| Literature DB >> 36138008 |
Mariela Cortés-López1, Laura Schulz1, Mihaela Enculescu1, Claudia Paret2,3,4, Bea Spiekermann1, Mathieu Quesnel-Vallières5,6, Manuel Torres-Diz7, Sebastian Unic8, Anke Busch1, Anna Orekhova1, Monika Kuban8, Mikhail Mesitov1, Miriam M Mulorz1, Rawan Shraim7,9, Fridolin Kielisch1, Jörg Faber2,3,4, Yoseph Barash5, Andrei Thomas-Tikhonenko7,10, Kathi Zarnack11,12, Stefan Legewie13,14,15, Julian König16.
Abstract
Following CART-19 immunotherapy for B-cell acute lymphoblastic leukaemia (B-ALL), many patients relapse due to loss of the cognate CD19 epitope. Since epitope loss can be caused by aberrant CD19 exon 2 processing, we herein investigate the regulatory code that controls CD19 splicing. We combine high-throughput mutagenesis with mathematical modelling to quantitatively disentangle the effects of all mutations in the region comprising CD19 exons 1-3. Thereupon, we identify ~200 single point mutations that alter CD19 splicing and thus could predispose B-ALL patients to developing CART-19 resistance. Furthermore, we report almost 100 previously unknown splice isoforms that emerge from cryptic splice sites and likely encode non-functional CD19 proteins. We further identify cis-regulatory elements and trans-acting RNA-binding proteins that control CD19 splicing (e.g., PTBP1 and SF3B4) and validate that loss of these factors leads to pervasive CD19 mis-splicing. Our dataset represents a comprehensive resource for identifying predictive biomarkers for CART-19 therapy.Entities:
Year: 2022 PMID: 36138008 DOI: 10.1038/s41467-022-31818-y
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 17.694