Recombinant Mouse PVRIG mFc Chimera Protein, CF

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When Recombinant Mouse PVRIG mFc Chimera (Catalog # 11315-PV) is immobilized at 1 µg/mL (100 µL/well), Recombinant Mouse Nectin‑2/CD112 (3869-N2) binds with an ED50 of 0.150-1.20 µg/mL.
2 μg/lane of Recombinant Mouse PVRIG mFc Chimera Protein (Catalog # 11315-PV) was resolved with SDS-PAGE under reducing (R) and non-reducing (NR) conditions and visualized by Coomassie® Blue staining, showing ...read more

Product Details

Summary
Reactivity MuSpecies Glossary
Applications Bioactivity
Format
Carrier-Free

Order Details

Recombinant Mouse PVRIG mFc Chimera Protein, CF Summary

Details of Functionality
Measured by its binding ability in a functional ELISA. When Recombinant Mouse PVRIG mFc Chimera (Catalog # 11315-PV immobilized at 1 µg/mL (100 µL/well), Recombinant Mouse Nectin-2/CD112 (Catalog # 3869-N2) binds with an ED50 of 0.150-1.20 µg/mL.
Source
Human embryonic kidney cell, HEK293-derived mouse PVRIG protein
Mouse PVRIG
(Ser35-Asp165)
Accession # NP_001365367.1
IEGRMDPMouse IgG2a
(Glu98-Lys330)
N-terminusC-terminus
Accession #
N-terminal Sequence
Glu33, Ser35
Structure / Form
Disulfide-linked homodimer
Protein/Peptide Type
Recombinant Proteins
Purity
>95%, by SDS-PAGE visualized with Silver Staining and quantitative densitometry by Coomassie® Blue Staining.
Endotoxin Note
<0.10 EU per 1 μg of the protein by the LAL method.

Applications/Dilutions

Dilutions
  • Bioactivity
Theoretical MW
41 kDa (monomer).
Disclaimer note: The observed molecular weight of the protein may vary from the listed predicted molecular weight due to post translational modifications, post translation cleavages, relative charges, and other experimental factors.
SDS-PAGE
48-61 kDa, under reducing conditions.

Packaging, Storage & Formulations

Storage
Use a manual defrost freezer and avoid repeated freeze-thaw cycles.
  • 12 months from date of receipt, -20 to -70 °C as supplied.
  • 1 month, 2 to 8 °C under sterile conditions after reconstitution.
  • 3 months, -20 to -70 °C under sterile conditions after reconstitution.
Buffer
Lyophilized from a 0.2 μm filtered solution in PBS with Trehalose.
Purity
>95%, by SDS-PAGE visualized with Silver Staining and quantitative densitometry by Coomassie® Blue Staining.
Reconstitution Instructions
Reconstitute at 500 μg/mL in PBS.

Notes

This product is produced by and ships from R&D Systems, Inc., a Bio-Techne brand.

Alternate Names for Recombinant Mouse PVRIG mFc Chimera Protein, CF

  • C7orf15
  • C7orf15MGC138295
  • CD112R
  • MGC104322
  • MGC138297
  • MGC2463
  • poliovirus receptor related immunoglobulin domain containing
  • Poliovirus receptor-related immunoglobulin domain-containing protein
  • PVRIG
  • transmembrane protein PVRIG

Background

PVRIG (poliovirus receptor related immunoglobulin domain-containing protein), also known as CD112 receptor (CD112R), is an approximately 34 kDa single transmembrane protein in the poliovirus receptor-like protein (PVR) family (1). It is composed of a single extracellular IgV domain, one transmembrane domain, and a long intracellular domain. The intracellular domain contains two tyrosine residues, one within an ITIM-like motif that is a potential docking site for phosphatases (1). The extracellular domain sequence of mouse PVRIG have approximately 64% and 87% similarity with human and rat PVRIG, respectively. The human PVRIG gene is preferentially expressed in lymphocytes, such as T cells and NK cells, but not in monocyte derived dendritic cells (1). PVRIG functions as a cell surface receptor for Nectin-2/CD112, a cell surface protein that is widely expressed on antigen-presenting cells and tumor cells. Disrupting the PVRIG/Nectin-2 interaction enhances human T cell response, suggesting PVRIG is a novel checkpoint for human T cells (1-3). Blocking PVRIG with neutralizing antibody is a feasible approach for NK cell mediated immunotherapy of cancers (4, 5).
  1. Zhu, Y. et al. (2016) J. Exp. Med. 213:167.
  2. Whelan, S. et al. (2019) Cancer Immunol Res. 7:257.
  3. Murter, B. et al. (2019) Cancer Immunol Res. 7:244.
  4. Li, J. et al. (2020) Haematologica. DOI:10.3324/haematol.2020.258574. 
  5. Sanchez-Correa, B. et al. (2019) Cancers (Basel) 11:877.

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