Render Target: SSR
Render Timestamp: 2024-12-19T21:15:13.675Z
Commit: f2d32940205a64f990b886d724ccee2c9935daff
XML generation date: 2024-12-06 01:01:08.033
Product last modified at: 2024-12-08T20:00:08.936Z
Cell Signaling Technology Logo
View Featured Offers >>
1% for the planet logo
PDP - Template Name: Antibody Sampler Kit
PDP - Template ID: *******4a3ef3a
  1. Products /
  2. Primary Antibodies /
  3. Gasdermin Family Antibody Sampler Kit

Gasdermin Family Antibody Sampler Kit #26776

    Product Information

    Kit Usage Information

    Protocols

    Background

    The gasdermin family, which includes GSDMA, GSDMB, GSDMC, GSDMD, and GSDME, has been shown to play a role in inflammation and cell death. Gasdermin D has been reported to have a critical role as a downstream effector of pyroptosis (1,2). Pyroptosis is a lytic type of cell death triggered by inflammasomes, multiprotein complexes assembled in response to pathogen-associated molecular patterns (PAMPs) or danger-associated molecular patterns (DAMPs) that result in the activation of caspase-1 and subsequent cleavage of pro-inflammatory cytokines IL-1β and IL-18 (3). Gasdermin D was identified by two independent groups as a substrate of inflammatory caspases, caspase-1 and caspase-11/4/5, producing two fragments: GSDMD-N and GSDMD-C. Cleavage results in release of an intramolecular inhibitory interaction between the N- and C-terminal domains, allowing the N-terminal fragment GSDMD-N to initiate pyroptosis through the formation of pores on the plasma membrane (4-7).

    Like other gasdermin family members, Gasdermin E (also called DFNA5) contains an amino-terminal pore forming domain that triggers pyroptosis. Cleavage of Gasdermin E at Asp270 is induced by apoptotic-associated caspase-3, converting apoptotic signals to pyroptosis (8). In addition, cleavage of Gasdermin E can be induced by Granzyme B secreted by NK cells and contributes to tumor suppressive activity (9). Gasdermin E expression is suppressed in several types of cancer, including gastric, colorectal, and breast carcinoma, and may be associated with decreased survival (10-12). In contrast, an increase in Gasdermin E, including the amino-terminal pore-forming fragment, is associated with conditions of excessive inflammation (13-15). Gasdermin A (GSDMA) is preferentially expressed in the epithelium of the skin and gastrointestinal tract and is frequently suppressed in gastric cancer (16-18). Gasdermin B (GSDMB) has been reported to be upregulated in several tumor types, and in breast cancer has been associated with metastasis and poor prognosis (19,20). In addition, Gasdermin B has been associated with immune disorders, including asthma (21,22). Gasdermin B can be cleaved by Granzyme A secreted from cytotoxic lymphocytes leading to pyroptotic cell death (23).
    1. Kayagaki, N. et al. (2015) Nature 526, 666-71.
    2. Shi, J. et al. (2015) Nature 526, 660-5.
    3. Broz, P. and Dixit, V.M. (2016) Nat Rev Immunol 16, 407-20.
    4. Aglietti, R.A. et al. (2016) Proc Natl Acad Sci USA 113, 7858-63.
    5. Ding, J. et al. (2016) Nature 535, 111-6.
    6. Liu, X. et al. (2016) Nature 535, 153-8.
    7. Sborgi, L. et al. (2016) EMBO J 35, 1766-78.
    8. Rogers, C. et al. (2017) Nat Commun 8, 14128.
    9. Zhang, Z. et al. (2020) Nature 579, 415-420.
    10. Kim, M.S. et al. (2008) Oncogene 27, 3624-34.
    11. Kim, M.S. et al. (2008) Biochem Biophys Res Commun 370, 38-43.
    12. Yokomizo, K. et al. (2012) Anticancer Res 32, 1319-22.
    13. Tan, G. et al. (2021) Cell Rep 35, 109265.
    14. Li, Y. et al. (2021) Cell Death Differ 28, 2333-2350.
    15. Shi, H. et al. (2021) Circ Res 129, 383-396.
    16. Tamura, M. et al. (2007) Genomics 89, 618-29.
    17. Saeki, N. et al. (2000) Mamm Genome 11, 718-24.
    18. Saeki, N. et al. (2007) Oncogene 26, 6488-98.
    19. Hergueta-Redondo, M. et al. (2014) PLoS One 9, e90099.
    20. Hergueta-Redondo, M. et al. (2016) Oncotarget 7, 56295-56308.
    21. Yu, J. et al. (2011) Pediatr Pulmonol 46, 701-8.
    22. Das, S. et al. (2016) Proc Natl Acad Sci USA 113, 13132-13137.
    23. Zhou, Z. et al. (2020) Science 368, eaaz7548. doi: 10.1126/science.aaz7548.

    Database Links

    UniProt ID: P57764 , Q96QA5 , Q8TAX9-1 , O60443


    Entrez-Gene Id: 79792 , 284110 , 55876 , 1687


    限制使用

    除非 CST 的合法授书代表以书面形式书行明确同意,否书以下条款适用于 CST、其关书方或分书商提供的书品。 任何书充本条款或与本条款不同的客书条款和条件,除非书 CST 的合法授书代表以书面形式书独接受, 否书均被拒书,并且无效。

    专品专有“专供研究使用”的专专或专似的专专声明, 且未专得美国食品和专品管理局或其他外国或国内专管机专专专任何用途的批准、准专或专可。客专不得将任何专品用于任何专断或治专目的, 或以任何不符合专专声明的方式使用专品。CST 专售或专可的专品提供专作专最专用专的客专,且专用于研专用途。将专品用于专断、专防或治专目的, 或专专售(专独或作专专成)或其他商专目的而专专专品,均需要 CST 的专独专可。客专:(a) 不得专独或与其他材料专合向任何第三方出售、专可、 出借、捐专或以其他方式专专或提供任何专品,或使用专品制造任何商专专品,(b) 不得复制、修改、逆向工程、反专专、 反专专专品或以其他方式专专专专专品的基专专专或技专,或使用专品开专任何与 CST 的专品或服专专争的专品或服专, (c) 不得更改或专除专品上的任何商专、商品名称、徽专、专利或版专声明或专专,(d) 只能根据 CST 的专品专售条款和任何适用文档使用专品, (e) 专遵守客专与专品一起使用的任何第三方专品或服专的任何专可、服专条款或专似专专

    For Research Use Only. Not For Use In Diagnostic Procedures.
    Cell Signaling Technology is a trademark of Cell Signaling Technology, Inc.
    All other trademarks are the property of their respective owners. Visit our Trademark Information page.