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Article

Application of Heterogeneous Catalysts in the First Steps of the Oseltamivir Synthesis

Instituto de Síntesis Química y Catálisis Homogénea (ISQCH), Facultad de Ciencias, CSIC—Universidad de Zaragoza, E-50009 Zaragoza, Spain
*
Author to whom correspondence should be addressed.
Catalysts 2017, 7(12), 393; https://doi.org/10.3390/catal7120393
Submission received: 17 November 2017 / Revised: 7 December 2017 / Accepted: 12 December 2017 / Published: 17 December 2017

Abstract

:
The first steps of oseltamivir synthesis from quinic acid involve acetalization and ester formation. These reactions are catalyzed by either acids or bases, which may be accomplished by heterogeneous catalysts. Sulfonic solids are efficient acid catalysts for acetalization and esterification reactions. Supported tetraalkylammonium hydroxide or 1,5,7-triazabicyclo[4.4.0]dec-5-ene are also efficient base catalysts for lactone alcoholysis and in this work, these catalysts have been applied in two alternative synthetic routes that lead to oseltamivir. The classical route consists of an acetalization, followed by a lactonization, and then a lactone alcoholysis. This achieves a 66% isolated yield. The alternative route consists of esterification followed by acetalization and is only efficient when an acetone acetal is used.

Graphical Abstract

1. Introduction

Pharmaceutical molecules are quintessentially specialty chemicals with structural complexity that require multistep synthetic routes [1]. In addition to atom economy, other parameters such as step [2,3] and pot [4] economy have to be considered in assessments of synthetic routes. The option to carry out multistep chemical transformations in one pot would be of great interest for the synthesis of pharmaceuticals [5]. Heterogeneous catalysts are viable options [6] as multifunctional heterogeneous catalysts and furthermore, different solids can be used to support sites that would otherwise be mutually incompatible in one reaction system [7].
Oseltamivir is one of the most important anti-influenza drugs, and has interesting synthetic approaches, with various routes having from four to 25 steps [8]. The highest overall yield and step economy is provided by a route beginning with (−)-shikimic acid [9] (Scheme 1), which is a natural product obtained from the Chinese star anise (Illicium verum). Hence, its availability and price generate a bottleneck for this synthesis, and in fact, the shortage of Tamiflu in 2005 during the avian flu pandemic is attributed to this problem.
Intensive research has been carried out to develop total synthesis of oseltamivir using commercially available starting materials. In some cases, the synthetic route starts from cyclic materials, as in Shibasaki’s [10] and Zutter’s [11] methods, in which one of the key steps is the desymmetrization of a meso intermediate, or Trost’s synthesis [12], using an asymmetric allylic alkylation as key step. In other cases, one of the key steps is the formation of the cyclohexene ring, for example through an asymmetric Diels–Alder reaction, as in Corey’s [13] and Fukuyama’s [14] methods. In all cases, the synthetic pathway involves several (nine to 14) steps. Some synthetic methods from sugars have been described [15,16], and are even more complicated. Very recently, the construction of the oseltamivir ring has been described in a three-component reaction system using highly efficient asymmetric organocatalysis [17].
For the moment, the most scalable route to oseltamivir involves (−)-quinic acid as the starting material (Scheme 1), as it shares a good number of steps with the well-known shikimic acid route. The first step of the oseltamivir syntheses, starting from (−)-quinic acid (1) [18,19], consists of the acetalization of the two cis hydroxyl groups in positions 3 and 4 with acetone, with concomitant lactonization of the carboxylic group and the cis hydroxyl at carbon 5, catalyzed by p-toluenesulfonic acid, leading to the acetal–lactone (2a) (Scheme 2). The lactone ring is then opened by a reaction with EtONa/EtOH, to obtain the acetal–ester (3ab). Notably, there is a pent-3-yl group in the final product that requires a transacetalization step. A weak point of this route is the use of dimethyl acetonide [20], and this could be circumvented if the acetalization were carried out directly with pentan-3-one to get (2b), and subsequently (3bb) as the acetal–ester product (Scheme 2). Alternatively, there could be a viable route via an initial esterification step, leading to the ethyl quinate (4b), with subsequent acetalization (Scheme 2).
In this manuscript, both alternatives starting from (−)-quinic acid (referred to henceforth as “quinic acid”) will be studied using heterogeneous catalysts, as well as the possibility to carry out the transformation in one pot. As the methyl ester has been also described in other synthetic pathways, the series of methyl esters (3aa, 4a) will be also explored.

2. Results and Discussion

2.1. Single Step One: Acetal Formation from Quinic Acid

The first step described in the Gilead [18] and Hoffmann-La Roche [9,19] routes is the acetalization of quinic acid with 2,2-dimethoxypropane in acetone catalyzed by p-toluenesulfonic acid (PTSA) (Scheme 3).
Many sulfonic solids have been described as catalysts for acid-catalyzed procedures [21,22,23], and several of them were chosen (Figure 1) as potentially interesting alternatives for PTSA:
  • Amberlyst IR-15 [24]: macroreticular sulfonated polystyrene–divinylbenzene with 20% cross-linking degree.
  • Deloxan ASP I/9 [25]: alkyl sulfonic polysiloxane.
  • SAC-13 [26]: nafion–silica composite, with perfluoroalkyl sulfonic groups.
  • sulfonated hydrothermal carbon (SHTC): prepared from glucose under mild conditions and sulfonated with sulfuric acid [27] that contains arylsulfonic groups and has shown improved activity in different esterification reactions [28,29].
The results obtained with all the sulfonic catalysts are collected in Table 1.
With 3.5 eq of 2,2-dimethoxypropane (DMP) heated at reflux in acetone, all the solid catalysts, with the exception of Amberlyst IR-15, led to yields of the acetal–lactone 2a higher (86–91%, entries 3, 7 and 9) than that obtained with PTSA (83%, entry 1). The reaction is significantly slower in the absence of DMP (entries 4, 8 and 10), or with DMP at room temperature (entry 11) or in a solvent other than acetone (entry 12).
In the case of pentan-3-one, the dimethyl acetal is not commercially available and the reactions that lead to 2b were carried out in the ketone heated at reflux. Given its higher boiling point, the reaction was faster and yields of over 90% were obtained after only 24 h (entries 13 and 14).

2.2. Single Step Two: Lactone Alcoholysis

The second step is the lactone alcoholysis to give the acetal–ester 3 (Scheme 4). This reaction is in fact a transesterification, which could be catalyzed by acids or bases, and the two types of solid catalysts were tested.
In the two acid-catalyzed reactions with ethanol (Table 2), the lactone ethanolysis was quite efficient, with yields of esters around 74%–77% (entries 1 and 3), but unfortunately, the side transacetalization reaction was also very efficient, and the main product was in both cases the ethyl quinate 4b, with a small amount of lactone 5 [30]. At room temperature (entries 2 and 4), the reaction was very slow.
Three heterogeneous basic catalysts were tested (Figure 2): Amberlite IRA-400 [31] (quaternary ammonium hydroxide) and 1,5,7-triazabicyclo[4.4.0]dec-5-ene (TBD), supported on either polystyrene (TBD-PS [32]) or silica (TBD-SiO2 [33]). Their activities were compared with tetramethylammonium hydroxide and TBD, which are the homogeneous counterparts. Only the lactone 2a and the ethyl ester 3ab were detectable in the reaction mixtures. While heated at reflux in ethanol, the 2a/3ab ratio was around 40:60, which seems to be the equilibrium position under those conditions. At lower temperature, the reaction is not so easily reversible, and 86% yield can be obtained with TBD-PS after only 24 h at 0 °C (entry 10). The homogeneous catalysts (entries 11–14) lead to similar or worse results, showing the positive effect of immobilization on the activity, together with the simple work-up of the reaction mixture when using heterogeneous catalysts. In the case of 3bb, 84% yield can be also obtained with TBD-PS at 0 °C (entry 17). Finally, the methyl ester 3aa can also be obtained from 2a and methanol with very high yield (96%) at 0 °C after 48 h (entry 18).

2.3. One-Pot Acetalization and Lactone Alcoholysis: Single Acid Catalyst

In spite of the transacetalization problems detected with acid catalysts, the direct one-pot synthesis of acetal–esters 3 (Scheme 5) was tried with the sulfonic solids, using 2,2-dimethoxypropane in a 1:1 mixture (v/v) of acetone and the corresponding alcohol (Table 3).
The reaction with ethanol led to five reaction products, two lactones in the form of acetal (2a) and free hydroxyls (5), two ethyl esters with acetal (3ab) and free quinate (4b), as well as the quinic acid acetal (6a). Total conversion of quinic acid was obtained in most cases, but the product distribution was quite different depending on the catalyst. However, the acetal–ester 3ab, the desired product, was not obtained with a significant yield. On the contrary, ethyl quinate 4b was the major product because of the transacetalization of 2a with ethanol in the presence of the acid catalyst.
Methanol is much more reactive than ethanol and consequently, the results are quite different. In fact, the yield of the desired acetal–ester 3aa was significant, around 25% with both Deloxan and SAC-13 (entries 5 and 7), although the yield of free ester 4a was also important in all the cases.
Finally, the reaction of quinic acid in a 1:1 mixture of ethanol and pentan-3-one (Scheme 6) was tried with the same acid catalysts (Table 4). The yields of the compounds with the acetal group (3bb and 6) were very low, showing the lower stability of the pentanone acetal. In view of the problems associated with the use of acid catalysts in the alcoholysis step, the sequential acetalization followed by alcoholysis was tested with two different catalysts.

2.4. One-Pot Sequential Process with One Acid and One Base Catalyst: Acetalization and Lactone Alcoholysis

In the sequential process (Scheme 7), the first acetalization reaction was carried out under the optimal conditions determined in the individual test, and once the reaction mixture was cooled at 0 °C, the basic catalyst TBD-PS and ethanol were added. As can be seen in the results (Table 5), the alcoholysis is less efficient under these new conditions. A significant amount of acetal–lactone 2a (53% with Deloxan, entry 1, and 38% with SHTC, entry 2) remained unreacted even after 48 h, and the conversion of 2b was even lower under the same conditions (entries 5 and 8), giving 13% of acetal–ester 3bb as the best result (entry 8). The filtration of the acid catalyst before addition of the basic catalyst and ethanol (entry 3) did not improve the results, demonstrating that the presence of the acid catalyst was not the reason for this lower efficiency. The combination of a ketone and a base catalyst may produce an aldol condensation as side reaction, as already detected in previous work [7].
Furthermore, about one-half of the converted 2a was transformed to a previously undetected new product, which was identified as the compound 7 (entries 1–3), which must arise from the simultaneous presence of acetone/DMP and a basic catalyst. In fact, when the acetone/DMP mixture was evaporated prior to the addition of ethanol and TBD-PS (entry 4), the conversion of acetal–lactone 2a was significantly improved and the compound 7 was not obtained. The simultaneous presence of the acid catalyst and ethanol did produce a partial transacetalization to the ethyl quinate 4b. The partial transacetalization was also observed when pentan-3-one was evaporated before the addition of TBD-PS and ethanol (entry 6). In view of the incompatibility of reagents and catalysts of the two reaction steps, the acid catalyst was filtered and pentan-3-one was evaporated before the addition of ethanol and TBD-PS to the crude mixture (entries 7 and 9). As expected, the reaction selectively formed the acetal–ester 3bb, with up to a 76% yield after 96 h (entry 9), showing that pure acetal–lactone 2b behaves much better than the crude one for the base-catalyzed lactone alcoholysis.

2.5. Single Step Three: Esterification of Quinic Acid

In view of the problems encountered in the sequential process of acetalization followed by alcoholysis, another strategy was conceived by changing the sequence order. This new sequence consists of an initial esterification of quinic acid to the corresponding quinate 4 (Scheme 8) and then the acetalization of this ester. Again, the main advantage would be the possibility of using a single acid catalyst and thus, the individual esterification step was studied (Table 6).
Both ethyl quinate 4b and lactone 5 were obtained in ethanol (entries 1–4), but the lactone underwent a slow acid-catalyzed alcoholysis, leading to more than a 90% yield of ethyl quinate 4 with SHTC (entry 4). The higher reactivity of methanol led to a faster alcoholysis reaction and, in general, higher methyl ester (4a) yields were obtained in shorter reaction times (entries 5–6).

2.6. Sequential Process with One or Two Acid Catalysts: Esterification and Acetalization

The sequence of esterification with ethanol followed by acetalization was then tried with both acetone and pentan-3-one (Scheme 9). In the first case, DMP was used to efficiently promote the acetalization reaction. Two efficient catalysts for the direct esterification of quinic acid with ethanol—Deloxan and SHTC—were chosen to act as the single catalyst for both reactions or to be combined as catalysts for the first and second reactions. The results are gathered in Table 7.
The combination of Deloxan for the esterification with ethanol, and SHTC for acetalization with acetone and DMP, was tested (entry 1). A long reaction time was used in the first reaction to reach the highest conversion of quinic acid, whereas room temperature and moderate time was used for the second reaction. The acetalization of ethyl quinate 4b was slower than acetalization of quinic acid. In fact, after 24 h, 13% of 4b remained unconverted. Moreover, the acetal–lactone 2a was also obtained (up to 24% yield), indicating that lactonization can also be produced from the ester. Longer reaction times did not change the result. In the absence of DMP, the acetalization was slower (entry 2), but the lactonization occurred in a similar ratio. The use of SHTC as the only catalyst for both reactions improves both conversion and selectivity to 3ab (74% yield, entry 4), but the best result was obtained with Deloxan as the only catalyst (entry 3), with almost complete conversion of 4b and 83% yield of the acetal–ester 3ab.
When acetalization was carried out at higher temperature (acetone reflux), conversion was higher but selectivity was much lower due to an extensive lactonization (entries 5 and 6). On the contrary, a decrease in reaction temperature to 0 °C (entries 7 and 8) improves the selectivity with respect to the desired acetal–ester when SHTC is the acetalization catalyst, but 83% was the maximum yield (entry 7) obtained in any case.
Finally, the formation of the most interesting acetal–ester 3bb was tried by the same methodology. The ethyl quinate 4b was not soluble in pure pentan-3-one and a small amount of ethanol was added in the second step to allow solubilization of the substrate. At room temperature (entries 9–12), the lack of ketal in the medium and the lower reactivity of the ketone made the reaction less efficient than in the case of acetone, and the yields of 3bb were low in all cases. Moreover, lactones 2b and 5 were also formed. At higher reaction temperatures (entries 13–15), the conversions were improved, but the lactonization side reaction occurred to a more significant level.

2.7. Process at Gram Scale

After the exploration of all the possibilities, the optimal procedure to get the acetal–ester of interest 3bb was to use a sequential two-step process using an acid catalyst for the acetalization with pentan-3-one, with concomitant lactonization, followed by a base-catalyzed ethanolysis of the lactone in the way described in Table 5. The chosen scale was 10 mmol of quinic acid (1.92 g) and the first reaction was carried out in pentan-3-one heated at reflux for 24 h, with Deloxan as the catalyst. After the catalyst filtration and evaporation of the ketone, the crude product was dissolved in ethanol, cooled to 0 °C and made to react using TBD-PS as the catalyst. This reaction was monitored by 1H NMR, was observed during the course of seven days, and led to a 73% yield for 3bb. Catalyst filtration and purification by column chromatography led to 1.89 g of pure 3bb (66% isolated yield), and thus illustrates the potential of this methodology for preparative purposes.
Although the recovery of the catalysts was not the primary objective of the work, the gram-scale synthesis permits one to test this aspect. Moreover, the use of the sequential method allows one to recover and reuse each catalyst separately, with the possibility of optimizing the number of runs for each one [34,35]. In this case, both catalysts were recovered and reused under the same conditions without any further pre-treatment. The analysis of the final reaction mixture showed a yield of 57%, slightly lower than in the first reaction, indicating a certain degree of deactivation. Further work would be necessary to identify the origin of this deactivation in order to optimize the recovery and reuse of this catalytic system.

3. Materials and Methods

See the Supplementary Materials for a full description of the catalysts and the general reaction methods.

3.1. Acetalization of Quinic Acid (1)

A mixture of quinic acid (192 mg, 1 mmol) and the acid catalyst (0.01 mmol) in acetone (4 mL) was heated at reflux for the required time. In some reactions, 2,2-dimethoxypropane (430 µL, 364 mg, 3.5 mmol) was also added to the mixture. After cooling to room temperature the catalyst was filtered off and the acetone was evaporated under reduced pressure. The yield of acetal–lactone 2a was determined by 1H NMR [36,37] using mesitylene as an internal standard. The acetalization with pentan-3-one was carried out under the same conditions to obtain acetal–lactone 2b [38].

3.2. Alcoholysis of Acetal–Lactones (2)

A mixture of the acetal–lactone (2a or 2b, 1 mmol) and the catalyst (0.01 mmol of acid catalyst or 0.1 mmol of basic catalyst) in alcohol (methanol or ethanol, 4 mL) was stirred at the required temperature for the required time. After allowing the reaction to reach room temperature the catalyst was filtered off and the solvent was evaporated under reduced pressure. Yields of the different products were determined by 1H NMR, using mesitylene as an internal standard.

3.3. One-Pot Acetalization and Lactone Alcoholysis with a Single Acid Catalyst

A mixture of quinic acid (192 mg, 1 mmol), 2,2-dimethoxypropane (430 µL, 364 mg, 3.5 mmol) and the acid catalyst (0.01 mmol) in an acetone/alcohol 1:1 (v/v) mixture (4 mL) was heated at reflux for 24 h. After cooling to room temperature, the catalyst was filtered off and the acetone was evaporated under reduced pressure. Yields of the different products obtained (2, 3, 4 and 5) were determined by 1H NMR, using mesitylene as an internal standard. The reaction with pentan-3-one was carried out in the same way, without 2,2-dimethoxypropane.

3.4. One-Pot Acetalization and Lactone Alcoholysis with One Acid and One Basic Catalyst

A mixture of quinic acid (192 mg, 1 mmol), 2,2-dimethoxypropane (430 µL, 364 mg, 3.5 mmol) and the acid catalyst (0.01 mmol) in acetone (4 mL) was heated at reflux for 4 h. Then the reaction mixture was cooled to 0 °C, TBD-PS (0.1 mmol) and ethanol (4 mL) were added and the reaction was stirred at 0 °C for at least 24 h. The catalysts were filtered off and the solvent was evaporated under reduced pressure. Yields of the different products obtained (2a, 3ab, and 6) were determined by 1H NMR using mesitylene as an internal standard. In the case of pentan-3-one, the first reaction was carried out without 2,2-dimethoxypropane and it was heated for either 24 or 48 h. The second reaction was carried out in the same way as for acetone.

3.5. Esterification of Quinic Acid

A mixture of quinic acid (192 mg, 1 mmol) and the acid catalyst (0.01 mmol) in alcohol (4 mL) was heated at reflux for the required time. After cooling at room temperature, the catalyst was filtered off and the solvent was evaporated under reduced pressure. Yields of ester 4 [39,40,41] and lactone 5 [30] were determined by 1H NMR using mesitylene as an internal standard.

3.6. Sequential Esterification and Acetalization with Two Acid Catalysts

A mixture of quinic acid (192 mg, 1 mmol) and the acid catalyst (0.01 mmol) in ethanol (4 mL) was heated at reflux for the required time. The catalyst was filtered off and the solvent was eliminated under reduced pressure. The ketone (4 mL) (in the case of the acetalization with pentan-3-one, 3 mL of pentan-3-one and 1 mL of EtOH) and the second acid catalyst (0.01 mmol) were added and the reaction was heated at the required temperature. 2,2-Dimethoxypropane (430 µL, 364 mg, 3.5 mmol) was also added when acetone was used in the acetalization step. The catalyst was filtered off and the ketone was evaporated under reduced pressure. Yields of all the products were determined by 1H NMR using mesitylene as an internal standard.

4. Conclusions

The acetal–esters derived from quinic acid (3aa, 3ab and 3bb) can be prepared using heterogeneous catalysis through two different synthetic routes. The desired pentanone acetal ethyl ester 3bb has been prepared on a gram scale with an isolated yield of 66% by a sequential procedure consisting of two reaction steps: the sulfonic acid-catalyzed acetalization and the base-catalyzed alcoholysis of the acetal lactone 2b. The second synthetic route involves an acid-catalyzed esterification of quinic acid followed by the acetalization, catalyzed either by the same acid or by a different solid. Although this route is effective for the isopropylidene derivative 3ab, the acetalization with pentan-3-one is much less efficient due to the competitive lactonization under the reaction conditions. These results demonstrate the potential of heterogeneous catalysts for multistep synthesis of pharmaceutical intermediates.

Supplementary Materials

catalyst descriptions, preparation details and full spectroscopic description of compounds 2a, 2b, 3aa, 3ab, 3bb, 4a, 4b, 5, 6 and 7, including improved assignation of 1H- and 13C-NMR signals. It is available online at www.mdpi.com/2073-4344/7/12/393/s1.
Supplementary File 1Supplementary File 2

Acknowledgments

This work was made possible by the financial support of the Spanish Ministerio de Economía y Competitividad (project CTQ2014-52367-R) and the Gobierno de Aragón (E11 Group co-financed by the European Regional Development Funds).

Author Contributions

José M. Fraile conceived and designed the experiments; Carlos J. Saavedra performed the experiments; José M. Fraile and Carlos J. Saavedra analyzed the data; José M. Fraile wrote the paper.

Conflicts of Interest

The authors declare no conflict of interest.

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Scheme 1. General routes to oseltamivir from (−)-shikimic and (−)-quinic acids.
Scheme 1. General routes to oseltamivir from (−)-shikimic and (−)-quinic acids.
Catalysts 07 00393 sch001
Scheme 2. Possible routes from (−)-quinic acid to the acetal–esters (3).
Scheme 2. Possible routes from (−)-quinic acid to the acetal–esters (3).
Catalysts 07 00393 sch002
Scheme 3. Acetalization of (−)-quinic acid.
Scheme 3. Acetalization of (−)-quinic acid.
Catalysts 07 00393 sch003
Figure 1. Sulfonic solids used as acid catalysts.
Figure 1. Sulfonic solids used as acid catalysts.
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Scheme 4. Alcoholysis of acetal–lactones 2.
Scheme 4. Alcoholysis of acetal–lactones 2.
Catalysts 07 00393 sch004
Figure 2. Solids used as base catalysts.
Figure 2. Solids used as base catalysts.
Catalysts 07 00393 g002
Scheme 5. One-step formation of dimethyl acetal and ester from quinic acid using 2,2-dimethoxypropane.
Scheme 5. One-step formation of dimethyl acetal and ester from quinic acid using 2,2-dimethoxypropane.
Catalysts 07 00393 sch005
Scheme 6. One-step formation of diethyl acetal and ethyl ester from quinic acid using pentan-3-one and ethanol.
Scheme 6. One-step formation of diethyl acetal and ethyl ester from quinic acid using pentan-3-one and ethanol.
Catalysts 07 00393 sch006
Scheme 7. One-pot sequential acetalization of quinic acid and lactone alcoholysis.
Scheme 7. One-pot sequential acetalization of quinic acid and lactone alcoholysis.
Catalysts 07 00393 sch007
Scheme 8. Esterification of quinic acid.
Scheme 8. Esterification of quinic acid.
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Scheme 9. Sequential esterification and acetalization of quinic acid.
Scheme 9. Sequential esterification and acetalization of quinic acid.
Catalysts 07 00393 sch009
Table 1. Results of the acetalization of quinic acid. 1
Table 1. Results of the acetalization of quinic acid. 1
EntryKetoneCatalyst 2T (°C)DMP 3Time (h)Yield (%)
1AcetonePTSA56Yes383
2(R = Me)IR-1556Yes348
4873
3 Deloxan56Yes391
4 56No310
5 25Yes6863
6 66Yes 4311
7 SAC-1356Yes386
8 56No315
2440
7264
9 SHTC56Yes390 5
10 56No39
2464
4880
11 25Yes2482
12 66Yes 4361
13Pentan-3-oneDeloxan101No24100
14(R = Et)SHTC101No2491
48100
1 Reaction conditions: quinic acid (1 mmol), catalyst (0.01 mmol), ketone (4 mL); 2 PTSA: p-toluenesulfonic acid; SHTC: sulfonated hydrothermal carbon; 3 DMP: addition of 2,2-dimethoxypropane (3.5 mmol); 4 with tetrahydrofuran (4 mL) as solvent instead of acetone; 5 average yield of two experiments.
Table 2. Results of the alcoholysis of acetal–lactones 2. 1
Table 2. Results of the alcoholysis of acetal–lactones 2. 1
EntryReactionCatalystTTimeYield (%)
(°C)(h)2345
12a + EtOHSAC-1378241317610
2 252487067
3 SHTC7824172729
4 252482099
5 IRA-4007854258--
6 TBD-SiO27844060--
7 2546931--
194555--
8 −20482179--
9 TBD-PS7843664--
10 046040--
241486--
481090 2--
11 Me4NOH78243961--
12 0243070--
483070--
13 TBD78244258--
14 0244258--
484357--
152b + EtOHTBD-SiO27844852--
16 TBD-PS7844456--
17 042971--
241684--
481486 2--
182a + MeOHTBD-PS0243169--
48496 2--
1 Reaction conditions: lactone 2 (1 mmol), alcohol (4 mL) and catalyst (0.01 mmol of acid or 0.1 mmol of base); 2 average yields of two experiments.
Table 3. Results of the one-step formation of dimethyl acetal and ester from quinic acid. 1
Table 3. Results of the one-step formation of dimethyl acetal and ester from quinic acid. 1
EntryAlcoholCatalystYield (%)
2a3456
1EtOHDeloxan 25689720
2 IR-155403268
3 SAC-13383381011
4 SHTC46024123 3
5MeOHDeloxan41252374
6 IR-1535945101
7 SAC-1338262673
8 SHTC39049120
1 Reaction conditions: quinic acid (1 mmol), 2,2-dimethoxypropane (3.5 mmol), catalyst (0.01 mmol) in acetone/alcohol (4 mL, 1:1 v/v), heated at reflux, 24 h; 2 average yields of two experiments; 3 the remaining 15% corresponds to unconverted quinic acid.
Table 4. Results of the one-step formation of diethyl acetal and ethyl ester from quinic acid. 1
Table 4. Results of the one-step formation of diethyl acetal and ethyl ester from quinic acid. 1
CatalystYield (%)
2b3bb4b5
Deloxan2734324
IR-153424717
SAC-1320105317
SHTC670294
1 Reaction conditions: quinic acid (1 mmol), catalyst (0.01 mmol) in pentan-3-one/ethanol (4 mL, 1:1 v/v), heated at reflux, 24 h.
Table 5. Results of the one-pot sequential acetalization of quinic acid and lactone alcoholysis. 1
Table 5. Results of the one-pot sequential acetalization of quinic acid and lactone alcoholysis. 1
EntryKetoneAcid CatalystTime (h)Yield (%)
1st2nd234b7a
1AcetoneDeloxan4245421-19
485326-16
2 SHTC4244128-31 2
483832-30
3 SHTC 34244823-28
1202546-29
4 SHTC 4424196516-
48114940-
5Pentan-3-oneDeloxan2424100---
4885-7 5-
6 Deloxan 42424532324-
7 Deloxan 624244753--
483565--
8 SHTC48248713--
1208713--
9 SHTC 548244654--
482971--
962476--
1 Reaction conditions: quinic acid (1 mmol), acid catalyst (0.01 mmol), ketone (4 mL), at reflux. In the case of the reaction with acetone, 2,2-dimethoxypropane (3.5 mmol) was also added. The second reaction was carried out at 0 °C after addition of TBD-PS (0.1 mmol) and ethanol (4 mL); 2 average yields of two experiments; 3 the acid catalyst is filtered before adding ethanol and TBS-PS; 4 the ketone is evaporated under vacuum before adding ethanol and TBS-PS; 5 lactone 5 was also obtained in 8%; 6 the acid catalyst is filtered and the pentan-3-one is evaporated under vacuum before adding ethanol and TBS-PS.
Table 6. Results of the esterification of quinic acid with ethanol or methanol. 1
Table 6. Results of the esterification of quinic acid with ethanol or methanol. 1
EntryAlcoholCatalystTime (h)Yield (%)
45
1EtOHDeloxan31912
247225 2
488119
688713
2 Deloxan 3248317
3 SAC-13246522
4 SHTC24829
489010
72937
5MeOHDeloxan48946
6 SHTC24937
1 Reaction conditions: quinic acid 1 (1 mmol), ethanol or methanol (4 mL), and catalyst (0.01 mmol) heated at reflux; 2 average yields of two experiments; 3 0.02 mmol of catalyst.
Table 7. Sequential esterification and acetalization of quinic acid with two acid catalysts. 1
Table 7. Sequential esterification and acetalization of quinic acid with two acid catalysts. 1
EntryAcid
catalyst 1
Esterification Time (h)Acid
catalyst 2
KetoneAcetalizationYield (%)
T (°C)Time (h)4b325
1Deloxan70SHTCAcetone25152956150
241363240
2Deloxan70SHTCAcetone 225402757160
3Deloxan 370-Acetone2540383140
4SHTC 396-Acetone25401174150
5Deloxan 370-Acetone5640749440
6SHTC 396-Acetone564009910
7Deloxan70SHTCAcetone070083170
8Deloxan 370-Acetone0401076140
9Deloxan70SHTCPentan-3-one2570642439
10Deloxan 370-Pentan-3-one2578799210
11SHTC48DeloxanPentan-3-one25784139416
12SHTC48SHTCPentan-3-one25784435138
13SHTC48DeloxanPentan-3-one40684714336
14SHTC48SHTCPentan-3-one40206212206
684114387
15SHTC48SHTCPentan-3-one10124208216
1 Reaction conditions: quinic acid (1 mmol), first acid catalyst (0.01 mmol), ethanol (4 mL), reflux. After the indicated time, the catalyst was filtered off, the ethanol was evaporated under reduced pressure and the second catalyst (0.01 mmol), ketone (4 mL) and DMP (3.5 mmol, only in the case of acetone) were added. In the case of pentan-3-one, 3 mL of ketone and 1 mL of ethanol were added in the second step, due to the lack of solubility of 4b in pure pentan-3-one. Temperature and time as indicated in the table; 2 in the absence of DMP; 3 as the two reactions were catalyzed by the same solid, the evaporation of ethanol was the only treatment after the first reaction.

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Fraile, J.M.; Saavedra, C.J. Application of Heterogeneous Catalysts in the First Steps of the Oseltamivir Synthesis. Catalysts 2017, 7, 393. https://doi.org/10.3390/catal7120393

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Fraile JM, Saavedra CJ. Application of Heterogeneous Catalysts in the First Steps of the Oseltamivir Synthesis. Catalysts. 2017; 7(12):393. https://doi.org/10.3390/catal7120393

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Fraile, José M., and Carlos J. Saavedra. 2017. "Application of Heterogeneous Catalysts in the First Steps of the Oseltamivir Synthesis" Catalysts 7, no. 12: 393. https://doi.org/10.3390/catal7120393

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