Effect of variable p (number of + values) on Stage-1 pre-indication labeling of training data.
1. Introduction
Epilepsy is a neurological disorder that changes the observable behavior of an individual to the point of inducing complete loss of consciousness. Pharmaceutical drugs may reduce or eliminate the problems of epilepsy, but not all people respond to pharmaceuticals favorably, and some may find the side effects undesirable. EEG-based epilepsy prediction may offer an acceptable alternative or complementary treatment to pharmaceuticals. Invasive, intra-cranial EEG provides signals that are directly from the brain, without the muscular activity that infests non-invasive, scalp EEG. However, intra-cranial EEG requires surgery, which increases risk and cost of health care, while reducing the number of people able to receive medical attention. Algorithms to predict the seizure event—the ictal state—may lead to new treatments for chronic epilepsy. Finding solutions that involve non-invasive procedures may result in treatments for the largest section of the population.
2. Background
Epilepsy prediction is greater than 1 minute of forewarning before there is any visible indication that a seizure will occur. The physician does not label the pre-ictal periods that precede the seizure—states that may indicate a seizure is near. Event characterization only labels the start time of the seizure. Consequently, labeled data for the pre-ictal state is non-existent, but is necessary to train a Support Vector Machine (SVM). Other researchers address this problem by assuming that the pre-ictal phase occurs immediately prior to a seizure [1]; see Figure 1 for an example.
The labeling scheme of Figure 1 results in better than random predictions [1] under the assumption that the pre-ictal region immediately precedes the seizure and may be exploited for epilepsy prediction. This SVM approach provides the most obvious way to label the training and testing data without any extra information being available about the EEG.
Assuming pre-ictal dynamics occur within an hour of the seizure has the added benefit of being more likely to satisfy caregivers’ requests to have forewarning within an hour of the seizure event. Netoff et al. achieve a specificity of 77% in classifying the pre-ictal region with no false positives with the above approach [1]. This level of accuracy is not high enough for a marketable prediction algorithm, but suggests that indicators of a seizure occur within an hour prior to a typical seizure. Netoff et al. use a “5 minute prediction horizon” where they label the pre-ictal region. They classify preictal as being within 5 minutes of the seizure and calculate specificities according to that labeling scheme. They assert that the short time frame makes the computational difficulty of the algorithm much more manageable than algorithms that have fewer restrictions on where the pre-ictal region is. They have a second stage of processing as well in which they look for 3 out of 5 pre-ictal indicators in a concentrated bundle in order to achieve prediction [1].
The assumption of pre-ictal indications near the event seems sound because a seizure resembles a dynamical phase transition. More specifically, the brain activity changes from some “normal” phase of brain activity into hyper-synchronous activity. The present work assumes that the brain dynamics within an hour of the seizure are approaching a phase transition, corresponding to measureable change in the scalp EEG. A simple example of a phase transition is liquid water becoming steam due to changes in pressure and temperature. However, scalp EEG exhibits nonlinear, chaotic features that are extremely difficult to predict over long periods and are extremely sensitive to initial conditions. Consequently, seizure prediction in a very complex system like the brain is very difficult. Indeed, Stacey
One must also choose whether to use monopolar (single channel) or bipolar EEG (difference between two monopolar channels). Mirowski et al. assert that epilepsy can be predicted more effectively with bipolar features [3] because of changes in the brain’s ability to synchronize regions during a seizure. Mirowski et al. consider their pre-ictal period to be 2 hours. They assert, “[most] current seizure prediction approaches can be summarized into (1) extracting features from EEG and (2) classifying them (and hence the patient’s state) into pre-ictal or inter-ictal”. They go on to enumerate more specifically on the bipolar feature set in Figure 2.
Figure 2 enumerates a feature set from all unique channel pairs [3]. After the enumeration, they use a grid search to find appropriate parameters with their SVM with a Gaussian kernel. Mirowski et al. use intra-cranial EEG data and obtain 100% accuracy for patient-specific machine learning models. However, no single model provides 100% accuracy for all patients [3], so they choose from among a variety of algorithms to achieve high accuracy on a patient specific basis.
By contrast, the present work uses non-invasive, scalp EEG. Moreover, the present work uses a SVM to extract seizure forewarning from the entire patient population. The goal is high accuracy. The long-term objective (not addressed in the present work) is lower health-care cost by using one algorithm for all patients to analyze scalp EEG on a smartphone.
Previous work by Hively
3. Phase-space analysis
We use one bipolar channel of
These data were uniformly sampled in time,
A patented zero-phase, quadratic filter enables analysis of scalp EEG by removing electrical activity from eye blinks and other muscular artifacts, which otherwise obscure the event forewarning. This filter retains the nonlinear amplitude and phase information [14]. The filter uses a moving window of 2
A trade-off is required between coarseness in the data to exclude noise, and precision in the data to accurately follow the dynamics. Thus, the artifact-filtered data (
Here, INT converts a decimal number to the closest lower integer. Takens’ theorem [15] gives a smooth, non-intersecting dynamical reconstruction in a sufficiently high dimensional space by a time-delay embedding. The symbolized data from Eq. (1) are converted into unique dynamical states by the Takens’ time-delay-embedding vector,
Takens’ theorem allows the
The states from Eq. (2) are nodes. The process flow,
The value, B, is the number of base cases, which establishes a normal range of activity for the patient. The value, N, is the number of sampled points that are in a cutset and graph, The value, w, as mentioned previously is the half-width of the eye-blink filter in sampled point units. The value, S, is the number of bins that the EEG is discretized into in order to create the base-s number represented by the vector y(i) in Figure 4. The value, d, is number of numerals in the base-s number or elements in the d dimensional vector, y(i). L is a time delay embedding that specifies the interval between points sampled in order to create a node. M is a second time delay embedding that specifies the interval between two connected nodes. The parameters mentioned are all used to generate the phase space graphs illustrated in Figure 4.
The dissimilarity measures involve counting unique nodes and links (those not in common between the two graphs): (1) nodes in graph A but not in B; (2) nodes in B but not in A; (3) links in A but not in B; and (4) links in B but not in A. Nodes and links in common between graphs do not indicate change and are not useful. These measures sum the absolute value of differences, which is better than traditional measures that use a difference of averages. Each measure is normalized to the number of nodes (links) in A (for A not in B) or in B (for B not in A). This feature vector,
The present work uses a SVM approach to obtain forewarning from the normalized dissimilarity measures—namely, we find nonlinear regions in the feature space using a SVM. Figure 5 shows the calculation of the dissimilarity measures [4]. The frequency of nodes and links is not used because Takens’ theorem guarantees topology, but not density—meaning Takens’ theorem doesn’t guarantee useful information in the repetition of nodes or links.
The dissimilarity measures in Figure 5 capture topology changes between two graphs. While node and link differences are basic graph measures, they quantify the hypothesis in a very simple and general way. Less commonality of nodes and links between two graphs produces larger dissimilarity measures, which are used to capture changes in topology. Topology change is a necessary, but not sufficient condition for a phase transition [17]. Our results show that changes in topology over extended periods indicate a higher likelihood of observing a phase transition as an indicator of an impending seizure. Additionally, the four graph dissimilarity measures from nodes and links rely on two concepts from set theory and Venn diagrams. Node dissimilarity and link dissimilarity are broken into two measures of dissimilarity each. Comparing two graphs (A and B) results in differences in nodes, as well as links. The dissimilarity measures are used as SVM features (for a total of 4 features in the Stage-1 SVM described below), and include the nodes in graph A that are absent from graph B, links in graph A that are absent from B, nodes in graph B has that are absent from graph A, and links in graph B that are absent from graph A. All four dissimilarity measures are normalized and vary with cutset. Figure 6 shows these dissimilarity measures varying with time and how each cutset results in features and labels (“+” for pre-ictal, and “–“ for inter-ictal).
Analysis of graph dissimilarity measures by a SVM allows quantification of the change in topology over time by determining how dissimilar the graphs must be to predict an epileptic event. The details of the forewarning algorithm are in Section 5—with a brief overview of Support Vector Machines in Section 4.
4. SVM with RBF kernels
SVMs are one of the most commonly used supervised learning tools. The SVM approach was originally designed as a two-class (binary) classifier, but has been expanded to single and multiple classes. A SVM without a kernel function performs linear classification by finding a hyper-plane in the feature space that best maximizes a margin of separation between two classes with a given list of features.
SVM kernels define the similarity between two points in the feature space. For example, with a radial-basis-function (RBF) kernel, two points are said to be similar when they are proximate to one another in the feature space. The RBF kernel function for two points in a feature space evaluates to 1 when the distance between the two points approaches zero. The RBF, Gaussian kernel function evaluates to 0 as the distance between the two points becomes very large. The region where the kernel function evaluates to zero is parameterized by the value of gamma (
Each point in Figure 7 is equivalent to one instance of a class. Positive class values are denoted by positive signs and negative class values are denoted by negative signs. The Cartesian dimensions are the feature values—such as a dissimilarity measure. More than two features (two dimensions) can be used with a SVM, but it is more difficult to visualize when more than 3 dimensions (features) are involved. The main requirement of a RBF kernel is that the training set has a representative sample of the data that will be observed in the future and enough features to make distinctions between classes. Additionally, the range and scale of each feature has a large effect on the value of
Here,
Once the vector
Once the vector
Without a kernel, the vector
LIBSVM makes the details of the linear algebra of the training and testing transparent to the user and is easily used with the intuitions given in this Section [19]. The effect of a RBF kernel is that points proximate to one another will be labeled as belonging to the same class. Multi-class classification is treated as several binary classifications and is beyond the scope of the present work.
5. SVM forewarning algorithm using graph dissimilarity features
Labeling training data as pre-ictal or inter-ictal requires assumptions that must be sound. Current epilepsy prediction algorithms offer guidance about acceptable assumptions. The goal is enough forewarning to stop or mitigate an event. Patients and caregivers [20] suggested 1-6 hours for safety, planning the day, and “driving myself to the hospital.” Non-parent caregivers preferred 25 minutes to 1 hour for travel to the patient’s location. Others gave 3-5 minutes, because longer forewarning was seen as more stressful to the patient. These requirements—as well as previous research indicating that these constraints are a reasonable request—led to the labeling scheme used for pre-ictal indications for a SVM. For epileptic event data sets, the pre-ictal region is labeled as being anywhere from 3.3 minutes to 70 minutes before the seizure. Each epileptic patient is labeled as being pre-ictal for the same length of time prior to the seizure. Each plus and minus sign in Table 1 represents a 3.3 minute window (consistent with a cutset length of 49716 points, sampled at 250 Hz). The number of pluses is determined by a parameter (p) that is varied during cross validation. Figure 6 shows how the signs in Table 1 relate to graphs, features, cutsets, and dissimilarity measures.
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Event data set | -----------------------------------+ | --------------------------+++++++++++++++++++++ |
Non-event data set | ------------------------------------- | -------------------------------------------------------------- |
Value of p | 1 | 21 |
The input labeling (e.g., Table 1) assumes only approximate correctness and uses class weights to vary the correctness likelihood. The SVM methodology is implemented in three Stages with 10-fold cross validation. Stage-1 constructs a classifier that can label the pre-ictal state indicators. Stage-2 determines how long a patient must exhibit pre-ictal indicators in order to be certain of a seizure. Stages 1 and 2 establish cross validation accuracy and error. The SVM forewarning algorithm and previous voting method algorithm [4] both imply that patients must be in abnormal states a higher portion of the time before they are likely to have a seizure. Datasets without seizures can have infrequent abnormal states as well. Stage-3 obtains two models that can be used for seizure prediction in an ambulatory setting. Cross validation results in k different classifiers that leave out disjoint sets of data to establish an off-training-set error (OTS error) to avoid overconfidence in accuracy. However, k slightly handicapped classifiers result in either less accuracy than is possible or more complexity in creating an ensemble. Stage-3 avoids this unnecessary choice by performing cross validation to create a final SVM model that includes all of the available data. Accuracy and error rates are statistically stronger, when they are reported from cross validation. The statistical claims are less robust, when one trains and tests on the same data. SVM with a RBF kernel is particularly susceptible to over-fitting—implying the need for cross validation. Figure 8 shows an outline of this three-Stage algorithm.
Figure 9 shows how Stages 1 and 2 flow together. Stage-3 involves training the RBF Model on all of the Stage-1 cutsets (4244 rows, instead of approximately 90% of it) and training the linear model on the all of the Stage-2 results (60 rows, instead of 90% of it). Then, one predicts on the training data to verify that the model is working as expected to produce
Figure 9 shows that event datasets are labeled in Stage-1 as pre-ictal (+) in a window of p cutsets prior to the seizure and inter-ictal (-) outside of this window. All cutsets in non-seizure datasets are labeled as inter-ictal (-). A cost sensitive SVM is used to account for the uncertainty in the pre-ictal and inter-ictal labeling. The motive for this labeling scheme is the caregiver’s desire to have forewarning within an hour of the event. Indicators are assumed to be near the event, and the time window is varied by the parameter (p) that is tested during cross validation. The assumption behind the design choice is that the pre-ictal state is a rare occurrence. Because there may be similar points in the feature space outside the hour time-frame being labeled as pre-ictal and inter-ictal, the variable for class weights are varied via a Monte-Carlo search over the parameter space during cross validation to determine how to tie-break. Other parameters are also varied randomly during the Monte-Carlo search, as shown in Table 2. To compensate for labeling uncertainty, the cost sensitive SVM adjusts a weight on the class labels to indicate how certain the labeling scheme is for the pre-ictal and the inter-ictal classes. The labeling scheme combined with the features, training set, class weights, and gamma creates regions in the feature space that will be associated with one class or another. Additionally, we use stratified cross validation—maintaining a ratio of 4 event patients and 2 non-event patients in each strata of cross validation. Cross validation is performed on 90% of the patients—54 patients in each training set and 6 patients in each test set—having varying numbers of cutsets due to having varying length observations. This process is repeated 10 times with disjoint sets of patients in each test set.
Successive, contiguous occurrences of pre-ictal indicators trigger an alert (prediction of an event). Non-event datasets have more inter-ictal indicators labeled with negative symbols, while event patients have fairly dense pre-ictal indicators—labeled with plus symbols. A single pre-ictal indicator is usually not enough to make accurate predictions.
The accuracy of the assumptions is reflected in the success rate of the predictions during cross validation. The parameters that appear to be uncertain are left as search variables, recognizing that more free parameters create a more computationally complex search. Too many variables result in a computational explosion in the CPU time to explore the search space. Each point in the parameter space corresponds deterministically with a cross-validation error rate. Assumptions about the certainty of the training or testing example’s labels are represented by class weights in a cost sensitive SVM. Table 2 shows the variables for the SVMs that were searched during the research for this paper.
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Sets the radius of the contribution of a single point to the decision boundary | Adjusts the pliability of the Stage-1 decision boundary given additional points |
Weighs how powerfully the + class influences the decision boundary | Weighs how powerfully the – class influences the decision boundary | Adjusts the pliability of the Stage-2 decision boundary given additional points | Number of cutsets prior to the event that are labeled as being in the positive class. |
Figure 4 and Table 3 lists other variables that might be searched in addition to those of the SVM. Those parameters were fixed in the present analysis because Takens’ theorem is sufficiently powerful to show significant changes in topology with many sets of parameters when those topological changes are normalized properly. The dissimilarity measures for a patient reflect relative differences in graph topology. The parameter values for the phase-space graph generation are shown in the Table 3. Recall that these parameters were described near and are contained in Figure 4. Throughout the entire analysis, the parameters to generate the phase space graphs were kept fixed. These values were found in our prior work [4] to give good forewarning using ensemble voting methods mentioned in the background section.
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12 | 7 | 56 | 77 | 49716 | 3 | 29 |
Statistical validation of forewarning requires measures of success. One measure is the number of true positives (TP) for known event datasets (Ev), to yield the true positive rate (sensitivity) of TP/Ev. A second measure is the number of true negatives (TN) for known non-event datasets (NEv). The true negative rate is TN/NEv (specificity). The goal is a sensitivity and specificity of unity. Consequently, minimizing the distance from ideal (
Eq. (6) is the objective function to be minimized for the OTS error rate and over-fit error rate. The OTS error rate is found from 10-fold cross validation from Stages 1 and 2. The over-fit error rate verifies that the final models in Stage-3 can correctly predict the training examples. Excessive false positives (inverse of a true negative) will cause real alarms to be ignored and needlessly expend caregiver resources. False negatives (inverse of a true positive) provide no forewarning of seizure events. A Monte-Carlo search is used over variables in Table 2 because the prediction distance has very irregular, fractal behavior—with sparse parameters generating good predictions and the gradients of the parameter space being highly irregular with many local maxima and minima [4].
The algorithm for forewarning is done in two Stages of processing after producing diffeomorphic graphs and their dissimilarity measures for each graph. Stage-1 uses a cost sensitive SVM type (CSVC) from LIBSVM [19] with a RBF kernel. For each iteration of the cross validation, the algorithm labels event data sets as having pre-ictal indicators within a one-hour window prior to the seizure; see Table 1. The length of this window (p cutsets) is part of the Monte Carlo search. All other values—non-event data and event data far away from the seizure (outside the variable window)—are labeled as inter-ictal indicators. The analysis trains on k-1 sets, then predicts on a single, left-out set; this analysis is repeated k times in a k-fold cross validation (with k being 10). Table 4 shows a small sample of Stage-1 predictions for two patient outputs, but in actuality there are 60 sets of predictions—like Table 7 in the results section.
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Event Data set | --------------------+--------------------+-----++-++----------+++E 53 | 3 |
Non Event Data set | -------------------------------------------------------NE no prediction | 0 |
After making the six predictions on six patients for one of ten cross validation runs, one creates a new set of cross validation folds (representing sets of patients) for the Stage-2 analysis out of the Stage-1’s predictions on the omitted set (similar to the middle column of Table 4). For the Stage-2 single feature, one scans each of the predictions made by the Stage-1 for the maximum number of contiguous occurrences of pre-ictal indicators. Specifically, the third column of Table 4 is obtained from scanning the second column of Table 4. Stage-2 of the algorithm has training and testing files that follow the format of the second and third columns of Table 5.
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Event Data set | +1.0 | 3 |
Non Event Data set | -1.0 | 0 |
The analysis labels the Stage-2 training and testing values as either event or non-event data sets. In general, there are fewer pre-ictal indicators (+ in Table 4) in the non-event data sets on successful cross validation runs. One determines the cross validation average prediction distance by training on values of maximum contiguous, pre-ictal indicators from k-1 subsets at the Stage-2, making k predictions on the omitted subset, and then taking the average of the prediction distances.
Stage-3 obtains the cross-validation prediction distance via two models that predict on the basis of all of the data available instead of 90% of it. Specifically, Stage-3 takes the 4244 cutsets labeled in Stage-1 and the sixty predictions from Stage-2 to create two SVM models for predicting on future patients. Stage-3 involves retraining both the RBF model (from Stage-1) and linear model (from Stage-2). Figure 10 illustrates the flow in Stage-3 after optimal parameters have been discovered via cross validation. Once the two models are obtained, they are used to predict on the original data sets to verify the model’s validity.
6. Representative results
From Eq. (6), the scenario of a classifier never getting the answer correct is
Table 6 shows representative SVM parameter values (from the Monte Carlo search) and results.
Table 6 shows that the best cross validation accuracy with an average prediction distance of 0.287 and a final model prediction distance of 0.056. Table 6 shows additional representative cross validation averages—D(Avg)—and final model prediction distances—D(final). Hundreds of runs resulted in cross validation prediction distances of <0.5. The best cross validation accuracy of.287 achieved thus far also has a fairly decent over-fit error rate of 0.056—which has a value of the objective function,
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1 | 3.929 | 9.732 | 19.160 | 24.860 | 1 | 3.723 | 0.287 | 0.056 | 21 |
2 | 2.640 | 87.825 | 32.867 | 81.832 | 1 | 2.945 | 0.342 | 0.025 | 22 |
3 | 2.860 | 10.022 | 85.200 | 50.843 | 2 | 8.033 | 0.374 | 0.075 | 18 |
4 | 0.964 | 85.719 | 71.740 | 33.237 | 2 | 9.259 | 0.396 | 0.125 | 19 |
5 | 7.709 | 2.587 | 28.705 | 26.903 | 2 | 2.347 | 0.413 | 0.050 | 20 |
6 | 2.207 | 75.920 | 52.493 | 36.102 | 2 | 8.994 | 0.438 | 0.125 | 18 |
7 | 6.783 | 18.035 | 49.974 | 30.441 | 2 | 6.985 | 0.456 | 0 | 21 |
Example 7 in Table 6 has an average cross validation accuracy of.456 with D(final)=0 (perfect prediction). Cross validation average accuracy or error rate is the more valid statistical claim. The best cross validation accuracy represented in Table 6 is in the same realm of accuracy as Netoff et al.’s intracranial methodology. Recall that Netoff et al. claim a specificity of 77.8% with no false positives, which is approximately a prediction distance of approximately.22 (
Figure 11 shows a plot of forewarning times (typically less than 1.5h) for the final-model of Example 7. The number of successive contiguous indicators to trigger forewarning was found to be 2 successive + values. Table 7 shows the Stage-1 predictions (Stage-3g of Figure 8 for all 60 patients) to produce the distribution of forewarning times in Figure 11. See Table 7 for the cutset indications (+ or -) that correspond to the parameters in Example 7 from Table 6.
In Figure 11, the solid black line is the occurrence frequency (arbitrary units) in half-hour bins. The blue line is the cumulative distribution of forewarning versus time. The red H-bar with the star in the middle indicates the mean value of the forewarning times (approximately 1 hour) and the sample standard deviation. The result in Example 7 of Table 6 is better than random guessing or biased heuristics with D(final)=0, despite poorer cross validation accuracy than other examples. This example shows most of the forewarning times of ≤1.5 hours with a statistically significant accuracy. One can visually make a prediction by scanning Table 7 from left to right and looking for 2 contiguous plus values. When 2 values are found, the seizure is highly likely to occur. One may be tempted to reduce the forewarn time by increasing the value of positive values that trigger a forewarning, but that would likely result in bad OTS error, which is why it is not the value found by the second and third stage SVMs.
7. Discussion
Ideally, we would like to achieve an average cross validation OTS prediction distance of zero, final model prediction distance of zero, and all forewarning times <1 hour. In order to achieve this goal, additional features will need to be explored that exploit topology and the distance metric that Takens’ theorem guarantees. Some modifications for Stage-2 improve the results (e.g., the choice of p cutsets prior to the event as a variable, and use of a RBF kernel instead of a linear one). More search parameters in Stage-1 (e.g., those in Table 3) should lead to better results with enough CPU time. Additional graph dissimilarity measures may be helpful. We have discovered more features for Stage-1 that may be of use. More data is needed for a robust statistical validation of the model.
The choice of optimal features is very difficult. Theorems guide the choice of parameters, features, and the algorithm. Some combination of theorem-based feature selection and occasional intuition derived from experimentation is the only way to keep the cost of the research initiative practical. Feature selection is one of many hard problems involved in epilepsy prediction. When one adds features, one often needs more data to make meaningful statistical assertions. Other important choices involve the type of kernel and the thresholding strategy. Linear kernels and thresholding strategies may perform well while Radial Basis Function (RBF) kernels perform poorly and vice versa. Our previous work [4] used a voting method that performed well. There is no guarantee that a set of features will behave similarly with different kernels and strategies to determine the threshold. Other measurement functions are possible under Takens’ theorem to create the phase-space states. Use of a single-class or multi-class SVM could also prove fruitful.
The results in Tables 6-7 and Figure 11 are encouraging, despite several limitations, which are discussed next. (1) We analyzed 60 datasets, 40 with epileptic events and 20 without events. Much more data (hundreds of datasets) are needed for strong statistical validation. (2) These data are from controlled clinical settings, rather than an uncontrolled (real-world) environment. (3) The results depend on careful adjustment of training parameters. (4) Only physician-selected portions of the EEG are available, rather than the full monitoring period. (5) The present approach uses retrospective analysis of archival data on a desktop computer. Real-world forewarning requires analyst-independent, prospective analysis of real-time data on a portable device. (6) The results give forewarning times of 4 hours or less. A time-to-event estimate is needed. (7) All EEG involved temporal lobe epilepsy; other kinds of epilepsy need to be included. (8) A prospective analysis of long-term continuous data is the acid test for any predictive approach. Prospective data were unavailable for the present analysis. Clearly, much work remains to address these issues.
8. Conclusions
The present work uses Support Vector Machine analysis to extend earlier work by Hively
Our non-invasive (scalp) EEG analysis resulted in cross validation error rates comparable to other invasive EEG approaches. Additional accuracy could be obtained by applying this methodology to specific patients on a per patient basis for custom EEG models if the data were available. Modifications could conceivably be made to the algorithm to improve the computational feasibility of per patient machine learning models. A research team could allow patients to start with group-based models that are less accurate while the patients collect and upload ambulatory data from their devices as they use them in real-world settings. Furthermore, businesses could be compensated for creating patient specific models from patients’ ambulatory data. Additionally, our algorithms have other applications as well, such as failure forewarning in machines [21] and bridges [22].
Acknowledgments
This manuscript has been authored by UT-Battelle, LLC, under contract DE-AC05-00OR22725 with the U.S. Department of Energy. The United States Government retains and the publisher, by accepting the article for publication, acknowledges that the United States Government retains a non-exclusive, paid-up, irrevocable, world-wide license to publish or reproduce the published form of this manuscript, or allow others to do so, for United States Government purposes.
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