Identification and characterization of novel TRPM1 autoantibodies from serum of patients with melanoma-associated retinopathy.

Juliette Varin,Juliette Wohlschlegel,Bernard Guillot,José-Alain Sahel,Margaret M Reynolds,Isabelle Audo,Ondine Becquart,José S Pulido,Robert M Duvoisin,Quentin Samaran,Christelle Michiels,Olivier Dereure,Sarah Tick,Catherine W Morgans,Christina Zeitz,Nassima Bouzidi

doi:10.1371/journal.pone.0231750

Abstract

Melanoma-associated retinopathy (MAR) is a rare paraneoplastic retinal disorder usually occurring in the context of metastatic melanoma. Patients present with night blindness, photopsias and a constriction of the visual field. MAR is an auto-immune disorder characterized by the production of autoantibodies targeting retinal proteins, especially autoantibodies reacting to the cation channel TRPM1 produced in melanocytes and ON-bipolar cells. TRPM1 has at least three different isoforms which vary in the N-terminal region of the protein. In this study, we report the case of three new MAR patients presenting different anti-TRPM1 autoantibodies reacting to the three isoforms of TRPM1 with variable binding affinity. Two sera recognized all isoforms of TRPM1, while one recognized only the two longest isoforms upon immunolocalization studies on overexpressing cells. Similarly, the former two sera reacted with all TRPM1 isoforms on western blot, but an immunoprecipitation enrichment step was necessary to detect all isoforms with the latter serum. In contrast, all sera labelled ON-bipolar cells on Tprm1+/+ but not on Trpm1-/- mouse retina as shown by co-immunolocalization. This confirms that the MAR sera specifically detect TRPM1. Most likely, the anti-TRPM1 autoantibodies of different patients vary in affinity and concentration. In addition, the binding of autoantibodies to TRPM1 may be conformation-dependent, with epitopes being inaccessible in some constructs (truncated polypeptides versus full-length TRPM1) or applications (western blotting versus immunohistochemistry). Therefore, we propose that a combination of different methods should be used to test for the presence of anti-TRPM1 autoantibodies in the sera of MAR patients.

Highlights

Paraneoplastic retinopathies are rare retinal disorders usually associated with the presence of autoantibodies against retinal proteins following the development of a primary tumor or a metastasis [1,2,3,4,5]
The full-field electroretinogram is critical for the proper diagnosis of melanoma-associated retinopathy (MAR) and typically shows ON-bipolar cell dysfunction resembling the ERG abnormalities seen in a sub-group of congenital stationary night blindness (CSNB), the complete form of SchubertBornschein, cCSNB [2,17,18,19]
We report three novel cases with MAR being females

Summary

Introduction

Paraneoplastic retinopathies are rare retinal disorders usually associated with the presence of autoantibodies against retinal proteins following the development of a primary tumor or a metastasis [1,2,3,4,5]. The full-field electroretinogram (ff-ERG) is critical for the proper diagnosis of MAR and typically shows ON-bipolar cell dysfunction resembling the ERG abnormalities seen in a sub-group of congenital stationary night blindness (CSNB), the complete form of SchubertBornschein, cCSNB [2,17,18,19]. In this condition, while applying the International Society for Clinical Electrophysiology of Vision (ISCEV) recommended protocol [20], in MAR patients and in cCSNB patients, ff-ERG abnormalities are as follows: under dark adapted (DA, scotopic) conditions, there is no detectable response to a dim (0.01 cd.s.m-2) flash. Intravitreal injection of sera from patients with MAR into monkey and mouse eyes

Objectives

Methods

Results

Conclusion