Abstract
Chronic NK-LDGL is characterized by the expansion of CD3−, CD16+ and/or CD56+ mature NK cells associated with anemia and/or neutropenia. There are many reports of concurrent LDGL expansions in patients with other types of bone marrow failure syndromes such as myelodysplastic syndrome (MDS) and aplastic anemia (AA). Bone marrow suppression through autoimmune mechanisms has been suggested to have importance in these diseases along with failed hemaptopoiesis through ineffective stem cell differentiation. The critical mechanism for failed hematopoiesis in patients with NK-LDGL is thought to be through a mechanism of antigen-driven expansion of autoreactive NK cells that delete mature myeloid cells in the peripheral compartments. We found that patients with NK-LDGL express a skewed repertoire of NK receptors. (
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