Extended Data Fig. 1: Identification of Clstn3b transcript species.
From: CLSTN3β enforces adipocyte multilocularity to facilitate lipid utilization
a, RNA-, ATAC-, CAGE-, and H3K4me3 ChIP-seq reads at the Clstn3 locus in mouse preadipocytes (day 0 of differentiation), adipocytes (day 5 of differentiation), cortex, and BAT. b, Summary of mouse Clstn3b transcript variants. Arrows mark positions of possible start codons (ATGs that are in-frame with Clstn3 exons 17/18). c, LeafCutter analysis of differential splice site utilization in mouse BAT and cerebral cortex. Intron clusters are ranked by statistical significance. Clstn3 (rank 8) is highlighted in red. d, LeafCutter output for the Clstn3 intron cluster. e, 5’RLM-RACE products from mouse BAT using gene-specific primers targeting Clstn3 exon 17. f, RT-PCR products from mouse BAT using primers targeting Clstn3b transcript variant 2. Black arrows mark positions of primers (F1-F7 = forward 1 through forward 7, R = reverse). *This splice site is actually two splice sites that are 4 base pairs apart. One (30%) is in-frame with Clstn3 exons 17/18 and produces a protein-coding transcript. The other (5.3%) is out-of-frame with Clstn3 exons 17/18 and produces a non-coding transcript.
