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ATM anticorps (pSer1981)

ATM Reactivité: Humain WB, IHC, ELISA, FACS, FM Hôte: Souris Monoclonal 10H11-E12 unconjugated
N° du produit ABIN6656104
  • Highlights
    • Anticorps monoclonal anti-ATM protéine kinase pS1981 (MOUSE)
    • Fabriqué par Rockland Immunochemicals, Inc.
    • ID du produit Rockland : 200-301-400
    Antigène Voir toutes ATM Anticorps
    ATM (Ataxia Telangiectasia Mutated (ATM))
    Épitope
    • 29
    • 16
    • 15
    • 13
    • 9
    • 8
    • 7
    • 7
    • 7
    • 5
    • 5
    • 3
    • 2
    • 2
    • 2
    • 2
    • 2
    • 2
    • 2
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    • 1
    AA 1974-1988, pSer1981
    Reactivité
    • 151
    • 78
    • 32
    • 1
    • 1
    • 1
    Humain
    Hôte
    • 130
    • 22
    • 5
    • 2
    Souris
    Clonalité
    • 128
    • 31
    Monoclonal
    Conjugué
    • 75
    • 9
    • 7
    • 5
    • 5
    • 4
    • 4
    • 4
    • 4
    • 4
    • 4
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 3
    • 2
    • 2
    Cet anticorp ATM est non-conjugé
    Application
    • 67
    • 46
    • 39
    • 31
    • 28
    • 23
    • 21
    • 18
    • 17
    • 10
    • 8
    • 7
    • 3
    • 2
    • 2
    • 2
    • 1
    • 1
    • 1
    Western Blotting (WB), Immunohistochemistry (IHC), ELISA, Flow Cytometry (FACS), Fluorescence Microscopy (FM)
     Réactivité croisée
    Humain, Souris, Rat (Rattus)
    Purification
    Anti-ATM phospho S1981 Monoclonal Antibody is directed against human ATM and is useful in determining its presence in various assays. This monoclonal anti-ATM antibody recognizes the phosphorylated epitope in native and over-expressed proteins found in various tissues and extracts.   By ELISA reactivity against SLAFEEGSpQSTTISS at a 1:1600 dilution shows an absorbance >3.000, whereas reactivity against SLAFEEGSQSTTISS shows and absorbance of 0.145.  Reactivity is observed against human ATM.  Cross reactivity with ATM from other mammalian sources has not been tested. The immunogen has 91% sequence homology with mouse ATM.
    Immunogène

    Immunogen: Anti-ATM phospho S1981 Antibody was produced from a synthetic peptide S-L-A-F-E-E-G-Sp-Q-S-T-T-I-S-S corresponding to aa 1974-1988 of human ATM.

    Immunogen Type: Peptide

    Clone
    10H11-E12
    Isotype
    IgG1
  • Indications d'application

    Immunohistochemistry Dilution: Not Recommended

    Application Note: Protein A Purified Mab anti-ATM has been tested by ELISA, Flow Cytometry, IF, and western blotting against both the native and recombinant forms of the protein. The antibody immunoprecipitates ATM from irradiated human and transfected mouse cells.  By immunofluorescence, foci are detected in irradiated human and mouse fibroblasts.  This antibody is not recommended for immunohistochemistry.  Instead, for IHC, use the clone 7C10D8 (p/n 200-301-500).

    ELISA Dilution: 1:20,000 - 1:100,000

    Flow Cytometry Dilution: 5 μg/mL

    Western Blot Dilution: 1:200 - 1:2,000

    IF Microscopy Dilution: 1:100 - 1:500

    Restrictions
    For Research Use only
  • Format
    Liquid
    Buffer

    Buffer: 0.02 M Potassium Phosphate, 0.15 M Sodium Chloride, pH 7.2

    0.01 % (w/v) Sodium Azide

    Stabilizer: None

    Agent conservateur
    Sodium azide
    Précaution d'utilisation
    This product contains Sodium azide: a POISONOUS AND HAZARDOUS SUBSTANCE which should be handled by trained staff only.
    Stock
    RT,4 °C,-20 °C
    Stockage commentaire
    Store Anti-ATM phospho S1981 Antibody at -20° C prior to opening. Aliquot contents and freeze at -20° C or below for extended storage. Avoid cycles of freezing and thawing. Centrifuge product if not completely clear after standing at room temperature. This product is stable for several weeks at 4° C as an undiluted liquid. Dilute only prior to immediate use.
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    Ashraf, Hamidullah, Hasanain, Pandey, Maheshwari, Singh, Siddiqui, Konwar, Sashidhara, Sarkar: "Coumarin-chalcone hybrid instigates DNA damage by minor groove binding and stabilizes p53 through post translational modifications." dans: Scientific reports, Vol. 7, pp. 45287, (2018) (PubMed).

    Gursoy-Yuzugullu, Carman, Serafim, Myronakis, Valente, Price: "Epigenetic therapy with inhibitors of histone methylation suppresses DNA damage signaling and increases glioma cell radiosensitivity." dans: Oncotarget, Vol. 8, Issue 15, pp. 24518-24532, (2018) (PubMed).

    Vadnais, Chen, Fraszczak, Yu, Boulais, Pinder, Frank, Khandanpour, Hébert, Dellaire, Côté, Richard, Orthwein, Drobetsky, Möröy: "GFI1 facilitates efficient DNA repair by regulating PRMT1 dependent methylation of MRE11 and 53BP1." dans: Nature communications, Vol. 9, Issue 1, pp. 1418, (2018) (PubMed).

    Valdez, Li, Murray, Liu, Nieto, Champlin, Andersson: "The PARP inhibitor olaparib enhances the cytotoxicity of combined gemcitabine, busulfan and melphalan in lymphoma cells." dans: Leukemia & lymphoma, Vol. 58, Issue 11, pp. 2705-2716, (2018) (PubMed).

    Chen, Cao, Zhang, Gu, Zhou, Li, Li, Tan, Zeng: "LRRK2 interacts with ATM and regulates Mdm2-p53 cell proliferation axis in response to genotoxic stress." dans: Human molecular genetics, Vol. 26, Issue 22, pp. 4494-4505, (2018) (PubMed).

    Göder, Emmerich, Nikolova, Kiweler, Schreiber, Kühl, Imhof, Christmann, Heinzel, Schneider, Krämer: "HDAC1 and HDAC2 integrate checkpoint kinase phosphorylation and cell fate through the phosphatase-2A subunit PR130." dans: Nature communications, Vol. 9, Issue 1, pp. 764, (2018) (PubMed).

    Higo, Naito, Sumida, Shibamoto, Okada, Nomura, Nakagawa, Yamaguchi, Sakai, Hashimoto, Kuramoto, Ito, Hikoso, Akazawa, Lee, Shiojima, McKinnon, Sakata, Komuro: "DNA single-strand break-induced DNA damage response causes heart failure." dans: Nature communications, Vol. 8, pp. 15104, (2018) (PubMed).

    Fujiwara, Muramatsu, Nishii, Tokunaka, Tahara, Ueno, Yamori, Sugimoto, Seimiya: "Cell-based chemical fingerprinting identifies telomeres and lamin A as modifiers of DNA damage response in cancer cells." dans: Scientific reports, Vol. 8, Issue 1, pp. 14827, (2018) (PubMed).

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    Inoue, Li, Tseng, Beerman, Elia, Bendall, Lemonnier, Kron, Cescon, Hao, Lind, Takayama, Planello, Shen, Shih, Larsen, Li, Snow, Wakeham, Haight, Gorrini, Bassi, Thu, Murakami, Elford, Ueda, Straley et al.: "Mutant IDH1 Downregulates ATM and Alters DNA Repair and Sensitivity to DNA Damage Independent of TET2. ..." dans: Cancer cell, Vol. 30, Issue 2, pp. 337-348, (2017) (PubMed).

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    Wangondu, Teal, Park, Heston, Delecluse, Miller: "DNA Damage Signaling Is Induced in the Absence of Epstein-Barr Virus (EBV) Lytic DNA Replication and in Response to Expression of ZEBRA." dans: PLoS ONE, Vol. 10, Issue 5, pp. e0126088, (2016) (PubMed).

    Modzelewski, Hilz, Crate, Schweidenback, Fogarty, Grenier, Freire, Cohen, Grimson: "Dgcr8 and Dicer are essential for sex chromosome integrity during meiosis in males." dans: Journal of cell science, Vol. 128, Issue 12, pp. 2314-27, (2016) (PubMed).

    Torres, Pandita, Kulak, Kumar, Formstecher, Horikoshi, Mujoo, Hunt, Zhao, Lum, Zaman, Yeaman, White, Pandita: "Role of the Exocyst Complex Component Sec6/8 in Genomic Stability." dans: Molecular and cellular biology, Vol. 35, Issue 21, pp. 3633-45, (2016) (PubMed).

    Qi, Qiu, Gu, Tian, Zhang: "ATM mediates spermidine-induced mitophagy via PINK1 and Parkin regulation in human fibroblasts." dans: Scientific reports, Vol. 6, pp. 24700, (2016) (PubMed).

  • Antigène
    ATM (Ataxia Telangiectasia Mutated (ATM))
    Autre désignation
    ATM (ATM Produits)
    Synonymes
    anticorps ATM, anticorps Atm, anticorps CG6535, anticorps Dmel\\CG6535, anticorps Tefu, anticorps atm, anticorps atm/tefu, anticorps dATM, anticorps tef, anticorps Xatm, anticorps at1, anticorps atdc, anticorps tel1, anticorps telo1, anticorps AT1, anticorps ATA, anticorps ATC, anticorps ATD, anticorps ATDC, anticorps ATE, anticorps TEL1, anticorps TELO1, anticorps AI256621, anticorps C030026E19Rik, anticorps telomere fusion, anticorps ATM serine/threonine kinase L homeolog, anticorps ATM serine/threonine kinase, anticorps ataxia telangiectasia mutated, anticorps ataxia telangiectasia mutated (atm), anticorps serine/threonine-protein kinase ATM, anticorps tefu, anticorps atm.L, anticorps atm, anticorps ATM, anticorps EDI_100660, anticorps CpipJ_CPIJ001772, anticorps BDBG_08252, anticorps PAAG_02532, anticorps MCYG_05088, anticorps VDBG_06833, anticorps ACLA_015700, anticorps LOC5565620, anticorps MGYG_07634, anticorps PGTG_14279, anticorps Atm
    Sujet

    Synonyms: mouse anti-ATM antibody, mouse anti-ATMpS1981 antibody, mouse anti- ATM pS1981 antibody, DKFZp781A0353 antibody, Human phosphatidylinositol 3 kinase homolog antibody, MGC74674 antibody, Serine protein kinase ATM antibody, T cell prolymphocytic leukemia antibody

    Background: Anti ATM pS1981 Antibody is a phospho site specific antibody and recognizes the product of the ATM gene that is mutated in the hereditary disease ataxia-telangiectasia. ATM codes for a protein kinase that acts as a master regulator of cellular responses to DNA double-strand breaks. ATM is normally inactive and the question of how it is activated in the event of DNA damage (due to ionizing radiation for instance) is central to understanding its function. ATM protein is now shown to be present in undamaged cells as an inactive dimer. Low doses of ionizing radiation, which induce only a few DNA breaks, activate at least half of the total ATM protein present, possibly in response to changes in chromatin structure.  The ATM gene encodes a 370- kDa protein that belongs to the phosphoinositide 3-kinase (PI(3)K) superfamily, but which phosphorylates proteins rather than lipids. The 350-amino-acid kinase domain at the carboxy terminus of this large protein is the only segment of ATM with an assigned function. Exposure of cells to IR triggers ATM kinase activity, and this function is required for arrests in G1, S and G2 phases of the cell cycle. Several substrates of the ATM kinase participate in these IR-induced cell-cycle arrests. These include p53, Mdm2 and Chk2 in the G1 checkpoint, Nbs1, Brca1, FancD2 and SMC1 in the transient IR-induced S-phase arrest, and Brca1 and hRad17 in the G2/M checkpoint. Ideal for Cancer, Cell Signaling, Chromatin, Neuroscience and Signal Transduction research.

    Gene Name: ATM

    ID gène
    472
    UniProt
    Q13315
    Pathways
    Signalisation p53, Apoptose, Réparation de l'ADN, Inositol Metabolic Process, Positive Regulation of Response to DNA Damage Stimulus
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