Principles of Doppler ultrasound - Wake Forest Baptist · PDF filePrinciples of Doppler ultrasound
Post on 18-Mar-2018
225 Views
Preview:
Transcript
1
Anatomy, Principles, and Techniques for Transcranial Doppler
J Kim MD
Jongyeol Kim, MD, RPVI, RVT
Associate Professor, Neurology
Texas Tech University Health Sciences
School of Medicine
J Kim MD
J Kim MD
Principles of Doppler ultrasound
Fd = 2·fo·v·cosθ/c, where fo = source frequency, v = scatter speed, c = propagation speed
V(cm) = 77·fd(kHz)/fo(MHz) ·cosθD
J Kim MD
Principles of Doppler ultrasound
V(cm) = 77·fd(kHz)/V(cm) = 77·fd(kHz)/fofo(MHz) ·(MHz) ·coscosθθDD
J Kim MD
θθ
F
r
F
t
Peak SystolicPeak Systolic End DiastolicEnd Diastolic
Range gateSample Volume
J Kim MD
2
Influence of insonation angle
J Kim MD
SampleVolume
Angle = 0
Angle = 30
SampleVolume
Influence of insonation angle
J Kim MD
Angle = 60
SampleVolume
Angle = 90
SampleVolume
Vascular Doppler
Spectral Analysis Parameters
Flow direction
J Kim MD
Peak systolic velocity End-diastolic velocity Spectral pattern
J Kim MD
7165 articles in March 2011 on PubMed 7687 articles as of October 2011 on PubMed
Acoustic properties of the skull
Three layers Middle layer (dipole): important on the attenuation
and scattering of the sound Outer and inner tables: refraction
J Kim MD
Temporal region: absence of bony spicules
Power loss depends on the thickness of the skull
Acoustic WindowsTrans
Temporal Frontal
J Kim MD
AWMWPWTrans
Orbital
Trans Foraminal
3
Circle of Willis
J Kim MD
AW
MW
PW
J Kim MD
J Kim MD
Insonation Depth
Range gate
J Kim MD
Insonation Depth
J Kim MD J Kim MD
4
Criteria for vessel identification I1. Insonation depth
2. Direction of the flow
3. Traceability of vessels
4. Flow velocities
J Kim MD
5. The site of the probe's position
Temporal
Orbital
Suboccipital
Submandibular
Criteria for vessel identification II
6. Spatial relationships
7. Transducer angle
8. Direction of the ultrasonic beam
J Kim MD
posterior, anterior, caudad, or cephalad
9. Response to carotid oscillation or compression
J Kim MD
Criteria for Normal TCD
Artery Depth(mm) Direction MFV( Cm/s)
M2-M1 MCA
40 - 65 < 80
A1-ACA 62 - 75 < 80
J Kim MD
ICA Siphon 60 - 64 < 70
OA 50 - 62 Variable
PCA 60 - 68 < 50
BA 80 - 100 < 60
VA 45 - 80 < 50
Parameter
Peak systolic flow velocity(PV) The maximum value of flow velocity in systole, at the
apex of the waveform End-diastolic flow velocity(EDV)
The velocity measured at end diastole, usually at the
J Kim MD
y ylowest point before a new waveform begins
Mean flow velocity(MV) Estimated as the average of the edge frequency over a
cardiac cycle The edge frequency is the envelope of instantaneous
peak velocities throughout the course of a cardiac cycle MV=(PV+2EDV)/3 = EDV+(PV-EDV)/3
TCD waveform
VS VM
J Kim MD
EDV
5
Time-averaged Mean of Maximum Velocity
The time mean of the peak velocity envelope, the envelope being a trace of the peak velocity as a function of time
Automatic electronic measurements: TAMMX, TAMX(Time average of the maximum; Siemans, Acuson), TAP (Time average peak; Philips ATL)
J Kim MD
TAP (Time average peak; Philips, ATL)
Manual tracing
Manual Measurement: a horizontal line or cursor can be placed so that the area above the line and under the peak of the waveform is the same as the area below the line and above the waveform outline
J Kim MD
J Kim MD J Kim MD
Indices PulsatilityPulsatility IndexIndex (PI)(PI)
ResistanceResistance IndexIndex (RI)(RI)
J Kim MD
FlowFlow AccelerationAcceleration (FA)(FA)
Pulsatility Index I Gosling and and King PI = PV - EDV/MV The shape of the waveforms as displayed by TCD
equipment Rounded waveform: a lower PI Peaked waveform: a higher PI
J Kim MD
Peaked waveform: a higher PI An estimate of downstream vascular resistance
Low-resistance vascular beds: low PI (PI = PV -EDV/MV)
High-resistance vascular beds: high PI Peripheral vessels
6
Pulsatility Index II The low PI of the cerebral vasculature
The brain's unique metabolic needs
The brain requires continuous blood flow throughout the cardiac cycle
High diastolic flow with low downstream resistance
J Kim MD
g
Ophthalmic artery: low EDV, high downstream resistance, high PI
ICA siphon: high EDV, low downstream resistance, low PI
Resistance Index
Pourcelot
Measure downstream vascular resistance
RI = PV - EDV/PV
Increased RI
J Kim MD
Reflect increased downstream vascular resistance
0.56 (0.07)
Elevated RI ( > 0.6 ) : Increased resistance to flow
Flow Acceleration
The inclination or slope of the systolic upstroke of the waveform
Flow acceleration (FA) = PV - EDV/time differential (T) Low FA: increased upstream resistance, such as severe
proximal ICA stenosis, aortic stenosis, or decreased cardiac
J Kim MD
pperformance
T
PV- EDV
Lindegaard Index or Ratio
The MCA-ICA flow velocity ratio; VMCA/VICA
Distinguish vasospasm from states of systemic hyperemia
ICA blood flow: measure from the neck, insonation depth of 40 to
J Kim MD
50 mm
Normal: 1.76 (0.10)
Increased index of at least 3: Consistent with angiographicvasospasm in the MCA in patients with subarachnoid hemorrhage
Stenosis of Large Cerebral Artery
Typical Features of stenosis of large basal cerebral artery
Acceleration of flow: increased flow velocity
Disturbed flow
Co-vibration phenomena
ild i
J Kim MD
Mild stenosis
Increased in peak velocity with minimal change in the rest of the Doppler pattern
Moderate to severe stenosis
Greater increase in peak velocity with spectral broadening, increase diastolic velocity, turbulent flow, poststenotic drop in peak velocity
Abnormal Waveforms
Dampened signal: Pulsatile flow with normal flow acceleration and decreased MFV (30% difference between hemispheres); any PI values
Blunted signal: Delayed flow acceleration with stepwise maximum velocity arrival during mid to late systole compared with contralateral side and focal decreased MFV and positive end-diastolic flow (low PI ≤
J Kim MD
side and focal decreased MFV and positive end diastolic flow (low PI ≤1.1).
Minimal signal: Presence of a flow signal with no end diastolic flow; PI ≥ 1.2.
Absent signal: No detectable flow
7
J Kim MD
ACA Crossover
Reversed flow in ipsilateral ACA
J Kim MD
Increased velocity of contralateral ACA: ACA > MCA by at least 25%
Posterior Collateral
J Kim MD
Increased PCA velocity: PCA > MCA
ECA to ICA Collateral
Reversed ophthalmic artery
J Kim MD
Decreased pulsatility in ophthalmic artery: internalization of ophthalmic
artery
Battery of TCD indices used to predict the angiographic severity of extracranial ICA
1) Reversed flow in the ipsilateral ophthalmic artery2) Reversed flow in the ipsilateral ACA3) Elevated flow velocity (>80 cm/s) in the contralateral ACA4) Absence of Doppler signal in the ipsilateral ophthalmic artery or carotid
J Kim MD
siphon, and5) Diminished PI and FA in the ipsilateral MCA
The presence of any one of these parameters the battery "positive" a 95% sensitivity for identifying greater than 70% ICA stenosis
(NASCET)
WilterdinkWilterdink et al. Stroke.et al. Stroke. 1997;28:1331997;28:133--136136
Subarachnoid hemorrhage Increased velocities due to narrowing of vessels after SAH
Most commonly during the first week
Progression from moderate to severe vasospasm can occur within 24hours
J Kim MD
Mean MCA Velocity
MCA/ICA Velocity
ratioInterpretation
< 120 cm/s < 3 Normal, nonspecific elevation or distal MCA spasm
> 120 cm/s 3 – 6 Vasospasm of proximal MCA
> 200 cm/s > 6 Severe spasm of proximal MCA
8
An average rate of rise in Flow Velocities of > 20 cm/s/day between days 3 and 7 after SAH
A rapid early rise in FVs ( > 25%/day)
J Kim MD
A mean absolute rise in MCA-FVs or ACA-FVs of 65±5 cm/s over 24-hour period and a higher VMCA/VICA ratio (6±0.2)
Specific clinical application of TCDApplications Rating Evidence
Quality Strength
Sickle cell disease Effective Class I Type A
Ischemic cerebrovascular disease Established Class II Type B
Subarachnoid hemorrhage Established Class II Type B
Arteriovenous malformations Established Class III Type C
J Kim MD
Cerebral circulatory arrest Established Class III Type C
Perioperative monitoring Possibly useful Class III Type C
Meningeal infection Possibly useful Class III Type C
Periprocedural monitoring Investigational Class III Type C
Migraine Doubtful Class II Type D
Cerebral venous thrombosis Doubtful Class III Type D
Recommendationsecommendations were made by Babikian VL, Feldmann E, Wechsler LR, Newell DW, Gomez CR, Bogdahn U, Caplan LR, Spencer MP, Tegeler CH, Ringelstein EB, Alexandrov AV, and endorsed by the
American Society of Neuroimaging . J Neuroimaging 2000
Application
Screening of children aged 2-16 years with sickle cell disease for assessing stroke risk
Detection and monitoring of angiographic vasospasm after spontaneous subarachnoid hemorrhage
J Kim MD
p g
Cerebral Thrombolysis: monitoring thrombolysis of acute MCA occlusions
Cerebral Microembolism Detection: the detection of cerebral microembolic signals in a variety of cardiovascular/ cerebrovascular disorders/procedures
Application
TCD monitoring: probably useful to detect hemodynamic and embolic events that may result in perioperative stroke during and after carotid endartectomy in settings where monitoring is felt to be necessary
J Kim MD
Monitoring during surgery for hemodynamic status
Vasomotor Reactivity Testing
Detection of right-to-left shunts
Application Diagnosis of intracranial occlusive disease
Ancillary test for confirmation or exclusion of extracranialocclusive disease Confirmation of well-collateralized chronic ICA occlusions
J Kim MD
Diagnosis and follow-up of internal carotid artery
Evaluation of hemodynamic effects of extracranial occlusivedisease on intracranial blood flow velocities ICA stenosis or ICA occlusion Subclavian steal mechanism Extracranial lesions
Application of TCD Functional tests
blood flow velocity during activation ofcircumscribed cortical areas: light and mentalstimulation of the visual cortex, etc
J Kim MD
Noninvasive ancillary tests and monitoringprocedures in animal experiments
Monitoring during experiments in space.
9
Cerebrovascular Disease Indication
Ischemic stroke Transient ischemic attack Asymptomatic patients with high risk
J Kim MD
Usage Proximal intracranial arterial stenosis Arterial occlusion Collaterals Evidence of microembolization Proving recannalization Enhancement of thrombolysis
Transcranial Color Duplex
Transcranial Doppler with Imaging
J Kim MD
Transcranial Color Doppler
Anatomical information
J Kim MD
References CH Tegeler Neurosonology 1996
Zweibel Introduction to vascular ultrasonography. 5th ed. 2005
Cerebrovascular ultrasound in stroke prevention and treatment
Assessment: transcranial Doppler ultrasonography: report of the
J Kim MD
Assessment: transcranial Doppler ultrasonography: report of the Therapeutics and Technology Assessment Subcommittee of the American Academy of Neurology. Neurology. 2004;62:1468-1481
American Society of Neurophysiologic Monitoring and American Society of Neuroimaging Joint Guidelines for Transcranial Doppler Ultrasonic Monitoring. J Neuroimaging. 2010 Mar 17. [Epub ahead of print]
Comparison of duplex and nonduplex transcranial Doppler ultrasonography. Ultrasound Q. 2008 ; 24:167-171.
J Neurosurg 57:769-774, 1982
Noninvasive transcranial Doppler ultrasound recording of flow velocity in basal cerebral arteries
RUNE AASLID, PH.D., THOMAS-MARC MARKWALDER, M.D., AND HEt,CE NORNES, M.D.
Department of Neurosurgery, University of Bern, Bern, Switzerland
~/ In this report the authors describe a noninvasive transcranial method of determining the flow velocities in the basal cerebral arteries. Placement of the probe of a range-gated ultrasound Doppler instrument in the temporal area just above the zygomatic arch allowed the velocities in the middle cerebral artery (MCA) to be determined from the Doppler signals. The flow velocities in the proximal anterior (ACA) and posterior (PCA) cerebral arteries were also recorded at steady state and during test compression of the common carotid arteries. An investigation of 50 healthy subjects by this transcranial Doppler method revealed that the velocity in the MCA, ACA, and PCA was 62 + 12, 51 __. 12, and 44 + 11 cm/sec, respectively. This method is of particular value for the detection of vasospasm following subarachnoid hemorrhage and for evaluating the cerebral circulation in occlusive disease of the carotid and vertebral arteries.
KEY WORDS �9 arterial flow velocity �9 collateral flow ultrasonics transcranial Doppler ultrasound �9 cerebral arteries internal carotid artery middle cerebral artery
D OPPLER ultrasound recording of the blood flow velocity in the extracranial arteries supplying the brain was reported by Miyazaki and
Kato ~ in 1965 and is now used routinely in neurolog- ical and neurosurgical practice. TM The velocity in the intracranial vessels has been observed by Doppler technique during surgeryfl ,s,9 and in children with open fontanels/ In adults, however, the skull is a severe obstacle to the penetration of ultrasound. Bone strongly attenuates the ultrasonic wave, making it impossible to record noninvasively the blood flow velocity from intracranial arteries by conventional Doppler instruments operating in the range from 5 to 10 MHz. At lower frequencies, 1 to 2 MHz, the attenuation in bone and soft tissues is considerably less. The skull bones are of varying thickness, and because the bone of the temporal region is thin, this would appear to be the most promising area for penetration of ultrasound. In fact, determination of midline deviation, using echo techniques, has dem- onstrated that some penetration of ultrasound is possible.
The present study investigates the blood flow ve- locities in the middle, anterior, and posterior cerebral
arteries (MCA, ACA, and PCA) using a noninvasive transcranial Doppler ultrasound technique.
Clinical Material and Methods
Fifty healthy subjects with no history of cerebral vascular disease were investigated. Their ages ranged from 20 to 65 years, with a mean of 36 years.
For the present study we used a laboratory proto- type range-gated Doppler instrument with the follow- ing characteristics. Emitted ultrasonic frequency 2 mHz; burst repetition rate 6.8 to 18 kHz; burst length 10/zsec; high pass filter 100 Hz; low pass filter 3.4 to 9 kHz; and emitted ultrasonic power 350 mW. The effective range for this apparatus is from 3.0 to 10 cm. Sampling can be done at preselected distances from the probe within this range by means of a gating system.
The emitting area of the ultrasonic transducer was 1.5 sq cm, which is about 10 times larger than the cross-sectional area of the MCA in adults. Without focusing, only a small portion of the ultrasonic energy can be directed at the location of interest. In addition, the transducer is not effective in receiving the weak Doppler shifted signals from the blood flow. For this
J. Neurosurg. / Volume 57 / December, 1982 769
R. Aaslid, T. M. Markwalder and H. Nornes
FIG. 2. Diagram of the area (dotted line) where Doppler signals from intracranial arteries were obtained. The zygo- matic arch is indicated. The most likely location to obtain signals is shown by the position of the probe.
FIG. 1. Upper: Spectral display of the Doppler signal from the middle cerebral artery (MCA). The horizontal line through the spectra represents a cursor that can be con- trolled up or down on the display. Lower: The outline of the spectra shown above. The cursor was placed so that the areas A1 and A~ were judged equal. The velocity ~ corre- sponding to this cursor position was calculated using the Doppler equation.
reason, the ultrasonic transducer was equipped with a polystyrene acoustic lens with a focal length of approximately 5 cm. The focused beam had a width of 4 mm at this distance.
The Doppler frequency spectrum was displayed on an Angioscan* frequency analyzer. The Doppler in- strument and the frequency-spectrum analyzer have direction discrimination. The normal cognate flow direction of the artery studied was displayed as posi- tive. The end-tidal pCO2 was determined using an infrared analyzer.
It is difficult to determine the angle between the ultrasonic beam and the direction of the intracranial arteries. However, assuming that the angle is sharp, accurate determinations of the velocity are still pos- sible2 ,5 If the angle ranges from 0 ~ to 30 ~ its cosine will vary between 1 and 0.86. Thus, the maximum error will be less than 15%. Under such conditions, one can assume that the true velocity, v (in cm/sec) is given by the relation: v = 0.039 f, where f is the Doppler frequency shift (in Hz).
Figure 1 illustrates a spectrum analysis of the Dop- pler signal from the MCA in a healthy 38-year-old man. The ordinate is expressed in cm/sec, as described above. The time-mean of the outline velocity was determined using the cursor of the spectrum analyzer. The cursor was placed so that the areas A1 and A2 were equal. The cursor was also used to determine the systolic and diastolic velocities of the signal.
* Angioscan frequency analyzer manufactured by Uni= gon Industries, Inc., Mount Vernon, New York.
The exact positioning of the ultrasound probe was rather critical in most subjects. A satisfactory signal could only be obtained in a restricted region above the zygomatic arch, from 1 to 5 cm in front of the ear (Fig. 2). An "ultrasonic window" had to be located in each individual by searching this region to obtain a maximum amplitude of the Doppler signals.
In order to record the velocity in the MCA, we first set the depth of the range-gate to 5.0 cm. Usually the signal was found after a short search (Fig. 3). In difficult cases, probing for several minutes was nec- essary before obtaining the Doppler signal. Then the depth setting was increased stepwise until the MCA signal became weak. This occurred at a depth of about 6 cm, depending on the skull diameter. By aiming the probe slightly caudally, we obtained signals from the terminal portion of the internal carotid artery (ICA): This artery runs at a blunt angle with the ultrasonic beam. The Doppler signals from the intracranial ICA have lower frequency shifts than those from the MCA.
The probe was then reaimed at the MCA, and the depth of the range-gate was reduced in steps of 0.5 cm. The probe was adjusted for maximum signal at each depth. From 4.5 to 3.5 cm, we could obtain signals from two or more branches. This tracking or scanning procedure could be performed with only slight adjustments in the direction of the probe, indi- cating that the ultrasonic beam was intercepting the artery at a sharp angle.
The signal from the proximal ACA was obtained by scanning the MCA signal progressively deeper until a velocity in the opposite direction was found. The depth of the range-gate and the tilt of the probe were then adjusted for the best signal from the ACA. The proximal ACA is rather short, and we were not able to track it over a distance of more than 0.5 to 1 cm. The instrument has a finite resolution, and it was sometimes difficult to obtain a proximal ACA signal without interference from the MCA. However, this never caused serious difficulty in interpreting the data,
770 J. Neurosurg. / Volume 57 / December, 1982
Doppler recording of cerebral arterial flow
FIG. 3. Frontal view of the ultrasound probe directed toward the middle cerebral artery (MCA). The cylinder around the MCA indicates the observation region (sampling volume) for the Doppler recording. The distance from the middle of the cylinder to the probe corresponds to the depth setting.
as the spectrum analyzer has direction discrimination, allowing velocities in both arteries to be recorded simultaneously.
The PCA signal was obtained by the following procedure. The MCA was located first, then the depth of the range-gate was increased stepwise until the signal became weak and disappeared. Then the probe was tilted and aimed at a location posterior and slightly caudal to that of the MCA signal. This area was searched until we found the Doppler signal. The depth was increased further until the low-frequency Doppler shift from the basilar artery was detected. This was the distal portion of the basilar artery which runs at a blunt angle with the ultrasonic beam. Ad- vancing the depth control still further disclosed flow in the opposite direction. This came from the PCA on the contralateral side. We then tracked the ipsilateral PCA from its origin at the basilar artery and laterally until the Doppler shift was maximal. This depth was used to determine the PCA velocity.
The velocity in the ICA's in the neck was measured using the same Doppler instrument and probe that was used for the transcranial recordings. The probe was placed slightly below the mandibular angle and aimed cranially. The depth of the range-gate was set in the range from 3.5 to 4.0 cm to achieve insonation at a sharp angle (less than 30~ The external carotid artery and the common carotid artery (CCA) were identified so as to ensure that we were recording well above the bifurcation.
Results
Doppler recordings of bilateral MCA blood flow velocities were obtained in all 50 subjects. However,
the Doppler signal was not of sufficient intensity to allow ACA velocity determination in 20% of the arteries investigated. For the PCA this failure rate was 40%.
An MCA velocity recording from a healthy 51- year-old man is shown in Fig. 4 upper. The ipsilateral CCA was compressed for approximately 4 seconds, causing an instant drop in the MCA velocity to 60% of control. In this case, the MCA velocity waveform became damped. When the compression was released, the velocity rose to 130% of the control value for a period of 4 to 5 seconds, then returned to the pre- occlusion level (not shown). The probe was then directed slightly caudally until a signal from the ter- minal ICA was obtained. A new compression test was performed (Fig. 4 lower). The velocity fell to zero, and some backflow caused by an external carotid artery "steal" was observed during the systole.
In the same subject, the proximal ACA exhibited a velocity pattern as shown in Fig. 5. The upper panel illustrates a reversal of flow in this artery when the ipsilateral CCA was compressed. The proximal ACA was supplying collateral flow to the MCA on the same side in this situation. During compression, irregular flow or turbulence could be heard in the Doppler signal, particularly in systole. This showed up in the spectra as a brief period of low-frequency noise. We interpret this as the effects of a high-velocity jet from the anterior communicating artery. A recording of the proximal ACA velocity during compression of the contralateral CCA is shown in Fig. 5 lower. The velocity increased to 280% of the control value, thus demonstrating an excellent collateral capacity of the anterior circle of Willis.
J. Neurosurg. / Volume57/December, 1982 771
R. Aaslid, T. M. Markwalder and H. Nornes
FIG. 4. Spectral display of the Doppler signal from the middle cerebral artery (MCA, upper) and the terminal internal carotid artery (ICA, lower) during test compressions of the common carotid artery (CCA) on the ipsilateral side in a 51-year-old man. The MCA velocity fell by 40% during compression. Note the reversed systolic flow in the terminal ICA. This indicates external carotid artery "steal."
FIG. 5. Spectral display of the Doppler signal from the proximal anterior cerebral artery (ACA) during test compression of the common carotid artery (CCA) on the ipsilateral side (upper), and on the contralateral side (lower). Arrows indicate irregular flow during systole.
772 J. Neurosurg. / Volume 57 / December, 1982
Doppler recording of cerebral arterial flow
FIG. 6. Spectral display of the Doppler signal from the proximal part of the posterior cerebral artery (PCA) during test compression of the common carotid artery (CCA) on the ipsilateral side. Velocity increased by 60% with return to preocclusion level.
Figure 6 displays a recording of the velocity in the proximal PCA during ipsilateral CCA compression. The velocity instantly rose to 160% of the control value, indicating its potential as a collateral flow source. When the depth of the range-gate was set to a slightly more distal portion of the PCA, we did not record any appreciable change in the velocity during ipsilateral CCA compression. Compression of the con- tralateral CCA did not influence the ipsilateral PCA velocity (not shown).
The MCA velocities at different depths in 10 sub- jects are shown in Fig. 7. The lower panel illustrates the mean values of these velocities at the standard depths for MCA recording. Our data show that the MCA velocity was relatively constant over a depth range from 6.0 to 4.0 cm, with slightly more occurring at 5.5 and 5.0 cm.
The MCA velocity in the whole series was 62 _ 12 cm/sec (mean + standard deviation), with a range of 33 to 90 cm/sec. The ratio between the MCA velocity on the left side and that on the right side was 1.01 +__ 0.14:1. Thus, in the normal adult the MCA velocities are nearly equal on the two sides. The MCA velocity did not correlate with age (r = 0.23) in this series. The velocity in the ACA was 51 _ 12 cm and that in the PCA was 44 + 11 cm/sec. The velocities in the extracranial ICA were 37 +_ 6.5 cm/sec. The ratio between the velocity in the MCA and that in the extracranial ICA was 1.7 + 0.4:1. The end-tidal pCO2 was 5.1 + 0.5 kPa during these studies.
Discussion
A range-gated Doppler instrument with a frequency of 2 MHz has provided satisfactory intracranial re- cordings of the velocities in the MCA. This artery runs almost directly toward the probe and is thus ideally located for Doppler ultrasonic recording with the technique described.
The ACA and PCA describe comparatively sharp angles with the ultrasonic beam in their proximal parts. The velocities calculated from the spectral dis- play probably reflect values close to true velocities in most individuals. In some subjects, however, the ve- locities in these arteries may be slightly underesti- mated and this must be kept in mind when evaluating readings from these two arteries. Our results indicate that the ACA and the PCA will also be within reach in practically all individuals with improvements in the instrumentation, particularly the probe design.
The velocities observed in the present study were in the same range as those found by Doppler techniques during surgery. Also, the responses we obtained to test occlusions of the carotid arteries followed the same pattern as those found in these previous stud- ies. s,9 We have never observed higher velocities in the branches of the MCA than in the parent artery, and this concurs with our Doppler findings at operations. The velocities in the ACA and the PCA were generally somewhat lower than in the MCA, but higher than in the extracranial ICA. Thus, our results indicate that in the normal subject the highest velocities in the cerebral circulation are found in the basal cerebral arteries.
The systolic peak velocity in the ACA and the MCA was about 1 m/sec in more than 50% of the individuals in these series. This velocity is of the same magnitude as the systolic velocity in the aorta. It is unusual in the human circulation that arteries only 2 to 4 mm in diameter can exhibit the same peak velocity as in the aorta. Furthermore, it is of particular interest to note that, in humans, aneurysms are most apt to occur in these two arterial areas.
Transcranial Doppler recording gives useful infor- mation on the intracranial flow directions and distri- butions. A special application of the method is the determination of the collateral capacity of the circle
J. Neurosurg. / Volume 57 / December, 1982 773
FIG. 7. Diagram of the velocities in the middle cerebral artery (MCA) in 10 normal subjects (10 upper panels). The abscissae are the depth settings at which the velocity deter- minations were made. Notice that the depths of the left and fight sides run toward the midline from each side. If more than one velocity is given at a certain depth, it indi- cates that determinations in two branches were made. The lower panel represents the means of the MCA velocities in 10 subjects. The standard deviations are indicated by vertical bars.
R. Aaslid, T. M. Markwalder and H. Nornes
of Willis. One can assume that the arterial lumen stays relatively constant during CCA test compres- sion. Therefore, the flow velocity in the MCA provides direct information on the relative change in the vol- ume flow when the CCA is occluded. Furthermore, the velocities in the ACA and PCA can be studied in the same way in order to determine their relative contribution to collateral flow.
The transcranial approach can be used for the detection of vasospasms following subarachnoid hem- orrhage. When the artery contracts, or the lumen is otherwise reduced, the velocity is practically inversely proportional to the vessel lumen area. Velocities ex- ceeding 200 cm/sec have been observed in spastic arteries (material to be published). Because the method is noninvasive, it can be repeated as often as necessary, and thus be a guide in the timing of oper- ations and in the general handling of these patients.
References
1. Brisman R, Grossman BL, Correll JW: Accuracy of transcutaneous Doppler ultrasonics in evaluating extra- cranial vascular disease. J Neurosurg 32:529-533, 1970
2. Friedrich H, Hfinsel-Friedfich G, Seeger W: [lntraoper- ative Doppler sonography of brain vessels.] Neurochi- rurgia (Stuttg) 23:89-98, 1980 (Ger)
3. Holen J, Aaslid R, Landmark K, et al: Determination of pressure gradient in mitral stenosis with a non-inva- sive ultrasound Doppler technique. Aeta Med Scand 199.'455-460, 1976
4. Keller H: Die eerebrovascul~e Doppler-Ultraschall- Untersuchung (cv-Doppler). Bull Schweiz Akad Med Wiss 36:129=142, 1980
5. Light H: Transcutaneous aortovelography. A new win- dow on the circulation? Br Heart J 38:433-442, 1976
6. Miyazaki M, Kato K: Measurement of cerebral blood flow by ultrasonic Doppler technique. Jpn Circ J 29:375-382, 1965
7. Muchaidze YA, Syutkina EV: Determination of the linear velocity of the cerebral blood flow in premature infants. Hum Physiol 5:595-599, 1979
8. Nornes H, Grip A, Wikeby P: Intraoperative evaluation of cerebral hemodynamics using directional Doppler technique. Part 1: Arteriovenous malformations. J Neu- rosurg 50:145-15 l, 1979
9. Nornes H, Grip A, Wikeby P: Intraoperative evaluation of cerebral hemodynamics using directional Doppler technique. Part 2: Saccular aneurysms. J Neurosurg 50:570-577, 1979
Manuscript received May 13, 1982. Address reprint requests to: Rune Aaslid, Ph.D., Neuro-
chirurgische Klinik, Inselspital, CH-3010 Bern, Switzerland.
774 J. Neurosurg. / Volume 57 / December, 1982
top related