It has been shown that transcutaneous electrical neurostimulation (TENS) reduces sympathetic tone. Spinal cord stimulation (SCS) has proven qualities to improve coronary, peripheral, and cerebral blood circulation. Therefore, we postulate that TENS and SCS affect the autonomic nervous system in analogous ways. In this line of thought, cervical application of TENS might be a useful and simple adjunct in the treatment of cerebrovascular disease by improving cerebral blood flow. Experiments were performed in order to assess whether cervical TENS is safe and whether an effect on cerebral blood flow velocity (CBFV) can be shown in healthy subjects.
Method
A controlled, non-randomized, phase 1 study was performed with 20 healthy volunteers. Cervical TENS was applied in several frequencies, with and without hyperventilation. Continuous registration of blood pressure, pulse, CBFV (estimated by transcranial Doppler sonography) and end-tidal carbon dioxide concentration was performed.
Findings
Cervical TENS was well-tolerated by all subjects. Despite small effects on heart rate (HR) and mean arterial blood pressure (MAP), a significant effect on middle cerebral artery (MCA) blood flow velocity was not demonstrated. No effect of age, gender, current or session order on MCA, HR, or MAP was found. TENS did not influence the effect of hyperventilation.
Conclusions
In these experiments, application of cervical TENS is proven to be a safe procedure. However, no effects on cerebral blood flow velocity could be detected, perhaps due to the intact cerebral autoregulation in the healthy volunteers.
Hinweise
Comment
This study seeks to evaluate the efficacy and application of electromagnetic fields to modulate and treat cerebrovascular disease. The device of choice was the transcutaneous electrical neurostimulator (TENS); the end-point followed was cerebral blood flow in the middle cerebral artery, as measured by transcranial doppler ultrasonography. Within the 20 patients examined, no significant difference in outcomes was noted.
While simple, this paper provides a vital critique of popular mode of treatment. The use of electromagnetic and other non-invasive techniques to modify physiology has been proposed for over a century. More and more we see variations on this in products from industry designed to treat diseases without pills or surgery. The pursuit of non-invasive therapies is wonderful, but this article reminds us of the need to be rational and critical in our evaluation of novel therapies.
Markus Bookland, MD
Christopher M. Loftus MD
Philadelphia, USA
Introduction
Spinal cord stimulation (SCS) is widely used in the treatment of pain. Although several mechanisms have been proposed, its exact mechanism of action remains unclear [13]. At least part of the effects of SCS is mediated by the autonomic nervous system, as shown by the fact that sympathetically mediated pain (e.g., visceral pain and complex regional pain syndromes) responds better than nociceptive pain to SCS treatment [13]. In addition, it has been demonstrated that SCS has autonomic (side)effects, such as increasing peripheral blood flow in Raynaud's phenomenon, peripheral ischemic pain, coronary disease, and complex regional pain syndromes [4, 11, 13]. Since the sympathetic fibers are located ventrally in the spinal cord and SCS electrodes are placed dorsally, these ventral fibers are not located within the electrical field. Therefore, these autonomic effect must be indirect, e.g., via antidromic pathways [13].
Transcutaneous electrical neurostimulation (TENS) has been used since 1974 to test the tolerance for stimuli in the work-up for SCS [1]. Some of the effects seen in SCS can be produced by TENS as well. Effects on peripheral blood flow have been shown, as well as increased coronary perfusion [12]. An experiment on autonomic cardiovascular reflexes demonstrated a decreased sympathetic response when using TENS [17]. Since the sympathetic effects as shown by SCS must be indirect effects of the electrical stimulation, we postulate that TENS produces these effects in the same way.
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In several studies, an increase of cerebral blood flow (CBF) has been described as a result of cervical SCS [2, 3, 9, 10]. The effects of SCS on CBF are most likely mediated through the sympathetic nervous system, since cerebral vasculature is highly sympathetically innervated and the vascular diameter is related to sympathetic tone [18]. Patel showed that this effect is mediated via a central pathway [15]. This pathway involves brainstem vasomotor centers that connect with the cerebral microvasculature through intrinsic nerve pathways. In experiments on rats, he showed that surgical sympathectomy failed to influence the CBF response caused by cervical SCS, while transsection of the spinal cord at the cervicomedullary junction completely abolished all increases in CBF. Taking into account the proven effect of TENS on peripheral blood flow and its (indirect) effect on sympathetic tone, TENS should be able to alter CBF, an analog to SCS. As such, TENS could be a useful non-invasive adjunct in the treatment of cerebrovascular disease (CVD).
TENS either has a direct effect on vascular diameter or has an effect on the sympathetic tone. If the latter is true, then, in resting conditions, there should be no effect on CBF. Therefore, in order to find out whether the sympathetic tone is reduced by TENS, the effects of TENS on CBF in hyperventilating subjects is of interest. Given that cerebral blood flow in response to hyperventilation might partially be sympathetically mediated [7, 8], this response should be reduced by TENS.
As cervical TENS is a novel potential therapeutic application in the treatment of CVD, this paper describes the experiments that were performed to assess the effects of TENS on CBF in healthy subjects and to register its potential side effects.
Materials and methods
Study design
The study was designed as a controlled (subjects were their own controls), non-randomized phase 1 experiment. Healthy volunteers were recruited from the general public by advertisement in the local newspapers. Cerebral blood flow velocity (CBFV) can be seen as a representation of CBF when the vascular cross-sectional area (CSA) remains constant (CBFV=CBF/CSA). Cerebral blood flow velocity was measured by transcranial Doppler (TCD) of the medial cerebral artery (MCA). The trial has been authorized by the local Research Ethical Board and the Dutch Central Commission of Human Research.
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Sample size calculation
The literature reports inter-individual standard deviation of flow velocities as about 15% [21] and the intra-individual standard deviation as 8% [14]. Sample size calculation is based on the requirement that a difference in flow velocities of 20 cm/s (ca 20%) between frequencies 2 and 120 Hz should be detected with a probability (power) of 90% when testing at a significance level of 5% two-sided. This results in a sample size of 20.
Treatment of subjects
The subjects were treated with conventional TENS, providing a continuous flow of symmetrical rectangular biphasic pulses (Schwa Medico, Pierenkemper GMBH; Wetzlarestr. 41-43, D-35630, Ehringhausen, Germany). Stimulation was performed at 90% of the highest tolerated current, with a pulse-width of 200 ms. Stimulation frequencies were 2, 20, 50, 100, and 120 Hz. In this way, the entire range of possible TENS frequencies and the most used frequencies in current TENS treatments were captured. Subjects were supine during the entire experiment. The TENS electrodes were applied cervical at the height of the mandible on both sides of the nuchal ligament (dermatome C2-C3). Doppler probes were applied to the skull for continuous registration of flow velocity in the MCA (left and right). Continuous registration of pulse and blood pressure was recorded by plethysmography.
For the first experiment (Fig. 1), five blocks of measurements took place for each TENS frequency, 5 min of registration without TENS, and followed by 5 min with TENS (so each TENS frequency had its own control-baseline). The order of frequencies was randomized (using the QuickCalcs online calculator, GraphPad Software, Inc.) in order to correct for possible alteration in time of the sympathetic tone during the experiment.
Fig. 1
Set-up of experiment 1: five blocks of baseline measurements followed by 5-min measurement with TENS in randomized frequencies 1 to 5
×
The second experiment (Fig. 2) was designed to examine whether TENS influences the normal cerebral regulation that physiologically occurs in reaction to hyperventilation. In the same way as the first experiment, blocks of measurements were recorded, now at a fixed frequency of 100 Hz. For practical purposes, only one frequency was used for this experiment. The frequency of 100 Hz was chosen because it has been used in previous TENS experiments to alter blood flow in coronary arteries [5]. During this part of the experiment, end-tidal partial carbon dioxide concentration (ETCO2) was measured in the exhaled air as a measure of hyperventilation. Hyperventilation was defined as a decrease of ETCO2 to 2%. Measurements were performed following the scheme below (in half of the subjects the order was reversed, i.e., first TENS with hyperventilation):
Fig. 2
Set-up of experiment 2: two blocks of baseline measurements, followed by a measurement with hyperventilation either with or without TENS. Order of measurements was reversed in half of subjects
Three minutes registration with hyperventilation (1 min to achieve an ETCO2 of 2%, 2 min measurement)
Ten minutes registration without TENS/hyperventilation
Three minutes registration with TENS and hyperventilation (1 min to achieve an ETCO2 of 2%, 2 min measuring)
Ten minutes registration without TENS or until baseline variables were approached
×
Data processing
Data was collected using a continuous TCD monitor (DIGI-LITEtm, Raanana, Israel), a plethysmograph for assessing blood pressure and pulse (Finometer-Pro, Finapress Medical Systems, Amsterdam, The Netherlands), an electrocardiograph (Finometer-Pro, Finapress Medical Systems, Amsterdam, The Netherlands), and a capnograph (Capnomac Ultima, GE Healthcare, Chalfont St Giles, UK). All analog output was routed to a computer via a digitizer. The data were continuously registered using Neuromon (incorporating Labview 7.1, National Instruments) software. Before statistical analysis, all artifacts were deleted from the data streams (e.g., reduced Doppler signal due to transducer dislodgement). In order to clean the data from noise, filtering was performed using in-house written routines in the Matlab environment (The Math Works, Inc., Natwick, MA, USA, Matlab 6.5). Bandwidths for the data were defined (50–150 bpm for HR, 5–100 cm/s for MCA, 60–180 mmHg for ABP, and 2–6% for CO2 in resting phase), and top and bottom 10% of data were deleted, replacing those by linear interpolation. Next, 3-min data streams were taken from each measurement, in each case a stream from −4 to −1 min before the start of TENS and a stream from +1 to +4 min after the start of TENS. From the hyperventilation data, a stream was taken from −2.5 to −0.5 min from the start of HV and another 2-min stream as soon as ETCO2 had stabilized around 2–2.5% (app. 15–20 mmHg). Average values of all streams were calculated and used for statistical analysis.
Statistical analysis
The purpose of the analysis was to find out (1) the effect of different TENS frequencies on cerebral blood flow and (2) whether the TENS frequency of 100 Hz modifies the effect of hyperventilation on cerebral blood flow. The data from the first experiment were used to address the first question and the data from the second experiment to address the second question. For each TENS frequency, we subtracted the measurement at the preceding non-TENS session from the measurement with TENS and used these “baseline-corrected” differences as basic outcomes in the analysis. We used all observations from the MCA side which had the highest blood flow velocity at baseline as measured by TCD. For both questions, the analysis consisted of fitting mixed effects regression models to the data [16]. For question 1, we have used the TENS frequency (at five levels), the order of observations, age, and gender of the participants as fixed effect explanatory variables. For question 2, the fixed effects were TENS frequency (0 or 100), ETCO2, age, and gender. Statistical tests were carried out at 5% level of significance. We used the statistical package R for computations (version 2.8.1; library nlme).
Results
A group of 11 females and nine males, all healthy subjects, completed the experiment, in age ranging from 25 to 65 years (median 46.5 years). Two more volunteers participated, but their measurements failed. In one individual, the temporal bony windows were insufficient to obtain adequate MCA signals. In the other, an exceptional amount of noise was perceived on all signals; therefore, the experiment was aborted.
All volunteers tolerated TENS well, though the highest tolerated current did vary from 10 to 35 mA. The only adverse events reported by the volunteers were pressure from the cap used to position the TCD probes and tingling sensations or dizziness as a result of the hyperventilation. All volunteers reached the predefined threshold of an ETCO2 of 2% during hyperventilation.
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Figure 3a shows box plots with values of MCA blood flow velocities, blood pressures (MAP), and pulse (HR) without TENS and per TENS frequency for the first experiment. Box plots in Fig. 3b show differences between MCA blood flow velocities, MAPs and HR, and their coupled baseline values. The mean differences and the corresponding confidence intervals for MCA, HR, and MAP are shown in Table 1. The effect of TENS on MCA was on average 0.78 cm/s (95% CI; 0.06 to 1.50), the effects at different TENS frequencies were not statistically significantly different (P = 0.80). For HR and MAP, too, the effects of different TENS frequencies did not differ (P = 0.06 and P = 0.14, respectively). Compared with the baseline, the HR was significantly lower at 120 Hz, and the MAP was significantly higher at 2, 50, and 100 Hz. However, the effects are so small, that they cannot be judged clinically relevant. No effect of age, gender, or session order on MCA, HR, or MAP was found.
Fig. 3
Box plots of mean values of cerebral blood flow velocities in MCA (centimeters per second), heart rate (HR; beats per minute), and mean arterial pressure (MAP; millimeters of Hg) at the different TENS frequencies (a 0 = baseline). The plots in b show the differences of the mean values when compared with baseline
Table 1
Differences of MCA blood flow velocities (MCA), heart rates (HR), and mean arterial blood pressures (MAP) for each TENS frequency compared with their coupled baseline values
MCA
HR
MAP
Frequency
Effect
95% CI
Effect
95% CI
Effect
95% CI
2 Hz
1.019
(−0.277, 2.315)
−0.233
(−1.410, 0.944)
2.133a
(0.720, 3.547)
20 Hz
0.399
(−0.897, 1.695)
−0.453
(−1.750, 0.844)
0.876
(−0.570, 2.322)
50 Hz
1.247
(−0.049, 2.543)
−0.116
(−1.369, 1.137)
2.565a
(1.152, 3.979)
100 Hz
0.874
(−0.423, 2.170)
0.713
(−0.500, 1.927)
2.180a
(0.766, 3.593)
120 Hz
0.347
(−0.931, 1.661)
−1.844a
(−3.057, −0.631)
0.668
(−0.778, 2.115)
Overall
0.781
(0.060, 1.501)
−0.390
(−0.971,0.191)
1.708
(0.825,2.591)
aSignificant effect
×
Figure 4a, b show box plots of values of MCA blood flow, blood pressure, and pulse for experiment 2: with and without TENS, and with and without hyperventilation. No significant effect of TENS on MCA, HR, or MAP on the effect of hyperventilation was detected (P values 0.43, 0.58, 0.31, respectively). ETC02 (difference between the measurements with and without hyperventilation) was found to be positively related to MCA and negatively to HR (P < 0.001).
Fig. 4
Box plots of mean values of MCA blood flow velocities (centimeters per second), heart rate (HR; beats per minute), and mean arterial pressure (MAP; millimeters of Hg), for baseline (c1 and c2), hyperventilation (HV), and hyperventilation combined with TENS (HV+; a). Differences of the mean values of TENS with (TENS+) and without (TENS−) hyperventilation, compared with their baselines are shown in (b)
×
Because the highest tolerated current varied between volunteers from 10 to 35 mA, we have also included the current in the fixed-effects model. No statistically significant effects of current could be found.
Discussion
We have studied whether TENS can influence the cerebral blood flow in healthy subjects. We postulated that TENS might influence cerebral blood flow via sympathetic pathways as observed in experiments with SCS [2, 3, 6, 9‐11, 13, 15]. Also, TENS has been shown to increase locoregional blood flow and sympathetic tone [12, 17].
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The purpose of this study was twofold: (1) to find out if the use of cervically applied TENS is safe and (2) to find out the effect on CBF in healthy subjects.
We suggested TENS might either (indirectly) create a sympathetic response that influences CBF or TENS might alter the sympathetic tone. To test the first way of action, we performed experiment 1 in which CBF was measured during stimulation with several TENS frequencies in resting healthy subjects. If only sympathetic tone is influenced by TENS, subjects in rest will not show an effect, but subjects that have to apply their autonomous nervous system might. Because the cerebral response to carbon dioxide changes might be partially sympathetically mediated [7, 8], we have also tested whether TENS influences the response to hyperventilation.
Because sympathetic tone can easily change during an experiment (an individual can become either more or less comfortable during the experiment), we have applied several measures to compensate for this effect. Firstly, we have randomized the order of applied TENS frequencies; secondly we have provided each frequency with its own control-baseline-measurement, and thirdly, the order of TENS with/without hyperventilation varied.
TENS was tolerated very well by all subjects. No adverse events were found. Also, systemic blood pressure and heart rate were not affected by TENS in a clinically relevant manner.
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As for the effect of TENS on CBF, no statistically significant effects were found for the individual TENS frequencies, neither at rest nor in the hyperventilation experiment. Overall, there was a small increase of MCA blood flow velocity (0.78 cm/s) when TENS is compared with rest. The fall in MCA blood flow velocity as a result of hyperventilation was a little less prominent when TENS was applied, but this did not reach statistical significance.
Several explanations can be advanced as to why no effect was found. Firstly, of course, there might be no effect at all. Secondly, TENS might not be powerful enough because subjects can only tolerate a certain amount of current. However, we did not find a difference between volunteers that tolerated higher and volunteers that tolerated lower currents. Thirdly, we have only used one frequency in the hyperventilation experiment; possibly, other frequencies give different results. Fourthly, one might have to apply TENS for a longer period, although we do not think this is plausible, given the results of other TENS studies. Finally, regulatory mechanisms of CBF are complex. CBF depends on several parameters including MAP, ICP, CO2, O2, and other (auto)regulatory mechanisms. The role of the sympathetic nervous system on these parameters remains unclear. Sympathetic tone does regulate MAP by means of peripheral vasoconstriction in organ beds, but there is ongoing debate about the sympathetic effects on cerebral vasculature [19, 20]. Also, the effects of CO2 might be far stronger than the sympathetic effects; possibly, sympathetic tone only has a modulating effect [8]. Moreover, the study was performed in healthy subjects with a powerful, intact autoregulation. This might have masked the effects of TENS on sympathetic tone.
The power analysis was aimed at finding a clinically significant effect; thus, with our experiments, we can only conclude that there seems to be no such effect in a healthy population. This does not yet prove that TENS does not influence the sympathetic nervous system and CBF, especially because we did notice a tendency towards less decreased blood flow velocities in reaction to hyperventilation when TENS was applied.
Possibly, an effect of TENS is appreciated in patients with disturbed autoregulation, e.g., patients with cerebral ischemia or following subarachnoid hemorrhage (with locally disturbed blood–brain barrier). Since cervical TENS did not have a clinically relevant effect on systemic blood pressure and heart rate, TENS can be safely applied to those patients. We think it is important to further investigate the effect of TENS on CBF in the presence of a disturbed autoregulation, especially since the influence of sympathetic tone is possibly much more significant in these pathological situations.
Open Access
This article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
Open AccessThis is an open access article distributed under the terms of the Creative Commons Attribution Noncommercial License (https://creativecommons.org/licenses/by-nc/2.0), which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
Comment
This study seeks to evaluate the efficacy and application of electromagnetic fields to modulate and treat cerebrovascular disease. The device of choice was the transcutaneous electrical neurostimulator (TENS); the end-point followed was cerebral blood flow in the middle cerebral artery, as measured by transcranial doppler ultrasonography. Within the 20 patients examined, no significant difference in outcomes was noted.
While simple, this paper provides a vital critique of popular mode of treatment. The use of electromagnetic and other non-invasive techniques to modify physiology has been proposed for over a century. More and more we see variations on this in products from industry designed to treat diseases without pills or surgery. The pursuit of non-invasive therapies is wonderful, but this article reminds us of the need to be rational and critical in our evaluation of novel therapies.
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