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Expansion Purification and Functional Assessment of Human Peripheral Blood NK Cells

机译:人外周血的扩增纯化和功能评估 NK细胞

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摘要

Natural killer (NK) cells play an important role in immune surveillance against a variety of infectious microorganisms and tumors. Limited availability of NK cells and ability to expand in vitro has restricted development of NK cell immunotherapy. Here we describe a method to efficiently expand vast quantities of functional NK cells ex vivo using K562 cells expressing membrane-bound IL21, as an artificial antigen-presenting cell (aAPC).NK cell adoptive therapies to date have utilized a cell product obtained by steady-state leukapheresis of the donor followed by depletion of T cells or positive selection of NK cells. The product is usually activated in IL-2 overnight and then administered the following day 1. Because of the low frequency of NK cells in peripheral blood, relatively small numbers of NK cells have been delivered in clinical trials.The inability to propagate NK cells in vitro has been the limiting factor for generating sufficient cell numbers for optimal clinical outcome. Some expansion of NK cells (5-10 fold over 1-2 weeks) has be achieved through high-dose IL-2 alone 2. Activation of autologous T cells can mediate NK cell expansion, presumably also through release of local cytokine 3. Support with mesenchymal stroma or artificial antigen presenting cells (aAPCs) can support the expansion of NK cells from both peripheral blood and cord blood 4. Combined NKp46 and CD2 activation by antibody-coated beads is currently marketed for NK cell expansion (Miltenyi Biotec, Auburn CA), resulting in approximately 100-fold expansion in 21 days.Clinical trials using aAPC-expanded or -activated NK cells are underway, one using leukemic cell line CTV-1 to prime and activate NK cells5 without significant expansion. A second trial utilizes EBV-LCL for NK cell expansion, achieving a mean 490-fold expansion in 21 days6. The third utilizes a K562-based aAPC transduced with 4-1BBL (CD137L) and membrane-bound IL-15 (mIL-15)7, which achieved a mean NK expansion 277-fold in 21 days. Although, the NK cells expanded using K562-41BBL-mIL15 aAPC are highly cytotoxic in vitro and in vivo compared to unexpanded NK cells, and participate in ADCC, their proliferation is limited by senescence attributed to telomere shortening8. More recently a 350-fold expansion of NK cells was reported using K562 expressing MICA, 4-1BBL and IL159.Our method of NK cell expansion described herein produces rapid proliferation of NK cells without senescence achieving a median 21,000-fold expansion in 21 days.
机译:天然杀伤(NK)细胞在针对各种感染性微生物和肿瘤的免疫监视中起着重要作用。 NK细胞的有限可用性和体外扩增的能力限制了NK细胞免疫疗法的发展。在这里,我们描述了一种使用表达膜结合IL21的K562细胞作为人工抗原呈递细胞(aAPC)有效地离体扩增大量功能性NK细胞的方法。迄今为止,NK细胞的过继治疗已经利用了通过稳定获得的细胞产物-供体的白细胞状态降低,然后耗尽T细胞或阳性选择NK细胞。该产品通常在IL-2中激活过夜,然后在第二天 1 给药。由于外周血中NK细胞的频率较低,因此在临床试验中已经递送了相对少量的NK细胞。无法在体外繁殖NK细胞一直是产生足够数量的细胞以获得最佳临床结果的限制因素。单独通过大剂量的IL-2 2 可实现NK细胞的扩增(1-2周内可扩增5-10倍)。可能通过释放局部细胞因子 3 ,自体T细胞的活化可以介导NK细胞的扩增。间充质基质或人工抗原呈递细胞(aAPC)的支持可以支持NK细胞从外周血和脐带血 4 的扩增。目前,通过抗体包被的磁珠结合的NKp46和CD2激活可用于NK细胞扩增(Miltenyi Biotec,Auburn CA),可在21天内扩增约100倍。目前正在进行使用aAPC扩增或活化的NK细胞的临床试验,其中一项使用 白血病细胞系CTV-1激活并激活NK细胞 5 扩张。第二项试验利用EBV-LCL进行NK细胞扩增,获得了平均 6 在21天内扩展了490倍。第三种利用转导的基于K562的aAPC 带有4-1BBL(CD137L)和膜结合IL-15(mIL-15) 7 , NK在21天内扩展了277倍。虽然,NK细胞使用K562-41BBL-mIL15扩增 与体内和体外相比,aAPC具有高度的细胞毒性 到未扩增的NK细胞并参与ADCC,其增殖受到以下因素的限制 衰老归因于端粒缩短 8 。最近是350倍 使用表达M562、4-1BBL和K562的K562报道了NK细胞的扩增 IL15 9 。本文所述的NK细胞扩增方法可使NK细胞快速增殖 没有衰老的情况下,在21天内实现了21,000倍的中值扩张。

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