NK cells derived from myeloid (M-CSFR+) precursors show abundant KIR expression and higher cytotoxicity compared with lymphoid (M-CSFR−) precursors. (A) Expression of KIR (combination of CD158a, CD158b, and CD158e1) is higher on NK cells derived from myeloid (M-CSFR+) precursors (right) compared with M-CSFR−–derived NK cells (left). A representative donor is shown (n = 4). (B) Percentages of KIR+ NK cells derived from CD56−CD117+M-CSFR+ (▵) and CD56−CD117+M-CSFR− (●) progenitors for 4 individual donors are shown (mean ± SEM; > 3 replicates for each donor). P < .001, by 2-way analysis of variance. (C) Expression of NKG2A and KIR on CD56-gated NK cells derived from CD56−CD117+M-CSFR− (left) and CD56−CD117+M-CSFR+ (right) progenitors. Shown is the presence of a potentially alloreactive population of NKG2A-KIR+ population in the population derived from the CD56−CD117+M-CSFR+ progenitors. (D) Cytotoxicity of M-CSFR+–derived (▵) and M-CSFR−–derived (■) NK cells against K562 targets and (E) against 721.221 human leukocyte antigen–negative B-lymphoblastoid cell line. Data points represent average cytotoxicity of triplicates ± SD at the specified effector-to-target (E:T) ratios. A representative donor is shown (n = 3).