Mercaptoethylamines

Reaction with Sulfur Nucleophiles, Because sulfai is highly nucleophilic, reactions of aziridines with sulfur nucleophiles generally proceed rapidly (111) and with good yields. The reaction of hydrogen sulfide [7783-06S-J with ethyleneimine yields cysteamine [60-23-1] (2-mercaptoethylamine) or bis(2-aminoethyl)sulfide [871-76-1] (2,112) depending on the molar ratio of the reactants. The use of NaHS for the synthesis of cysteamine has also been described (113). 

Primary and secondary aliphatic and aromatic amines react readily with thiiranes to give 2-mercaptoethylamine derivatives (Scheme 76) (76RCR25, 66CRV297). The reaction fails or gives poor yields with amines which are sterically hindered e.g. N,iV-dicyclohexylamine) or whose nitrogen atom is weakly basic e.g. N,A/ -diphenylamine). Aromatic amines are less reactive and higher reaction temperatures are usually required for them. The reaction mechanism is Sn2 and substituted thiiranes are attacked preferentially at the least hindered... 

Pantothenic acid, sometimes called vitamin B3, is a vitamin that makes up one part of a complex coenzyme called coenzyme A (CoA) (Figure 18.23). Pantothenic acid is also a constituent of acyl carrier proteins. Coenzyme A consists of 3, 5 -adenosine bisphosphate joined to 4-phosphopantetheine in a phosphoric anhydride linkage. Phosphopantetheine in turn consists of three parts /3-mercaptoethylamine linked to /3-alanine, which makes an amide bond with a branched-chain dihydroxy acid. As was the case for the nicotinamide and flavin coenzymes, the adenine nucleotide moiety of CoA acts as a recognition site, increasing the affinity and specificity of CoA binding to its enzymes. 

Aromatic aldehydes such as benzaldehyde, anisaldehyde, or 4-pyridinealdehyde react with neat N,S-silylated 2-mercaptoethylamines 475 at 20°C to give the N,S-... 

The crystal and molecular structure of the Ni11 complex of the simplest amino-thiolate ligand 2-mercaptoethylamine (aet) (454) has been determined and shows that the complex, contrary to earlier belief, has a trans configuration.1277... 

The use of a 500-fold molar excess of 2-mercaptoethylamine over the concentration of antibody presence was found to result in a partially reduced antibody in which two disulfides were reduced to yield four thiols (Sun et al., 2005). This strategy can be used to retain a biospecific antibody construct for subsequent discrete conjugation at the hinge region between the heavy chains. 

Figure 1.77 Disulfide reducing agents such as 2-mercaptoethylamine can be used to cleave the disulfide bonds in the hinge region of antibody molecules. Either intact IgG molecules or F(ab )2 fragments may be reduced in this manner to yield monofunctional antigen binding fragments.

Purify the reduced IgG from excess 2-mercaptoethylamine and reaction by-products by dialysis or gel filtration using a desalting resin. All buffers should contain 1-10 mM EDTA to preserve the free sulfhydryls from metal-catalyzed oxidation. The sulfhydryl-containing half antibody now may be used in conjugation protocols that use —SH-reactive heterobifunctional crosslinkers (Chapter 5, Section 1). 

Figure 22.30 An iodoacetamide derivative of PE containing an extended spacer arm can be constructed through a carbodiimide coupling of iodoacetic acid to PE, followed by reaction with 2-mercaptoethylamine, and finally another reaction with iodoacetate.

For reduction of the cystamine disulfides, add 20 pi of 1.0 M DTT and incubate at room temperature for 15 minutes. This will release 2-mercaptoethylamine from the cystamine modification site and create the free sulfhydryl on the 5 terminus of the oligonucleotide. 

CdS CdF2, Cd(C104)2, CdCl2, Cdl2, Cd(CH3COO)2, Cd(HCOO)2 + 2-mercaptoethylamine hydrochloride, cysteine, ethylenediamine, triethanolamine, monoethanolamine, nitrilotriacetic acid trisodium salt Na2S XRD, UV, AFM, Auger, XPS 77,78... 

The actual pathway by which fatty acid oxidation occurred was established by Lynen (1952-1953). Its unique and characteristic reaction was the thioclastic attack by coenzyme A on the B-ketoacyl CoA derivative, splitting off the 2C fragment, acetyl CoA. Free coenzyme A was very difficult to isolate and although it was synthesized in Todd s laboratory in Cambridge in the mid-1950s, much of the early work from Lynen s laboratory utilized A-acetyl cysteamine as a not very efficient (ca.1%) coenzyme A analogue. It carried the essential thiol group of the B-mercaptoethylamine end of CoA and could be used in most, but not all, of the steps in the spiral. 

Semitelechelic HPMA polymers were synthesized by free radical polymerization of HPMA using 2,2 -azobis(isobutyronitrile) (AIBN) as the initiator and alkyl mercaptans as chain transfer agents. Alkyl mercaptans with different functional groups, namely, 2-mercaptoethylamine, 3-mercapto-propionic acid, 3-mercaptopropionic hydrazide, and methyl 3-mercapto-propionate, were used as the chain transfer agents ST HPMA polymers... 

Figure 1 The effect of concentration ratio of mercaptans ( , 2-mercaptoethylamine , methyl 3-mercaptopropionate , 3-mercaptopropionic acid , 3-mercaptopropionic hydrazide) to HPMA on the weight average molecular weight (SEC) of ST HPMA polymers (data from Reference [20]). 

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