Synthesis of enantiopure 3,6,7,8-tetrahydrochromeno[7,8-d]imidazoles via asymmetric ketone hydrogenation in the presence of RuCl2[Xyl-P-Phos][DAIPEN]

Palmer, Andreas Marc; Chiesa, Vittoria; Holst, Hans Christof; Paih, Jacques Le; Zanotti‐Gerosa, Antonio; Nettekoven, Ulrike

doi:10.1016/j.tetasy.2008.08.022

Cited by 10 publications

(14 citation statements)

References 18 publications

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“…The reaction outcome was still susceptible to the exact structure of the substrate; some analogues gave competing reactions. 342,343 Earlier results with ferrocene-based bisphosphines (7) and BINAP (10) systems under hydrogen required protection of the phenolic hydroxy group. 344 Merck has used an asymmetric hydrogen transfer reaction to prepare the phenylethanol derivative 207 (Scheme 74); the asymmetric hydrogenation approach has been discussed (Scheme 68).…”

Section: Catalyst Recyclementioning

confidence: 99%

Asymmetric homogeneous hydrogenations at scale

Ager¹,

2012

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Asymmetric hydrogenations are increasingly being used to introduce stereogenic centres into products used in the life sciences industries. There are a number of potential pitfalls when moving from a laboratory reaction to a manufacturing process, not least of which is safety. Time-to-market pressure leads to short development times, which in the past could be a large barrier for the implementation of catalytic steps; now there are new ways to minimise this problem. The potential problems associated with impurities and other methods that can shut down the hydrogenation reactions are highlighted in this critical review (353 references).

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Section: Catalyst Recyclementioning

confidence: 99%

Asymmetric homogeneous hydrogenations at scale

Ager¹,

2012

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“…In the course of our P-CAB lead optimization program, we identified several compounds belonging to the classes of 7 H -8,9-dihydropyrano[2,3- c ]imidazo[1,2- a ]pyridines 3 (e.g., BYK 311319, 4 ) and 3,6,7,8-tetrahydrochromeno[7,8- d ]imidazoles 7 (e.g., BYK 405879, 8 ) that are potent reversible inhibitors of the gastric proton pump enzyme and possess promising pharmacological properties. , Consequently, we designed an asymmetric synthesis that permitted the ready preparation of multigram quantities of target compounds 3 and 7 (Scheme ). , …”

Section: Introductionmentioning

confidence: 99%

“…In both classes, the same retrosynthetic strategy was applied comprising the asymmetric catalytic hydrogenation of ketones 1 and 5 and subsequent Mitsunobu cyclization of the resulting diols 2 and 6 affording P-CABs 3 and 7 . In collaboration with Johnson Matthey, Catalysis and Chiral Technologies, we developed for the hydrogenation reaction the previously unknown catalyst RuCl 2 [( S )-Xyl-P-Phos][( S )-DAIPEN] 9 (Figure ), which belongs to the class of Noyori catalysts of the general formula RuCl 2 [PP][NN]. − The RuCl 2 [PP][NN]-catalyzed hydrogenation of ketones is typically performed in the presence of catalytic amounts of a base using 2-propanol as a solvent . However, due to the presence of the acidic phenol group, an excess of the base was required for the reduction of ketones 1 and 5 (one equivalent of base to deprotonate the phenol moiety and a small excess to activate the hydrogenation catalyst). , Despite the similarity of ketones 1 and 5 , the efficiency of the hydrogenation reaction varied considerably between the two structural classes.…”

Section: Introductionmentioning

confidence: 99%

“…In collaboration with Johnson Matthey, Catalysis and Chiral Technologies, we developed for the hydrogenation reaction the previously unknown catalyst RuCl 2 [( S )-Xyl-P-Phos][( S )-DAIPEN] 9 (Figure ), which belongs to the class of Noyori catalysts of the general formula RuCl 2 [PP][NN]. − The RuCl 2 [PP][NN]-catalyzed hydrogenation of ketones is typically performed in the presence of catalytic amounts of a base using 2-propanol as a solvent . However, due to the presence of the acidic phenol group, an excess of the base was required for the reduction of ketones 1 and 5 (one equivalent of base to deprotonate the phenol moiety and a small excess to activate the hydrogenation catalyst). , Despite the similarity of ketones 1 and 5 , the efficiency of the hydrogenation reaction varied considerably between the two structural classes. In the imidazo[1,2- a ]pyridine class, the hydrogenation of ketones 1 was feasible at high S/C ratios giving the corresponding chiral alcohols 2 in excellent yields and optical purities (e.g., R′ = R′′ = Me, Ar = Ph: 1.2 equiv of t -BuOK, catalyst 9 , S/C = 1000:1, 2-PrOH, t -BuOH, H 2 O, 80 bar H 2 , 65 °C, 22 h, 93% yield, 98% ee or 1.1 equiv of t -BuOK, catalyst 9 , S/C = 5000:1, 2-PrOH, t -BuOH, H 2 O, 25 bar H 2 , 75 °C, 15 h, 75% yield, 97% ee) .…”

Section: Introductionmentioning

confidence: 99%

“…In the imidazo[1,2- a ]pyridine class, the hydrogenation of ketones 1 was feasible at high S/C ratios giving the corresponding chiral alcohols 2 in excellent yields and optical purities (e.g., R′ = R′′ = Me, Ar = Ph: 1.2 equiv of t -BuOK, catalyst 9 , S/C = 1000:1, 2-PrOH, t -BuOH, H 2 O, 80 bar H 2 , 65 °C, 22 h, 93% yield, 98% ee or 1.1 equiv of t -BuOK, catalyst 9 , S/C = 5000:1, 2-PrOH, t -BuOH, H 2 O, 25 bar H 2 , 75 °C, 15 h, 75% yield, 97% ee) . In contrast, in the benzimidazole class, higher amounts of hydrogenation catalyst were required to ensure a smooth transformation of ketones 5 to diols 6 (e.g., R′ = R′′ = Me, Ar = Ph: 1.5 equiv of t -BuOK, catalyst 9 , S/C = 310:1, 2-PrOH, t -BuOH, H 2 O, 80 bar H 2 , 65 °C, 23 h, 70%, 98% ee) . Moreover, under certain reaction conditions (high S/C ratio, presence of a large excess of a base), a competing reaction was observed .…”

Section: Introductionmentioning

confidence: 99%

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Large-Scale Asymmetric Synthesis of the 3,6,7,8-Tetrahydrochromeno[7,8-d]imidazole BYK 405879: A Promising Candidate for the Treatment of Acid-Related Diseases

Palmer¹,

Webel²,

Scheufler³

et al. 2008

Org. Process Res. Dev.

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A process for the synthesis of the potassium-competitive acid blocker BYK 405879 (8) was established based on the approach used in medicinal chemistry (asymmetric hydrogenation of prochiral ketone 15 and Mitsunobu cyclization of the resulting alcohol 34). Several critical reaction steps were optimized. The synthesis of prochiral ketones was accomplished using ethyl 3-(2-methylphenyl)-3-oxopropanoate instead of 1-[1-(2-methylphenyl)vinyl]pyrrolidine, a reagent that was difficult to prepare and possesses limited shelf life. The catalyst loading of the asymmetric hydrogenation step was reduced significantly from a S/C ratio of 100:1 to a S/C ratio of 2500:1 by benzyl protection of ketone 15. After the Mitsunobu cyclization, the removal of byproduct was easily accomplished through acid-base extraction, and pure BYK 405879 (8) was then obtained by means of crystallization in the presence of succinic acid.

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Asymmetric Hydrogenation ofCOandCNBonds in Stereoselective Synthesis

Andrushko

2013

Stereoselective Synthesis of Drugs and Natural Products

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Asymmetric hydrogenation is the simplest way of creating new chiral centers, and the technology is continuing to be an industrial flagship for chiral synthesis. In particular, stereoselective hydrogenation of ketones and imines are of a great importance as it is providing an efficient access to the optically active alcohols and amines. This chapter is focused on a practical approach to homogeneous hydrogenations of CO and CN bonds to provide a variety of valuable, biologically active compounds and natural products under mild reaction conditions with high enantio‐ and diastereoselectivity and excellent atom economy. Asymmetric hydrogenation is a highly application‐oriented method, and therefore, examples of industrial applications of the relevant technologies are appropriately illustrated throughout the text.

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Synthesis of enantiopure 3,6,7,8-tetrahydrochromeno[7,8-d]imidazoles via asymmetric ketone hydrogenation in the presence of RuCl2[Xyl-P-Phos][DAIPEN]

Cited by 10 publications

References 18 publications

Asymmetric homogeneous hydrogenations at scale

Asymmetric homogeneous hydrogenations at scale

Large-Scale Asymmetric Synthesis of the 3,6,7,8-Tetrahydrochromeno[7,8-d]imidazole BYK 405879: A Promising Candidate for the Treatment of Acid-Related Diseases

Asymmetric Hydrogenation ofCOandCNBonds in Stereoselective Synthesis

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