# Acute hemiplegia as initial presentation in FIP1L1-PDGFRA-rearranged myeloid neoplasm with eosinophilia: a case report

**Authors:** Min Cheng, Wenjie Shi, Jin Xu, Doudou Wei, Yue Sun, Qian Jiang, Yongjie Li

PMC · DOI: 10.3389/fonc.2026.1628690 · Frontiers in Oncology · 2026-02-10

## TL;DR

A rare case of a myeloid neoplasm with eosinophilia presented as a stroke and was successfully treated with imatinib.

## Contribution

This case report adds new clinical insights into the diagnosis and treatment of FIP1L1-PDGFRA-rearranged myeloid neoplasm.

## Key findings

- Acute hemiplegia can be the first sign of F/P-rearranged myeloid neoplasm with eosinophilia.
- Low-dose imatinib effectively resolved both eosinophilia and vascular stenosis in this case.
- Long-term remission was achieved without the need for additional antithrombotic therapies.

## Abstract

Myeloid neoplasms harboring the FIP1L1-PDGFRA (F/P) fusion gene infrequently manifest as acute cerebral infarction. The F/P fusion gene induces proliferation within the eosinophilic lineage, resulting in a clonal hypereosinophilic syndrome that may lead to cerebral infarction. This condition demonstrates a high responsiveness to imatinib therapy.

A 27-year-old man presented with acute hemiplegia and was found to have significant eosinophilia. Neuroimaging revealed acute-subacute infarcts with concurrent focal stenosis of the right middle cerebral artery. He was diagnosed with F/P-rearranged myeloid neoplasm associated with myeloid sarcoma. Treatment with low-dose imatinib monotherapy (100 mg/day) resulted in rapid resolution of both eosinophilia and the vascular stenosis. Over 9 years of follow-up without adjuvant antithrombotic agents, he has maintained sustained molecular remission and normal neurological function, with no recurrent stroke.

This case provides new clinical data for the diagnosis and treatment of this type of eosinophilia, and highlights the importance of early recognition, workup, and treatment. Peripheral hypereosinophilia may cause tissue damage, leading to hypereosinophilic syndrome with cerebral infarction. F/P+ clonal hypereosinophilic syndrome is a rare diagnosis to consider in patients with unexplained cerebral infarction and hypereosinophilia. In these instances, it is imperative to conduct a peripheral blood test for the F/P fusion gene early in the diagnostic evaluation of hypereosinophilic syndrome. Upon confirmation of the diagnosis, initiation of imatinib therapy should occur promptly. This treatment approach has resulted in a swift and sustained complete cytologic and molecular remission, no recurrence of cerebral infarction, obviating the need for intensive chemotherapy, statins, anticoagulant or anti-platelet agents.

## Linked entities

- **Chemicals:** imatinib (PubChem CID 5291)
- **Diseases:** myeloid neoplasm (MONDO:0005170), hypereosinophilic syndrome (MONDO:0015691), cerebral infarction (MONDO:0002679)

## Full-text entities

- **Genes:** F12 (coagulation factor XII) [NCBI Gene 2161] {aka HAE3, HAEX, HAF}, THBD (thrombomodulin) [NCBI Gene 7056] {aka AHUS6, BDCA-3, BDCA3, CD141, THPH12, THRM}, WT1 (WT1 transcription factor) [NCBI Gene 7490] {aka AWT1, GUD, NPHS4, WAGR, WIT-2, WT-1}, CD34 (CD34 molecule) [NCBI Gene 947], FIP1L1 (factor interacting with PAPOLA and CPSF1) [NCBI Gene 81608] {aka FIP1, Rhe, hFip1}, F5 (coagulation factor V) [NCBI Gene 2153] {aka FVL, PCCF, RPRGL1, THPH2, fV}, VWF (von Willebrand factor) [NCBI Gene 7450] {aka F8VWF, VWD}, PDGFRB (platelet derived growth factor receptor beta) [NCBI Gene 5159] {aka CD140B, IBGC4, IMF1, JTK12, KOGS, OPDKD}, KIT (KIT proto-oncogene, receptor tyrosine kinase) [NCBI Gene 3815] {aka C-Kit, CD117, MASTC, PBT, SCFR}, MME (membrane metalloendopeptidase) [NCBI Gene 4311] {aka CALLA, CD10, CMT2T, NEP, SCA43, SFE}, F3 (coagulation factor III, tissue factor) [NCBI Gene 2152] {aka CD142, TF, TFA}, CD40LG (CD40 ligand) [NCBI Gene 959] {aka CD154, CD40L, HIGM1, IGM, IMD3, T-BAM}, FUT4 (fucosyltransferase 4) [NCBI Gene 2526] {aka CD15, ELFT, FCT3A, FUC-TIV, FUTIV, LeX}, PDGFRA (platelet derived growth factor receptor alpha) [NCBI Gene 5156] {aka CD140A, PDGFR-2, PDGFR2}, PRAME (PRAME nuclear receptor transcriptional regulator) [NCBI Gene 23532] {aka CT130, MAPE, OIP-4, OIP4}, RNASE3 (ribonuclease A family member 3) [NCBI Gene 6037] {aka ECP, RAF1, RNS3}
- **Diseases:** diabetes (MESH:D003920), valvular dysfunction (MESH:D006349), weakness (MESH:D018908), rearranged (MESH:D002869), Cancer (MESH:D009369), cardioembolic occlusion (MESH:D000083262), HE (MESH:D004802), vasculopathic injury (MESH:D014947), cardiac inflammation (MESH:D007249), fibrosis (MESH:D005355), cerebral artery (MESH:D002539), Cardiogenic embolism (MESH:D013575), myocardial remodeling (MESH:D064752), pain (MESH:D010146), stenosis (MESH:D003251), fever (MESH:D005334), hematopoietic neoplasms (MESH:D019337), damage (MESH:D020263), lymphadenopathy (MESH:D008206), bleeding (MESH:D006470), paralysis (MESH:D010243), drooling (MESH:D012798), blood hypercoagulability (MESH:D019851), stroke (MESH:D020521), coagulation (MESH:D001778), bone marrow hyperplasia (MESH:D001855), Ischemic strokes (MESH:D002544), cerebrovascular disease (MESH:D002561), vascular endothelial injury (MESH:D057772), acute cerebral infarction (MESH:D056989), dizziness (MESH:D004244), anemia (MESH:D000740), left ventricular thrombus (MESH:D013927), hypertension (MESH:D006973), myeloid sarcoma (MESH:D023981), Leukemia (MESH:D007938), atherosclerotic (MESH:D050197), middle cerebral artery (MESH:D020244), HES (MESH:D017681), nuchal rigidity (MESH:D009127), disseminated intravascular coagulation (MESH:D004211), cognitive impairment (MESH:D003072), tissue damage (MESH:D017695), Myeloproliferative grade III (MESH:D001254), infarction (MESH:D007238), organ damage (MESH:D000092124), hemiplegia (MESH:D006429), cardiac (MESH:D006331), allergies (MESH:D004342), cortical dysfunction (MESH:D054220)
- **Chemicals:** uric acid (MESH:D014527), triglycerides (MESH:D014280), Aspirin (MESH:D001241), Gleevec (MESH:D000068877), anti (-), creatinine (MESH:D003404)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

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## Figures

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## References

16 references — full list in the complete paper: https://tomesphere.com/paper/PMC12929143/full.md

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Source: https://tomesphere.com/paper/PMC12929143