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A Safe and Efficient Method For Conversion of 1,2- and 1,3Diols to Cyclic Carbonates Utilizing Triphosgene
Robert M. Burk* and Michael B. Roof DepmmmtdCbanisciems.~lac. 2525Dupont Drive, Irvine, Califomia 92715
Absbttctz Rcachn~ Qtrlphasgenela the prasence qfpyrldlne with a war&y Qdials la&aYng hlndmd tdaty andI3-cyclicdials pro&W high yirldr #the corrc~~ cyclic carhmatrcs.
Roper choice of protecting group8 is critical in the synthesis* and derivatixation2 of prostaglandins. Durhtgthecourseofour research it was necessary to protect 1,3dihydmxyprostanoid intermediates with a base
labile protec&g group. An obvious choice was a cyclic bomnate which has pmviously been used in protection of ptostaglandins as 9.1 l-cyclic bomnatesf when selective functionalization of the Shydtoxyl group was desired
However, cyclic boronates am highly susceptible to hydrolysis and therefore can not he conveniently handled in multiple chemical sequences. For this reason we decided upon use of a cyclic carbonate but wem surprised to discover that no general methodology existed for this transformation. Although them are numerous documented pmcedmes for conversion of 1,Zdiols and 1,3-acyclic dials to cyclic carbonates using phosgene, p-niuophenyl chlomfotmate, uichloroacetyl chloride, 1, l-carhonyldiimidazole or carbon monoxide our attempted employment of these pmcedurest with 1,3cyclic diols were either unsuccessful or very low yielding. In this note we wish to describe the use of triphosgene in a highly efficient method for protection of diols, especially 1,3-
395
396
pyrldlne CHpCIL
Recently, Eckert~ mported the use of niphosgene as a safe, stabk phosgene mplaccnmt snd example of its use in various chlcrofonnylation. chlorination. carbonylation and dehydration reactions. Interestingly, to date
the chemical utility of triphosgene6 remains relatively unexploited as it has only btar mported in the pmpamtkn of N-carboxy-a-amino acid anhydrides, synthesis of j&rand Mactams,* and chlorination of benxylic or allylic
alcoho1s.c Similar application of triphosgene to our systems as described in the above reports (R3N, THF or EtOAc or benzene, 23 + SOC) resulted in either no carbonylation or competing chlorination at the hydroxy positions. However, subsequent experimentation at lower temperatures, which eliminated chlorination side in Table 1.
reactions, led to the following general pmcedum for carbonylation of diols as ill-
In a typical small scale experiment a solution of Uiphosgene (0.5 equiv) in CH$Zl3 (1.0 mLJ was added dtopwise to a solution of pyridine (6.0 equiv) and the diol (0.5 mmol) in CH3Cl3 (1.5 mL) cooled to -70 C. Once addition was complete the reaction was then allowed to warm to room temperature on its own accord The msultant homogenous solution was quenched with saturated aqueous ammonium chloride and the aqueous portion was separated and extracted with CH3Cl3. The organic extract was washed with 1N HCl. saturated aqueous NaHC@ brine, dried (NazSO.t), filtered and concentrated in vacno. Rroducts were puritYed by flash column
chromatography on silica gel. In conclusion, we have provided a new, general procedure for protection of 1Mihydroxycyclopentanes as cyclic carbonates. The reported methodology can also serve as an alternative for carbonate protection of hindered 1,3-acyclic and 1,2-cyclic diols. We anticipate further applications of
niphosgene use in the ptotection of this functionality in the future. Adsaowkdgment: The authors acknowkdge the encouragement and support of Dr. Michael ELGarst.
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Table 1. Synthesis of Cyclic Carbonates With Tripbosgene Entry Diolr Carbon&a Yield(%)b
1.
AA
0-L
87
2.
92
3.
84
4.
99
5.
oc;*o
a3
6. 7.
85 99
8.
94
Wl reactions wue conducted under Nz annosphuv. byield of pun pmducts after silica gel chmmatography and c-on bytheir~HNMR,~3CNMR,IRandmassspccea. VieId fur multigram scale reaction carried out wing 10 quiv pyridinc and 0.5 qti triphosgcne in CH$l2 (0.08 M).
References
8nd Notes:
1.
For comprehensive reviews on pmstaglandin synthesis, please see: (a) Cotey, E. I. and Cheng, X. -M. The Logic ofChemicai Synthes& John Wiley and Sons, Inc.:New York, 1989; Chapter 11; (b) New Synthetic Routes to Prostagiandinsand Thromboxanes,Roberts, S. M. and Scheimmmn, F. Eds.; Academic Press: London, 1982; (c) Bindra, J. S. and Bindra, R Prostaglandin Synthesis. Academic Press:
London, 1977; (d) Mitra, A. The Synthesis of Prostagiandins,John Wiley and Sons, Inc.: New York, 1977.
2.
Far recent examples and leading tehrences: (a) Collins, P. W.; Kramer, S. W.; Gasiaki, A. F.; W&r, R. M.; Jones, P. H.; Gulliison,
(b)
Collins, P. W.; Gasiecki, A. F.; Jones, P. H.; Bauer, R. F.; Gullikson, G. W.; Woods, E. M.; Bianchi, R. G.; Ibid. 1986,29,1195; (c) Bundy, G. L.; Morton, D. R.; Peterson, D. C.; Nishizawa, E. E.; (d) Schaaf, T. K.; Johnson, M. R.; Constantine, J. W.; Bindra, J. S.;
(e) Hayashi, M.; Arai, Y.; Wakatsuka, H; Kawamm, hi.;
Tanouchi, T.; Wakatsuka, H.; Arai. Y.; Yamoto, T.; Kajiwam, I.; Konishi, Y.; Tsuda, T.; Matsumoto. K. Ibid. 1980.23.519. 3. Set reference 2c and Morozowich, W.; Oesterling. T. 0.; Miller, W. L.; Lawson, C. F.; Comette, J. C.; Weeks. J. R.; Douglas, S. L. J. Pharm. Sci. 1979,68,949.
4.
Greene, T. W. and Wuts, P. G. M. ProtectiveGroups in Organic Synthesis,John Wiky and Sons, Inc.: New York, 1991.
5. 6.
Eckert, H. and Forster, B. Angew. Chem. ht. Ed. Engl. 1987,26,894. Triphosgene was recently reported in the preparation of the reagent di(2-pyridyl) carbonate: Ghosh, A. K.; Duong, T. T.; McKee, S. P. Tetrahedron Lett. 1991,32. 4251. (b) Daly, W. H. and Poche. D.
7.
(a) Wilder, R. and Mobashery, S. J. Org. Chem. 1992,57,2755; Tetrahedron L&t. 1980.29.5859.
8. 9.
Gill, G. B.; Pattenden, G.; Reynolds, S. J. Tetrahedron Len. 1989,30,3229. Goren, Z.; Heeg, M. J.; Mobashery, S. J. Org. Chem. 1991,56,7186.