Abstract
Amblyopia is a neurodevelopmental disorder of vision caused by abnormal visual experience during early childhood that is often considered to be untreatable in adulthood. Recently, it has been shown that a novel dichoptic videogame-based treatment for amblyopia can improve visual function in adult patients, at least in part, by reducing inhibition of inputs from the amblyopic eye to the visual cortex. Non-invasive anodal transcranial direct current stimulation has been shown to reduce the activity of inhibitory cortical interneurons when applied to the primary motor or visual cortex. In this double-blind, sham-controlled cross-over study we tested the hypothesis that anodal transcranial direct current stimulation of the visual cortex would enhance the therapeutic effects of dichoptic videogame-based treatment. A homogeneous group of 16 young adults (mean age 22.1 ± 1.1 years) with amblyopia were studied to compare the effect of dichoptic treatment alone and dichoptic treatment combined with visual cortex direct current stimulation on measures of binocular (stereopsis) and monocular (visual acuity) visual function. The combined treatment led to greater improvements in stereoacuity than dichoptic treatment alone, indicating that direct current stimulation of the visual cortex boosts the efficacy of dichoptic videogame-based treatment. This intervention warrants further evaluation as a novel therapeutic approach for adults with amblyopia.
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Keywords: Amblyopia, Plasticity, tDCS, Stereopsis, Inhibition
Introduction
Amblyopia, sometimes referred to as “lazy eye”, is a neurodevelopmental disorder of vision arising from decorrelated binocular input during early visual development (prevalence, approximately 3 %) [1]. Amblyopia results in decreased visual acuity in an otherwise healthy eye and is often associated with suppression of inputs from the amblyopic eye to the visual cortex [2, 3]. This causes an impairment of binocular visual functions such as stereoscopic depth perception. Conventional amblyopia treatment emphasizes patching or penalization of the fellow-fixing (non-amblyopic) eye to force the use of the amblyopic eye [4–6]. While effective at improving visual acuity [6, 7], current treatment is often associated with residual monocular [8] and binocular [9] deficits, and a high rate of recurrence [10]. It has been argued that the monocular treatment approach may not be maximally effective, as it does not directly address suppression [11, 12]. In fact, participants with deeper suppression may have less successful monocular treatment outcomes [13]. Moreover, the standard monocular approach to amblyopia treatment is often considered to be ineffective for adult patients who are past the critical period of visual cortex development [14].
Recent evidence from animal models has shown that reduced cortical inhibition allows for recovery of vision in adult amblyopic eyes [15–19]. This has led to the development of amblyopia treatment interventions designed to reduce suppressive mechanisms within the human visual cortex [11, 20–26]. One approach, based on psychophysical models of binocular vision and supported by initial clinical studies in adults [11, 23, 27] and children [22] involves dichoptic (separate images to each eye) presentation of high contrast images to the amblyopic eye and lower contrast images to the fellow eye. This dichoptic treatment approach has recently been implemented in the form of a videogame that can be played using video goggles [22] or on an iPod touch equipped with a lenticular overlay screen [23].The contrast imbalance overcomes suppression and allows patients to see with both eyes simultaneously. Repeated exposure to such stimuli results in a lasting reduction in suppression, and improvements in both binocular and monocular visual function [11, 22, 23, 27].
In addition to behavioral interventions, non-invasive brain stimulation techniques, such as repetitive transcranial magnetic stimulation and transcranial direct current stimulation (tDCS), are capable of modulating inhibitory networks within targeted areas of the human brain [25, 28–31]. The use of non-invasive brain stimulation techniques for the treatment of amblyopia is developing rapidly [25, 26, 32], and tDCS is particularly attractive owing to its low cost and the possibility that it can be used in the patient’s own home [33]. Anodal tDCS (a-tDCS) tends to increase and cathodal tDCS (c-tDCS) tends to decrease excitability in the stimulated region. Several mechanisms have been proposed for these effects, including alteration of the resting membrane potential [34] and N-methyl-D-aspartate receptor-dependent long term potentiation (LTP)- or long term depression (LTD)-like mechanisms [35]. Of particular relevance for amblyopia, a-tDCS has been associated with a reduction in gamma-aminobutyric acid-mediated inhibition. These effects have been observed when a-tDCS is applied to either the motor [29, 30] or visual [28] cortices. Furthermore, there is evidence that a-tDCS of the visual cortex can enhance the effects of visual rehabilitation for visual field loss following stroke [36, 37]. This is consistent with studies reporting that a-tDCS can augment physiotherapeutic interventions for motor impairments following stroke [38, 39] and enhance learning/skill acquisition [29].
The aim of this study was to determine whether a-tDCS can enhance the effects of dichoptic treatment in adults with amblyopia. To explore the potential of this multimodal treatment approach we designed a double-blind sham-controlled cross-over study in which adults with amblyopia received daily sessions of dichoptic treatment combined with a-tDCS of the visual cortex. Our hypothesis was that dichoptic treatment and a-tDCS would result in greater improvements in visual function than dichoptic treatment alone.
Methods
Participants
Sixteen adults with amblyopia (mean age 22.07 ± 1.1 years SEM) were recruited from the ophthalmology clinics at Zhongshan Ophthalmic Center, Guangzhou, China. Inclusion criteria were a visual acuity of 0 LogMar or better in the fellow fixing eye, at least 0.2 LogMar difference in visual acuity between the eyes, and no contraindications for tDCS. Five participants had previously undergone patching therapy, and 11 patents had received no previous treatment. Clinical details of all participants are summarized in Table 1. Best refractive correction was worn during all testing sessions and prismatic correction was provided when necessary. The study protocols were approved by the Ethics Committee of Zhongshan Ophthalmic Center, Sun Yat-sen University, and complied with the Declaration of Helsinki. All participants provided informed consent.
Table 1.
Identification | Age/sex | History and previous treatment | Type of amblyopia | Visual acuity (logMAR) | Current refraction |
---|---|---|---|---|---|
G1-1 | 18/M | Not known, patching | RE | 0.0 | Plano |
LE Aniso | 0.73 | +5.75 –1.25 × 5 | |||
G1-2 | 20/F | Not known, none | RE | 0.0 | +0.25 |
LE Strab | 1.03 | Plano | |||
G1-3 | 19/F | Detected age 8 years, patching | RE | 0.0 | −1.25 |
LE Aniso | 0.22 | −0.25 –0.5 × 145 | |||
G1-4 | 22/F | Not known, patching | RE | 0.0 | −1.5 |
LE Aniso | 0.4 | +3.0 | |||
G1-5 | 22/M | Not known, none | RE Aniso | 0.16 | +5 –0.5 × 35 |
LE | 0.0 | +2.5 –0.5 × 155 | |||
G1-6 | 25/F | Detected age 7 years, surgery | RE Strab | 0.75 | −1.25 |
LE | 0.0 | −0.75 | |||
G1-7 | 31/F | Not known, none | RE | 0.0 | −3.25 |
LE Strab | 0.42 | −2.25 | |||
G1-8 | 20/M | Detected age 5 years, patching | RE | 0.0 | +1.25 –0.75 × 15 |
LE Aniso | 1.0 | +6.5 –1.0 × 95 | |||
G2-1 | 21/F | Not known, none | RE | 0.0 | −0.5 |
LE Aniso | 0.15 | +3.25 –1.0 × 80 | |||
G2-2 | 23/F | Not known, patching | RE | −0.8 | +4.75 –1.0 × 10 |
LE Strab | 1.03 | +4.5 –1.25 × 5 | |||
G2-3 | 17/M | Not know, none | RE Mixed | 1.05 | +4.25 –0.5 × 50 |
LE | 0.0 | −0.25 | |||
G2-4 | 31/M | Not known, none | RE Aniso | 0.58 | +5.0 –2.0 × 120 |
LE | 0.0 | +7.75 –1.0 × 30 | |||
G2-5 | 19/M | Detected age 6 years, surgery | RE | 0.0 | 0 –0.5 × 165 |
LE Strab | 0.55 | −1.0 –0.75 × 15 | |||
G2-6 | 24/F | Not known, none | RE Strab | 0.7 | −5.0 –0.75 × 180 |
LE | 0.0 | −4.5 –1.25 × 170 | |||
G2-7 | 19/F | Not known, none | RE Aniso | 0.38 | +8.0 –2.0 × 175 |
LE | 0.0 | +3.25 –1.5 × 165 | |||
G2-8 | 29/F | Detected age 8 years, none | RE Aniso | 1.0 | −1.25 –1.0 × 85 |
LE | 0.0 | +3.75 –0.75 × 165 |
G1 participants who received anodal-transcranial direct current stimulation (tDCS) first (group 1), G2 patients who received sham-tDCS first (group 2), M male, F female, RE right eye, LE left eye, Aniso anisometropic amblyopia, Strab strabismic amblyopia
Study Design
A sham-controlled, cross-over, double-blind study design was adopted (Fig. 1). Participants were randomized into 2 groups. Both groups received an identical dichoptic treatment regimen of 10 sessions lasting 65 mins. Both groups also received tDCS during the first 15 mins of each treatment session; however, group 1 received a-tDCS of the visual cortex during the first 5 training sessions and motor cortex tDCS [sham-tDCS (s-tDCS)] during the second 5 sessions. In group 2, the order of tDCS conditions was reversed.
Measurements of best-corrected visual acuity and stereopsis were made prior to the first training session (pre), after 5 days of treatment (post-5d) and after 10 days of treatment (post- 10d). In 8 available patients, visual acuity and stereopsis were also measured at 2 weeks (post- 2w) and 3 months (post-3 m) after the final treatment session.
Clinical Assessment
Visual acuity was measured using a tumbling E chart with decimal progression presented using a Topcon ACP-8 projector and viewed from a distance of 3 m. A forced-choice testing method was employed. Lines 1.0–0.2 contained 5 optotypes, lines 0.18–0.05 contained 3 optotypes, and visual acuity was scored using the standard technique of subtracting 0.02 or 0.03 logMAR units, respectively, for each correctly identified optotype. Stereopsis was assessed using the Randot Stereo Test at a 40-cm viewing distance. This test relies on dichoptic separation of 2 disparity-shifted images using polarized glasses and requires patients to detect shapes presented in depth. Measurements of stereopsis can be made in the range of 800 to 40 seconds of arc. Clinical data were collected by an investigator masked to the grouping of the participants.
Dichoptic Treatment
Dichoptic treatment was administered in a clinical assessment room using an iPod touch equipped with a lenticular overlay screen. The videogame-based treatment is described in detail elsewhere [23]. In brief, it consists of a modified version of Tetris, which requires the player to tessellate falling blocks together [23]. Some blocks are presented to the amblyopic eye at high contrast, some to the fellow eye at low contrast, and some to both eyes to aid fusion. Successful game play can only occur if suppression of the amblyopic eye is overcome, thereby allowing all bocks to be perceived simultaneously.
Participants were seated in a chair with their head placed in a chinrest to ensure exact alignment of the lenticular screen. The iPod touch was controlled using a Bluetooth keyboard. Interocular suppression was assessed at the start of each treatment session using an established psychophysical technique that provides a measurement of the interocular contrast difference required to overcome suppression of the amblyopic eye [13, 40, 41]. This technique has recently been modified to allow for measurements to be made in the context of high anisometropia [42]. The suppression measurement was used to set the contrast of the Tetris blocks presented to the fellow eye; amblyopic eye blocks were always presented at 100 % contrast.
Each treatment session was divided into 3 blocks of Tetris play. The first block lasted 15 mins and the second 2 blocks lasted 25 mins. Each block was separated by a 5-min break (Fig. 1). tDCS was delivered during the first block.
tDCS
tDCS was administered using a direct current stimulator (Chattanooga Ionto DJO International, Guildford, Surrey, UK) according to established safety guidelines [43]. This device complies with international electrotechnical commission (IEC) 60601 and is CE-approved. The device is not Food and Drug Administration-approved for tDCS. The stimulating current was delivered via 2 rubber electrodes housed in saline-soaked sponge pockets (Chattanooga Intelect). The sizes of the stimulating and reference electrode were 4 × 6 cm and 8 × 12 cm, respectively. The large size of the reference electrode was chosen to render the electrode inert owing to a low current density [44].
For the a-tDCS condition the stimulating and reference electrode were positioned over Oz and Cz, respectively [28, 45–50], as defined by the 10–20 electroencephalography coordinate system [51].The direct current was ramped up to 2 mA, kept constant for 15 mins, and then ramped down.
Sham stimulation differed from real stimulation in 2 ways. First, sham tDCS was only delivered for 30 s, whereby the current was ramped up to 2 mA and then turned off out of view of the patient [51]. Second, the tDCS electrodes were placed over the motor cortex to ensure that the 30-s period of stimulation could not influence visual cortex function. The stimulating electrode was placed over the nondominant primary motor cortex and the reference electrode was placed over the dominant primary motor cortex (corresponding to 10–20 electroencephalography positions C3 and C4).
Statistical Analysis
Prior to statistical analysis, visual acuity measurements were converted to logMAR units and stereoacuity values were converted to stereosensitivity (stereosensitivity = stereoacuity-1), as many patients had no measureable stereopsis prior to treatment (sensitivity of 0). Visual acuity and stereosensitivity measures made after 5 treatment sessions were normalized to baseline measurements (pretreatment) by subtraction. Measurements made after 10 treatment sessions were normalized to the measurements made after 5 treatment sessions by subtraction. In order to assess any a-tDCS-specific effects on the results of dichoptic treatment, mixed analyses of variance were conducted on normalized data with a between-subject factor “group” (group 1 vs group 2) and within-subject factor “time” (post-5d and post-10d). Post hoc analyses were conducted using paired sample t tests. Means and standard error are reported in the text.
Results
No participants reported any adverse effects apart from a slight tingling sensation under the electrodes.
In agreement with previous studies [11, 23, 24], dichoptic training resulted in improved visual acuity and stereopsis. After all 10 treatment sessions 14 of the 16 participants (78.8 %) exhibited improved stereopsis, including 12 participants who had no measurable stereopsis prior to treatment. The mean improvement was 0.003 ± 0.0004 arc s-1 (t15 = −3.382, p = 0.004) (Fig. 2a). The improvement in amblyopic eye visual acuity ranged from 0.16 to 0.53 logMAR and the mean improvement was 0.34 logMAR ± 0.04 SEM (t15 = 8.725, p < 0.0001) (Fig. 2b). There was a strong positive correlation (Pearson’s r = 0.955, p < 0.0001) between each patient’s baseline visual acuity (pre) and their visual acuity improvement, indicating that patients with deeper amblyopia exhibited greater acuity improvements (Fig. 2c). This correlation remained significant when each patient’s average acuity before and after treatment (mean of pre and post-10d measurements) was compared with their improvement in visual acuity (r = 0.866, p < 0.0001).
A mixed analyis of variance conducted on the normalized stereopsis data revealed an interaction between time and group (F1, 14 = 10.5, p = 0.006), indicating that the effect of a-tDCS differed significantly from the effect of s-tDCS. As shown in Fig. 3a, a-tDCS enhanced the improvement in stereoacuity (group 1 pre to post-5d t7 = −2.553, p = 0.038; group 2 post-5d to post-10d t7 = −3.55, p = 0.009), whereas s-tDCS did not (group 1 post-5d to post-10d t7 = −1.256, p = 0.250; group 2 pre to post-5d t7 = −1.323, p = 0.227). It is notable that across both groups 12/16 patients experienced improved stereopsis when dichoptic treatment was combined with tDCS compared with 4/16 when dichoptic treatment was delivered alone.
Unlike the stereosensitivity measurements, there was no interaction between time and group for the amblyopic eye visual acuity data (Fig. 3b), indicating no difference between a-tDCS and s-tDCS for this measure.
Clinical measurements made at post-2w and post-3 m after the combined treatment in a subset of 8 available patients indicated that the improvements remained stable for both stereopsis (pre to post-2w t5 = −2.611, p = 0.048; pre to post-3 m t5 = −2.445, p = 0.058) and visual acuity (pre to post-2w t7 = 5.36, p = 0.001; pre to post-3 m t7 = 5.841, p = 0.001) (Table 2). Although the post-3 m results for stereopsis were statistically marginal, none of the patients that improved returned to their baseline levels of stereopsis (Table 2).
Table 2.
ID | Amblyopic visual acuity (logMAR) | Stereosensitivity (arc s-1) | RDK suppression (% contrast) | ||||||||||
---|---|---|---|---|---|---|---|---|---|---|---|---|---|
Pre | Post-5d | Post-10d | Post-2w | Post-3 m | Pre | Post-5d | Post-10d | Post-2w | Post-3m | Pre | Post-5d | Post-10d | |
G1-1 | 0.70 | 0.48 | 0.48 | 0.45 | 0.40 | 0 | 0.00125 | 0.00125 | 0.00125 | 0.00125 | 0 | 28 | 22 |
G1-2 | 1.00 | 0.57 | 0.55 | 0.55 | 0.52 | 0 | 0 | 0 | 0 | 0 | 10 | 29 | 38 |
G1-3 | 0.22 | 0.15 | 0.10 | 0.10 | 0.08 | 0.00125 | 0.00500 | 0.01000 | 0.00500 | 0.00250 | 34 | 50 | 78 |
G1-4 | 0.40 | 0.21 | 0.21 | 0.22 | 0.22 | 0 | 0 | 0 | 0 | 0 | 2 | 15 | 20 |
G1-5 | 0.16 | 0.12 | 0.08 | – | – | 0.00125 | 0.00500 | 0.00500 | – | – | 32 | 65 | 77 |
G1-6 | 0.73 | 0.57 | 0.30 | – | – | 0 | 0.00125 | 0.00125 | – | – | 28 | 36 | 40 |
G1-7 | 0.42 | 0.33 | 0.18 | – | – | 0 | 0.00125 | 0.00250 | – | – | 45 | 100 | 100 |
G1-8 | 1.00 | 0.70 | 0.42 | – | – | 0 | 0 | 0 | – | – | 0 | 13 | 14 |
G2-1 | 0.15 | 0.05 | 0.03 | 0.00 | −0.05 | 0.00125 | 0.00500 | 0.01000 | 0.01000 | 0.01000 | 2 | 33 | 41 |
G2-2 | 1.00 | 0.57 | 0.55 | 0.45 | 0.42 | 0 | 0 | 0.00125 | 0.00125 | 0.00250 | 19 | 100 | 100 |
G2-3 | 1.00 | 0.60 | 0.55 | 0.52 | 0.60 | 0 | 0 | 0.00125 | 0.00250 | 0.00250 | 2 | 15 | 20 |
G2-4 | 0.57 | 0.35 | 0.27 | 0.30 | 0.38 | 0 | 0 | 0.00125 | 0.00125 | 0.00125 | 26 | 37 | 69 |
G2-5 | 0.55 | 0.33 | 0.17 | – | – | 0 | 0 | 0.00250 | – | – | 25 | 37 | 54 |
G2-6 | 0.38 | 0.25 | 0.15 | – | – | 0.00125 | 0.00250 | 0.00500 | – | – | 35 | 48 | 51 |
G2-7 | 0.70 | 0.42 | 0.25 | – | – | 0 | 0 | 0.00125 | – | – | 24 | 29 | 40 |
G2-8 | 1.00 | 0.70 | 0.48 | – | – | 0 | 0 | 0 | – | – | 0 | 16 | 19 |
Measurements of visual acuity, stereosensitivity (s arc-1) and suppression for individual participants. Suppression was measured as the Weber contrast that could be tolerated in the fellow eye when the amblyopic eye was presented with a stimulus at 100 % contrast and larger values indicate weaker suppression (less contrast difference between the eyes was required). Measurements are provided prior to treatment (Pre) after 5 days (post-5d), after 10 days (post-10d), 2 weeks after the final treatment session (post-2w) and 3 months after the final treatment session (post-3 m)
G1 participants who received anodal-transcranial direct current stimulation (tDCS) first (group 1), G2 patients who received sham-tDCS first (group 2); RDK random dot kinematogram
Discussion
This study has produced confirmatory and novel results. First, in agreement with previous work [11, 22–24, 52], we found that a short period (2 weeks) of dichoptic treatment resulted in pronounced and lasting gains in visual acuity and stereopsis in adult patients with amblyopia, and, second, the novel finding that a-tDCS enhances the effect of dichoptic treatment on stereopsis. These results are consistent with the idea that the adult visual cortex has sufficient plasticity to recover function in adulthood [53–55] and provide the first evidence that brain stimulation techniques can augment treatment interventions for amblyopia.
The dichoptic treatment approach used in this study is based on psychophysical studies demonstrating that information from the amblyopic eye is subject to a strong inhibitory drive from the fellow eye prior to binocular combination [56]. The treatment is designed to reduce suppression of the amblyopic eye and therefore improve binocular functions, such as stereopsis [11, 23]. The fact that monocular function also improves, even though the fellow eye is never occluded during treatment, emphasizes the importance of binocular dysfunction in the visual deficits associated with amblyopia [57–59].
Significant gains in visual function achieved by both groups of patients in this study further support the argument that dichoptic treatment is an effective approach to amblyopia therapy [11, 23, 24]. The magnitude of the stereopsis improvements we report after 2 weeks of dichoptic treatment are consistent with previous studies using this technique in adult patients for comparable periods of time [20, 21, 23, 52]. Interestingly, the improvements in visual acuity were 0.15 log units larger than those reported in previous studies using dichoptic treatment and those using patching of the fellow combined with extended periods (40 h) of videogame play [60]. The protocol in the current study allowed for training sessions to be precisely timed and closely monitored. In addition, the interocular contrast offset used within the videogame was calibrated at the start of every session. These factors may have optimized the treatment effects on visual acuity. The fact that 11/16 (69 %) of the patients in the current study had not previously received treatment may also have resulted in large acuity gains as greater improvements may occur in older patients who have not previously been treated [61].
A novel finding of this study was that a-tDCS enhanced the effects of dichoptic treatment for stereopsis. The rationale for the application of a-tDCS to amblyopia is based on previous work showing that a-tDCS reduces gamma-aminobutyric acid-mediated inhibition [28–30], a key mechanism underlying suppression of the amblyopic eye [3, 57]. A reduction in inhibition may also enhance the potential for experience dependant plasticity [15, 29, 62, 63]. It is possible that a-tDCS further reduced suppression of the amblyopic eye, therefore enhancing the effects of dichoptic treatment on stereopsis, which requires precise binocular integration. a-tDCS did not appear to enhance the effects of dichoptic treatment on amblyopic eye visual acuity in this study; however, it is likely that any effect of a-tDCS was masked by the pronounced improvements in visual acuity that occurred with the dichoptic treatment alone.
a-tDCS of the visual cortex has been reported to enhance the rehabilitation of visual field deficits following stroke [36, 37] and non-invasive transorbital alternating current stimulation has been applied to patients with chronic optic neuropathy [64]. Here we have shown for the first time that a-tDCS can enhance treatment effects in adults with amblyopia, raising the possibility that a-tDCS can improve outcomes for adult patients with amblyopia who are typically left untreated.
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Acknowledgments
This work was supported by a Faculty of Science Research Development Fund and Early Career Research Excellence Award, University of Auckland; an Auckland Medical Research Foundation Project Grant; and a Health Research Council Grant to BT; a National Natural Science Foundation of China Grant (81200715); a Thrasher Research Fund for Early Career Award to JL; and a Canadian Institutes of Health Research Grant (53346) to RFH. We thank Dr Long To and Dr Jeremy Cooperstock for their collaboration, and Dr Avinesh Pillai for valuable assistance with the statistical analysis.
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Footnotes
Daniel P. Spiegel and Jinrong Li contributed equally to this work.
Contributor Information
Minbin Yu, Email: max-yu@tom.com.
Benjamin Thompson, Email: b.thompson@auckland.ac.nz.
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