Bispecific and trispecific killer cell engagers directly activate human NK cells through CD16 signaling and induce cytotoxicity and cytokine production

GleasonM.K.; VernerisM.R.; TodhunterD.A.; ZhangB.; McCullarV.; ZhouS.X.; Panoskaltsis-MortariA.; WeinerL.M.; ValleraD.A.; MillerJ.S.

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Bispecific and trispecific killer cell engagers directly activate human NK cells through CD16 signaling and induce cytotoxicity and cytokine production

机译：双特异性和三特异性杀伤细胞参与分子通过CD16信号直接激活人类NK细胞并诱导细胞毒性和细胞因子产生

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This study evaluates the mechanism by which bispecific and trispecific killer cell engagers (BiKEs and TriKEs) act to trigger human natural killer (NK) cell effector function and investigates their ability to induce NK cell cytokine and chemokine production against human B-cell leukemia. We examined the ability of BiKEs and TriKEs to trigger NK cell activation through direct CD16 signaling, measuring intracellular Ca2+ mobilization, secretion of lytic granules, induction of target cell apoptosis, and production of cytokine and chemokines in response to the Raji cell line and primary leukemia targets. Resting NK cells triggered by the recombinant reagents led to intracellular Ca2+ mobilization through direct CD16 signaling. Coculture of reagent-treated resting NK cells with Raji targets resulted in significant increases in NK cell degranulation and target cell death. BiKEs and TriKEs effectively mediated NK cytotoxicity of Raji targets at high and loweffector-to-target ratios and maintained functional stability after 24 and 48 hours of culture in human serum. NK cell production of IFN-γ, TNF-α, granulocyte macrophage colony-stimulating factor (GM-CSF), interleukin (IL)-8, macrophage inflammatory protein (MIP)-1α, and regulated and normal T cell expressed and secreted (RANTES) was differentially induced in the presence of recombinant reagents and Raji targets. Moreover, significant increases in NK cell degranulation and enhancement of IFN-γ production against primary acute lymphoblastic leukemia and chronic lymphocytic leukemia targets were induced with reagent treatment of resting NK cells. In conclusion, BiKEs and TriKEs directly trigger NK cell activation through CD16, significantly increasing NK cell cytolytic activity and cytokine production against tumor targets, showing their therapeutic potential for enhancing NK cell immunotherapies for leukemias and lymphomas.

机译：这项研究评估了双特异性和三特异性杀伤细胞参与分子（BiKEs和TriKEs）触发人类自然杀伤（NK）细胞效应子功能的机制，并研究了它们诱导NK细胞细胞因子和趋化因子抵抗人类B细胞白血病的能力。我们检查了BiKEs和TriKEs通过直接CD16信号触发NK细胞活化，测量细胞内Ca2 +动员，溶胞颗粒的分泌，诱导靶细胞凋亡以及对Raji细胞系和原发性白血病产生反应的细胞因子和趋化因子的能力。目标。重组试剂触发的静息NK细胞通过直接CD16信号传导导致细胞内Ca2 +动员。试剂处理的静息NK细胞与Raji靶标的共培养导致NK细胞脱粒和靶标细胞死亡的显着增加。 BiKEs和TriKEs在高和低效应物-靶标比率下有效介导Raji靶的NK细胞毒性，并在人血清中培养24和48小时后保持功能稳定性。 NK细胞产生的IFN-γ，TNF-α，粒细胞巨噬细胞集落刺激因子（GM-CSF），白介素（IL）-8，巨噬细胞炎性蛋白（MIP）-1α以及调节和正常T细胞的表达和分泌（在重组试剂和Raji靶标的存在下差异诱导RANTES）。而且，通过静息NK细胞的试剂处理，诱导了针对原发性急性淋巴细胞白血病和慢性淋巴细胞性白血病靶细胞的NK细胞脱颗粒的显着增加和IFN-γ产生的增强。总之，BiKE和TriKE通过CD16直接触发NK细胞活化，显着提高NK细胞对肿瘤靶标的细胞溶解活性和细胞因子的产生，显示出它们增强白血病和淋巴瘤NK细胞免疫疗法的治疗潜力。

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《Molecular cancer therapeutics》 |2012年第12期|共11页
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GleasonM.K.; VernerisM.R.; TodhunterD.A.; ZhangB.; McCullarV.; ZhouS.X.; Panoskaltsis-MortariA.; WeinerL.M.; ValleraD.A.; MillerJ.S.;
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1. Bispecific and trispecific killer cell engagers directly activate human NK cells through CD16 signaling and induce cytotoxicity and cytokine production [J] . GleasonM.K., VernerisM.R., TodhunterD.A., Molecular cancer therapeutics . 2012,第12期

机译：双特异性和三特异性杀伤细胞参与分子通过CD16信号直接激活人类NK细胞并诱导细胞毒性和细胞因子产生
2. Cytotoxic potential of IL-15-activated cytokine-induced killer cells against human neuroblastoma cells [J] . Cappel Claudia, Huenecke Sabine, Suemmerer Anica, Pediatric blood & cancer . 2016,第12期

机译：IL-15激活的细胞因子诱导的杀伤细胞对人神经母细胞瘤细胞的细胞毒性潜力
3. Signal transducer and activator of transcription 3 (STAT3) and Suppressor of Cytokine Signaling (SOCS3) balance controls cytotoxicity and IL-10 expression in decidual-like natural killer cell line NK-92. [J] . Braunschweig A, Poehlmann TG, Busch S, AJRI: American Journal of Reproductive Immunology . 2011,第4期

机译：信号转导和转录激活因子3（STAT3）和细胞因子信号传导抑制因子（SOCS3）的平衡控制着蜕膜样自然杀伤细胞系NK-92中的细胞毒性和IL-10表达。
4. Anti-breast tumor activities of CpG ODN-activated dendritic cells co-cultured with cytokine-induced killer cells in vitro and in vivo [C] . Gabriele Ghisellini Asian Pacific Confederation of Chemical Engineering congress . 2008

机译：CpG ODN激活的树突状细胞与细胞因子诱导的杀伤细胞在体外和体内共培养的抗乳腺癌肿瘤活性
5. CD16xCD33 bispecific killer cell engager (BiKE) activates natural killer (NK) cells from myelodysplastic syndrome (MDS) patients against primary MDS and myeloidderived suppressor cell (MDSC) CD33-positive targets. [D] . Gleason, Michelle K. 2014

机译：CD16xCD33双特异性杀伤细胞接合剂（BiKE）激活来自骨髓增生异常综合征（MDS）患者的自然杀伤（NK）细胞，以抵抗原发性MDS和髓样抑制细胞（MDSC）CD33阳性靶标。
6. Bispecific and trispecific killer cell engagers directly activate human NK cells through CD16 signaling and induce cytotoxicity and cytokine production [O] . Michelle K. Gleason, Michael R. Verneris, Deborah A. Todhunter, -1

机译：双特异性和三特异性杀手细胞烘焙者通过CD16信号传导直接激活人NK细胞并诱导细胞毒性和细胞因子产生
7. Bispecific and Trispecific Killer Cell Engagers Directly Activate Human NK Cells through CD16 Signaling and Induce Cytotoxicity and Cytokine Production [O] . Michelle K. Gleason, Michael R. Verneris, Deborah A. Todhunter, 2012

机译：双特异性和三特异性杀手细胞烘焙者通过CD16信号传导直接激活人NK细胞，并诱导细胞毒性和细胞因子产生

Bispecific and trispecific killer cell engagers directly activate human NK cells through CD16 signaling and induce cytotoxicity and cytokine production

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