examined. The main stem of the PCA (P1, P2 and P3) and 4 main cortical branches – the anterior temporal artery (ATA), the occipital temporal artery (OTA), the parietooccipital artery (POA) and the calcarine artery (CA) – were assessed using an axial transtemporal approach. Systolic and diastolic blood flow velocities (BFVs) were recorded at rest and during visual stimulation.

Results: Identification of the P1 segment of the PCA was successful in 97.5% (117/120) of cases. The P2 and P3 segments were visualized in all cases. The 4 main cortical branches could be identified to varying degrees: ATA in 88%, OTA in 96%, POA in 69% and CA in 62%. There was an evoked flow response in the P2 main stem and in all cortical branches. The most pronounced increase in diastolic/systolic BFV after visual stimulation test was seen in the CA (42%/35%), followed by P2 (30%/24%), the POA (27%/27%), the OTA (16%/13%) and the ATA (9%/8%).

Conclusion: Insonation through the temporal bone window with TCCD confidently allows the assessment of the P1 to P3 segments of the PCA as well as the 2 proximal branches, the ATA and the OTA. An ultrasound-based classification of PCA anatomy and its cortical branches may be used as a noninvasive method for the evaluation of posterior circulation pathology.


 

Key words

brain - blood vessels - ultrasound

Introduction

Infarctions in the territory of the posterior cerebral artery (PCA) are reported in 5–10% of ischemic strokes [1]. Main causes are thought to be embolic occlusions, but intrinsic vessel stenosis and occlusions may occur [2]. Despite the clinical relevance, less attention has been paid to the specific vessel anatomy of the PCA. For clinical use the PCA can be divided into 4 segments from P1 to P4 [3]. P1 represents its shortest and most proximal segment, with a mean length of less than 10 mm, [4] [5] [6] running from its origin at the top of the BA to its side-to-end anastomosis with the posterior communicating artery (PCoA). P2 begins at the junction with PCoA and has the longest course. It can be further subdivided into an anterior (proximal) and posterior (distal) part, each about 25 mm in length [5]. P3 begins at the posterior margin of the midbrain and runs slightly upward and medially within the quadrigeminal cistern. It reaches the medial surface of the occipital lobe, often ending at the anterior limit of the calcarine fissure. At this point P3 usually divides into 2 major branches defining P4; the calcarine artery (CA) and the parietooccipital artery (POA). This distal bifurcation can be found at varying depths ranging from 6 to 67 mm ([Fig. 1] [2] [3]).

Zoom
Fig. 1 Schematic drawing of PCA segments (adapted from Huber) in the axial view (top) and the sagittal view (bottom): Brown=P1 segment, dark green=P2 segment, yellow=P3 segment, 1=anterior temporal artery, 2=occipitotemporal artery, 3=parietooccipital artery, 4=calcarine artery.
Zoom
Fig. 2 TCCD, color mode images, axial planes. a pontomesencephalic plane, b mesencephalic plane, c thalamic plane. Red indicates flow toward the probe, blue indicates flow away from the probe. Midbrain encircled in white. The third ventricle is outlined by white dashed lines. 1=proximal P2 segment, 2=anterior temporal artery, 3=distal P2 segment, 4=occipitotemporal artery, 5=P3 segment, 6=calcarine artery, 7=straight sinus, 8=parietooccipital artery.
Zoom
Fig. 3 TCCD, right: color mode image, axial mesencephalic plane, midbrain encircled in white. Calcarine artery detected at a depth of 83 mm. Left: Doppler spectra of the calcarine artery at rest (top) and during visual stimulation (bottom). Note the systolic and diastolic flow velocity increase of 35% and 40%, respectively.

The branching pattern of the cortical arteries of the PCA has been mapped by several groups. The number of proper arterial branches mentioned in the literature varies depending on the method of investigation and the study material [5] [7]. Zeal and Rhoton anatomically identified 7 main arterial branches that occur with varying consistency [5]. The most constantly developed arteries are the anterior temporal artery (ATA) arising from the anterior (64%) or posterior (20%) part of P2, and the occipitotemporal artery (OTA) (synonym: posterior temporal artery) most frequently arising from the distal segment of P2. The OTA is a firm branch coursing in a posterolateral direction, supplying the inferior temporal and occipital surfaces and the lingual gyrus. The POA occurs as a single terminal branch, in about half of the cases arising from P3 as part of a terminal bifurcation with the CA. In 40% of cases it branches off the distal P2 and in 10% even from the proximal P2 [5]. From its medial origin the POA rises upward and laterally to the parietooccipital fissure and during its course often crosses the proximal calcarine fissure. The CA is the second terminal PCA branch. In about half of cases it arises from P3 but may depart from the distal P2 in 42% of cases. In 10% it may also branch off the POA [5]. Its irrigation area includes, but is not limited to, the visual cortex.

MRA and CTA techniques also allow good visualization of the major PCA branches, but no detailed assessment has been reported up to now [8] [9], and to our knowledge, no previous studies on flow rates measured with TCCD have been previously published. Early sonographic PCA assessments using transcranial Doppler (TCD) divided the PCA into a P1 and P2 segment, based on the detected flow direction. A flow direction towards the transducer was defined as the P1 segment, and a flow away from the transducer as the P2 segment [10]. However, this nomenclature does not correspond to real anatomy. TCCD allows a more precise anatomical correlation and PCA assessment in relation to its junction with the PCoA. Using TCCD, the proximal P2 shows – identical to P1 – a flow direction towards the transducer and the distal P2 and P3 and P4 show a flow away from the transducer [11]. Based on anatomical data, we analyzed the main PCA segments as well as the PCA branches ATA, OTA, POA and CA, the latter of which have not yet been described and classified with TCCD. In addition, blood flow in the P2 segment as well as in the 4 cortical branches was analyzed during a visual stimulation test to prove the hypothesis that the magnitude of responses relate to each vessel’s participation in feeding the striatal and peristriatal visual cortex.


 

Materials and Methods

Healthy subjects with a sufficient acoustic temporal bone window, i. e., the M1 segment of the middle cerebral artery (MCA) and the P1 and P2 segment of the PCA were easily visualized on both sides, were recruited at the neurological center of the Segeberger Kliniken in Germany. Subjects with an insufficient acoustic temporal bone window were excluded. Informed written consent was obtained from all subjects. The study was approved by the local ethics committee. Subjects were investigated in the supine position without a contrast enhancer. TCCD was performed using a Power Vision 6000 SSA-370 A ultrasound system (Toshiba, Tokyo, Japan) with a 2.5-MHz phased-array transducer.

All vessels were examined using an axial insonation plane through the temporal bone window, which is most easily achieved by placing the probe directly preauricularly and superior to the zygomatic arch. In the mesencephalic plane, the P1 and the proximal P2 were visualized red-colored with a flow towards the transducer. The junction between P1 and P2 was defined by the concomitant visualization of the distal ICA if no PCoA was visible. The origin of the ATA was defined as a red-colored vessel at the junction between the proximal and distal P2 with a flow towards the probe. The origin of the OTA was defined as a comma-shaped, red-colored vessel at the distal P2. Reflecting the slightly upward vessel course, the distal P2 was defined by its blue-colored visualization with a flow away from the probe mainly in a midbrain–thalamic insonation plane. P3 was defined as the main course of the PCA within the quadrigeminal cistern. A bifurcation in the quadrigeminal cistern or more distal in the thalamic plane was defined as the origin of the POA and CA, both vessels representing P4. A vessel course upward and lateral into the parietooccipital fissure (between the thalamic and the cella media plane) was allocated to the POA. A midbrain-plane vessel course near to the interhemispheric space was allocated to the CA. In cases of doubt regarding the differentiation between the POA and CA, the vessel with the stronger response to the visual stimulation test was defined as the CA.

The systolic and diastolic blood flow velocity (BFV) in the PCA main stem and the cortical branches was measured at rest and during a visual stimulation test. Since the depicted vessels were curved or their length was usually short (<1 cm), all flow velocity measurements were performed without angle correction. Subjects were examined on both sides. Baseline systolic and diastolic BFVs were measured with the subject’s eyes closed. Visual activation was achieved by eye opening and looking at a checker-chart on the ceiling for 20 s. BFVs were measured at the end of the 20 s and the increase of flow was calculated as the percent increase above baseline levels for all studied vessels. Statistical analysis of the difference in average BFV increase between branches was performed using the Kruskal-Wallis test (non-parametric ANOVA) and multiple comparisons between the 5 groups were performed using Dunn’s post-test.


 

Results

60 healthy subjects, aged 18–62 years (39±10.9), were included in the study. P1 was successfully identified in 97.5% (117/120) of the cases. P2 and P3 were visualized in all cases. BFVs were almost identical with slightly higher values in P2 and P3 compared with P1 ([Table 1]).

Table 1 PCA main stem detection rates and flow velocities.

Detection rate (%)

V diast (cm/s)

V syst (cm/s)

P1

97.5

28.1±8.5 (11–52)

59.8±14.3 (27–103)

P2

100

27±6 (16–43)

58±11 (39–104)

P3

100

29.9±7.9 (18–58)

62.6±12.0 (30–94)

Mean±standard deviation, range ( ), flow velocities without angle correction

Following the defined criteria, the 4 main cortical PCA branches were identified to varying degrees: ATA in 88% of cases, OTA in 96% of cases, POA and CA in 69% and 62% of cases, respectively. The highest BFVs were measured in the POA, followed by the CA and the OTA with similar values. The ATA showed the lowest BFVs ([Table 2]).

Table 2 PCA cortical branches: detection rates, flow velocities and response to checker-chart visual stimulation.

Detection rate (%)

V diast at rest (cm/s)

V diast stimulation (cm/s)

Change V diast (%)

V syst at rest (cm/s)

V syst stimulation (cm/s)

Change Vsyst (%)

ATA

88

12±4 (5–2)

13±5 (7–30)

8.5

26±9 (12–56)

28±11 (13–63)

8.2

OTA

96

16±5 (8–27)

19±6 (9–35)

16

34±9 (18–57)

38±12 (19–70)

12.6

POA

69

21±8 (9–62)

26±10 (10–71)

27.4

40±14 (19–100)

51±18 (23–124)

27.1

CA

62

16±6 (5–31)

22±8 (7–47)

41.6

33±10 (14–62)

43±13 (19–83)

34.7

P2

100

27±6 (16–43)

34±8 (20–52)

29.5

58±11 (39–104)

72±13 (48–117)

23.9

Mean±standard deviation, range ( ), flow velocities without angle correction

Visual stimulation led to a BFV increase in P2 and all 4 cortical PCA branches. The most pronounced increase in diastolic/systolic BFV was found in the CA (42%/35%), followed by P2 (30%/24%), the POA (27%/27%), the OTA (16%/13%) and the ATA (9%/8%) ([Table 2]). Non-parametric ANOVA yielded a significant difference for diastolic and systolic flow increases (KW=123.06 and 106.53, p<0.0001). Multiple comparisons (systolic and diastolic BFV rise) showed a significant difference between groups (p<0.01) except for the comparison of PCA vs. POA and ATA vs. OTA.


 

Discussion

This study shows that the main segments of the PCA as well as the most relevant cortical branches can be identified by TCCD and differentiated according to real anatomical conditions. In addition, a separate analysis of flow responses to visual stimulation in selected cortical branches of the PCA has not been published previously.

In our study, the segments P1 to P3 were visualized in nearly all of our cases. Similar high detection rates of 72–100% have been reported for P1 and P2 [12] [13] [14] [15]. Data for the cortical branches, however, were missing. The 2 proximal branches, the ATA and OTA, can be reliably identified with non-contrast-enhanced TCCD. The detection rates of 82% (ATA) and 96% (OTA) correspond with the anatomical data of Zeal who reported rates of 84% and 96%, respectively [5]. In contrast, the detection rates differ markedly in regard to the POA and CA with detection rates in our study of 69% and 62% but an anatomical presence in 96% and 100%, respectively [5]. The main reason for this may be the restriction of insonation quality through the temporal bone for the visualization of more dorsally located vessels.

Regarding flow rate response to visual stimulation, our reported BFVs in P1 and P2 correspond to the data from the literature [12] [13] [14]. The highest cortical branch BFVs with closed eyes were found in the POA, followed by the OTA, CA and ATA. The vessel diameter is correlated to the significance of the artery and absolute BFV values correspond to the amount of perfused brain parenchyma by the selected artery. The perfusion area of the POA includes large parietal and occipital areas and that of the OTA temporal and occipital areas whereas the ATA is more restricted to anterior parts of the temporal lobe and the hippocampus. The wide inter-individual range in BFV in selected branches indicates the high variability in the perfusion area. This has been shown in anatomical studies for the OTA and CA [16]. Our findings are in good accordance with the anatomical literature. Diameter measurements of the POA, OTA, CA and ATA were reported to be 1.6 mm, 1.6 mm, 1.4 mm and 1.3 mm, respectively [5]. Similar data of 1.5 mm, 1.6 mm, 1.3 mm and 1.2 mm were reported recently.

Like functional magnetic resonance imaging (fMRI) and positron emission tomography (PET), ultrasound allows the assessment of changes in local neuronal activity by measuring changes in blood flow velocities in a selected vessel segment, which corresponds to changes in regional blood flow (rCBF). In contrast to MRI and PET, ultrasound methods have a high temporal resolution allowing instant assessment of regional CBF changes. The major disadvantage of functional ultrasound, however, is the limited spatial resolution. Despite this, a large number of studies using TCD focusing on sensory, motor and cognitive functions, especially concerning language lateralization in man have been published in recent years [17] [18]. An evoked flow response of PCA main stem flow to visual stimuli has been demonstrated using TCD shortly after its introduction in clinical medicine with a mean BFV increase of about 20% in healthy subjects [19] [20] [21] [22]. PCA visual evoked flow has been used to separate PCA signals from vessels of the anterior circulation and from the superior cerebellar artery (SCA) [23] and to distinguish patients in a vegetative state [24].

However, data on flow responses in select cortical branches has not previously been reported. Our results show that the major evoked increase in diastolic BFVs after visual stimulation was as expected in the CA with 41.6% followed by the POA and OTA with 27.4% and 16.2%, respectively. The weakest effect was observed in the ATA with an increase of 8.5% only. The obvious response in the POA and less in the OTA may be explained by their contribution to the perfusion of the striatal and peristriatal cortex in 20–35% and 3–22.5% of cases, respectively. The P2 segment showed an increase of diastolic BVF of 29.5%, which corresponds to discussed data from the literature. [25] [26]

Our observations may be doubly useful. First, the new TCCD vessel nomenclature allows a more exact anatomical description of PCA vessel anatomy and pathology. Instead of mere detection of main stem PCA pathology [27] [28], the newly described PCA segments may facilitate the recognition of vessel stenoses in more distal parts and in selected branches. It may also facilitate a more precise definition of main stem occlusions and a more elaborate description of collateral leptomeningeal PCA flow in MCA occlusion [25] [26].

Second, the ability to examine select cortical branches may open new possibilities in functional Doppler of the visual system. One major obstacle of TCCD is that it allows only hand-held examination of the vessels, limiting the measurement of BFV changes during the visual task. Here, either newly developed TCCD probe holders, or information transfer (depth, probe position, wave form, BFV, and flow direction) from TCCD to TCD, might be a solution.

Limitations of our study have to be mentioned. One is the subjects’ relatively young age. A lower frequency of successful visualization in older subjects is expected due to a diminished temporal acoustic window. The use of echo-contrast agents can ameliorate the sensitivity of TCCD markedly [29]. However, the use of a contrast agent may require that different reference values are used [30]. Also, variations of PCA cortical branches have to be considered, e. g., a common temporal branch which bifurcates or trifurcates into several smaller branches, a middle temporal artery between the ATA and OTA, or a small hippocampal artery present as the first cortical branch of the PCA [5], leading to confusion with the ATA. Also a prominent posterior choroid or posterior pericallosal artery may arise from the P2 and P3 segments [23]. Finally, the main stem of the PCA may be confused with the SCA, which runs parallel and close together with the PCA at their origins from the basilar artery [23].


 

Conclusion

Non-contrast-enhanced TCCD insonation through the temporal bone window allows visualization not only of the PCA main stem from the P1 to the P3 segments but also the cortical PCA branches, with the proximal ATA and OTA more readily visualized than the peripherally located POA and CA. The above nomenclature allows more accurate assessment of vascular disease location. Evoked flow velocity responses to a visual stimulus can be analyzed in PCA branches. Different reaction patterns can be used to distinguish branches, e. g., the POA from the CA, and open the door for new functional testing in cognitive and visual disorders.


 

 

Correspondence

Dr. Petrea E Frid, MD
Department of Neurology
Institute for Clinical Sciences
Skåne University Hospital
Malmö
Sweden S-20502   
Phone: +46/731/500 943   
Fax: +46/403/33 055   


  Permissions and Reprints
Zoom
Fig. 1 Schematic drawing of PCA segments (adapted from Huber) in the axial view (top) and the sagittal view (bottom): Brown=P1 segment, dark green=P2 segment, yellow=P3 segment, 1=anterior temporal artery, 2=occipitotemporal artery, 3=parietooccipital artery, 4=calcarine artery.
Zoom
Fig. 2 TCCD, color mode images, axial planes. a pontomesencephalic plane, b mesencephalic plane, c thalamic plane. Red indicates flow toward the probe, blue indicates flow away from the probe. Midbrain encircled in white. The third ventricle is outlined by white dashed lines. 1=proximal P2 segment, 2=anterior temporal artery, 3=distal P2 segment, 4=occipitotemporal artery, 5=P3 segment, 6=calcarine artery, 7=straight sinus, 8=parietooccipital artery.
Zoom
Fig. 3 TCCD, right: color mode image, axial mesencephalic plane, midbrain encircled in white. Calcarine artery detected at a depth of 83 mm. Left: Doppler spectra of the calcarine artery at rest (top) and during visual stimulation (bottom). Note the systolic and diastolic flow velocity increase of 35% and 40%, respectively.