Maleimide stability

Phosphorus containing poly(maleimide-amines) were synthesized from N,N -bisdichloromaleimido-3,3 -diphenyl alkylphosphine oxides and aromatic diamines or piperazine [144]. The polymers prepared from piperazine are soluble in DMF, DM AC, DMSO, etc., but have poor thermal stability and flame retardancy. 

Poly(hydroxyphenyl maleimide)-b-PBA was added to thermosetting phenol resin to improve heat resistance [63]. PVC blended with poly(vinyl copolymer having cyclohexyl maleimide group)-b-PVC showed improved heat resistance and tensile strength with thermal stability during processing [64]. 

Mataka and coworkers reported the studies of the Diels-Alder reactions of [3.3] orthoanthracenophanes 96 and 97, of which anthraceno unit, the potential diene, has two nonequivalent faces, inside and outside. The reactions of 96 with dien-ophiles gave the mixtures of inside and outside adducts with the ratios between 1 1 and 1 1.5. However, the ratio changes drastically, in favor of the inside adducts, when 97 reacts with dienophiles such as maleic anhydride, maleimide and naphto-quinone [55] (Scheme 46). Mataka suggested that the Jt-facial selectivity is controlled by an orbital interaction between the electron-poor dienophiles and the Jt-orbital of the facing aromatics, which would lead to a stabilization of the transition state, while Nishio suggested that the selectivity is due to the attractive k/k or CH/jt interaction [53]. 

In addition, the PEG-based heterobifunctional crosslinkers described in Chapter 18, Section 2, provide enhanced water-solubility for antibody conjugation applications. Conjugation of antibody molecules using a maleimide-PEG -NHS ester compound actually increases the solubility of the antibody and may help to maintain stability for certain sensitive monoclonals better than the traditional aliphatic crosslinkers. The methods described below for SMCC may be used with success for PEG-based reagents or other maleimide-NHS ester heterobifunctionals. 

The correct ratio of lipid constituents is important to form stable liposomes. For instance, a reliable liposomal composition for encapsulating aqueous substances may contain molar ratios of lecithin cholesterol negatively charged phospholipid (e.g., phosphatidyl glycerol (PG)) of 0.9 1 0.1. A composition that is typical when an activated phosphatidylethanolamine (PE) derivative is included may contain molar ratios of phosphatidylcholine (PC) cholesterol PG derivatized PE of 8 10 1 1. Another typical composition using a maleimide derivative of PE without PG is PC male-imide-PE cholesterol of 85 15 50 (Friede et al., 1993). In general, to maintain membrane stability, the PE derivative should not exceed a concentration ratio of about l-10mol PE per lOOmol of total lipid. 

The photopolymerization of mixtures of maleimides and vinyl ethers is shown to be an efficient, rapid process in the absence of external photo initiators. Polymerization proceeds both in the presence and absence of oxygen. Films produced by the photopolymerization of maleimide/vinyl ether systems exhibit little absorbance at wavelengths greater than 300 nm. The thermal stability of these films are also excellent. 

In order for maleimide/vinyl ether photoinitiator free photopolymerization to be useful, it is important that the cured films have good thermal/UV stability. Since there are no small molecule photoinitiators added to the uncured mixture initially, there is no residual small molecule photo initiator present in the final crosslinked film. This accounts for the enhanced UV stability we have observed for cured maleimide/vinyl ether films. In addition, TGA thermograms of photocured films of the MPBM/CHVE mixture (Figure 8) exhibit excellent thermal stability, with decomposition occurring at higher temperatures than for a simple UV cured HDDA film with 3 weight percent DMAP photoinitiator. (Such thermal stability would be... 

However, due to the aromatic ring adjacent to its maleimide functional group, MBS displays less stability toward maleimide ring opening than SMCC (see this chapter Section 1.3). Unlike SMCC, MBS is therefore not recommended for preparing freeze-dried, maleimide-activated proteins, since during the processing necessary to purify and stabilize the derivative much activity can be lost by hydrolysis. 

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