Purpose: To evaluate tumor control and ocular safety associated with high-dose intravitreal (IVT) topotecan (100 µg) for isolated recurrent solid retinal tumors in children with retinoblastoma. Methods: This retrospective case series was based on a prospectively maintained clinical database and included 10 eyes of 10 patients with isolated recurrent solid retinal tumors following prior systemic and/or intra-arterial chemotherapy. All eyes received IVT topotecan (100 µg/0.1 mL) using a standardized injection protocol, with adjunctive focal consolidation therapy (laser photocoagulation and/or cryotherapy) administered as clinically indicated. Primary outcomes included complete tumor regression, globe salvage, ocular toxicity, and metastatic events. Results: The mean interval from the last prior treatment to recurrence was 13 (range, 3–24) months. Each eye received a median of 2 injections (range, 1–6; mean, 2.7 injections). Complete tumor regression was achieved in all eyes (100%). No clinically appreciable ocular toxicity, systemic toxicity, enucleations, or metastatic events occurred during a mean follow-up of 12 (range, 6–24) months. Conclusions: High-dose IVT topotecan combined with focal consolidation therapy appears to be a promising treatment option for isolated recurrent solid retinal tumors in retinoblastoma, achieving excellent tumor control with low observed toxicity during the available follow-up period.
ShieldsCLShieldsJACaterJDe PotterP.Classification and management of retinoblastoma. Curr Opin Ophthalmol. 1994;5(3):16-24.
2.
MunierFLGaillardMCBalmerABeck-PopovicM.Intravitreal chemotherapy for vitreous seeding in retinoblastoma: recent advances and perspectives. Saudi J Ophthalmol. 2013;27(3):147-150. doi:10.1016/j.sjopt.2013.06.003
3.
FrancisJHMarrBPBrodieSEAbramsonDH.Efficacy and toxicity of intravitreal chemotherapy for retinoblastoma: four-year experience. Ophthalmology. 2017;124(4):488-495.
4.
ShieldsCLManjandavidaFPArepalliSKalikiSShieldsJA.Intravitreal chemotherapy for retinoblastoma: rationale and technique. Retina Today. 2014;5(1):56-60.
5.
SchaiquevichPBuitragoETaichP, et al. Ocular pharmacology of topotecan and its potential use as an intravitreal agent. Retina. 2013;33(7):1324-1332.
6.
FrancisJHAbramsonDHJiXShieldsCLMarrBP.Topotecan toxicity compared with melphalan in intravitreal injections for retinoblastoma. Retina. 2020;40(6):1045-1052.
7.
FandiñoACSánchezAVDel SoleMJGiarolaLBSchaiquevichP.Retinal toxicity of topotecan after repeated intravitreal administration in rabbits. Exp Eye Res. 2016;145:265-271.
8.
Del SoleMJClausseMNejamkinP, et al. Ocular and systemic toxicity of high-dose intravitreal topotecan in rabbits: implications for retinoblastoma treatment. Exp Eye Res. 2022;218:109026. doi:10.1016/j.exer.2022.109026
9.
AbramsonDHFrancisJHMarrBPDunkelIJ.High-dose intravitreal topotecan for retinoblastoma. Br J Ophthalmol. 2019;103(5):644-647.
10.
ShieldsCLMedinaREvansH, et al. High-dose intravitreal topotecan for recurrent retinoblastoma, subretinal seeds and vitreous seeds. Retina. 2025;45(1):1-6. doi:10.1097/IAE.0000000000004283
11.
Bravo-GonzalezADominguez-RuizPGonzálezM, et al. The role of intravitreal chemotherapy as an adjunctive treatment for retinoblastoma: a systematic review and single-arm meta-analysis. Am J Ophthalmol. 2025;273:130-140. doi:10.1016/j.ajo.2024.12.012
