Brilliant Violet 510™ anti-mouse CD4 Antibody

Pricing & Availability
Clone
RM4-5 (See other available formats)
Regulatory Status
RUO
Other Names
L3T4, T4
Isotype
Rat IgG2a, κ
Ave. Rating
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Product Citations
publications
RM4-5_BV510_CD4_Antibody_FC_082312
C57BL/6 mouse splenocytes were stained with CD3 APC and CD4 (clone RM4-5) Brilliant Violet 510™.
  • RM4-5_BV510_CD4_Antibody_FC_082312
    C57BL/6 mouse splenocytes were stained with CD3 APC and CD4 (clone RM4-5) Brilliant Violet 510™.
Compare all formats See Brilliant Violet 510™ spectral data
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100553 125 µL 137€
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100559 50 µg 194€
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Description

CD4 is a 55 kD protein also known as L3T4 or T4. It is a member of the Ig superfamily, primarily expressed on most thymocytes and a subset of T cells, and weakly on macrophages and dendritic cells. It acts as a co-receptor with the TCR during T cell activation and thymic differentiation by binding MHC class II and associating with the protein tyrosine kinase lck.

Product Details
Technical Data Sheet (pdf)

Product Details

Verified Reactivity
Mouse
Antibody Type
Monoclonal
Host Species
Rat
Immunogen
BALB/c mouse thymocytes
Formulation
Phosphate-buffered solution, pH 7.2, containing 0.09% sodium azide and BSA (origin USA).
Preparation
The antibody was purified by affinity chromatography and conjugated with Brilliant Violet 510™ under optimal conditions.
Concentration
µg sizes: 0.2 mg/mL
µL sizes: lot-specific (to obtain lot-specific concentration and expiration, please enter the lot number in our Certificate of Analysis online tool.)
Storage & Handling
The antibody solution should be stored undiluted between 2°C and 8°C, and protected from prolonged exposure to light. Do not freeze.
Application

FC - Quality tested

Recommended Usage

Each lot of this antibody is quality control tested by immunofluorescent staining with flow cytometric analysis. For immunofluorescent staining using the µg size, the suggested use of this reagent is ≤0.5 µg per million cells in 100 µl volume. For immunofluorescent staining using the µl size, the suggested use of this reagent is 5 µl per million cells in 100 µl staining volume or 5 µl per 100 µl of whole blood. It is recommended that the reagent be titrated for optimal performance for each application.

Brilliant Violet 510™ excites at 405 nm and emits at 510 nm. The bandpass filter 510/50 nm is recommended for detection, although filter optimization may be required depending on other fluorophores used. Be sure to verify that your cytometer configuration and software setup are appropriate for detecting this channel. Refer to your instrument manual or manufacturer for support. Brilliant Violet 510™ is a trademark of Sirigen Group Ltd.


Learn more about Brilliant Violet™.

This product is subject to proprietary rights of Sirigen Inc. and is made and sold under license from Sirigen Inc. The purchase of this product conveys to the buyer a non-transferable right to use the purchased product for research purposes only. This product may not be resold or incorporated in any manner into another product for resale. Any use for therapeutics or diagnostics is strictly prohibited. This product is covered by U.S. Patent(s), pending patent applications and foreign equivalents.
Excitation Laser
Violet Laser (405 nm)
Application Notes

The RM4-5 antibody blocks the binding of GK1.5 antibody and H129.19 antibody to CD4+ T cells, but not RM4-4 antibody. Additional reported applications (for the relevant formats) include: blocking of ligand binding, in vivo depletion of CD4+ cells1, and immunohistochemistry of acetone-fixed frozen tissue sections2,3,11 and paraffin-embedded sections11. Clone RM4-5 is not recommended for immunohistochemistry of formalin-fixed paraffin sections. Instead, acetone frozen or zinc-fixed paraffin sections are recommended. The Ultra-LEAF™ Purified antibody (Endotoxin < 0.01 EU/µg, Azide-Free, 0.2 µm filtered) is recommended for functional assays (Cat. No. 100575 and 100576).

Application References
  1. Kruisbeek AM. 1991. In Curr. Protocols Immunol. pp. 4.1.1-4.1.5. (Block, Deplete)
  2. Nitta H, et al. 1997. Cell Vision 4:73. (IHC)
  3. Fan WY, et al. 2001. Exp. Biol. Med. 226:1045.
  4. Muraille E, et al. 2003. Infect. Immun. 71:2704. (IHC)
  5. León-Ponte M, et al. 2007. Blood 109:3139. (FC)
  6. Bourdeau A, et al. 2007. Blood doi:10.1182/blood-2006-08-044370. (FC)
  7. Matsumoto M, et al. 2007.J. Immunol.178:2499. PubMed
  8. Shigeta A, et al. 2008. Blood 112:4915. PubMed
  9. Zaborsky N, et al. 2010. J. Immunol. 184:725. PubMed
  10. Rodrigues-Manzanet R, et al. 2010. P. Natl Acad Sci USA 107:8706. PubMed
  11. Whiteland JL, et al. 1995. J. Histochem. Cytochem. 43:313. (IHC)
Product Citations
  1. Miragaia RJ, et al. 2019. Immunity. 50:493. PubMed
  2. Apte SH, et al. 2020. Clin Transl Immunology. 9:e1209. PubMed
  3. Wang L, et al. 2019. Cell Rep. 29:1848. PubMed
  4. Shibata K, et al. 2022. Nat Commun. 13:6948. PubMed
  5. Wilfahrt D, et al. 2021. Elife. 10:. PubMed
  6. Gern BH, et al. 2021. Cell Host Microbe. 29(4):594-606.e6. PubMed
  7. Wang D, et al. 2018. Immunity. 48:659. PubMed
  8. Lancaster JN, et al. 2019. Nat Commun. 10:2220. PubMed
  9. Baram T, et al. 2021. Cells. 10:. PubMed
  10. Piepke M, et al. 2021. J Neuroinflammation. 18:265. PubMed
  11. Hu W, et al. 2021. Nat Immunol. 22:1163. PubMed
  12. Clemmensen HS, et al. 2021. MBio. 12:. PubMed
  13. Delacher M, et al. 2021. Immunity. 54(4):702-720.e17. PubMed
  14. Plumlee CR, et al. 2020. Cell Host Microbe. 29(1):68-82.e5. PubMed
  15. Konrath KM, et al. 2022. Cell Rep. 38:110318. PubMed
  16. Neubert K, et al. 2014. J Immunol. 192:5830. PubMed
  17. Zhu B, et al. 2021. Immunity. 54(6):1200-1218.e9. PubMed
  18. Lee JY, et al. 2020. Cell. 180(1):79-91.e16.. PubMed
  19. Liu YJ, et al. 2020. Theranostics. 10:5225. PubMed
  20. Woodworth JS, et al. 2021. Nat Commun. 12:6658. PubMed
  21. Marangoni F, et al. 2021. Cell. . PubMed
  22. Latif AL, et al. 2021. Nat Commun. 0.667361111. PubMed
  23. Blankenhaus B, et al. 2014. PLoS Pathog. 10:1003913. PubMed
  24. Zirngibl F, et al. 2021. J Immunother Cancer. 9:. PubMed
  25. Clemmensen HS, et al. 2020. Front Immunol. 11:585359. PubMed
  26. Dikiy S, et al. 2021. Immunity. 54(5):931-946.e11. PubMed
  27. Stump CT, et al. 2021. Open Biol. 11:210245. PubMed
  28. Kawakami R, et al. 2021. Immunity. 54(5):947-961.e8. PubMed
  29. Grzelak A, et al. 2018. Int J Mol Sci. 19:. PubMed
  30. Teixeira L, et al. 2016. Sci Rep. 6:23475. PubMed
  31. Xu Z, et al. 2020. Cancer Immunol Res. 1354:8. PubMed
  32. Kaur A, et al. 2019. Cancer Discov. 9:64. PubMed
  33. Lima-Junior DS, et al. 2021. Cell. . PubMed
  34. Liu Z, et al. 2020. Cell. 178(6):1509-1525.e19.. PubMed
  35. Galle-Treger L, et al. 2016. Nat Commun. 7:13202. PubMed
  36. Echevarría-Vargas IM, et al. 2018. EMBO Mol Med. 10:e8446. PubMed
  37. Fu Y, et al. 2021. Front Cell Dev Biol. 9:689727. PubMed
  38. Jandke A, et al. 2020. Nat Commun. 3.075694444. PubMed
  39. Stacy A, et al. 2021. Cell. 184(3):615-627.e17. PubMed
  40. Renoux F, et al. 2020. Cell Reports. 31(13):107826. PubMed
  41. Phalke SP, et al. 2019. PLoS One. 14:e0218827. PubMed
  42. Revathikumar P, et al. 2018. PLoS One. 13:e0193210. PubMed
  43. Kim DK, et al. 2022. Nat Commun. 13:6292. PubMed
  44. Kwok T, et al. 2022. Front Aging. 3:838943. PubMed
  45. Lofano G, et al. 2015. J Immunol. 195: 1617-1627. PubMed
  46. Blanchfield L,et al. 2017. J Immunol. 10.4049/jimmunol.1700792. PubMed
  47. Jiang L, et al. 2020. Cell. 183(5):1219-1233.e18. PubMed
  48. Filskov J, et al. 2019. Sci Rep. 9:14085. PubMed
  49. Renner K, et al. 2020. Cell Reports. 29(1):135-150.e9.. PubMed
  50. Hoyer FF, et al. 2020. Immunity. 51(5):899-914.e7.. PubMed
  51. Seo GY et al. 2018. Cell host & microbe. 24(2):249-260 . PubMed
  52. Xiao Z, et al. 2022. Mater Today Bio. 15:100297. PubMed
  53. Alterauge D, et al. 2020. Cell Rep. 33:108232. PubMed
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  55. Dammeijer F, et al. 2020. Cancer Cell. 38(5):685-700.e8. PubMed
RRID
AB_2561388 (BioLegend Cat. No. 100553)
AB_2562608 (BioLegend Cat. No. 100559)

Antigen Details

Structure
Ig superfamily, 55 kD
Distribution

Majority of thymocytes, T cell subset

Function
TCR co-receptor, T cell activation
Ligand/Receptor
MHC class II molecule
Cell Type
Dendritic cells, T cells, Thymocytes, Tregs
Biology Area
Immunology
Molecular Family
CD Molecules
Antigen References

1. Barclay A, et al. 1997. The Leukocyte Antigen FactsBook Academic Press.
2. Bierer BE, et al. 1989. Annu. Rev. Immunol. 7:579.
3. Janeway CA. 1992. Annu. Rev. Immunol. 10:645.

Gene ID
12504 View all products for this Gene ID
UniProt
View information about CD4 on UniProt.org

Related FAQs

I am unable to see expression of T cell markers such as CD3 and CD4 post activation.
TCR-CD3 complexes on the T-lymphocyte surface are rapidly downregulated upon activation with peptide-MHC complex, superantigen or cross-linking with anti-TCR or anti-CD3 antibodies. PMA/Ionomycin treatment has been shown to downregulate surface CD4 expression. Receptor downregulation is a common biological phenomenon and so make sure that your stimulation treatment is not causing it in your sample type.
Go To Top Version: 2    Revision Date: 01-29-2013

For Research Use Only. Not for diagnostic or therapeutic use.

 

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This data display is provided for general comparisons between formats.
Your actual data may vary due to variations in samples, target cells, instruments and their settings, staining conditions, and other factors.
If you need assistance with selecting the best format contact our expert technical support team.

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