A bioassay for the detection of neutralizing antibodies against the Î±-melanocyte stimulating hormone analog afamelanotide in patients with erythropoietic protoporphyria.

[erythropoietic protoporphyria]

The tridecapeptide afamelanotide (Scenesse Â®) is a congener of Î±-melanocyte stimulating hormone (Î±-MSH ). Upon binding to the melanocortin 1 receptor (MC 1 R ) on the surface of pigment cells of the skin , the melanocytes , Î±-MSH or afamelanotide trigger the synthesis of cAMP , which stimulates the synthesis of melanin and therefore induces skin tanning . In a recent trial , afamelanotide administered as controlled release implants protected erythropoietic protoporphyria (EPP ) patients from sunlight induced phototoxic skin reactions . Administration of biological therapeutic peptides may elicit unwanted immunogenic responses in recipients of these products . Although in a previous study using ELISA technique we excluded any newly developed immunogenicity during prolonged exposure to afamelanotide , we confirmed the previously published existence of low titers of antibodies against Î±-MSH in drug-naÃ¯ve individuals that cross-reacted with afamelanotide . In order to investigate whether such antibodies are neutralizing , i .e . could block the biological effect of afamelanotide , we developed a cell culture-based bioassay . The basis of our assay was the measurement of afamelanotide-induced cAMP formation in a strain of the B 16 mouse melanoma cell line , G 4 F -7 , expressing the transfected human MC 1 R . Average half -effective concentrations of the natural hormone Î±-MSH and its congener afamelanotide were 38 .8 Â± 10 .6 and 10 .9 Â± 7 .17 nM (n =5 ), respectively . Neutralizing antibodies would reduce the cAMP formation . Two neutralizing anti-Î±-MSH antibodies served as positive controls . cAMP formation in the G 4 F -7 cells after addition of sera of drug-naÃ¯ve (n =6 ) and of drug-exposed EPP patients (n =17 ) was significantly lower than after that from healthy volunteers (n =13 ). There was no difference between drug-naÃ¯ve and drug-exposed patients . Using forskolin as a hormone-independent stimulator of cAMP formation , we excluded an unspecific interference of EPP sera with cAMP formation . We conclude that afamelanotide even after prolonged application to EPP patients did not elicit neutralizing antibodies . Further , the low titer immunoreactivity observed in sera of some drug-naÃ¯ve individuals had no effect on the biological activity of afamelanotide .

Diseases
Validation

Diseases presenting "positive controls" symptom

cowden syndrome

erythropoietic protoporphyria

familial hypocalciuric hypercalcemia

krabbe disease

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