109621-22-9

Basic information

• Product Name: [6-(18)O]β-hydroxyhyoscyamine
• Synonyms: [6-(18)O]β-hydroxyhyoscyamine
• CAS NO: 109621-22-9
• Molecular Weight: 307.375
• Mol File: 109621-22-9.mol
• Article Data: 3

Chemical Properties

• CAS DataBase Reference: [6-(18)O]β-hydroxyhyoscyamine(CAS DataBase Reference)
• NIST Chemistry Reference: [6-(18)O]β-hydroxyhyoscyamine(109621-22-9)
• EPA Substance Registry System: [6-(18)O]β-hydroxyhyoscyamine(109621-22-9)

Safety Data

• Hazardous Substances Data: 109621-22-9(Hazardous Substances Data)

Upstream product

• 101-31-5 Hyoscyamine 
• 6415-90-3 (-)-hyoscyamine hydrobromide 

Relevant articles and documents

Changes in Regioselectivity of H Atom Abstraction during the Hydroxylation and Cyclization Reactions Catalyzed by Hyoscyamine 6β-Hydroxylase

Hyoscyamine 6β-hydroxylase (H6H) is an αKG-dependent nonheme iron oxidase that catalyzes the oxidation of hyoscyamine to scopolamine via two separate reactions: hydroxylation followed by oxidative cyclization. Both of these reactions are expected to involve H atom abstraction from each of two adjacent carbon centers (C6 vs C7) in the substrate. During hydroxylation, there is a roughly 85:1 preference for H atom abstraction from C6 versus C7; however, this inverts to a 1:16 preference during cyclization. Furthermore, 18O incorporation experiments in the presence of deuterated substrate are consistent with the catalytic iron(IV)-oxo complex being able to support the coordination of an additional ligand during hydroxylation. These observations suggest that subtle differences in the substrate binding configuration can have significant consequences for the catalytic cycle of H6H.

Functional characterization of recombinant hyoscyamine 6β-hydroxylase from Atropa belladonna

(-)-Hyoscyamine, the enantiomerically pure form of atropine, and its derivative scopolamine are tropane alkaloids that are extensively used in medicine. Hyoscyamine 6β-hydroxylase (H6H, EC 1.14.11.11), a monomeric α-ketoglutarate dependent dioxygenase, converts (-)-hyoscyamine to its 6,7-epoxy derivative, scopolamine, in two sequential steps. In this study, H6H of Atropa belladonna (AbH6H) was cloned, heterologously expressed in Escherichia coli, purified and characterized. The catalytic efficiency of AbH6H, especially for the second oxidation, was found to be low, and this may be one of the reasons why Atropa belladonna produces less scopolamine than other species in the same family. 6,7-Dehydrohyoscyamine, a potential precursor for the last step of epoxidation, was shown not to be an obligatory intermediate in the biosynthesis of scopolamine using purified AbH6H with an in vitro 18O labeling experiment. Moreover, the nitrogen atom in the tropane ring of (-)-hyoscyamine was found to play an important role in substrate recognition.