This antibody recognizes CD112, a type I transmembrane glycoprotein expressed by myelomonocytic and megakaryocytic cells, and by CD34+ hematopoietic progenitors.

Applications

Flow Cytometry, IP, IHC-Fr

Dilutions

Flow Cytometry: 1-4 µg/ml.

Reactivity

Human

Immunogen

NIH/3T3 cells transfected with human Nectin-2.

Host

Mouse

Clonality

Monoclonal

Clone ID

R2.525

Isotype

IgG1

Light Chains

kappa

Conjugate

Unconjugated

Purification

Protein A chromatography.

Concentration

1 mg/ml

Product Form

Liquid

Formulation

Supplied in Phosphate Buffered Saline, pH 7.4, with 15 mM Sodium Azide.

Storage

Shipped at 4°C. Upon delivery aliquot and store at -20°C. Avoid freeze/thaw cycles.

Synonyms

CD 112, CD112, CD112 antigen, Herpes virus entry mediator B, Herpes virus entry protein B, Herpesvirus entry mediator B, Herpesvirus entry protein B, Hve B, HveB, Nectin-2, Nectin2, Poliovirus receptor like 2, Poliovirus receptor related 2, Poliovirus receptor related 2 (herpesvirus entry mediator B), Poliovirus receptor related protein 2, Poliovirus receptor-related protein 2, PRR 2, PRR2, PVRL 2, PVRL2, PVRL2_HUMAN, PVRR 2, PVRR2

Isotype Controls

Suitable Secondaries

See all Anti-Mouse IgG Secondaries →

Disclaimer

This product is for research use only. It is not intended for diagnostic or therapeutic use.

Citations for this Clone (1)

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Cell-to-cell spread of wild-type herpes simplex virus type 1, but not of syncytial strains, is mediated by the immunoglobulin-like receptors that mediate virion entry, nectin1 (PRR1/HveC/HIgR) and nectin2 (PRR2/HveB).

References: Anti-Nectin 2 Antibody [R2.525] (ab23601)

Abstract:

The immunoglobulin-like receptors that mediate entry of herpes simplex virus type 1 (HSV-1) into human cells were found to mediate the direct cell-to-cell spread of wild-type virus. The receptors here designated Nectin1alpha and -delta and Nectin2alpha were originally designated HIgR, PRR1/HveC, and PRR2alpha/HveB, respectively. We report the following. (i) Wild-type HSV-1 spreads from cell to cell in J cells expressing nectin1alpha or nectin1delta but not in parental J cells that are devoid of entry receptors. A monoclonal antibody to nectin1, which blocks entry, also blocked cell-to-cell spread in nectin1-expressing J cells. Moreover, wild-type virus did not spread from a receptor-positive to a receptor-negative cell. (ii) The antibody to nectin1 blocked transmission of wild-type virus in a number of human cell lines, with varying efficiencies, suggesting that nectin1 is the principal mediator of wild-type virus spread in a variety of human cell lines. (iii) Nectin1 did not mediate cell fusion induced by the syncytial strains HSV-1(MP) and HFEM-syn. (iv) Nectin2alpha could serve as a receptor for spread of a mutant virus carrying the L25P substitution in glycoprotein D, but not of wild-type virus, in agreement with its ability to mediate entry of the mutant but not of wild-type virus.

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