Promoter swapping of truncated PDGFRB drives Ph-like acute lymphoblastic leukemia.
Bunpei MiyazakiToshihide UenoMasanaka SugiyamaShinya KojimaAyumu ArakawaKayoko TaoKazuki TanimuraKouya ShiraishiShigehiro YagishitaShinji KohsakaMamoru KatoNobutaka KiyokawaYasushi GotoYasushi YatabeAkinobu HamadaHiroyuki ManoChitose OgawaYosuke TanakaPublished in: NPJ precision oncology (2023)
Philadelphia chromosome (Ph)-like acute lymphoblastic leukemia (ALL) is a subset of ALL that demonstrated a high treatment failure rate. One of the hallmarks of Ph-like ALL is PDGFRB gene fusion, with fusion partner proteins often harboring dimerization domains and enhancing the kinase activity of PDGFRB. We determined a novel oncogenic PDGFRB fusion gene, NRIP1::PDGFRB, from a pediatric patient with ALL, encoding a protein with the carboxy-terminal kinase domain of PDGFRB, without the partner peptide. We confirmed the oncogenic potential of NRIP1::PDGFRB in vitro and the efficacy of all ABL1-specific inhibitor generations, including imatinib, dasatinib, nilotinib, and ponatinib, in suppressing this potential. PDGFRB activation mechanism may include juxtamembrane domain truncation in the predicted peptide. In conclusion, we determined a novel fusion gene pattern in Ph-like ALL.