4948-43-0

Basic information

• Product Name: spirostan-3-yl acetate
• CAS NO: 4948-43-0
• Molecular Formula: C₂₉H₄₆O₄
• Molecular Weight: 458.6731
• Mol File: 4948-43-0.mol

Chemical Properties

• Boiling Point: 527.5°C at 760 mmHg
• Flash Point: 221.8°C
• Density: 1.11g/cm³
• Vapor Pressure: 3.23E-11mmHg at 25°C
• Refractive Index: 1.539
• CAS DataBase Reference: spirostan-3-yl acetate(CAS DataBase Reference)
• NIST Chemistry Reference: spirostan-3-yl acetate(4948-43-0)
• EPA Substance Registry System: spirostan-3-yl acetate(4948-43-0)

Safety Data

• Hazardous Substances Data: 4948-43-0(Hazardous Substances Data)

Upstream product

• 838087-02-8 (25S)-5β-furost-20(22)-ene-3β,26-diyl diacetate 
• 108-24-7 acetic anhydride 
• 39636-34-5 Acetic acid (4aS,4bS,6aS,7S,8R,10aS,10bR,12aS)-8-(4-hydroxy-3-methyl-butyl)-4a,6a,7-trimethyl-octadecahydro-9-oxa-pentaleno[2,1-a]phenanthren-2-yl ester 
• 39636-34-5 dihydrotigogenin 3-acetate 
• 88908-42-3 C₂₉H₄₇IO₄ 
• 88908-42-3 C₂₉H₄₇IO₄ 
• 77-60-1 tigogenin 
• 74808-10-9 2,3,4,6-tetra-O-acetyl-d-glucopyranosyl trichloroacetimidate 
• 92052-38-5 4-O-(2',3',4',6'-tetra-O-acetyl-β-D-glucopyranosyl)-2,3,6-tri-O-acetyl-α-D-glucopyranosyl trichloracetimidate 
• 75-36-5 acetyl chloride 
• 126-19-2 sarsasapogenin 
• 512-07-2 (25R)-5β-spirostan-3-one 
• 77-60-1 3-epismilagenin 
• 116949-76-9 (25R)-3β-acetoxy-5α,14β-spirost-8-en-11-one 

Downstream Products

• 77-60-1 Neotigogenin 
• 66934-60-9 tomatidine acetate 
• 77-59-8 tomatidine 
• 66934-60-9 (22R,25R)-3β-acetoxy-(5α)-spirosolane 
• 469-00-1 sarsasapogeninoic acid 
• 16787-53-4 (25S)-3β-hydroxy-5β-spirostan-23-one 
• 914477-77-3 (23R,25S)-3β-acetoxy-16β,23:23,26-diepoxy-5β-cholestan-22-one 
• 1236306-02-7 (23R,25S)-23-phenylseleno-5β-spirostan-3β-ol acetate 
• 35319-92-7 (25S)-3β-acetoxy-5β-spirostan-23-one 
• 1380412-89-4 [23(23')E, 25S]-23(23')-benzylidene-5β-spirostan-3β-ol acetate 
• 359416-36-7 3β-acetoxy-16β-hydroxy-5β-bisnorcholanoic acid 22->16 lactone 
• 511-92-2 (25S)-5β-Spirostan 
• 126-19-2 sarsasapogenin 
• 289042-56-4 3-O-p-bromobenzoylsarsasapogenin 

Relevant articles and documents

Concise large-scale synthesis of tomatidine, a potent antibiotic natural product

Tomatidine has recently generated a lot of interest amongst the pharmacology, medicine, and biology fields of study, especially for its newfound activity as an antibiotic agent capable of targeting multiple strains of bacteria. In the light of its low natural abundance and high cost, an efficient and scalable multi-gram synthesis of tomatidine has been developed. This synthesis uses a Suzuki–Miyaura-type coupling reaction as a key step to graft an enantiopure F-ring side chain to the steroidal scaffold of the natural product, which was accessible from low-cost and commercially available diosgenin. A Lewis acid-mediated spiroketal opening followed by an azide substitution and reduction sequence is employed to generate the spiroaminoketal motif of the natural product. Overall, this synthesis produced 5.2 g in a single pass in 15 total steps and 15.2% yield using a methodology that is atom economical, scalable, and requires no flash chromatography purifications.

Sarsasapogenin-structure-modified derivatives, pharmaceutical compositions thereof and applications of the compositions

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Epimerization of C-22 in (25R)- and (25S)-sapogenins

Most of the naturally occurring steroidal sapogenins (C-23 non-substituted frameworks), possess an R configuration at the spiro C-22 center. Their C-22 epimers have become important targets in biological research. This paper describes a procedure to obtain 22S-spirostans from 22R-sapogenins and pseudosapogenin skeletons, without affecting the chirality at either C-25 or C-20. An optimal way to synthesize the pair of C-22 stereoisomers of 23-acetyldiosgenin is also reported. The latter was obtained from a 22,26-epoxycholestane or from 23-acetylfurostene compounds.

Epimerization of C-22 in (25R)- and (25S)-sapogenins

Most of the naturally occurring steroidal sapogenins (C-23 non-substituted frameworks), possess an R configuration at the spiro C-22 center. Their C-22 epimers have become important targets in biological research. This paper describes a procedure to obtain 22S-spirostans from 22R-sapogenins and pseudosapogenin skeletons, without affecting the chirality at either C-25 or C-20. An optimal way to synthesize the pair of C-22 stereoisomers of 23-acetyldiosgenin is also reported. The latter was obtained from a 22,26-epoxycholestane or from 23-acetylfurostene compounds.

The crystal structure of 3-epismilagenin acetate and 23-oxo-3-epismilagenin acetate

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