H6416
Noggin human
recombinant, expressed in HEK 293 cells, HumanKine®, suitable for cell culture
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About This Item
MDL number:
UNSPSC Code:
12352202
biological source
human
recombinant
expressed in HEK 293 cells
Assay
≥95% (SDS-PAGE)
form
lyophilized powder
potency
≤200 ng/mL ED50
quality
endotoxin tested
mol wt
dimer 65 kDa (glycosylated)
packaging
pkg of 1 mg
pkg of 10 μg
pkg of 100 μg
storage condition
avoid repeated freeze/thaw cycles
technique(s)
cell culture | mammalian: suitable
impurities
≤1 EU/mg
UniProt accession no.
storage temp.
−20°C
Gene Information
human ... NOGG(9241)
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General description
A bone morphogenetic protein (BMP) antagonist is coded by noggin. The node, notochord and dorsal somite shows its expression. It possess a cystine-knot domain, having two β-strand finger-like loops.
Application
Noggin human has been used a supplement in 20% complete medium for isolation of crypts, establishment of human enteroid cultures. It has also been used as a growth factor supplement for pancreatic endoderm specification medium.
Biochem/physiol Actions
Noggin is essential for the normal mouse development. Noggin is required for cartilage morphogenesis and joint formation. It is also an inhibitor of bone morphogenic protein (BMPs) signaling, which is necessary for the growth and patterning of neural tube and somites. Studies indicate Noggin may play a critical role in the formation of gradients of BMP activity. Noggin is produced in the mesoderm in developing embryos and has been shown to have a high affinity to BMP binding protein. When Noggin binds to BMPs, inhibition occurs, preventing BMPs from interacting with receptors on the cell surface. Knockout mice lacking expression of Noggin die at birth from multiple defects including bony fusion of the appendicular skeleton. Noggin has a high binding affinity to heparin and heparan sulfate proteoglycans at the cell surface. Heparan sulfate-bound Noggin remains active and capable of binding BMP4 at the plasma membrane. Noggin can also be competitively displaced by heparin when bound to cells that express heparan sulfate proteoglycan.
Noggin is required for cartilage morphogenesis and joint formation. It is also an inhibitor of bone morphogenic protein (BMPs) signaling, which is necessary for the growth and patterning of neural tube and somites. Studies indicate Noggin may play a critical role in the formation of gradients of BMP activity. Noggin is produced in the mesoderm in developing embryos and has been shown to have a high affinity to BMP binding protein. When Noggin binds to BMPs, inhibition occurs, preventing BMPs from interacting with receptors on the cell surface. Studies indicate Noggin plays a critical role in the formation of gradients of BMP activity. Knockout mice lacking expression of Noggin die at birth from multiple defects including bony fusion of the appendicular skeleton.
Noggin has a high binding affinity to heparin and heparan sulfate proteoglycans at the cell surface. Heparan sulfate-bound Noggin remains active and capable of binding BMP4 at the plasma membrane. Noggin can also be competitively displaced by heparin when bound to cells that express heparan sulfate proteoglycan.
Noggin has a high binding affinity to heparin and heparan sulfate proteoglycans at the cell surface. Heparan sulfate-bound Noggin remains active and capable of binding BMP4 at the plasma membrane. Noggin can also be competitively displaced by heparin when bound to cells that express heparan sulfate proteoglycan.
Preparation Note
HumanKine Noggin is expressed in human HEK 293 cells using a scaleable suspension cell culture system. The protein is a highly stable, authentically glycosylated,disulfide linked 65 kDa homodimer. Production in human HEK 293 cells offers authentic glycosylation. Glycosylation contributes to stability in cell growth media and other applications.
Analysis Note
The specific activity was determined by the dose dependent inhibition of rhBMP4 induced alkaline phosphate production by ATDC5 cells.
Legal Information
HumanKine is a registered trademark of Proteintech Group, Inc. and Humanzyme, Inc
Storage Class Code
13 - Non Combustible Solids
WGK
WGK 3
Flash Point(F)
Not applicable
Flash Point(C)
Not applicable
Regulatory Information
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The BMP signaling and in vivo bone formation
Cao X, et al.
Gene, 357(1), 1-1 (2005)
The Bone Morphogenetic Proteins and Their Antagonists
Vitamins and Hormones, 99(9), 63-90 (2015)
E M De Robertis
Mechanisms of development, 126(11-12), 925-941 (2009-09-08)
Embryos and developing organs have the remarkable ability of self-regenerating after experimental manipulations. In the Xenopus blastula half-embryos can regenerate the missing part, producing identical twins. Studies on the molecular nature of Spemann's organizer have revealed that self-regulation results from
In Vitro Differentiation of Pluripotent Stem Cells into Functional beta Islets Under 2D and 3D Culture Conditions and In Vivo Preclinical Validation of 3D Islets
Bose B
Methods in Molecular Biology (2015)
Grzegorz Pietz et al.
PloS one, 12(9), e0185025-e0185025 (2017-09-22)
Celiac disease is a chronic inflammatory disease of the small intestine mucosa due to permanent intolerance to dietary gluten. The aim was to elucidate the role of small intestinal epithelial cells in the immunopathology of celiac disease in particular the
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