CD16 +NK-92 and anti-CD123 monoclonal antibody prolongs survival in primary human acute myeloid leukemia xenografted mice

Brent A. Williams; Xing-Hua Wang; Jeffrey V. Leyton; Sonam Maghera; Bishoy Deif; Raymond M. Reilly; Mark D. Minden; Armand Keating

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CD16 +NK-92 and anti-CD123 monoclonal antibody prolongs survival in primary human acute myeloid leukemia xenografted mice

机译：CD16 + NK-92和抗CD123单克隆抗体可延长原代人急性髓细胞白血病异种移植小鼠的生存期

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Patients with acute myeloid leukemia (AML) often relapse after initial therapy because of persistence of leukemic stem cells that frequently express the IL-3 receptor alpha chain CD123. Natural killer (NK) cell-based therapeutic strategies for AML show promise and we explore the NK cell lines, NK-92 and CD16 ~(+) NK-92, as a treatment for AML. NK-92 has been tested in phase I clinical trials with minimal toxicity; irradiation prior to infusion prevents risk of engraftment. The CD16 negative NK-92 parental line was genetically modified to express the high affinity Fc gamma receptor, enabling antibody-dependent cell-mediated cytotoxicity, which we utilized in combination with an anti-CD123 antibody to target leukemic stem cells. NK-92 was preferentially cytotoxic against leukemic stem and progenitor cells compared with bulk leukemia in in vitro assays, while CD16 ~(+) NK-92 in combination with an anti-CD123 mAb mediated antibody-dependent cell-mediated cytotoxicity against CD123 ~(+) leukemic targets. Furthermore, NK-92 infusions (with or without prior irradiation) improved survival in a primary AML xenograft model. Mice xenografted with primary human AML cells had a superior survival when treated with irradiated CD16 ~(+)NK-92 cells and an anti-CD123 monoclonal antibody (7G3) versus treatment with irradiated CD16 ~(+)NK-92 cells combined with an isotype control antibody. In this proof-of-principle study, we show for the first time that a CD16 ~(+)NK-92 cell line combined with an antibody that targets a leukemic stem cell antigen can lead to improved survival in a relevant pre-clinical model of AML.

机译：急性髓细胞性白血病（AML）的患者通常在初次治疗后复发，原因是白血病干细胞的持续表达经常表达IL-3受体α链CD123。基于自然杀伤（NK）细胞的AML治疗策略显示出前景，我们探索NK细胞系NK-92和CD16〜（+）NK-92作为AML的治疗方法。 NK-92已在I期临床试验中进行了测试，毒性最低。输注前进行辐射可防止植入风险。对CD16阴性NK-92亲本系进行了基因修饰，以表达高亲和力Fcγ受体，从而实现了抗体依赖性细胞介导的细胞毒性，我们将其与抗CD123抗体联合用于靶向白血病干细胞。与大量白血病相比，NK-92在体外测定中优先针对白血病干细胞和祖细胞，而CD16〜（+）NK-92与抗CD123 mAb介导的抗体依赖性细胞介导的细胞毒性对CD123〜（ +）白血病目标。此外，NK-92输注（有或无事先照射）可改善原发性AML异种移植模型的存活率。与经辐照的CD16〜（+）NK-92细胞和经放射的CD16〜（+）NK-92细胞及抗CD123〜（+）NK-92细胞和抗CD123单克隆抗体（7G3）相比，异种移植有原代人AML细胞的小鼠存活率更高。同型对照抗体。在这项原理验证研究中，我们首次显示CD16〜（+）NK-92细胞系与靶向白血病干细胞抗原的抗体相结合，可以在相关的临床前模型中提高生存率AML。

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《Haematologica 》 |2018年第10期| 共10页
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Brent A. Williams; Xing-Hua Wang; Jeffrey V. Leyton; Sonam Maghera; Bishoy Deif; Raymond M. Reilly; Mark D. Minden; Armand Keating;
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1. Development of a new anti-CD123 monoclonal antibody to target the human CD123 antigen as an acute myeloid leukemia cancer stem cell biomarker [J] . Abdollahpour-Alitappeh Meghdad, Razavi-Vakhshourpour Sepand, Abolhassani Mohsen Biotechnology and Applied Biochemistry . 2018 ,第6期

机译：开发新的抗CD123单克隆抗体，以靶向人CD123抗原作为急性髓性白血病癌症干细胞生物标志物
2. HUMAN ASCITES DOES NOT AFFECT NK-92 CYTOTOXICITY AND INTRAPERITONEAL COMPARED WITH INTRAVENOUS ADMINISTRATION OF NK-92 SHOWS SUPERIOR SURVIVAL IN HUMAN OVARIAN CANCER XENOGRAFTED MICE [J] . Marcus P., Swift B. E., Warrington J. M., Cytotherapy . 2018 ,第5Suppla期

机译：与NK-92的静脉内给药相比，人类腹水不会影响NK-92细胞毒性和腹膜内，所述NK-92显示出人卵巢癌异种移植小鼠的优异存活
3. A Phase 1 study of the safety, pharmacokinetics and anti-leukemic activity of the anti-CD123 monoclonal antibody CSL360 in relapsed, refractory or high-risk acute myeloid leukemia [J] . He Simon Z., Busfield Samantha, Ritchie David S., Leukemia and lymphoma . 2015 ,第5期

机译：关于CD123单克隆抗体CSL360在复发性，难治性或高危急性髓系白血病中的安全性，药代动力学和抗白血病活性的1期研究
4. Antibody-targeting of Drug-loaded Micelles to Acute Myeloid Leukemia Cells [C] . Michael P. Baranello, Steven Tau, Danielle S.W. Benoit Society for Biomaterials annual meeting and exposition . 2015

机译：载药胶束针对急性髓样白血病细胞的抗体靶向。
5. Characterization of the biology of human acute myeloid leukemia stem cells. [D] . Hope, Kristin Jill. 2007

机译：人类急性髓细胞白血病干细胞生物学特性的表征。
6. CD16+NK-92 and anti-CD123 monoclonal antibody prolongs survival in primary human acute myeloid leukemia xenografted mice [O] . Brent A. Williams, Xing-Hua Wang, Jeffrey V. Leyton, 2018

机译：CD16 + NK-92和抗CD123单克隆抗体可延长原代人急性髓细胞白血病异种移植小鼠的生存期
7. CD16+NK-92 and anti-CD123 monoclonal antibody prolongs survival in primary human acute myeloid leukemia xenografted mice [O] . Brent A. Williams, Xing-Hua Wang, Jeffrey V. Leyton, 2018

机译：CD16 + NK-92和抗CD123单克隆抗体延长原发性人急性髓性白血病异种移植小鼠的存活
8. Chemotherapy in a Transplantable Myeloid Leukemia in Brown Norway Rats: Studies on BNML as a Model for Human Acute Myeloid Leukemia [R] . Golly, L. P. 1980

机译：Brown Norway大鼠可移植骨髓性白血病的化疗：BNmL作为人类急性髓性白血病模型的研究

CD16 +NK-92 and anti-CD123 monoclonal antibody prolongs survival in primary human acute myeloid leukemia xenografted mice

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