Introduction
The sympathetic nervous system (SNS) is important in cardiac pathophysiology. By increasing
heart rate and arterial blood pressure, the SNS plays a central role to adapt cardiac
performance to conditions of increased external needs.1 Accordingly, a sympathetic
surge instantaneously ameliorates left ventricular (LV) contractility and relaxation,
abruptly increasing cardiac working capacities. However, while an elevated sympathetic
tone may be beneficial in the short term, a chronic elevation of SNS activity, as
in the case of congestive heart failure (CHF), has been clearly associated with a
significantly higher rate of adverse events.2,3 Accordingly, an accurate evaluation
of cardiac SNS activity has become a sine qua non in modern clinical cardiology. However,
most of the techniques for the assessment of cardiac sympathetic tone (i.e., baroreflex
sensitivity) offer an indirect estimation of its level of activation.4 Nuclear cardiac
imaging has been considered the reference standard for the evaluation of cardiac innervation,
allowing the evaluation of SNS activity in (semi)-quantitative terms. Therefore, in
the last decades, both positron emission tomography (PET)5 and conventional nuclear
imaging techniques [either planar scintigraphy or single-photon emission computed
tomography (SPECT)] have been demonstrated to allow the characterization of cardiac
sympathetic innervation.6 On one hand, PET imaging, with its higher image resolution,
radiotracers’ versatility, and intrinsically quantitative nature, is widely considered
the quality standard of cardiac SNS evaluation. On the other hand, conventional nuclear
imaging, with its robustness, availability, and relatively limited operational costs,
still represents the most frequently performed imaging test for cardiac innervation
imaging. More specifically, despite the theoretical advantages of more refined techniques
(i.e., PET and SPECT), planar scintigraphy with 123I-metaiodobenzylguanidine (123I-MIBG)
remains the workhorse of innervation imaging. Consequently, after almost 30 years
from their introduction in the research arena, the two measures of cardiac sympathetic
tone derived at planar scintigraphy, namely the heart-to-mediastinum (H/M) ratio and
the washout rate of 123I-MIBG, still represent the most validated measures of LV innervation
that are available, with the H/M ratio as reference standard.7 So, a depressed H/M
ratio of 123I-MIBG has been shown to associate with a significantly worse prognosis,
independently of LV ejection fraction.3 Moreover, in those years, a plethora of small-numbered
studies have demonstrated the association between abnormal H/M values and various
measures of LV structural and functional impairment, almost translating it as a universal
marker of cardiac risk. Nevertheless, despite these apparently promising results,
cardiac innervation imaging has a minimal, if any, clinical role in western countries,
with currently no indications in major clinical guidelines, except for Japan.
In order to understand this, some of the most evident limitations of cardiac 123I-MIBG
imaging should be carefully considered.
Standardization of Protocol
The scan protocol that is used for 123I-MIBG planar imaging varies widely, with the
delayed acquisition—the clinically relevant one—more often performed 4 hours after
tracer injection.7 However, this rather lengthy imaging protocol ends up consistently
affecting patients' compliance, reducing the possible throughput of the technique,
and discouraging the performance of additional, albeit time-consuming, dedicated cardiac
acquisitions (i.e., SPECT when performed with traditional Anger cameras).
Interestingly, the specifics of this apparently standardized protocol are based more
on habits than on experimental proof. In fact, solid evidence has demonstrated that
the real kinetics of 123I-MIBG in human hearts is consistently more rapid than initially
hypothesized,8 theoretically allowing a significantly faster image protocol, with
the late scan performed even 1 hour after tracer administration.9
Instrumentation
It has been demonstrated that, due to the specific emission spectrum of 123I-photons,
medium-energy collimators should be better used for cardiac 123I-MIBG imaging, in
order to obtain both high-quality images and accurate estimates of the H/M ratio.10
However, the majority of the diagnostic and prognostic data regarding 123I-MIBG imaging,
including the ones coming from the ADMIRE-HF study,3 have been obtained with low-energy
collimators, making the validity of the results obtained somehow questionable.
For similar reasons, no clinically useful cut-off value of H/M ratio has yet been
proposed, since the most frequently used normalcy value of 1.6 (derived from 202 historical
controls gathered from 7 studies)11 has been only validated in patients with CHF,
demonstrating, anyway, an unsatisfactory diagnostic accuracy as a biomarker of cardiac
risk.
The elevated methodological inhomogeneity of 123I-MIBG reports is even more evident
when studies performed, for instance, in Japan and Europe/US are compared, with the
former often using different instrumentation and scanning protocols (i.e., medium-energy
collimators). These technical disparities may allow to question the generalizability
of the many analysis of pooled 123I-MIBG data derived from studies performed in population
of patients with different ethnicities (Caucasian vs Asiatic) and imaged in different
scanning conditions.12
All together, these basic technical disadvantages of planar 123I-MIBG imaging allow
to question the role of cardiac innervation parameters as clinically useful biomarkers
of cardiac risk. While more elegant imaging techniques are available—SPECT and PET—they
are even less validated than planar imaging and are rarely employed for clinical purposes.
According to the authors’ beliefs, a redefinition of the role of cardiac sympathetic
innervation imaging is eagerly needed, clearly identifying the methodology to be used
and the specific fields of application.
In this respect, the most relevant limitations of current cardiac innervation imaging
modalities in specific clinical settings (i.e., CHF and ventricular arrhythmias) will
be further discussed.
Cardiac Innervation Imaging in Heart Failure: Chances and Limits
SNS plays a central role in the genesis and maintenance of CHF. In fact, evidence
has conclusively demonstrated that an increased SNS activity is not only associated
with the presence of CHF, but rather represent one of its most prominent (con)-causative
factors.4 In the last decades, nuclear cardiac imaging has allowed the characterization
of the interaction between sympathetic dysregulation and abnormal LV function, showing
that patients with CHF typically present a condition of SNS hyper-activation coupled
with post-synaptic myocardial sympathetic desensitization, due to reduced beta-adrenoceptor
density and catecholamine spill-over.3,13 In this respect, despite a number of small
mechanistic studies have suggested the possible value of cardiac innervation imaging
in the risk stratification and management of patients with CHF, the most solid evidence
in favor of its application in clinical practice comes from the ADMIRE-HF study.3
By enrolling nearly one thousand subjects with depressed LV ejection fraction and
moderately symptomatic CHF (NYHA class II-III) of mixed etiology (66% ischemic and
34% non-ischemic), the ADMIRE-HF study demonstrated that the H/M ratio of 123I-MIBG
was able to risk-stratify patients independently of other commonly measured cardiac
functional parameters, such as LV ejection fraction and BNP. However, in order to
be introduced in clinical practice, any biomarker must have a number of necessary
qualities that should be always taken into account: a cut-off value characterized
by a relevant accuracy in unmasking high-risk patients, the clear definition of the
categories of patients where it should be applied, and the demonstration of its significant
impact on patient management in terms of either prognosis or cost-benefit. Accordingly,
despite the encouraging results coming from ADMIRE-HF, relevant limitations of the
studies performed so far have prevented the clinical application of cardiac innervation
imaging. First of all, no real cut-off of H/M ratio actually exists. In fact, the
H/M ratio is rather characterized by a continuous association with patients risk14
and the cut-off values proposed so far have only shown a modest diagnostic accuracy
in discriminating patients' risk categories.15 Moreover, while the ADMIRE-HF trial
was designed to include only patients with severely compromised LV systolic function,
it was demonstrated that 43% of them had a LV ejection fraction >35% at core-lab analysis,16
making the main results of the study rather questionable and a clear definition of
the category of patients that may benefit from innervation imaging still lacking.
However, the prominent limitation of the existing literature regarding cardiac SNS
imaging is that it lacks a prospective evaluation of the prognostic impact of innervation
parameters on clinical decision-making and patient management. In fact, as in the
case of any biomarker, it should be determined whether measures of cardiac sympathetic
tone may be used to guide and monitor therapeutic interventions, helping the clinician
to prognosticate the result of specific therapies and to decide, for instance, on
the non-use of an otherwise indicated strategies. To date, only few studies performed
in patients mainly suffering from CHF have evaluated how cardiac sympathetic innervation
parameters might predict patient response to selected cardioactive treatments, suggesting
the existence of some correlation between measures of innervation at baseline and
the effect of the therapies.17,18 However, most of those reports did not assess true
patient outcomes but rather surrogate endpoint of treatment efficacy (i.e., change
in LV ejection fraction)17 and were not randomizing patients to strategies with and
without innervation imaging.18
After all those years, all the different disease-modifying therapeutic strategies
that can be adopted in patients with CHF are only selected according to the presence
of classical cardiac structural and functional abnormalities (i.e., ECG abnormalities
or a depressed LV ejection fraction), disregarding any parameter of sympathetic innervation.
In other words, despite the existing evidence, no one would ever exclude any patient
with CHF from a given treatment, either pharmacological or device-based [i.e., cardiac
resynchronization therapy (CRT)], based on the findings of cardiac innervation imaging,
such as a depressed H/M ratio of 123I-MIBG. More innovative imaging techniques, such
as SPECT acquisition particularly if performed with dedicated CZT devices, might allow
to overcome some of the limitations of planar 123I-MIBG scans, giving the opportunity
to obtain a three-dimensional measures of cardiac sympathetic tone despite a contained
acquisition time.18 However, a reliable prospective validation of the added value
of such imaging modalities in the management of CHF is eagerly awaited.
Innervation Imaging in Patients with IHD and Increased Cardiac Risk
Sympathetic nervous terminals are significantly more sensitive to ischemia than myocardial
cells. In fact, after an acute myocardial infarction, the area of LV sympathetic denervation
typically exceeds the extent of myocardial necrosis.19 Thereafter, during the recovery
phase, autonomic nerve terminals sprout from the borderzone of the infarction with
progressive cardiac reinnervation. However, the healing process is frequently incoherent,
leading to the formation of islands of viable but denervated myocardium surrounded
by hyper-innervated regions that ultimately represent possible sites of origin of
malignant ventricular arrhythmias.20
Accordingly, it is not surprising that measures of cardiac sympathetic denervation
have been repeatedly associated with an increased risk of arrhythmic events, possibly
helping to better risk-stratify cardiac patients. Specifically, results coming from
the ADMIRE-HF study have shown that patients with a H/M ratio <1.6 had a significantly
higher incidence of malignant ventricular arrhythmic episodes, even fatal, than those
with a relatively preserved cardiac sympathetic tone.3 However, despite some initially
encouraging data, 123I-MIBG scintigraphy has proved to be a rather inaccurate method
for the prediction of malignant ventricular arrhythmias, since patients with a preserved
innervation (i.e., H/M ratio >1.6) still have a significant incidence of arrhythmic
events or sudden cardiac deaths (roughly 3% in the ADMIRE-HF cohort), and does not
select patients that may have improved survival with implantable cardioverter defibrillator
(ICD) implantation.17 Therefore, for many categories of patients, the presence of
a significantly depressed LV ejection fraction (i.e., less than 30%-35%) is frequently
considered the only indication for ICD therapy.
Interestingly, after many years, the currently on-going ADMIRE-ICD study (NCT02656329)
will be the first randomized trial to evaluate the efficacy of 123I-MIBG imaging for
guiding the decision of ICD implantation. However, since this study will only enroll
patients with a narrow range of EF values (between 30% and 35%), it could, curiously,
further limit the categories of patients that could benefit from cardiac innervation
imaging.
In this scenario, planar scintigraphy badly adapts to appropriately describe the patterns
of cardiac sympathetic denervation in patients with IHD and post-ischemic LV dysfunction
who frequently show areas of viable myocardium interposed within scarred regions.
In fact, limited evidence has suggested that the use of tomographic imaging techniques,
such as SPECT or PET, would allow an accurate depiction of the regional distribution
of sympathetic nerve terminals and a better risk stratification than traditional planar
measures.19 Moreover, by integrating information coming also from the evaluation of
myocardial perfusion data, the innervation imaging of the future will probably allow
the combined assessment of two of the most relevant cardiac functional parameters
and the accurate localization of the areas of viable myocardium showing a depressed
sympathetic innervation. In fact, the presence of those myocardial regions showing
an “innervation/perfusion mismatch” (i.e., at the border zone of myocardial scars),
representing preferred sites of origin of malignant ventricular arrhythmias,20 has
been clearly associated with adverse patients' prognosis.19 An elevated regional burden
of jeopardized myocardium with impaired sympathetic innervation may possibly represent
an additional marker of risk in patients with IHD, possibly predicting the need for
aggressive therapeutic strategies.19,20 Nevertheless, while the possible clinical
impact of those innovative parameters of regional sympathetic denervation has been
recently suggested by some small studies, an appropriate validation of this diagnostic
approach is still awaited and the current clinical role of innervation imaging in
the management of patients at risk of malignant ventricular arrhythmias almost inexistent.
Conclusion
Nuclear cardiac imaging is the only accurate tool for the assessment of the interaction
between LV sympathetic innervation and cardiac function. Among the different methodologies
that have been proposed, a rather rudimentary technique, namely planar 123I-MIBG scintigraphy,
still remains the state-of-the-art for the evaluation of cardiac sympathetic innervation.
However, while evidence has been accumulating on the possible role of innervation
imaging for the risk stratification and disease management of cardiac patients, none
of these techniques has never reached the clinical arena and is mainly considered
a purely research investigation. A number of reasons may justify this apparent conundrum.
First of all, large trials focused on specific categories of patients to clearly identify
the possible fields of applications of cardiac innervation imaging (i.e., management
of patients with borderline indication for ICD implantation or selection of patients
with malignant ventricular arrhythmias undergoing invasive procedures) are still lacking.
On the other hand, the panel of clinically available nuclear techniques should be
further implemented, with the progressive abandonment of “old-fashioned” methodologies
and measures (i.e., H/M ratio of 123I-MIBG), and the introduction of innovative markers
of risk obtained with novel technologies (i.e., CZT cameras), such as the regional
extent of LV sympathetic denervation or the burden of innervation/perfusion mismatch.
Otherwise, it is conceivable that nuclear innervation imaging will remain one of the
“holy grails” of modern cardiology, with a solid pathophysiologic background but limited,
if any, clinical applications and patients will be further treated according to other
biomarkers, such as LV ejection fraction.