Inhibition of CRAC with a human anti-ORAI1 monoclonal antibody inhibits T-cell-derived cytokine production but fails to inhibit a T-cell-dependent antibody response in the cynomolgus monkey

Gaida, Kevin; Salimi-Moosavi, Hossein; Subramanian, Raju; Almon, Valerie; Knize, Anna; Zhang, Ming; Lin, Fen‐Fen; Nguyen, Hung Q.; Zhou, Lei; Sullivan, John K.; Wong, Min‐Liang; McBride, Helen J.

doi:10.3109/1547691x.2014.915897

Cited by 14 publications

(9 citation statements)

References 38 publications

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“…It is worth noting, however, that attempts to translate the therapeutic potential of these mAbs in vivo have not yet succeeded. In vivo tests in cynomologus monkeys injected with the 2C1.1 mAb revealed unexpected generation of antigen-specific antibodies, despite robust inhibition of T-cell cytokine production (IL-2) ex vivo (114). This result was interpreted to indicate that full inhibition of the CRAC channel is required to suppress the antibody response, rather than the partial suppression achieved by the administration of anti-CRAC channel mAbs.…”

Section: J Monoclonal Antibodiesmentioning

confidence: 99%

Store-Operated Calcium Channels

Prakriya

Lewis

2015

Physiological Reviews

971

1,214

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Store-operated calcium channels (SOCs) are a major pathway for calcium signaling in virtually all metozoan cells and serve a wide variety of functions ranging from gene expression, motility, and secretion to tissue and organ development and the immune response. SOCs are activated by the depletion of Ca(2+) from the endoplasmic reticulum (ER), triggered physiologically through stimulation of a diverse set of surface receptors. Over 15 years after the first characterization of SOCs through electrophysiology, the identification of the STIM proteins as ER Ca(2+) sensors and the Orai proteins as store-operated channels has enabled rapid progress in understanding the unique mechanism of store-operate calcium entry (SOCE). Depletion of Ca(2+) from the ER causes STIM to accumulate at ER-plasma membrane (PM) junctions where it traps and activates Orai channels diffusing in the closely apposed PM. Mutagenesis studies combined with recent structural insights about STIM and Orai proteins are now beginning to reveal the molecular underpinnings of these choreographic events. This review describes the major experimental advances underlying our current understanding of how ER Ca(2+) depletion is coupled to the activation of SOCs. Particular emphasis is placed on the molecular mechanisms of STIM and Orai activation, Orai channel properties, modulation of STIM and Orai function, pharmacological inhibitors of SOCE, and the functions of STIM and Orai in physiology and disease.

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Section: J Monoclonal Antibodiesmentioning

confidence: 99%

Store-Operated Calcium Channels

Prakriya

Lewis

2015

Physiological Reviews

971

1,214

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“…Two independently developed monoclonal antibodies selectively bound ORAI1 (but not ORAI2 and ORAI3), inhibited CRAC currents and SOCE in lymphocytes and suppressed the proliferation and cytokine production of human PBMCs and synovial fluid cells from rheumatoid arthritis patients in vitro (358, 359). In vivo treatment with anti-ORAI1 antibodies ameliorated the severity of xenogeneic T cell–mediated GvHD in mice (358) and reduced the production of IL-2, IL-4, and IL-17 by ex vivo–stimulated T cells isolated from cynomolgus monkeys (360). Collectively, these data suggest that CRAC channel inhibition may be useful for the treatment of autoimmune diseases, transplant rejection, and allergic diseases.…”

Section: Ion Channels As Drug Targets For Immunotherapymentioning

confidence: 99%

“…Whereas proinflammatory cytokine production was impaired in T cells from Orai1 − / − , Orai1 R93W , Stim1 fl/fl CD4-Cre , or Stim2 fl/fl Cd4-Cre mice with various degrees of CRAC channel dysfunction (126, 127, 164, 168, 169), memory CD8 + T cell responses and antibody production were only impaired in Stim1 fl/fl Stim2 fl/fl Cd4-Cre mice whose T cells lack CRAC channel function completely (183). Similarly, inhibitory ORAI1 antibodies partially reduced SOCE and cytokine secretion by T cells but did not impair T-dependent antibody production (360). Patients homozygous for mutations in ORAI1 or STIM1 that lack SOCE completely, but not their heterozygous relatives with partial impairment of SOCE, show increased susceptibility to viral and bacterial infections (26, 123).…”

Section: Ion Channels As Drug Targets For Immunotherapymentioning

confidence: 99%

Ion Channels in Innate and Adaptive Immunity

Feske¹,

Wulff

Skolnik

2015

Annu. Rev. Immunol.

569

616

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Ion channels and transporters mediate the transport of charged ions across hydrophobic lipid membranes. In immune cells, divalent cations such as calcium, magnesium, and zinc have important roles as second messengers to regulate intracellular signaling pathways. By contrast, monovalent cations such as sodium and potassium mainly regulate the membrane potential, which indirectly controls the influx of calcium and immune cell signaling. Studies investigating human patients with mutations in ion channels and transporters, analysis of gene-targeted mice, or pharmacological experiments with ion channel inhibitors have revealed important roles of ionic signals in lymphocyte development and in innate and adaptive immune responses. We here review the mechanisms underlying the function of ion channels and transporters in lymphocytes and innate immune cells and discuss their roles in lymphocyte development, adaptive and innate immune responses, and autoimmunity, as well as recent efforts to develop pharmacological inhibitors of ion channels for immunomodulatory therapy.

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“…The study conducted on monkeys aimed to compare its efficacy with that of FK-506; however, it focused solely on safety evaluation and was not a disease model in particular. 27 Hence, specific indications could not be discussed.…”

Section: Discussionmentioning

confidence: 99%

Anti‐ORAI1 antibody DS‐2741a, a specific CRAC channel blocker, shows ideal therapeutic profiles for allergic disease via suppression of aberrant T‐cell and mast cell activation

et al. 2020

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ORAI1 constitutes the pore‐forming subunit of the calcium release‐activated calcium (CRAC) channel, which is responsible for store‐operated calcium entry into lymphocytes. It is known that ORAI1 is essential for the activation of T cells and mast cells and is considered to be a potent therapeutic target for autoimmune and allergic diseases. Here, we obtained a new humanized antibody, DS‐2741a, that inhibits ORAI1 function. DS‐2741a bound to human‐ORAI1 with high affinity and without cross‐reactivity to rodent Orai1. DS‐2741a demonstrated suppression of CRAC‐mediated human and mouse T‐cell activation and mast cell degranulation in human ORAI1 knock‐in mice. Furthermore, DS‐2741a ameliorated house dust mite antigen‐induced dermatitis in the human ORAI1 knock‐in mouse. Taken together, DS‐2741a inhibited T‐cell and mast cell functions, thus improving skin inflammation in animal models of atopic dermatitis and reinforcing the need for investigation of DS‐2741a for the treatment of allergic diseases in a clinical setting.

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Inhibition of CRAC with a human anti-ORAI1 monoclonal antibody inhibits T-cell-derived cytokine production but fails to inhibit a T-cell-dependent antibody response in the cynomolgus monkey

Cited by 14 publications

References 38 publications

Store-Operated Calcium Channels

Store-Operated Calcium Channels

Ion Channels in Innate and Adaptive Immunity

Anti‐ORAI1 antibody DS‐2741a, a specific CRAC channel blocker, shows ideal therapeutic profiles for allergic disease via suppression of aberrant T‐cell and mast cell activation

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