Specificity, synergy, and mechanisms of splice-modifying drugs

Author:

Ishigami YumaORCID,Wong Mandy S.,Martí-Gómez Carlos,Ayaz Andalus,Kooshkbaghi Mahdi,Hanson Sonya M.ORCID,McCandlish David M.ORCID,Krainer Adrian R.ORCID,Kinney Justin B.ORCID

Abstract

AbstractDrugs that target pre-mRNA splicing hold great therapeutic potential, but the quantitative understanding of how these drugs work is limited. Here we introduce mechanistically interpretable quantitative models for the sequence-specific and concentration-dependent behavior of splice-modifying drugs. Using massively parallel splicing assays, RNA-seq experiments, and precision dose-response curves, we obtain quantitative models for two small-molecule drugs, risdiplam and branaplam, developed for treating spinal muscular atrophy. The results quantitatively characterize the specificities of risdiplam and branaplam for 5’ splice site sequences, suggest that branaplam recognizes 5’ splice sites via two distinct interaction modes, and contradict the prevailing two-site hypothesis for risdiplam activity at SMN2 exon 7. The results also show that anomalous single-drug cooperativity, as well as multi-drug synergy, are widespread among small-molecule drugs and antisense-oligonucleotide drugs that promote exon inclusion. Our quantitative models thus clarify the mechanisms of existing treatments and provide a basis for the rational development of new therapies.

Funder

U.S. Department of Health & Human Services | National Institutes of Health

U.S. Department of Health & Human Services | NIH | Office of Extramural Research, National Institutes of Health

MEXT | Japan Society for the Promotion of Science

Alfred P. Sloan Foundation

Publisher

Springer Science and Business Media LLC

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