- Research
- Open access
- Published:
Identifying the presence and severity of dementia by applying interpretable machine learning techniques on structured clinical records
BMC Medical Informatics and Decision Making volume 22, Article number: 271 (2022)
Abstract
Background
Dementia develops as cognitive abilities deteriorate, and early detection is critical for effective preventive interventions. However, mainstream diagnostic tests and screening tools, such as CAMCOG and MMSE, often fail to detect dementia accurately. Various graph-based or feature-dependent prediction and progression models have been proposed. Whenever these models exploit information in the patients’ Electronic Medical Records, they represent promising options to identify the presence and severity of dementia more precisely.
Methods
The methods presented in this paper aim to address two problems related to dementia: (a) Basic diagnosis: identifying the presence of dementia in individuals, and (b) Severity diagnosis: predicting the presence of dementia, as well as the severity of the disease. We formulate these two tasks as classification problems and address them using machine learning models based on random forests and decision tree, analysing structured clinical data from an elderly population cohort. We perform a hybrid data curation strategy in which a dementia expert is involved to verify that curation decisions are meaningful. We then employ the machine learning algorithms that classify individual episodes into a specific dementia class. Decision trees are also used for enhancing the explainability of decisions made by prediction models, allowing medical experts to identify the most crucial patient features and their threshold values for the classification of dementia.
Results
Our experiment results prove that baseline arithmetic or cognitive tests, along with demographic features, can predict dementia and its severity with high accuracy. In specific, our prediction models have reached an average f1-score of 0.93 and 0.81 for problems (a) and (b), respectively. Moreover, the decision trees produced for the two issues empower the interpretability of the prediction models.
Conclusions
This study proves that there can be an accurate estimation of the existence and severity of dementia disease by analysing various electronic medical record features and cognitive tests from the episodes of the elderly population. Moreover, a set of decision rules may comprise the building blocks for an efficient patient classification. Relevant clinical and screening test features (e.g. simple arithmetic or animal fluency tasks) represent precise predictors without calculating the scores of mainstream cognitive tests such as MMSE and CAMCOG. Such predictive model can identify not only meaningful features, but also justifications of classification. As a result, the predictive power of machine learning models over curated clinical data is proved, paving the path for a more accurate diagnosis of dementia.
Background
According to recent surveys, dementia is underdiagnosed. ICD codes alone cannot serve as a reliable gold standard for investigating the demographic characteristics or the clinical associations of the condition using electronic health records [1].
There is no single diagnostic test that can determine if a person has any form of dementia. However, clinicians employ various tools and tests to detect the presence of dementia, whether due to Alzheimer’s disease or some other cause. The Mini’ Mental State Examination (MMSE) is the most common test for measuring cognitive impairment [2]. Creavin et al. [3] attempt to determine the diagnostic accuracy of MMSE at various cut points for dementia in people aged 65 years and over. The authors conclude that MMSE contributes to a diagnosis of dementia in low prevalence settings. But this work also suggests that MMSE should not be used in isolation to confirm or exclude the disease. An alternative approach is to use the Clock Drawing Test (CDT) [4], which provides a simple scoring system for the rapid screening for cognitive impairment in patients with mild cognitive impairment [5].
More recently, a variety of automatic speech-based tools have also been used to detect dementia. These approaches usually employ machine learning classifiers trained with various vocal features, derived from recorded data resulting from standard spoken tasks provided to individuals [6, 7]. Automatic speech-based tools can also use lexical and conversation analysis-inspired features derived from transcripts of recorded data [8], in conversations led by neurologists or intelligent virtual agents. As another example, the CogAware tool [9] provides textual analysis for transcripts of individuals describing the “cookie theft” picture [10], in order to automatically detect whether they are originated from a patient with dementia or a cognitively normal individual.
A powerful but underutilised resource that could be employed to rapidly and automatically detect dementia is a patient’s electronic medical record (EMR). EMRs are increasingly available sources of information that contain large quantities of heterogeneous data. EMRs can include MR images of the brain that demonstrate cortical atrophy or comprise demographic and clinical information, as well as patient performance in cognitive tests. This information has been used to train machine learning models to detect the presence and severity of dementia [11,12,13]. Such models have also been used to assess the risk of converting to Dementia from a Mild Cognitive Impairment stage [14, 15].
Demographic and clinical information from EMRs has also been analysed by Shao et al. [1]; they utilise both structured and unstructured EMRs to define individual patients’ risk scores for dementia. The authors also combine structured data features, consisted of standard codes and medications from EMRs, with topic features, extracted from a topic modelling approach on free-text clinical notes. Finally, they employ a logistic regression model using the selected features as predictors. A similar retrospective study is combined by Ford et al. [16], using structured data including medical diagnoses, primary care tests and investigations, lifestyle information and prescribing data. Their survey compared various machine-learning models with baseline epidemiological approaches to identify undetected dementia in UK primary care patients and concludes that logistic regression and random forest algorithms allow for important features to be exposed and may be the best approaches for this prediction task.
In this paper, we examine whether the values of various features in electronic medical records can consistently decide the patient’s cognitive status, i.e. if the patient suffers from dementia and the level of its severity. This is realised in an automated way, by employing machine learning models that analyse a big dataset of EMRs, and validating the models’ effectiveness.
For this purpose, we employ EMRs that comprise structured information such as demographics, MMSE, and performance on the CAMCOG—a screening instrument for dementia. CAMCOG includes tests sensitive to different cognitive domains, and is part of the Cambridge Mental Disorders of the Elderly Examination (CAMDEX) [17]. CAMCOG has high levels of sensitivity and specificity when used to distinguish individuals with mild dementia from those who are cognitively intact. We analyse these data using a random forests model, providing an automatic classifier that effectively discriminates dementia patients from control individuals and estimates the severity of the disease for the former.
However, machine learning algorithms usually work as a black-box tool, without the ability to interpret individual predictions. Thus, an emerging challenge is to achieve the explainability of decisions taken by such models, in order to provide clinicians with the ability to understand the rationale of the model. Towards these directions, we employ decision tree models that are able to visualise a set of configurable rules for predictions made. Since MMSE and CAMCOG scores can directly provide an estimation of dementia severity, we decided to exclude those from the training of our decision trees, in order to investigate other interesting features that are clinically useful.
Methods
Problem statement
The problem addressed in this work is related to detecting the presence of a form of dementia in individuals based on a set of available demographic and psychometric features. A relevant extension of the problem above is accurately deciding the severity of the disease for patients with dementia. These two problems are formulated as follows:
-
1
Problem (a)—Predict Dementia, No Dementia: This problem addresses the issue of identifying if a patient has dementia or not in a specific episode (correctly diagnose dementia). In this task, we classify a patient-episode into “Dementia (1)” or “No-Dementia (0)”. We also identify relevant features for the classification decision.
-
2
Problem (b)—Predict No Dementia, Minimal or Mild Dementia, and Moderate or Severe Dementia: We further refine the previous problem to have a better understanding of the severity of dementia. We classify dementia patients into two more classes, “Minimal or Mild” and “Moderate or Severe”. We discover the important features behind the classification decision.
Approach
Our approach initially demands a data cleaning and curation process. Since all real-world clinical datasets contain a big amount of noise and missing values, we need to define a set of general rules, in order to be able to complete missing features and ignore features that are sparse. This process includes the filling of stable parameters throughout the patient’s lifetime, such as height, and removing parameters where the majority of values in patient episodes are meaningless (e.g. ‘not known’ or ‘not asked’).
The problems previously defined are formulated as simple classification tasks, addressed by machine learning models. These models’ algorithms are based on a supervised learning Decision Tree (DT) method to make the decisions easily interpretable by clinicians. They predict the class of patients by inferring decision rules from training data features.
A decision tree is composed of nodes and leaves. A node represents a dichotomous threshold for the value of some feature in the dataset (a.k.a. decision threshold). A leaf represents a patient subgroup in whom the likelihood of belonging to the positive class (in this case, developing dementia) cannot be refined by any additional dichotomous test. Nodes and leaves are connected by branches, each of which represents an additional condition; any path through the decision tree represents the outcome of a series of conditional statements.
To better understand the concept of decision trees, consider the example tree in Fig. 1. In this tree, the goal is to decide whether an individual has some form of dementia or not (binary classification). As we can see, each intermediate node entails a discriminating feature and a threshold. Based on the value of this feature, a clinician must follow the appropriate branch, until reaching a leaf node. Leaf nodes conclude to a decision (“Dementia” / “No Dementia”), based on the majority of cases in the training sample. To make our trees more informative and self-explainable, we have visualized the percentages in pie charts, the size of which depends on the number of cases falling in this leaf node. It is also used to find the class probability, which is the fraction of the same class in a leaf.
Predictive models
Our objective is to predict the classification of dementia patients as described in the problem statement, based on various patient record parameters provided as features in machine learning-based predictive models. We utilize the random forest algorithm for class prediction and the local interpretable model-agnostic explanations (LIME) [18] for explaining the model decision for any patient-episode. As a last step, we train a decision tree classifier, feeding important data features obtained by the random forest classifier model.
A random forest algorithm is an ensemble learning method that generates different decision trees. The decision of an algorithm averages the results provided by different decision trees. Individual decision trees usually have high variance and are prone to overfitting. Therefore, to control overfitting, decision trees are trained on different sub-samples of the dataset instances. A random forest model does not provide an explanation for each individual test instance classification. However, it gives a list of global important features based on the complete sample of the training data considering impurity. To determine the importance of a feature, the random forest model measures how much this feature impacts the total reduction of the classification criterion, i.e. how discriminating this feature is for the data instances to candidate classes. The greater the number, the more important the feature.
In contrary, LIME provides a local explanation of the prediction for each instance of the complete sample of the test data. LIME utilizes local surrogate models to explain the black-box behaviour of the machine learning model and its prediction. In terms of weight, LIME calculates each feature contribution for the predicted class of a test instance. As a result, the contribution or weight of each feature may vary depending on the test instance (local explainability of the prediction). The relevance of the feature is reflected on its weight. The weight’s importance can be interpreted by applying this to the prediction probability of a predicted class (Figs. 2, 3).
Experiments
Dataset
In our experiments, we employ clinical data from the OPTIMA (Oxford Project to Investigate Memory and Ageing) [19,20,21] dataset. The OPTIMA project was a long-term cohort study (1988–2008) of ageing and dementia that included persons over 70 with normal or minimally impaired cognition and studied their physical, metabolic, imaging, clinical, and cognitive indices until death.
The OPTIMA dataset comprises 1035 different patients with 9584 episodes and their features documented. The collection also includes unique patient identifiers; they, when combined with episode dates, uniquely identify each assessment of a patient’s status. Each episode has 1593 distinct features. The features are derived from various sources of information, including demographic characteristics, YES/NO questions related to health and well-being, rating scales, medical history, physical examinations, neuropsychological assessments, and performance of cognitive tests. As will be concluded, only a subset of these features will be important for the prediction tasks.
An important issue in OPTIMA dataset, is that 62% of the values are missing. This occurs due to a variety of reasons. For example, clinicians may note down only the most relevant feature values about a patient’s current condition and neglect others. They may also ignore some repeated feature across episodes, such as demographics and prolonging comorbidities (diabetes or hypertension). Based on this, we devise pre-processing and cleaning techniques able to curate missing values based on the supervision of our clinicians.
Determining classes for the predictive model
The predictive models are trained on patient-episode data (a.k.a. data instance). We note that there are substantial differences between each patient’s different episode features. In specific, our models use two kinds of features that change between episodes as follows:
-
Demographic (e.g. age or weight) or clinical features (e.g. comorbidities). The majority of these values usually change between two episodes (especially for long time intervals).
-
Cognitive examinations or memory and arithmetic tests (e.g. RECALLS OBJECTS, SUBTRACTS MONEY), taken by patients in each episode with the supervision of a clinician. Resulting values can be much different even in consecutive episodes, as the cognitive state of the individual deteriorates.
As a result, we avoid the potential information leakage introduced when the same episode or patient episodes with the same values could be part of both training and test data.
There are no direct features to suggest if a patient episode is labelled as “Dementia” or “No Dementia”. Therefore, supported by our clinicians, we define our ground truth, and label each data instance based on the features with values illustrated in Tables 1, 2, and 3. Features and values in Tables 1, 2 are used to identify if a patient episode falls under the “Dementia” or “No Dementia” classes, respectively. In addition, 3385 episodes are dropped because all their values are NULL, None or Unknown in the class determining features ( in Tables 1, 2, and 3). Moreover, a patient-episode is labelled as “Dementia”, if and only if, any other episode of the same patient is labelled as dementia, according to the criteria of the ground truth. Therefore, all the patient’s episodes fall into one of two categories: “Dementia” or “No Dementia”. Features and values in Table 3 are used to label a data instance with the value of the dementia severity (Minimal, Mild, Moderate, Severe). In case of several labels, the one representing the higher severity is considered.
Data cleaning and pre-processing
Various related works examined in [22] show that features related to demographics (e.g. age, gender and education), health (e.g. BMI, diabetes, depression, high cholesterol, and traumatic brain injury), and lifestyle factors (e.g. smoking, alcohol, physical activity, cognitive activity, and fish intake) are essential in the diagnosis of dementia. We identify 242 such features in the OPTIMA dataset. Applying the curation rules suggested by our clinicians, we are able to complete a few of the missing values on some features. This can be done by adding values implicitly provided by other closely related features. Curated features include “Petersen MCI”, “Depressive Illness”, “Cerebro Vascular Disease Present”, and “Anxiety/Phobic”. For example, our clinical experts can first identify closely related features for the “Depressive Illness” feature (with possible values: “absent” and “present”); these features include “Severity of depression”, “Feeling depressed”, “Depressed mood” and “Depression/Dysphoria: Severity”). The missing values of the ‘Depressive Illness” feature, are filled by taking into account values of the related features. For example, “Mild” or “Moderate” from “Depression/Dysphoria: Severity” entails the value “present” in “Depressive Illness”. Using these curation rules, around 70% of the missing values are completed.
The OPTIMA dataset feature-guide is included in the Additional file 5: Table S1 in supplementary information section. It is used to identify meaningless values in the data features. It consists of feature labels, their descriptions (data types and format of features), including the range of numerical features and categories of categorical features. We replace all such meaningless values with missing values (NULL). For example, “IDENTIFIES YEAR” feature should have ‘YES’ and ‘NO’ values only, so all other cases are considered as missing values.
As data sparsity can cause improper learning to the models, we decided to drop some dataset episodes and features, according to the number of missing values. An episode is removed if at least 50% of the feature values are missing. On the other hand, a full feature is removed if at least 5% of the episodes have missing values in this feature. Those percentages were chosen after experimentation with different thresholds, as they exhibited the best performance possible. This whole procedure leaves our models with the features mentioned in Table 4 for Problem (a) and Problem (b). Further, during pre-processing, categorical features are transformed into one-hot encoding. After the curation process, we end up with 3579 data instances (episodes) to perform experiments for Problem (a) and Problem (b).
Model training and feature selection
We employ a random forest classifier to train our predictive models with the default parameters of sklearn library,Footnote 1 except for the maximum depth of the tree, which is set to 5. A random forest model utilises a stratified shuffle split cross-validator which splits data into 5 folds of train and test set with reshuffling. Each fold preserves the percentage of samples for each class. After each fold, we record 50 most impurity-based important features from the model training and store into a set to have a distinct feature list. These important features are utilised to train a decision tree classification model to enhance interpretability of the random forest model outcomes. A maximum depth of 5 is used to generate generalised decision trees without overfitting.
Following a most common approach as per the empirical study, we choose the split ratio (70:30) between the training and testing set and utilise a stratified method to preserve class frequencies in both sets. Both problems represent the same experimental settings. In Problem (a), the “No Dementia” and “Dementia” classes contain 1829 and 1750 episodes, respectively, while, in Problem (b), the “No Dementia”, “Minimal or Mild dementia”, and “Moderate or Severe dementia” classes have 1829, 1281, and 469 episodes, respectively. The population size of dataset (Train:Test) in both problems are equal to 3579 (2505:1074) patient episodes.
Tables 5, 6, 7, 8, 9 and Table 10 report the results of Problem (a) and Problem (b), respectively, using the random forest and decision tree algorithms.
Evaluation Metrics We measure the performance of the predictive models in terms of precision, recall, and f1-score. In Problem (a), precision is the ratio of correctly predicted patients in the “Dementia” class to the total patients predicated as dementia. Alternatively, recall represents the ratio between the number of patients correctly predicted in the “Dementia” class to all patients in the “Dementia” class. Lastly, f1-score is the harmonic mean of precision and recall. The same metrics are also utilised for the classification of patients into the “No Dementia” class. We do not take accuracy (ratio between total correctly predicted patients to the total patients) into the account, as it is the least significant compared to the f1-score. We use the same metrics for Problem (b).
Results
The random forest predictive model’s performance is measured after each fold in terms of macro-averaged precision, recall, and f1-score of each class. We represent the results of the random forest models in Tables 5 and 7 for Problem (a) and Problem (b) considering patient episodes as data instances into the training and testing set.
In order to validate that the considering several episodes of the same patient does not induce overfitting, the models are also trained and validated at patient-level. In the patient-level setting, each patient record that includes all his/her episodes is included either in the training or testing sets but, not in both.
Tables 6 and 8 report on the results for Problem (a) and Problem (b) respectively for patient-level setting. The performance of the predictive models is very similar at patient-episode and patient-level setting. This suggests that treating each patient’s episode as a data instance does not introduce overfitting into the models.
Moreover, we also show the results of the decision tree models for the two problems in Tables 9 and 10, respectively. The decision tree predictive model for Problem (a) provides similar results for both classes. The decision tree predictive model for Problem (b) accomplishes better results for “No Dementia” and “Minimal or Mild dementia” classes, compared to “Moderate or Severe dementia” classes. The outcomes reported in Tables 9 and 10 suggest that Problem (b) is more complex to solve than Problem (a). The complexity is introduced because the “Dementia” class is divided into the classes “Minimal or Mild” and “Moderate or Severe” dementia classes for Problem (b), which causes a high imbalance between the three classes.
Baseline Results We built our own baseline to compare the findings of our model. Our proposed methodology comprises the following cleaning and preprocessing steps:
-
1
Imputing missing values, computed from meaningless values and based on curation rules provided by the clinicians.
-
2
Selection of relevant features, guided by clinicians’ recommendations.
-
3
Identifying and replacing corrupted and meaningless values in features with null values, as well as removing problematic features.
-
4
One-hot encoding of categorical features for better explainability for the models
We define our baseline as a plain classification model that does not include these steps. The dataset for this model consists of 4536 episodes for training (70%) and testing(30%) for Problem (a) and Problem(b) using decision tree model. Results of the baseline model for the two problems are presented in Tables 11 and 12, respectively. We find no significant differences in precision, recall, or f1-score. However, there are differences in the decision trees generated by our baseline and our proposed model. In the supplementary information section, we provide the baseline decision trees in files (Additional file 3: Figure S3 and Additional file 4: Figure S4). The decision trees differ both in appearing features and in decision thresholds of certain features that cannot be interpretable. For Problem (a), out of nineteen features, the following three have non-interpretable decision thresholds:
-
HANDED: Decision threshold=5 (in two nodes)
-
WRITES A SENTENCE: Decision threshold=5
As can be observed in the OPTIMA feature guide, the “HANDED” feature is categorical with values 1, 2, 3, 8, 9, reflecting the handwriting capability of the person. Values 8 and 9 represent ’NotKnown’ and ’NotAsked’ respectively; according to our curation rules, they are considered meaningless. On the other hand, the “WRITES A SENTENCE” feature is binary. In none of these cases, the decision threshold value is interpretable, with respect to the meaning of the feature.
Similarly, in the baseline model decision tree for Problem (b), out of twenty-five features, the following four binary ones have non-interpretable decision thresholds:
-
KNOWS RECENT NEWS ITEM: Decision threshold=5
-
RECALLS OBJECTS 1 APPLE: Decision threshold=6
-
COGNITIVE IMPAIRMENT: Decision threshold=5
-
CERBRO-VASCULAR DISEASE PRESENT: Decision threshold=5
The aforementioned unmeaningful decision boundaries for both problems, appear as a result of the large amount of noise and missing values in the OPTIMA dataset for many important features. Contrary, in the decision trees of our model where data have been curated according to the preprocessing steps 1–4, none of the decision thresholds suffers from this problem. In all cases, the decision thresholds are meaningful, since all decisions taken are based on the different categories of each feature range of values.
Interpretation of results
The resulting Decision Trees for Problems (a) and (b) are provided in Figs. 1 and 4, respectively.
The decision tree of Fig. 1, first separates the group into two main groups based on the strength of their verbal recall. Group one (n = 1370) (Fig. 3) recalled two or more of the six items (e.g. a shoe, a typewriter, a set of scales, a suitcase, a barometer, and a lamp), pictures of which they were asked to name and remember at the beginning of the CAMCOG.
Group two (n = 1135) (Fig. 2) recalled one or zero of these items. Not surprisingly, a large majority (around 90%) of the latter group are judged to suffer from dementia, while in the former the dementia diagnosis rate is only 16%. These distributions can be refined slightly by comparing the outcomes in groups based on other aspects of the assessment. For instance, the probability of dementia in a member of group two is much lower (40%), if the patient is aware of any recent news item and generates thirteen or more items in the ‘animal fluency’ task. Such patients would have had an isolated memory impairment that did not impair their independence, and would, therefore, probably have met the criteria for amnestic mild cognitive impairment (MCI). However, patients of group two may fall into a pure Dementia class by following the specific rules defined in paths A or B, illustrated in the decision tree 1. Patients in path A were not oriented to time and were not aware of any recent news item, while also not recalling basic recent public figures like the prime minister. Patients in path B were also not aware of any recent news item, but were oriented to time. However, although being less than 85 at the time of the episode, they seem unable to recall very recent information (in specific, all five elements of an address that they were asked to put on an envelope a few minutes ago).
Similarly, those in group one, who generated less than 13 items on animal fluency and failed a mental arithmetic task, had a 95% chance of suffering from dementia. Contrary, the dementia risk was around 45% in those who generated less than 13 animals, but passed mental arithmetic. The patients in group one, who had the lowest risk (5%) of dementia, were those who generated 13 or more animals and were basically oriented to time and place (identifying the current year, their country and streets). They were also aware of recent news items, as can be seen following path C.
In the decision tree of Fig. 4, the outcome of the classification is changed, such that, diagnoses of dementia are divided into those with minimal or mild dementia, and those with moderate to severe manifestations of the condition. As can be observed, the large majority of the moderate to severe cases are among the 1128 participants on the left tree branch (Fig. 5), scoring less than two on the verbal recall feature (A sub-test of the CAMCOG). However, the risk of severe dementia in these individuals ranges from 5% in those who list four or more animals and are aware of any recent news item, to 87% when three or fewer animals are generated and the town that they are in cannot be recalled.
For patients of the former group, path B rules lead to the highest possibility of minimal or mild dementia. For patients of the latter group, an absolute probability of moderate or severe dementia is provided if they are not able to recognise simple object such as an apple and cannot identify similarities for at least two kinds of fruits, as shown in path A.
Likewise, almost all cases of severe dementia in the group with better verbal recall (two or more items) occur in patients who fail a basic mental arithmetic task. Conversely, the group (Fig. 6) who are at least risk (less than 5%) of dementia of any degree are those with both accurate mental arithmetic and good verbal fluency (13 or more animals generated), as well as orientation (able to recall their address and identify their country and basic streets), as can be seen following path C.
Model explanation
To understand the machine learning model’s black-box behaviour, we perform local model interpretation over our random forest model using LIME (Local Interpretable Model-Agnostic Explanations) [18]. We also make use of a decision tree classifier model for explaining the reasons behind our predictions. Here, we consider two examples from each problem’s testing set to understand the decisions of our random forest model.
Figures 7, 8, 9, and 10 depict the contribution of the top 10 features for predicting the class for the respective problems for a test instance. LIME calculates the contribution of each feature for the predicted class of the test instance in terms of weight. We only show top 10 features based on their weights in Figs. 7, 8, 9, and 10. The weight of the feature represents its importance. The left parts of the figures show the weights of the top 10 important features, while making class decisions, whereas the right parts of the figures represent the probabilities of the different classes, the names of the top 10 features and their values in the test instance. The weight’s importance can be interpreted by applying this to the prediction probabilities.
For example, in the right part of Fig. 10, features in green colours support the “Moderate or Severe” class and features in other colours support “No Dementia” and “Minimal or Mild dementia” classes. The left part of Fig. 10 measures the impact of these features in terms of weight while deciding for “NOT Moderate-Severe Dementia” (thus, “No-Dementia” or “Minimal or Mild Dementia”) and “Moderate-Severe Dementia”. If the features ‘NUMBER OF ANIMALS LISTED’ and ‘IDENTIFIES DATE’ are removed, the classifier should be able to predict class ’Moderate-Severe Dementia’ with a probability of \(0.97-0.04-0.02 = 0.91\).
Discussion
The biology and pathophysiology of dementia and its many underlying causes (e.g. Alzheimer’s disease that is the most common, at least in later life) are diverse and subject to the influence of different factors (e.g. comorbidity, lifestyle, and genetics). They demand individualised and precise treatment to differentiate the conditions of each dementia patient. The approach described in this paper has shown the unpredictability that derives from a complex interplay of factors impacts on the accuracy and efficiency of diagnosis. This complexity could be addressed using automated models based on machine learning, resulting in better performance of existing diagnostic tools.
Similar works also employ machine learning techniques aiming to address the most basic problem: predicting various dementias and/or detect probable dementia cases among undiagnosed patients analysing structured data features (prescribed medications, comorbidities etc.) from EMRs [16, 23] or even unstructured clinical notes [1]. Our study mainly differs in the variety, size, and granularity of the predictors utilized. In specific, we combine a huge set of demographic and clinical features with baseline arithmetic or memory tests, provided in the OPTIMA dataset. The most important of those predictors can be further used to produce a set of simple rules in the context of a decision tree, in order to assist a clinician in decision-making during the diagnostic process. These rules involve basic parameters (e.g. age) and simple cognitive tests (e.g. ‘Identifies date’) that can be easily applied by a medical expert to receive a prediction for an individual patient with a certain confidence. Visual models as such can assist in making our results interpretable by the experts, in contrast to decisions made by black-box machine learning tools. Moreover, our study applies the same approach to address a more advanced multi-class problem: detecting the presence and the severity level of dementia in the same patient cohort. This problem is also effectively addressed using a random forest model, and a similar set of simple rules is provided via a second decision tree.
Since the OPTIMA dataset is based on the London population, location and time have a substantial impact on numerous features like “Remembers Lindbergh”, “Recognise Picture Barometer”, “Remembers WW II Date”, and “Knows Prime Minister”. These features should alter in name depending on the location and time, but the essence of each feature will remain the same. In the United States, for example, “Knows Prime Minister” feature should be translated to “Knows President” (i.e. recognizing the most powerful political position). As a result, our models aid the recognition of features based on inherent nature, but they must be retrained for new locations and periods.
Improvements in the diagnostic process will significantly enhance a clinician’s ability to offer the management plan most appropriate to an individual patient, both at present and when disease-modifying treatments become available for sporadic neurodegenerative dementia. To be given a diagnosis of any untreatable condition is a life-changing event. When the condition is neurodegenerative dementia, patients need to make changes to their current lives and future plans, to consider legal rights appropriate to their future selves, and if possible, maximise the utility of their residual cognitive resources. While the disease remains untreatable, there are negative as well as positive aspects to early diagnosis, and where accuracy is concerned, it is more important to avoid false-positive than false-negative diagnoses. However, the advent of disease-modifying treatments will change this: identifying a neurodegenerative condition as early as possible in the course of its evolution will limit the damage already done and therefore improve the outcome of treatment. At the same time, it will become as important not to miss a true positive as to misclassify a true negative.
Once diagnosed, a patient with Alzheimer’s disease needs to be kept under regular clinical assessment. Whether conducted in the context of primary care or a specialist clinic, ongoing assessment aims to ensure that the patient’s social and medical needs (including the choice and dose of symptomatic treatments) are optimally aligned with their cognitive abilities. Because current methods of assessment are both time-consuming and prone to inaccuracy and error, an a priori estimate of the likely trajectory of decline would alert the clinician to any anomalous results, and therefore, ensure that the best decisions are always made at the most appropriate time.
Conclusions and future directions
This paper presented automated prediction models for detecting the presence of dementia in the Electronic Medical Records of patients of a large ageing study, based on psychometric tests and demographic factors. Our study focused both on the accuracy, by employing different machine learning techniques, and interpretability, by visualising resulting models with the method of decision trees. The decision trees produced identified the most discriminating—and thus important—features for dementia detection, as well as for the disease severity classification. Cognitive test features seem to be the most relevant, including various memory (e.g. recollection of objects) and arithmetic (e.g. subtraction of money) tasks that patients have been asked to take, with their performance determining the sub-group in which they fall with certain probability. Sub-groups define either a specific severity level of the disease or a non-dementia condition (e.g. patients with MCI). The predictive models assist the clinician in determining the order in which the most relevant questions should be addressed while assessing a patient’s cognitive abilities.
Our work aims at thoroughly investigating and highlighting key characteristics that yield the presence and severity of dementia and creating an accurate prediction tool. Moreover, the decision tree approach ignores mainstream cognitive tests such as MMSE and CAMCOG, employed in most of the related work, in order to focus on simple rules, represented by simple arithmetic and memory tasks. Such a rule-based tool can easily assist clinicians in the early detection of dementia in primary care. To adopt this approach, the end-user of this tool would only have to assign the tasks depicted in the decision trees to her patients, in order to assess their condition with a certain confidence (based on the proportion of each sub-group in the tree). Thus, we hope that these results and tool can represent building blocks for individualised clinical decisions (Additional file 1 and 2: Figures S1 and S2).
As for future challenges, we plan to validate the proposed prediction models, including random forests and interpretable decision trees, in other patient cohorts. An extensive evaluation across different populations would ensure the current approach does not suffer from a lack of scientific validity. More importantly, an extensive assessment will provide empirical proof of the generality of the properties of the proposed methods.
Availability of data and materials
Code is available on www.github.com/SDM-TIB/dementia_detection.git. The data that support the findings of this study were provided from the Oxford Project to Investigate Memory and Ageing (OPTIMA) via a bilateral agreement with the IASIS project and cannot be publicly shared.
Abbreviations
- BMI:
-
Body mass index
- CAMCOG:
-
Cambridge Cognition Examination
- CAMDEX:
-
Cambridge Mental Disorders of the Elderly Examination
- CDT:
-
Clock Drawing Test
- DT:
-
Decision Tree
- EMR:
-
Electronic Medical Record
- ICD:
-
International Classification of Diseases
- LIME:
-
Local Interpretable Model-agnostic
- MCI:
-
Mild Cognitive Impairment
- OPTIMA:
-
Oxford Project to Investigate Memory and Ageing
- MMSE:
-
Mini-Mental State Examination
References
Shao Y, Zeng QT, Chen KK, Shutes-David A, Thielke SM, Tsuang DW. Detection of probable dementia cases in undiagnosed patients using structured and unstructured electronic health records. BMC Med Inform Decis Mak. 2019;19(1):128.
Arevalo-Rodriguez I, Smailagic N, i Figuls MR, Ciapponi A, Sanchez-Perez E, Giannakou A, Pedraza OL, Cosp XB, Cullum S. Mini-mental state examination (mmse) for the detection of Alzheimer’s disease and other dementias in people with mild cognitive impairment (mci). Cochrane Database Syst Rev 2015;3.
Creavin ST, Wisniewski S, Noel-Storr AH, Trevelyan CM, Hampton T, Rayment D, Thom VM, Nash KJ, Elhamoui H, Milligan R, et al. Mini-mental state examination (mmse) for the detection of dementia in clinically unevaluated people aged 65 and over in community and primary care populations. Cochrane Database Syst Rev 2016;1.
Borson S, Brush M, Gil E, Scanlan J, Vitaliano P, Chen J, Cashman J, Sta Maria MM, Barnhart R, Roques J. The clock drawing test: utility for dementia detection in multiethnic elders. J Gerontol Ser A Biomed Sci Med Sci. 1999;54(11):534–40.
Rakusa M, Jensterle J, Mlakar J. Clock drawing test: a simple scoring system for the accurate screening of cognitive impairment in patients with mild cognitive impairment and dementia. Dement Geriatr Cogn Disord. 2018;45(5–6):326–34.
Satt A, Sorin A, Toledo-Ronen O, Barkan O, Kompatsiaris I, Kokonozi A, Tsolaki M. Evaluation of speech-based protocol for detection of early-stage dementia. In: Interspeech, 2013:1692–1696
Satt A, Hoory R, König A, Aalten P, Robert PH. Speech-based automatic and robust detection of very early dementia. In: Fifteenth annual conference of the International Speech Communication Association 2014.
Mirheidari B, Blackburn D, Walker T, Reuber M, Christensen H. Dementia detection using automatic analysis of conversations. Comput Speech Lang. 2019;53:65–79.
Rentoumi V, Paliouras G, Danasi E, Arfani D, Fragkopoulou K, Varlokosta S, Papadatos S. Automatic detection of linguistic indicators as a means of early detection of alzheimer’s disease and of related dementias: a computational linguistics analysis. In: 2017 8th IEEE international conference on cognitive infocommunications (CogInfoCom), 2017;000033–000038. IEEE
Goodglass H, Kaplan E, Barresi B. Boston diagnostic aphasia examination record booklet. Philadelphia: Lippincott Williams & Wilkins; 2001.
Möller C, Pijnenburg YA, van der Flier WM, Versteeg A, Tijms B, de Munck JC, Hafkemeijer A, Rombouts SA, van der Grond J, van Swieten J, et al. Alzheimer disease and behavioral variant frontotemporal dementia: automatic classification based on cortical atrophy for single-subject diagnosis. Radiology. 2016;279(3):838–48.
Shankle WR, Mani S, Dick MB, Pazzani MJ. Simple models for estimating dementia severity using machine learning. MedInfo 1998;98.
Vyas A, Aisopos F, Vidal M-E, Garrard P, Paliouras G. Calibrating mini-mental state examination scores to predict misdiagnosed dementia patients. Appl Sci. 2021;11(17):8055.
Grueso S, Viejo-Sobera R. Machine learning methods for predicting progression from mild cognitive impairment to Alzheimer’s disease dementia: a systematic review. Alzheimer’s Res Ther. 2021;13(1):1–29.
Katsimpras G, Aisopos F, Garrard P, Vidal M-E, Paliouras G. Improving early prediction of dementia progression using machine learning methods. ACM Trans Comput Healthc (HEALTH). 2022;3(3):1–16.
Ford E, Rooney P, Oliver S, Hoile R, Hurley P, Banerjee S, van Marwijk H, Cassell J. Identifying undetected dementia in UK primary care patients: a retrospective case–control study comparing machine-learning and standard epidemiological approaches. BMC Med Inform Decis Mak. 2019;19(1):248.
Huppert FA, Jorm AF, Brayne C, Girling DM, Barkley C, Beardsall L, Paykel ES. Psychometric properties of the camcog and its efficacy in the diagnosis of dementia. Aging Neuropsychol Cogn. 1996;3(3):201–14.
Ribeiro MT, Singh S, Guestrin C. “Why should I trust you?”: explaining the predictions of any classifier. CoRR 2016. arXiv:1602.04938
Clarke R, Smith AD, Jobst KA, Refsum H, Sutton L, Ueland PM. Folate, vitamin b12, and serum total homocysteine levels in confirmed Alzheimer disease. Arch Neurol. 1998;55(11):1449–55.
Budge M, De Jager C, Hogervorst E, Smith A. Oxford project to investigate memory and ageing (optima). Total plasma homocysteine, age, systolic blood pressure, and cognitive performance in older people. J Am Geriatr Soc. 2002;50(12):2014–8.
Oulhaj A, Wilcock GK, Smith AD, de Jager CA. Predicting the time of conversion to mci in the elderly: role of verbal expression and learning. Neurology. 2009;73(18):1436–42.
Warren-Gash C. Dementia risk prediction models what do policymakers need to know? Technical report, University of Cambridge (March 2019). https://www.phgfoundation.org/documents/dementia-risk-prediction-models.pdf
Nori VS, Hane CA, Crown WH, Au R, Burke WJ, Sanghavi DM, Bleicher P. Machine learning models to predict onset of dementia: a label learning approach. Alzheimer’s Dement Transl Res Clin Interv. 2019;5:918–25.
Acknowledgements
The authors would like to acknowledge the project IASIS’ consortium for their collaboration in this work.
Funding
Open Access funding enabled and organized by Projekt DEAL. This paper is supported by European Union’s Horizon 2020 research and innovation programme under Grant Agreement No. 727658, Project IASIS (Integration and analysis of heterogeneous big data for precision medicine and suggested treatments for different types of patients). The principal grant support for OPTIMA over more than 20 years has come from Bristol-Myers Squibb, Merck & Co. Inc., Medical Research Council, Charles Wolfson Charitable Trust, Alzheimer’s Research UK, Norman Collisson Foundation and the NIHR Oxford Biomedical Research Centre. Maria-Esther Vidal is partially supported by the Leibniz Association in the program “Leibniz Best Minds: Programme for Women Professors”, project TrustKG-Transforming Data in Trustable Insights with grant P99/2020.
Author information
Authors and Affiliations
Contributions
All the authors defined the problems addressed in this paper. FA, AV, and M-EV devised the solution. AV implemented the machine learning models and executed all the experiments. PG analysed and explained the results from the clinical perspective. Lastly, all the authors contributed to writing and editing the manuscript; they also read and approved the final manuscript.
Corresponding author
Ethics declarations
Ethics approval and consent to participate
OPTIMA offered permission to the authors of this article to use the OPTIMA dataset that aided our research. The OPTIMA study’s ethics guidelines are followed when collecting data from participants. With the approval of all participants, the dataset was created, processed and shared by OPTIMA. The research work reported in this article has been conducted in compliance with the relevant guidelines and regulations of both OPTIMA and BMC journal.
Consent for publication
Not applicable.
Competing interests
The authors declare that they have no competing interests.
Additional information
Publisher’s Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Supplementary information
Additional file 1: Figure S1.
The decision tree predicts the dementia classes ("Dementia"/"No Dementia") of 2505 patients for the Problem (a). This figure file provides high resolution for better visibility.
Additional file 2: Figure S2.
The decision tree predicts the dementia classes ("No Dementia"/"Minimal or Mild Dementia"/"Moderate or Severe Dementia") of 2505 patients for the Problem (b). This figure file provides high resolution for better visibility.
Additional file 3: Figure S3.
Decision Tree predicts the dementia classes ("Dementia"/"No Dementia") for the Problem (a) using baseline method. The decision trees differ in appearance as well as decision thresholds for certain non-interpretable attributes
Additional file 4: Figure S4.
Decision Tree predicts the dementia classes ("No Dementia"/"Minimal or Mild Dementia"/"Moderate or Severe Dementia") for the Problem (b) using baseline method. The decision trees differ in appearance as well as decision thresholds for certain non-interpretable attributes
Additional file 5: Table S1.
Optima dataset feature guide in excel format
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.
About this article
Cite this article
Vyas, A., Aisopos, F., Vidal, ME. et al. Identifying the presence and severity of dementia by applying interpretable machine learning techniques on structured clinical records. BMC Med Inform Decis Mak 22, 271 (2022). https://doi.org/10.1186/s12911-022-02004-3
Received:
Accepted:
Published:
DOI: https://doi.org/10.1186/s12911-022-02004-3