key: cord-0682481-msembamw
authors: Banderas García, Sandra; Aragón, David; Azarfane, Brahim; Trejo, Fernando; Garrell-Salat, Xavier; Sánchez-Montalvá, Adrián; Otero-Romero, Susana; Garcia-Arumi, Jose; Zapata, Miguel Angel
title: Persistent reduction of retinal microvascular vessel density in patients with moderate and severe COVID-19 disease
date: 2022-01-11
journal: BMJ Open Ophthalmol
DOI: 10.1136/bmjophth-2021-000867
sha: cc0b0e1888bf235c39ea731e3936749c8c4fc491
doc_id: 682481
cord_uid: msembamw

OBJECTIVE: This study aims to analyse the possible recovery or worsening in retinal microvasculature after 8 months in a previously studied COVID-19 cohort. METHODS AND ANALYSIS: A cross-sectional case–control study and a prospective longitudinal cohort study. Participants were the subjects of our previous study who re-enrolled for a new examination including a fundus photograph (retinography), an optical coherence tomography (OCT) scan and an OCT angiography. COVID-19 diagnosed patients were divided into three groups: group 1: mild disease, asymptomatic/paucisymptomatic subjects who received outpatient care; group 2: moderate disease and group 3: severe disease, both of which required hospital admission because of pneumonia. Statistical analyses were performed using SPSS software (V.23.0). Cross-sectional intergroup differences were analysed by means of analysis of variance for normally distributed variables and the Kruskal-Wallis test for non-normally distributed ones. In reference to the prospective part of the study (intragroup differences, baseline with 8-month comparison), a paired t-test was used for normally distributed data and Wilcoxon signed ranks sum for non-normally distributed data. RESULTS: The fovea-centered superficial and deep vascular densities were significantly diminished in severe cases compared with mild cases (p=0.004; p=0.003, respectively, for superficial and deep) and to controls (p=0.014; p=0.010), also in moderate cases to mild group (p=0.004; p=0.003) and to controls (p=0.012; p=0.024). In the longitudinal study, no significant statistical differences were found between baseline and 8-month follow-up vessel density values. CONCLUSION: We demonstrated persistent reduction in the central vascular area over time in patients with moderate and severe COVID-19.

Microvascular alterations in patients with COVID-19 have recently been described in several organs 1 including the skin, lungs and retina. 2 The SARS-CoV-2 was associated with organ dysfunction and generalised coagulopathy. 3 COVID-19 is believed to bind the angiotensin-converting enzyme 2 (ACE2) receptor located on virtually all endothelia with high affinity. 4 It activates the renin/ angiotensin system leading to a downregulation in ACE2 expression and increasing angiotensin II. Angiotensin II is known to be a potent vasoconstrictor and enhancer of the expression of tissue factor and plasminogen activator inhibitor leading to thrombosis. It also provokes complement activation via formation of reactive oxygen species and downregulation of C1 inhibitor, which increases vascular permeability and cytokine release, enhancing its thrombotic effect. [5] [6] [7] SARS-CoV-2 infection induces a generalised microvascular thrombotic disorder and markedly elevated D-dimer, which has been associated with a worse prognosis of the disease. 8 Retinal vascular changes in the form of decrease in radial peripapillary capillary plexus perfusion density, 9 reduction in vessel density (VD) of foveal area and larger foveal

What is already known about this subject? Open access avascular area 2 10 have been reported in patients with COVID-19 using optical coherence tomography angiography (OCT-A). Funduscopy exams have shown other features that are positively correlated with disease severity such as retinal venous diameter, presence of haemorrhages and cotton wool spots. 11 In a previous study in which we assessed the state of retinal vascularisation via OCT-A in a cohort of 69 patients with COVID-19, we found lower central retina VD of the superficial plexus, in relation to the severity of the infection. 10 OCT-A provides a safe and non-invasive diagnostic way of studying retinal vascular plexuses: superficial capillary plexus (SCP), deep capillary plexus (DCP) and choriocapillaris. 12 OCT-A triton uses a central wavelength of 1.050 nm with 100.000 A-scans per second to detect motion contrast and visualise blood flow in vivo. The OCT-A software uses a commercially available algorithm, OCTRA, which has been shown to provide highly sensitive detection of low blood flow in microvasculature, used in DRI OCT triton equipment. 13 The long-term consequences of COVID-19 on retinal vascularisation are still unknown, as most of the available studies are cross-sectional. 2 10 Here, we provided an 8-month follow-up analysis of our previously studied cohort.

We present a cross-sectional case-control study (8-month follow-up) and a prospective longitudinal cohort study (baseline and 8-month follow-up) performed at the Vall d'Hebron University Hospital (Barcelona, Spain). We included the participants of our previous study (June-July 2020). 10 Cases were defined as patients between 18 and 55 years of age with laboratory-confirmed SARS-CoV-2 infection in the 3 months previous to enrolment in the study (June-July 2020). They were divided into: group 1: mild disease, asymptomatic/paucisymptomatic subjects who received outpatient care; group 2: moderate disease and group 3: severe disease, both of which required hospital admission because of pneumonia. Group 3 subjects developed acute respiratory distress syndrome with intensive care unit stay and interleukin 6 (IL-6) values in excess of 40 pg/mL at some point during hospitalisation. The control group consisted of healthy participants with negative serology for SARS-CoV-2 and any viral symptom in the 4 weeks prior to enrolment.

Exclusion criteria were consistent with the previous study: known prior ophthalmological diseases, myopia greater than −6 dioptres, diabetic retinopathy and active vascular diseases with retinopathy (multiple myeloma, hyperglobulinemia and malignant hypertension). Only one eye per patient is included in the analyses (the left one) in order to minimise the risk of bias.

All case and control subjects were asked to reconsent to participate in the extension phase of the study 8 months later (between 17 November 2020 and 29 January 2021). Data from the baseline examination was compared with the data obtained 8 months later. The control group was reassessed to confirm that they continued to meet the inclusion criteria, that is, no viral symptoms 4 weeks prior to the new assessment and negative serology. A flow chart depicts drop-outs (figure 1).

Neither patients nor members of the public were involved in the design, conduct, reporting or dissemination plans of our research.

A repetition of the same ocular examination from baseline was performed on all the subjects 8 months later: a 50° colour photograph of the retina posterior pole (retinography), a macula-centred high-definition OCT (scan radial 12 mm) and an automatically fovea-centred OCT-A (4.5×4.5 mm) were performed. All three imaging techniques were obtained with the DRI OCT Triton Swept Source equipment (Topcon Corporation, Tokyo, Japan). 

Retinography images and radial OCT sections were analysed by two different ophthalmologists (SBG and DA). A third ophthalmologist carried out a double evaluation of the images (MAZ). A search for any abnormality such as haemorrhages, cotton wool spots or OCT layer hyperreflectivities was carried out.

In contrast to our previous study, we gathered data from automatic segmentation from both superficial capillary plexus and deep capillary plexus from the macular region. Superficial layer VD was automatically segmented: from the internal limiting membrane (ILM) at a depth of 2.6 µm to the inner plexiform layer (IPL)/ inner nuclear layer (INL) at a depth of 15.6 µm. IPL/ INL at 15.6 µm to INL/outer plexiform layer at 70.2 µm automatically encompasses the deep layer VD. The specified software calculated VD, and data were collected from superior, inferior, nasal, temporal and central areas. All captures with a signal strength index of less than 40, incorrect segmentation or motion artefacts were excluded. Figure 2 shows an example of the images obtained.

The area of the foveal avascular zone (FAZ) in the superficial capillary plexus was analysed by means of manual delineation of randomly numbered images with ImageJ Software (National Institutes of Health) by three different blinded observers (SBG, DAR and MAZ). The surface area was measured in square pixels and was converted to square millimetres using the formula given by the software (scale setting): delineated area (mm 2 )=delineated area (pixel 2 )/total surface area (pixel 2 ) * total surface area (mm 2 ). No editing of the image was performed to increase contrast or change colours prior to manual delineation.

Statistical analyses were performed using SPSS (V.23.0) software. Normal distribution of the variables was checked using the Kolmogorov-Smirnov test. In the first part of the study, cross-sectional intergroup differences were analysed (8-month time). Quantitative variables that followed a normal distribution were studied with an analysis of variance (ANOVA) using Bonferroni correction. A Kruskal-Wallis test was performed to compare quantitative variables not normally distributed. Qualitative variables were examined using the χ 2 test. 

In reference to the prospective part of the study (intragroup differences), a paired t-test was used for normally distributed data in order to compare baseline and 8-month changes in the VD mean for superficial plexus as well as for the FAZ mean area. A Wilcoxon signed ranks sum test was used for not normally distributed VD means.

Significance was fixed at p values below 0.05.

We included a total of 75 patients from our previous study 9 who reagreed to participate with no exclusion criteria (figure 1). Control group was formed by 19 subjects. Among patients with laboratory-confirmed SARS-CoV-2 infection, group 1 included 18 participants, group 2 included 21 and group 3 included 17. Mean duration from PCR-confirmed diagnosis to ophthalmological examination time was 8.74 months (SD 0.68) for group 2 and 8.20 months (SD 0.62) for group 3. As in the previous study, there were no statistically significant differences between groups in terms of age, gender, smoking or diabetes record (table 1). The mean age was lower in the control group and group 1 than in groups 2 and 3, with no statistical significance. In reference to ethnicity, there was statistical difference: a predominance of Caucasian origin in all groups with a statistically significant greater presence of Latin origin in groups 2 and 3 (p=0.008).

No new abnormalities in previously healthy colour fundus images and structural OCT sections were found.

No abnormalities attributable to SARS-CoV-2 were found.

In line with our previous findings, there were two subjects who presented asymptomatic small pigment epithelial detachments and one group 2 patient with a small haemorrhage suggestive of a Valsalva manoeuvre (size of approximately 100 µm, round and well-circumscribed under ILM in the premacular area).

At macroscopic scale, no abnormalities such as neovascularisation, ischaemic areas, vascular dilatation or abnormal organisation of vessels were detected after careful consideration of OCT-A images by three observers (SBG, DA and MAZ) either in control or in case groups. The FAZ tended to have a larger area in severe cases, with a statistically significant difference in means among groups (p<0.001, (online supplemental figure 2) and 

Normally distributed data of superficial temporal and nasal deep VD were analysed with ANOVA, and a statistical difference was noted (p=0.002; p=0.010). After Bonferroni correction for multiple measurements, a statistical difference was found only between group 1 and group 2 (p<0.001, p=0.006) with no differences among other groups. Non-normally distributed data from temporal deep VD was analysed using Kruskal-Wallis, with a significant statistical difference in means among groups (p=0.043) which, after a Mann Whitney U test, was found to be between the control group and group 2 (p=0.021) and between group 2 and group 3 (p=0.011).

No other statistically significant results were found. Table 2 shows a summary of all comparisons.

VD differences between male and female within every group were also examined (online supplemental table) as general tendency to lower values in female data were found. The following statistically significant different means were found: superficial central VD at baseline for group 1 was higher in women than men (p=0.034); superficial inferior VD at baseline for group 2 was higher in men than women (p=0.009); deep central VD for group 2 at 8-month follow-up was higher in men than women (p=0.039) also for group 3 at 8-month follow-up (p=0.031); and deep inferior VD for group 2 at 8-month follow-up was higher in women group than men group (p=0.018).

A paired t-test was performed for normally distributed data and a Wilcoxon signed rank test for non-normally distributed variables (table 3) . Comparison of the VD means of every area of the superficial plexus between baseline and its value at the 8 month follow-up was made. FAZ areas are also included in the prospective analysis. No statistically significant differences were found (online supplemental figure 2 ).

The main finding of this study is lower central retinal VD in superficial and deep plexuses in patients who have suffered from moderate and severe COVID-19 pneumonia. This is the first study to provide evidence of the persistence of these findings after 8-month follow-up. Open access SARS-CoV-2 virus is suspected to cause a type of microvascular angiopathy 14 consisting of acute endothelial dysfunction mediated by proinflammatory cytokines such as tumour necrosis factor alpha or IL-6 that lead to an enhanced risk of microvascular thrombosis and eventually multiorgan dysfunction. Direct injury as a result of the infection via this process has been reported in postmortem studies in organs such as brain, 15 liver 16 and kidney. 17 This increase in micro thrombosis could lead to diminished vascular density in affected organs such as the vascular plexuses of the retina.

The severe and moderate infection groups in our study showed signs of respiratory distress and increased IL-6 in the latter group, which are believed to be signs of an underlying thrombotic microangiopathy. 18 IL-6 increase is a sign of inflammation in SARS-CoV-2 disease linked to an unfavourable outcome of the disease and the best predictor for the requirement of invasive mechanical ventilation. 19 IL-6 correlates with macrophage activation in severe COVID-19 cases 20 and seems to have a role in microvascular angiopathy by inhibition of ADMTS-13 activity, raising levels of fibrinogen, plasminogen inhibitor-1 and C reactive protein. 21 22 In our first study, 10 we demonstrated the existence of a reduction in the central VD of the superficial plexus via OCT-A and a tendency to a larger FAZ area. Other groups have ratified our findings with similar results. 2 23 24 There may be three reasons for this: one, ACE2 expressed in the endothelium of the retina 20 with direct effect; two, induced-endothelitis; and three, metabolic changes by serum IL-6 leading to disturbances of the blood retina barrier and dysfunction of vessels. 25 In the present study, reduction of vascular density remains stable after 8 months (online supplemental figure 2 ). This is the most important finding of the present study, that is, the persistence of significant lower VDs in severe and moderate disease. A comparison with the control group to evaluate the impact of ageing was undertaken, which proves the consistency of the persistently reduced central SCP, DCP and enlarged FAZ area, and this correlates with the results of other groups at 6 months. 23 As a tendency to a negative correlation was found regarding sex and central VD in our previous study, 10 we decided to examine possible differences in VD data between male and female groups at baseline and at follow-up (online supplemental material). Guemes-Villahoz et al 23 suggested that women could undergo either slower recovery or progressive worsening of retinal VD and questioned whether this might have any relationship to major persistence of neurological symptoms after the illness in the female population. In our study, VDs of all areas in the female group, although generally lower than in the male group, were mostly no different. We found no other reports in the literature with evidence supporting the possibility that women would be at higher risk of COVID-19 vascular-related events. Further research in this direction is planned.

The long-term consequences of COVID-19 in the retina have not been examined. As far as we know, no clinical or fundoscopic macroscopic abnormalities were discovered at follow-up, such as we could expect as a consequence of the reduced VD. We found only one isolated case report of persistent cotton wool spots on fundus examination at 6 months. 23 For the moment, none of our patients presented any clinical consequences of the microvascular abnormalities evidenced herein. Some studies have tried to relate retinal fibre nerve layer and ganglion cell layer thicknesses with decreases in VD, but no structural correlations have been found. 24 It is still not known whether vasculature structures of the retinal plexuses are more vulnerable to thrombotic events than other body plexuses, as these abnormalities seem to remain clinically silent. We believe long-term follow-up is needed to assess future possible ischaemic/neovascular diseases of the retina, especially in patients who have suffered from severe COVID-19.

If persistent microvascular changes are found in the retina beyond 8 months, it may be presumed that other organs and their plexuses may have sustained longterm damage. Current studies focus their attention on 'persistent COVID-19' 26 and reveal frequencies of up to 72% of concentration ability difficulties, 68% of insomnia, 64% of memory impairment, 75% of fatigue, 55% of tachycardia and 63% of nonproductive cough, Open access among other symptoms. There is currently a controversy regarding the relationship between psychological and functional impairment, systemic consequences and initial severity. Some studies, such as that of Huang et al, 27 did find an association between acute COVID-19 disease severity, persistence of symptoms such as fatigue, weakness, anxiety, impaired pulmonary diffusion capacities and chest imaging abnormalities. Further studies are needed to assess whether recovery symptoms in critical illness patients are comparable with those typically seen in acute respiratory distress syndrome survivors, 28 or whether persistent poor health after COVID-19 is finally not associated with respiratory complications. 29 How perfusion reduction during acute SARS-CoV-2 infection leads to long-term sequelae of the virus in several organs and how this correlates to later symptoms is currently being examined in research papers: pancreatic islets, 30 heart, 31 brain 32 or kidney. 26 If this were the case, VD of the retina measured by OCT-A would be of use as a marker of widespread organ injury in post-COVID-19 patients. Hekimsoy et al 33 have already established a negative correlation between retinal perfusion and idiopathic pulmonary arterial hypertension, a pathology that has been studied in recent times in the context of COVID-19 34 and that results in a higher fatality rate when SARS-CoV-2 infection occurs. Further studies to correlate systemic signs/symptoms are necessary to elucidate this question. Interestingly, perfusion studies with tomography angiography in the lungs and kidneys of COVID-19 patients showed perfusion deficits suggestive of microvascular occlusion with no detectable major dysfunction, similar to our findings. 35 We acknowledge a series of limitations in our study. First, the small sample size of the case cohort, as a consequence of the prospective nature of the study, with reduced number of patients willing to attend a second ophthalmic examination, lower surveillance rates in moderate and severe disease groups, and the study of only one eye per patient. Second, the absence of comorbidities in our population might need to be taken into account when assessing comparability to our studies. Cotton wool spots and retinal haemorrhages are reported in patients with COVID-19 who commonly also have other pre-existing comorbid conditions. 36 We believe that the lack of comorbidities might be beneficial for measuring the real impact of the SARS-CoV-2 infection on VD, since the presence of multiple pathologies might affect its values. Third, no retinal periphery studies have been performed, and we lack any information regarding functional translation of our changes, for example, via electroretinography or microperimetry, which would be of use to state with confidence that there are no clinical consequences. Fourth, a longer follow-up than 8 months should be carried out. Prospective studies on larger cohorts will be needed for follow-up of retinal microvascular abnormalities in post-COVID-19 patients, especially in moderate and severe cases, to detect progression, reversibility or vascular consequences.

In conclusion, this is the first study to find persistently reduced VDs in the retina 8 months after COVID-19 infection. We demonstrate persistent tendency towards a larger FAZ area and reduction in the central area of the superficial and deep plexuses, with correlation to disease severity. Therefore, we believe close follow-up of patients with severe disease should be performed, in order to detect possible long-term systemic and ophthalmological disease sequelae.

Contributors MAZ and SBG made a substantial contribution to the present work in the design of the study, acquisition, analysis and interpretation of data, manuscript drafting and approval of the version of the manuscript to be published. AS-M and SO-R contributed to acquisition of data, conception and design of the study, critical revision for important intellectual content and approval of the version to be published. DA, BA, XG-S and FT participated in the data acquisition, critical revision for important intellectual content and approval of the present version of the manuscript. JG-A's contribution to the present work included conception and design of the study, critical revision for important intellectual content and approval of the present document. SBG is the guarantor and accepts full responsibility for the work, conduct of the study, had access to the data, and controlled the decision to publish. All the authors hereby mentioned meet all four ICMJE criteria for authorship and are accountable for all aspects of the work regarding its accuracy and integrity.

Funding The authors have not declared a specific grant for this research from any funding agency in the public, commercial or not-for-profit sectors.

Competing interests None declared.

Ethics approval The study was approved by the Vall d'Hebron University Hospital ethical committee under the number PR (AG) 337/2020, and all enrolled subjects signed an informed consent statement. Participants gave informed consent to participate in the study before taking part.

Provenance and peer review Not commissioned; externally peer reviewed.

Data availability statement Data are available on reasonable request. All data relevant to the study are included in the article or uploaded as supplementary information. All data relevant to the study are included in the article or uploaded as supplementary information, but additional data are available on reasonable request.

Supplemental material This content has been supplied by the author(s). It has not been vetted by BMJ Publishing Group Limited (BMJ) and may not have been peer-reviewed. Any opinions or recommendations discussed are solely those of the author(s) and are not endorsed by BMJ. BMJ disclaims all liability and responsibility arising from any reliance placed on the content. Where the content includes any translated material, BMJ does not warrant the accuracy and reliability of the translations (including but not limited to local regulations, clinical guidelines, terminology, drug names and drug dosages), and is not responsible for any error and/or omissions arising from translation and adaptation or otherwise.

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Acknowledgements We would like to acknowledge the contribution of the Surgery Department of the Autonomous University of Barcelona (UAB -Departament de Cirurgia i Ciències Morfològiques).