• IHC staining of FFPE human breast carcinoma tissue with NM23 antibody (clone NME1/2738). HIER: boil tissue sections in pH 9 10mM Tris with 1mM EDTA for 20 min and allow to cool before testing.
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NSJ Bioreagents

V9511-20UG

NM23 Antibody / NME1, 20 ug

NM23 Antibody / NME1, 20 ug

$259.00 USD
$259.00 USD
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The nm23 gene, a potential suppressor of metastasis, was originally identified by differential hybridization between two murine melanoma sub-lines, one with a high and the second with a low metastatic capacity. Highly metastatic sub-lines exhibit much lower levels of nm23 than less metastatic cells. Based on sequence analysis, nm23 appears highly related to nucleotide diphosphate kinases (NDP). In humans, NDP kinases A and B are identical to two isotypes of human nm23 homologs, namely nm23-H1 and H2, respectively. nm23-H2 is identical in sequence to PuF, a transcription factor that binds to nuclease hypersensitive elements at positions 142 to 115 of the human c-Myc promotor.

Specifications

Catalog No V9511-20UG
Family Primary antibody
Qty 20 ug
Formulation 0.2 mg/ml in 1X PBS with 0.1 mg/ml BSA (US sourced), 0.05% sodium azide
Format Purified
Clone NME1/2738
Host Animal Mouse
Clonality Monoclonal (mouse origin)
Isotype Mouse IgG2b, kappa
Species Reactivity Human
Application ELISA, WB, IHC-P
Application Details ELISA (order BSA-free format for coating),Western blot: 1-2ug/ml,Immunohistochemistry (FFPE): 1-2ug/ml
Application Note Optimal dilution of the NM23 antibody should be determined by the researcher.
Localization Nucleus, Cytoplasm
Immunogen Recombinant full-length human NME1 protein was used as the immunogen for the NM23 antibody.
Purity Protein A/G affinity
Storage Aliquot the NM23 antibody and store frozen at -20oC or colder. Avoid repeated freeze-thaw cycles.
Limitation This NM23 antibody is available for research use only.
Uniprot # P15531
Status Available
PDF Link https://www.nsjbio.com/tds-pdf/nm23-antibody-nme1-nme12738-v9511
Title NM23 Antibody / NME1
Description The nm23 gene, a potential suppressor of metastasis, was originally identified by differential hybridization between two murine melanoma sub-lines, one with a high and the second with a low metastatic capacity. Highly metastatic sub-lines exhibit much lower levels of nm23 than less metastatic cells. Based on sequence analysis, nm23 appears highly related to nucleotide diphosphate kinases (NDP). In humans, NDP kinases A and B are identical to two isotypes of human nm23 homologs, namely nm23-H1 and H2, respectively. nm23-H2 is identical in sequence to PuF, a transcription factor that binds to nuclease hypersensitive elements at positions 142 to 115 of the human c-Myc promotor.
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