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Προσθήκη:1002, Χουανμάο Κτίριο, Νο.105, Mengcheng Δρόμος, Hefei Πόλη, 230061, Κίνα
ΑΡΙΘΜΟΣ CAS: 108212-75-5
Μοριακός Τύπος: C55H74IN3O21S4
Μοριακό Βάρος: 1368,35000
EINECS NO: 813-745-9
MDL NO: NA
Περιγραφή προϊόντος:
Όνομα προϊόντος: Calicheamicin CAS NO: 108212-75-5
Συνώνυμα:
καλιχεαμυκίνη γάμμα1(Ι);
Καλιχεαμυκίνη 1Ι;
Καλιχεαμυκίνη Γάμμα1;
Χημικές Φυσικές Ιδιότητες:
Εμφάνιση: Πούδρα
Προσδιορισμός : Μεγαλύτερο ή ίσο με 99,0 τοις εκατό
Density: 1.57±0.1 g/cm3(Predicted)
Άλφα: D26 -124 βαθμοί (c=0,98 τοις εκατό , EtOH)
Pka: 7.13±0.60(Predicted)
The calicheamicins are a class of enediyne antitumor antibiotics derived from the bacterium Micromonospora echinospora, with calicheamicin 1 being the most notable. It was isolated originally in the mid-1980s from the chalky soil, or "calichi pits", located in Kerrville, Texas. The sample was collected by a scientist working for Lederle Labs. It is extremely toxic to all cells and, in 2000, a CD33 antigen-targeted immunoconjugate N-acetyl dimethyl hydrazide calicheamicin was developed and marketed as targeted therapy against the non-solid tumor cancer acute myeloid leukemia (AML). Calicheamicin 1 and the related enediyne esperamicin are the two of the most potent antitumor agents known.
Calicheamicins are a series of enediyne antitumor antibiotics originally isolated from the bacterium Micromonospora echinospora. They exert high cytotoxicity and have been applied in tumor therapies for over a decade-- a CD33 antigen-targeted immuno-conjugate: N-acetyl dimethyl hydrazide calicheamicin, was developed as a targeted therapy for non-solid tumor cancer acute myeloid leukemia (AML). Calicheamicin has several derivatives with different chemical modifications, among which 1 is the most well-characterized. Calicheamicin 1 contains an aglycon consisting of a bicycle tridec-9-ene-2,6-diyne system with a labile methyl trisulfide group and an aryltetrasaccharide chain. Calicheamicins also contain enediyne moieties that are structurally similar to other enediynes, such as esperamicins, neocarzinostatin, and kedarcidin, etc. After reduction by cellular thiols, the calicheamicin enediyne moieties rearrange to produce a 1, 4-benzenoid diradical.
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