Dear Sir,

We appreciate Dr. Taylor’s interest in our paper as well as drawing our attention to environmental factors that may influence XFS in Australian aboriginal people. Certainly, this is an area that deserves further investigation. Dr Taylor’s review article presents some interesting findings, particularly regarding the high incidence of XFS in Aboriginal individuals. (1)

Consistent with recent literature, Dr. Taylor identified a ‘latitude effect’. Interestingly however, XFS was more commonly observed at lower latitudes, which contrasts other findings of high altitude exposure associated with XFS in an American population. (2)

The recognition of solar radiation exposure as an environmental factor associated with XFS is plausible due to accumulating evidence that supports this relationship. (3) While providing some useful insights, this article justifies the lack of understanding and the need for further research on environmental factors.

1. Taylor HR. Pseudoexfoliation, an environmental disease? Trans Ophthalmol Socs UK 1979; 99: 302- 307
2. Stein JD, Pasquale LR, Talwar N, Kim DS, Reed DM, Nan B, Kang JH, Wiggs JL,Richards JE. Geographic and climatic factors associated with exfoliation syndrome. Arch Ophthalmol. 2011 Aug;129(8):1053-60.
3. Jiwani AZ, Pasquale LR. Exfoliation Syndrome and Solar Exposure: New Epidemiological Insights Into the Pathophysiology of the Disease. International ophthalmology clinics. 2015;55(4):13.

We have read with great interest the e-letter from Karakucuk et al. published in BJO responding to our paper titled ‘Acute retinal toxicity associated with a mixture of perfluorooctane and perfluorohexyloctane: Failure of another indirect cytotoxicity analysis ’ and we appreciate their positive appreciation of our research work.
We consider extraordinarily important that they have reported four more cases in their country, thus, supporting that acute toxicity cases were not a Spanish problem as has been stated by some retinologist at an European congress (Barcelona, September 2017).
We believe that this letter should encourage other colleagues from other countries from all over the world to report cases that certainly exist, according to non-official information from several companies.
We completely agree that the ISO (the International Organization for Standardization) guidelines to determine the in vitro cytotoxicity of intraocular medical devices should be immediately changed. These guidelines should adopt direct cytotoxicity methods to be performed with finished, sterilized, and ready for release products. The analytical method utilized should include cells or tissues close to those of the retina to guarantee specific sensitivity and should be scientifically validated.
We support the suggestion of increasing chemical research, because some companies are promoting chemical tests, as a “safety guarantee”, whose scientific validity and their direct correlation with biological tests has not yet been established. As you mentioned the presence of variable concentrations of non-fully fluorinate compounds are undesirable, but these compounds have not been related to acute toxic pictures such as those mentioned in our paper, and probably in your patients, although they could be the bases of variable intraocular inflammatory responses, that prevent the use of PFO as a long-term endotamponade agent.

Dear Editor:

We read the article ‘Acute retinal toxicity associated with a mixture of perfluorooctane and perfluorohexyloctane: Failure of another indirect cytotoxicity analysis ’ by Coco et al. with great interest.[1] In this study, the authors reported on ocular toxicity due to perfluorooctane (PFO). They advised that the protocols used to determine the cytotoxicity of intraocular medical devices (which have been approved by the Organisation for the Standardisation of International Standards based on indirect methods) should be revised to ensure safety. We congratulate Coco et al.1 for their report because we believe that it has the potential to be a significant contribut or to the literature on this topic.

As is commonly known, PFO is saturated with PFO liquids, which have highly stable carbon-fluorine bonds that consequently make them inert. PFO has highly specific gravity, low viscosity, optical clarity immiscibility in water and interface tension towards water. It is regularly used in vitreoretinal surgery for complex retinal detachment repair because it displaces subretinal fluid and blood anteriorly, unfolds the retina in giant retinal tear cases and provides counter traction and retinal stabilisation during membrane peeling in eyes with proliferative vitreoretinopathy.[2,3] These properties make PFO useful for intraocular surgery. However, some limitations exist regarding PFO use as a long- term tamponade such as amaurosis, a lack of light perception, optic nerve atrophy, acute retinal necrosis and retinal vascular occlusion (both arterial and/or venous) with disseminated haemorrhages.

Notably, there are controversial results regarding PFO toxicity in the literature. [3-9] The present study was one of the few reports to discuss ocular toxicity due to PFO in the last few years.
Using the current study by Coco et al.1 as a foundation, we would like to share our findings regarding the ocular toxicity of PFO. In our clinic, four patients underwent uneventful vitreoretinal surgery with PFO on the same day by two experienced surgeons (BB, SG). Each patient presented with vitritis, hypopyon and acute retinal toxicity, with no increases seen in either postoperative increased intraocular pressure or pain. Figure 1 (https://i.hizliresim.com/6NQWR0.jpg) shows macular atrophy due to PFO toxicity.

Ocular toxicity may be either mechanical or chemical due to inhibition of and/or changes to tissue functionality and/or rearrangement of tissue parts and inflammatory reactions and/or immune reactions that result in function loss. In the past, intraocular injections of aminoglycoside caused occlusive vascular changes, which were attributed to the pH of the antibiotic.[10] The mechanism of PFO ocular toxicity may be similar. In addition, concentration and contact time may lead to toxicity. For instance, in 2013, some cases of acute blindness due to PFO were reported by Chile’s Health Authorities, while four cases were reported in Spain to the Agency of Medicines and Medical Devices. The problems were attributed to careless manipulation of the Turkish product ; variable concentrations of perfluorodecalin were found in the octane, after which the product was withdrawn.

Unfortunately, scientific reports have yet to clarify the causes of acute blindness. These results may help clinicians choose a short-term ocular tamponade when performing a vitrectomy. In addition, when faced with severe early postoperative intraocular inflammation, such as either vitritis or hypopyon, they should use PFO with care due to the possibility of toxicity and consider early systemic steroid treatment.
In conclusion, more chemical research is needed to clarify the acute ocular toxicity of PFO to ensure the safety of human patients. Additionally, immediate updates to both the European and Organisation for the Standardisation of International Standards guidelines for the biological evaluation of ophthalmic devices are needed.

REFERENCES

1. Coco RM, Srivastava GK, Andrés-Iglesias C, et al. Acute retinal toxicity associated with a mixture of perfluorooctane and perfluorohexyloctane: Failure of another indirect cytotoxicity analysis British Journal of Ophthalmology Published Online First: 29 March 2018. doi: 10.1136/bjophthalmol-2017-311471.
2. Loewenstein A, Humayun MS, de Juan E Jr, et al. Perfluoroperhydrophenanthrene versus perfluoro-n-octane in vitreoretinal surgery. Ophthalmology. 2000;107:1078–1082.
3. Abboud EB, Al-Falah M. Nine Years of Retained Perfluoro-n-octane in the Anterior Chamber after Retinal Detachment Repair with No Signs of Ocular Toxicity. Middle East African Journal of Ophthalmology. 2014;21(3):279-282. doi:10.4103/0974-9233.134697.
4. Stefano Zenoni, Mario R Romano, Sonia Palmieri, Natalia Comi, Edoardo Fiorentini, Piero Fontana. Ocular tolerance and efficacy of short-term tamponade with double filling of polydimethyloxane and perfluoro-n-octane. Clinical Ophthalmology 2011:5 443–449.
5. Zeana D, Becker J, Kuckelkorn R, Kirchhof B. Perfluorohexyloctane as a long-term vitreous tamponade in the experimental animal. Experimental perfluorohexyloctane substitution. Int Ophthalmol. 1999;23(1):17-24.
6. Chang S, Sparrow JR, Iwamoto T, Gershbein A, Ross R, Ortiz R. Experimental studies of tolerance to intravitreal perfluoro-n-octane liquid. Retina. 1991;11(4):367-74. PMID: 1813951.
7. Alharbi SS, Asiri MS. Reversible Corneal Toxicity of Retained Intracameral Perfluoro-n-octane. Middle East African Journal of Ophthalmology. 2016;23(3):277-279. doi:10.4103/0974-9233.186160.
8. Pastor JC, Coco RM, Fernandez-Bueno I, Alonso-Alonso ML, Medina J, Sanz-Arranz A, Rull F, Gayoso MJ, Dueñas A, Garcia-Gutierrez MT, Gonzalez-Buendia L, Delgado-Tirado S, Abecia E, Ruiz-Miguel M, Serrano MA, Ruiz-Moreno JM, Srivastava GK. Acute retinal damage after using a toxic perfuoro-octane for vitreo-retinal surgery. Retina. 2017 Jun;37(6):1140-1151. doi: 10.1097/IAE.0000000000001680.
9. Pradeep S, Chhablani JK, Patel B, Rani P. Delayed inflammation associated with retained perfluorocarbon liquid. Indian J Ophthalmol. 2011 Sep-Oct;59(5):396-8. doi: 10.4103/0301-4738.83623. PMID: 21836352.
10. Waltz K, Margo CE. Intraocular gentamicin toxicity. Arch Ophthalmol 1991;109:911.

Figure Legends:
Figure 1: A 34-year-old man with a macula on a bullous retinal detachment of his right eye. His preoperative visual acuity was 16/20. He was operated on with a 23-G pars plana vitrectomy plus SF6 and a laser. One week after surgery, he complained of very low visual acuity, and he had vitritis, hypopyon and acute retinal toxicity. The patient treated with intravenous methylprednisolone ( 1 mg/kg) and topical prednisolone, moxifloxacin, nepafenac eyedrops four times a day during 4 weeks. One month after surgery, profound atrophy of all layers of the retina were seen on optical coherence tomography. His final visual acuity was counting fingers.

Dear Editor,
We read with interest the paper by Gaier et al.1 The collection of 5 eyes affected by acute A-AION and analyzed with OCT-A is remarkable, due to the rare disease presentation. The main finding of the paper was that during the acute phase of A-AION, diffusely dilated superficial peripapillary capillaries were detectable on OCT-A. Interestingly, peripapillary capillary dilatation was also noted in the fellow eye. Unfortunately, the figures presented by the authors are too small to allow the reader to qualitatively appreciate the capillaries dilatation. More detailed images and a quantitative vessels analysis would have helped to document the microvascular changes.
They hypothesized that the capillary dilatation may represent a form of luxury perfusion in the setting of short ciliary arterial compromise or a centrally mediated autoregolatory mechanisms in the setting of reduced perfusion of the optic nerve. These hypotheses are interesting, but it is important to differentiate the RNFL thickness increase from the capillary dilatation, as peripapillary capillary plexus density and RNFL thickness are highly correlated and fit well with a nonlinear stacked-layer model.2
Moreover, the authors stated that OCT-A laminar analysis did not highlight the choroidal/choriocapillaris perfusion defects seen on FA. However, a recent study3 showed a tight correspondence between the choroidal perfusion defects visible on FA (and even better on indocyanine green angiography) and on OCT-A at the level of the choriocapillary in a single case of acute A-AION.
The choroidal defects noted on FA by Gaier et al.1 were slightly distant from optic disc border and they did not fit inside the small scan area of the OCT-A exam. Larger OCT-A scan size could help to highlight choriocapillaris perfusion defect in those cases.

References
1 Gaier ED, Gilbert AL, Cestari DM, Miller JB. Optical coherence tomography angiography identifies peripapillary microvascular dilation and focal non-perfusion in giant cell arteritis. Br J Ophthalmol Published Online First: [2017 Nov 9] DOI: 10.1136/bjophthalmol-2017-310718

2 Jia Y, Simonett JM, Wang J1, et al. Wide-Field OCT Angiography Investigation of the Relationship Between Radial Peripapillary Capillary Plexus Density and Nerve Fiber Layer Thickness. Invest Ophthalmol Vis Sci. 2017;58:5188-5194.

3Balducci N, Morara M, Veronese C, et al. Optical coherence tomography angiography in acute arteritic and non-arteritic anterior ischemic optic neuropathy. Graefes Arch Clin Exp Ophthalmol 2017;255:2255-2261.