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Anti-AXL (extracellular)-FITC Antibody

Anti-AXL (extracellular)-FITC Antibody

ArtNr	ALO-ATR-032-F-5x50ul
Hersteller	Alomone
Menge	5 x 50 ul
Quantity options	10 x 50 ul 2 x 50 ul 50 ul 5 x 50 ul
Kategorie	Oncology Antibodies By Cell Type Blastoma Carcinoma Hematology Leukemia Sarcoma Flow Cytometry Primary Antibodies
Typ	Antibody Polyclonal
Format	Lyophilized
Applikationen	FC
Specific against	Human (Homo sapiens), Mouse (Murine, Mus musculus), Rat (Rattus norvegicus)
Host	Rabbit
Isotype	IgG
Konjugat/Tag	FITC
Purity	Affinity purified on immobilized antigen.
Formula	PBS pH7.4, 1% BSA with 0.05% sodium azide
Sequence	(C)RLAYQGQDTPEVLMD, corresponding to amino acid residues 368 - 382 of human AXL
ECLASS 10.1	32160702
ECLASS 11.0	32160702
UNSPSC	12352203
Versandbedingung	Raumtemperatur
Lieferbar
Specificity	Polyclonal
Manufacturer - Type	Antibodies
Manufacturer - Applications	FC, LCI
Manufacturer - Category	Antibodies
Manufacturer - Targets	AXL Receptor Tyrosine Kinase, Tyrosine-Protein Kinase Receptor UFO, AXL Oncogene, Tyro7, UFO, ARK
Manufacturer - Conjugate / Tag	Fluorescein isothiocyanate (FITC)
Country of Origin	Israel
Shipping Temperature	Shipped at room temperature. Product as supplied can be stored intact at room temperature for several weeks. For longer periods, it should be stored at -20°C
Storage Conditions	Storage before Reconstitution: The antibody ships as a lyophilized powder at room temperature. Upon arrival, it should be stored at -20°C - Storage after Reconstitution: The reconstituted solution can be stored at 4°C, protected from the light, 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).
Manufacturer - Format	Lyophilized powder
Short description	A Rabbit Polyclonal Antibody to AXL (extracellular) conjugated to the fluorescent dye FITC
Description	AXL Receptor Tyrosine Kinase, Tyrosine-Protein Kinase Receptor UFO, AXL Oncogene, Tyro7, UFO, ARK - A Rabbit Polyclonal Antibody to AXL (extracellular) conjugated to the fluorescent dye FITC
Clonality	Polyclonal
Homology	Mouse, Rat – 14 out of 15 amino acids residues identical
Standard quality control of each lot	Western blot analysis (unlabeled antibody, #ATR-032), and direct flow cytometry (labeled antibody).
Peptide confirmation	Confirmed by amino acid analysis and mass spectrometry
Reconstitution	50 µl double distilled water (DDW).
Antibody Concentration After Reconstitution	1 mg/ml
Preservative	1% BSA, 0.05% NaN3
Immunogen Location	Extracellular, N-term.
Specificity	AXL
Immunogen source species	Human
PH	7, 4
UNSPSC	41116161
Antigen Preadsorption Control	1 µg peptide per 1 µg antibody
Scientific Background	AXL, also known as Tyrosine Kinase Receptor UFO and Tyro7, is a member of the receptor tyrosine kinase TAM family, that includes the receptors Tyro3, AXL and MERTK 1, 2.The TAM family receptors are widely expressed in normal cells and tissues, such as monocytes, platelets, endothelial cells, brain and heart, where they regulate cell survival, non-inflammatory clearance of apoptotic cells by phagocytic cells, natural killer cell differentiation, platelet aggregation, and more 1, 2.The TAM family receptors show structural similarities with other tyrosine kinase receptors, that is, an extracellular N-terminal domain containing two immunoglobulin-like and two fibronectin 3 domains, followed by a hydrophobic single pass transmembrane domain, and a cytoplasmic C-terminal tail containing a tyrosine kinase domain1, 2.Axl and the other TAM receptors can be activated via their ligands, growth arrest specific 6 protein (Gas6) and Protein S (Pros1), which are members of the family of vitamin K-dependent proteins 3.Both AXL receptor and its high affinity ligand Gas6, are key regulators of immune cell activation, and have been shown to be expressed in cancer cells where they promote survival and invasion and contribute to resistance to various therapies 3, 4, 5. AXL expression is linked to increased risk of metastasis and poor survival in a variety of solid cancers including breast cancer, non-small cell lung carcinoma, ovarian cancer, and clear cell renal carcinoma 3, 4. AXL activation in cancer cells and various stromal cells also results in tumor microenvironment deregulation, leading to modulation of angiogenesis, fibrosis, immune response and hypoxia 3, 4.Based on these findings, AXL has been identified as a critical therapeutic target for solid cancers, and indeed several therapeutic modalities including small molecules and monoclonal antibodies, are currently being developed 2, 4.

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ALO-ATR-032-F-5x50ul-safety-datasheet.pdf