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HRK Supply Nifuroxazide raw Materials powder
Product Overview:
Nifurphenol hydrazide is mainly used to prevent and treat bacillary dysentery and enteritis. Prevention and treatment of intestinal or urinary diseases caused by E. coli, Salmonella, Pasteurella (including Riederia), aerogenes, Proteus, necrobacterium and staphylococcus. It can effectively prevent dysentery, has wide antibacterial spectrum, high antibacterial activity and low antibacterial concentration. No cross-resistance with sulfonamides, quinolones and other antibiotics.
HRK Supply Nifuroxazide raw Materials powder Attributes
CAS:965-52-6
MF:C12H9N3O5
MW:275.22
EINECS:213-522-0
Specification: 99% min Nifuroxazide Powder
Sample:Nifuroxazide Powder
Packaging:1kg/bag, 25kg/drum
Brand: Henrikang
Appearance:yellow
Storage: Cool Dry Place
Shelf Life: 2 Years
Test Method: HPLC
HRK Supply Nifuroxazide raw Materials powder Details
Nifuroxazide Powder Usage and Synthesis.
1. Lower blood pressure
Nifurfenzide has a antihypertensive effect by dilating vascular smooth muscle cells and reducing peripheral resistance.
2. Lower blood sugar
The drug is able to improve insulin sensitivity, improve glucose metabolism, and lower blood sugar levels.
3. Anti-angina
Nifurfenzide can increase coronary blood flow, improve myocardial blood supply insufficiency, and relieve angina pectoris symptoms.
4. Anti-arrhythmia
The drug has the effect of regulating the conduction of electrical signals in the heart, which can prevent or correct abnormal heart rhythm.
5. Anti-myocardial ischemia
Nifurphenol hydrazide can inhibit myocardial contractility, reduce myocardial oxygen consumption and improve myocardial ischemia.
Uses of Nifuroxazide.
Prevention and treatment of intestinal or urinary diseases caused by E. coli, Salmonella, Pasteurella (including Riederia), aerogenes, Proteus, necrobacterium and staphylococcus. It can effectively prevent dysentery and promote animal feeding.
In vitro study of Nifuroxazide.
Nifuroxazide is a nitrofuran compound inhibitor that inhibits STAT transcription factor signal transduction. Nifuroxazide inhibits STAT3 constitutive phosphorylation by reducing Jak kinase self-phosphorylation, thereby reducing myeloma cell viability without affecting normal peripheral blood mononuclear cells. Nifuroxazide decreased tyrosine phosphorylation of Jak and TYK2, but had no effect on EGF receptor tyrosine kinase or Src kinase, indicating the relative specificity of Nifuroxazide for Jak2 and TYK2. Nifuroxazide did not inhibit Akt or MAPK phosphorylation. Nifuroxazide inhibits the constitutive phosphorylation of STAT3 in MM cells by reducing the self-phosphorylation of Jak kinase, and leads to downregulation of the STAT3 target gene Mcl-1. Nifuroxazide caused a decrease in survival activity of primary myeloma cells and myeloma cell lines containing STAT3 activation, but did not affect normal peripheral blood mononuclear cells. While bone marrow stromal cells provide signals for myeloma cells to survive, nifuroxazide blocks this survival advantage. nifuroxazide showed stronger cytotoxicity when bound to the histone deacetylase inhibitor peptide or the MEK inhibitor UO126 compared to the interaction of STAT3 with other cellular pathways.
Product method of Bulk Nifuroxazide Powder.