Scalable Asymmetric Syntheses of Foslevodopa and Foscarbidopa Drug Substances for the Treatment of Parkinson’s Disease

Huters, Alexander D.; Stambuli, James P.; Klix, Russell C.; Matulenko, Mark A.; Chan, V. S.; Simanis, Justin A.; Hill, David R.; Reddy, Rajarathnam E.; Towne, Timothy B.; Bellettini, John R.; Kotecki, Brian J.; Cardinal-David, Benoit; Ji, Jianguo; Voight, Eric A.; Shou, Minshan; Selvakumar, Balaraman; Ashok, Abhishek; Ghosh, Soma

doi:10.1021/acs.joc.1c00905

Cited by 7 publications

(13 citation statements)

References 40 publications

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“…In a recent variation of the aminocatalytic α-hydrazination of α-branched aldehydes pioneered by Brässe and Barbas, independently, an industrial group at AbbVie Inc. (North Chicago, IL, USA) has reported the α-hydrazination of aldehyde 16 as a key step in the total synthesis of foscarbidopa, a phosphate prodrug of carbidopa for the treatment of Parkinson’s disease ( Scheme 6 ) [ 53 ]. Under optimized conditions using tetrazole-proline catalyst C2 and TFA as additives in acetonitrile, the hydrazine-aldehyde 17 was obtained in 84% yield and 57% ee .…”

Section: Methods Based On Enamine Activationmentioning

confidence: 99%

Catalytic Asymmetric α-Functionalization of α-Branched Aldehydes

et al. 2023

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Aldehydes constitute a main class of organic compounds widely applied in synthesis. As such, catalyst-controlled enantioselective α-functionalization of aldehydes has attracted great interest over the years. In this context, α-branched aldehydes are especially challenging substrates because of reactivity and selectivity issues. Firstly, the transient trisubstituted enamines and enolates resulting upon treatment with an aminocatalyst or a base, respectively, would exhibit attenuated reactivity; secondly, mixtures of E- and Z-configured enamines/enolates may be formed; and third, effective face-discrimination on such trisubstituted sp2 carbon intermediates by the incoming electrophilic reagent is not trivial. Despite these issues, in the last 15 years, several catalytic approaches for the α-functionalization of prostereogenic α-branched aldehydes that proceed in useful yields and diastereo- and enantioselectivity have been uncovered. Developments include both organocatalytic and metal-catalyzed approaches as well as dual catalysis strategies for forging new carbon–carbon and carbon–heteroatom (C-O, N, S, F, Cl, Br, …) bond formation at Cα of the starting aldehyde. In this review, some key early contributions to the field are presented, but focus is on the most recent methods, mainly covering the literature from year 2014 onward.

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Section: Methods Based On Enamine Activationmentioning

confidence: 99%

Catalytic Asymmetric α-Functionalization of α-Branched Aldehydes

et al. 2023

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“…The (±)-aldehyde product (152) was isolated as its bisulfite adduct (±)-153. In the next step, the bisulfite adduct (153) was cleaved in situ with sodium bicarbonate, and the aldehyde intermediate (152) was phosphorylated using tetrabenzyl pyrophosphate (142, TBPP) to provide (±)-aldehyde 154 in 92% yield over the two steps. The (±)-aldehyde 154 was converted preferentially to the (S)-enantiomer of hydrazine intermediate 156 using catalyst (R)-155 with excellent conversion (93%) in 60% ee, which was increased to >99% ee upon crystallization.…”

Section: Foscarbidopa (149)mentioning

confidence: 99%

“…Finally, hydrogenolysis of (S)-acid 157 using Pd/C as catalyst enabled isolation of foscarbidopa (149) in 97% yield and >99% ee. 153 With foslevodopa (139) and foscarbidopa (149) in hand, the viability of this prodrug combination in continuous subcutaneous dosing studies was assessed both in preclinical and Phase I clinical trials. 152 One year stability at high concentration of foslevodopa (139) and foscarbidopa (149) aqueous solution (e.g., 240:12 and 360:18 mg/mL respectively) across a wide pH range (6.5−9.2) showed excellent pharmacokinetic profile (PK) and tolerability were observed in preclinical species.…”

Section: Foscarbidopa (149)mentioning

confidence: 99%

Parkinson’s Disease: Advances in Treatment and the Syntheses of Various Classes of Pharmaceutical Drug Substances

Hill,

Huters,

Towne

et al. 2023

Chem. Rev.

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“…Regioselective larger-scale routes to both FLD and FCD were subsequently developed in collaboration with process chemistry. 34 With FLD/FCD in hand, we assessed their stability, solubility, and effectiveness in continuous SC dosing studies both preclinically and in PhI clinical trials. 30 We were surprised to find excellent stability (<2% change for >1 year) at high concentration (e/g/, 240/12 and 360/18 mg/mL) across a wide pH range (6.5−9.2) with excellent PK and tolerability in preclinical species.…”

mentioning

confidence: 99%

“…This solid form isolation was a key step forward in building confidence to pursue alternative routes to FCD. Regioselective larger-scale routes to both FLD and FCD were subsequently developed in collaboration with process chemistry …”

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confidence: 99%

Fueling the Pipeline via Innovations in Organic Synthesis

Voight

Greszler

Kym

2021

ACS Med. Chem. Lett.

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The paramount importance of synthetic organic chemistry in the pharmaceutical industry arises from the necessity to physically prepare all designed molecules to obtain key data to feed the design–synthesis–data cycle, with the medicinal chemist at the center of this cycle. Synthesis specialists accelerate the cycle of medicinal chemistry innovation by rapidly identifying and executing impactful synthetic methods and strategies to accomplish project goals, addressing the synthetic accessibility bottleneck that often plagues discovery efforts. At AbbVie, Discovery Synthesis Groups (DSGs) such as Centralized Organic Synthesis (COS) have been deployed as embedded members of medicinal chemistry teams, filling the gap between discovery and process chemistry. COS chemists provide synthetic tools, scaffolds, and lead compounds to fuel the pipeline. Examples of project contributions from neuroscience, cystic fibrosis, and virology illustrate the impact of the DSG approach. In the first ten years of innovative science in pursuit of excellence in synthesis, several advanced drug candidates, including ABBV-2222 (galicaftor) for cystic fibrosis and foslevodopa/foscarbidopa for Parkinson’s disease, have emerged with key contributions from COS.

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Scalable Asymmetric Syntheses of Foslevodopa and Foscarbidopa Drug Substances for the Treatment of Parkinson’s Disease

Cited by 7 publications

References 40 publications

Catalytic Asymmetric α-Functionalization of α-Branched Aldehydes

Catalytic Asymmetric α-Functionalization of α-Branched Aldehydes

Parkinson’s Disease: Advances in Treatment and the Syntheses of Various Classes of Pharmaceutical Drug Substances

Fueling the Pipeline via Innovations in Organic Synthesis

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