首页> 外文期刊>Bone marrow transplantation >Cytolytic activity of NK cell clones against acute childhood precursor-B-cell leukaemia is influenced by HLA class I expression on blasts and the differential KIR phenotype of NK clones.
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Cytolytic activity of NK cell clones against acute childhood precursor-B-cell leukaemia is influenced by HLA class I expression on blasts and the differential KIR phenotype of NK clones.

机译:NK细胞克隆对急性儿童期前体B细胞白血病的细胞溶解活性受HLA I类在母细胞上的表达和NK克隆的差异KIR表型的影响。

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摘要

Relapse after allo-SCT in patients with acute leukaemia remains a major problem. A beneficial impact of alloreactive natural killer (NK) cells has been reported for myeloid malignancies, but has been questionable for B-lineage ALL. We analysed lysis of primary paediatric precursor-B-ALL blasts by 285 NK cell clones to investigate whether HLA class I expression on the blasts and phenotypic killer cell Ig-like receptor (KIR) expression on NK cells affect the lytic activity against ALL blasts. Precursor-B-ALL blasts with low HLA-I expression were lysed by a majority (79%) of NK cell clones, whereas those with high HLA-I expression showed low susceptibility to NK clones independent of their KIR expression patterns. NK cell activity against susceptible blasts was regulated by differential surface expression of the three major KIRs (CD158a, CD158b, CD158e). NK clones with none of these three KIRs or a single KIR that recognized no ligand, were not inhibited by the targets and exerted higher lysis (P = <0.0005) in comparison to NK clones expressing KIRs with a ligand on the ALL blasts. In conclusion, the quantity of HLA-I expression on precursor-B-ALL blast regulates overall NK cell susceptibility; in case of reduced HLA expression, differential surface expression of KIRs affects NK cell alloreactivity against those blasts.
机译:急性白血病患者在异基因SCT治疗后复发仍然是一个主要问题。据报道,同种异体反应性自然杀伤(NK)细胞对骨髓恶性肿瘤具有有益作用,但对B谱系ALL却存在疑问。我们分析了285个NK细胞克隆对初级儿科前体B-ALL母细胞的裂解,以调查母细胞上的HLA I类表达和NK细胞的表型杀伤细胞Ig样受体(KIR)表达是否影响针对ALL母细胞的裂解活性。具有低HLA-1表达的前体BALL原始细胞被大多数(79%)NK细胞克隆裂解,而具有高HLA-1表达的前胚B-ALL细胞对NK克隆的敏感性较低,而与它们的KIR表达模式无关。 NK细胞对敏感胚细胞的活性受三种主要KIR(CD158a,CD158b,CD158e)表面差异表达的调节。与所有ALL母细胞上表达带有配体的KIR的NK克隆相比,这三个KIR均不具有NK克隆或单个KIR不能识别配体的NK克隆不受靶标抑制,并具有更高的裂解作用(P = <0.0005)。总之,前体-B-ALL blast上HLA-1表达的量调节了整体NK细胞敏感性。在HLA表达降低的情况下,KIR的表面差异表达会影响NK细胞对这些胚细胞的同种反应性。

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