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. 2023 Jun;37(6):1287-1297.
doi: 10.1038/s41375-023-01878-0. Epub 2023 Apr 26.

SRSF2-P95H decreases JAK/STAT signaling in hematopoietic cells and delays myelofibrosis development in mice

Christophe Willekens  1   2   3 Lucie Laplane  1   4 Tracy Dagher  1   2 Camelia Benlabiod  1   2   4 Nicolas Papadopoulos  5   6 Catherine Lacout  1 Philippe Rameau  7 Cyril Catelain  7 Alexia Alfaro  7 Valérie Edmond  1 Nicolas Signolle  7 Valentine Marchand  1   2 Nathalie Droin  1   2   7 Remco Hoogenboezem  8 Rebekka K Schneider  8   9 Alex Penson  10 Omar Abdel-Wahab  10 Stephane Giraudier  11 Florence Pasquier  1   3 Caroline Marty  1   2 Isabelle Plo  1   2 Jean-Luc Villeval  1   2 Stefan N Constantinescu  5   6   12   13 Françoise Porteu  1   2 William Vainchenker  1   2 Eric Solary  14   15   16
Affiliations

SRSF2-P95H decreases JAK/STAT signaling in hematopoietic cells and delays myelofibrosis development in mice

Christophe Willekens et al. Leukemia. 2023 Jun.

Abstract

Heterozygous mutation targeting proline 95 in Serine/Arginine-rich Splicing Factor 2 (SRSF2) is associated with V617F mutation in Janus Activated Kinase 2 (JAK2) in some myeloproliferative neoplasms (MPNs), most commonly primary myelofibrosis. To explore the interaction of Srsf2P95H with Jak2V617F, we generated Cre-inducible knock-in mice expressing these mutants under control of the stem cell leukemia (Scl) gene promoter. In transplantation experiments, Srsf2P95H unexpectedly delayed myelofibrosis induced by Jak2V617F and decreased TGFβ1 serum level. Srsf2P95H reduced the competitiveness of transplanted Jak2V617F hematopoietic stem cells while preventing their exhaustion. RNA sequencing of sorted megakaryocytes identified an increased number of splicing events when the two mutations were combined. Focusing on JAK/STAT pathway, Jak2 exon 14 skipping was promoted by Srsf2P95H, an event detected in patients with JAK2V617F and SRSF2P95 co-mutation. The skipping event generates a truncated inactive JAK2 protein. Accordingly, Srsf2P95H delays myelofibrosis induced by the thrombopoietin receptor agonist Romiplostim in Jak2 wild-type animals. These results unveil JAK2 exon 14 skipping promotion as a strategy to reduce JAK/STAT signaling in pathological conditions.

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