AUTHOR=Egyed Miklos , Kajtar Bela , Foldesi Csaba , Skov Vibe , Kjær Lasse , Hasselbalch Hans Carl 

TITLE=Ropeginterferon-alfa2b resolves angina pectoris and reduces JAK2V617F in a patient with clonal hematopoiesis of indeterminate potential: A case report

JOURNAL=Frontiers in Hematology

VOLUME=1

YEAR=2022

URL=https://www.frontiersin.org/journals/hematology/articles/10.3389/frhem.2022.1005666

DOI=10.3389/frhem.2022.1005666

ISSN=2813-3935

ABSTRACT=<p>The <italic>JAK2V617F</italic> mutation is an acquired somatic mutation, which is prevalent in patients with the Philadelphia-chromosome negative myeloproliferative neoplasms (MPNs). In these diseases the mutation gives rise to constitutive JAK-STAT signaling with increased blood cell counts and <italic>in vivo</italic> activation of neutrophils and platelets as well, which altogether contribute to a chronic inflammatory and thrombogenic state with a 12-fold increased risk of coronary disease. Treatment with recombinant interferon-alpha2 (rIFN) reduces the <italic>JAK2V617F</italic> allelic burden in a large number of MPN-patients. Long-term treatment with rIFN associates with low-burden <italic>JAK2V617F</italic> in a subset of patients and a decreased thrombosis risk as well. In the general population the <italic>JAK2V617F</italic> mutation has been shown to associate with ischemic heart disease and thrombosis. Based upon the above observations we herein report the first patient with CHIP-<italic>JAK2V617F</italic>, in whom treatment with rIFN resolved severe angina pectoris. During a short period off rIFN the symptoms reappeared to resolve in concert with reduction of <italic>JAK2V617F</italic> allele burden, when rIFN was reinstituted. The <italic>JAK2V617F</italic> mutation may be a novel therapeutic target to prohibit the development of cardiovascular diseases using rIFN either as monotherapy or in combination with potent anti-inflammatory agents.</p>