Open-access Early Detection and Monitoring of Cancer Chemotherapy-Related Left Ventricular Dysfunction by Imaging Methods

Keywords: Neoplasms/mortality; Antineoplastic Agents/adverse effects; Ventricular Dysfunction, Left/diagnostic imaging; Anthracyclines/adverse effects; Trastuzumab/radiation effects

Introduction

Cancer has been the second leading cause of death in Brazil since 2006, and it is predicted to surpass cardiovascular disease (CVD) as the leading cause of death between 2020 and 2025.1 Cancer and CVD have risk factors in common, such as obesity, sedentarism, arterial hypertension, tobacco use, diabetes mellitus, advanced age, and dietary pattern. The co-prevalence of cancer and CVD is therefore elevated. The diagnosis and prevention of both diseases may be carried out in an integrated manner.2 Oncological treatment with chemotherapy (CT) has led to an increase in survival, but it has also led to the risk of cardiotoxicity (CTX), the incidence of asymptomatic ventricular dysfunction or even cardiomyopathy.3 Early diagnosis of CTX is important, given that the sooner this myocardial event is diagnosed, the higher the chances of recovering systolic function.4

The objective of monitoring left ventricular (LV) function during cancer treatment is to detect cardiac dysfunction during the subclinical phase, rather than when a symptomatic patient already has reduced ejection fraction. The groups of chemotherapeutic medications that most frequently cause myocardial aggression are anthracyclines (ANT), widely used in the treatment of solid tumors and hematological malignancies, and monoclonal antibodies, the typical example of which is trastuzumab (TZU).5,6 The CTX of ANT was initially described as dose-cumulative, irreversible, and caused by mitochondrial injury. In contrast, TZU-related CTX, which is not dose dependent, is irreversible and does not cause mitochondrial injury. In both aggressions, however, the possibility of reverse remodeling and recovery of ventricular function has been reported. Case series of patients undergoing treatment with ANT reported an incidence of 15% to 17% of some degree of decrease in LV ejection fraction (LVEF), calculated by Simpson's method, and 2% to 3% of severe heart failure (HF).7 More recent case series, however, have related lower incidences.

There are different definitions used for the diagnosis of ventricular dysfunction related to cancer treatment, which are extrapolated from diverse clinical situations and which have little specific validation. Currently, one of the most used definitions is as a decrease in LVEF of more than 10% of the baseline value, to values below the cutoff of 53%, with or without symptoms, it being necessary to repeat the exam 2 or 3 weeks after the initial measurement.8 According to Zamorano et al.9 this lower limit for LVEF normality is 50%, also with a 10% reduction. Other definitions quantify a decrease in LVEF of more than 10% to LVEF below 55%, in asymptomatic patients, or a decrease of more than 5% to LVEF below 55% in symptomatic patients.10 Initially, endomyocardial biopsy was the gold standard used for cardiotoxicity, but its invasive character and risk of complications led to its progressive replacement by imaging methods. Various techniques have been proposed as tools for diagnosis and prognosis of CTX associated with CT, with emphasis on serum biomarkers, conventional echocardiography, two-dimensional strain echocardiography, radionuclide ventriculography (RNV), and cardiac magnetic resonance imaging (CMRI). The objective of this review is to present clinicians with the main advantages and disadvantages of different imaging methods for diagnosing and monitoring chemotherapy-related left ventricular dysfunction, regarding critical analysis, accuracy, limitations, and clinical perspectives.

Methods

This review followed adaptations of the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) methodology principles. The bibliographic search included the databases MEDLINE, SciELO, and LILACS. The descriptors used were cardiotoxicity; left ventricular dysfunction; antineoplastics; anthracyclines; diagnostic techniques and procedures; echocardiography; Doppler echocardiography; two-dimensional/three-dimensional/contrast echocardiography; scintigraphy; nuclear medicine; computed tomography; magnetic resonance. The reference lists of the articles found in the electronic search were also consulted and relevant articles were, thus, identified. The objective was to answer the question which is the most appropriate imaging method for the early detection of ventricular dysfunction in patients submitted to cancer CT within the context of clinical practice. Two independent researchers independently analyzed all abstracts. The review considered original articles with the following study designs: clinical trial, cohort, case-control, meta-analysis, and reviews that had expert consensus; considering articles published in the period between January 1998 and June 2017, whose full texts were available in English, Spanish, or Portuguese. The studies were selected in accordance with the following criteria: (a) the underlying disease was cancer, with a diagnosis confirmed by histopathology; (b) treatment included CT with ANT, TZU, or other known myocardial depressants; and (c) diagnostic methods such as echocardiography, computed tomography, nuclear medicine, or magnetic resonance imaging were used. The following were excluded: case reports, articles with other types of oncological therapy, and duplicate articles. Two hundred and twenty-one abstracts in the databases fulfilled the search criteria, and 162 articles were excluded.

Hereafter, we will critically analyze each of the methods, highlighting their advantages, disadvantages, and clinical applicability regarding the detection of CT-induced CTX. A summary of this analysis is given in Table 1.

Table 1
Advantages, disadvantages, and applicability of imaging methods for detecting chemotherapy-related cardiotoxicity

Two-dimensional echocardiography

Two-dimensional echocardiography (2D ECHO) with Doppler is the method most frequently used before, during, and after CT, given that it is not invasive; it does not use ionizing radiation; it is highly available and cost-effective. It evaluates systolic and diastolic function, cardiac valves, and the pericardium, thus offering an analysis of diverse manifestations of CTX.11 The quantification of LVEF is the most accepted for measuring LV systolic function, and it is an important parameter in the algorithm for monitoring CT-induced CTX, capable of diagnosis and prognosis of clinical results, supporting the decision to continue or stop antineoplastic therapy.8 It is important that this measure be accurate, with minimal temporal variability. However, LVEF measured by 2D ECHO has an elevated temporal variability, approximately 10% [9,1%-11,8%], and in order to be able to detect a 10% alteration in LVEF safely, the measure should have a lower temporal variability. It is thus possible to affirm that LVEF measured by 2D ECHO is less reliable.12

Reduced LVEF following CT is considered a late finding that may indicate irreversible myocardial aggression and impede evolution with adequate therapy. Diastolic dysfunction may precede and predict late systolic dysfunction; however, no parameter of diastolic function has definitively shown to be predictive of CTX, and the studies are conflicting.13-17

The right ventricle (RV) is commonly affected by CT, in an early manner, with a higher number of affected segments than the LV, predominantly in the interventricular septum.18 Its routine evaluation should follow the recommendations set forth by Lang et al.19 In this manner, the quantification of RV systolic and diastolic function would be important for serial monitoring, but there is a significant technical difficulty which restricts its routine use in clinical practice.

In summary, a disadvantage of 2D ECHO is the elevated intra- and inter-examiner variability that compromises the method's reproducibility.

Three-dimensional echocardiography

Unlike 2D ECHO, the evaluation of LVEF volumes by 3D ECHO is not based on geometrical suppositions; it is not affected by shortened views,20 and it is quantified by an automated edge-tracking algorithm.21 Studies with CMRI have shown that evaluations of LVEF and LV volumes by 3D ECHO have better accuracy and reproducibility,22,23 as well as lower temporal variability for serial monitoring of LVEF.12

The study by Walker et al.23 evaluated the accuracy of measuring LVEF with 2D ECHO, RNV, and 3D ECHO with relation to CMRI, in patients who used Doxorubicin (DOX) and TZU. The left ventricle final diastolic volume (LVFDV) showed a modest correlation between 2D ECHO and CMRI (r = 0.64 baseline, r = 0.69 at 12 months); the correlation of LVFDV between 3D ECHO and CMRI was shown to be stronger (r = 0.87 baseline; r = 0.95 at 12 months); LVEF measured by 2D ECHO had a weak correlation with CMRI (r = 0.31 baseline, r = 0.42 at 12 months). Both 3D ECHO and RNV showed a strong correlation when comapred with CMRI (r = 0.91 baseline, r = 0.90 at 12 months). When compared with RNV, the serial measurement of LVEF via 3D ECHO was shown to be more viable, accurate, and reproducible for serial LVEF monitoring in these patients.

Echocardiography is the method of choice for serial evaluation of patients undergoing CT, considering availability, cost, and risk. Accurate LVEF calculation should be carried out with the best available method in the echocardiography laboratory, ideally 3D ECHO. In the event that 2D ECHO is used, Simpson's is the preferred method.8 When utilizing 2D ECHO, contrast should be associated to improve the accuracy and reproducibility of the measurements of LVEF and volumes.24

Myocardial two-dimensional strain echocardiography

Two-dimensional speckle tracking echocardiography (2D STE) is an accurate technique, which is easy to perform and which has good reproducibility. It measures myocardial deformation through strain and strain rate in the three spatial planes, i.e. longitudinal, circumferential, and radial. Left ventricular systolic global longitudinal strain (LVGLS) has an intra- and inter-observer variability of 4.9% to 8.6%, which is lower than the that of the measurement of LVEF.25 Its prognostic value is incremental to LVEF for the prediction of all-cause mortality in the general population.26 Strain and strain rate are attributed to have the capacity to detect subclinical LV dysfunction and cardiac dysfunction related to CT, especially with the use of ANT and TZU.

In the study by Charbonnel et al.,27 LVGLS measured before treatment and after low doses (150 mg/m2) of ANT was shown to be a predictor of alterations in LVEF 12 months after the initial dose; CTX occurred in 6 of the 86 patients (7.0%). Pre-CT evaluation of LVGLS was observed to have a predictor value with an area under the ROC curve of 0.76, with a predictor threshold of (-)19.95% for LVGLS; in the evaluation with low doses, LVGLS provided incremental predictive information on CTX with an area under the ROC curve of 0.82, for a predictor threshold of (-)17.45% for LVGLS.

The study by Mousavi et al.28 demonstrated that LVGLS was a strong predictor of symptomatic HF in pre-CT evaluation of patients undergoing CT with ANT. Age and LVGLS were also predictors of all-cause mortality. LVGLS greater than (-)16% was associated with a 4.7-fold increase in the occurrence of symptomatic HF.

Our cardio-oncology research group studied pre-CT LVGLS as a predictor of LV dysfunction and found data (yet to be published) similar to those of the above-cited authors.27,28

In 52 patients with breast cancer undergoing CT with ANT, who were studied 1 week before CT and after the complete cycle, a significant decrease in LVGLS occurred, which was not accompanied by a decrease of more than 10% in LVEF, which suggests that LVGLS is more sensitive than LVEF in detecting alterations in systolic function.17

In patients with non-Hodgkin's lymphoma, followed for 6 months, there was a significant reduction in LVGLS and an increase in cardiac troponin T (cTnT); LVEF, however, remained within reference values. When alterations in LVGLS and cTnT were included in the multivariate analysis, only the decrease in LVGLS between the baseline and the third cycle of CT was an independent predictor of CTX; there was, however, no long-term follow-up to determine the clinical relevance of these findings in predicting late cardiac events.29

Sawaya et al.30 followed 43 patients with breast cancer treated with ANT and TZU, performing 2D STE and measuring biomarkers at baseline and at 3 and 6 months. High-sensitivity cardiac troponin I (hsTnI) and LVGLS were early markers of subsequent decreases in LVEF. Patients who presented neither a decrease of more than 10% in LVGLS nor an elevation in hsTnI during the third month had a 3% probability of a decreased LVEF in the sixth month. Patients who had a decrease of more than 10% in LVGLS and/or an elevation in hsTnI presented a risk of CTX during the sixth month 9 times greater than those without either of these alterations. The authors infer that the presence of these markers does not mandate the suspension of CT but rather alerts that there is a necessity for closer cardiac monitoring, earlier initiation of “cardioprotective” measures, or the use of alternative, less cardiotoxic therapies.30

Sawaya et al.31 followed 81 patients treated with ANT, taxanes, and TZU, 26 of which developed CTX, 5 with symptoms of HF. LVGLS and hsTnI were predictors of CTX, and LVGLS greater than (-)19% was present in all of those who developed symptoms of HF.

According to Negishi et al.32 a relative reduction in LVGLS of more than 11%, with respect to the pre-CT exam, is the best predictor of CTX. In the absence of a pre-CT exam, LVGLS greater than (-)20,5% would also be a predictor of CTX, albeit, with a lower area under the ROC curve (0.67); they thus suggest using relative reduction rather than absolute value.

Forty-two patients with ANT and TZU regimes were followed for 12 months, and 10 of them developed CTX. LVGLS, left ventricular systolic global radial strain (GRS), and S' detected a pre-clinical reduction in the third month, and all 10 who developed CTX had a reduction in LVEF at 6 months.33

Even though there is a consensus regarding the need for cardiac function monitoring via non-invasive imaging after exposure to CT, the method to be utilized and the monitoring time have yet to be defined. Evidence suggests that a reduction in LVGLS precedes a decrease in LVEF; however, long-term follow-up is necessary to determine the clinical relevance of these findings.

Radionuclide ventriculography

RNV was the first scintigraphic method for serial evaluation of LVEF in patients undergoing CT.34,35 Its advantages include excellent accuracy, an estimated intra- and inter-variability of less than 5%, independence from LV geometry, and the possibility of being performed in patients with large body surfaces.36,37 Gated single-photon emission computed tomography (SPECT) has currently been used to measure LVEF; nevertheless, the American Society of Nuclear Cardiology recommends that serial monitoring be performed by RNV as a Class I indication, whereas the gated blood-pool SPECT technique is a Class IIb indication.36 Limitations to the routine use of nuclear imaging include patients with arrhythmias; incompleteness of information on the right ventricle, the atria, the valves, and the pericardium; repeated exposure to ionizing radiation; and higher costs compared to echocardiography. In 2016, the American Society of Clinical Oncology published guidelines on the prevention and monitoring of cardiac dysfunction in adult cancer patients, recommending the use of RNV or CMRI in cases where echocardiography is not available or technically feasible, for example, in cases with inadequate ultrasound windows.38 In addition to evaluating systolic function, RNV has demonstrated value in following diastolic function in patients exposed to cardiotoxic medications.

Radionuclide ventriculography versus echocardiography

RNV was more sensitive than echocardiography in detecting early decreases in LVEF.39,40 However, in these small studies, there was a high incidence of CTX (over 48%) without long-term follow-up. This limitation did not allow for correlations to be drawn with HF incidence. In a study of breast cancer patients who received ANT and TZU, measurements of LVEF by 3D ECHO and RNV were comparable, with CMRI used as a reference.23 A document titled “American Society of Echocardiography Expert Consensus Statement for Multimodality Imaging Evaluation of Adult Patients During and After Cancer Therapy”8 recommends the use of 2D ECHO or 3D ECHO for evaluating LVEF before, during, and after CT. In the case of inadequate image quality, the use of CMRI is recommended; RNV is not mentioned as a routine method. The specific availability of each service certainly interferes with the choice of method. There are currently new scintigraphic methods with other markers of early myocardial injury,35 which are capable of subclinically detecting LV dysfunction and which could predict the development of subsequent LV dysfunction or HF, such as sympathetic neural imaging with the 123I-meta-iodobenzylguanidine (123I-mIBG) technique, imaging of cell death (111In-antimiosina), targeted therapy imaging (111In-TZU), and molecular metabolic imaging of PET. All of these techniques have yet to be clinically validated for use in this CTX situation.

Studies with the adrenergic marker of neuronal integrity 123I-mIBG carried out in patients using ANT demonstrated that scintigraphy with mIBG is capable of identifying patients with a higher risk of CTX with great accuracy.41

Cardiac magnetic resonance imaging

Functional evaluation (cine MR and tagging/strain)

CMRI is the gold standard evaluation of LVEF volumes, using the technique of cine MR with quantification by Simpson's method. Its routine utilization is limited by availability and cost.42,43 In addition to accurately evaluating left and right ventricular function, CMRI can identify other probable causes associated with cardiomyopathy, such as myocardial invasion of the tumor, amyloidosis, sarcoidosis, myocarditis, and atherosclerotic coronary disease. CMRI should always be considered the first step before endomyocardial biopsy.8

Draft et al.44 detected subclinical abnormalities in geometry and ventricular function, such as a significant increase in final systolic volume, decreased LVEF and increased average circumferential strain in patients receiving low to moderate doses of anthracyclines. These markers are not usual criteria for CTX and the relation with prediction of future events is unknown. Armstrong et al.45 also detected subclinical cardiac dysfuntion using CMRI, analyzing LVEF and LV volume. No study of CMRI to date has demonstrated that alterations in myocardial function indexes after CT with ANT were predictors of subsequent CTX or HF. An ongoing observational study is assessing whether LV function measured by CMRI in patients using ANT, with or without TZU, will be able to predict a decrease in LVEF in 24 months.46

According to Plana et al.,8 CMRI should be used to confirm alterations in LVEF reported by other techniques or when there is a conflict between measurements from different techniques. This is only justified in the event that there is a plan to modify or interrupt CT. It is of little interest to use CMRI for diastolic function analysis due to the fact that its accuracy is similar to that of echocardiography.47,48

There are few studies on the evaluation of myocardial strain by CMRI for evaluating CT-related CTX. In the trial by Draft et al.,44 there was an early increase in midwall circumferential strain, after a month of therapy with ANT, associated with subclinical abnormality in ventricular function, demonstrated by a decrease in LVEF evaluated by CMRI. It is necessary to determine if these markers are associated with cardiovascular events in survivors of cancer.

Tissue characterization (myocardial enhancement/T1 mapping/T2 mapping)

Myocardial tissue characterization of CTX dates back to the 1980s, when necropsy and biopsy studies revealed that myocardial inflammation and cardiomyocyte edema are early findings of CTX, which occur prior to reduced myocardial function, as opposed to myocardial fibrosis, which is a late finding.49,50 In addition to its functional evaluation, CMRI is capable of performing morphological and tissue evaluation in a qualitative (visual) and quantitative manner, as percentage of muscle affected.51 Myocardial interstitial injuries may or may not be reversible, depending on different factors which include the degree of interstitial fibrosis. In this manner, CMRI is able to establish the differential diagnosis between reactive, infiltrative, and scar fibrosis.52

It is possible to evaluate CTX on the tissue level with early and late enhancement techniques.52 The main disadvantage is that, in the large majority of subclinical disease cases, there is no visually detectable fibrosis to be quantified and this technique is negative.

T1 mapping has been validated for detection of interstitial fibrosis not detected by late enhancement techniques, and the results are informed through the quantification of myocardial relaxation time in milliseconds.53 During postcontrast, the lower the myocardial T1, the higher the degree of interstitial fibrosis. T1 mapping has shown to be an independent predictor of CTX in patients treated with ANT who were followed for a period of 3 years.54 Extracellular volume (ECV) fraction which indicates the expansion of interstitial space corrected by hematocrit was also a strong imaging biomarker.54

T2 mapping is responsible for the quantification of cardiomyocyte edema, and it assists in the characterization of acute, subacute, or chronic damage.55 The results of T2 mapping are also represented by time in milliseconds. A study with 9 patients who received ANT showed that average T2 values > 59 ms were associated with CTX.56

Myocardial tissue characterization by CMRI may detect early myocardial injury during CT and identify subclinical myocardial alterations in cancer survivors; however, prospective studies are needed to confirm this hypothesis. The cost-effectiveness of using CMRI in comparison with other sequential follow-up techniques for patients undergoing CT still needs to be quantified.

Cardiac computed tomography (coronary angiotomography)

Coronary angiotomography is a method with growing clinical applicability that uses low doses of radiation (1-2 mSv) and iodinated contrast (50 mL).57 In addition to its classical indications, it is possible to quantify the volumes and ejection fractions of both ventricles.58 After the study by Nacif et al.,59 the use of angiotomography for the quantification of myocardial interstitial fibrosis via the quantification of VEC may be of great clinical utility. VEC values greater than 35% are associated with interstitial fibrosis.

Rational approach strategy for early detection of CTX

In Figure 1, we propose a flowchart showing the rational approach for patients undergoing CT. This algorithm is based on a review of the literature and the authors' expertise. It thus lacks validation in randomized controlled clinical trials. This approach should be adapted to the reality of each service's supply and demand conditions.8 Faced with a cancer patient, the following steps are recommended: (a) integrated actions, shared by cardiologists and oncologists, within a multidisciplinary team; (b) clinical evaluation of estimated global cardiovascular risk, previous diseases, previous chemo- or radiotherapy and, when indicated, specific intervention prior to CT; (c) within the institution's limitations, consider two-dimensional echocardiography with measurements of strain. (d) In the event that baseline cardiac evaluation is not available for all patients, prioritize those with high risks of CTX, such as those with CVD or cardiovascular risk factors; LV systolic dysfunction; over 65 years of age; a regimen with doses of ANT (DOX) greater than 350 mg/m2; or combination CT (Figure 1).

Figure 1
Proposal for cardiovascular monitoring of patients undergoing chemotherapy based on information in the literature and authors' expertise. ECG: electrocardiogram; CT: chemotherapy; RT: radiation therapy; 2D-ECHO: two-dimensional echocardiography; RNV: radionuclide ventriculography; CMRI: cardiac magnetic resonance imaging; ECHO: echocardiography.

If one the following is detected in a patient being monitored: LVEF < 53%, LVGLS below the lower limit of normality, or elevated troponins, in the absence of symptoms, the cardiologist should be consulted and the risk-benefit ratio related of CT discussed with the oncologist. Whether to continue or not is, however, the oncologist's decision. The healthcare flowcharts depend on the cardiotoxic potential of the CT regimen. In accordance with documents by the American and European societies of echocardiography, patients with cumulative doses below 240 mg/m2 of DOX should repeat the cardiac evaluation at the conclusion of the CT regimen and 6 months later.8 In patients with doses above 240 mg/m2 there should be a new evaluation before each additional 50 mg/m2 cycle. In patients receiving TZU, there should, ideally, be an echocardiogram every 3 months.8 Owing to the unavailability of data, in patients undergoing therapy with vascular endothelial growth factor inhibitors, evaluation with echocardiography 1 month after the initial dose and, subsequently, every 3 months, is recommended.8

Subclinical detection of left ventricular dysfunction

To date, there is no evidence regarding the treatment of asymptomatic patients with preserved LVEF and alterations exclusively in strain. However, the rationale for measuring strain is based on the possibility of frequently monitoring patients at risk and, as soon as a decrease in LVEF is detected, initiating therapy and obtaining reverse remodeling.

For the purpose of detecting subclinical dysfunction, baseline LVGLS is the marker for comparison of post-CT measurements. A relative reduction of more than 15% can confirm the dysfunction. This altered value should be confirmed by a new exam 2 or 3 weeks later. Elevated TnI with or without alterations in LVGLS is also considered a marker of myocardial injury; there are, however, multiple causes of elevations in TnI, as well as doubts regarding its prognostic value for ventricular dysfunction. Whenever the need for suspending CT is considered in asymptomatic patients, it is necessary to measure LVEF using a more accurate method, such as RNV or CMRI.8

There are no studies with safe levels of evidence demonstrating the benefits of pharmacological “cardioprotective” treatment in patients undergoing CT. When considering the hypothesis of continuing CT notwithstanding alternations in LV function, echocardiographic re-evaluation is necessary before the new cycle, with the awareness that the risk of CTX will progressively increase.

Additional imaging exams are not necessary for patients who have concomitant risk factors, in the presence of normal GLS or troponins during CT and 6 months after the last CT with ANT. Following completion of the therapeutic regimen, there should be annual clinical cardiovascular examination and the use of cardiac imaging in accordance with the services available.8

Conclusions

Monitoring LVEF by 2D ECHO is the most executable strategy for detecting CT-related cardiovascular disease in large groups of patients; this method should, however, be considered in the context of its numerous limitations. 3D ECHO is the method of choice when considering accuracy together with availability, limitations regarding repetition, and ease of execution. When this is not available, the addition of contrast to 2D ECHO should be encouraged, seeing that this increases accuracy. LVGLS is the best parameter of myocardial deformation for subclinical detection of LV dysfunction; however, there is no solid evidence showing the benefits of initiating early “cardioprotective” therapy based on its results. RNV has a high diagnostic accuracy for ventricular dysfunction and may be an alternative in the event of doubts regarding echocardiography. CMRI assists in differential diagnoses with other causes of cardiomyopathies.

The decision to interrupt or continue a chemotherapeutic regimen is clinical, joint, and multidisciplinary, and it is based on the risk-benefit ratio for each patient.

Randomized controlled clinical trials with long-term follow-up are necessary to determine whether early detection of cardiac dysfunction is a predictor of LVEF reduction and, above all, HF and major cardiovascular events.

  • Sources of Funding
    There were no external funding sources for this study.
  • Study Association
    This article is part of the thesis of Doctoral submitted by Mário Luiz Ribeiro, from Universidade Federal Fluminense.

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Publication Dates

  • Publication in this collection
    21 Feb 2019
  • Date of issue
    Mar 2019

History

  • Received
    05 Mar 2018
  • Reviewed
    21 Nov 2018
  • Accepted
    05 Dec 2018
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