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Literature DB >> 17217281

Directed reductive amination of beta-hydroxy-ketones: convergent assembly of the ritonavir/lopinavir core.

Dirk Menche¹, Fatih Arikan, Jun Li, Sven Rudolph.

Abstract

An efficient procedure for the directed reductive amination of beta-hydroxy-ketones (3) for the stereoselective preparation of 1,3-syn-amino alcohols (6) is reported. The operationally simple protocol uses Ti(iOPr)4 for coordination of the intermediate imino alcohol (5) and PMHS as the reducing agent. The method was expanded to an asymmetric aldol reductive amination sequence to allow a highly convergent synthesis of the hydroxy-amine core of the HIV-protease inhibitors ritonavir and lopinavir. [reaction: see text].

Entities: Chemical Gene

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Year: 2007 PMID： 17217281 DOI： 10.1021/ol062715y

Source DB: PubMed Journal: Org Lett ISSN： 1523-7052 Impact factor: 6.005

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Cited

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3. N-acyldihydropyridones as synthetic intermediates. A stereoselective synthesis of acyclic amino alcohols containing multiple chiral centers.

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5. Synthesis of cis- and trans-3-aminocyclohexanols by reduction of β-enaminoketones.

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6. Silicon Industry Waste Polymethylhydrosiloxane-Mediated Benzotriazole Ring Cleavage: A Practical and Green Synthesis of Diverse Benzothiazoles.

Authors: Mangal S Yadav; Anoop S Singh; Anand K Agrahari; Nidhi Mishra; Vinod K Tiwari
Journal: ACS Omega Date: 2019-04-11

7. Modular synthesis of the pyrimidine core of the manzacidins by divergent Tsuji-Trost coupling.

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