The homeobox transcription factors HoxA9 and Meis1 are causally involved in the etiology of acute myeloid leukemia. Garcia-Cuellar and colleagues applied degron techniques to elucidate the leukemogenic contribution of Meis1. They provided the molecular correlation of the experimental observation that Meis1 enhances leukemogenesis in combination with HoxA9 while on its own it has no discernible effect on hematopoietic development.

A number of patients with a clinical presentation of “triple-negative” acquired thrombocytosis do not display the characteristic histological features of essential thrombocytosis or myeloproliferative neoplasm, raising the question of appropriate therapeutic management. In a cohort of 130 patients with chronic, non-reactive triple-negative thrombocytosis, Lemoine and colleagues had bone marrow biopsies reviewed centrally, and then asked whether targeted NGS could help reach a diagnosis. They showed that characterization of triple-negative thrombocytosis relies on thorough clinical, biological, histological and genetic studies.