Abstract
Introduction
Joubert syndrome (JS) is an autosomal recessive disorder characterized by a congenital malformation of the mid-hindbrain and a large spectrum of clinical features including congenital retinal dystrophy. The function of different retinal elements (rod, cone, bipolar cells) can be objectively evaluated by electroretinogram (ERG) recordings. Our work aims to evaluate the retinal function (by ERG recordings) in patients with JS with or without congenital retinal dystrophy. In addition, since clinical trials should be performed in the near future in JS, our results could provide information about the possible usefulness of ERG recordings in the assessment of the efficacy of treatments targeted to improve the retinal involvement.
Methods
In this observational and prospective study, 24 children with genetic identification for JS (mean age 10.75 ± 6.59 years) and 25 healthy age-similar normal control subjects (control group, mean age 10.55 ± 3.76 years) were enrolled. On the basis of the presence/absence of retinal dystrophy at fundus examination, patients with JS were divided into two groups: patients with JS with retinal dystrophy (16 children, mean age 11.00 ± 6.74 years, providing 16 eyes; JS-RD group) and patients with JS without retinal dystrophy (8 children, mean age 10.50 ± 6.45 years, providing 8 eyes; JS-NRD group). In patients with JS and controls, visual acuity (VA), dark-adapted, light-adapted, and 30-Hz flicker ERGs were performed according to International Society for Clinical Electrophysiology of Vision (ISCEV) standard protocols.
Results
When compared to controls, patients in the JS-RD and JS-NRD groups showed significant abnormalities of the values of dark-adapted, light-adapted, and 30-Hz flicker ERG parameters. The ERG and VA changes were not significantly correlated.
Conclusions
Our results suggest that a dysfunction of photoreceptors and bipolar cells occurs in patients with JS with or without retinal dystrophy. The retinal impairment can be detected by ERG recordings and this method should be proposed to evaluate the effectiveness of adequate treatment targeted to improve the retinal impairment in patients with JS.
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Why carry out this study? |
Joubert syndrome (JS) is an autosomal recessive disorder characterized by congenital malformation of the mid-hindbrain and a large spectrum of clinical features including congenital retinal dystrophy. |
The function of different retinal elements (rod, cone, bipolar cells) can be objectively evaluated by using different types (dark-adapted, light-adapted, and 30-Hz flicker) of electroretinogram (ERG) recordings. |
This observational and prospective study was carried out to evaluate the retinal function (by ERG recordings) in patients with JS with (JS-RD group) or without (JS-NRD group) congenital retinal dystrophy. Our results should provide information about the possible usefulness of ERG recordings in the assessment of the efficacy of treatments targeted to improve the retinal condition. |
What was learned from the study? |
When compared to controls, patients in the JS-RD and JS-NRD groups showed significant abnormalities of the values of dark-adapted, light-adapted, and 30-Hz flicker ERG parameters. The ERG and visual acuity changes were not significantly correlated. |
In patients with JS with or without retinal dystrophy, a dysfunction of photoreceptors and bipolar cells occurs and this can be detected by ERG recordings. ERG methods should be proposed to evaluate the effectiveness of adequate treatment aimed to improve the retinal impairment of patients with JS. |
Introduction
Joubert syndrome (JS) is an autosomal recessive disorder characterized by a congenital malformation of the mid-hindbrain and a large spectrum of clinical features; the disease was first described by Marie Joubert [1] who observed four siblings with cognitive impairment, ataxia, episodic tachypnea, eye movement abnormalities, and cerebellar vermis agenesis. At present, the diagnosis is based on the presence of the typical “molar tooth sign” on brain imaging, characterized by cerebellar vermian hypoplasia, thickened and horizontalized superior cerebellar peduncles, and a deepened interpeduncular fossa [2].
The prevalence of JS has been estimated at approximately 1:100,000 in the USA [3]. The pathology can occur as an isolated neurological disorder or can be associated with variable involvement of other organs like the liver, kidney, and retina (defined as “Joubert syndrome related-disorders” [2, 3]).
In patients with JS over 30 genes are known [4, 5], all encoding proteins of the primary cilium, a subcellular organelle found on the surface of most cellular types, making JS part of the expanding spectrum of “ciliopathies” [6].
The visual system is also involved [7] and, in particular, congenital retinal dystrophy [8,9,10], jerky eye movements, nystagmus, strabismus [1], oculomotor apraxia [11, 12], coloboma [13, 14], and ptosis and extraocular muscle limitation [15] are described in these patients.
In genetic disorders involving the retinal structures, a current and interesting goal is to increase the retinal function by different types of treatment, including gene therapy. At present, there are no reported clinical trials on JS aiming to improve the retinal condition.
Since in JS the visual dysfunction is mainly related to the presence of congenital retinal dystrophy [7,8,9], a particular interest is to assess the function of different retinal elements (rod, cone, bipolar cells) by using an objective approach such as the recordings of different types (dark-adapted, light-adapted, and 30-Hz flicker) of electroretinogram (ERG) responses, by standardized International Society for Clinical Electrophysiology of Vision (ISCEV) protocols [16].
In rare diseases, such as JS, the monitoring of retinal function over time and/or after specific treatments is a debated topic, because it is not easy to find appropriate tests that can evaluate both visual function and retinal function at the same time. Although ERG is a sensitive objective tool for evaluation of retinal function, it is generally neglected in the list of instrumental tests for accurately monitoring potential changes after targeted innovative treatments. Therefore, our aim was to evaluate the functional condition of different retinal elements (by ERG recordings) in patients with JS with or without congenital retinal dystrophy. In addition, since appropriate clinical trials could be performed in the near future for JS, our results might provide new information on the possible usefulness of ERG recordings to evaluate the efficacy of treatments targeted to improve the retinal condition.
Methods
Patients
In this observational and prospective study, 24 children (mean age 10.75 ± 6.59 years) with a neuroradiologically proven “molar tooth sign” and with genetic identification for JS and 25 healthy age-similar (mean age 10.55 ± 3.76 years) control subjects were included. Patients with JS were enrolled at the Department of Child Neurology and Child Psychiatry IRCCS C. Mondino, Pavia, and underwent complete ophthalmological evaluation (see below) at the Section of Ophthalmology, University of Pavia, IRCCS Fondazione Policlinico San Matteo, Pavia. Patients with JS underwent a complete diagnostic workup including a detailed assessment of renal, liver, and heart function, and received genetic counselling. DNA for genetic studies by a next-generation-sequencing-based analysis of 120 ciliary genes, including 27 genes known to cause JS [17], were available for all 24 enrolled patients.
Patients with JS and controls had a complete ophthalmological examination including best corrected visual acuity (BCVA) assessment. Anterior segment evaluation with a slit lamp was performed depending on the patients’ cooperation. Cycloplegic refraction (cyclopentolate 1%) and dilated fundus examination with indirect ophthalmoscopy were performed on each patient.
On the basis of the presence/absence of retinal dystrophy at fundus examination, patients with JS were divided into two groups:
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Patients with JS with retinal dystrophy: 16 children, providing 16 eyes (JS-RD group)
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Patients with JS without retinal dystrophy: 8 children, providing 8 eyes (JS-NRD group)
Demographic data, identified mutation, observed type of retinal dystrophy, and visual acuity detected in controls and JS-RD and JS-NRD groups are reported in Table 1.
All procedures performed in this study were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Helsinki declaration and its later amendments or comparable ethical standards. The study was approved by the local institutional review board (Scientific Committee of Section of Ophthalmology, University of Pavia, IRCCS Fondazione Policlinico San Matteo, Pavia, Italy). Informed consent was obtained from all individual participants included in the study.
Visual Acuity Evaluation
In verbal children, BCVA was assessed by the modified Early Treatment Diabetic Retinopathy Study (ETDRS) charts (Lighthouse, Low vision products, Long Island City, NY, USA) and expressed in logMAR values obtained at the distances of 4, 2, 1, and 0.5 m. In preverbal and nonverbal children, BCVA was measured with Teller acuity cards (TACs) and the values were converted to logMAR.
Electroretinography Assessment
Dark-adapted, light-adapted, and 30 Hz flicker ERGs (flicker ERG) were performed according to ISCEV standard protocols by using skin electrodes [16].
In the analysis of dark-adapted and light-adapted ERGs we considered a- and b-wave implicit time (IT) and a- and b-wave peak-to-peak amplitude (A). In the analysis of flicker ERG the peak-to-peak amplitude (A) was considered (Fig. 1).
Statistical Analysis
The Anderson–Darling and Kolmogorov–Smirnov tests were applied to verify that data were normally distributed. Only one eye was chosen for each patient.
Differences of values of BCVA and of all ERG parameters between controls and both JS groups were evaluated by the one-way analysis of variance (ANOVA). Pearson’s test was used to assess the relationship between the values of BCVA and those of all ERG parameters. All statistical analyses were performed using SPSS version 26 (Statistical Package for Social Science IBM) and a p value less than 0.01 was considered as statistically significant.
Results
Visual Acuity Data
On average, a significant (p < 0.01) reduction in BCVA values was observed when data from the JS-RD group were compared to those of controls and of the JS-NDR group. In the JS-RD group, the greatest BCVA reduction was detected in patients with INPP5E, TMEM67, and C5orf42 mutations. In the JS-NDR group, no significant (p > 0.01) differences in BCVA values were found with respect to those of controls.
ERG Analysis
In Fig. 1 are reported representative examples of dark-adapted ERG, light-adapted ERG, and flicker ERG responses assessed in one control subject (C#12 eye), in one JS patient with retinal dystrophy (JS-RD#9 eye) and in one patient without retinal dystrophy (JS-NRD#6 eye).
On Table 2 are reported the correlation between the individual values of dark-adapted ERG, light-adapted ERG, and flicker ERG parameters and the corresponding values of BCVA observed in JS-RD and JS-NRD groups.
Table 3 presents the mean data of light-adapted ERG, dark-adapted ERG, and flicker ERG parameters detected in controls and JS-RD and JS-NRD groups together with a relative statistical analysis between groups.
The ERG results are reported separately in the following subsections.
Dark-Adapted ERG
On average, in the JS-RD group a-wave and b-wave ITs and A values were respectively significantly (p < 0.01) increased and reduced when compared to control ones.
In the JS-RD group, the greatest delay of a-wave and b-wave IT and the greatest reduction of a-wave and b-wave A were observed in patients with INPP5E mutation.
Considering individual patients with JS-RD, the a-wave and b-wave ITs and A values were not significantly (p > 0.01) correlated with the corresponding values of BCVA.
On average, when compared to those of controls, in the JS-NRD group a significant (p < 0.01) increase in a-wave and b-wave IT values and a significant (p < 0.01) reduction in a-wave and b-wave A values were found. JS-NRD and JS-RD groups showed no significant (p > 0.01) differences between the mean values of all dark-adapted ERG parameters. When considering the individual JS-NRD values, the greatest delay of a-wave IT, the greatest reduction in b-wave A, and the greatest reduction of a-wave A were found in patients with CC2D2A mutation, whereas the greatest reduction of a-wave A and delay of b-wave IT were detected in patients with C5orf42 mutation.
In JS-NRD, no significant (p > 0.01) linear correlation between the individual values of a-wave and b-wave ITs and A values with the corresponding values of BCVA was observed.
Light-Adapted ERG
On average, in the JS-RD group a significant (p < 0.01) increase in a-wave and b-wave ITs and a significant (p < 0.01) reduction in a-wave and b-wave A values were found with respect to control ones.
Considering the individual values detected in patients with JS-RD, the greatest increase of a-wave and b-wave IT and the greatest reduction of a-wave and b-wave A values were found in patients with INPP5E mutation.
The increase of a-wave and b-wave ITs and the reduction of a-wave and b-wave A values observed in individual patients with JS-RD were not significantly (p > 0.01) linearly correlated with the corresponding values of BCVA.
On average, in the JS-NRD group a significant (p < 0.01) increase in a-wave IT values and a significant (p < 0.01) reduction in a-wave and b-wave A values with respect to those of control ones were detected. No significant (p > 0.01) differences were observed for the b-wave IT values between JS-NRD and control groups. No significant (p > 0.01) differences of the mean values of all light-adapted ERG parameters were found between the JS-RD and JS-NRD groups.
In the JS-NRD group, when considering the individual values, the greatest delay of a-wave and b-wave IT in the greatest reduction of a-wave A were found in patients with C5orf42 mutation, whereas the greatest reduction of b-wave A was observed in patients with CC2D2A mutation. In the JS-NRD group, no significant (p > 0.01) linear correlations were observed between the individual values of a-wave and b-wave ITs and A values and the corresponding values of BCVA.
Flicker ERG
On average, in the JS-RD group, significantly (p < 0.01) reduced amplitude values were found with respect to control ones. In this group, the greatest reduction of amplitude was observed in patients with INPP5 mutation. Considering individual patients with JS-RD, amplitudes were not significantly (p > 0.01) linearly correlated with the corresponding values of BCVA. On average, when compared to controls, in the JS-NRD group a significant (p < 0.01) reduction in amplitude was found. JS-RD and JS-NRD groups showed no significant (p > 0.01) differences in amplitude values.
Considering individual JS-NRD values, the greatest reduction of amplitude was detected in patients with CC2D2A mutation. In JS-NRD, no significant (p > 0.01) linear correlations were observed between the individual amplitude values and the corresponding values of BCVA.
Discussion
The aim of our work was to evaluate the retinal function (by ERG recordings) in patients with JS with or without retinal dystrophy. As a consequence of the ERG findings, this technique could be suggested as an objective method for the evaluation of effectiveness of credible treatment in future clinical trials.
In our study, we performed three different types of ERG recordings that allowed us to evaluate selectively the function of different retinal elements. In particular, in accordance with ISCEV standards for clinical electroretinography, we recorded dark-adapted ERG that is a combined response arising from photoreceptors (a-wave) and bipolar cells (b-wave) of both the rod and cone systems (rod dominated), light-adapted ERG that reflects the bioelectrical activity of the cone (a-waves), and cone ON and OFF bipolar cells (b-wave), and light-adapted 30-Hz flicker ERG that evaluates the cone-pathway-driven response [16].
In our patients with JS-RD we found significant abnormal dark- and light-adapted ERG and flicker ERG responses when compared to controls. Our findings are consistent with the very few articles present in the literature [7, 18, 19]. Our results suggest that in patients with JS-RD there is a dysfunction of both rod and cone systems and ON and OFF bipolar cells [16]. The observed dysfunction can be ascribed to both rod and cone disorganization of photoreceptor outer segments. This is suggested by the findings obtained in animal models with an electron microscopy evaluation [20, 21], and by morphological evidence in human studies performed by using optical coherence tomography assessment [22, 23].
In our cohort of patients with JS-RD, the greatest ERG abnormalities were detected in patients with INPP5E mutation and this may represent a novel finding since in other previous similar published works [7, 18, 19] there is a lack of information about the relationship between the increase of a- and b-wave ITs and the reduction of a- and b-wave A values and the specific detected mutation.
The genetic mutation can impact at different levels and times in retinal development and metabolism, resulting in a retinal functional and morphological involvement. All this can be explained by the data that in all JS genetic types, the mutation implies a Wnt or hedgehog (Shh) signal dysfunction and it is the role of Wnt and Shh genes as regulator for normal laminar organization of the retinal elements is well known [24,25,26,27]. In addition, the lack or a dysfunction of Wnt may induce a retinal pigmented epithelium hypertrophy or hyperplasia (as observed in 8 of our 16 patients with JS-RD) and failure of ventral retinal development originating in a retinal coloboma (as observed in 4 of our 16 patients with JS-RD) [27].
In our JS-RD group, large BCVA reduction was detected in patients with INPP5E, TMEM67, and C5orf42 mutations and this is consistent with all data previously reported by Brooks et al. [19].
In the JS-RD group, no significant correlations were found between the reduction of BCVA and ERG abnormalities. This can because the data we obtained by performing different types of ERG recordings reflect the bioelectrical activity of different retinal elements of the whole retina with a negligible contribution of the macular region, which is strictly implicated in the visual acuity assessment. For this requirement, it would be useful to perform multifocal ERG recordings that, by applying the “ring analysis” [28,29,30,31,32,33], allow a functional evaluation of cones and bipolar cells located in the macular area [34]. Nevertheless, the multifocal ERG recordings require a particular ability to maintain a stable fixation for the entire duration of the examination and we believe that cannot be correctly performed in children with a low visual acuity such as our patients with JS-RD.
An interesting finding of our work is that significant abnormal ERG values (dark- and light-adapted and flicker responses) were also detectable in patients with JS without retinal dystrophy (JS-NRD group). Such as for other diseases (i.e., diabetes without retinopathy) [35], a retinal dysfunction, in the absence of retinal dystrophy at fundus examination, may also occur.
The observed ERG findings may suggest that all previously cited retinal development and metabolism changes [24,25,26,27] can also occur patients in the JS-NRD group, inducing a dysfunction of both rod and cone systems and ON and OFF bipolar cells.
Since in the JS-NRD group no significant changes in BCVA with respect to controls were found, it is likely that the macular area is spared from this involvement; however, to exclude this possibility a multifocal ERG assessment would be required. Also in this case, the same aforementioned limitation (ability to maintain a stable fixation) persists.
Our cohort of patients with JS-NRD comprised only eight children whereas there were 16 patients with JS-RD enrolled; this is in accordance with data reporting a less frequent absence of retinal dystrophy in this syndrome [5, 20]. The greatest ERG abnormalities were found in patients with both CC2D2A and C5orf42 mutations, whereas in the JS-RD group it was in patients with INPP5E mutation. It is worth noting that none of our enrolled patients with JS-NRD had INPP5E mutation. Our ERG findings are similar to that reported in only one case by Brooks et al., although the mutation was not specified [19].
All ERG findings detected in our patients with JS were similar to those observed in patients with other retinal dystrophies (see Creel for a review [36]). Recently, to obtain an increase of retinal function, several clinical trials have been performed in patients with inherited retinal dystrophies by using different types of treatments. In many of these studies [37,38,39,40,41,42,43,44] the efficacy of the treatment was evaluated by measuring the changes of the ERG responses. Actually, no similar studies have been performed or are ongoing in patients with JS with retinal functional or morphological involvement.
Conclusion
Our results suggest that a dysfunction of photoreceptors and bipolar cells occurs in patients with JS with or without retinal dystrophy. The retinal impairment can be detected by ERG recordings, evaluating objectively the retinal function changes; this method, associated with psychophysical visual function measures (visual acuity and visual field), may be proposed as a tool able to evaluate the effectiveness of adequate treatment, targeted to improve the retinal impairment in patients with JS.
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Acknowledgements
We thank the participants of the study. The contribution of the Bietti Foundation for this study was supported by the Italian Ministry of Health and Fondazione Roma.
Funding
No funding or sponsorship was received for this study or publication of this article.
Authorship
All named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this article, take responsibility for the integrity of the work as a whole, and have given their approval for this version to be published.
Disclosures
Giulio Ruberto, Vincenzo Parisi, Chiara Bertone, Sabrina Signorini, Mauro Antonini, Enza Maria Valente, Federica Manzoni, Valentina Serpieri and Riccardo Fausto declare that they have no conflict of interest. Luciano Quaranta is a member of the journal’s Editorial Board.
Compliance with Ethics Guidelines
All procedures performed in this study were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Helsinki declaration and its later amendments or comparable ethical standards. The study was approved by the local institutional review board (Scientific Committee of Section of Ophthalmology, University of Pavia, IRCCS Fondazione Policlinico San Matteo, Pavia, Italy). Informed consent was obtained from all individual participants included in the study.
Data Availability
All authors had full access to all of the data in this study and take complete responsibility for the integrity of the data and accuracy of the data analysis. The datasets generated and/or analyzed during the current study are available from the corresponding author on reasonable request.
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Ruberto, G., Parisi, V., Bertone, C. et al. Electroretinographic Assessment in Joubert Syndrome: A Suggested Objective Method to Evaluate the Effectiveness of Future Targeted Treatment. Adv Ther 37, 3827–3838 (2020). https://doi.org/10.1007/s12325-020-01432-9
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DOI: https://doi.org/10.1007/s12325-020-01432-9