Mesyl introduction

Alkenylation of cyclopentenone with the alkenylstannane 719 has been used for the introduction of an a,>-chain into a prostaglandin derivative[590]. Even the vinyl mesylate (methanesulfonate) 720 can be used for coupling with alkenylstannanes[59l]. 

The oxygen atom at 21 is similarly an expendable group. Reaction of 241 (obtained from 185 by the usual procedure for introduction of the 9a-fluoro group) with methanesulfonyl chloride affords the 21 mesylate (242a). Replacement of the leaving group at 21 with iodine by means of potassium iodide in acetone followed by reduction of the halogen with zinc in acetic acid leads to fluorometholone (243). ... 

The treatment of CML has experienced a dramatic change since the introduction of imatinib. Imatinib mesylate (STI-571 ... 

Introduction of a trimethylsilyl group at the terminal alkynyl position of the foregoing chiral mesylates reverses the regiochemistry of the addition reactions (Table 9.35) [50]. In these systems, the allenyl adducts are strongly favored in additions that are highly diastereo- and enantioselective. 

The bromoallene (-)-kumausallene (62) was isolated in 1983 from the red alga Laurencia nipponica Yamada [64a], The synthesis of the racemic natural product by Overman and co-workers once again employed the SN2 -substitution of a propargyl mesylate with lithium dibromocuprate (Scheme 18.22) [79]. Thus, starting from the unsymmetrically substituted 2,6-dioxabicyclo[3.3.0]octane derivative 69, the first side chain was introduced by Swern oxidation and subsequent Sakurai reaction with the allylsilane 70. The resulting alcohol 71 was protected and the second side chain was attached via diastereoselective addition of a titanium acetylide. The synthesis was concluded by the introduction of two bromine atoms anti-selective S -substitution of the bulky propargyl mesylate 72 was followed by Appel bromination (tetrabromo-methane-triphenylphosphine) of the alcohol derived from deprotection of the bromoallene 73. 

Chemical Properties. Methanesulfonyl chloride (MSC) is a reactive chemical which allows introduction of the mesyl group, CH3SO 2, into a... 

The classic ionic methods for the removal of an unwanted hydroxyl group are summarized in detail in the book by Larock [6]. One method involves—for primary and unhindered secondary alcohols—the synthesis of the corresponding mesylates or tosylates. These compounds are prepared readily and then transformed into the corresponding deoxy compounds by reduction [7], Alternatively, introduction of a thiolate or halogen by a nucleophilic reaction can also be used. These compounds can then be readily desulfurized or dehalogenated (Scheme 1). Tertiary alcohols present no problem either, because a... 

A tandem one-pot elimination-intramolecular Diels-Alder reaction occurs when the mesylate of 4-homoallylic azetidinone having a orc-alkene or alkyne substituent is heated in a sealed tube in the presence of an equimolecular quantity of l,8-diazabicyclo[5.4.0]undec-7-ene (DBU). The method has been used to produce derivatives of oxace-pham. In a similar way, the 3,4-disubstituted azetidinone mesylate 473 afforded an 88% yield of 474. The method can be further elaborated through the introduction of a novel [3,3]-sigmatropic rearrangement of a-allenic mesylates thus, 475 yielded 476 on thermolysis C1999TL1015, 2000JOC3310, 2005EJ098>. 

In the previous subsection, it was shown that the Ferrier reaction offers an opportunity to convert glycal derivatives into unsaturated sugar derivatives, which have an isolated double bond between C(2) and C(3). The Tipson-Cohcn reaction is another important reaction for the introduction of isolated double bonds.29 In this procedure, a cis or tram diols are converted into disulfonates (mesylates or tosylates) which are reductively eliminated with sodium iodide and zinc in refluxing DMF (Scheme 3.6a). In this reaction, the C(3) sulfonate is substituted by an iodide, which then is reductively removed by zinc with concomitant elimination of the second sulfonate moiety, introducing a double bond. Stereoelectronic effects make nucleophilic substitutions at C(3) more favourable than similar reactions at C(2) (see Section 3.2.3). Probably, the elimination proceeds through a boat conformation. In this case, the iodide and tosylate are in a syn relation. In most cases, E2 elimination proceeds via a transition state involving an anti orientation. Nevertheless, syn elimination becomes the dominant mode of reaction when structural features prohibit an anti orientation. 

The silver-catalyzed cycloisomerization of allenic carboxylic acids to butenolides was also reported by Marshall and co-workers.329 Starting from the enantiomerically enriched propargyl mesylate 390, palladium-catalyzed hydroxycarbonylation led to the chiral allenecarboxylates 391 which afforded the butenolides 392 upon treatment with silver nitrate (Scheme 114). Unfortunately, partial racemization could not be avoided in this two-step sequence. In a related study, Ma and Shi330 have shown that the combination of Pd(PPh3)4 and Ag2C03 promotes the cyclization of allenecarboxylates to the corresponding butenolides, accompanied by the introduction of aryl or alkenyl groups at C3. 

A large number of aza crowns are made by these routes. Stepwise addition of CH2CH2NHTs groups occurs readily by reaction of the appropriate tolu-enesulfonamide with 2-bromoacetamide followed by borane reduction and A-tosylation. If a trimethylene spacer is desired, then reaction of the tosyla-mide with acrylonitrile followed by reduction and tosylation gives good yields of the desired product (Scheme 1.2). An example of such a sequence is provided by the synthesis of the symmetrical [24]-N6 cycle, 4 (Scheme 1.3).9 In this particular case, introduction of the desired C3 spacer was undertaken on the. electrophilic component by conjugate addition of the tosylamide with methyl acrylate followed by reduction with LiAlH4 and mesylation. 

The first group93) chose an approach by which the introduction of the upper side chain was achieved by reaction of the optically active epoxide 165 with the sodium derivative of diethylmalonate to the mixture of the isomers 166 and 167. The desired isomer 166 was isolated in 20% yield by chromatography on silica gel. The stereocontrolled opening of the epoxide which had been prepared out of 163 via the mesylate 164 was the prerequisite for the correct configuration of the prostanoid side chains in compound 171. 

The SLibstitiilion of an inorganic ester group, such as /t-toluenesulfonate (tosylate), methanesul-I onate (mesylate), trifluoromethancsulfonate (triflate), cyclic sulfate, etc., by fluorine is one of the most important methods for the introduction of fluorine into aliphatic molecules. It is an indirect method for the substitution of a hydroxy group with a fluorine. By using an in situ esterification, e.g, with trifluoromethancsulfonyl fluoride, and fluorination, c.g. with tetrabutyl-ammonium fluoride, it also provides a one-pot reaction for realizing this reaction. 

The carbonyl group in 115 allowed the introduction of the C3 unit essential for ring A later via the dimethylhydrazone. The primarily a-alkylated product was epimerized and transformed into mesylate 116, which was needed for the key reaction. The B ring-forming fragmentation 116 117 was effected by reduc-... 

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