Functionalization chloromethylation

The limitations of this reagent are several. It caimot be used to replace a single unactivated halogen atom with the exception of the chloromethyl ether (eq. 5) to form difluoromethyl fluoromethyl ether [461 -63-2]. It also caimot be used to replace a halogen attached to a carbon—carbon double bond. Fluorination of functional group compounds, eg, esters, sulfides, ketones, acids, and aldehydes, produces decomposition products caused by scission of the carbon chains. 

Strong Base Anion Exchangers. As ia the synthesis of weak base anion exchangers, strong base resias are manufactured from styrenic as well as acryhc copolymers. Those based on copolymers of styrene and divinylben2ene are chloromethylated and then aminated. These reactions are the same as for the styrenic weakbase resias. The esseatial differeace is the amine used for amination. Trimethyl amine [75-50-3] N(CH2)3, and /V, /V- dim ethyl eth a n ol amine [108-01 -0] (CH2)2NCH2CH20H, are most commonly used. Both form quaternary ammonium functional groups similar to (8). 

The six-position may be functionalized by electrophilic aromatic substitution. Either bromination (Br2/CH2Cl2/-5°) acetylation (acetyl chloride, aluminum chloride, nitrobenzene) " or chloromethylation (chloromethyl methyl ether, stannic chloride, -60°) " affords the 6,6 -disubstituted product. It should also be noted that treatment of the acetyl derivative with KOBr in THF affords the carboxylic acid in 84% yield. The brominated crown may then be metallated (n-BuLi) and treated with an electrophile to form a chain-extender. To this end, Cram has utilized both ethylene oxide " and dichlorodimethyl-silane in the conversion of bis-binaphthyl crowns into polymer-bound resolving agents. The acetylation/oxidation sequence is illustrated in Eq. (3.54). 

Montanari and coworkers have been particularly active in this area. They have generally utilized crowns or cryptands having long arms attached to them. These lipophilic arms are typically terminated in a primary or secondary amino function which may serve as a nucleophile in the reaction with a chloromethylated polystyrene residue. 

A functional group is introduced to the polystyrene 10 by chloromethylation Blanc reaction) in order to allow for reaction with the substrate 11. The polymer-bound diester is then treated with base to initiate the Dieckmann condensation. 

Substitution of a dipeptide unit by a cychc dipeptide derivative within a peptide chain can induce certain conformational restraints that may alter the biological response via changing receptor selectivity. A facile procedure for synthesis of pyrazinone ring-containing opioid mimetics [21] has been elaborated, based on the cycHzation of readily available dipep-tidyl chloromethyl ketones [22] (Scheme 6). This method affords 2(IH)-pyrazinone derivatives containing substituents with desired functional groups at positions 3 and 6 in high yield. 

Hoomaert has studied Diels-Alder reactions of pyridine oquinodimethane analogs generated from functionalized o-bis(chloromethyl)pyridines <96T(52)11889>. The photochemical cycloaddition of 2-alkoxy-3-cyano-4,6-dimethylpyridine with methacrylonitrile gives a bicyclic azetine, 6-alkoxy-3,5-dicyano-2,5,8-trimethyl-7-azabicyclo[4.2.0]octa-2,7-diene, in moderate yield <96CC1349>. Regiospecific hydroxylation of 3-(methylaminomethyl)pyridine to 5-(methylaminomethyl)-2-(17/)-pyridone by Arthrobacter ureafaciens has been reported <96MI173>. 

Coumarincarboxylate derivatives are versatile, efficient, low molecular weight, nonpeptidic protease inhibitors. Both esters and amides behave as time-dependent inhibitors of a-chymotrypsin but the esters are clearly more efficient than the corresponding amides. The criteria for a suicide mechanism are met. The presence of a latent alkylating function at the 6-position (chloromethyl group) is required to produce to inactivation by a suicide mechanism (Scheme 11.3, pathway a). Aryl esters, in particular the meta-substituted phenyl esters are the best inhibitors. Thus, m-chlorophenyl 6-(chloromethyl)-2-oxo-27/-l-benzopyran-3-carboxylate is one of the well-known inactivator of a-chymotrypsin (kJK, = 76(),000M s 1 at pH 7.5 and 25 °C, Table 11.1). 

The 6-chloromethyl substituent (series 5 and 6) is required for the inactivation of a-chymotrypsin. Nevertheless, there is only a transient inactivation of HLE and thrombin through the formation of a stable acyl-enzyme in spite of the presence of this group as demonstrated by the spontaneous or hydroxylamine-accelerated reactivation of the treated enzymes (Scheme 11.3, pathway b).21 HLE is specifically inhibited when such an alkylating function is absent (series 7), always through the formation of a transient acyl-enzyme (Table 11.2). 

Even in solution the relative rigidity of the polymer support can play a significant role in the reactivity of attached functional groups. Contrasting studies conducted with chloromethylated derivatives of poly(arylene ether sulfone) (Tg 175°C), phenoxy resin (Tg= 65°C) and polystyrene (Tg= 105°C) allow evaluation of chain rigidity effects. We have shown that the rates of quaternization of chloromethylated poly(arylene ether sulfones) and phenoxy resin deviate from the anticipated second order process at... 

Our objective In this paper is to illustrate the methods for functionalizing poly(arylene ether sulfone). Particular attention will be paid to bromination, nitration, aminatlon, chloromethyl-ation, and aminomethylatlon of 1 and its corresponding model compound. 

The chloromethylated polymers are very reactive substrates for nucleophilic attach further elaboration can be accomplished under homogeneous conditions In aprotlc solvents, or under heterogeneous conditions In the presence of phase transfer catalysts. The following examples are representative of approaches to functionalized condensation polymers via chloromethylated Intermediates. 

PECH was modified under similar reaction conditions, except that dimethylformamide (DMF) was used as the reaction solvent. In addition, the phase-transfer-catalyzed etherification of the chloromethyl groups of PECH with sodium 4-methoxy -4 -biphenoxide was used to synthesize PECH with direct attachment of the mesogen to the polymer backbone. Similar notations to those used to describe the functionalized PPO are used for functionalized PECH. In this last case, PPO was replaced with PECH. Esterification routes of both PPO and PECH are presented in Scheme I. 

Alkyl methacrylates, hydrolysis of polymeric ester functionality, 259 Aluminum-hydrogen bond, nucleophilic substitution, 264 Amines alkylation, 28 benzyl-group cleavage, 25 Aminomethylation chloromethylated polymers, 19 Deltfpine reaction, 19 Anionic polymerization advantages, 85... 

A group of peptide derivatives such as peptide arginals and boronic acid peptide derivatives belong to another class of reversible thrombin inhibitors. One such inhibitor is PPACK (D-Phe-Pro-Arg chloromethyl ketone), which functions as a powerful irreversible thrombin inhibitor by alkylating the histidine residue at the catalytic site of thrombin (58). It, however, is unstable in neutral solution, as it undergoes cyclization and inactivation. However, the D-methyl derivative of D-Phe-Pro-Arg-H (D-Mephe-Pro-Arg-H) called efegatran, with a molecular mass of 515 Da, is a stable selective reversible inhibitor of thrombin with a K. of approximately 100 nM. The basic amino terminus in this compound is responsible for promoting the specificity toward thrombin (63). 

A second strategy is to attach a linker (also referred to as a handle or anchor) to the resin followed by assembly of the molecule. A linker is bifunctional spacer that serves to link the initial synthetic unit to the support in two discrete steps (Fig. 3). To attach a linker to a chloromethyl-PS resin, a phenol functionality such as handle 4 is used to form an ether bond (Fig. 4). To attach the same handle to an amino-functionalized support, acetoxy function 5 or a longer methylene spacer of the corresponding phenol is applied to form an amide bond. Both of these resins perform similarly and only differ in their initial starting resin [4], An alternative approach is to prepare a preformed handle in which the first building block is prederivatized to the linker and this moiety is attached to the resin. For peptide synthesis, this practice is common for the preparation of C-terminal peptide acids in order to reduce the amount of racemization of the a-carbon at the anchoring position [5],... 

Tetramethyl-l,3-disilacyclobutane had been prepared earlier by Knoth and Lindsey [10], but a multistep synthesis was involved which was not generalizable to the synthesis of Si-functional 1,3-disilacyclobutanes. The reaction shown in eq. 4, provided it is carried out in the right way, represents a good, general route to 1,3-disilacyclobutanes. This reaction was reported first by Muller and his coworkers [11]. In this work, diethyl ether was used as reaction solvent and the product yield was only around 4%. Somewhat better yields were obtained" by Russian workers [12], but it was the detailed studies of the (chloromethyl)chlorosilane/ magnesium reaction by Kriner [13] which provided a good synthesis of... 

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