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Details of Grant 

EPSRC Reference: EP/K504154/1
Title: Manufacture of chiral amines using catalytic and flow processing methods
Principal Investigator: Blacker, Professor AJ
Other Investigators:
McGowan, Professor P
Researcher Co-Investigators:
Project Partners:
Department: Sch of Chemistry
Organisation: University of Leeds
Scheme: Technology Programme
Starts: 01 February 2013 Ends: 31 January 2015 Value (£): 180,950
EPSRC Research Topic Classifications:
Catalysis & Applied Catalysis Reactor Engineering
EPSRC Industrial Sector Classifications:
Chemicals
Related Grants:
EP/K504166/1
Panel History:  
Summary on Grant Application Form
Chiral amines are important building blocks used in 40% of pharmaceutical products and 20% crop protection compounds

and are high value chemical intermediates. However, current methods of manufacture are inefficient, wasteful, and often

unsuitable for complex structures. In particular, a lack of good methods to make secondary and heterocyclic chiral amines

was identified by the collaborating end users. The usual processes employ enantiomer resolution (50% max yield), which

adds processing steps and costs. In fact, the ASC pharmaceutical roundtable has listed this class of reactions as one of the

most important to solve, and continuous processing as the No 1 target in the key green engineeing reseacrh areas. The

chiral amine processes have all been studied and published by Blacker and Xiao using batch processing but not in flow.

Separation of the catalyst and its cost within the processes have prevented industry adoption. These issues will be

overcome in the current project using the Cp-star catalysts in flow.

The Leeds team is responsible for the testing, process development and scale-up/out of up to 5 different processes to

make homochiral secondary or tertiary heterocyclic amines (WP2). The studies require solid supported catalysts (Cp-Star)

and ligands generated at Liverpool (WP1) and YPT (WP3) and Leeds will test these in flow process equipment already in

the iPRD process lab, or slurry reactors developed and transferred to Leeds by AMT (WP4). The starting materials and

analytical methods will be supplied by the collaborating end-user companies (AZ, Pfizer, Syngenta and Dr Reddys)(WP5)

and the process data Leeds generates on product quality, cost, productivity will be used to compare with existing poor

methods for chiral amine manufacture. The processes to make homochiral amines are: (a) asymmetric reductive amination

(catalyst being developed at Liverpool, Leeds can undertake scale-up if required); (b) asymmetric transfer hydrogenation;

(c) amine DKR by immobilised enzyme resolution, continuous product separation and Cp-star catalysed racemisationrecycle

(d) crystallisation induced asymmetric transformation involving chiral amine crystallisation and catalysed

racemisation of the mother liquors (e) redox-neutral amine alkylation using hydrogen borrowing enantioselectively alkylate

amines. The chiral amines required by industry are heterocyclic secondary and tertiary amines such as piperidine,

piperazine, pyrrolidies, indolines etc. Within the project the companies will supply real examples of each class of chiral

amine to illustrate the potential for this technology. The use of flow methodology facilitates screening of multiple

compounds.

The flow reactors that will be used are fixed and trickle bed, cascade CSTR and the novel slurry reactors that are being

designed by AMT and transferred to Leeds for evaluation in these systems. The reactors are all meso-scale which is

required to generate data suitable for scale-up to manufacture. The measurable outputs of the work are entantioselectivity,

conversion, yield, kinetics and reation rate, mass balance (ie green metrics eg process efficiency and waste), productivity,

manufacturing process cost prediction (raw material, operational and capital). This data will be compared with existing

processes to the same products to enable cost benefit analysis thereby achieve the main objective of this part of the

project.
Key Findings
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Potential use in non-academic contexts
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Impacts
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Summary
Date Materialised
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Project URL:  
Further Information:  
Organisation Website: http://www.leeds.ac.uk