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Li, G.; Zhao, M.; Xu, F.; Yang, B.; Li, X.; Meng, X.; Teng, L.; Sun, F.; Li, Y. Polylactic Acid. Encyclopedia. Available online: (accessed on 15 June 2024).
Li G, Zhao M, Xu F, Yang B, Li X, Meng X, et al. Polylactic Acid. Encyclopedia. Available at: Accessed June 15, 2024.
Li, Ge, Menghui Zhao, Fei Xu, Bo Yang, Xiangyu Li, Xiangxue Meng, Lesheng Teng, Fengying Sun, Youxin Li. "Polylactic Acid" Encyclopedia, (accessed June 15, 2024).
Li, G., Zhao, M., Xu, F., Yang, B., Li, X., Meng, X., Teng, L., Sun, F., & Li, Y. (2020, November 17). Polylactic Acid. In Encyclopedia.
Li, Ge, et al. "Polylactic Acid." Encyclopedia. Web. 17 November, 2020.
Polylactic Acid

As a degradable and environmentally friendly polymer, polylactic acid, also known as polylactide, is favored by researchers and has been used as a commercial material in various studies. Lactic acid, as a synthetic raw material of polylactic acid, can only be obtained by sugar fermentation. Good biocompatibility and biodegradability have led it to be approved by the U.S. Food and Drug Administration (FDA) as a biomedical material. Polylactic acid has good physical properties, and its modification can optimize its properties to a certain extent. Polylactic acid blocks and blends play significant roles in drug delivery, implants, and tissue engineering to great effect.  This entry introduces synthesis and biological application of polylactic acid.

PLA materials drug delivery polymer L- and D-lactic acid

1. Introduction 

The progress and optimization of high polymer materials play an important role in industrial production, especially in the fields of electronics, chemical and medical treatment. Since the synthesis of artificial plastics in the early 20th century, plastic polymer materials have been used in different fields and subject to significant development. At first, chemical polymers produced in the petroleum industry were favored due to their low cost, ease of production, excellent mechanical properties, and good heat sealability. Their rapid production had a negative impact on resources, economies, the environment, and safety, for example, (a) the use of oil and gas resources has led to increases in the prices of oil and natural gas; (b) the progress of global environmental warming; (c) the use of nonrecyclable materials; and (d) the occurrence of cross-contamination. Toxicity risk results from consumers' inability to metabolize their monomers [1][2]. That is to say, in the natural environment, it is not easy for plastics to spontaneously be completely degraded, especially in the face of large-scale use of plastic film coverings and packaging, which generate a large amount of waste and cause serious pollution and damage to the ecosystem [3]. Under the destruction of the environment due to the development of industry, the threat to human health is enormous, and millions of dollars are spent every year to deal with it. Therefore, research and development in the field of renewable, biodegradable plastics is attracting increasing attention from researchers. Biodegradable materials can gradually and spontaneously degrade in the natural environment, lastly entering nature in the form of small molecules. Polylactic acid (PLA) is a kind of lactic acid (LA) derivative produced from renewable resources such as wheat, straw, corn, and sorghum, and it is completely biodegradable [4][5]. It is environmentally friendly, and can be decomposed into water and carbon dioxide by microbes. Given the problem of global pollution, focusing on improving the environment is a win–win situation; thus, it is considered the most promising biodegradable polymer material on the market [6][7]. Although LA, the monomer of PLA, can be easily obtained in nature, it is traditionally produced by the fermentation of sugars and conversion into monomers after hydrolysis [8]. However, while a variety of synthetic methods have been studied for industrial and commercial use, none of these is simple, easy to operate, or economical. There are strict requirements with respect to the catalysts, synthesis steps, and purification equipment used in the synthesis process [9]. Fortunately, a moderate way is provided by biological methods using enzyme-catalyzed synthesis processes, which make biocompatible materials more readily available than drastic chemical reactions. In terms of nature, polylactic acid possesses good thermoplasticity and can be used to prepare and process plastics in order to make, for example, films and fibers [10][11]. Polylactic acid is not easily affected by solvent swelling and dissolution during industrial processing. Processing temperature is generally 170–230 °C, so it is also suitable for extrusion, spinning, biaxial stretching, and injection blow-molding processing methods [12][13][14]. Simultaneously, PLA material has good biocompatibility, biodegradability, gloss, and transparency, and antibacterial, flame-retardant, and oil- and water-resistant properties. It has a very wide range of uses, such as in packaging materials and nonwoven fabrics, and in the clothing, manufacturing, and healthcare industries [15][16][17][18][19]. At first, it is used in medical sutures and bone screws because of these properties. The ester bonds of the polymer backbone are broken by hydrolysis without additional surgeries, and the degradation products are non-toxic and avoid part of the immune response, which make it an ideal candidate for biomedical applications. The promising development of nanomedicine benefits from the synthesis of nanomaterials. The synthesis of nanomaterials provides a good prospect for the development of nanomedicine. Nano-polymers can be used to encapsulate chemical drugs, proteins, and genetic drugs to enhance the circulation of drugs in the human body while reducing the toxic side effects of drugs. PLA occupies an indispensable position in modern industrial technology.

2. PLA Synthesis and Properties

2.1. LA

LA is a monomer that comprises polylactic acid, and its existence is very common. It plays a vital role in the glycolytic energy cycle in organisms, as well as being an important substance for maintaining the growth and development of living organisms [20]. LA was first extracted from fermented milk by Swedish scientists in 1881. As the simplest hydroxy acid, there is an asymmetric carbon atom in the molecule that is optically active, so there are two optical isomers, l-lactic acid and d-lactic acid, as shown in Figure 1 [21][22]. LA obtained from animal muscle is dextrorotatory LA, while the other, lactic acid obtained by fermentation, is levorotatory LA. In the beginning, commercial LA was mainly derived from the fermentation of sugars by bacteria [23]. Sugars used for LA fermentation include starch, glucose, lactose, and maltose, produced by corn and potatoes. Fermentation is typically carried out for 3–5 days under low pH (about 5.0) and low oxygen at a temperature of about 40 °C [24]. However, this method produces a certain degree of toxicity as the concentration of fermented lactic acid increases, and the reaction continues. To obtain high-purity LA and improve the output efficiency of lactic acid, purification also constitutes a major problem [25]. In the beginning, the typical purification method was to add calcium hydroxide or calcium carbonate to the fermentation broth to neutralize the acid. The resulting calcium lactate could be evaporated, crystallized, and acidified to obtain further crude LA and insoluble calcium sulfate (gypsum). LA used in food or medicine often needs to be further purified to obtain a higher degree of LA. Subsequent studies showed that it can then be neutralized with recycled ammonia or sodium hydroxide. Subsequently, ultrafiltration, dyeing, and electrodialysis were developed as new processes for the low-cost production of LA [26].

Figure 1. Enantiomers of lactic acid.

Chemical synthesis methods have also been applied for the industrial production of LA. These fall into roughly three types: (a) The lactonitrile method. Lactonitrile is hydrolyzed by sulfuric acid to obtain crude LA. The crude LA is added to ethanol for esterification, and refined LA is obtained by distillation, concentration, and decomposition. (b) The acrylonitrile method. Like the above method, but with acrylonitrile replacing lactonitrile, hydrolyzed with sulfuric acid. Then, the hydrolyzed product was reacted with methanol; the crude ester is sent to the distillation tower, and the refined ester is heated and vacuumed to obtain the product. (c) The propionic acid method. Using propionic acid as raw material, crude LA is obtained through chlorination and hydrolysis; then, the product is obtained through esterification, rectification, and hydrolysis. Only a few manufacturers use this method due to the expensive raw materials [27].

Chemical methods are able to achieve large-scale continuous production of LA, and the U.S. Food and Drug Administration (FDA) has approved the resulting product; however, the raw materials are generally toxic. They do not accord with the standards of green chemistry. Some recent studies showed that, by adding bacteria and substrate-degrading enzymes for simultaneous saccharification and fermentation, starch or cellulosic biomass can be saccharified and simultaneously converted into LA; this process can be used as a replacement for the above-mentioned traditional fermentation steps [28][29]. This process reduces costs and improves efficiency.

2.2. PLA Polymer

Since LA is a chiral molecule with d-type and l-type isomers, three forms of polylactic acid are formed: poly-l-lactic acid (PLLA), poly-d-lactic acid (PDLA), and poly-d,l-lactic acid (PDLLA). With respect to optical activity, there are two compositions-L and D enantiomers-such that polylactic acid can be crystallized into three forms (α, β, and γ) [30][31][32]. In 1932, Carothers (DuPont) synthesized low-molecular-weight PLA products. However, due to the high cost of synthesis and poor product stability, this synthesis was not considered a success [33]. In 1954, DuPont produced a higher-molecular-weight PLA, and applied for a patent intending to enter the commercial market. Research on polymers attracted significant attention from society. With advances in medicine and public health, PLA began to be used in surgical sutures and bone implants in the 1960s. Today, PLA resin has been approved by the FDA and European regulatory authorities for use in food- and drug-delivery systems [12][34]. This has also led people to realize that, while PLLA has some advantages, it also has some disadvantages. For example, due to its high crystallinity and slow degradation rate, it can trigger an inflammatory response in the body. Fortunately, d-lactic acid degrades more quickly. If l-lactic acid and d,l-lactic acid monomers are used to synthesize PLLA, the above problems are avoided [35][36].

Three methods for the synthesis of polymer PLA (Mw > 10,000) were reported: (a) direct condensation polymerization; (b) azeotropic dehydration condensation; and (c) lactide ring-opening polymerization, as shown in Figure 2.

Figure 2. Synthesis of polylactic acid (PLA) from l- and d-lactic acids [28]. Adapted from Auras et al. by permission of Wiley–VCH Verlag GmbH & Co. KGaA.

2.3. PLA Properties

PLA has very good market prospects and excellent commercial value, with a range of applications from industrial to civilian use. Interest in its mass production stems from its good performance; for example, PLA has good physical properties and can be used to yield various plastic products, such as fast-food lunch boxes, and fabrics for industrial and civilian use [37][38][39][40]. Good tensile strength and ductility make it suitable for different processing means, such as melt-extrusion molding, injection molding, blown film molding, foam molding, and vacuum molding. Its good biocompatibility has led it to be widely used in the field of biochemical medicine. High-molecular-weight PLA has been used to produce non-dismantling surgical sutures and low-molecular-weight PLA as a slow-release drug-packaging agent [41].

Polymer PLA possesses good characteristics with regard to gloss, transparency, hand feel, and heat resistance. The dissolution of PLA depends on its degree of crystallinity. Amorphous polymers are soluble in various organic solvents, including acetone, acetonitrile, and methylene chloride. Furthermore, crystalline PLA can only be dissolved in dichloromethane or benzene at high temperatures. Mechanical properties and crystallization behavior are closely related to the molecular weight and stereochemical composition of the main chain. The hydroxy compound determines the molecular weight. The degree of crystallinity affects the degradation of PLA [42][43]. Highly crystalline polymers last for several months, with metabolism only taking place after a few years, while polymers with low crystallinity can be decomposed in a few weeks. Glass transition (Tg) directly affects the performance of the material with respect to both use and processing [44]. The good news is that the crystalline state does not affect the Tg. Jamshidi's research found that the Tg of PLA with a molecular weight of 22,000 g mol−1 was 55 °C, which is only 5 °C away from polymers of infinite molecular weight. Impact resistance increases with increasing crystallinity and molecular weight. Pure PDLA and PLLA have a melting point (Tm) of 207 °C. When they are mixed in equal proportions, racemic crystals with better mechanical properties are formed. The Tm of this crystal is 230 °C, and ultimate tensile strength is 50 MPa. Tg and Tm are vital physical parameters with respect to the properties of polylactic acid. The heat of fusion (△Hm) of 100% pure crystals is 93.7 J g −l. Subsequent research results showed that, with low PLA content, the Tm and Tg of PLA are decreased.

PLA has sufficient thermal stability to retard degradation and maintain molecular weight and performance. At temperatures greater than 200 °C, PLA undergoes hydrolysis, lactide recombination, oxidative main-chain scission, and intermolecular or intramolecular transesterification.

The degradation of PLA is contingent on many factors, including time, temperature, low-molecular-weight impurities, and catalyst concentration [27][45][46]. Studies found that simply modifying the purified pure polymer affects degradation. For example, acetylation of the hydroxyl end increases the decomposition temperature by 26 °C and ameliorates the decrease in molecular weight. At present, there is a general theory that the phenomenon resulting in PLA degradation is the process of simple proton-catalyzed hydrolysis chain scission [47]. Since the reaction is reversible, the purity of the polymer affects the degradation process during the synthesis reaction process, that is, the purity of the polymer can be used to explain the degradation kinetics of PLA. Furthermore, the crystallinity of the compound, as described above, determines the degradation rate and autocatalysis. When PLA is hydrolyzed and degraded in a biological environment, enzymes also participate. However, the specific role of enzymes in the reaction is currently unclear. Whether the reaction is catalyzed directly or by removing byproducts, so that the reaction is beneficial to forward progress, is not known. Supposing PLA is mainly degraded by hydrolysis, the degradation of polylactide is divided into two stages: the nonenzymatic melting of ester groups and the random scission of low-molecular-weight polymers by microorganisms to produce carbon dioxide and water [48][49].

2.4. Improvement of PLA Properties

Although PLA has good biocompatibility and stretchability, the properties of this seemingly promising polymer are not perfect and still need to be improved [50]. For example, PLA is extremely hydrophobic. This property makes it unsuitable for drug delivery, and its low impact toughness causes it to have certain disadvantages as a material for implants in the field of bone transplantation in a high-mechanical-strength environment [51]. However, certain methods can be employed to effectively improve the above deficiencies of PLA and make it more suitable for application in various fields. As a nanocomposite, the properties of PLA can be improved by adding modified additives during synthesis, or by directly blending it with other polymers. Copolymers with low Tg and flexibility may be more suitable for use in implantable medical devices and drug-delivery systems [52][53][54]. Therefore, increasing attention is being devoted to improving the low-temperature performance and malleability of PLA. For example, polyglycolic acid(PGA) has a high melting point (228 °C) and high Tg (37 °C) [55]. Its addition can lead to an amorphous polymer with a lower Tg, and this polymer is compatible with pure polymer. Compared with l-lactide, PGA has a higher hydrolysis rate due to its increased hydrophilicity. Therefore, the copolymer of ethylene glycol (5) and lactide, which has increased hydrophilicity and flexibility, has long been used commercially in biocompatible surgical sutures. Furthermore, since the ester bond of PLA is sensitive to enzymes, it can easily be catalyzed and hydrolyzed, leading to the disadvantage of too-fast drug release in drug-delivery systems. The copolymer consisting of LA and glycolic acid in a ratio of 2:23 known as VIRYL (Ethicon Inc.) [29] improves the controlled release of the drug. The copolymer formed with ε-caprolactone (6) changes the properties from rigidity to elasticity. The Tg of poly(ε-caprolactone) is −60 °C, and its Tm is approximately 59.5 °C. When the monomer is combined with pure l-lactide, l-PLA blocks are formed that exhibit high flexibility and crystallization with a high Tm. However, to synthesize tough polymers with favorable low-temperature properties, these blocks must be sufficiently large. Grijpma used a 1:1 ratio to synthesize a block with a longer sequence, a Tg of −39 °C, and a tensile strength of 18.2 MPa. Compared with the ε-caprolactone monomer, the monomer possessed increased tensile strength ranging from 0.6 to 48 MPa; an improvement exceeding 400%. Using tin octoate as a catalyst, copolymerization of lactide with different amounts of BMD (15), which is a polymer with carboxyl functional side chains, can be used to prepare PLA.

A simpler modification method is to blend two different polymers. The blending effect is amazing. The blend shows superior physical and mechanical properties than those of the original polymer [56]. Another method is to add plasticizers. Some plasticizers, such as low-molecular-weight citric acid, succinic acid, tartaric acid, and oxalate, are blended with PLA to change its mechanical and thermodynamic properties. There are many reports on using citrate and montmorillonite (MMT) to change toughness and plasticity [57][58][59][60]. The addition of plasticizer reduces the Tg of PLA by 26 °C. Adding PEG (polyethylene glycol) to the PLA/MMT blend produces more agglomerated structures, and the elongation at break of the material remains below 5% [60]. In order to change the biocompatibility of PLA via the blending method, starch can be used [29]. This low-cost method is simpler than synthesizing copolymers, and it also changes the mechanical properties. The accretion of starch leads to a reduction in tensile strength and elongation, and enhanced water absorption, which has advantages and disadvantages, such as an increase in the brittleness of the material. The addition of plasticizers can make up for this shortcoming. The use of polyether can develop a good hydrophilic, nontoxic, biodegradable, biocompatible, and flexible polymer. Zhu and coworkers used a 1.0:1.2 molar ratio of lactide and ethylene oxide to synthesize polymerides due to their different hydrophilicity levels, making it possible to control degradation and drug release. The above-mentioned block copolymers usually have the thermal properties of the two substances of which they are constituted. Copolymers formed by polyethylene oxide (PEO) and PLA have the same mechanical properties as those of the aforementioned ε-caprolactone and PLA copolymers. However, due to the addition of PEO, the hydrophilicity of this polymer is relatively high, which leads to accelerated hydrolyzation and molecular-weight degradation. Kimura also discovered that using polypropylene oxide instead of PEO makes it possible to obtain ABA block copolymers with higher molecular weights.

The above methods change the physical and rheological performance of PLA. The crosslinking method influences the thermal and rheological properties of the material without affecting its mechanical properties. The implementation of crosslinking is very easy; the multifunctional monomer can be added during the polymerization process. For example, when crosslinking with 5,5′-bis(oxepane-2-one) (bis(E-caprolactone), so that the PLA solvent swells less, the gel fraction is greater than 96%. Furthermore, a small amount of crosslinking agents also causes coagulation, and glue fractions greater than 80% can be used to produce impact-resistant machined products. Polymer free-radical recombination is another effective method for inducing crosslinking in polymers. The formation of free radicals by peroxides has proven to be an efficient and controllable way to produce different levels of crosslinked PLA [9].

As mentioned above, the polymer can be degraded by ordinary hydrolysis of the ester bond, without enzymes. The degraded hydrolysate is nontoxic and is metabolized in the human body, subsequently being eliminated from the body through urine. PLA has good biocompatibility and degradability, which has led to its being widely used in the medical field [61][62][63][64]. In addition to being used in sutures, PLA is a bioabsorbable material and is widely used in orthopedic surgery [32][65]. Fixed devices such as dissolvable suture nets and absorbable steel plates are good examples of its medical applications. Compared with traditional metal-steel plates, PLA does not corrode bones after being implanted in the human body. Because it can be absorbed into and degraded within the body, time and money are saved, while simultaneously reducing the need for secondary operations. PLA also has great potential as a drug-delivery carrier. It can effectively control the release of drugs at the lesion site and decrease the side effects caused by drug bursts; it can also be modified to accurately deliver drugs to lesion sites, reducing side effects and improving bioavailability. This undoubtedly provides a good platform for drug-delivery systems. In the next section, we focus on applying PLA in the biomedical field [66].

3. Application

Good biocompatibility is an important reason for the wide use of PLA in the field of biomedicine. The intermediate LA product can be metabolized by the human body and is nontoxic and harmless. Its degradation can be used for drug release. By controlling the metabolism rate of the carrier in the body, it is possible to ensure the effective concentration of the drug while reducing side effects, which gives it obvious advantages for use both in drug delivery and as a material for implants. Good biocompatibility also ensures that there is no inflammatory reaction in the surrounding tissue due to rejection after it enters the human body [67][68][69].

3.1. Tissue Engineering

Blood transfusions carry with them the danger of viral infection; for this reason, research into artificial blood has attracted a great deal of attention. The main component of blood is red blood cells, which transport oxygen [70][71][72][73]. Microcapsules can encapsulate animal hemoglobin [74][75]. Oxygen enters the microcapsule through the membrane wall and is combined with hemoglobin so that that the hemoglobin is able to transport oxygen. This method of embedding can also prevent animal hemoglobin from being produced in the blood. The antigen–antibody reaction extends the half-life. Some studies used liposomes to encapsulate hemoglobin. However, liposomes have a low entrapment rate and are unstable when entering the blood circulation. They easily release hemoglobin and have a short half-life [76][77][78]. Su et al. found that, when PLA was used as the membrane material, the embedding rate of hemoglobin was very low, only 7.9%. When using a PLA–PEG copolymer, the embedding rate reached 90%. Additionally, when preparing the microcapsules, since the inner and outer water phases are both aqueous solutions, the hydrophilic PEG block stretched toward both the inner and outer water phases. The PEG stretched toward the inner water phase was biocompatible. It had good properties and a certain protective effect on hemoglobin, and helped maintain protein activity during storage [79][80][81].

3.2. Drug Delivery

PLA can be degraded into LA and metabolized in the human body. It is a material approved by the FDA for biomedical use. In the 1970s, Yolles et al. used PLA for drug-delivery research, and prepared a PLA complex containing naltrexone. The in vitro release rate was 67% at 35 days. In vivo experiments proved that the complex had a blocking effect on morphine. Ruan et al. used PLA copolymers to prepare PLA–PEG–PLA microspheres containing paclitaxel [82][83]. The prepared microspheres were uniform in size and had a porous structure inside that promoted drug release. In vitro release reached 49% in one month, prolonging drug action time in the body and improving its efficacy. This sustained-release drug-delivery system avoids inconsistent local concentration due to drug release, thereby enhancing the therapeutic effect. Compared with traditional dosage forms, this slow-release "smart" drug-delivery system has many advantages: reducing the side effects of drugs on the gastrointestinal tract and avoiding high local drug concentrations within a given period, which may lead to allergies or even poisoning. Additionally, degradable materials can be degraded in specific environments, meaning that external polymer materials could be modified to achieve the controlled release of drugs [84][85][86].

For some specific diseases such as tumors and tuberculosis, therapeutic drugs can possess high toxicity and extensive side effects. In addition to the killing effect at the lesion site, they also cause great damage to normal tissue. At the same time, the process of treatment requires multiple and frequent administrations [87]. Therefore, targeted drug systems are worthy of study [88]. This kind of coating material, combined with target selection achieved through the affinity of the functional group, can quickly target the lesion site with the drug, improve its bioavailability, and reduce its toxic side effects and toxicity to other tissue types [89][90]. However, the polymer must be chemically modified to be more useful for targeting or eliciting a stimulatory response. As shown in Figure 3, a kind of pH sensitive linkage was designed to modify doxorubicin loaded PLA nanoparticles which make it easy to disintegrate in tumor microenvironment. Therefore, modified PLAs such as PLGA (Polylactoglycolic acid) are usually used in drug-delivery systems. Ferric oxide plays an important role in drug-delivery systems for magnetic nanoparticles. Fang et al. used PLGA to embed ferroferric oxide, and then encapsulated doxorubicin (DOX) inside to form a nanocomposite carrier. This carrier maintains high sensitivity to the external magnetic field, thus achieving magnetic targeting by the carrier. This nanoparticles also has good antitumor activity [91].

Figure 3. High drug loading and pH-responsivity PLA-g-doxorubicin (DOX) nanoparticles [91]. Reprinted from Cheng with permission from Express Polymer Letters.

3.3. Implants

Bone damage caused by natural disasters, traffic accidents, sports trauma, bone-tumor resection, congenital bone diseases, metabolic osteoporosis (OP). And a variety of bone repairs and fractures was a major issue that threatens human health [92][93][94][95]. The repair of bone damage caused by OP-induced fractures or other problems is a major problem in the 21st century [96][97][98][99]. In order to address this, scaffold materials based on the biomimetic human extracellular matrix (ECM) are considered to be the most promising biomedical materials for use in bone-tissue regeneration and repair. With respect to biological safety and the characteristics of metabolites, PLA is considered to be an advantageous material in comparison to copolymers such as PGA and polycaprolactone [100][101]. Although the properties of PLA are not perfect, by blending it with hydroxy phosphate lime (HA), the scaffold can be given osteoinduction and bone conduction properties. Additionally, the elastic modulus of the scaffold can be improved. Quirk et al. used the adsorption method to incorporate RGD-immobilized polylysine into PLA. All of these physical modification methods are unstable when compared to the chemical modification of biologically active factors [102]. Therefore, with a view towards the long-term application of tissue-engineering materials, chemical modification methods have attracted a great deal of attention. Some researchers used PEG, PGA, and PLA to copolymerize and improve the biological functionality of PLA. By copolymerizing lactide and lecithin, Iwasaki successfully introduced the phospholipid choline molecule (MPC), a cell-active biological membrane component, into the PLA structure. Results showed that the phospholipid choline molecule reduced protein adsorption and platelet adhesion on the material surface. The addition of phospholipid choline molecules inhibited the adhesion of white blood cells. Yasuhiko's award-winning phospholipid choline molecule was copolymerized with 2-ethylhexyl acrylic acid (EHMA) and then blended with PLGA, reducing the inflammatory response of the material. Junji et al. copolymerized MPC-containing double bonds with n-butyl methyl methacrylate and PLA. The amount of protein adhesion on the surface of the material was reduced, which enhanced the adhesion of cells and materials. Adjusting MPC and PLA makes it possible to control the adhesive growth ability of cells. Therefore, the biomimetic modified PLA materials described above effectively improve biocompatibility and impart new biological activities to the material, which can be useful for broadening the applicability of PLA biomedical materials for use in implanting medical devices in the body, especially with respect to built-in devices with good blood compatibility. This is of significant scientific importance, and possesses great value. Drug-eluting stents are currently available on the market for clinical applications. Drugs are adsorbed onto the stent. Several medical device companies developed PLA-based stents and put them into production [103][104]. Nowadays, 3D-printed biodegradable scaffolds have good biocompatibility, and promote angiogenesis and osteogenesis, thereby benefiting bone development and reconstruction. Some studies evaluated PLA scaffolds made using 3D-printing technology, finding that it results in less inflammation, making it a promising material for repairing bone damage [105][106].

4. Conclusions

Completely degradable PLA material solves the white-pollution problem caused by petroleum-based materials, and has become the top priority in the sustainable development of science and technology. Because PLA has  disadvantages such as brittleness, poor mechanical properties, slow crystallization speed, and low crystallinity, it is severely restricted in many aspects, especially with respect to blown films. In order to overcome the shortcomings of PLA, scientists modified it using physical or chemical methods and prepared a series of ideal materials with good biodegradability, flexibility, and heat resistance. Along with its low price, promising research results in this area have guaranteed and expanded the application of PLA in many fields, providing a platform for production and manufacturing in the fields of industry, 3D printing, advanced technology, and the biomedical field.

Stents based on PLA have been commercialized. However, its application in drug delivery still faces great challenges in the field of biomedicine. Although there have been many studies using PLA to synthesize nanocarriers for the treatment of tumors and other diseases, none of the nanoparticle has been successfully marketed in actual production. Side effects and toxicity are essential in this field among the many reasons for this phenomenon. The size, position and shape of the nanoparticles are all important features, and positively charged nanoparticles can cause certain cytotoxicity, oxidative stress, and even DNA damage. The excessive of reactive oxygen species (ROS) can cause local inflammation. In addition, hemolysis tests are required before nanoparticles are tested in vivo, as slight red blood cell damage may be caused by PLA nanoparticles. The microenvironment of the disease site is complex. For example, the pH levels in tumors and inflammation sites are often lower than normal. Some researchers used this feature to modify PLA. Nanoparticles prepared with PEG–PLA are stable in a neutral environment, but their degradation is accelerated in an acid environment. Thus, the role of targeted drug delivery is realized. However, such seemingly ideal nanoparticles are difficult to achieve in vivo for the complex environment of blood makes nanoparticles facing huge challenges. Brittle nanoparticles will be destroyed by enzymes after entering the blood circulation, or electromagnetically adsorbed and aggregated with proteins, which will trigger immune rejection. Therefore, commercialization of polymer nanoparticles and their application to the human body still face great challenges.

In the process of commercialization of PLA, the price is a key issue to be solved. To solve the problem of the price of PLA, it is necessary to start with the production of raw materials by improving the production efficiency of lactic acid and obtaining high-quality LA at low cost. A further improvement in the production process of LA is required due to the low-cost materials and high-performance microorganisms. It can be seen that the optimization of the production process of LA is also a challenge for the bulk production of PLA.


  1. Siracusa, V.; Rocculi, P.; Romani, S.; Dalla Rosa, M. Biodegradable polymers for food packaging: A review. Trends Food Sci. Technol. 2008, 19, 634–643.
  2. Mohanty, A.K.; Misra, M.; Hinrichsen, G. Biofibres, biodegradable polymers and biocomposites: An overview. Macromol. Mater. Eng. 2000, 276, 1–24.
  3. Bordes, P.; Pollet, E.; Averous, L. Nano-biocomposites: Biodegradable polyester/nanoclay systems. Prog. Polym. Sci. 2009, 34, 125–155.
  4. Adsul, M.G.; Varma, A.J.; Gokhale, D.V. Lactic acid production from waste sugarcane bagasse derived cellulose. Green Chem. 2007, 9, 58–62.
  5. Singhvi, M.; Joshi, D.; Adsul, M.; Varma, A.; Gokhale, D. D-(−)-Lactic acid production from cellobiose and cellulose by Lactobacillus lactis mutant RM2-24. Green Chem. 2010, 12, 1106–1109.
  6. Abdel-Rahman, M.A.; Tashiro, Y.; Zendo, T.; Sonomoto, K. Improved lactic acid productivity by an open repeated batch fermentation system using Enterococcus mundtii QU 25. RSC Adv. 2013, 3, 8437–8445.
  7. Abdel-Rahman, M.A.; Tashiro, Y.; Sonomoto, K. Lactic acid production from lignocellulose-derived sugars using lactic acid bacteria: Overview and limits. J. Biotechnol. 2011, 156, 286–301.
  8. Abdel-Rahman, M.A.; Sonomoto, K. Opportunities to overcome the current limitations and challenges for efficient microbial production of optically pure lactic acid. J. Biotechnol. 2016, 236, 176–192.
  9. Chen, C.C.; Chueh, J.Y.; Tseng, H.; Huang, H.M.; Lee, S.Y. Preparation and characterization of biodegradable PLA polymeric blends. Biomaterials 2003, 24, 1167–1173.
  10. Martin, O.; Averous, L. Poly (lactic acid): Plasticization and properties of biodegradable multiphase systems. Polymer 2001, 42, 6209–6219.
  11. John, R.P.; Anisha, G.S.; Nampoothiri, K.M.; Pandey, A. Direct lactic acid fermentation: Focus on simultaneous saccharification and lactic acid production. Biotechnol. Adv. 2009, 27, 145–152.
  12. Gupta, B.; Revagade, N.; Hilborn, J. Poly (lactic acid) fiber: An overview. Prog. Polym. Sci. 2007, 32, 455–482.
  13. Graupner, N.; Herrmann, A.S.; Muessig, J. Natural and man-made cellulose fibre-reinforced poly(lactic acid) (PLA) composites: An overview about mechanical characteristics and application areas. Compos. Part. A-Appl. Sci. Manuf. 2009, 40, 810–821.
  14. Dutkiewicz, S.; Grochowska-Lapienis, D.; Tomaszewski, W. Synthesis of poly(L(+) lactic acid) by polycondensation method in solution. Fibres Text. East. Eur. 2003, 11, 66–70.
  15. Anakhu, P.I.; Bolu, C.C.; Abioye, A.A.; Onyiagha, G.; Boyo, H.; Jolayemi, K.; Azeta, J. Innovative Foundry Technology and Material Using Fused Deposition Modeling and Polylactic Acid Material in Sand Casing. Arch. Foundry Eng. 2018, 18, 65–71.
  16. Deng, K.; Chen, H.; Zhao, Y.; Zhou, Y.; Wang, Y.; Sun, Y. Evaluation of adaptation of the polylactic acid pattern of maxillary complete dentures fabricated by fused deposition modelling technology: A pilot study. PloS ONE 2018, 13, e0201777.
  17. Liu, Z.; Wang, Y.; Wu, B.; Cui, C.; Guo, Y.; Yan, C. A critical review of fused deposition modeling 3D printing technology in manufacturing polylactic acid parts. Int. J. Adv. Manuf. Technol. 2019, 102, 2877–2889.
  18. Shao, W.; He, J.; Han, Q.; Sang, F.; Wang, Q.; Chen, L.; Cui, S.; Ding, B. A biomimetic multilayer nanofiber fabric fabricated by electrospinning and textile technology from polylactic acid and Tussah silk fibroin as a scaffold for bone tissue engineering. Mater. Sci. Eng. C-Mater. Biol. Appl. 2016, 67, 599–610.
  19. Tsukegi, T.; Nagasawa, N.; Horii, T.; Nishida, H. Chemical Recycling Technology of Polylactic Acid/talc-Application into Agricultural Materials. Kobunshi Ronbunshu 2015, 72, 361–368.
  20. Varadarajan, S.; Miller, D.J. Catalytic upgrading of fermentation-derived organic acids. Biotechnol. Prog. 1999, 15, 845–854.
  21. Chanfreau, S.; Mena, M.; Porras-Dominguez, J.R.; Ramirez-Gilly, M.; Gimeno, M.; Roquero, P.; Tecante, A.; Barzana, E. Enzymatic synthesis of poly-L-lactide and poly-L-lactide-co-glycolide in an ionic liquid. Bioprocess. Biosyst. Eng. 2010, 33, 629–638.
  22. Gupta, A.P.; Kumar, V. New emerging trends in synthetic biodegradable polymers-Polylactide: A critique. Eur. Polym. J. 2007, 43, 4053–4074.
  23. Yao, K.; Tang, C. Controlled Polymerization of Next-Generation Renewable Monomers and Beyond. Macromolecules 2013, 46, 1689–1712.
  24. Fukushima, K.; Kimura, Y. An efficient solid-state polycondensation method for synthesizing stereocomplexed poly (lactic acid)s with high molecular weight. J. Polym. Sci. Part. A-Polym. Chem. 2008, 46, 3714–3722.
  25. Bud, R. A history of lactic-acid making-a chapter in the history of biotechnology-benninga,h. Ann. Sci. 1993, 50, 597–597.
  26. Lampe, K.J.; Namba, R.M.; Silverman, T.R.; Bjugstad, K.B.; Mahoney, M.J. Impact of Lactic Acid on Cell Proliferation and Free Radical-Induced Cell Death in Monolayer Cultures of Neural Precursor Cells. Biotechnol. Bioeng. 2009, 103, 1214–1223.
  27. Athanasiou, K.A.; Niederauer, G.G.; Agrawal, C.M. Sterilization, toxicity, biocompatibility and clinical applications of polylactic acid/polyglycolic acid copolymers. Biomaterials 1996, 17, 93–102.
  28. Auras, R.; Harte, B.; Selke, S. An overview of polylactides as packaging materials. Macromol. Biosci. 2004, 4, 835–864.
  29. Nampoothiri, K.M.; Nair, N.R.; John, R.P. An overview of the recent developments in polylactide (PLA) research. Bioresour. Technol. 2010, 101, 8493–8501.
  30. Chamberlain, B.M.; Cheng, M.; Moore, D.R.; Ovitt, T.M.; Lobkovsky, E.B.; Coates, G.W. Polymerization of lactide with zinc and magnesium beta-diiminate complexes: Stereocontrol and mechanism. J. Am. Chem. Soc. 2001, 123, 3229–3238.
  31. Oksman, K.; Skrifvars, M.; Selin, J.F. Natural fibres as reinforcement in polylactic acid (PLA) composites. Compos. Sci. Technol. 2003, 63, 1317–1324.
  32. Tsuji, H. Poly (lactide) stereocomplexes: Formation, structure, properties, degradation, and applications. Macromol. Biosci. 2005, 5, 569–597.
  33. Peres, C.; Matos, A.I.; Conniot, J.; Sainz, V.; Zupancic, E.; Silva, J.M.; Graca, L.; Gaspar, R.S.; Preat, V.; Florindo, H.F. Poly (lactic acid)-based particulate systems are promising tools for immune modulation. Acta Biomater. 2017, 48, 41–57.
  34. Nicolas, J.; Mura, S.; Brambilla, D.; Mackiewicz, N.; Couvreur, P. Design, functionalization strategies and biomedical applications of targeted biodegradable/biocompatible polymer-based nanocarriers for drug delivery. Chem. Soc. Rev. 2013, 42, 1147–1235.
  35. Discher, D.E.; Ahmed, F. Polymersomes. Annu. Rev. Biomed. Eng. 2006, 8, 323–341.
  36. Saeidlou, S.; Huneault, M.A.; Li, H.; Park, C.B. Poly (lactic acid) crystallization. Prog. Polym. Sci. 2012, 37, 1657–1677.
  37. Inkinen, S.; Hakkarainen, M.; Albertsson, A.-C.; Sodergard, A. From Lactic Acid to Poly(lactic acid) (PLA): Characterization and Analysis of PLA and Its Precursors. Biomacromolecules 2011, 12, 523–532.
  38. Suryanegara, L.; Nakagaito, A.N.; Yano, H. The effect of crystallization of PLA on the thermal and mechanical properties of microfibrillated cellulose-reinforced PLA composites. Compos. Sci. Technol. 2009, 69, 1187–1192.
  39. Carrasco, F.; Pages, P.; Gamez-Perez, J.; Santana, O.O.; Maspoch, M.L. Processing of poly (lactic acid): Characterization of chemical structure, thermal stability and mechanical properties. Polym. Degrad. Stab. 2010, 95, 116–125.
  40. Fortunati, E.; Armentano, I.; Zhou, Q.; Iannoni, A.; Saino, E.; Visai, L.; Berglund, L.A.; Kenny, J.M. Multifunctional bionanocomposite films of poly (lactic acid), cellulose nanocrystals and silver nanoparticles. Carbohydr. Polym. 2012, 87, 1596–1605.
  41. Vasir, J.K.; Labhasetwar, V. Biodegradable nanoparticles for cytosolic delivery of therapeutics. Adv. Drug Deliv. Rev. 2007, 59, 718–728.
  42. Li, H.; Huneault, M.A. Effect of nucleation and plasticization on the crystallization of poly (lactic acid). Polymer 2007, 48, 6855–6866.
  43. Liu, H.; Zhang, J. Research Progress in Toughening Modification of Poly (lactic acid). J. Polym. Sci. Part. B-Polym. Phys. 2011, 49, 1051–1083.
  44. Huda, M.S.; Drzal, L.T.; Mohanty, A.K.; Misra, M. Effect of fiber surface-treatments on the properties of laminated biocomposites from poly (lactic acid) (PLA) and kenaf fibers. Compos. Sci. Technol. 2008, 68, 424–432.
  45. Abdel-Rahman, M.A.; Tashiro, Y.; Sonomoto, K. Recent advances in lactic acid production by microbial fermentation processes. Biotechnol. Adv. 2013, 31, 877–902.
  46. Agarwal, M.; Koelling, K.W.; Chalmers, J.J. Characterization of the degradation of polylactic acid polymer in a solid substrate environment. Biotechnol. Prog. 1998, 14, 517–526.
  47. Gritsch, L.; Conoscenti, G.; La Carrubba, V.; Nooeaid, P.; Boccaccini, A.R. Polylactide-based materials science strategies to improve tissue-material interface without the use of growth factors or other biological molecules. Mater. Sci. Eng. C-Mater. Biol. Appl. 2019, 94, 1083–1101.
  48. Codari, F.; Lazzari, S.; Soos, M.; Storti, G.; Morbidelli, M.; Moscatelli, D. Kinetics of the hydrolytic degradation of poly (lactic acid). Polym. Degrad. Stab. 2012, 97, 2460–2466.
  49. de Jong, S.J.; Arias, E.R.; Rijkers, D.T.S.; van Nostrum, C.F.; Kettenes-van den Bosch, J.J.; Hennink, W.E. New insights into the hydrolytic degradation of poly (lactic acid): Participation of the alcohol terminus. Polymer 2001, 42, 2795–2802.
  50. Zalusky, A.S.; Olayo-Valles, R.; Wolf, J.H.; Hillmyer, M.A. Ordered nanoporous polymers from polystyrene-polylactide block copolymers. J. Am. Chem. Soc. 2002, 124, 12761–12773.
  51. Agrawal, C.M.; Athanasiou, K.A. Technique to control pH in vicinity of biodegrading PLA-PGA implants. J. Biomed. Mater. Res. 1997, 38, 105–114.
  52. Ray, S.S.; Okamoto, M. Biodegradable polylactide and its nanocomposites: Opening a new dimension for plastics and composites. Macromol. Rapid Commun. 2003, 24, 815–840.
  53. Vaz, C.M.; van Tuijl, S.; Bouten, C.V.C.; Baaijens, F.P.T. Design of scaffolds for blood vessel tissue engineering using a multi-layering electrospinning technique. Acta Biomater. 2005, 1, 575–582.
  54. Luckachan, G.E.; Pillai, C.K.S. Biodegradable Polymers-A Review on Recent Trends and Emerging Perspectives. J. Polym. Environ. 2011, 19, 637–676.
  55. Sodergard, A.; Stolt, M. Properties of lactic acid based polymers and their correlation with composition. Prog. Polym. Sci. 2002, 27, 1123–1163.
  56. Maiti, P.; Yamada, K.; Okamoto, M.; Ueda, K.; Okamoto, K. New polylactide/layered silicate nanocomposites: Role of organoclays. Chem. Mater. 2002, 14, 4654–4661.
  57. Paul, M.A.; Alexandre, M.; Degee, P.; Henrist, C.; Rulmont, A.; Dubois, P. New nanocomposite materials based on plasticized poly (L-lactide) and organo-modified montmorillonites: Thermal and morphological study. Polymer 2003, 44, 443–450.
  58. Paul, M.A.; Delcourt, C.; Alexandre, M.; Degee, P.; Monteverde, F.; Rulmont, A.; Dubois, P. (Plasticized) polylactide/(organo-)clay nanocomposites by in situ intercalative polymerization. Macromol. Chem. Phys. 2005, 206, 484–498.
  59. Pluta, M.; Paul, M.A.; Alexandre, M.; Dubois, P. Plasticized polylactide/clay nanocomposites. I. The role of filler content and its surface organo-modification on the physico-chemical properties. J. Polym. Sci. Part. B-Polym. Phys. 2006, 44, 299–311.
  60. Tanoue, S.; Hasook, A.; Iemoto, Y.; Unryu, T. Preparation of poly (lactic acid)/poly(ethylene glycol)/organoclay nanocomposites by melt compounding. Polym. Compos. 2006, 27, 256–263.
  61. Lasprilla, A.J.R.; Martinez, G.A.R.; Lunelli, B.H.; Jardini, A.L.; Maciel Filho, R. Poly-lactic acid synthesis for application in biomedical devices-A review. Biotechnol. Adv. 2012, 30, 321–328.
  62. Kim, Y.; Dalhaimer, P.; Christian, D.A.; Discher, D.E. Polymeric worm micelles as nano-carriers for drug delivery. Nanotechnology 2005, 16, S484–S491.
  63. Pluta, M.; Paul, M.A.; Alexandre, M.; Dubois, P. Plasticized polylactide/clay nanocomposites. II. The effect of aging on structure and properties in relation to the filler content and the nature of its organo-modification. J. Polym. Sci. Part. B-Polym. Phys. 2006, 44, 312–325.
  64. Shasteen, C.; Choy, Y.B. Controlling Degradation Rate of Poly (lactic acid) for Its Biomedical Applications. Biomed. Eng. Lett. 2011, 1, 163–167.
  65. Vieira, A.C.; Guedes, R.M.; Tita, V. Damage-induced hydrolyses modelling of biodegradable polymers for tendons and ligaments repair. J. Biomech. 2015, 48, 3478–3485.
  66. Grande, R.; Carvalho, A.J.F. Compatible Ternary Blends of Chitosan/poly (vinyl alcohol)/poly(lactic acid) Produced by Oil-in-Water Emulsion Processing. Biomacromolecules 2011, 12, 907–914.
  67. Mitragotri, S.; Burke, P.A.; Langer, R. Overcoming the challenges in administering biopharmaceuticals: Formulation and delivery strategies. Nat. Rev. Drug Discov. 2014, 13, 655–672.
  68. Nottelet, B.; Darcos, V.; Coudane, J. Aliphatic polyesters for medical imaging and theranostic applications. Eur. J. Pharm. Biopharm. 2015, 97, 350–370.
  69. Tan, D.S. Diversity-oriented synthesis: Exploring the intersections between chemistry and biology. Nat. Chem. Biol. 2005, 1, 74–84.
  70. Aggarwal, P.; Hall, J.B.; McLeland, C.B.; Dobrovolskaia, M.A.; McNeil, S.E. Nanoparticle interaction with plasma proteins as it relates to particle biodistribution, biocompatibility and therapeutic efficacy. Adv. Drug Deliv. Rev. 2009, 61, 428–437.
  71. Weiss, G.; Goodnough, L.T. Medical progress: Anemia of chronic disease. New Engl. J. Med. 2005, 352, 1011–1023.
  72. Moghimi, S.M.; Hunter, A.C.; Murray, J.C. Long-circulating and target-specific nanoparticles: Theory to practice. Pharmacol. Rev. 2001, 53, 283–318.
  73. Hebert, P.C.; Wells, G.; Blajchman, M.A.; Marshall, J.; Martin, C.; Pagliarello, G.; Tweeddale, M.; Schweitzer, I.; Yetisir, E.; Canadian Critical Care Trials, G. A multicenter, randomized, controlled clinical trial of transfusion requirements in critical care. New Engl. J. Med. 1999, 340, 409–417.
  74. Chang, T.M.S. From artificial red blood cells, oxygen carriers, and oxygen therapeutics to artificial cells, nanomedicine, and beyond. Artif. Cells Blood Substit. Biotechnol. 2012, 40, 197–199.
  75. Chang, T.M.S.; Powanda, D. Analysis of polyethylene-glycol-polylactide nano-dimension artificial red blood cells in maintaining systemic hemoglobin levels and prevention of methemoglobin formation. Artif. Cells Blood Substit. Immobil. Biotechnol. 2003, 31, 231–247.
  76. Levi, M.; Friederich, P.W.; Middleton, S.; de Groot, P.G.; Wu, Y.P.; Harris, R.; Biemond, B.J.; Heijnen, H.F.G.; Levin, J.; ten Cate, J.W. Fibrinogen-coated albumin microcapsules reduce bleeding in severely thrombocytopenic rabbits. Nat. Med. 1999, 5, 107–111.
  77. Mansouri, S.; Fatisson, J.; Miao, Z.; Merhi, Y.; Winnik, F.M.; Tabrizian, M. Silencing Red Blood Cell Recognition toward Anti-A Antibody by Means of Polyelectrolyte Layer-by-Layer Assembly in a Two-Dimensional Model System. Langmuir 2009, 25, 14071–14078.
  78. Mansouri, S.; Merhi, Y.; Winnik, F.M.; Tabrizian, M. Investigation of Layer-by-Layer Assembly of Polyelectrolytes on Fully Functional Human Red Blood Cells in Suspension for Attenuated Immune Response. Biomacromolecules 2011, 12, 585–592.
  79. Waring, M.J.; Arrowsmith, J.; Leach, A.R.; Leeson, P.D.; Mandrell, S.; Owen, R.M.; Pairaudeau, G.; Pennie, W.D.; Pickett, S.D.; Wang, J.; et al. An analysis of the attrition of drug candidates from four major pharmaceutical companies. Nat. Rev. Drug Discov. 2015, 14, 475–486.
  80. Langer, R.; Vacanti, J.P. Tissue engineering. Science 1993, 260, 920–926.
  81. Zhang, Y.; Sophocleous, A.M.; Schwendeman, S.P. Inhibition of Peptide Acylation in PLGA Microspheres with Water-soluble Divalent Cationic Salts. Pharm. Res. 2009, 26, 1986–1994.
  82. Dong, Y.; Feng, S.-S. Nanoparticles of poly(D,L-lactide)/methoxy poly(ethylene glycol)-poly(D,L-lactide) blends for controlled release of paclitaxel. J. Biomed. Mater. Res. Part. A 2006, 78, 12–19.
  83. Pan, J.; Feng, S.-S. Targeted delivery of paclitaxel using folate-decorated poly(lactide)-vitamin E TPGS nanoparticles. Biomaterials 2008, 29, 2663–2672.
  84. Betancourt, T.; Byrne, J.D.; Sunaryo, N.; Crowder, S.W.; Kadapakkam, M.; Patel, S.; Casciato, S.; Brannon-Peppas, L. PEGylation strategies for active targeting of PLA/PLGA nanoparticles. J. Biomed. Mater. Res. Part. A 2009, 91, 263–276.
  85. Gref, R.; Minamitake, Y.; Peracchia, M.T.; Trubetskoy, V.; Torchilin, V.; Langer, R. Biodegradable long-circulating polymeric nanospheres. Science 1994, 263, 1600–1603.
  86. Italia, J.L.; Bhardwaj, V.; Kumar, M.N.V.R. Disease, destination, dose and delivery aspects of ciclosporin: The state of the art. Drug Discov. Today 2006, 11, 846–854.
  87. Zhao, J.; Mi, Y.; Liu, Y.; Feng, S.-S. Quantitative control of targeting effect of anticancer drugs formulated by ligand-conjugated nanoparticles of biodegradable copolymer blend. Biomaterials 2012, 33, 1948–1958.
  88. Cheng, C.J.; Tietjen, G.T.; Saucier-Sawyer, J.K.; Saltzman, W.M. A holistic approach to targeting disease with polymeric nanoparticles. Nat. Rev. Drug Discov. 2015, 14, 239–247.
  89. Kamaly, N.; Xiao, Z.; Valencia, P.M.; Radovic-Moreno, A.F.; Farokhzad, O.C. Targeted polymeric therapeutic nanoparticles: Design, development and clinical translation. Chem. Soc. Rev. 2012, 41, 2971–3010.
  90. Mura, S.; Nicolas, J.; Couvreur, P. Stimuli-responsive nanocarriers for drug delivery. Nat. Mater. 2013, 12, 991–1003.
  91. Yu, Y.; Chen, C.-K.; Law, W.-C.; Weinheimer, E.; Sengupta, S.; Prasad, P.N.; Cheng, C. Polylactide-graft-doxorubicin Nanoparticles with Precisely Controlled Drug Loading for pH-Triggered Drug Delivery. Biomacromolecules 2014, 15, 524–532.
  92. Cummings, S.R.; San Martin, J.; McClung, M.R.; Siris, E.S.; Eastell, R.; Reid, I.R.; Delmas, P.; Zoog, H.B.; Austin, M.; Wang, A.; et al. Denosumab for Prevention of Fractures in Postmenopausal Women with Osteoporosis. New Engl. J. Med. 2009, 361, 756–765.
  93. Harris, S.T.; Watts, N.B.; Genant, H.K.; McKeever, C.D.; Hangartner, T.; Keller, M.; Chesnut, C.H.; Brown, J.; Eriksen, E.F.; Hoseyni, M.S.; et al. Effects of risedronate treatment on vertebral and nonvertebral fractures in women with postmenopausal osteoporosis - A randomized controlled trial. Jama-J. Am. Med. Assoc. 1999, 282, 1344–1352.
  94. Liberman, U.A.; Weiss, S.R.; Broll, J.; Minne, H.W.; Quan, H.; Bell, N.H.; Rodriguez-Portales, J.; Downs, R.W. Jr.; Dequeker, J.; Favus, M. Effect of oral alendronate on bone mineral density and the incidence of fractures in postmenopausal osteoporosis. The Alendronate Phase III Osteoporosis Treatment Study Group. New Engl. J. Med. 1995, 333, 1437–1443.
  95. Scalbert, A.; Manach, C.; Morand, C.; Remesy, C.; Jimenez, L. Dietary polyphenols and the prevention of diseases. Crit. Rev. Food Sci. Nutr. 2005, 45, 287–306.
  96. Hamad, K.; Kaseem, M.; Yang, H.W.; Deri, F.; Ko, Y.G. Properties and medical applications of polylactic acid: A review. Express Polym. Lett. 2015, 9, 435–455.
  97. Yu, L.; Dean, K.; Li, L. Polymer blends and composites from renewable resources. Prog. Polym. Sci. 2006, 31, 576–602.
  98. Manolagas, S.C. Birth and death of bone cells: Basic regulatory mechanisms and implications for the pathogenesis and treatment of osteoporosis. Endocr. Rev. 2000, 21, 115–137.
  99. Pandey, K.B.; Rizvi, S.I. Plant polyphenols as dietary antioxidants in human health and disease. Oxidative Med. Cell. Longev. 2009, 2, 270–278.
  100. Garg, S.; Bourantas, C.; Serruys, P.W. New concepts in the design of drug-eluting coronary stents. Nat. Rev. Cardiol. 2013, 10, 248–260.
  101. Gollwitzer, H.; Thomas, P.; Diehl, P.; Steinhauser, E.; Summer, B.; Barnstorf, S.; Gerdesmeyer, L.; Mittelmeier, W.; Stemberger, A. Biomechanical and allergological characteristics of a biodegradable poly(D,L-lactic acid) coating for orthopaedic implants. J. Orthop. Res. 2005, 23, 802–809.
  102. Manavitehrani, I.; Fathi, A.; Wang, Y.; Maitz, P.K.; Mirmohseni, F.; Cheng, T.L.; Peacock, L.; Little, D.G.; Schindeler, A.; Dehghani, F. Fabrication of a Biodegradable Implant with Tunable Characteristics for Bone Implant Applications. Biomacromolecules 2017, 18, 1736–1746.
  103. Mc Conville, C.; Major, I.; Friend, D.R.; Clark, M.R.; Woolfson, A.D.; Malcolm, R.K. Development of polylactide and polyethylene vinyl acetate blends for the manufacture of vaginal rings. J. Biomed. Mater. Res. Part. B-Appl. Biomater. 2012, 100, 891–895.
  104. Wehmoeller, M.; Neuking, K.; Epple, M.; Annen, T.; Eufinger, H. Mechanical characteristics of functionally graded biodegradable implants for skull bone reconstruction. Mater. Und Werkst. 2006, 37, 413–415.
  105. Yan, Y.; Chen, H.; Zhang, H.; Guo, C.; Yang, K.; Chen, K.; Cheng, R.; Qian, N.; Sandler, N.; Zhang, Y.S.; et al. Vascularized 3D printed scaffolds for promoting bone regeneration. Biomaterials 2019, 190, 97–110.
  106. Zhang, H.; Mao, X.; Du, Z.; Jiang, W.; Han, X.; Zhao, D.; Han, D.; Li, Q. Three dimensional printed macroporous polylactic acid/hydroxyapatite composite scaffolds for promoting bone formation in a critical-size rat calvarial defect model. Sci. Technol. Adv. Mater. 2016, 17, 136–148.
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