Dear Editor,
We have read with interest the paper by Klimova et al. Some statements in the paper are confusing and may even mislead the readers.

The authors claim in the survival section of the paper that: "Vitreoretinal lymphoma is a life-threatening disease, with a 5-year survival rate of 71% in our study". Vitreoretinal lymphoma (VRL) may affect vision, and in very advanced cases that we rarely see in recent years, may destroy the eye. However, VRL per se is not what that kills the patients, but the associated brain lymphoma or in some case the systemic lymphoma.

According to the results in this study (and the title of the paper), "Combined (local and systemic) treatment in patients with PVRL showed favorable results in comparison with local therapy alone (p=0.695). However, the statistical significance was not reached". It is no wonder that they claim that combined treatment is better than local treatment when they have 60% relapses. However, no other study of intra-vitreal (IVit) Methotrexate showed such a high relapse rate. In our experience, the relapse rate is extremely low with IVit methotrexate alone. Actually, in summarizing our ten years results we had no recurrence of the intraocular disease (2) and summarizing now our 20-year experience with 113 eyes, we had only two cases of recurrences (unpublished data). It is difficult to explain the poor results of the authors’ patients, using either intravitreal methotrexate alone or in combination with systemic high dose methotrexate.

In their discussion, the authors write that "Vitreoretinal lymphomas are considered to be systemic disease….". It should be emphasized that this disease is in most cases a unique type of lymphoma that affects immune-privileged organs: the brain, the eye, and the testis, and only in some cases (17% in our experience), the eye disease accompanies systemic lymphoma.

References

1) Klimova A, Heissigerova J, Rihova E, et al. Combined treatment of primary vitreoretinal lymphomas significantly prolongs the time to first relapse. Br J Ophthalmol 2018, doi: 10.1136/bjophthalmol-2017-311574

2) Frenkel S, Hendler K, Siegal T, et al. Intravitreal methotrexate for treating vitreoretinal lymphoma: 10 years of experience. Br J Ophthalmol 2008;92:383-8.

Sincerely Yours,

Jacob Pe'er, M.D.
Shahar Frenkel, M.D., Ph.D.
Ocular Oncology Service
Department of Ophthalmology
Hadassah – Hebrew University Medical center
Jerusalem, Israel

Dear Sir,

We are writing this letter in response to a “letter to the editor” from Drs. Leahey and Meadows about our recently published paper “Second primary malignancies in retinoblastoma patients treated with intra-arterial chemotherapy: the first 10 years”.1 There are a number of incorrect statements in their letter and we hope this letter will clarify those errors made by them.

1) Drs. Leahey and Meadows state that…”the author’s report is profoundly misleading with regard to the risk of SPMs following OAC”. To prove that they then state that the median follow-up range is 2.5 years with a maximum follow-up of 12 years. How is that “profoundly misleading”? In the same paragraph they then state that patients failing OAC required radiation therapy and suggest that all of these second neoplasms are a consequence of radiation. That is not true. In our paper (page 273, Table 3) we documented that not one of the children who developed a second tumor had received radiation. How could radiation be the cause of a second tumor if the patients never received radiation? Dr. Leahey and Meadows also wrote that…”patients failing OAC require radiation”. That’s not true. On page 272 we stated that…”patients who received external beam radiation prior to presentation at our clinic were excluded from analysis”. None of the patients in this series received radiation after OAC and no patient in our center has received radiation in the past 10 years. We do not dispute that radiation affects the development of second cancers in germline affected retinoblastomas-but that is not the explanation for these cancers in our report.

2) In the many large series published worldwide on second cancers in retinoblastoma patients secondary AML does not appear to be a cancer that develops2,3 unless systemic chemotherapy is used4. In fact there are published series of secondary AML in retinoblastoma patients published prior to the introduction of OAC and in each case systemic chemotherapy was implicated as the cause. There has not been an increase in sAML in our patients treated with OAC and no other center has suggested or reported an increase in sAML after adopting OAC.

3) Drs. Leahey and Meadows imply that the Melphalan given for OAC is responsible for the secondary AML but that seems unlikely and is not consistent with the published, peer review literature. The Japanese used similar doses of Melphalan in their series of patients treated with intra-arterial chemotherapy (published in 2011) between 1988 and 2007.5 In their 343 patients they meticulously pointed out that long-term follow-up of these patients did not reveal an increase in second cancers and in fact all of the second cancers but one they attributed to the use of external beam radiation combined with chemotherapy. The one patient they had who developed secondary AML they attributed to the four courses of systemic chemotherapy utilizing Vincristine, Carboplatin and Etoposide. We don’t understand why Dr. Leahey and Meadows implicate the Melphalan but not the seven cycles of multiagent systemic chemotherapy they delivered. This child did not have AML while under our care. Finally, FLT3 mutations (present in this child) have usually been associated with topoisomerase induced sAML and de novo (no prior chemotherapy) sAML and not sAML from alkylating agents (e.g. Melphalan). 6 Their child’s sAML may be unrelated to any chemotherapy but more likely the systemic chemotherapy (with doses a hundred times the small amount of Melphalan delivered by OAC) is the culprit.

4) Secondary AML from chemotherapy is well known in pediatric oncology and well known by Drs. Leahey and Meadows. It is a devastating and often lethal complication of systemic chemotherapy and was the subject of a paper by Drs. Leahey and Meadows in 1999.7 They described this complication as a…”late effect of chemotherapy” in their cohort of 228 patients. We agree that secondary AML can be a late and devastating effect of systemic chemotherapy and that is why we have abandoned it for intraocular retinoblastoma and one of the reasons we developed OAC.

5) Drs. Leahey and Meadows correctly state that the goal of retinoblastoma is to cure the child of cancer (and suggest that OAC does not do that). A large, collaborative manuscript (which included their patients) was published a December 2017 on the worldwide experience with OAC8 since we introduced it in 20069. In 1139 patients who received 4396 infusions only three patients died of metastatic disease (all from Argentina and all had prior systemic chemotherapy). The conclusion is clear: using OAC to save children’s eyes and vision does not compromise patient survival.

6) Drs. Leahey and Meadows and the Philadelphia retinoblastoma team have considerable experience with OAC over the past 10 years and have published more than 20 papers on the subject. They have not published on their second tumor experience in the OAC era. We challenge them to collect and publish their data on second cancers in germline patients treated with OAC alone. If they have additional sAML cases we suggest their use of multi-agent systemic chemotherapy for retinoblastoma is the cause (as we abandoned that 12 years ago because of that well documented adverse effect).

7) We are saddened by this patient’s course but have no way of evaluating the risk/benefit discussion that Drs. Leahey and Meadows had with the family when they decided to use adjuvant multiagent chemotherapy which may have induced resistance and then a total of seven cycles of multiagent chemotherapy which are proven to cause secondary AML. The conclusion from this case is that we should all avoid systemic chemotherapy in retinoblastoma if there is a better option…and for intraocular disease fortunately there is: OAC.

References

1. Habib LA, Francis JH, Fabius AW, Gobin PY, Dunkel IJ, Abramson DH. Second primary malignancies in retinoblastoma patients treated with intra-arterial chemotherapy: the first 10 years. Br J Ophthalmol. 2018;102(2):272–275. doi:10.1136/bjophthalmol-2017-310328.

2. Kleinerman RA, Yu C-L, Little MP, et al. Variation of second cancer risk by family history of retinoblastoma among long-term survivors. J Clin Oncol. 2012;30(9):950–957. doi:10.1200/JCO.2011.37.0239.

3. Abramson DH, Frank CM. Second nonocular tumors in survivors of bilateral retinoblastoma: a possible age effect on radiation-related risk. Ophthalmology. 1998;105(4):573–9–discussion579–80. doi:10.1016/S0161-6420(98)94006-4.

4. Gombos DS, Hungerford J, Abramson DH, et al. Secondary acute myelogenous leukemia in patients with retinoblastoma: is chemotherapy a factor? Ophthalmology. 2007;114(7):1378–1383. doi:10.1016/j.ophtha.2007.03.074.

5. Suzuki S, Yamane T, Mohri M, Kaneko A. Selective ophthalmic arterial injection therapy for intraocular retinoblastoma: the long-term prognosis. Ophthalmology. 2011;118(10):2081–2087. doi:10.1016/j.ophtha.2011.03.013.

6. Godley LA, Larson RA. Therapy-related myeloid leukemia. Semin Oncol. 2008;35(4):418–429. doi:10.1053/j.seminoncol.2008.04.012.

7. Leahey AM, Teunissen H, Friedman DL, Moshang T, Lange BJ, Meadows AT. Late effects of chemotherapy compared to bone marrow transplantation in the treatment of pediatric acute myeloid leukemia and myelodysplasia. Med Pediatr Oncol. 1999;32(3):163–169.

8. Abramson DH, Shields CL, Jabbour P, et al. Metastatic deaths in retinoblastoma patients treated with intraarterial chemotherapy (ophthalmic artery chemosurgery) worldwide. Int J Retina Vitreous. 2017;3:40. doi:10.1186/s40942-017-0093-8.

9. Abramson DH, Dunkel IJ, Brodie SE, Kim JW, Gobin YP. A phase I/II study of direct intraarterial (ophthalmic artery) chemotherapy with melphalan for intraocular retinoblastoma initial results. Ophthalmology. 2008;115(8):1398–404–1404.e1. doi:10.1016/j.ophtha.2007.12.014.

Having read the article of secondary primary malignancies (SPM) in patients treated with ophthalmic artery chemosurgery (OAC) (1), we wish to update Dr. Habib’s report. A patient with unilateral Group D heritable retinoblastoma (RB) treated by their team with 5 OAC treatments in 2012 through 2013 developed acute myeloid leukemia (AML) on 4/26/2017 and died 3 months later.
Following an intraocular recurrence after OAC and subsequent enucleation the patient’s care was transferred to our institution. Despite adjuvant chemotherapy he developed widespread bone and marrow metastases 8 months after enucleation. He then underwent intensive chemotherapy and an autologous stem cell transplant. Twenty eight months later he developed AML with a fms-like tyrosine kinase 3 (FLT3) mutation. Melphalan administered during all OAC treatments and the drugs administered following that failure must be implicated in this outcome (2). By failing to eradicate retinoblastoma, metastatic disease ensued requiring further treatment and subsequently, AML.
The author’s report is profoundly misleading with regard to the risk of SPMs following OAC. Although the maximum period of follow-up is 12 years, the median is 2.5 years. Patients failing OAC required radiation therapy and are known to be 3 times more likely to develop additional cancers (3). We await that follow-up.
The goal of RB care is cure. This patient’s course illustrates the danger of failing to prevent metastatic disease with initial therapy. As Dr. Desjardins wrote in her recent review “ local administration [via OAC] cannot be used to treat micrometastases in advanced forms of the disease “ (4). Although metastatic RB can be treated if it develops (5), not all patients survive.

References:
1. Habib LA, Francis JH, Fabius A et al. Second primary malignancies in retinoblastoma patients treated with intra-arterial chemotherapy: the first 10 years. Br J Ophthalmol 2018; 102: 272-5.
2. Levine EG and Bloomfield CO. Leukemias and myelodysplastic syndromes secondary to drugs, radiation and environmental exposures. Semin Oncol 1982; 19: 471-84.
3. Kleinerman RA, Tucker MA, Tarone RE, et al. Risk of new cancers after radiotherapy in long-term survivors of retinoblastoma: an extended follow-up. J Clin Oncol 2005; 23: 2272-9.
4. Kassoux N, Lumbroso L, Levy-Gabriel C et al. Retinoblastoma: updates on current management. Asia-Pac J Ophthalmol 2017; 6: 290-5.
5. Dunkel IJ, Khakoo Y, Kernan NA et al. Intensive multi-modal therapy for patients with stage 4A metastatic retinoblastoma. Pediatr Blood Cancer 201; 55: 55-9.

We thank the authors for their comments and insights on our paper ‘Pterygia are indicators of an increased risk of developing cutaneous melanomas’.
We agree that there was selection bias within the pterygium cases. All cases were identified as hospital in-patients and therefore represent that small select portion of the population who were receiving treatment for (or removal of) their pterygium. We made no assumptions about whether these cases were more or less severe than untreated pterygia or whether the removals were performed for cosmetic or other reasons. The strengths of this study are that it included all in-hospital cases treated in Western Australia over a 30 year time period, without prejudice.
While melanoma is an uncommon problem in China, it is a major health issue in Australia and New Zealand. The clinical relevance of this study should be viewed against the background of the world’s highest incidence rates of cutaneous melanoma that currently exist, with up to 60 cases per 100,000 population1-3 in Australia and New Zealand. Contrast this with the incidence rates of East Asian countries of approximately 0.7 cases per 100,000 population.4 Both non-melanoma and melanoma skin cancers are a major health priority for cancer prevention research. We are not suggesting that pterygium be used as the sole indicator for a population wide screening program. There are well established major screening and surveillance programs in place in Australia. Our study adds a new variable to the calculation of risk for individuals (along with skin colour, hair colour, latitude and sun exposure). We do not believe our findings will cause increased anxiety to people who develop pterygium but will be a useful aid to increasing awareness of the health risks associated with high levels of solar radiation that are a part of life in Australia.
Table 5 age groups are correct as shown but could also be written as: <50 (aged 0 to 49.99) years and ≥50 (aged 50 or more) years.
The suggested correction (>50 years and <49 years) would exclude all people aged 50 years which would be incorrect for the data shown.
Julie Crewe
Tim Threlfall
Antony Clark
Paul Sanfilippo
Professor David Mackey

References
1 MacLennan R, Green AC, McLeod GRC, Martin NG. Increasing Incidence of Cutaneous Melanoma in Queensland, Australia. JNCI: Journal of the National Cancer Institute. 1992;84(18):1427-32 DOI:10.1093/jnci/84.18.1427
2 Marks R. The Changing Incidence and Mortality of Melanoma in Australia. In: Dummer R, Nestle FO, Burg G, editors. Cancers of the Skin: Proceedings of the 8th World Congress. Berlin, Heidelberg: Springer Berlin Heidelberg; 2002. p. 113-21.
3 Garbe C, Leiter U. Melanoma epidemiology and trends. Clinics in Dermatology. 2009;27(1):3-9 https://doi.org/10.1016/j.clindermatol.2008.09.001
4 Makredes M, Hui SK, Kimball AB. Melanoma in Hong Kong between 1983 and 2002: a decreasing trend in incidence observed in a complex socio–political and economic setting. Melanoma Research. 2010;20(5):427-30 DOI:10.1097/CMR.0b013e3283281072