Скачать книгу

D. Bourissou, S. Moebs‐Sanchez, B. Martin‐Vaca, C. R. Chimie 2007, 10, 775–794.

      178 178. J. Pretula, S. Slomkowski, S. Penczek, Adv. Drug Deliv. Rev. 2016, 107, 3–16.

      179 179. D. A. Rothrock and R. F. Conyne, GB 588834, 1947 (to Resinous Prod. & Chemical Co.).

      180 180. N. A. Higgins, U.S. Patent 2,683,136, 1954 (to Du Pont).

      181 181. T. Kusunoki, T. Unrinin, O. Morimoto, US Patent 8,642,717, 2014 (to Toyo Boseki).

      182 182. G. Gobius du Sart, W. de Lang, WO 2020245063, 2020 (to Total Corbion PLA bv).

      183 183. P. Gruber, J. J. Kolstad, E. S. Hall, R. S. E. Conn, EP 0,615,532, 2000 (to Cargill Inc.).

      184 184. J. J. Kolstad, D. R. Witzke, M. H. Hartmann, E. S. Hall, J. F. Nageroni, EP 1,070,097, 2001 (to Cargill Inc.).

      185 185. A. Södergård, J.‐F. Selin, M. Niemi, C.‐J. Johansson, K. Meinander, EP 0,737,219, 1999 (to Fortum Oyj).

      186 186. S. C. de Vos, EP 2,271,696, 2012 (to Purac Biochem bv).

      187 187. D. G. Lowrance, U.S. Patent 1,995,970, 1935 (to Du Pont).

      188 188. P. Gruber, J. J. Kolstad, C. Ryan, EP 0,615,529, 1994 (to Cargill Inc.).

      189 189. H. Ohara, S. Sawa, M. Ito, Y. Fujii, M. Oota, H. Yamaguchi, U.S. Patent 5,770,682, 1998 (to Shimadzu Corp.).

      190 190. H. Ohara, T. Okamoto, U.S. Patent 5,728,847, 1998 (to Shimadzu Corp.).

      191 191. H. Ohara, S. Sawa, T. Kawamoto, EP 0,664,309, 1995 (to Shimadzu Corp.).

      192 192. Crystallizing and Drying of PLA, NatureWorks LLC, available at https://www.natureworksllc.com/~/media/Files/NatureWorks/Technical‐Documents/Processing‐Guides/ProcessingGuide_Crystallizing‐and‐Drying_pdf.pdf (accessed date 23 February 2021).

      193 193. F. G. Hutchinson, EP 0,244,114, 1987 (to ICI PLC).

      194 194. K. Yamamoto, T. Tani, T. Aoki, Y. Hata, EP 1,310,517, 2003 (to Wako Pure Chem. Ind. Ltd.; Tadeka Chem. Ind. Ltd.).

      195 195. E. Feghali, L. Tauk, P. Ortiz, K. Vanbroekhoven, W. Eevers, Polym. Degrad. Stab. 2020, 179, 109241.

      Ann‐Christine Albertsson, Indra Kumari Varma, Bimlesh Lochab, Anna Finne‐Wistrand, Sangeeta Sahu and Kamlesh Kumar

      High molar mass poly(lactic acid) (PLA) is obtained by either the polycondensation of lactic acid or ring‐opening polymerization (ROP) of the cyclic dimer 2,6‐dimethyl‐1,4‐dioxane‐2,5‐dione, commonly referred to as dilactide or lactide (LA). The stereochemistry of LA plays a crucial role in dictating the properties of the polymers which have already been described in earlier chapters (Chapters 1 and 3).

      L‐Lactide (LLA) is prepared with relatively high enantiopurity from corn starch fermentation, which polymerized to form poly(L‐lactide) (PLLA). PLLA is a versatile, semicrystalline, degradable polymer with a relatively high melting (T m) and glass transition temperature (T g). PLLA has mechanical properties which makes it interesting for many applications such as degradable plastic for disposable consumer products [1–3]. It is also of interest in medical applications [4], due to its favorable interactions with the cells. PLLA is also explored as a degradable scaffold where the transplanted cells could remold their intrinsic tissue superstructural organization, and thereby led to the desirable three‐dimensional structure and physiological functionality of a regenerated organ [5]. However, certain shortcomings of PLLA may need to be overcome to extend its applications. In particular, high crystallinity [6], brittle behavior with a very‐low elongation at break value, and the hydrophobic nature of the polymer demands a long degradation time. The properties of PLLA are tailored by copolymerization (random, block, and graft), change in molecular architecture (hyperbranched polymers, star shaped, or dendrimers), introduction of polar groups such as carboxyl, amino, or thiol‐based via end group or main‐chain functionalization, or blending with other polymers. Physical properties, such as T g, T m, crystallinity, hydrophobicity, and mechanical properties are significantly affected by such modifications. Furthermore, functionalization of PLLA can provide specific bio‐interactions with cells, which is specifically needed in tissue engineering. Several reviews have summarized how functionalization of lactide and copolymerization with other hydroxyl‐acid‐based monomers influence the properties and applications of the resultant copolymers [5,7–15]. In this chapter, preparation of polymers and copolymers of LAs with different structures, using polycondensation and ROP, is described. The influence of macromolecular structure and composition on the properties of structurally modified polymers is also discussed. The stereocopolymers of LA prepared by the polymerization of various stereoisomers are discussed in a subsequent section in this book and will not be discussed here.

Schematic illustration of structures explored as comonomers with lactide monomer. Schematic illustration of structures of catalysts used in lactide polymerization.

Скачать книгу