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MABE1816-25UG Sigma-AldrichAnti-p21/Waf1/Cip1 Antibody, clone HUGO-291

Anti-p21/Waf1/Cip1, clone HUGO-291 Antibody, Cat. No. MABE1816, is a highly specific rat monoclonal antibody that targets p21 and has been tested for use in Immunohistochemistry (Paraffin) and Western Blotting.

MABE1816-25UG

25 μg

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Description
Catalogue Number	MABE1816-25UG
Description	Anti-p21/Waf1/Cip1 Antibody, clone HUGO-291
Alternate Names	Cyclin-dependent kinase inhibitor 1 CDK-interacting protein 1 Melanoma differentiation-associated protein
Background Information	Cyclin-dependent kinase inhibitor 1 (UniProt: P39689; also known as CDK-interacting protein 1, Melanoma differentiation-associated protein, p21) is encoded by the Cdkn1a (also known as Cip1, Waf1) gene (gene ID: 12575) in murine species. p21 belongs to the Cip and Kip family of CDK inhibitors. It binds to and inhibits cyclin-dependent kinase activity, preventing phosphorylation of critical cyclin-dependent kinase substrates and blocking cell cycle progression. It binds tightly to the G1 and S phase kinases, cyclin E/Cdk2, cyclin D/Cdk4, and cyclin A/Cdk2, and effectively inhibits their activity. However, its effects on G2/M kinases is minimal. It binds the cyclin subunit through a conserved Cy1 motif in the N-terminal half and through a weaker and Cy2 motif in the C-terminal half. p21 also inhibits proliferating cell nuclear antigen (PCNA) and binds to and blocks the inactivation of retinoblastoma protein (Rb), which is essential for cell cycle progression. It is an important effector of p53 and is important in the DNA-damage checkpoint. It is expressed in all adult tissues, with 5-fold lower levels observed in the brain. Is cyclin binding site is localized to amino acids 14-24 and CDK binding occurs in the region of 53-58 residues. P21 can undergo phosphorylation at threonine 140 and serine 141, which impairs its binding to PCNA. However, phosphorylation of threonine 140 by PIM2 enhances its stability and inhibits cell proliferation. p21 is shown to suppress tumor growth by promoting cell cycle arrest in response to various stimuli. However, it is often misregulated in various human cancers. (Ref.: Abbas, T., and Dutta, A (2009). Nat Rev Cancer. 9(6); 400-414).

References

Product Information
Format	Purified
Presentation	Purified rat monoclonal antibody IgG2a in buffer containing 0.1 M Tris-Glycine (pH 7.4), 150 mM NaCl with 0.05% sodium azide.

Applications
Application	Anti-p21/Waf1/Cip1, clone HUGO-291 Antibody, Cat. No. MABE1816, is a highly specific rat monoclonal antibody that targets p21 and has been tested for use in Immunohistochemistry (Paraffin) and Western Blotting.
Key Applications	Immunohistochemistry (Paraffin) Western Blotting
Application Notes	Immunohistochemistry (Paraffin) Analysis: A 1:25 dilution from a representative detected p21 in mouse colon tissue sections. Immunohistochemistry (Paraffin) Analysis: A representative lot detected p21 in Immunohistochemistry applications (Munoz-Espin, D., et. al. (2013). Cell. 155(5):1104-18; Le Roux, I., et. al. (2015). Nat Commun.6:8528).

Biological Information
Immunogen	GST/His-tagged full-length murine recombinant p21 protein.
Clone	HUGO-291
Concentration	Please refer to lot specific datasheet.
Host	Rat
Specificity	Clone HUGO-291 is a rat monoclonal antibody that specifically detects p21 protein.
Isotype	IgG2aκ
Species Reactivity	Human Mouse
Species Reactivity Note	Human, Mouse
Antibody Type	Monoclonal Antibody
Entrez Gene Number	NP_031695.1
Gene Symbol	Cdkn1a Cip1 Waf1
Purification Method	Protein G purified
UniProt Number	P39689
Molecular Weight	~26 kDa observed; 17.78 kDa calculated. Uncharacterized bands may be observed in some lysate(s).

Physicochemical Information

Dimensions

Materials Information

Toxicological Information

Safety Information according to GHS

Safety Information

Product Usage Statements
Quality Assurance	Evaluated by Western Blotting in human small intestine tissue lysate. Western Blotting Analysis: 1 µg/mL of this antibody detected p21/Waf1/Cip1 in human small intestine tissue lysate.
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 Conditions	Stable for 1 year at 2-8°C from date of receipt.

Packaging Information
Material Size	25 μg

Transport Information

Supplemental Information

Specifications

Global Trade Item Number
Catalog Number	GTIN
MABE1816-25UG	04061841039075

Documentation

Anti-p21/Waf1/Cip1 Antibody, clone HUGO-291 SDS

Title
Safety Data Sheet (SDS)

Anti-p21/Waf1/Cip1 Antibody, clone HUGO-291 Certificates of Analysis

Title	Lot Number
Anti-p21/Waf1/Cip1, clone HUGO-291 - 3277851	3277851

References

Reference overview	Pub Med ID
Numb is required to prevent p53-dependent senescence following skeletal muscle injury. Le Roux, I; Konge, J; Le Cam, L; Flamant, P; Tajbakhsh, S Nat Commun 6 8528 2015 Show Abstract Regeneration relies on coordinated action of multiple cell types to reconstitute the damaged tissue. Here we inactivate the endocytic adaptor protein Numb in skeletal muscle stem cells prior to chronic or severe muscle injury in mice. We observe two types of senescence in regenerating muscle; a transient senescence in non-myogenic cells of control and Numb mutant mice that partly depends on INK4a/ARF activity, and a persistent senescence in myogenic cells lacking Numb. The senescence levels of Numb-deficient muscle is reduced to wild type levels by an anti-oxidant treatment or p53 ablation, resulting in functional rescue of the regenerative potential in Numb mutants. Ex vivo experiments suggest that Numb-deficient senescent cells recruit macrophages to sustain inflammation and drive fibrosis, two hallmarks of the impaired muscle regeneration in Numb mutants. These findings provide insights into previously reported developmental and oncogenic senescence that are also differentially regulated by p53.	26503169
Programmed cell senescence during mammalian embryonic development. Muñoz-Espín, D; Cañamero, M; Maraver, A; Gómez-López, G; Contreras, J; Murillo-Cuesta, S; Rodríguez-Baeza, A; Varela-Nieto, I; Ruberte, J; Collado, M; Serrano, M Cell 155 1104-18 2013 Show Abstract Cellular senescence disables proliferation in damaged cells, and it is relevant for cancer and aging. Here, we show that senescence occurs during mammalian embryonic development at multiple locations, including the mesonephros and the endolymphatic sac of the inner ear, which we have analyzed in detail. Mechanistically, senescence in both structures is strictly dependent on p21, but independent of DNA damage, p53, or other cell-cycle inhibitors, and it is regulated by the TGF-β/SMAD and PI3K/FOXO pathways. Developmentally programmed senescence is followed by macrophage infiltration, clearance of senescent cells, and tissue remodeling. Loss of senescence due to the absence of p21 is partially compensated by apoptosis but still results in detectable developmental abnormalities. Importantly, the mesonephros and endolymphatic sac of human embryos also show evidence of senescence. We conclude that the role of developmentally programmed senescence is to promote tissue remodeling and propose that this is the evolutionary origin of damage-induced senescence.	24238962

Reference overview

Pub Med ID

Numb is required to prevent p53-dependent senescence following skeletal muscle injury.
Le Roux, I; Konge, J; Le Cam, L; Flamant, P; Tajbakhsh, S
Nat Commun 6 8528 2015

Show Abstract

26503169

Programmed cell senescence during mammalian embryonic development.
Muñoz-Espín, D; Cañamero, M; Maraver, A; Gómez-López, G; Contreras, J; Murillo-Cuesta, S; Rodríguez-Baeza, A; Varela-Nieto, I; Ruberte, J; Collado, M; Serrano, M
Cell 155 1104-18 2013

Show Abstract

24238962

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