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Utility of <scp>CD36</scp> as a novel addition to the immunophenotypic signature of <scp>RAM</scp>‐phenotype acute myeloid leukemia and study of its clinicopathological characteristics

Devasis Panda, Gaurav Chatterjee, Rohan Sardana, Twinkle Khanka, Sitaram Ghogale, Nilesh Deshpande, Yajamanam Badrinath, Dhanalaxmi Shetty, Gaurav Narula, Shripad Banavali, Nikhil Patkar, Sumeet Gujral, Papagudi Ganesan Subramanian, Prashant Tembhare

2020Cytometry Part B Clinical Cytometry24 citationsDOIOpen Access PDF

Abstract

INTRODUCTION: In 2016, Children Oncology Group (COG) described a new high-risk subtype of acute myeloid leukemia (AML) with a distinct immunophenotypic-signature, RAM-phenotype (RAM-AML). Data on clinical and laboratory features of RAM-AML are still limited to COG report only. Herein, we report the clinicopathological characteristics and detailed immunophenotypic features of RAM-AML patients. In COG report, 38% of RAM-AML belonged to acute megakaryoblastic leukemia (AMKL)-subtype. Hence, we further compared the immunophenotypic features RAM-AML with non-RAM-AMKL diagnosed during the same study period. METHODS: We included RAM-AML and non-RAM AMKL patients diagnosed between January 2017 and December 2019. We studied their morphological, cytochemical, immunophenotyping, cytogenetic, and molecular characteristics. Mean fluorescent intensity (MFI) and expression-pattern of immunophenotypic markers of RAM-AML were compared with non-RAM AMKLs patients. RESULTS: We identified 11 RAM-AML (1%) and 21 non-RAM AMKL (1.9%) patients in 1102 pediatric-AML patients. Seven of 11 (63.64%) patients belonged to FAB-M7-subtype. CD56, CD117, and CD33 demonstrated overexpression, whereas CD45 and CD38 showed under-expression in RAM-AML patients. CD36 was consistently negative in RAM-AML, whereas moderate-bright positive in non-RAM AMKLs patients (p < 0.0001). On principle component analysis, addition of CD36 enhanced the visual-separation between RAM-AML and non-RAM AMKL clusters. Cytogenetic and molecular studies did not show any recurrent abnormality; however, RNA-sequencing study revealed CBFA2T3-GLIS2-fusion in three of seven (42.8%) RAM-AML patients. CONCLUSION: We report the clinicopathological characteristics and the detailed immunophenotypic profile in the world's second series of RAM-AML patients. We further report a novel finding of CD36-negative expression as an additional parameter to the multidimensional immunophenotypic signature of this entity.

Topics & Concepts

Myeloid leukemiaPhenotypeSignature (topology)ImmunophenotypingCD36MyeloidBiologyImmunologyCancer researchFlow cytometryGeneGeneticsGeometryMathematicsAcute Myeloid Leukemia ResearchAcute Lymphoblastic Leukemia researchRetinoids in leukemia and cellular processes
Utility of <scp>CD36</scp> as a novel addition to the immunophenotypic signature of <scp>RAM</scp>‐phenotype acute myeloid leukemia and study of its clinicopathological characteristics | Litcius