Rabbit Recombinant Monoclonal GSDMD antibody. Carrier free. Suitable for WB and reacts with Mouse samples.
IgG
Rabbit
pH: 7.2 - 7.4
Constituents: PBS
Liquid
Monoclonal
IP | Flow Cyt | WB | IHC-P | ICC/IF | |
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Mouse | Not recommended | Not recommended | Tested | Not recommended | Not recommended |
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Gasdermin-DPrecursor of a pore-forming protein that plays a key role in host defense against pathogen infection and danger signals (PubMed:26375003, PubMed:26375259, PubMed:26611636, PubMed:27383986, PubMed:27385778, PubMed:27418190). This form constitutes the precursor of the pore-forming protein: upon cleavage, the released N-terminal moiety (Gasdermin-D, N-terminal) binds to membranes and forms pores, triggering pyroptosis (PubMed:26375003, PubMed:26375259, PubMed:26611636, PubMed:27383986, PubMed:27385778, PubMed:27418190).Gasdermin-D, N-terminalPromotes pyroptosis in response to microbial infection and danger signals (PubMed:26375003, PubMed:26375259, PubMed:26611636, PubMed:27383986, PubMed:27385778, PubMed:27418190, PubMed:32820063, PubMed:34289345, PubMed:35705808, PubMed:37988464, PubMed:38530158, PubMed:38538834, PubMed:38632402). Produced by the cleavage of gasdermin-D by inflammatory caspases CASP1 or CASP4/CASP11 in response to canonical, as well as non-canonical (such as cytosolic LPS) inflammasome activators (PubMed:26375003, PubMed:26375259, PubMed:26611636, PubMed:27383986, PubMed:27385778, PubMed:27418190, PubMed:35705808, PubMed:38632402). After cleavage, moves to the plasma membrane where it strongly binds to inner leaflet lipids, including monophosphorylated phosphatidylinositols, such as phosphatidylinositol 4-phosphate, bisphosphorylated phosphatidylinositols, such as phosphatidylinositol (4,5)-bisphosphate, as well as phosphatidylinositol (3,4,5)-bisphosphate, and more weakly to phosphatidic acid and phosphatidylserine (PubMed:27339137, PubMed:27383986). Homooligomerizes within the membrane and forms pores of 10-15 nanometers (nm) of inner diameter, allowing the release of mature interleukin-1 (IL1B and IL18) and triggering pyroptosis (PubMed:27383986, PubMed:29195811, PubMed:29274245, PubMed:33883744, PubMed:38530158, PubMed:38538834). Gasdermin pores also allow the release of mature caspase-7 (CASP7) (PubMed:35705808). In some, but not all, cells types, pyroptosis is followed by pyroptotic cell death, which is caused by downstream activation of ninjurin-1 (NINJ1), which mediates membrane rupture (cytolysis) (PubMed:38632402). Also forms pores in the mitochondrial membrane, resulting in release of mitochondrial DNA (mtDNA) into the cytosol (PubMed:37001519). Gasdermin-D, N-terminal released from pyroptotic cells into the extracellular milieu rapidly binds to and kills both Gram-negative and Gram-positive bacteria, without harming neighboring mammalian cells, as it does not disrupt the plasma membrane from the outside due to lipid-binding specificity (PubMed:27383986). Under cell culture conditions, also active against intracellular bacteria, such as Listeria monocytogenes (PubMed:27383986). Also active in response to MAP3K7/TAK1 inactivation by Yersinia toxin YopJ, which triggers cleavage by CASP8 and subsequent activation (PubMed:30361383, PubMed:30381458). Required for mucosal tissue defense against enteric pathogens (PubMed:37988464). Activation of the non-canonical inflammasome in brain endothelial cells can lead to excessive pyroptosis, leading to blood-brain barrier breakdown (PubMed:38632402). Strongly binds to bacterial and mitochondrial lipids, including cardiolipin. Does not bind to unphosphorylated phosphatidylinositol, phosphatidylethanolamine nor phosphatidylcholine (PubMed:27383986).Gasdermin-D, p13Transcription coactivator produced by the cleavage by CASP3 or CASP7 in the upper small intestine in response to dietary antigens (PubMed:37327784). Required to maintain food tolerance in small intestine: translocates to the nucleus and acts as a coactivator for STAT1 to induce the transcription of CIITA and MHC class II molecules, which in turn induce type 1 regulatory T (Tr1) cells in upper small intestine (PubMed:37327784).Gasdermin-D, p40Produced by the cleavage by papain allergen (PubMed:35794369). After cleavage, moves to the plasma membrane and homooligomerizes within the membrane and forms pores of 10-15 nanometers (nm) of inner diameter, allowing the specific release of mature interleukin-33 (IL33), promoting type 2 inflammatory immune response (PubMed:35749514, PubMed:35794369).
Gsdmdc1, Gsdmd, Gsdmdc1, Gasdermin-D, Gasdermin domain-containing protein 1
Rabbit Recombinant Monoclonal GSDMD antibody. Carrier free. Suitable for WB and reacts with Mouse samples.
IgG
Rabbit
pH: 7.2 - 7.4
Constituents: PBS
Liquid
Monoclonal
Yes
EPR20859-147
Affinity purification Protein A
Blue Ice
+4°C
+4°C
Do Not Freeze
ab255985 is the carrier-free version of Anti-cleaved C-terminal GSDMD antibody [EPR20859-147] ab255603.
Our RabMAb® technology is a patented hybridoma-based technology for making rabbit monoclonal antibodies. For details on our patents, please refer to RabMAb® patents.
This product is a recombinant monoclonal antibody, which offers several advantages including:
For more information, read more on recombinant antibodies.
Our carrier-free antibodies are typically supplied in a PBS-only formulation, purified and free of BSA, sodium azide and glycerol. The carrier-free buffer and high concentration allow for increased conjugation efficiency.
This conjugation-ready format is designed for use with fluorochromes, metal isotopes, oligonucleotides, and enzymes, which makes them ideal for antibody labelling, functional and cell-based assays, flow-based assays (e.g. mass cytometry) and Multiplex Imaging applications.
Use our conjugation kits for antibody conjugates that are ready-to-use in as little as 20 minutes with 1 minute hands-on-time and 100% antibody recovery: available for fluorescent dyes, HRP, biotin and gold.
This product is compatible with the Maxpar® Antibody Labeling Kit from Fluidigm, without the need for antibody preparation. Maxpar® is a trademark of Fluidigm Canada Inc.
This supplementary information is collated from multiple sources and compiled automatically.
Cleaved C-terminal GSDMD also known as cleaved gasdermin D is a protein involved in cellular processes influencing cell death. It is a fragment derived from gasdermin D (GSDMD) after cleavage which is facilitated by inflammatory caspases. This cleavage removes an inhibitory domain allowing the active N-terminal to initiate its functions. The molecular weight of GSDMD is approximately 53 kDa. Cleaved GSDMD is often detected through methods like Western blot particularly in immune cells such as macrophages and monocytes.
Cleaved C-terminal GSDMD contributes significantly to the process of pyroptosis a form of programmed cell death that is inflammation-driven. This fragmented form is important for forming pores in the cell membrane leading to cellular lysis and the release of pro-inflammatory signals. Gasdermin D including its cleaved form is not known to be part of a large complex on its own but acts autonomously after activation by other proteins like caspase-1.
Cleaved C-terminal GSDMD participates actively in the inflammatory response particularly in the inflammasome pathway. The protein is closely linked to caspases like caspase-1 that activate it leading to pyroptotic cell death. This pathway also intersects with other innate immune components such as the NLRP3 inflammasome to magnify inflammatory signals and recruit additional immune cells to sites of infection or damage.
Cleaved C-terminal GSDMD plays a role in conditions featuring excessive inflammation like septicemia and inflammatory bowel disease (IBD). In these diseases aberrant activation and overproduction of cleaved GSDMD can magnify tissue damage through uncontrolled cell death and inflammation. Also in septicemia GSDMD interacts with proteins like caspase-11 which can exacerbate inflammatory cytokine release and worsen the disease course.
We have tested this species and application combination and it works. It is covered by our product promise.
We have not tested this specific species and application combination in-house, but expect it will work. It is covered by our product promise.
This species and application combination has not been tested, but we predict it will work based on strong homology. However, this combination is not covered by our product promise.
We do not recommend this combination. It is not covered by our product promise.
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The lysates were kindly provided by our collaborator Dr Feng Shao's lab, NIBS.
The molecular weight observed is consistent with literature (PMID: 26375003). C-terminal fragment is secreted and soluble (PMID: 27339137).
Blocking/Dilution buffer: 5% NFDM/TBST.
This data was developed using the same antibody clone in a different buffer formulation containing PBS, BSA, glycerol, and sodium azide (Anti-cleaved C-terminal GSDMD antibody [EPR20859-147] ab255603).
All lanes: Western blot - Anti-cleaved C-terminal GSDMD antibody [EPR20859-147] (Anti-cleaved C-terminal GSDMD antibody [EPR20859-147] ab255603) at 1/1000 dilution
Lane 1: iBMM (mouse immortalized bone marrow derived macrophages) treated with 500ng/ml Bsak plus 500ng/ml anthrax protective antigen (PA) for 2h. Cell lysate at 10 µg
Lane 2: iBMM (mouse immortalized bone marrow derived macrophages) treated with 500ng/ml Bsak plus 500ng/ml anthrax protective antigen (PA) for 2h. Concentrated cell supernatant at 10 µg
All lanes: Western blot - Goat Anti-Rabbit IgG H&L (HRP) (Goat Anti-Rabbit IgG H&L (HRP) ab97051) at 1/100000 dilution
Predicted band size: 53 kDa
Observed band size: 22 kDa
Exposure time: 3min
The lysates were kindly provided by our collaborator Dr Feng Shao's lab, NIBS.
The molecular weight observed is consistent with literature (PMID: 26375003). C-terminal fragment is secreted and soluble (PMID: 27339137).
Blocking/Dilution buffer: 5% NFDM/TBST.
This data was developed using the same antibody clone in a different buffer formulation containing PBS, BSA, glycerol, and sodium azide (Anti-cleaved C-terminal GSDMD antibody [EPR20859-147] ab255603).
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