High-throughput RNA isoform sequencing using programmed cDNA concatenation.
Aziz M Al'KhafajiJonathan T SmithKiran V GarimellaMehrtash BabadiVictoria PopicMoshe Sade-FeldmanMichael GatzenSiranush SarkizovaMarc A SchwartzEmily M BlaumAllyson DayMaura CostelloTera BowersStacey GabrielEric BanksAnthony A PhilippakisGenevieve M BolandPaul C BlaineyNir HacohenPublished in: Nature biotechnology (2023)
Full-length RNA-sequencing methods using long-read technologies can capture complete transcript isoforms, but their throughput is limited. We introduce multiplexed arrays isoform sequencing (MAS-ISO-seq), a technique for programmably concatenating complementary DNAs (cDNAs) into molecules optimal for long-read sequencing, increasing the throughput >15-fold to nearly 40 million cDNA reads per run on the Sequel IIe sequencer. When applied to single-cell RNA sequencing of tumor-infiltrating T cells, MAS-ISO-seq demonstrated a 12- to 32-fold increase in the discovery of differentially spliced genes.