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Home › Products › G-Protein Coupled Receptors › Formyl Peptide Receptors › Antibodies

Certificate of Analysis

Anti-Human FPR1 (extracellular) Antibody

N-formyl peptide receptor 1, fMLP receptor

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Overview

Cat #: AFR-001
Alternative Name N-formyl peptide receptor 1, fMLP receptor
Lyophilized Powder yes
Type: Polyclonal
Host: Rabbit
Reactivity: h
Immunogen
  • Peptide (C)NFSPWTNDPKERIN, corresponding to amino acid residues 179-192 of human FPR1 (Accession P21462). 2nd extracellular loop.
Accession (Uniprot) Number P21462
Gene ID 2357
Peptide confirmation Confirmed by amino acid analysis and mass spectrometry.
Homology Human only. Not recommended for use with rat and mouse samples.
RRID AB_11121684.
Purity Affinity purified on immobilized antigen.
Form Lyophilized powder. Reconstituted antibody contains phosphate buffered saline (PBS), pH 7.4, 1% BSA, 0.05% NaN3.
Isotype Rabbit IgG.
Storage before reconstitution The antibody ships as a lyophilized powder at room temperature. Upon arrival, it should be stored at -20°C.
Reconstitution 25 µl, 50 µl or 0.2 ml double distilled water (DDW), depending on the sample size.
Antibody concentration after reconstitution 0.8 mg/ml.
Storage after reconstitution The reconstituted solution can be stored at 4°C for up to 1 week. For longer periods, small aliquots should be stored at -20°C. Avoid multiple freezing and thawing. Centrifuge all antibody preparations before use (10000 x g 5 min).
Standard quality control of each lot Western blot analysis.
Applications: ifc, lci, wb
May also work in: ic*, ih*
Western blot
  • Human HL-60 promyelocytic leukemia, human THP-1 acute monocytic leukemia, human T-84 colorectal carcinoma and human U-87 MG glioblastoma cell lysates (1:200).
  • Western blot analysis of human HL-60 promyelocytic leukemia (lanes 1 and 5), human THP-1 acute monocytic leukemia (lanes 2 and 6), human T-84 colorectal carcinoma (lanes 3 and 7) and human U-87 MG glioblastoma (lanes 4 and 8) cell lysates:
    Western blot analysis of human HL-60 promyelocytic leukemia (lanes 1 and 5), human THP-1 acute monocytic leukemia (lanes 2 and 6), human T-84 colorectal carcinoma (lanes 3 and 7) and human U-87 MG glioblastoma (lanes 4 and 8) cell lysates:
    1-4. Anti-Human FPR1 (extracellular) Antibody (#AFR-001), (1:200).
    5-8. Anti-Human FPR1 (extracellular) Antibody, preincubated with Human FPR1 (extracellular) Blocking Peptide (#BLP-FR001).
Indirect flow cytometry
  • Live intact human THP-1 acute monocytic leukemia cells (1:25).
  • The blocking peptide in not suitable for this application.
Scientific background

Chemotactic factors from both Gram-positive and Gram-negative bacteria are short peptides with N-formyl methionine at the N-terminus (extensively reviewed in reference 1). These peptides are released from bacteria during infection and activate formyl peptide receptors (FPR), members of the G-protein coupled receptor (GPCR) superfamily. In humans, the FPR family consists mainly of three receptors, FPR1, FPR2/ALX (formerly FPRL1), and FPR3 (formerly FPRL2) which all couple to the Gi subtype of G-proteins and ultimately lead to the activation of phospholipase C and intracellular Ca2+ increase1,2.

FPRL1, or FPR2/ALX as it is commonly called, is a seven transmembrane protein like all GPCRs. This receptor was originally cloned by screening a HL60 neutrophil cDNA library with a FPR1 cDNA probe3. FPR2/ALX shares 69% identity with FPR1 and despite its high homology, it displays relatively low affinity for fmlf, the most potent N-formyl peptide released by bacteria3.

FPR1 was originally found in neutrophils and later found to be distributed in myeloid and non-myeloid cells as is the case for FPR2/ALX and FPR3 (FPR3 though is not expressed in neutrophils). FPR1 is also expressed in multiple organs and tissues including epithelial cells in organs with secretory functions, endocrine cells, liver hepathocytes, smooth muscle cells and endothelial cells, brain spinal cord and both motor and sensory neurons4. FPR2/ALX has a similar tissue distribution to that of FPR1.

While N-formyl peptides were the first peptides found to activate these receptors, the ligand diversity for FPR has proven to be quite broad and demonstrates to be both pro- and anti-inflammatory. They include peptidic ligands originating from bacterial and viral sources (including HIV), endogenous ligands such as chemokines and annexins, short peptides associated with inflammation and infection. Indeed, peptides from Herpes, Ebola and coronavirus 229E are ligands of FPR11.

Application key:

CBE- Cell-based ELISA, FC- Flow cytometry, ICC- Immunocytochemistry, IE- Indirect ELISA, IF- Immunofluorescence, IFC- Indirect flow cytometry, IHC- Immunohistochemistry, IP- Immunoprecipitation, LCI- Live cell imaging, N- Neutralization, WB- Western blot

Species reactivity key:

H- Human, M- Mouse, R- Rat
Lyophilized Powder
For research purposes only, not for human use
Last Update: 03/01/2024

Specifications

Citations

Citations

Applications

Scientific Background

Specific Control Product

  • Human FPR1 (extracellular) Blocking Peptide (#BLP-FR001) is the original antigen used for immunization during Anti-Human FPR1 (extracellular) Antibody (#AFR-001) generation. The blocking peptide binds and ‘blocks’ Anti-Human FPR1 (extracellular) primary antibody, this makes it a good negative reagent control to help confirm antibody specificity in western blot and immunohistochemistry applications. This control is also often called a pre-adsorption control.

    Human FPR1 (extracellular) Blocking Peptide (#BLP-FR001)

Related Products

Antibodies

  1. Anti-Human FPR2/ALX (extracellular) Antibody (#AFR-002)

Pharmacological tools

Activators/Agonists: peptides/peptide toxins
  1. N-Formyl-Met-Leu-Phe (#GPF-100)

Resources

  • In Focus: Formyl Peptide Receptors

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Resources

  • In Focus: Formyl Peptide Receptors

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