Abstract
Due to its rarity, no large studies have evaluated the outcomes of p230-CML patients treated with tyrosine kinase inhibitors (TKI). We describe the clinical course of two patients with p210/p230 co-expressed CML and provide a comprehensive review of 65 cases of p230-CML. Case-1 was a 35-year old male diagnosed with p210/p230-CML in chronic phase (CP) who progressed to extramedullary blast crises (EMBC) in the form of leukemia cutis (LC) after 4-years of imatinib therapy. TK domain (TKD) mutation was negative. Treatment with dasatinib resulted in resolution of LC, but patient defaulted treatment and died. Case-2 was a 25-year old male with p210/p230-CML in accelerated phase (AP) who progressed to EMBC-LC (T315I(+)) after 1-year of imatinib therapy. He responded transiently to dasatinib, but succumbed to progressive disease. Literature review revealed that patients with p230-CML had female predominance, a lower total leucocyte count and higher platelets at presentation than p210-CML. About 18% had extreme thrombocytosis (> 1000 × 10(9)/L) and 29.5% had additional cytogenetic abnormalities at diagnosis. The proportion of transformations to AP/BC (30% vs. 25%) and deaths (37.5% vs. 27%) was similar in the pre-TKI and TKI era. As compared to imatinib, frontline treatment with 2nd -generation TKI improved the median survival. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s12288-025-02151-3.