Bordetella pertussis toxin Activators
Bordetella pertussis toxin Activators would constitute a class of compounds that interact with and modulate the activity of the pertussis toxin, a protein exotoxin produced by the bacterium Bordetella pertussis. Pertussis toxin is a multi-subunit protein complex that plays a key role in the pathogenesis of whooping cough, a highly contagious respiratory disease. Activators in this context would bind to the pertussis toxin and enhance its enzymatic activity, which is typically involved in disrupting signaling pathways within host cells. Enhancing the activity could involve increasing the toxin's ADP-ribosyltransferase action, which modifies host cell proteins, thus leading to changes in the regulation of intracellular communication.
To explore the potential of such activators, a thorough understanding of the structure and function of the pertussis toxin would be necessary. Detailed structural analyses, possibly through X-ray crystallography or cryo-electron microscopy, would allow for the identification of specific domains or motifs within the toxin that are amenable to binding by small molecules or peptides that could act as activators. Once potential binding sites are identified, chemical libraries might be screened to find molecules that can engage with the toxin in a manner that enhances its natural function. These interactions could be validated using a range of in vitro assays, such as those that measure the enzymatic activity of the toxin in the presence of the potential activator molecules. Binding studies such as fluorescence anisotropy or SPR can provide kinetic data on the interaction between the toxin and the activators.
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| Product Name | CAS # | Catalog # | QUANTITY | Price | Citations | RATING |
|---|---|---|---|---|---|---|
Magnesium sulfate anhydrous | 7487-88-9 | sc-211764 sc-211764A sc-211764B sc-211764C sc-211764D | 500 g 1 kg 2.5 kg 5 kg 10 kg | $46.00 $69.00 $163.00 $245.00 $418.00 | 3 | |
Low magnesium concentrations are known to induce virulence factors in some bacteria; it might influence PT expression. | ||||||
Manganese(II) chloride beads | 7773-01-5 | sc-252989 sc-252989A | 100 g 500 g | $19.00 $31.00 | ||
Manganese ions can affect bacterial regulatory systems, potentially impacting PT expression. | ||||||
Iron(III) chloride | 7705-08-0 | sc-215192 sc-215192A sc-215192B | 10 g 100 g 500 g | $41.00 $46.00 $87.00 | ||
Iron availability is a regulatory signal for many bacterial virulence factors, possibly including PT. | ||||||
Zinc | 7440-66-6 | sc-213177 | 100 g | $48.00 | ||
Zinc can act as a cofactor for regulatory proteins and might modify PT expression under certain conditions. | ||||||
Copper(II) sulfate | 7758-98-7 | sc-211133 sc-211133A sc-211133B | 100 g 500 g 1 kg | $46.00 $122.00 $189.00 | 3 | |
Copper stress can induce protective responses in bacteria, potentially affecting toxin gene regulation. | ||||||
Adenosine 3′,5′-cyclic monophosphate | 60-92-4 | sc-217584 sc-217584A sc-217584B sc-217584C sc-217584D sc-217584E | 100 mg 250 mg 5 g 10 g 25 g 50 g | $116.00 $179.00 $265.00 $369.00 $629.00 $1150.00 | ||
cAMP is a second messenger in bacteria that can modulate the expression of numerous genes, including toxins. | ||||||
Nicotinic Acid | 59-67-6 | sc-205768 sc-205768A | 250 g 500 g | $62.00 $124.00 | 1 | |
Niacin may serve as a precursor for NAD, which is involved in bacterial metabolism and could influence PT expression. | ||||||
D(+)Glucose, Anhydrous | 50-99-7 | sc-211203 sc-211203B sc-211203A | 250 g 5 kg 1 kg | $38.00 $198.00 $65.00 | 5 | |
Carbon catabolite repression in bacteria can affect the expression of virulence factors like PT. | ||||||
Sodium Chloride | 7647-14-5 | sc-203274 sc-203274A sc-203274B sc-203274C | 500 g 2 kg 5 kg 10 kg | $19.00 $30.00 $60.00 $110.00 | 15 | |
High salt concentrations can activate stress responses and potentially alter virulence gene expression. | ||||||
Glycerol | 56-81-5 | sc-29095A sc-29095 | 100 ml 1 L | $56.00 $153.00 | 12 | |
As a carbon source, glycerol may affect PT expression through metabolic regulatory pathways. | ||||||