Dimeric stereospecific sites

PA = 226 kcal moP ), the predominant formation (6.4 to 1) of the (7 ,5 )-di-2-butyl ether over the (R,R) and (5, 5 )-forms is attributed to a simple backside displacement in the proton-bound adduct of the starting 2-butanol enantiomer with inversion of configuration of the reaction site and loss of a molecule of water. When tri-n-propylamine is replaced by the less basic NH3 (PA = 196 kcal moF ), fast neutralization of the proton-bound dimers of the starting 2-butanol is prevented and, therefore, they can grow, producing aggregates that resemble solution microenvironments in which SnI pathways may be accessible as well. In them or in their primary substituted derivatives, consecutive nucleophilic displacements may take place. As a consequence, the stereospecificity of the process is lost and the [(R,S)-di-2-butyl ether]/[(7 ,7 )- and (5, 5 )-di-2-butyl ethers] ratio falls down to 1.2. In this case. 

Receptor dimerization does not appear sufficient for signaling, however. Introduction of interreceptor disulfide bonds at different sites within the juxtamembrane region of ErbB receptors results in both active and inactive dimers (Burke et al, 1997). Requirement for a stereospecific dimer is also seen for cytokine receptors (Jiang and Hunter, 1999) and suggests that conformational information is transmitted across the plasma... 

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