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Protease: 225 results found.

legs4life.com Legs4life Spot the early warning signs of a leg ucler- Smith & Nephew
Acticoat* and Acticoat*7 are unique antimicrobial barrier dressings over partial and full thickness wounds.
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soygen.net Soygen Haelan 951
Soygen is soybean protein beverage with metabolic equol for adjuvant cancer treatment. Soygen contains large quantities of single cell proteins. Haelan 951 immun plus fermentation process hydrolyzes many of the soybean proteins into amino acids and compounds that are rich in nitrogen and fermentation metabolites of isoflavones such as genistein, protease inhibitors, saponins, phytosterols, and inositol hexaphosphate compounds in soybeans.
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amura.co.uk Drug Discovery Company, Structure base drug discovery Company, Pre Clinical Development Company in UK
Discovery of Drugs, Pre Clinical Therapeutic Programmes, Intellectual Property, Intellectual Technologies, Bicyclic Molecular Scaffold in UK
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innovatis.com Roche Applied Science: LightCycler, MagNA Pure LC, Lumi-Imager, PCR
Roche Applied Science is your premier partner in PCR, nucleic acid isolation, apoptosis, tissue dissociation, protease inhibition, chemiluminescent and fluorescent detection. We offer leading systems like LightCycler, MagNA Pure LC.
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tendinitis.com Tendinitis/Tendonitis Treatment & Bursitis Symptoms, Types, Treatment and Prevention
Tendinitis/tendonitis treatment and bursitis symptoms, types and treatment.
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viracept.com Viracept | ViiV Healthcare
Find out more about products from ViiV Healthcare, a specialised HIV/AIDS company with the aim of delivering effective and new HIV medicines as well as support communities affected by HIV
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smbiochemicals.com SMBiochemicals-QVD-OPH-Z-VAD-FMK- Z-DEVD-FMK-Caspase inhibitor and substrates
Q-VD-OPH, A new generation broad spectrum Caspase Inhibitor QVDOPH is a non- FMK new generation broad spectrum inhibitor that offers improvement in potency, stability and toxicity over the bench mark caspase inhibitor Z-VAD-FMK. Q-VD-OPH doesn’t cross reacts with cathepsins or calpains and FMK (Fluoromethyl Ketones) does. The improvements derive from significant changes that include replacement of the carbobenzoyloxy blocking group (Z) with a Quinoline derivative (Q), modification of the tripeptide sequence from VAD to VD, and replacement of fluoromethyl ketone (FMK) with the non toxic 2,6-difluorophenoxy methyl (OPH) group. The mechanism of action involves the formation of an irreversible thioether bond between the aspartic acid derivative in the inhibitor and the active site cysteine with displacement of 2,6-difluorphenoxy group. Q-VD-OPH is a small hydrophobic compound . Therefore, DMSO is required for solubilization. Stock solutions as high as 200 mg / ml have been prepared in DMSO. To retain solubility in water at concentrations above 1 mg / ml, 80 % DMSO is suggested. Q-VD-OPH is effective in vitro at concentrations of 10uM to 20uM. For tissue culture studies 10mM or 20mM stock solutions are prepared in DMSO and diluted 1:1000 directly into the tissue culture medium. For studies in vivo Q-VD-OPH has been administered in 80% to 100% DMSO to assure solubility at the doses given. A dose of 20mg/Kg has been used most frequently. Q-VD-OPH has been shown to inhibit recombinant Caspases 2, 3, 8 and 9 with IC50 values ranging from 25 to 400 nM. A preliminary acute toxicity screen was done in which mice were injected IP with 200 mg/kg, 500 mg/kg or 1000 mg /kg in 100 % DMSO. Mice were sacrificed and autopsied 24 hours later. No gross pathologies were seen and no evidence of toxicity was observed in histological sections from major organs. Q-VD-OPH, A new generation broad spectrum Caspase Inhibitor Q-VD-OPH is a non- FMK new generation broad spectrum inhibitor that offers improvement in potency, stability and toxicity over the bench mark caspase inhibitor Z-VAD-FMK. Q-VD-OPH doesn’t cross reacts with cathepsins or calpains and FMK (Fluoromethyl Ketones) does. The improvements derive from significant changes that include replacement of the carbobenzoyloxy blocking group (Z) with a Quinoline derivative (Q), modification of the tripeptide sequence from VAD to VD, and replacement of fluoromethyl ketone (FMK) with the non toxic 2,6-difluorophenoxy methyl (OPH) group. The mechanism of action involves the formation of an irreversible thioether bond between the aspartic acid derivative in the inhibitor and the active site cysteine with displacement of 2,6-difluorphenoxy group. Q-VD-OPH is a small hydrophobic compound . Therefore, DMSO is required for solubilization. Stock solutions as high as 200 mg / ml have been prepared in DMSO. To retain solubility in water at concentrations above 1 mg / ml, 80 % DMSO is suggested. Q-VD-OPH is effective in vitro at concentrations of 10uM to 20uM. For tissue culture studies 10mM or 20mM stock solutions are prepared in DMSO and diluted 1:1000 directly into the tissue culture medium. For studies in vivo Q-VD-OPH has been administered in 80% to 100% DMSO to assure solubility at the doses given. A dose of 20mg/Kg has been used most frequently. Q-VD-OPH has been shown to inhibit recombinant Caspases 2, 3, 8 and 9 with IC50 values ranging from 25 to 400 nM.
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thrivus.com Thrivus.com (Empowering Biomedical Research and Clinical Diagnostics)
Thrivus Company Limted - providing reagents and supplies to empower biomedical research and clinical diagnostics
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enzymesinc.com Enzymes, Inc. Home - Digestive Enzyme Supplements to Improve Health through Nutrition
Digestive enzymes improve health through better nutrition. A basic enzyme regiment contains Amylase, Cellulase, Lipase, Protease, Alpha-galactosidase,Invertase
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pharmaleads.com Pharmaleads, expert in substrate and inhibitor design
Pharmaleads provides leading companies with innovative substrates for proteases (ECE, NEP, botulinum toxins,...), phosphatases and kinases.
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