Degradable,microporous vascular prosthesis from segmented polyurethane

Small caliber (1.5 mm I. D.) vascular prostheses have been prepared from fractionated segmented polyurethane.The microporous and compliant prosthesis when implanted in the abdominal aorta of the rat, induced the growth of a neo-conduit, with a cellular structure similar to that of the natural artery. The process of growth of the neo-artery was accompanied by a progressive degradation of the prosthesis.Presented in part at the 11th Annual Meeting of the European Society of Artificial Organs, Alpbach-Innsbruck, September 1984.     

Hollow giant lipid vesicles prepared by coaxially electrospraying solutions of phospholipid and degradable polyelectrolyte

Hollow giant lipid vesicles were prepared in a single step by coaxially electrospraying separate solutions of phospholipid and a degradable polyelectrolyte. We synthesized a hydrolytically degradable cationic polyelectrolyte, poly(β-amino esters) (PBAE), and employed it as a degradable microgel template to form giant vesicles. Droplets of the phospholipid solution and the degradable polyelectrolyte solution were electrosprayed from coaxial double needles into a receiving solution. The PBAE formed a microgel by crosslinking with multivalent anions in the receiving solution, and the phospholipids formed bilayers on the microgel. Hollow giant lipid vesicles were successfully obtained and the mean diameters were 7.6 μm (C.V. 58 %). Substrates (calcein, dextran, and polymeric microparticles) were successfully encapsulated in the giant vesicles. Microscopic observations of microparticle mobility inside a giant vesicle indicated the fluidity of its aqueous interior. Investigations using fluorescently labeled PBAE also suggested the degradation of PBAE, and the release of fluorescent PBAE fragments from the encapsulated microgel, to form hollow giant lipid vesicles.     

Shape Memory Properties and Enzymatic Degradability of Poly(ε‐caprolactone)‐Based Polyurethane Urea Containing Phenylalanine‐Derived Chain Extender

Biodegradable shape memory polymers are promising biomaterials for minimally invasive surgical procedures. Herein, a series of linear biodegradable shape memory poly(ε‐caprolactone) (PCL)‐based polyurethane ureas (PUUs) containing a novel phenylalanine‐derived chain extender is synthesized. The phenylalanine‐derived chain extender, phenylalanine‐hexamethylenediamine‐phenylalanine (PHP), contains two chymotrypsin cleaving sites to enhance the enzymatic degradation of PUUs. The degradation rate, the crystallinity, and mechanical properties of PUUs are tailored by the content of PHP. Meanwhile, semicrystalline PCL is not only hydrolytically degradable but also vital for shape memory. Good shape memory ability under body temperature is achieved for PUUs due to the strong interactions in hard segments for permanent crosslinking and the crystallization‐melt transition of PCL to switch temporary shape. The PUUs would have a great potential in application as implanting stent.     

Polyurethane microporous membranes as pericardial substitutes

Pericardial substitutes were prepared from stable and degradable segmented polyurethanes and/or polyurethane/polyhydroxybutyrate composites.Polyurethane membranes implanted as pericardial substitute in the rabbit, did not activate adhesion and epicardial reaction over 3 months.Polyurethane/polyhydroxybutyrate membranes induced minimal adhesion or epicardial reaction, yet stimulated the growth of epithelium on the polymeric substrate and reduced the incidence of infection.     

Dual functional polyelectrolyte multilayer coatings for implants: permanent microbicidal base with controlled release of therapeutic agents

Here we present a new bifunctional layer-by-layer (LbL) construct made by combining a permanent microbicidal polyelectrolyte multilayered (PEM) base film with a hydrolytically degradable PEM top film that offers controlled and localized delivery of therapeutics. Two degradable film architectures are presented: (1) bolus release of an antibiotic (gentamicin) to eradicate initial infection at the implant site, or (2) sustained delivery of an anti-inflammatory drug (diclofenac) to cope with inflammation at the site of implantation due to tissue injury. Each degradable film was built on top of a permanent base film that imparts the implantable device surface with microbicidal functionality that prevents the formation of biofilms. Controlled-delivery of gentamicin was demonstrated over hours and that of diclofenac over days. Both drugs retained their efficacy upon release. The permanent microbicidal base film was biocompatible with A549 epithelial cancer cells and MC3T3-E1 osteoprogenitor cells, while also preventing bacteria attachment from turbid media for the entire duration of the two weeks studied. The microbicidal base film retains its functionality after the biodegradable films have completely degraded. The versatility of these PEM films and their ability to prevent biofilm formation make them attractive as coatings for implantable devices.     

Erosion of multilayered films fabricated from degradable polyamines: Characterization and evidence in support of a mechanism that involves polymer hydrolysis

Multilayered polyelectrolyte assemblies fabricated using hydrolytically degradable polyamines ( 1 – 3 ) erode gradually when incubated in physiologically relevant media. This investigation sought to characterize physically and chemically the erosion of films fabricated from these polymers and sodium poly(styrene sulfonate) (SPS) and to investigate specifically the potential role of polymer hydrolysis in governing film erosion. The characterization of erosion using reflective infrared spectroscopy revealed changes in the carbonyl region of the spectrum that were consistent with the generation of polymer hydrolysis products. To evaluate the role of the esters in these materials more directly, we also synthesized a structural analogue of polymer 2 containing amide functionality rather than ester functionality. Assemblies fabricated from this amide-containing polymer did not erode significantly or release SPS into solution when incubated in phosphate-buffered saline (PBS). Finally, we characterized the erosion of assemblies fabricated from polymer 1 in PBS buffer prepared with D₂O rather than H₂O. These assemblies eroded significantly more slowly in deuterated media than in buffer prepared with H₂O. These results, when combined, provide support for the view that polymer hydrolysis plays an important role in governing the erosion of assemblies fabricated from these degradable polymers. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 44: 5161–5173, 2006     

Backbone‐Degradable Polymers Prepared by Chemical Vapor Deposition

Polymers prepared by chemical vapor deposition (CVD) polymerization have found broad acceptance in research and industrial applications. However, their intrinsic lack of degradability has limited wider applicability in many areas, such as biomedical devices or regenerative medicine. Herein, we demonstrate, for the first time, a backbone‐degradable polymer directly synthesized via CVD. The CVD co‐polymerization of [2.2]para ‐cyclophanes with cyclic ketene acetals, specifically 5,6‐benzo‐2‐methylene‐1,3‐dioxepane (BMDO), results in well‐defined, hydrolytically degradable polymers, as confirmed by FTIR spectroscopy and ellipsometry. The degradation kinetics are dependent on the ratio of ketene acetals to [2.2]para ‐cyclophanes as well as the hydrophobicity of the films. These coatings address an unmet need in the biomedical polymer field, as they provide access to a wide range of reactive polymer coatings that combine interfacial multifunctionality with degradability.     

Thiophosphate/Phosphonate‐Containing Cross‐Linked PEGs and Their Use for the Stabilization of Silver Nanoparticles

A simple strategy was developed to obtain poly(ethylene glycol) (PEG)‐based materials incorporating phosphonate functions and thiophosphate groups from readily accessible symmetrical PEG compounds and trifunctional thiophosphates. These materials are obtained in a two‐step procedure, via the formation of THF soluble, hyperbranched PEG‐based polyazomethines that are subsequently functionalized with dimethylphosphite. The resulting materials are hydrolytically degradable, and upon exposure to aqueous solutions of silver acetate they afford stable colloidal solutions of silver.     

Structure/property relationships in erodible multilayered films: influence of polycation structure on erosion profiles and the release of anionic polyelectrolytes

We have investigated the influence of polymer structure on the erosion profiles of multilayered polyelectrolyte assemblies fabricated from sodium poly(styrene sulfonate) (SPS) and three different hydrolytically degradable polyamines. We synthesized three structurally related poly(beta-amino ester)s (polymers 1-3) having systematic variations in both charge density and hydrophobicity. These changes in structure did not influence film thickness significantly, but polymer structure was found to play an important role in defining the rates at which multilayered assemblies fabricated from these materials eroded in physiologically relevant media. Films 60 nm thick fabricated from polymer 1 and SPS eroded completely in 50 h when incubated in PBS buffer at 37 degrees C, as determined by ellipsometry. Analogous films fabricated from polymers 2 and 3 eroded and released SPS into solution over significantly longer time periods ranging from approximately 150 h (ca. 6 days) to 370 h (ca. 15 days), respectively. These differences are consistent with a systematic increase in the hydrophobicity of polymers 1-3 as well as the relative rates at which these polymers degrade hydrolytically. This work demonstrates that it is possible to tailor the rates at which thin, multilayered polyelectrolyte assemblies release incorporated anionic polyelectrolytes over a large range of time periods simply by changing the structure of the degradable polyamine used to fabricate a film. The principles reported here may therefore contribute to the design of multilayered assemblies that permit a broad range of spatial and temporal control over the release of therapeutic agents from coated surfaces.     

Micellar and Antibody-Targeted Polymer Therapeutics

Summary: Synthesis, physicochemical and some biological properties of new actively targeted antibody-containing and passively targeted micellar polymer - doxorubicin conjugates were investigated. Polymer precursors used for the synthesis of the conjugates were based on semitelechelic N-(2-hydroxypropyl)methacrylamide (HPMA) copolymers with reactive groups situated at the polymer chain end or on multivalent copolymer with groups randomly distributed along the polymer backbone. Micellar HPMA-copolymer-based pharmaceuticals were prepared by self-assembly of copolymer–doxorubicin conjugates containing hydrophobic cholesterol ligands attached to the copolymer via hydrolytically degradable spacer. pH-Controlled release of cholesterol derivative is a key-point for disintegration of the micellar drug carrier after delivering the drug to the tumor tissue. Synthesis of star antibody-targeted polymer conjugates takes advantage of reduction of disulfide bridges in antibody with dithiothreitol followed by conjugation with the semitelechelic copolymer thus avoiding modification of the binding site in the antibody for its antigen. Both conjugates differing in their molecular architecture and mechanism of action are promising candidates for in vivo antitumor therapy.     

Storage Stability Study of Salicylate-based Poly(anhydride-esters)

Storage stability was evaluated on a biodegradable salicylate-based poly(anhydride-ester) to elucidate the effects of storage conditions over time. The hydrolytically labile polymer samples were stored in powdered form at five relevant storage temperatures (−12 °C, 4 °C, 27 °C, 37 °C, 50 °C) and monitored over four weeks for changes in color, glass transition temperature, molecular weight, and extent of hydrolysis. Samples stored at lower temperatures remained relatively constant with respect to bond hydrolysis and molecular weight. Whereas, samples stored at higher temperatures displayed significant hydrolysis. For hydrolytically degradable polymers, such as these poly(anhydride-esters), samples are best stored at low temperatures under an inert atmosphere.     

Synthesis of hyperbranched degradable polymers by atom transfer radical (Co)polymerization of inimers with ester or disulfide groups

Degradable hyperbranched polymers with multiple alkyl halide chain ends were synthesized by the atom transfer radical polymerization of inimers containing ester (2‐(2′‐bromopropionyloxy)ethyl acrylate) or disulfide (2‐(2′‐bromoisobutyryloxy)ethyl 2′′‐methacryloyloxyethyl disulfide) groups. Both the homo‐ and copolymerizations (with styrene in the former case and methyl methacrylate in the latter) were studied. The hyperbranched polymers derived from the ester‐type inimer were hydrolytically degradable under basic conditions, whereas those derived from the disulfide‐containing inimer could be efficiently degraded in the presence of reducing agents such as tributylphosphine. © 2009 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2009     

Tunable drug release from hydrolytically degradable layer-by-layer thin films

The development of new thin film fabrication techniques that allow for precise control of degradation and drug release properties could represent an important advance in the fields of drug delivery and biomedicine. Polyelectrolyte layer-by-layer (LBL) thin films can be assembled with nanometer scale control over spatial architecture and morphology, yet very little work has focused on the deconstruction of these ordered thin films for controlled release applications. In this study, hydrolytically degradable LBL thin films are constructed by alternately depositing a degradable poly(beta-amino ester) (polymer 1) and a series of model therapeutic polysaccharides (heparin, low molecular weight heparin, and chondroitin sulfate). These films exhibit pH-dependent, pseudo-first-order degradation and release behavior. The highly versatile and tunable properties of these materials make them exciting candidates for the controlled release of a wide spectrum of therapeutics.     

Synthesis and characterization of novel h‐HTBN/PEG PU copolymers: effect of surface properties on hemocompatibility

This work reported the hydrophilicity, hemocompatibility, and cytotoxicity of novel polyurethane (PU) scaffolds for tissue engineering, especially the hydrolysis effect of a soft‐segmented component, a hydrolytically‐modified hydroxyl‐terminated poly(butadiene‐co‐acrylonitrile) (h‐HTBN), on these properties. The PU copolymers were prepared by coupling poly(ethylene glycol) (PEG) with the h‐HTBN together with the help of 1,1‐methylene bis‐(4‐isocyanatocyclohexane) as a bridging reagent. The structure of PU copolymers was characterized by Fourier transformation infrared spectrometry (FTIR). The experimental results indicated that the hydrolytically‐modified HTBN increases water absorption and decreases water contact angles, improving surface hydrophilicity. The synthesized h‐HTBN/PEG PU copolymers display low hemolysis activity, and a little amount of platelet adhesion and activation, implying good compatibility. The methyl tretrazolium (MTT) assays elicited that the cytotoxicity is related to the component ratios of h‐HTBN to PEG and the hydrolysis modification of HTBN. The PU scaffolds can be employed as potential candidates for blood contacting applications. Copyright © 2009 John Wiley & Sons, Ltd.     

Degradability of poly(lactic acid)-containing nanoparticles: enzymatic access through a cross-linked shell barrier

Comparative studies of bulk samples of hydrolytically degradable poly(lactic acid) (PLA) vs core-shell block copolymer micelles having PLA cores revealed remarkable acceleration in the proteinase K enzymatic hydrolysis of the nanoparticulate forms and demonstrated that even with amidation-based shell cross-linking the core domain remained accessible. Kinetic analyses by (1)H NMR spectroscopy showed less than 20% lactic acid released from enzymatically catalyzed hydrolysis of poly(l-lactic acid) in bulk, whereas ca. 70% of the core degraded within 48 h for block copolymer micelles of poly(N-(acryloyloxy)succinimide-copolymer-N-acryloylmorpholine)-block-poly(L-lactic acid) (P(NAS-co-NAM)-b-PLLA), with only a slight reduction to ca. 50% for the shell cross-linked derivatives. Rigorous characterization measurements by NMR spectroscopy, fluorescence spectroscopy, dynamic light scattering, atomic force microscopy, and transmission electron microscopy were employed to confirm core excavation. These studies provide important fundamental understanding of the effects of nanoscopic dimensions on protein-polymer interactions and polymer degradability, which will guide the development of these degradable nanoconstructs to reach their potential for controlled release of therapeutics and biological clearance.     

In vitro study of a HPγ-cyclodextrin grafted PET vascular prosthesis for application as anti-infectious drug delivery system

Hydroxypropyl-γ-cyclodextrin (HPγ-CD) was grafted onto woven polyester (PET) vascular prosthesis by using citric acid (CTR) as crosslinking agent. A polyCTR-HPγ CD polymer was physically fixed onto the PET fibers. An optimal compromise between fixation temperature and fixation time was found and a grafting rate of 6.7% was obtained. The study of the inclusion of ciprofloxacin (CFX) and HPγ-CD was evidenced by using spectrophotometry. Sorption tests also showed that modified prosthesis could adsorb 5 times more CFX than the control. Biological tests revealed proliferation rates of human pulmonary micro-vascular endothelial cells (HPMEC) of 73 and 48% on virgin and modified prostheses respectively. We demonstrated that this was rather due to the increase of surface roughness of the fibers after their modification than to a toxic effect the polyCTR-HPγCD polymer coating. Prostheses samples modified with HPγCD and impregnated with CFX stayed up to 24 h in blood plasma. At various moments some aliquots were withdrawn from the medium and a positive antibacterial activity against Staphylococcus epidermidis was observed within the 24 h period for the grafted sample, whilst that of the virgin one had disappeared within 4 h. So, cyclodextrin coating of vascular prostheses may be suitable for the controlled release of CFX, and thus should help to the prevention of post surgery complications.     

Base-triggered self-amplifying degradable polyurethanes with the ability to translate local stimulation to continuous long-range degradation

A new type of base-triggered self-amplifying degradable polyurethane is reported that degrades under mild conditions, with the release of increasing amounts of amine product leading to self-amplified degradation. The polymer incorporates a base-sensitive Fmoc-derivative into every repeating unit to enable highly sensitive amine amplified degradation. A sigmoidal degradation curve for the linear polymer was observed consistent with a self-amplifying degradation mechanism. An analogous cross-linked polyurethane gel was prepared and also found to undergo amplified breakdown. In this case, a trace amount of localized base initiates the degradation, which in turn propagates through the material in an amplified manner. The results demonstrate the potential utility of these new generation polyurethanes in enhanced disposability and as stimuli responsive materials.

A new type of base-triggered self-amplifying degradable polyurethane is reported that degrades under mild conditions, with the release of increasing amounts of amine product leading to self-amplified degradation.     

Synthesis and characterization of novel h‐HTBN/PEG PU copolymers for tissue engineering: degradation,phase behavior,and mechanical properties

The phase behavior of the as‐prepared polyether polyurethane (PU) elastomers was investigated by dynamic mechanical analysis (DMA), polarized optical microscope (POM), and atomic force microscopy (AFM). This PU copolymers were composed of different compositions of two soft segments, poly(ethylene glycol) (PEG) and hydrolytically modified hydroxyl‐terminated poly(butadiene‐co‐acrylonitrile) (h‐HTBN) oligomers. The microphase separation behavior is confirmed to occur between soft and hard segments as well as soft and soft segments as the h‐HTBN is incorporated into the PU system, depending on soft‐soft and/or soft‐hard microdomain composition, molecular weight (MW) of PEG, and hydrolysis time of HTBN. The driving force for this phase separation is mainly due to the formation of inter‐ and intramolecular hydrogen bonding interaction. The PU‐70, PU‐50 samples with non‐reciprocal composition seem to exhibit larger microphase separation than any other PU ones. The hydrolysis degradation, thermal stability, and mechanical properties of the copolymers were assessed by gravimetry, scanning electron microscope (SEM), thermal gravity analysis (TGA), and tensile test, respectively. The experimental results indicated that the incorporation of h‐HTBN soft segment into PEG as well as low MW of PEG leads to increased thermal and degradable stability based on the intermolecular hydrogen bond interaction. The PU‐70 and PU‐50 copolymers exhibit better mechanical properties such as high flexibility and high ductility because of their larger microphase separation architecture with the hard domains acting as reinforcing fillers and/or physical crosslinking agents dispersed in the soft segment matrix. Copyright © 2009 John Wiley & Sons, Ltd.     

Preparation of an environmentally friendly antifouling degradable polyurethane coating material based on medium-length fluorinated diols

A novel medium-length fluorinated diols and poly(L-lactide) (PLLA) were synthesized via Michael addition reaction and ring-opening polymerization, respectively. Subsequently, Synthetic medium-length fluorinated diols and PLLA were combined to prepare new polyurethane composites with degradability and low surface energy. The compositional analysis and structural characterization of synthetic materials were characterized by using fourier transform infrared spectroscopy (FT-IR) and proton nuclear magnetic resonance spectra (¹HNMR). Thermogravimetric analysis(TGA) indicated that the introduction of medium-length fluorinated diols improved the thermal stability of the polyurethane. The biodegradation and low surface energy of the polyurethane were investigated by static hydrolysis experiment and water contact angle test. It was found that the degradation rate of the polyurethane increased as measurement time went on when the PLLA content was under 40%, and the water contact angle increased from 71.12° to 108.24° with the increase of fluorine content, which indicated that the degradable and low surface energy polyurethane has a potential as a coating material for a marine antifouling coating application.     

Synthesis and in vitro degradation of poly(N‐vinyl‐2‐pyrrolidone)‐based graft copolymers for biomedical applications

This work is devoted to the design of a novel family of hydrosoluble biomaterials: poly(N‐vinyl‐2‐pyrrolidone) (PVP)‐based graft copolymers. A synthesis route has been elaborated in which ω‐functionalized PVP is prepared via chain‐transfer radical polymerization, end‐group modified, and subsequently grafted onto a polyhydroxylated backbone, typically dextran or poly(vinyl alcohol). The resulting graft copolymer biomaterials are designed for use in various biomedical applications, particularly as materials with a stronger potential for plasma expansion than already existing products have. The graft copolymers are potentially degradable because the PVP grafts are connected to the polyol backbone via a hydrolytically labile carbonate or ester linkage. The degradation of the graft copolymers was performed in vitro over a period of 6 weeks. © 2002 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 40: 3652–3661, 2002