To the Editor,
We read with great interest the article entitled “Central corneal basal cell density and nerve parameters in ocular surface disease and limbal stem cell deficiency: a review and meta-analysis”. In the analysis, the authors found a similar reduction of basal cell density (BCD) and corneal nerve parameters between the limbal stem cell deficiency (LSCD) group and the ocular surface disorders (OSD) group. However, several missteps in the study methods occurred.
First, the analysis included ocular diseases that could lead to LSCD in the OSD group (eg, severe and chronic vernal and atopic keratoconjunctivitis, bullous keratopathy, and ocular graft-versus-host disease).[1] Second, acute microbial infectious keratitis, which is generally not considered as an OSD because of its distinct pathology, was included in the OSD group. Third, the severity of LSCD and OSD was not considered in the analysis. As previously demonstrated, the decrease in BCD and basal nerve density is positively correlated with LSCD severity.[2 3] Fourth, the overall sample size was very small. Lastly, no sensitivity/meta-regression analysis was done despite the significant heterogeneity in the OSD group.
We repeated the analysis after removing 7 studies wrongly included into the OSD group (Al-Aqaba &al, Leonardi &al, Muller &al -2 reports-, Moein &al, Cavalcanti &al, Tepelus &al) and not including them in the LSCD group because of heterogeneity of the study populations. We found a significant difference in the weighted mean difference of corneal nerve fiber length (P = 0.003) and a trend for a significant reduction in BCD (P = 0.06) in the LSCD group.
Because of the significant flaws in the study methods, the results of the analysis are incorrect and the conclusions are misleading. Understanding the pathophysiology and clinical characteristics of diseases is necessary to conduct a meaningful and sound meta-analysis.

Clemence Bonnet, MD, Tran Tu, MS, Sophie X. Deng, MD, PhD

References
1. Deng SX, Borderie V, Chan CC, et al. Global Consensus on Definition, Classification, Diagnosis, and Staging of Limbal Stem Cell Deficiency. Cornea 2019;38(3):364-75 doi: 10.1097/ICO.0000000000001820[published Online First: Epub Date]|.
2. Chan EH, Chen L, Rao JY, Yu F, Deng SX. Limbal Basal Cell Density Decreases in Limbal Stem Cell Deficiency. Am J Ophthalmol 2015;160(4):678-84 e4 doi: 10.1016/j.ajo.2015.06.026[published Online First: Epub Date]|.
3. Chuephanich P, Supiyaphun C, Aravena C, Bozkurt TK, Yu F, Deng SX. Characterization of the Corneal Subbasal Nerve Plexus in Limbal Stem Cell Deficiency. Cornea 2017;36(3):347-52 doi: 10.1097/ICO.0000000000001092[published Online First: Epub Date]|.

Optic disc drusen pose a diagnostic challenge when trying to differentiate between papilloedema and pseudopapilloedema.1 Dahlman-Noor et al highlight the importance of a structured history when evaluating children with optic nerve head (ONH) swelling. The authors recommend a future study to explore the diagnostic accuracy of an algorithm published by the Royal College of Paediatrics and Child Health (RCPCH) which details key features of the history (e.g. headache, vomiting, visual symptoms) that should trigger neuroimaging.2

As part of a prospective study of children referred to our regional paediatric ophthalmology service for assessment for ONH swelling, we implemented this algorithm. 122 children under 16 years of age were assessed from 1st January to 31st December 2018. 93% (113/122) had optic disc drusen, 4% (5/122) had normal optic discs, and 3% (4/122) had papilloedema. Two cases of papilloedema were caused by idiopathic intracranial hypertension (IIH) and two by venous sinus thrombosis.

Of the 118 patients with drusen or normal discs, only one fulfilled the RCPCH criteria for neuroimaging: a 14-year-old girl with persistent headaches and vomiting. Neuroimaging and lumbar puncture were unremarkable, and her symptoms were ultimately attributed to migraine.

For the four patients with papilloedema, the algorithm-derived questions would have triggered neuroimaging in three cases. This yields a specificity of 99% but a sensitivity of only 75%.

One patient with IIH did not fulfil the criteria for neuroimaging. This 13-year-old girl was asymptomatic despite having marked bilateral optic disc swelling and raised intracranial pressure. The ONH abnormalities were identified on routine optometric examination.

The high specificity of the RCPCH algorithm indicates that when the screening questions are positive, it is likely that a child has intracranial pathology and neuroimaging is justified. However, in our cohort, the sensitivity was insufficient for the algorithm to act as a screening tool in isolation.

 
1. Chang MY, Velez FG, Demer JL, et al. Accuracy of Diagnostic Imaging Modalities for Classifying Pediatric Eyes as Papilledema Versus Pseudopapilledema. Ophthalmology. 2017;124(12):1839-1848.
2. Walker D, Grundy R, Kennedy C et al. The diagnosis of brain tumours in children. www.rcph.ac.uk/bpp.

We read with interest the BMJ Editorial Novel Coronavirus disease 2019 (COVID-19): The importance of recognising possible early ocular manifestation and using protective eyewear1. This highlights the need for risk mitigation in the context of commonplace eye examinations using the slit-lamp biomicroscope and direct ophthalmoscope, both requiring very close proximity manoeuvres within a few centimetres of the patients’ eye, nose and mouth. Droplet spread during eye examination likely increases during these prolonged direct examination techniques. Those at most risk are trainees working in accident and emergency, opticians or acute care settings who are required to see patients presenting with “red eye” for which conjunctivitis is a common cause.

Patients with conjunctivitis can be safely manged by the non-specialist using simple observation and history enquiry2 supplemented by a phone captured image. Remote-site consultation allows further discussion allowing an eye image and clinical details to be scrutinised without the requirement for on-site attendance. Currently, clinicians use mobile phone consultations to supplement and enhance care provision and it would seem prudent to adopt this more widely to minimise risk of Covid-19 transmission which might be acquired through public transport travel, waiting room exposure or face to face consultation. Notwithstanding confidentiality issues of commonly used freeware with private image messaging capabilities e.g Whatsapp, secure ophthalmology data transmission, for example “Attend Anywhere” have been evaluated in Scotland (Livingstone I personal communication) and might be usefully adopted more widely3.

Ophthalmology is one of the highest patient volume specialties with an elderly patient demographic attending for chronic age-related eye diseases often with systemic co-morbidities rendering them a high-risk vulnerable group. To our knowledge there is no consistent UK-wide policy for protecting patients or professionals from Covid-19 transmission in the eye care setting. In the current climate of escalating Covid-19 numbers we suggest remote-site diagnosis using external eye image capture and/or video-consultation to be rapidly adopted by ophthalmologists as a risk mitigating, cost-effective approach to efficient triage and remote site management for all patients with the symptoms and signs of conjunctivitis who should not be referred to on-site hospital eye services.

References
1. Li J, Lam D, Chen Y, et al. Novel Coronavirus disease 2019 (COVID-19): The importance of recognising possible early ocular manifestation and using protective eyewear. Br J Ophthalmol 2020;104(3):297-298
2. Timlin H, Butler L, Wright M. The accuracy of the Edinburgh Red Eye Diagnostic Algorithm. Eye (Lond) 2015; 29(5): 619–624
3. Poyser O, Livingstone I, Ferguson A, et al. Real-Time Tele-Ophthalmology in the Emergency Department.) Invest. Ophthalmol. Vis. Sci. 2019;60(9):6124

There is no unified consensus in the peripheral nerve literature regarding the optimum type of interposition nerve graft for target tissue reinnervation. There are multiple well-designed peer reviewed studies by leading experts in peripheral nerve surgery supporting the use of acellular nerve allografts (ANAs) as viable alternatives to nerve autografts at various gap lengths [1-3]. While there are no trials directly comparing the use of ANAs to nerve autografts in corneal neurotization, Avance® allografts have now become “on label” for corneal neurotization given the successful clinical outcomes reported by several tertiary care centers [4].

In comparing the study by Catapano et al. to the study by Leyngold et al. it is important to note that the average follow up in the former was 24 months whereas it was only 6 months in the latter [4,5]. In addition, 88% of the patients in the paper by Catapano et al. were under 18 years of age vs. 14% in the paper by Leyngold et al. As stated in my previous correspondence, Park et al has shown that pediatric age is correlated to improved results in corneal neurotization irrespective of the technique [6]. Catapano et al. noted continued improvement in central corneal sensation (CCS) up to two years postoperatively. The reported CCS at 6 months postoperatively was only 30.0±26.8mm with a significant number (44%) of patients in their study having CCS at or below 10mm and peripheral corneal sensation (PCS) at or below 30mm at that time. Among the three patients (43%) reported by Leyngold et al. who had corneal sensation measurements under 35mm one had a follow up of only 3 months, second patient achieved an improvement of 34mm at 10 months after surgery despite multiple medical comorbidities and extensive conjunctival scarring, and the last patient was shown to have corneal nerve regeneration on in vivo confocal microscopy, improved ocular surface and visual acuity despite a small improvement in average corneal sensation. Also, four patients in the study by Catapano et al. were found to have persistent epithelial defects (PEDs) 24 months after the surgery (21%) compared to only 1 patient (14%) reported by Leyngold et al. at 1 month postoperatively.

Finally, the authors state that they “have yet to encounter a suboptimal neurotization outcome with use of nerve autografts to route sensory axons of the great auricular nerve to the cornea” based on only two of their published cases [7]. Such a small number of cases is not sufficient to draw significant conclusions regarding clinical outcomes of their reported technique.

References:
1. Brooks DN, Weber RV, Chao JD, et al. Processed nerve allografts for peripheral nerve reconstruction: A multicenter study of utilization and outcomes in sensory, mixed, and motor nerve reconstructions. Microsurgery. 2012 Jan; 32(1)

2. Zuniga JR, Williams F, Petrisor D. A case-and-control, multi-site, positive controlled, prospective study of the safety and effectiveness of immediate inferior alveolar nerve processed nerve allograft reconstruction with ablation of the mandible for benign pathology. J Oral Maxillofac Surg. 2017 Dec; 75(12): 2669-2681.

3. Rinker BD, Zoldos J, Weber RV, et al. Use of processed nerve allografts to repair nerve injuries greater than 25 mm in the hand. Ann Plast Surg. 2017 Jun; 78(6S Suppl 5): S292-S295. 10.1097/SAP.0000000000001037

4. Leyngold IM, Yen MT, Tian J, et al. Minimally invasive corneal neurotization with acellular nerve allograft: surgical technique and clinical outcomes. Ophthalmic Plast Reconstr Surg 2019;35:133–40.

5. Catapano J, Fung SSM, Halliday W, et al. Treatment of neurotrophic keratopathy with minimally invasive corneal neurotisation: long-term clinical outcomes and evidence of corneal reinnervation. British J Ophthalmol. 2019:bjophthalmol-2018-313042.

6. Park J, Charlson E, Leyngold IM, et al. Corneal neurotization: A review of pathophysiology and outcomes. Ophthalmic Plast Reconstr Surg. 2020; Jan 8. doi: 10.1097/IOP.0000000000001583. [Epub ahead of print]

7. Jowett N, Pineda II R. Corneal neurotisation by great auricular nerve transfer and scleral-corneal tunnel incisions for neurotrophic keratopathy. Br J of Ophthalmol. 2018 Nov 23. pii: bjophthalmol-2018-312563