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

Dr. Leyngold states we ‘fail to support [our] viewpoint with peer reviewed studies.’ Our position against the use of acellular nerve allografts (ANAs) in corneal neurotisation was grounded on robust evidence from basic science literature demonstrating their inferior performance relative to autografts for large gap nerve repair. No clinical trial comparing the two techniques exists, and in our opinion there lacks the necessary equipoise to perform such a study.

The regeneration-restrictive properties of long-segment ANAs renders them unsuitable for use in directing sensory axons to the cornea. The largest single-centre study on Avance® ANA use for peripheral nerve repair demonstrated meaningful recovery in only 54% of cases where allografts longer than 50 mm were employed [1]. Remarkably, exploitation of the suboptimal capacity of ANAs to support nerve regeneration has been proposed as a means to inhibit axon growth in the surgical management of painful neuromas [2].

In his defence of off-label use of Avance® allografts in corneal neurotisation, Dr. Leyngold cites his case-series wherein sensory improvement of 35 mm or more was documented in two of seven eyes (29%). In contrast, Catapano et al. noted sensory improvement of 35 mm or more in 16 of 18 cases (89%) where nerve autografts were employed to route healthy trigeminal sensory axons to anaesthetic corneas [3]. In our own experience, we 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 [4].

When counselling patients on corneal neurotisation, surgeons need be aware of the considerable evidence pointing to a higher risk of procedural failure where ANAs are substituted for nerve autografts. Articles supporting ANA use should be scrutinized for declared or undeclared conflicts of interest that may influence perception of the surgical outcome.

References:
1. Leckenby JI, Furrer C, Haug L, Juon Personeni B, Vogelin E. A retrospective case series reporting the outcomes of Avance nerve allografts in the treatment of peripheral nerve injuries. Plast Reconstr Surg 2019 doi: 10.1097/prs.0000000000006485[published Online First: Epub Date]|.
2. Hong T, Wood I, Hunter DA, et al. Neuroma Management: Capping Nerve Injuries With an Acellular Nerve Allograft Can Limit Axon Regeneration. Hand 2019:1558944719849115 doi: 10.1177/1558944719849115[published Online First: Epub Date]|.
3. 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 Journal of Ophthalmology 2019:bjophthalmol-2018-313042 doi: 10.1136/bjophthalmol-2018-313042[published Online First: Epub Date]|.
4. Jowett N, Pineda Ii R. Corneal neurotisation by great auricular nerve transfer and scleral-corneal tunnel incisions for neurotrophic keratopathy. Br J Ophthalmol 2019;103(9):1235-38 doi: 10.1136/bjophthalmol-2018-312563[published Online First: Epub Date]|.

Given the lack of level 1 evidence there is no unified consensus among peripheral nerve experts on the optimum type of interposition nerve graft for target tissue reinnervation. There are multiple peer reviewed studies by leading experts in peripheral nerve surgery supporting the use of acellular nerve allografts (ANAs) as viable alternatives for peripheral nerve reconstruction at various gap lengths [1-3]. Moreover, as the authors correctly point out in their correspondence, no trials exist comparing the use of ANAs to nerve autografts in corneal neurotization, nullifying their claim of nerve autograft superiority for this procedure. Of note, Avance® allografts have become “on label” for corneal neurotization since my last correspondence.

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. 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. Catapano et al reported mean CCS at 30.0±26.8mm at 6 months postoperatively, 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 the last patient was shown to have corneal nerve regeneration on in vivo confocal microscopy, improved ocular surface and visual acuity. 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]. This quantity of cases is not sufficient to draw any conclusions regarding clinical outcomes of this 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. 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.

5. 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.

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

To the Editor:
We herein respond to the letter written by Camus et al raising the issue of “ultra-low” dose radiation therapy (4 Gy) vs. the “standard low-dose” radiation therapy (24-30 Gy) for lymphomas of the orbit, eyelid, and conjunctiva, also referred to as “ocular adnexal lymphoma” (OAL). First off, it is important to point out that the goals of the retrospective multicenter general review of marginal zone lymphoma coordinated by Professor Steffen Heegaard in Denmark which also included some of our patients from M. D. Anderson was not to compare the efficacy of various treatment strategies.(1) Indeed it is challenging to draw practice altering conclusions from a retrospective multi-center study given the usual limitations, most notably the variation in staging and treatment approaches across various continents as noted by Camus et al.

However, we agree with Camus et al that our encouraging preliminary observations in 22 patients with OAL treated with ultra-low dose radiation therapy (4Gy) suggested a very good response rate (100% ORR:86% CR, 14%% PR) for B-cell orbital and ocular adnexal lymphomas;(2) as such we started a prospective trial of ultra-low dose radiation for ocular adnexal lymphoma patients at MD Anderson Cancer Center soon thereafter (Clinicaltrials.gov identifier NCT02494700)The study aims to evaluate the efficacy of response adapted radiation therapy for this patient population, whereby all patients are treated to an initial 4 Gy in 2 fractions and the additional 20 Gy (to complete the current standard of care radiation therapy dose of 24 Gy, is reserved for non-responders). The total accrual goal for this prospective trial is 50 patients; to date we have enrolled 41 patients in this prospective trial and have also treated at least 30 additional patients off protocol with the ultra-low dose regimen (inclusive of the patients reported in our initial retrospective analysis). We fully expect to publish the results of this prospective trial in a major oncology journal once the total accrual goal is reached. Based on our interim analysis and our collective observations in over 70 orbits treated with ultra-low dose radiation therapy (4Gy) at MD Anderson to date, we are optimistic that this significant lowering of dose of radiation therapy will be a major paradigm shift for management of low grade ocular adnexal lymphomas in routine practice in the future.

As Camus et al pointed out this much lower dose of radiation therapy is associated with significantly less ocular toxicity, it is less expensive, more convenient for patients (only two sessions of radiation), and importantly can also be repeated in cases of relapse or progression over time in the orbit. With regards to the issue of follow up time, we have been carefully following our original 22 patients treated with ultra-low dose radiation (4 Gy) and published in 2016.(2) We plan to publish a follow-up study on those original 22 patients once the median follow up time gets closer to 5 years. This may coincide with the publication of our prospective trial data and hopefully the two follow up publications will decrease the understandable sense of “dilemma” expressed by Camus et al regarding the ideal radiation dose for low grade , stage IE, ocular adnexal lymphomas.

Corresponding Author:
Bita Esmaeli, MD, FACS
Orbital Oncology & Ophthalmic Plastic Surgery
Department of Plastic Surgery
The University of Texas MD Anderson Cancer Center
1515 Holcombe Blvd, Unit 1488, Houston, Texas 77030
Tel: 713-792-4457. Fax: 713-794-4662

1. Hindsø TG, Esmaeli B, Holm F, et al. International multicentre retrospective cohort study of ocular
adnexal marginal zone B-cell lymphoma. Br. J. Ophthalmol. 2019;bjophthalmol-2019-314008.
2. Pinnix CC, Dabaja BS, Milgrom SA, et al. Ultra-low-dose radiotherapy for definitive management of
ocular adnexal B-cell lymphoma. Head Neck. 2017;39(6):1095–1100.