Growth control of hybridoma cells with an artificially induced EpoR-gp130 heterodimer

Kawahara, Masahiro; Ogo, Yuko; Tsumoto, Kouhei; Kumagai, Izumi; Ueda, Hiroshi; Nagamune, Teruyuki

doi:10.1007/s10616-006-9035-2

Cited by 6 publications

(3 citation statements)

References 23 publications

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“…As one of many such examples, replacing the ECD of the erythropoietin (Epo) receptor (EpoR) with those of epidermal growth factor receptor (EGFR), insulin-like growth factor receptor (IGFR), or c-Kit produces an active construct that induces STAT5 phosphorylation and Ba/F3 proliferation in a ligand-dependent manner (Ohashi, Maruyama, Liu, & Yoshimura, 1994). Similarly, fusion of the gp130 ICD to EpoR ECD leads to Epo-mediated activation of STAT1 and STAT3, consistent with activation of the full-length gp130 by its native ligands (Kawahara et al, 2006; Schaeffer et al, 2001). Other examples of receptor ectodomain swapping have been reported for the type I IFN (Pattyn et al, 1999) and IL-4/IL-13 (Fujiwara, Hanissian, Tsytsykova, & Geha, 1997; Heller et al, 2012) systems, and in all cases, the chimeric receptors elicit some extent of activation of the expected Jak/STAT signaling molecules.…”

Section: Ligand–receptor Complex Formation: Geometry and Affinitysupporting

confidence: 59%

Multifarious Determinants of Cytokine Receptor Signaling Specificity

Moraga

Spangler

Mendoza

et al. 2014

Advances in Immunology

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Cytokines play crucial roles in regulating immune homeostasis. Two important characteristics of most cytokines are pleiotropy, defined as the ability of one cytokine to exhibit diverse functionalities, and redundancy, defined as the ability of multiple cytokines to exert overlapping activities. Identifying the determinants for unique cellular responses to cytokines in the face of shared receptor usage, pleiotropy, and redundancy will be essential in order to harness the potential of cytokines as therapeutics. Here, we discuss the biophysical (ligand–receptor geometry and affinity) and cellular (receptor trafficking and intracellular abundance of signaling molecules) parameters that contribute to the specificity of cytokine bioactivities. Whereas the role of extracellular ternary complex geometry in cytokine-induced signaling is still not completely elucidated, cytokine-receptor affinity is known to impact signaling through modulation of the stability and kinetics of ternary complex formation. Receptor trafficking also plays an important and likely underappreciated role in the diversification of cytokine bioactivities but it has been challenging to experimentally probe trafficking effects. We also review recent efforts to quantify levels of intracellular signaling components, as second messenger abundance can affect cytokine-induced bioactivities both quantitatively and qualitatively. We conclude by discussing the application of protein engineering to develop therapeutically relevant cytokines with reduced pleiotropy and redirected biological functionalities.

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Section: Ligand–receptor Complex Formation: Geometry and Affinitysupporting

confidence: 59%

Multifarious Determinants of Cytokine Receptor Signaling Specificity

Moraga

Spangler

Mendoza

et al. 2014

Advances in Immunology

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“…For JAK/STAT cytokine receptors, it has been previously established that genetically modified chimeric receptors in which the extracellular domain (ECD) of a cytokine receptor has been fused with the intracellular domain (ICD) of a different receptor activated signaling in a ligand-dependent manner ( Fujiwara et al, 1997 ; Heller et al, 2012 ; Kawahara et al, 2006 ; Ohashi et al, 1994 ; Pattyn et al, 1999 ; Schaeffer et al, 2001 ). However, for this concept to be practically useful, soluble ligands that co-opt endogenous receptors and assemble non-natural dimers on natural cells and tissues are required.…”

Section: Introductionmentioning

confidence: 99%

Synthekines are surrogate cytokine and growth factor agonists that compel signaling through non-natural receptor dimers

Moraga

Spangler

Mendoza

et al. 2017

eLife

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Cytokine and growth-factor ligands typically signal through homo- or hetero-dimeric cell surface receptors via Janus Kinase (JAK/TYK), or Receptor Tyrosine Kinase (RTK)-mediated trans-phosphorylation. However, the number of receptor dimer pairings occurring in nature is limited to those driven by natural ligands encoded within our genome. We have engineered synthethic cytokines (synthekines) that drive formation of cytokine receptor dimer pairings that are not formed by endogenous cytokines and that are not found in nature, and which activate distinct signaling programs. We show that a wide range of non-natural cytokine receptor hetero-dimers are competent to elicit a signaling output. We engineered synthekine ligands that assembled IL-2Rβ/IL-4Rα or IL-4Rα/IFNAR2 receptor heterodimers, that do not occur naturally, triggering signaling and functional responses distinct from those activated by the endogenous cytokines IL-2, IL-4, and IFN. Furthermore, hybrid synthekine ligands that dimerized a JAK/STAT cytokine receptor with a receptor tyrosine kinase (RTK) also elicited a signaling response. Synthekines represent a new family of synthetic ligands with pre-defined receptors, but 'orphan' functions, that enable the full combinatorial scope of dimeric signaling receptors encoded within the human genome to be exploited for basic research and drug discovery.DOI: http://dx.doi.org/10.7554/eLife.22882.001

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“…The literature is full of studies arguing in favour of both models, making it difficult to navigate and draw strong conclusions. Early studies using chimeric cytokine‐receptors, where the ECD of a cytokine receptor was swapped with the ECD of another cytokine receptor, suggested that the topological requirement for signal activation by cytokines are quite lax [ 142 , 143 , 144 , 145 , 146 ]. In all studies, the chimeric receptor triggered signalling to levels comparable to those induced by the wild‐type receptor.…”

Section: Cytokine‐receptor Complex Stability/kinetics and Signallingmentioning

confidence: 99%

Molecular and cellular factors determining the functional pleiotropy of cytokines

2022

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Cytokines are soluble factors vital for mammalian physiology. Cytokines elicit highly pleiotropic activities, characterized by their ability to induce a wide spectrum of functional responses in a diverse range of cell subsets, which makes their study very challenging. Cytokines activate signalling via receptor dimerization/oligomerization, triggering activation of the JAK (Janus kinase)/STAT (signal transducer and activator of transcription) signalling pathway. Given the strong crosstalk and shared usage of key components of cytokine signalling pathways, a long-standing question in the field pertains to how functional diversity is achieved by cytokines. Here, we discuss how biophysicalfor example, ligand-receptor binding affinity and topologyand cellularfor example, receptor, JAK and STAT protein levels, endosomal compartmentparameters contribute to the modulation and diversification of cytokine responses. We review how these parameters ultimately converge into a common mechanism to fine-tune cytokine signalling that involves the control of the number of Tyr residues phosphorylated in the receptor intracellular domain upon cytokine stimulation. This results in different kinetics of STAT activation, and induction of specific gene expression programs, ensuring the generation of functional diversity by cytokines using a limited set of signalling intermediaries. We describe how these first principles of cytokine signalling have been exploited using protein engineering to design cytokine variants with more specific and less toxic responses for immunotherapy.

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Growth control of hybridoma cells with an artificially induced EpoR-gp130 heterodimer

Cited by 6 publications

References 23 publications

Multifarious Determinants of Cytokine Receptor Signaling Specificity

Multifarious Determinants of Cytokine Receptor Signaling Specificity

Synthekines are surrogate cytokine and growth factor agonists that compel signaling through non-natural receptor dimers

Molecular and cellular factors determining the functional pleiotropy of cytokines

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