Progen Matériel de laboratoire
SMAD4 / DPC4 (RBT-SMAD4), RMab

SMAD4 / DPC4 (RBT-SMAD4), RMab

For In Vitro Diagnostic Use

Clone RBT-SMAD4 IgG Rabbit Monoclonal

Description

SMAD4 antibody, also known as DPC4 or SMAD family member n°4, detects the protein involved in cell signaling in mammals. SMAD4 forms with SMAD3 a complex which can bind to DNA and modify the expression of several genes related to cellular activities such as proliferation or differentiation. SMAD4 serves as a mediator between extracellular growth factors from the TGFβ family and genes inside the cell nucleus. The abbreviation coin co-SMAD stands for common mediator. SMAD4 is also defined as a signal transducer. SMAD4, is often found mutated in many cancers. The mutation can be inherited or acquired during an individual’s lifetime. If inherited, the mutation affects both somatic and sexual cells. If the SMAD4 mutation is acquired, it will only exist in certain somatic cells. Indeed, SMAD4 is not synthesized by all cells. The protein is present in skin, pancreatic, colon, uterus and epithelial cells. It is also produced by fibroblasts. The functional SMAD4 participates in the regulation of the TGF-β signal transduction pathway, which negatively regulates growth of epithelial cells and the extracellular matrix (ECM). When the structure of SMAD4 is altered, expression of the genes involved in cell growth is no longer regulated and cell proliferation can go on without any inhibition. The important number of cell divisions leads to the forming of tumors and then to multiploid colorectal cancer and pancreatic carcinoma. It is found inactivated in at least 50% of pancreatic cancers. SMAD4 is also found mutated in the autosomal dominant disease juvenile polyposis syndrome (JPS). JPS is characterized by hamartomatous polyps in the gastrointestinal (GI) tract. These polyps are usually benign, however they are at greater risk of developing gastrointestinal cancers, in particular colon cancer. Approximately 55% of pancreatic cancers bear deletions or mutations in SMAD4 antibody expression. Patients undergoing surgical resection of their pancreatic adenocarcinoma, survival of patients whose tumors expressed SMAD4 protein was significantly longer (unadjusted median survival, 19.2 months) as compared with 14.7 months without SMAD4 protein expression (P = 0.03). This SMAD4 survival benefit persisted after adjustment for prognostic factors including tumor size, margin status, lymph node status, pathological stage, blood loss, and use of adjuvant chemoradiotherapy.

Synonymes

SMAD4, anti-Smad4, anti Smad4, deleted in pancreatic carcinoma locus 4, deletion target in pancreatic carcinoma 4, DPC4, hSMAD4, JIP, MADH4, mothers against decapentaplegic homolog 4, mothers against decapentaplegic Drosophila homolog of 4, Mothers against DPP homolog 4, SMAD 4, SMAD family member 4, SMAD mothers against DPP homolog 4, MAD homolog 4, MYHRS

Caractéristiques

Type
Rabbit Monoclonal
Clone
RBT-SMAD4
Isotype
IgG
Réactivité
Paraffin, Frozen
Localisation
Nuclear, Cytoplasmic
Contrôle
Pancreas, Testis, Breast, Bone Marrow, Colon
Usage prévu
For In Vitro Diagnostic Use

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