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MAB386 Anti-Myelin Basic Protein Antibody, a.a. 82-87

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MAB386
1 mL  
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      Overview

      Replacement Information

      Key Spec Table

      Species ReactivityKey ApplicationsHostFormatAntibody Type
      B, Ch, Gp, H, M, R, Sh, RbELISA, ICC, IHC, RIA, WBRCulture SupernatantMonoclonal Antibody
      Description
      Catalogue NumberMAB386
      Brand Family Chemicon®
      Trade Name
      • Chemicon
      DescriptionAnti-Myelin Basic Protein Antibody, a.a. 82-87
      Alternate Names
      • MBP
      Background InformationThe two major components of CNS myelin are Myelin Basic Protein (MBP) and proteolipid protein (PLP), occuring in roughly equimolar proportions. There are many neurological disorders associated with deficiencies of myelin assembly and structure. For example Multiple Sclerosis is a human disease due to multiple factors but generally characterized by the degradation of the myelin sheath. MBP ususally refers to the 18.5 kDa isoform, which is one of the most abundant proteins of the myelin sheath of adult human and bovine CNS. Genetically, MBP is the product of differential splicing of a single mRNA transcript. In humans there are 4 isoforms, 21.5, 20.2, 18.5, and 17.2 kDa. Thus, MBP are present in multiple isoforms, part of a large family of developmentally expressed, translocatable, and highly post-translationally modifed proteins with multiple binding partners. Structurally, MBP displays a predominately unorganized form with greater than 75% in random coil. Other non-CNS related functions of myelin include insulin induction and glucagon release from pancreatic islets.
      References
      Product Information
      FormatCulture Supernatant
      HS Code3002 15 90
      Control
      • Brain tissue
      PresentationLiquid containing 0.1% sodium azide.
      Quality LevelMQ100
      Applications
      ApplicationAnti-Myelin Basic Protein Antibody, a.a. 82-87 is an antibody against Myelin Basic Protein for use in ELISA, IC, IH, RIA & WB.
      Key Applications
      • ELISA
      • Immunocytochemistry
      • Immunohistochemistry
      • Radioimmunoassay
      • Western Blotting
      Application NotesImmunohistochemistry:
      A previous lot of this antibody was used on frozen sections.

      ELISA/RIA:
      1:1000 dilution of a previous lot of this antibody was used in ELISA/RIA.

      Western Blotting:
      Identifies an 18-20kDa band in westerns.

      Optimal working dilutions must be determined by end user.
      Biological Information
      ImmunogenBovine myelin basic protein
      Epitopea.a. 82-87
      Clone12
      ConcentrationPlease refer to the Certificate of Analysis for the lot-specific concentration.
      HostRat
      SpecificityReacts with MBP from all species tested. It reacts weakly with peptides ending in the phe 91 where the 91-92 phe-phe bond is broken. Synthetic peptide 82-99 reacts very well as does intact MBP. Mapped to the region DENPVV.
      IsotypeIgG2a
      Species Reactivity
      • Bovine
      • Chicken
      • Guinea Pig
      • Human
      • Mouse
      • Rat
      • Sheep
      • Rabbit
      Species Reactivity NoteReacts with MBP from all species tested including human, bovine, sheep, rabbit, mouse, rat, guinea pig and chicken.
      Antibody TypeMonoclonal Antibody
      Entrez Gene Number
      Entrez Gene SummaryThe protein encoded by the classic MBP gene is a major constituent of the myelin sheath of oligodendrocytes and Schwann cells in the nervous system. However, MBP-related transcripts are also present in the bone marrow and the immune system. These mRNAs arise from the long MBP gene (otherwise called "Golli-MBP") that contains 3 additional exons located upstream of the classic MBP exons. Alternative splicing from the Golli and the MBP transcription start sites gives rise to 2 sets of MBP-related transcripts and gene products. The Golli mRNAs contain 3 exons unique to Golli-MBP, spliced in-frame to 1 or more MBP exons. They encode hybrid proteins that have N-terminal Golli aa sequence linked to MBP aa sequence. The second family of transcripts contain only MBP exons and produce the well characterized myelin basic proteins. This complex gene structure is conserved among species suggesting that the MBP transcription unit is an integral part of the Golli transcription unit and that this arrangement is important for the function and/or regulation of these genes
      Gene Symbol
      • MBP
      • MGC99675
      • Golli-mbp
      Purification MethodUnpurified
      UniProt Number
      UniProt SummaryFUNCTION: SwissProt: P02686 # The classic group of MBP isoforms (isoform 4-isoform 14) are with PLP the most abundant protein components of the myelin membrane in the CNS. They have a role in both its formation and stabilization. The smaller isoforms might have an important role in remyelination of denuded axons in multiple sclerosis. The non- classic group of MBP isoforms (isoform 1-isoform 3/Golli-MBPs) may preferentially have a role in the early developing brain long before myelination, maybe as components of transcriptional complexes, and may also be involved in signaling pathways in T- cells and neural cells. Differential splicing events combined to optional post-translational modifications give a wide spectrum of isomers, each of them having maybe a specialized function. Induces T-cell proliferation.
      SIZE: 304 amino acids; 33117 Da
      SUBUNIT: Homodimer; isoform 3 exists as a homodimer.
      SUBCELLULAR LOCATION: Myelin membrane; Peripheral membrane protein; Cytoplasmic side. Note=Cytoplasmic side of myelin.
      TISSUE SPECIFICITY: MBP isoforms are found in both the central and the peripheral nervous system, whereas Golli-MBP isoforms are expressed in fetal thymus, spleen and spinal cord, as well as in cell lines derived from the immune system.
      DEVELOPMENTAL STAGE: Expression turns on abruptly in fetus of 14 to 16 weeks. Even smaller isoforms seem to be produced during embryogenesis, some of these persisting in the adult. Expression of isoform MBP2 is more evident at 16 weeks and its relative proportion declined thereafter.
      PTM: Several charge isomers of MBP; C1 (the most cationic, least modified, and most abundant form), C2, C3, C4, C5, C6, C7, C8-A and C8-B (the least cationic form); are produced as a result of optional PTM, such as phosphorylation, deamidation of glutamine or asparagine, arginine citrullination and methylation. C8-A and C8-B contain each two mass isoforms termed C8-A(H), C8-A(L), C8-B(H) and C8-B(L), (H) standing for higher and (L) for lower molecular weight. C3, C4 and C5 are phosphorylated. The ratio of methylated arginine residues decreases in aging, making the protein more cationic. & The N-terminal alanine is acetylated (isoform 3, isoform 4, isoform 5 and isoform 6). & Arg-241 was found to be 6% monomethylated and 60% symmetrically dimethylated.
      DISEASE: SwissProt: P02686 # The reduction in the surface charge of citrullinated and/or methylated MBP could result in a weakened attachment to the myelin membrane. This mechanism could be operative in demyelinating diseases such as chronical multiple sclerosis (MS), and fulminating MS (Marburg disease).
      SIMILARITY: SwissProt: P02686 ## Belongs to the myelin basic protein family.
      Molecular Weight18-20 kDa
      Physicochemical Information
      Dimensions
      Materials Information
      Toxicological Information
      Safety Information according to GHS
      Safety Information
      Product Usage Statements
      Quality AssuranceEvaluated by Western Blot on Mouse brain lysates.

      Western Blot Analysis:
      1:500 dilution of antibody lot detected four isoforms of MBP on 10 µg of Mouse brain lysates.
      Usage Statement
      • Unless otherwise stated in our catalog or other company documentation accompanying the product(s), our products are intended for research use only and are not to be used for any other purpose, which includes but is not limited to, unauthorized commercial uses, in vitro diagnostic uses, ex vivo or in vivo therapeutic uses or any type of consumption or application to humans or animals.
      Storage and Shipping Information
      Storage ConditionsStable for 1 year at -20ºC from date of receipt.
      Packaging Information
      Material Size1 mL
      Transport Information
      Supplemental Information
      Specifications
      Global Trade Item Number
      Catalogue Number GTIN
      MAB386 04053252264856

      Documentation

      Anti-Myelin Basic Protein Antibody, a.a. 82-87 MSDS

      Title

      Safety Data Sheet (SDS) 

      Anti-Myelin Basic Protein Antibody, a.a. 82-87 Certificates of Analysis

      TitleLot Number
      Anti-Myelin Basic Protein, a.a. 82-87 3083055
      Anti-Myelin Basic Protein, a.a. 82-87 - 2384662 2384662
      Anti-Myelin Basic Protein, a.a. 82-87 - 2446682 2446682
      Anti-Myelin Basic Protein, a.a. 82-87 - NG1820780 NG1820780
      Anti-Myelin Basic Protein, a.a. 82-87 - 1974466 1974466
      Anti-Myelin Basic Protein, a.a. 82-87 - 2089859 2089859
      Anti-Myelin Basic Protein, a.a. 82-87 - 2204897 2204897
      Anti-Myelin Basic Protein, a.a. 82-87 - 2266471 2266471
      Anti-Myelin Basic Protein, a.a. 82-87 - 2326323 2326323
      Anti-Myelin Basic Protein, a.a. 82-87 - 3018721 3018721

      References

      Reference overviewApplicationSpeciesPub Med ID
      Nuclear export inhibitors avert progression in preclinical models of inflammatory demyelination.
      Haines, JD; Herbin, O; de la Hera, B; Vidaurre, OG; Moy, GA; Sun, Q; Fung, HY; Albrecht, S; Alexandropoulos, K; McCauley, D; Chook, YM; Kuhlmann, T; Kidd, GJ; Shacham, S; Casaccia, P
      Nature neuroscience  18  511-20  2015

      Show Abstract
      25706475 25706475
      Transplantation of mouse embryonic stem cell-derived oligodendrocytes in the murine model of globoid cell leukodystrophy.
      Kuai, XL; Ni, RZ; Zhou, GX; Mao, ZB; Zhang, JF; Yi, N; Liu, ZX; Shao, N; Ni, WK; Wang, ZW
      Stem cell research & therapy  6  30  2015

      Show Abstract
      25888852 25888852
      Systemic inflammation in early neonatal mice induces transient and lasting neurodegenerative effects.
      Cardoso, FL; Herz, J; Fernandes, A; Rocha, J; Sepodes, B; Brito, MA; McGavern, DB; Brites, D
      Journal of neuroinflammation  12  82  2015

      Show Abstract
      25924675 25924675
      An aberrant sugar modification of BACE1 blocks its lysosomal targeting in Alzheimer's disease.
      Kizuka, Y; Kitazume, S; Fujinawa, R; Saito, T; Iwata, N; Saido, TC; Nakano, M; Yamaguchi, Y; Hashimoto, Y; Staufenbiel, M; Hatsuta, H; Murayama, S; Manya, H; Endo, T; Taniguchi, N
      EMBO molecular medicine  7  175-89  2015

      Show Abstract
      25592972 25592972
      Peripheral nervous system plasmalogens regulate Schwann cell differentiation and myelination.
      da Silva, TF; Eira, J; Lopes, AT; Malheiro, AR; Sousa, V; Luoma, A; Avila, RL; Wanders, RJ; Just, WW; Kirschner, DA; Sousa, MM; Brites, P
      The Journal of clinical investigation  124  2560-70  2014

      Show Abstract
      24762439 24762439
      Progressive disorganization of paranodal junctions and compact myelin due to loss of DCC expression by oligodendrocytes.
      Bull, SJ; Bin, JM; Beaumont, E; Boutet, A; Krimpenfort, P; Sadikot, AF; Kennedy, TE
      The Journal of neuroscience : the official journal of the Society for Neuroscience  34  9768-78  2014

      Show Abstract
      25031414 25031414
      Gene co-regulation by Fezf2 selects neurotransmitter identity and connectivity of corticospinal neurons.
      Lodato, S; Molyneaux, BJ; Zuccaro, E; Goff, LA; Chen, HH; Yuan, W; Meleski, A; Takahashi, E; Mahony, S; Rinn, JL; Gifford, DK; Arlotta, P
      Nature neuroscience  17  1046-54  2014

      Show Abstract
      Immunocytochemistry24997765 24997765
      Myelin basic protein induces neuron-specific toxicity by directly damaging the neuronal plasma membrane.
      Zhang, J; Sun, X; Zheng, S; Liu, X; Jin, J; Ren, Y; Luo, J
      PloS one  9  e108646  2014

      Show Abstract
      25255088 25255088
      Glial ankyrins facilitate paranodal axoglial junction assembly.
      Chang, KJ; Zollinger, DR; Susuki, K; Sherman, DL; Makara, MA; Brophy, PJ; Cooper, EC; Bennett, V; Mohler, PJ; Rasband, MN
      Nature neuroscience  17  1673-81  2014

      Show Abstract
      25362471 25362471
      Effects of intra-amniotic lipopolysaccharide and maternal betamethasone on brain inflammation in fetal sheep.
      Kuypers, E; Jellema, RK; Ophelders, DR; Dudink, J; Nikiforou, M; Wolfs, TG; Nitsos, I; Pillow, JJ; Polglase, GR; Kemp, MW; Saito, M; Newnham, JP; Jobe, AH; Kallapur, SG; Kramer, BW
      PloS one  8  e81644  2013

      Show Abstract
      24358119 24358119

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      Categories

      Life Science Research > Antibodies and Assays > Primary Antibodies