IL15 Trispecific Killer Engagers (TriKE) Make Natural Killer Cells Specific to CD33+ Targets While Also Inducing Persistence,<i>In Vivo</i>Expansion, and Enhanced Function

Vallera, Daniel A.; Felices, Martin; McElmurry, Ron; McCullar, Valarie; Zhou, Xianzheng; Schmohl, Joerg Uwe; Zhang, Bin; Lenvik, Alexander J.; Panoskaltsis‐Mortari, Angela; Verneris, Michael R.; Tolar, Jakub; Cooley, Sarah; Weisdorf, Daniel J.; Blazar, Bruce R.; Miller, Jeffrey S.

doi:10.1158/1078-0432.ccr-15-2710

Cited by 312 publications

(308 citation statements)

References 45 publications

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“…Thus, the data presented in this study support current NK-based therapeutic strategies, including injections of IL2 or IL15 into patients with cancer or targeted therapies, including cytokines such as trispecifi c killer engagers ( 10 ). The cytokines IL12, IL18, IL21, and IFN β decreased STAT5 activity and induced VEGF expression in NK cells; however, these cytokines are also known to be potent activators of NK cell cytotoxicity or cytokine production.…”

Section: Ncr1 -Icresupporting

confidence: 70%

STAT5 Loss Awakens the Dark Force in Natural Killer Cells

Cerwenka

2016

Cancer Discovery

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Summary: Natural killer cells (NK) are commonly considered to be potent antitumor effector cells. The study by Gotthardt and colleagues challenges this concept and reveals that STAT5-defi cient/inhibited NK cells induce angiogenesis and promote tumor progression. These unexpected fi ndings shed new light on potential adverse effects of JAK-STAT inhibitors in the clinics. Cancer Discov; 6(4); 347-9. ©2016 AACR . Gotthardt et al., p. 414 (7). See related article byWithin the tumor microenvironment the interaction of tumor cells and immune cells critically shapes the progression of malignant disease ( 1 ). There is now increasing evidence that certain types of immune cells have the potential not only to effi ciently control, but also to promote tumor growth. For instance, M1 macrophages in tumors can directly kill tumor cells, whereas M2 macrophages support tumor angiogenesis and tumor development. So far, natural killer (NK) cells that effi ciently lyse tumor cells and produce infl ammatory cytokines such as IFN γ and TNF α are mainly associated with potent antitumor activity. Individuals with high NK cell activity have a lower risk to develop cancer ( 2 ). NK cell infi ltration in the tumor is frequently correlated with improved prognosis for patients with cancer, and in many mouse tumor models depletion of NK cells leads to accelerated tumor growth ( 1 ). These studies imply an important role of NK cells in tumor immunosurveillance and support clinical application of NK cell-based therapies in the clinic for cancer treatment. More recently, additional immunoregulatory functions have been attributed to NK cells. In infectious disease, NK cells were shown to kill activated T cells and to produce IL10 and TGF β , resulting in the downregulation of immune responses. Accordingly, a recent study revealed that high numbers of tumor-infi ltrating NK cells did not correlate with favorable prognosis and even might promote tumor progression ( 3 ). The mechanisms underlying NK cell-mediated tumor progression are poorly understood. Moreover, the molecular switches determining NK cell-mediated antitumor or protumor activity have not been elucidated. Strategies to counteract the potential tumor-promoting activity of NK cells could improve current NK cell-based antitumor therapies.The JAK-STAT pathway is activated in many tumor cells and promotes tumor progression. JAK-STAT inhibitors have been extensively explored for cancer treatment, and more than 20 JAK-STAT inhibitors are being tested in clinical trials ( 5 ). The JAK-STAT pathway is also critical for lymphocyte activation, for instance by the cytokines IL2, IL12, IL15, and IL18 that mediate NK cell activity and/or development. Accordingly, NK cells from patients with myeloproliferative neoplasm treated with a JAK inhibitor show impaired functional activity ( 5 ). A previous study by the Sexl lab ( 6 ) Δ / Δ Ncr1 -iCre Tg -Vav-Bcl2 mice showed severe functional defects in vitro , including impaired proliferation and decreased cytotoxicity and IFN γ production toward tumor...

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Section: Ncr1 -Icresupporting

confidence: 70%

STAT5 Loss Awakens the Dark Force in Natural Killer Cells

Cerwenka

2016

Cancer Discovery

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“…PBMCs were collected, and NK cells were enriched as described previously. 4 HL-60, K562, 5 HMC-1.1, HMC-1.2, and ROSA KIT D816V cell lines were maintained in culture as described. 6,7 Functional assays Fluorochrome-conjugated antibodies were from BD Bioscience (anti-CD3), Biolegend (anti-CD117, CD34, CD45, CD2, CD25, CD30, CD56, CD16, CD57, CD158a, CD158b, NKB1, NKG2A, CD107a, tumor necrosis factor-a [TNF-a], interferon-g [IFN-g]), and the CellTrace Violet Cell Proliferation Dye kit and the Live/Dead Fixable Aqua Dead Cell Stain Kit were from Invitrogen.…”

Section: Methodsmentioning

confidence: 99%

“…Flow cytometry and analysis were as described. 4 PBMCs were treated at 30 nmol/L of 161533 TriKE or anti-CD16 scFv as indicated. rhIL-15 was diluted to provide equivalent biological activity to the IL-15 linker of 161533 TriKE.…”

Section: Methodsmentioning

confidence: 99%

Trispecific killer engager CD16xIL15xCD33 potently induces NK cell activation and cytotoxicity against neoplastic mast cells

Yun¹,

Felices²,

Vallera

et al. 2018

Blood Advances

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“…Recently, to take advantage of the stimulation and proliferation capacity of IL-15, 80 a trispecific killer engager (TriKE) construct was proposed using IL-15 to link the 2 antibody arms for the purpose of boosting anti-tumor activity. 88 …”

Section: Retargeting Of Nk Cellsmentioning

confidence: 99%

Bispecific antibodies in cancer immunotherapy

Chen

et al. 2016

Human Vaccines & Immunotherapeutics

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Cancer immunotherapy has recently generated much excitement after the continuing success of the immunomodulating anti-CTLA-4 and anti-PD-1 antibodies against various types of cancers. Aside from these immunomodulating antibodies, bispecific antibodies, chimeric antigen receptor T cells, and other technologies are being actively studied. Among the various approaches to cancer immunotherapy, 2 bispecific antibodies are currently approved for patient care. Many more bispecific antibodies are now in various phases of clinical development and will become the next generation of antibody-based therapies. Further understanding of immunology and advances in protein engineering will help to generate a greater variety of bispecific antibodies to fight cancer. Here, we focus on bispecific antibodies that recruit immune cells to engage and kill tumor cells.

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IL15 Trispecific Killer Engagers (TriKE) Make Natural Killer Cells Specific to CD33+ Targets While Also Inducing Persistence,In VivoExpansion, and Enhanced Function

Cited by 312 publications

References 45 publications

STAT5 Loss Awakens the Dark Force in Natural Killer Cells

STAT5 Loss Awakens the Dark Force in Natural Killer Cells

Trispecific killer engager CD16xIL15xCD33 potently induces NK cell activation and cytotoxicity against neoplastic mast cells

Bispecific antibodies in cancer immunotherapy

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