Overlap between telangiectasia and photoreceptor loss increases with progression of macular telangiectasia type 2
Authors:
Paul S. Micevych aff001; Hee Eun Lee aff001; Amani A. Fawzi aff001
Authors place of work:
Department of Ophthalmology, Feinberg School of Medicine, Northwestern University, Chicago, Illinois, United States of America
aff001
Published in the journal:
PLoS ONE 14(10)
Category:
Research Article
doi:
https://doi.org/10.1371/journal.pone.0224393
Summary
Objectives
To examine the topographical correlation between ellipsoid zone loss and telangiectasia in the deep capillary plexus in patients with macular telangiectasia type 2 (MacTel).
Methods
38 eyes (20 subjects) diagnosed with MacTel were imaged with OCTA between March 2016 and June 2019 in this single center, cross-sectional observational study. The en face OCTA and OCT were evaluated for areas of deep capillary plexus telangiectasia and ellipsoid zone loss, respectively, and their outlines were superimposed to study their overlap (mm2). The primary outcome was percentage of overlap and its relationship to MacTel stage. Secondary outcomes included the relationship between neovascularization and hyperreflective foci as well as correlations between ellipsoid zone loss, deep capillary plexus telangiectasia and visual acuity.
Results
In nonproliferative MacTel stage, ellipsoid zone loss was localized to margins of telangiectatic areas (mean overlap = 15.2%). In proliferative stages, ellipsoid zone loss showed a higher degree of overlap with telangiectatic areas (mean overlap = 62.8%). Overlap increased with advancing MacTel stages, with an overall average of 45.3%. Overlap correlated highly with ellipsoid zone loss (r = 0.831; p<0.0001). Telangiectasia was present in all 38 eyes (range: 0.08mm2–0.99mm2), while ellipsoid zone loss was absent in 6 (range: 0.00–3.32mm2). Visual acuity correlated most strongly with ellipsoid zone loss (r = 0.569; p = 0.0002), followed by overlap (r = 0.544; p = 0.0004), and finally, telangiectasia (r = 0.404; p<0.0118). Presence of hyperreflective foci on OCT correlated with the presence and intraretinal location of neovascularization.
Conclusions
Ellipsoid zone loss occurs at the margins of deep capillary plexus telangiectasia in nonproliferative MacTel, with progressively increasing overlap as MacTel advances, peaking in proliferative disease. Deep capillary plexus telangiectasia and its overlap with ellipsoid zone loss are two promising markers of nonproliferative MacTel, while hyper-reflective foci are markers for proliferative MacTel.
Keywords:
Face – Eye diseases – Eyes – Photoreceptors – Visual acuity – Capillaries – Vasculogenesis – Ellipsoids
Introduction
Idiopathic macular telangiectasia type 2 (MacTel) is a rare, acquired macular disease that leads to progressive vision impairment. The pathophysiology of MacTel is believed to be neurodegenerative, characterized by primary loss of supportive Müller cells with secondary, reactive vascular changes.[1] Characteristic vascular and neurodegenerative findings define the disease; these include loss of foveal translucency, crystalline deposits, intra-retinal cavitary lesions, loss of macular pigment, widened capillary spaces, right-angle venules, capillary ectasia, and late-stage neovascularization (outer retinal progressing to subretinal).[2–6] In recent years, optical coherence tomography angiography (OCTA) has been used to better characterize the macular capillary network in MacTel. OCTA has been shown superior to fundus fluorescein angiography (FFA) in visualizing the deep capillary plexus (DCP).[7] The DCP is of particular interest in MacTel as it harbors the majority of vascular changes[3], is poorly perfused (as marked by lower parafoveal vascular density[8, 9]), and may show evidence of MacTel before the superficial capillary plexus (SCP).[10]
MacTel is classically viewed as having nonproliferative and proliferative stages based on the absence or presence of neovascularization.[11] Nonproliferative MacTel has been further subclassified based on the topographical location of vascular anomalies in the SCP and DCP on OCTA.[8, 12] Based on depth of neovascularization, proliferative MacTel can be further subclassified[13] based on location of the neovascularization in the outer retina or in the subretinal space.[14, 15] The classification of MacTel is evolving, and a staging system using OCT and autofluorescence is on the horizon. The newly proposed classification system by Chew et al. delineates MacTel into 7 stages (0–6) based on the presence and location of ellipsoid zone (EZ) loss, presence and location of macular pigmentary deposits, presence of OCT hyperreflective foci (HF), and the presence of subretinal neovascularization–factors shown most influential in progression of disease[16]. One of the limitations of this recent classification is that it does not consider the vascular findings of MacTel, since OCTA was not included in these baseline studies. Given our goal of characterizing the vascular telangiectasia, we relied mainly on OCTA MacTel classifications, with slight modification.[8, 12]
The pathogenesis of the vascular abnormalities in MacTel is thought to be intricately related to neurodegeneration. Studies in mouse models have shown that selective ablation of Müller cells leads to photoreceptor apoptosis and outer retinal neovascularization.[17] These studies suggest a possible causal link between neurodegenerative loss of the photoreceptors and subsequent angiogenesis in the proliferative phase of MacTel, though this relationship has not been explored in human MacTel. EZ loss, a marker of the zone of photoreceptor degeneration, has been shown to be an independent marker of disease severity[18–20] and visual function[21, 22] in MacTel patients. Using OCTA in proliferative MacTel, researchers have shown that the neovascular lesion and the zone of EZ loss show almost complete overlap in eyes with outer retinal neovascularization.[13, 21] However, to better define the entire spectrum of MacTel pathology, it is important to explore these neurovascular pathologies in eyes that span the entire disease spectrum, especially those in the earlier stages.
The relationship between EZ loss and the nonproliferative vascular abnormalities in MacTel has not been previously explored. Furthermore, while EZ loss is a critical component of the pathology, there are no defined markers for the early vascular changes in MacTel. In this study, we therefore set out to study the topographic overlap between DCP telangiectasia (a marker of early vascular pathology in MacTel) and the zone of EZ loss (a marker of neurodegenerative pathology). Quantifiable markers of early MacTel prior to development of EZ loss are scarce, so we explored DCP telangiectasia and the overlap between it and the EZ loss as two potential novel parameters. Based on the strong evidence for neurovascular basis of the pathology in MacTel, we hypothesized that DCP telangiectasia would topographically overlap with regions of EZ loss.
Methods
Subjects
This was an observational, cross-sectional study of 20 patients (38 eyes) diagnosed with MacTel between March 2016 and June 2019 in the Department of Ophthalmology at Northwestern University in Chicago, Illinois. One subject underwent follow up OCTA at 6 months. Written informed consent was obtained from all participants. This research was approved by the Institutional Review Board of Northwestern University, followed the tenets of the Declaration of Helsinki, and was performed in accordance with the Health Insurance Portability and Accountability Act regulations.
Patients underwent OCTA imaging of both eyes during a single clinic visit, as well as color fundus photography, fundus autofluorescence (FAF), and FFA as clinically indicated. Diagnosis of MacTel was made based on characteristic funduscopic findings (perifoveal translucency, inner retinal crystals, non-tapering angled venules, and ectatic capillaries) with typical FFA patterns (telangiectatic capillaries with late-phase hyperfluorescence). All subjects underwent a complete ophthalmological examination, including corrected Snellen visual acuity, which in this study is expressed using the LogMAR scale.
Subjects were staged based on OCTA criteria as follows. Stage I is defined by vascular anomalies temporal to the fovea in the deep or superficial capillary plexus. Stage II is defined by multi-quadrant vascular anomalies in the deep or superficial capillary plexus. Stage III is defined by proliferative MacTel, which we further subdivide into stage IIIa with outer retinal neovascularization and stage IIIb with subretinal neovascularization. For future reference, subjects were also staged using the recently proposed Chew et al. classification.[16] This proposed classification is described in S1 Appendix and its staging criteria are listed in S2 Appendix.
OCTA protocol
All subjects were imaged with RTVue-XR Avanti system (Optovue Inc., Fremont, California, USA). 3x3 mm OCTA scans were acquired for this study. The system captures two consecutive B-scans at each location, including 304 A-scans at a rate of 70,000 scans per second. RTVue-XR Avanti uses a bandwidth of 45mm and a light source centered on 840nm. RTVue-XR Avanti utilizes split-spectrum amplitude-correlation angiography (SSADA) software (version 2017.1.0.151). The SSADA algorithm generates angiographic flow information by quantifying the difference in OCT amplitude (decorrelation) between two consecutive B-scans. Superficial projection artifacts were reduced by using the built-in flow artifact removal software.
Image analysis
Default segmentation parameters were used to study the macular capillary beds separately as en face angiograms of the SCP and DCP. The SCP is segmented from the inner limiting membrane (ILM) to 55μm above the inner plexiform layer (IPL). The DCP is segmented from 6μm above the IPL to 50μm below the IPL. En face OCT of the EZ was segmented by manually adjusting the choriocapillaris slab to center onto the EZ, as visualized on cross-sectional OCT. We imported 3x3mm images of the SCP, DCP, and EZ into Photoshop software (Adobe systems, San José, CA) for superimposition and area calculations.
Telangiectatic vessels in the DCP were identified as non-tapering or dilated capillaries and traced individually. One or more circumscribed areas encompassing the telangiectatic vessels were subsequently quantified using Photoshop. The primary exclusion criteria for telangiectatic-appearing changes was superficial vessel artifact, so all focal areas suggestive of DCP telangiectasia were cross-referenced for overlying SCP artifact. A second masked examiner evaluated telangiectasia in a random sample of 10 eyes to study reliability of this measurement. Areas of EZ loss were identified on en-face OCT as dark or hyporeflective regions that demonstrated a concurrent EZ defect on cross-sectional OCT, as has been done in prior studies.[13] Areas of en-face hyporeflectivity without a topographically associated EZ defect on cross-sectional OCT were excluded due to minimize any potential for shadowing from overlying retinal pathology. Subsequently, maps of DCP telangiectasia were superimposed onto EZ loss maps to illustrate regional overlap. Areas of telangiectasia, EZ loss, and their overlap were quantified in mm2 on Photoshop. Total pixels were divided by the square resolution of each image (pixels/mm)2 to generate units of area in mm2. Percentage of overlap was calculated relative to telangiectasia and stratified by disease stage.
Statistical analysis
Pearson correlation coefficients were calculated for relationships between area of EZ loss, telangiectasia, percent overlap, and visual acuity (LogMAR). As a proxy of inter-rater reliability, an intraclass correlation (ICC) value was calculated for telangiectasia area measurements comparing the two graders. Two-tailed t-tests were performed to evaluate the difference in percent overlap between groups of MacTel subjects using the OCTA and OCT-based stages. We performed all statistical analyses using JMP 14.0 software (SAS Institute, Cary, NC, USA) and significance was set at p<0.05.
Results
Subject demographics, visual acuity, and OCTA-based disease stages are reported in Table 1. For reference, recently proposed OCT-based (Chew et al.) disease stages are listed in S2 Appendix. To assess reliability of the telangiectasia measurement, we quantified inter-rater reliability (ICC = 0.85; p = 0.0002) in 10 randomly selected eyes. Superimposition of telangiectasia maps onto areas of EZ loss unveiled a dynamic relationship between DCP telangiectasia and EZ loss, as illustrated in Figs 1 and 2. All 38 eyes (100%) showed evidence of DCP telangiectasia on OCTA, whereas only 32 of 38 eyes (84.2%) demonstrated evidence of EZ loss. EZ loss was predominantly localized to margins of telangiectasia areas in early OCTA-based stages (stages I-II). In more advanced, proliferative disease (stages IIIa-IIIb), EZ loss overlapped more centrally with areas of telangiectasia and neovascularization.
Overall, the mean percentage of telangiectasia-EZ overlap was 45.3% (standard deviation 0.35; range 0.0–1.0). As shown in Fig 3, the degree of overlap increased with progressive EZ loss, showing a strong linear correlation (r = 0.831; p<0.0001). Visual acuity correlated most strongly with EZ loss (r = 0.569; p = 0.0002), followed by overlap (r = 0.544; p = 0.0004), and finally, telangiectasia (r = 0.404; p<0.0118). Using OCTA staging, the overlap increased progressively with advancing disease stage; stage I: 2.22% stage II: 28.2%, stage IIIa: 47.4%, stage IIIb: 72.0%. There were statistically significant differences between nonproliferative stage I and nonproliferative stage II (p<0.0441), as well as between proliferative stages (IIIa-IIIb; 62.8%) and nonproliferative stages (I-II; 15.2%; p<0.0001), and between outer retinal and subretinal proliferative stages (IIIa and IIIb; p<0.0447). We also evaluated our findings using OCT-based Chew et al. staging[16], as shown in S3 Appendix. Similar to the OCTA staging mean overlap generally increased with advancing disease stage; stage 0: 0%, stage 1: 16.8%, stage 2: 13.9%, stage 3: 45.9%, stage 4: 51.2%, stage 5: no subjects, stage 6: 72.0%. There were significant differences between grouped stages 0–2 and 3–5 (p = 0.0003), as well as between grouped stages 3–5 and stage 6 (p = 0.0410).
Two eyes with DCP telangiectasia without EZ disruption are displayed in Fig 4. An eye with stage IIIb subretinal proliferative MacTel demonstrating 100% overlap between EZ loss and telangiectasia is shown in Fig 5. Only mild telangiectatic change is visible on fundus photography or FFA, but significant distortion and dilation is seen on OCTA of the DCP.
Baseline and 6-month follow-up imaging were analyzed in one subject, as illustrated in Fig 6. DCP telangiectasia and EZ loss showed subtle topographical dynamic changes. Most prominently, the small area of EZ loss at baseline showed recovery and disappeared at 6 months.
The presence of HF on OCT reflected the presence and depth of neovascularization (Figs 2 and 5). HF were present in 100% of subjects (15/15) with subretinal neovascularization (stage IIIb), 77.8% of subjects (7/9) with outer retinal proliferation (stage IIIa), and only 7.1% of subjects (1/14) without neovascularization (stage I-II).
Discussion
In this pilot study, we sought to examine the intricate relationship between vascular and neurodegenerative changes in MacTel by exploring the topographical relationship between EZ loss and DCP telangiectasia. We originally hypothesized that areas of EZ loss would directly overlie areas of telangiectasia, but instead found that the topographical relationship varies by disease stage, as visualized in Fig 2. Qualitatively, telangiectasia was located along the margins of EZ loss in early MacTel (stages I-II; Fig 1) and more centrally overlapping in late, proliferative disease (stages IIIa-IIIb; Fig 5). Quantitatively, this was reflected by a stepwise increase in overlap with increasing disease stage as well as by the linear correlation between overlap and EZ loss, as shown in Fig 3.
The topographical relationship, with central photoreceptor loss surrounded by telangiectasia, is consistent with the prevailing hypothesis on MacTel pathogenesis. Neurodegenerative changes in MacTel, characterized by the loss of Müller cells and ensuing loss of photoreceptors, are believed to precede and cause the vascular abnormalities.[1, 17] Novel therapies for MacTel target Müller cell dysfunction through ciliary neurotrophic factor (CNTF) therapy and have been shown to slow photoreceptor degeneration in preclinical models by activating gp130 receptor in Müller cells.[23] Surgical implantation of slow-release intravitreal CNTF has shown promise in slowing retinal degeneration in subjects with MacTel.[24] From a pathophysiologic perspective, mouse models have shown that photoreceptor loss can promote a local pro-angiogenic environment leading to outer retinal neovascularization.[25–27] In the normal retina, photoreceptors synthesize and release an endogenous inhibitor of vascular endothelial growth factor A (VEGF-A), known as soluble VEGF receptor-1 (sFLT-1).[28] This molecule is thought to play an important role in establishing and maintaining the normal avascularity of the outer retina.[28] Using immunostaining methods, sFLT-1 levels have been shown to decrease in eyes with age-related macular degeneration, which, like MacTel, can exhibit vascular invasion of the outer retina.[28] Other factors that inhibit outer retinal neovascularization include very low-density lipoprotein receptor (VLDLR) expression.[25] VLDLR knockout mice exhibit retinal neovascular changes similar to those seen in type 3 neovascularization.[25] Derangements in these anti-angiogenic signaling mechanisms may explain the topographical relationship between EZ loss and telangiectasia in early MacTel, as well as the outer retinal vascular invasion in proliferative stages of MacTel.
Interestingly, vascular changes are already present in MacTel prior to the development of outer retinal neovascularization, most prominently in the DCP as reflected in the OCTA grading paradigm.[8, 12] It is not well understood whether the loss of photoreceptors plays a role in influencing these earlier vascular changes, prior to development of outer retinal neovascularization. Based on our results, we propose that “photoreceptors at risk” along the margins of EZ loss (and before the development of structural abnormalities) may be the initial source of signaling to the overlying vasculature. We propose that subclinical dysfunction in these photoreceptors may suppress the normal antiangiogenic signaling. As the neurodegenerative process progresses, areas of photoreceptor loss accrue. As EZ loss and antiangiogenic signaling is further disrupted, telangiectasia worsens culminating in the development of outer retinal neovascularization. This is supported by our results that show stepwise increase in overlap between telangiectasia and EZ with advancing disease stage on OCTA, suggesting progressive disruption of these vascular barriers as photoreceptor compromise advances. To further confirm this result, we examined the degree of overlap in our dataset against the recently proposed OCT-based MacTel clinical classification.[16] As shown in S3 Appendix, we found that the overlap progressively increased with advancing stage using this scale as well, an encouraging finding that confirms our hypothesis. This result needs to be further validated in larger datasets.
Current models suggest that photoreceptor loss induces vascular change, so it may seem paradoxical that 6 subjects were identified with telangiectasia without evidence of EZ loss. To explain these results, we would like to distinguish photoreceptor loss (marked by EZ loss on OCT) and “photoreceptors at risk” where preclinical dysfunction is not yet visible as structural EZ loss. We propose that these photoreceptors at risk may be responsible for the zones of telangiectasia. The implication of this finding is that DCP telangiectasia could predict the locations of future EZ deficits along its margins. Taken further, the area of telangiectasia at the DCP may therefore be a quantifiable marker of disease severity. Telangiectasia may be particularly relevant as a marker of early stages (I-II) of MacTel, when other established pathologies, such as presence of outer retinal neovascularization, EZ loss, or HF, may not yet be apparent. Several other findings in this study suggest that telangiectasia area may be a useful marker of early disease progression. First, we show that the total area of telangiectasia correlated significantly with visual acuity. Secondly, the qualitative OCTA findings in our 6-month return MacTel subject (Fig 4) show that areas of telangiectasia, as well as EZ loss are highly dynamic, and while EZ loss completely disappeared, telangiectasia did not. Future studies are needed to further evaluate whether these dynamic changes reflect improvement or progression of disease.
We also document an association between HF and neovascularization that warrants further discussion. We found that the vast majority of HF were associated with neovascular lesions (either intraretinal or subretinal). The presence of HF could signal underlying neovascularization, which, especially if intraretinal, may go unnoticed when OCTA is not available. This finding is supported by a recent OCTA-based study using the presence of HF as an identifying feature of neovascularization in MacTel.[20] In line with our findings, this study also found a correlation between progressive vascular abnormalities (culminating with neovascularization as marked by HF) and progressive EZ loss.
Our study should be considered with an understanding of its limitations. Our sample size in a single center (38 eyes) is relatively small, consistent with the low prevalence of MacTel. We used a manual method to outline and quantify areas of telangiectasia in this study, which had sufficient inter-rater agreement (ICC = 0.85), but could still benefit from automated methods to improve accuracy and reliability. OCTA stages, as used in this study, have not been widely validated and their correspondence with disease severity remain unknown–another valuable area of future study. For this reason, we also examined our findings using the recently proposed OCT-based clinical classification from Chew et al.[16] Moreover, our cross-sectional study was designed to evaluate disease at a single point in time, so we are not able to evaluate how EZ loss and telangiectasia evolve over time in an individual. Future studies with serial multimodal imaging are needed to further explore these neurovascular pathologic relationships over time. Moreover, future investigation with AO-SLO for subtle photoreceptor changes at the margins of EZ loss would be valuable to investigate the hypothesis and anatomic correlates of “photoreceptors at risk” in MacTel.
In conclusion, this study offers new insight into the early pathogenesis of MacTel and fits well within the current understanding of disease pathogenesis. We found an evolving topographical relationship between EZ loss and telangiectasia, which increased as a function of disease progression from minimal overlap in nonproliferative to complete overlap in proliferative stages, where HF are a key feature. Furthermore, we found the degree of overlap progressively increases with increasing stage based on the OCTA-based classification as well as the recently proposed OCT classification.[16] Finally, we found that the total area of DCP telangiectasia and its overlap with EZ loss correlate inversely to visual acuity and that telangiectasia may present prior to EZ loss in MacTel. Overall, we propose that DCP telangiectasia and the degree of overlap with EZ loss may present two novel parameters that could provide important insights in the early stages of MacTel and suggest future longitudinal studies to examine this relationship, as well as the concept of “photoreceptors at risk” in greater detail.
Supporting information
S1 Appendix [docx]
Abstract for Chew et al. classification.
S2 Appendix [docx]
Staging of MacTel using OCT-based Chew et al. criteria.
S3 Appendix [docx]
Degree of overlap across disease stage using OCT-based Chew et al. criteria.
Zdroje
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