"Does antisense platform company, Ionis Pharmaceuticals, provide an aspirational blueprint for PYC?"
The Ionis story is remarkable for the determination to succeed when everyone was denouncing antisense as unworkable. While Ionis is an aspirational model it would appear that Sarepta may provide more of a working model when it comes to the chemical backbone of oligonucleotides. From what I can piece together Ionis design ASOs with a phosphorothioate backbone which carries a strong negative charge. Sarepta, on the other hand have a differentiated approach to RNA technology and utilise a phosphorodiamidate backbone that is neutrally charged - PMOs.
The problem with PMOs is that they have poor cellular uptake. We have previously referred to the article Antisense-mediated splice intervention to treat human disease: the odyssey continues, published online 22 May 2019;
"Successful translation of peptide-phosphorodiamidate morpholino drugs that are currently in development and clinical evaluation (for example, for DMD) may well begin a new era for splice-modifying therapies, particularly if tissue or cell targeting can be achieved, perhaps leading to reduced dosages."
The dosage achieved by PYC in an animal model of blinding eye disease is 60 times lower than the dose used in similar pre-clinical studies of naked antisense oligonucleotides. Its inspirational to read the story of Ionis to understand what is possible with a novel antisense platform. Stanley Crooke from Ionis said that Spinraza was the break through that mattered the most. Inherited eye disease is a great place to start a story about a new era of splice-modifying therapies.
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