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AB113531

Anti-FPR1 抗体

Anti-FPR1 antibody

5

(2 Reviews)

|

(16 Publications)

Rabbit Polyclonal FPR1 antibody. Suitable for WB, IHC-P, ICC/IF and reacts with Human samples. Cited in 16 publications. Immunogen corresponding to Synthetic Peptide within Human fMet-Leu-Phe receptor conjugated to Keyhole Limpet Haemocyanin.

別名を表示する

N-formyl peptide receptor 1, N-formylpeptide chemoattractant receptor, fMet-Leu-Phe receptor, fMLP receptor, FPR1

3 Images
Immunohistochemistry (Formalin/PFA-fixed paraffin-embedded sections) - Anti-FPR1 antibody (AB113531)
  • IHC-P

Unknown

Immunohistochemistry (Formalin/PFA-fixed paraffin-embedded sections) - Anti-FPR1 antibody (AB113531)

ab113531 at 5ug/ml staining FPR1 in Formalin-Fixed, Paraffin-Embedded Human spleen tissue by Immunohistochemistry.

Immunocytochemistry/ Immunofluorescence - Anti-FPR1 antibody (AB113531)
  • ICC/IF

Unknown

Immunocytochemistry/ Immunofluorescence - Anti-FPR1 antibody (AB113531)

ab113531 at a 1/100 dilution staining FPR1 in Human MCF7 cells by Immunofluorescence. The cells on the right were incubated with the immunizing peptide.

Western blot - Anti-FPR1 antibody (AB113531)
  • WB

Unknown

Western blot - Anti-FPR1 antibody (AB113531)

All lanes:

Western blot - Anti-FPR1 antibody (ab113531) at 1/500 dilution

Lane 1:

K562 cell extract

Lane 2:

K562 cell extract with immunizing peptide

Predicted band size: 38 kDa

false

Key facts

宿主種

Rabbit

クローン性

Polyclonal

アイソタイプ

IgG

キャリアフリー

No

交差種

Human

アプリケーション

IHC-P, ICC/IF, WB

applications

免疫原

Synthetic Peptide within Human fMet-Leu-Phe receptor conjugated to Keyhole Limpet Haemocyanin. The exact immunogen used to generate this antibody is proprietary information.

P21462

Reactivity data

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出荷温度及び保存条件

製品の状態
Liquid
精製方法
Affinity purification Protein A
バッファー組成
pH: 7.4 Preservative: 0.02% Sodium azide Constituents: PBS, 50% Glycerol (glycerin, glycerine), 0.88% Sodium chloride
出荷温度
Blue Ice
短期保存温度
+4°C
長期保存温度
-20°C
保管に関する情報
Stable for 12 months at -20°C

補足情報

This supplementary information is collated from multiple sources and compiled automatically.

FPR1 also known as fMet-Leu-Phe receptor (fMLP receptor) is a G-protein coupled receptor with a molecular mass of approximately 38 kDa. It primarily expresses on the surface of myeloid cells like neutrophils monocytes and macrophages. FPR1 mediates responses to chemotactic factors guiding immune cells to sites of infection or inflammation by detecting formyl peptides from bacterial and mitochondrial origins.
Biological function summary

FPR1 plays an important role in initiating and regulating innate immune responses. It is not part of a complex but functions through association with G-proteins which activate intracellular signaling cascades. Its activation leads to rapid cellular responses such as chemotaxis superoxide production and degranulation which are essential for effective pathogen clearance by the immune system.

Pathways

FPR1 involvement in chemotaxis and MAP kinase signaling highlights its importance in immune surveillance. It integrates signals from bacteria-derived formylated peptides linking the external chemotactic cues to the internal migratory response of leukocytes. Other proteins like the chemokine CXC receptor family operate in complementary pathways to FPR1 collectively orchestrating immune trafficking and activation.

Defective FPR1 function is implicated in chronic inflammatory conditions and impaired host defense mechanisms such as systemic lupus erythematosus (SLE) and certain bacterial infections. In SLE altered FPR1 activity disrupts normal immune response contributing to disease persistence. FPR1's interaction with proteins like CD14 further highlights its role in modulating inflammatory responses relevant to these conditions.

製品プロトコール

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ターゲットの情報

Pattern recognition G-protein coupled receptor (PRR/GPCR) involved in innate recognition of N-formyl-methionyl peptides derived from invading microbes and host mitochondria as pathogen- and damage-associated molecular patterns (PAMPs and DAMPs). Functions as a sensor of PAMPs and DAMPs released upon microbial infection or tissue damage, triggering immune cell activation and chemotaxis to eliminate pathogens and restore tissue homeostasis (PubMed : 24108355, PubMed : 25605714, PubMed : 35217703, PubMed : 36064945). Peptide binding leads to conformational changes coupled to heterotrimeric G(i) protein signaling. Upon GDP to GTP conversion, G(i)-alpha subunit dissociates from G-beta and G-gamma subunits. Free G(i)-alpha subunit inhibits cyclic adenylate cyclase and cAMP synthesis whereas the G-beta and G-gamma dimer activates downstream phospholipase C-beta and phosphoinositide 3-kinase signaling cascades leading to Ca(2+) influx (PubMed : 10514456, PubMed : 15153520, PubMed : 1712023, PubMed : 25605714, PubMed : 35217703, PubMed : 36064945). Displays two affinity states for peptide agonists, low and high, likely accounting for selective signaling of myeloid cell functions at different phases of the inflammatory response. Subnanomolar concentrations of peptide agonists induce myeloid cell chemotaxis, whereas micromolar concentrations trigger degranulation and superoxide production (PubMed : 2161213, PubMed : 2176894, PubMed : 24108355, PubMed : 25605714). May recognize a myriad of bacterial signal peptides indicative of an evolutionary conserved detection mechanism in host defense against bacterial infection. Triggers bactericidal functions of neutrophils and phagocytes in response to N-formyl-Met-Leu-Phe (fMLF) which is part of the signal peptide sequences of hundreds distinct bacterial strains (PubMed : 25605714). In the homeostatic wound healing response to tissue injury, senses 'necrotaxis' DAMP-type signals released in the form of mitochondria-derived N-formylated peptides and guides neutrophil trafficking toward necrotic cells within the injury site (By similarity). In the context of antitumor immunity, interacts with ANXA1 and guides dendritic cell positioning in close proximity to necrotic tumor cells, allowing for tumor-associated antigen uptake and cross-presentation to T cells (PubMed : 24108355, PubMed : 26516201). Receptor for TAFA4, mediates its effects on chemoattracting macrophages, promoting phagocytosis and increasing reactive oxygen species (ROS) release (PubMed : 25109685). Receptor for cathepsin CTSG, leading to increased phagocyte chemotaxis (PubMed : 15210802). Beyond canonical N-terminal formylated peptide agonists, can also be activated by C-terminal amidated peptides, which appear to all share a tripartite structure motif oriented around a carboxyl group (PubMed : 24108355, PubMed : 25605714). Differential signaling is also defined by receptor oligomerization state. Pro-resolving ligands, such as lipoxin A4 or ANXA1, induce the formation of FPR1 : FPR2 heterodimers triggering proapoptotic JNK pathway in neutrophils (PubMed : 24108355).. (Microbial infection) Used by Y. pestis as a receptor on human immune cells. Upon infection, Y. pestis releases N-formyl peptides that activate FPR1-mediated immune signaling and chemotaxis. This leads to Y. pestis docking on FPR1 via the lcrV needle cap protein of its type III secretion system (T3SS) followed by the delivery of effector proteins into host immune cells, ultimately triggering immune cell apoptosis.
See full target information fMet-Leu-Phe receptor

文献 (16)

Recent publications for all applications. Explore the full list and refine your search

Cell biology and toxicology 41:97 PubMed40483281

2025

Annexin A1-FPR1 Interaction in dendritic cells promotes immune microenvironment modulation in Thyroid Cancer.

Applications

Unspecified application

Species

Unspecified reactive species

Hongwei Jiang,Lirun Kuang,Tianyi Zhang,Xupeng Zhao

RSC medicinal chemistry 16:1397-1409 PubMed39886349

2025

Development of small-molecule fluorescent probes targeting neutrophils -formyl peptide receptors.

Applications

Unspecified application

Species

Unspecified reactive species

Qi Xu,Kalwant S Authi,Liliya N Kirpotina,Igor A Schepetkin,Mark T Quinn,Agostino Cilibrizzi

Cell research 33:585-603 PubMed37337030

2023

An invasive zone in human liver cancer identified by Stereo-seq promotes hepatocyte-tumor cell crosstalk, local immunosuppression and tumor progression.

Applications

Unspecified application

Species

Unspecified reactive species

Liang Wu,Jiayan Yan,Yinqi Bai,Feiyu Chen,Xuanxuan Zou,Jiangshan Xu,Ao Huang,Liangzhen Hou,Yu Zhong,Zehua Jing,Qichao Yu,Xiaorui Zhou,Zhifeng Jiang,Chunqing Wang,Mengnan Cheng,Yuan Ji,Yingyong Hou,Rongkui Luo,Qinqin Li,Liang Wu,Jianwen Cheng,Pengxiang Wang,Dezhen Guo,Waidong Huang,Junjie Lei,Shang Liu,Yizhen Yan,Yiling Chen,Sha Liao,Yuxiang Li,Haixiang Sun,Na Yao,Xiangyu Zhang,Shiyu Zhang,Xi Chen,Yang Yu,Yao Li,Fengming Liu,Zheng Wang,Shaolai Zhou,Huanming Yang,Shuang Yang,Xun Xu,Longqi Liu,Qiang Gao,Zhaoyou Tang,Xiangdong Wang,Jian Wang,Jia Fan,Shiping Liu,Xinrong Yang,Ao Chen,Jian Zhou

Nature immunology 23:518-531 PubMed35354953

2022

Neutrophils direct preexisting matrix to initiate repair in damaged tissues.

Applications

Unspecified application

Species

Unspecified reactive species

Adrian Fischer,Juliane Wannemacher,Simon Christ,Tim Koopmans,Safwen Kadri,Jiakuan Zhao,Mahesh Gouda,Haifeng Ye,Martin Mück-Häusl,Peter W Krenn,Hans-Günther Machens,Reinhard Fässler,Philipp-Alexander Neumann,Stefanie M Hauck,Yuval Rinkevich

Frontiers in pharmacology 12:696697 PubMed34393780

2021

The Role of Formyl Peptide Receptor 1 in Uterine Contraction During Parturition.

Applications

Unspecified application

Species

Unspecified reactive species

Chaolu Chen,Shuaiying Zhu,Long Bai,Meihua Sui,Danqing Chen

Annals of translational medicine 8:1174 PubMed33241023

2020

Inhibition of formyl peptide receptor 1 activity suppresses tumorigenicity and attenuates the invasion and migration of lung adenocarcinoma cells under hypoxic conditions .

Applications

Unspecified application

Species

Unspecified reactive species

Bo Huang,Hongrong Guo,Jie Ding,Jun Li,Hongjuan Wang,Jianqun Xu,Quan Zheng,Lijun Zhou,Qin Dai

Cells 9: PubMed33255171

2020

New Pieces in the Puzzle of uPAR Role in Cell Migration Mechanisms.

Applications

Unspecified application

Species

Unspecified reactive species

Anna Gorrasi,Anna Maria Petrone,Anna Li Santi,Mariaevelina Alfieri,Nunzia Montuori,Pia Ragno

Journal of the American Heart Association 9:e017820 PubMed33225820

2020

Aging Impairs Mitochondrial Function and Mitophagy and Elevates Interleukin 6 Within the Cerebral Vasculature.

Applications

Unspecified application

Species

Unspecified reactive species

Daniel J Tyrrell,Muriel G Blin,Jianrui Song,Sherri C Wood,Daniel R Goldstein

Respirology (Carlton, Vic.) 26:233-240 PubMed33078507

2020

Acute cigarette smoke-induced eQTL affects formyl peptide receptor expression and lung function.

Applications

Unspecified application

Species

Unspecified reactive species

Simon D Pouwels,Valerie R Wiersma,Immeke E Fokkema,Marijn Berg,Nick H T Ten Hacken,Maarten van den Berge,Irene Heijink,Alen Faiz

Scientific reports 10:17249 PubMed33057069

2020

Application of small molecule FPR1 antagonists in the treatment of cancers.

Applications

Unspecified application

Species

Unspecified reactive species

Djevdet S Ahmet,Haneen A Basheer,Anwar Salem,Di Lu,Amin Aghamohammadi,Patrick Weyerhäuser,Andrea Bordiga,Juman Almeniawi,Sabah Rashid,Patricia A Cooper,Steven D Shnyder,Victoria Vinader,Kamyar Afarinkia
View all publications

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