Pharmacokinetic Analysis of Melphalan after Superselective Ophthalmic Artery Infusion in Preclinical Models and Retinoblastoma Patients

Schaiquevich, Paula; Buitrago, Emiliano; Taich, Paula Juliana; Torbidoni, V.; Ceciliano, Alejandro; Fandiño, Adriana; Asprea, Marcelo; Requejo, Flavio; Abramson, David H.; Bramuglia, Guillermo F.; Chantada, Guillermo

doi:10.1167/iovs.12-9501

Cited by 61 publications

(75 citation statements)

References 29 publications

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“…Or it could be used to reduce large uveal melanomas to a size that could appropriately receive definitive treatment with plaque brachytherapy. In support of this, it is known from the retinoblastoma literature that intra-arterial melphalan results in a substantial dose of drug to the choroid [23]. Or perhaps it could be used in the management of other ocular melanomas, such as refractory conjunctival melanomas with orbital extension.…”

Section: Discussionmentioning

confidence: 93%

Chemoreduction of Orbital Recurrence of Uveal Melanoma by Intra-Arterial Melphalan

et al. 2018

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Background/Aims: The treatment of orbital melanoma poses a management challenge. This case explores the delivery of high-dose melphalan to an orbital recurrence of uveal melanoma via intra-arterial delivery of melphalan to the orbit. A 62-year-old man developed recurrent orbital disease 7 months after enucleation for a large uveal melanoma. He received 6 monthly intra-arterial infusions of melphalan to the orbit, ranging in dose from 20 to 30 mg per infusion. Following the last infusion, mild temporary erythema was noted on the forehead along the distribution of the supratrochlear artery. The orbital recurrence was reduced in size by 66% in the longest dimension as measured by magnetic resonance imaging (MRI). However, 9 months following intra-arterial melphalan, tumor regrowth was detected on MRI, and additional treatment options were pursued. Conclusion: This case demonstrates that intra-arterial melphalan can result in nonsustained tumor regression of recurrent orbital uveal melanoma. It suggests that local delivery of high-dose melphalan may be helpful as a neoadjuvant treatment for uveal melanoma, and future studies will be useful to confirm the value of this approach in additional cases of recurrent and possibly in primary uveal melanoma.

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Section: Discussionmentioning

confidence: 93%

Chemoreduction of Orbital Recurrence of Uveal Melanoma by Intra-Arterial Melphalan

et al. 2018

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“…15 These levels are beyond the 50% minimum inhibitory concentration in vitro for melphalan to achieve control of retinoblastoma tumor with only minimal (57 ng/ml) concentrations in the plasma after direct ophthalmic artery infusion. 15 The RPE choroid to vitreous ratio of melphalan also indicates limited trans-retina diffusion of melphalan, which has been attributed to its poor affinity to the L-type amino acid transporter (LAT1) along the bloodretina barrier, an important pharmacokinetic property with significant clinical implications. 16 Topotecan exhibits a similar high ratio of vitreous to plasma concentration in animal studies after ophthalmic artery infusion that is well over the 50% minimum inhibitory concentration; however, studies on relative RPE choroid to vitreous concentration after ophthalmic artery infusion are not to our knowledge, available.…”

Section: Discussionmentioning

confidence: 96%

“…14 The rationale for using melphalan in IAC is to minimize its systemic toxicity through direct intra-arterial intraocular infusion. [14][15] In animal studies, the concentration of melphalan after a single ophthalmic artery infusion in the retinal pigment epithelium (RPE) choroid is 295.2 ng/g of tissue compared to 170.1 ng/g of vitreous humor, assuming a normal vitreous density of 1 g/ml. 15 These levels are beyond the 50% minimum inhibitory concentration in vitro for melphalan to achieve control of retinoblastoma tumor with only minimal (57 ng/ml) concentrations in the plasma after direct ophthalmic artery infusion.…”

Section: Discussionmentioning

confidence: 99%

“…[14][15] In animal studies, the concentration of melphalan after a single ophthalmic artery infusion in the retinal pigment epithelium (RPE) choroid is 295.2 ng/g of tissue compared to 170.1 ng/g of vitreous humor, assuming a normal vitreous density of 1 g/ml. 15 These levels are beyond the 50% minimum inhibitory concentration in vitro for melphalan to achieve control of retinoblastoma tumor with only minimal (57 ng/ml) concentrations in the plasma after direct ophthalmic artery infusion. 15 The RPE choroid to vitreous ratio of melphalan also indicates limited trans-retina diffusion of melphalan, which has been attributed to its poor affinity to the L-type amino acid transporter (LAT1) along the bloodretina barrier, an important pharmacokinetic property with significant clinical implications.…”

Section: Discussionmentioning

confidence: 99%

“…Also, infusion of both melphalan and topotecan does not affect each drug's penetration, and there is in vitro evidence of synergistic cytotoxicity of the two drugs that favors combination therapy when higher doses of melphalan are necessary for advanced disease. 15,19 The pharmacokinetic properties of melphalan delivered by ophthalmic artery infusion are reflected in its clinical activity toward control of solid tumor and SRS relative to VS. In a series of 70 eyes treated with IAC, Shields and associates reported complete solid tumor regression in 94%, SRS regression in 95%, and VS regression in 87% after a mean 3 cycles of IAC.…”

Section: A C C E P T E D Accepted Manuscriptmentioning

confidence: 99%

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