Compositions for tissue augmentation

FIELD OF THE INVENTION

[0002] The present invention relates to biomaterials for tissue augmentation, precursor components capable of forming biomaterials and to the uses for such biomaterials. In particular, the present invention relates to the in situ formation of biomaterials for augmentation of soft and hard tissues.

BACKGROUND OF THE INVENTION

[0003] One of the areas in which technological advances have significantly enhanced surgery involves the use of synthetic materials for implantation in the body to assist in surgical reconstruction and repair. Biomaterials of synthetic polymeric origin are now widely accepted for tissue related applications, as tissue regeneration matrices, as tissue adhesives, as drug delivery matrices, in the prevention of surgical adhesions, for coating surfaces of synthetic implants and as tissue augmentation material. A lot of work has been done in the development of polymeric systems which can be applied as liquids which crosslink in situ to form biomaterials at the site of need on and/or in the body. Depending on the chemical structure of the precursor components and their stoichiometry, the biomaterials have varying physical and chemical properties.

[0004] Orthopedic Surgery

[0005] Orthopedic surgery has historically been the most significant application for biomaterials. It addresses medical concerns in the musculoskeletal system and the treatment of diseases and disturbances to its components, particularly bones, cartilage, ligaments, and tendons. The musculoskeletal system produces movement and responds to forces, therefore it is susceptible to injury and stress-related diseases, which can devastatingly affect the mobility. Any replacement and enforcement of these tissues has to perform in the same mechanical environment, and attainment of the relevant mechanical performance is not trivial. Further, as part of the aging process, tissue changes its shape and consistency. In particular, some tissues lose their form; thus augmentation or restoration is desirable. The loss of bone mass and stability, as occurs in osteoporosis, can be particularly devastating to an individual. A number of other diseases also disturbs the bone and joint function, leading to pain, loss of movement, or loss of vital function. One such prominent example is osteoarthritis, which is largely a mechanical disruption to the cartilage and underlying bone at the joints.

[0006] Hard Tissue Augmentation

[0007] Although a biomaterial used for augmenting hard tissue can be applied in different ways, a particular preferred way is through minimal invasive surgery. Compression fractures are particularly problematic in osteoporotic women. Minimally invasive surgery is the procedure of choice for treating vertebral compression fractures or osteoporotic vertebrae. This treatment is known as vertebroplasty. Before vertebroplasty was developed, surgeons did not treat compression fractures because intervention in these patient cases was risky and only inadequate tools were available. Vertebroplasty, a procedure in which the vertebral body is filled percutaneously with polymethylmethacrylate (PMMA) was developed to fulfill the treatment gap.

[0008] PMMA is mainly known as bone cement and is used off-label in this indication. PMMA is a hard, brittle polymer, tolerated by tissues and generally resistant to degradation. PMMA as used in vertebroplasty is a powder liquid system (PMMA co-polymer/monomeric methylmethacrylate) mixed in the operation room to a viscous paste and pulled up in to a syringe immediately prior to injection into the vertebra.

[0009] Vertebroplasty is a very effective treatment for compression fractures. It relieves pain in the majority of cases by preventing the micro-movement of the spongy tissue structure inside the vertebra and providing mechanical stabilization of existing microfractures (Mathis J. et al., Am. J. Neuroradiol. 22: 373-381 (2001)). The risk factors and problems in vertebroplasty are mainly associated with the toxicity of methylmethacrylate. The highly toxic methylmethacrylate may leach out into the blood stream before it is crosslinked sufficiently, causing blood pressure drop and migration of the bone cement into the veins with the possibility of ending up in the lungs or causing hypotension. Although this is a risk common to all uses of PMMA, it is increased in vertebroplasty due to the fact that PMMA is injected under pressure into a closed space inside fractured bone. This increases the risk for leakage. The exothermic polymerization process is a further deficiency of PMMA since it often leads to substantial damage of the surrounding tissue. Thus, PMMA is far from the ideal biomaterial for hard tissue augmentation, in general, and for application in vertebroplasty, in particular.

[0010] Handling is also an issue. The final preparation of the PMMA mixture has to be performed in the operation room. The individual components are measured, mixed to a homogenous mixture and the mixture is filled into the appropriate device for application, which is a syringe in the case of vertebroplasty. This procedure is time-consuming, susceptible to mistakes and bears health hazards for the person preparing the PMMA caused by inhalation of the powder during mixing and the volatile methylmethacrylate.

[0011] Even after successful injection and polymerization, PMMA can cause complications. PMMA is very hard and can cause stress-shelding and/or collapse of the vertebrae adjacent to the treated vertebra which then may fracture as well. (Ferguson S. et. al, Transactions of the 47th Annual Meeting of the ORS, 0280 (2001)).

[0012] Compositions which have to form biomaterials at the site of injection in the human or animal body and which have to augment osteoporotic vertebrae have to comply with various needs. First, the treatment should reduce or completely remove the pain associated with fractured vertebrae so that the patient can leave the bed. Second, the mechanical properties of the osteoporotic vertebra must be improved. This is evident when comparing compressive strength and Young's modulus E of a young healthy vertebra (vertebra in its ideal state) to an osteoporotic vertebra. The compressive strength of the spongy inner part of an ideal vertebra can be up to eightfold greater than that of an osteoporotic vertebra. Similarly, the Young's modulus E of the spongy part of an ideal vertebra can be up to a hundredfold greater than the Young's modulus E of an osteoporotic one. It is accepted that the mechanical properties of an ideal vertebra can hardly be re-established but people suffering from osteoporosis are mainly at an advanced age and do not seek to undertake great physical efforts which require the presence of ideal vertebrae. Thus as long as the patient is free of pain and has regained mobility to a substantial part of his vertebrae, the treatment is successful.

[0013] Biomaterials which are made from polymeric hydrophilic systems, such as PEG derivatives, have been described in the prior art, such as in U.S. Pat. Nos. 5,626,863; 6,166,130; 6,051,648; 5,874,500; 6,258,351 and in WO 00/44808. These biomaterials are not suitable for use in hard tissue augmentation due to their lack of mechanical performance, such as strength and stiffness and due to extensive swelling. Uncontrollable swelling makes biomaterials unacceptable for application in limited spaces as in vertebrae. The material expands and can press against nerves, such as the spinal cord, or protrudes uncontrollable from the place of injection.

[0014] Therefore, there exists a need for new biomaterials which can be used for hard tissue augmentation. In particular due to the growth in the elderly population, there is a need for a replacement of PMMA in vertebroplasty.

[0015] It is therefore an object of the present invention to provide a biomaterial for tissue augmentation.

[0016] It is a further object of the present invention to provide a biomaterial for hard tissue augmentation, preferably as a replacement for PMMA.

[0017] It is a further object to provide an augmentation material for use in vertebroplasty which does not have the disadvantages and risks associated with the use of PMMA.

SUMMARY OF THE INVENTION

[0018] Methods for making biomaterials for augmentation of soft and hard tissues, kits containing precursors for forming the biomaterials, and the resulting biomaterials are described herein. The biomaterials are formed from at least a first and a second precursor component. The first precursor component contains at least two nucleophilic groups, and the second precursor component contains at least two electrophilic groups. The nucleophilic and electrophilic groups of the first and second precursor components form covalent linkages with each other at physiological temperatures. The precursors are selected based on the desired properties of the biomaterial. In the preferred embodiment, the first precursor is a siloxane. Optionally, the biomaterials contain additives, such as thixotropic agents, radiopaque agents, or bioactive agents. In the preferred embodiment, the biomaterials are used to augment at least one vertebra of the spine (vertebroplasty).

BRIEF DESCRIPTION OF THE DRAWINGS

[0019]

FIG. 1

a
shows a comparison of Young's modulus (MPa) between a control and an augmented group of vertebrae for both low and high volume fractions (VF) (* p<0.05).

[0020]
FIG. 1B (lower picture) shows a comparison of strength (MPa) between a control and an augmented group of vertebrae for both low and high volume fractions (VF) (p<0.05).

[0021]
FIG. 2 is a graph the maximal applied stress (Smax) divided by volume fraction (FV) (MPa) versus the number of cycles to failure (Nf), which compares the fatigue result of augmented trabecular bone (augmented group) to non-augmented trabecular bone (control group).

DETAILED DESCRIPTION OF THE INVENTION

[0022] Definitions

[0023] “Biomaterial” or “Pharmaceutical composition” as generally used herein refers to a material intended to interface with biological systems to evaluate, treat, augment, or replace any tissue, organ or function of the body. Biomaterial refers to the complete material (precursor plus all additives, fillers, base or solvents) at and after having reached and passed its gel-point.

[0024] “Mixture of precursor components” as generally used herein refers to the precursor components after being mixed and before the mixture has reached its gel-point.

[0025] “Nucleophilic group” as generally used herein refers to functional groups, such as thiols and amines, and refers to molecules which contain the functional groups.

[0026] “Conjugation” can refer both to alternation of carbon-carbon, carbon-heteroatom or heteroatom-heteroatom multiple bonds with single bonds, or to the linking of a functional group to a macromolecule, such as a synthetic polymer or a protein. Double bonds spaced by a CH or CH2 unit are referred to as “homoconjugated double bonds”.

[0027] “Biocompatibility or biocompatible” as generally used herein refers to the ability of a material to perform with an appropriate host response in a specific application. In the broadest sense, this means a lack of adverse effects to the body in a way that would outweigh the benefit of the material and/or treatment to the patient.

[0028] “In situ formation” as generally used herein refers to the ability of mixtures of precursor components which are substantially not crosslinked prior to and at the time of injection to form covalent linkages with each other at a physiological temperature at the site of injection in the body.

[0029] “Oligomer and polymers” are used in the usual sense of the terms. An oligomer is a low-molecular weight polymer. Oligomers typically contain between two and ten monomer units. As used herein, polymers typically contain more than 10 monomeric units.

[0030] “Cross-linking” as generally used herein means the formation of covalent linkages. However, it may also refer to the formation of non-covalent linkages, such as ionic bonds, or combinations of covalent and non-covalent linkages.

[0031] “Functionality” as generally used herein means the number of reactive sites on a molecule. “Reactive sites” refer to nucleophilic and electrophilic groups that are able to react in a self-selective reaction at least but not exclusively under conditions in the human or animal body.

[0032] “Multifunctional” as generally used herein means more than one electrophilic and/or nucleophilic functional group per molecule (i.e. monomer, oligmer or polymer).

[0033] “Self selective reaction” as generally used herein means that the first precursor component of the composition reacts much faster with the second precursor component of the composition and vice versa than with other compounds present both in the mixture or at the site of the reaction. As used herein, the nucleophile preferentially binds to a electrophile, rather than to other biological compounds, and an electrophile preferentially binds to a strong nucleophile rather than to other biological compounds.

[0034] “Polymeric network” means the product of a process in which substantially all of the monomers, oligo- or polymers are bound by intermolecular covalent linkages through their available functional groups to result in one huge molecule.

[0035] “Physiological” means conditions as they can be found in living vertebrates. In particular, physiological conditions refer to the conditions in the human body such as temperature, pH, etc. Physiological temperatures means in particular a temperature range of between 35° C. to 42° C., preferably around 37° C.

[0036] “Soft tissue” means non-skeletal tissue, i.e. exclusive of bones, ligaments, cartilage, spinal disc and fibrous tissue.

[0037] “Hard tissue” means bone, cartilage and ligament. In particular bone.

[0038] “Augmentation” means the act of augmenting, making larger and particularly making stronger by addition and increase of material; furthermore it means the state of being augmented; as used herein augmentation means in particular to strengthen tissue; augmentation also encompasses cementation of artificial joints like artificial hips and knees within the body.

[0039] “Crosslink density” is defined as the average molecular weight between two crosslinks (Mc) of the respective molecules.

[0040] “Equivalent weight” is defined as mmol of functional group/g of substance

[0041] “Respective counterpart” means the reaction partner of a molecule. The respective counterpart to the electrophilic group is the nucleophilic group and vice versa.

[0042] “Hydrogel” means a class of polymeric material which is extensively swollen in a aqueous medium, but which does not dissolve in water.

[0043] “Swelling” means the increase in volume and/or mass by uptake of water by the biomaterial. The terms “water-uptake” and “swelling” are used synonymously throughout this application.

[0044] “Compressive strength” means the maximum stress a material can sustain under crush loading. Compressive strength is calculated by dividing the maximum load by the original cross-sectional area of a specimen in a compression test.

[0045] “Thixotropic fluids” refer to fluids which show a time dependent response to shear. When subjected to a fixed shear rate, they will decrease in viscosity over time. Often this is seen as a large initial viscosity loss, followed by gradual further loss. Once shear is removed, thixotropic fluids recover viscosity. These fluids are usually considered pseudoplastic as well, but only in that they show decreasing viscosity in response to increasing shear rate. Pseudoplastic fluids are commonly considered simply shear-thinning. More specifically, they show decreasing viscosity in response to increasing shear rate. Moreover, they immediately recover their non-sheared viscosity once shear is removed.

[0046] “Stiffness” is defined as measure of resistance of plastic to bending. It includes both plastic and elastic behavior. Stiffness of the biomaterials is measured by measurement of Young's modulus E.

[0047] “Strain” is change per unit length in a linear dimension of a part or specimen, usually expressed in % strain based on original length of the specimen (ΔL/Lo). True or natural strain is based on instantaneous length, and is equal to ln×lo, where I is instantaneous length and lo is original length of the specimen. Shear strain is the change in angle between two lines originally at right angles.

[0048] “Stress” is defined as load on specimen divided by the area through which it acts and generally contains units of Pa or MPa. As used with most mechanical tests, stress is based on original cross-sectional area without taking into account changes in area due to applied load. This sometimes is called conventional or engineering stress. True stress is equal to the load divided by the instantaneous cross-sectional area through which it acts.

[0049] “Modulus of Elasticity/Young's modulus E” is defined as the rate of change of strain as a function of stress and generally contains units of Pa or MPa. Young's Modulus is the slope of the straight line portion of a stress-strain diagram. Tangent modulus of elasticity is the slope of the stress-strain diagram at any point. Depending on the type of loading represented by the stress-strain diagram. Modulus used alone generally refers to tensile modulus of elasticity (or modulus of elasticity in tension). Moduli of elasticity in tension and modulus of elasticity in compressive are approximately equal and are known as Young's modulus.

[0050] “Gel point” is defined as being the point where the viscous modulus and complex modulus cross each other and viscosity increases. The viscous modulus is at the end lower that at the beginning, the complex modulus is at the end higher than at the beginning. Thus the gel point is the stage at which a liquid begins to take on the semisolid characteristics of a gel.

[0051] I. Compositions

[0052] An in situ crosslinkable composition for the manufacture of a pharmaceutical composition or biomaterial for augmenting hard tissue is described herein. The composition contains at least a first and a second multifunctional precursor component. Optionally additives and/or biologically active agents may be added to the precursor components. The precursor components are mixed and polymerize in situ to form a biomaterial. The structure of the precursor components is selected based on the type of biomaterial that is desired.

[0053] A. Precursors

[0054] The first precursor component contains at least two nucleophilic groups, and the second precursor component contains at least two electrophilic groups. The first and second precursor components are selected such that the nucleophilic and electrophilic groups form covalent linkages with each other at physiological temperatures.

[0055] The precursor components are multifunctional monomers, oligomers and/or polymers. Preferably the precursor components are multifunctional monomers and oligomers. Preferably the molecular weight of the first and second precursor component is in a range of between 100 g/mol to 900 g/mol, preferably 200 g/mol to 700 g/mol and even more preferably 400 g/mol to 550 g/mol.

[0056] The functionality of the first and/or second precursor component is at least three. In a preferred embodiment, the first precursor component has a functionality of four, and the second precursor component a functionality of three. In another embodiment, the first precursor component has a functionality of three, and the second precursor component a functionality of four. However the 3 to 4 functionality is not a prerequisite for the polymeric network to form a biomaterial with the mechanical properties needed for vertebroplasty because the mechanical performance also depends on the structure of the molecule. A small and compact molecule will form a polymeric network with greater strength than an extended molecule, although the functionality, molecular weight and reaction partner might be the same for both molecules.

[0057] As a general guideline, the ratio of the first and second precursor components is selected such that the majority of the functional groups of both components react with the respective counterparts. The ratio of the equivalent weights of the electrophilic groups (second precursor component) and the nucleophilic groups (first precursor component) is in the range of between 0.7 and 1.1, more preferably between 0.8 and 1.0.

[0058] a. Nucleophilic Groups

[0059] The nucleophilic groups of the first precursor component are able to react with conjugated unsaturated groups. The nucleophiles that are useful are those that are reactive towards conjugated unsaturated groups via addition reactions, in particular in a self-selective nucleophilic addition reaction under conditions in the human or animal body. The reactivity of the nucleophile depends on the identity of the unsaturated group. The identity of the unsaturated group is first limited by its reaction with water at physiologic pH. Thus, the useful nucleophiles are generally be more nucleophilic than water at physiologic pH. Preferred nucleophiles are commonly found in biological systems, for reasons of toxicology, but are not commonly found free in biological systems outside of cells.

[0060] The usefulness of particular nucleophiles depends upon the situation envisioned and the amount of self-selectivity desired. In the preferred embodiment, the nucleophile is a thiol. However, amines may be effective nucleophiles.

[0061] Thiols are present in biological systems outside of cells in paired form, as disulfide linkages. When the highest degree of self-selectivity is desired (e.g. when the gelation reaction is conducted in the presence of tissue and chemical modification of that tissue is not desirable), then a thiol acts as a strong nucleophile.

[0062] There are other situations, however, where the highest level of self-selectivity may not be necessary. In these cases, an amine may serve as an adequate nucleophile. Here, particular attention is paid to the pH, in that the deprotonated amine is a much stronger nucleophile than the protonated amine. Thus, for example, the alpha amine on a typical amino acid (pK as low as 8.8 for asparagine with an average pK of 9.0 for all 20 common amino acids, except proline) has a much lower pK than the side chain epsilon amine of lysine (pK 10.80). As such, if particular attention is paid to the pK of an amine used as the strong nucleophile, substantial self-selectivity can be obtained. By selection of an amine with a low pK, and then formulation of the final precursor such that the pH is near that pK, one could favor reaction of the unsaturation with the amine provided, rather than with other amines present in the system. In cases where no self-selectivity is desired, the pK of the amine used as the nucleophile is les important. However, to obtain reaction rates that are acceptably fast, the pH is adjusted to be the pH of the final precursor solution so that an adequate number of these amines are deprotonated.

[0063] The nucleophilic groups may be contained in molecules with great flexibility in overall structure. For example, a difunctional nucleophile could be presented in the form of Nuc-P-Nuc, where P indicates a monomer, oligomer or polymer and Nuc refers to the nucleophile. Likewise, a branched polymer, P, could be derivatized with a number of nucleophiles to create P-(Nuc)i., where I is greater than 1. The nucleophile could be part of the repeating structure, e.g. (P-Nuc)i. Clearly, not all of the P or the nucleophiles in such a structure need to be identical.

[0064] Preferred First Precursor Components

[0065] In a preferred embodiment, the first precursor component is a siloxane derivative containing thiols and/or amines as nucleophilic groups. The cyclosiloxane derivative may have the following formula:

[0066] where n=3-6, preferably 4; R1=alkyl, preferably C1-C6-alkyl; and R2″=alkyl, preferably C2-C3-alkyl; X=—SH, —NH2.

[0067] These molecules contain a nearly ideal combination of characteristics which are desired for the intended use of hard tissue augmentation. They are small, compact, and hydrophobic with a high degree of functionality. Particularly preferred is 2,4,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane; using the above formula, n=4; R1=CH3; R2″=C2H4; X=—SH (21).

[0068] In a further embodiment, the first precursor component is a cyclohexyl-; pentaerithritol-; 1,1,1, tris-(hydroxy-methyl)propane-; or 1,1,1 tris-(hydroxy-methyl)propanol-derivative that contains at least two alkyl chains with end-standing thiol and/or amine groups.

[0069] Derivatives of cyclohexyl preferably have the following formula:

[0070] where n=6; R1=H, alkyl preferably C1 to C4, R2″=alkyl, preferably C1 to C4 alkyl; and X=—SH. The most preferred derivative is 1,2,4-Tris (2-mercaptoethyl)-cyclohexane; using the above formula, n=6; R1=H; R2″=C2H4; X=—SH. (22).

[0071] Preferably pentaerithritol, 1,1,1 tris-(hydroxy-methyl)propane and 1,1,1 tris-(hydroxy-methyl)propanol are converted into alkylether or alkylester derivatives comprising at least three alkyl-chains with end-standing thiol groups. The length of the alkyl chain and the functionality are determined by the requirement of hydrophobicity, size and intended cross-link density based on the intended use. The length of the alkyl chain also depends on the reaction partner. If the reaction partner is small and compact with a functionality of at least three, the alkyl chains of the pentaerithritol, 1,1,1 tris-(hydroxy-methyl)propane and 1,1,1 tris-(hydroxy-methyl)propanol derivatives can be longer.

[0072] Particularly preferred compounds are 3-(3-Mercapto-.propoxy)-2,2-bis-(3-mercapto-propoxymethyl)-propan-1-ol (23); 2-[2,2-Bis-(2-mercapto-ethyoxymethyl)-butoxy]-ethanethiol (24); tri(3-mercaptopropyl)TMP (25); Pentaerithritol tetrakis(2-mercaptoproprionate) (26); and pentaerythritol tetrakis(3-mercaptopropyl)ether (27).

1TABLE 1Preferred first precursor components

[0073] b. Electrophilic Groups

[0074] The electrophilic groups of the second precursor component are preferably conjugated unsaturated groups. Structures of P and the conjugated unsaturated groups may be similar to those described above for the nucleophiles. It is only necessary that one conjugated unsaturated precursor contain greater than or equal to two such conjugated unsaturated groups.

[0075] It is possible to perform nucleophilic addition reactions, in particular Michael addition reactions, on a wide variety of conjugated unsaturated compounds. In the structures shown below, a monomeric, oligomeric or polymeric structure is indicated as P. Various preferred possibilities for the specific identity of P are discussed further herein. P can be coupled to reactive conjugated unsaturated groups in structures such as those numbered 1 to 20.

2TABLE 2Molecular structures containingP and conjugated unsaturated groups

X = H, CH3, CN, COOW R = H, W, Phenyl-(Ph) Y = NH, O, 1,4-Ph W = C1-C5 aliphatic chain

A, B = H, alkyl R = H, alkyl Y = O, NH, 1,4-Ph

X = CN, COOW Y = OW, Ph W = C1-C5 aliphatic chain

X = N, CH

A X = CH Y = CH R = H, W—P (W = NH, O, nihil) B X = N Y = N R = H, P C X—Y = C═C R = W—P (W = NH, O, nihil)

X, Y = H, P P, P P, H P, aliphatic chain

Y = O, NH X =alkali or alkali earth metal ion, P W = P, 1,4-Ph—P

X = halogen, sulphonate

Y = O, NH X = alkali or alkali earth metal ion, P W = P, 1,4-Ph—P

[0076] Reactive double bonds can be conjugated to one or more carbonyl groups in a linear ketone, ester or amide structure (1a, 1b, 2) or to two in a ring system, as in a maleic or paraquinoid derivative (3, 4, 5, 6, 7, 8, 9, 10). In the latter case, the ring can be fused to give a naphthoquinone (6, 7, 10) or a 4,7-benzimidazoledione (8) and the carbonyl groups can be converted to an oxime (9, 10). The double bond can be conjugated to a heteroatom-heteroatom double bond, such as a sulfone (11), a sulfoxide (12), a sulfonate or a sulfonamide (13), or a phosphonate or phosphonamide (14). Finally, the double bond can be conjugated to an electron-poor aromatic system, such as a 4-vinylpirydinium ion (15). Triple bonds can be used in conjugation with carbonyl or heteroatom-based multiple bonds (16, 17, 18, 19, 20).

[0077] Structures such as 1a, 1b and 2 are based on the conjugation of a carbon-carbon double bond with one or two electron-withdrawing groups. One of them is always a carbonyl, increasing the reactivity passing from an amide, to an ester, and then to a phenone structure. The nucleophilic addition is easier upon decreasing the steric hindrance, or increasing the electron-withdrawing power in the alpha-position. For example, the following relationship exists, CH3<H<COOW<CN, where CH3 has the least electron-withdrawing power and CN has the most electron-withdrawing power.

[0078] The higher reactivity obtained by using the last two structures can be modulated by varying the bulkiness of the substituents in the beta-position, where the nucleophilic attack takes place; the reactivity decreases in the order P<W<Ph<H. Thus, the position of P can be used to tune the reactivity towards nucleophiles. This family of compounds includes some compounds for which a great deal is known about their toxicology and use in medicine. For example, water-soluble polymers with acrylates and methacrylates on their termini are polymerized (by free radical mechanisms) in vivo. Thus, acrylate and methacrylate-containing polymers have been used in the body in clinical products, but with a dramatically different chemical reaction scheme.

[0079] The structures 3-10 exhibit very high reactivity towards nucleophiles, due both to the cis configuration of the double bond and the presence of two electron-withdrawing groups. Unsaturated ketones react faster than amides or imides, due to the stronger electronegativity of these carbonyl groups. Thus, cyclopentendione derivatives react faster-than maleimidic ones (3), and para-quinones react faster than maleic hydrazides (4) and cyclohexanones, due to more extended conjugation. The highest reactivity is shown by naphthoquinones (7). P can be placed in positions where it does not reduce the reactivity of the unsaturated group, that is in the opposite part of the ring (3, 5), on another ring (7, 8) or O-linked through a para-quinone mono-oxime (9, 10). To decrease the rate of the nucleophilic addition reaction, P can be also linked to the reactive double bond (6, 8).

[0080] The activation of double bonds to nucleophilic addition can be obtained by using heteroatom-based electron-withdrawing groups. In fact, heteroatom-containing analogues of ketones (11, 12), esters and amides (13, 14) provide similar electron-withdrawing behavior. The reactivity towards nucleophilic addition increases with electronegativity of the group. Thus the structures have the following relationship, 11>12>13>14, where II is the most electronegative and 14 is the least electronegative. The reactivity towards nucleophilic addition is also enhanced by the linkage with an aromatic ring. A strong activation of double bonds can also be obtained, using electron-withdrawing groups based on aromatic rings. Any aromatic structure containing a pyridinium-like cation (e.g., derivatives of quinoline, imidazole, pyrazine, pyrimidine, pyridazine, and similar sp2-nitrogen containing compounds) strongly polarizes the double bond and makes possible quick Michael-type additions.

[0081] Carbon-carbon triple bonds conjugated with carbon- or heteroatom-based electron-withdrawing groups, can easily react with sulfur nucleophiles, to give products from simple and double addition. The reactivity is influenced by the substituents, in a manner similar to double bond-containing analogous compounds discussed above.

[0082] The formation of ordered aggregates (liposomes, micelles) or the simple phase separation in water environment increase the local concentration of unsaturated groups and so the reaction rate. In this case, the latter depends also on the partition coefficient of the nucleophiles, which increases for molecules with enhanced lipophilic character.

[0083] Preferred Second Precursor Components

[0084] In the preferred embodiment, the second precursor molecule is a monomer, oligomer or polymer that contains acrylates, itaconates or itaconamides as the conjugated unsaturated group. In particular, the second precursor component may be a derivative of 1,1,1 tris(hydroxymethyl)propane, pentaerithritol or triglycerol that contains at least two, and preferably three, conjugated unsaturated groups, such as acrylates, itaconates or itaconamides.

[0085] Preferred second precursor components are listed in Table 3 below and include Trimethylolpropane triacrylate (28); Triglycerol-penta(1-methyl itaconate) (29); 1,1,1-tris(hydroxymethyl)propane-tris(1-n-butyl itaconate) (30); Pentaerythritol-tetra(1-n-butyl itaconate) (31); N,N′,N″,N′″-tetrakis(1-hydrogen-itaconyl)-triethylenetetraamine (32); 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33); and Trimethylolpropane tris[poly(propyleneglycol), itaconamide terminated] ether (34).

3TABLE 3Preferred Second Precursor Components

[0086] Particularly preferred is Trimethylolpropane triacrylate (28) as the second precursor component in an in situ crosslinkable composition for hard tissue augmentation and particularly vertebroplasty.

[0087] Method of Making Second Precursor Component

[0088] Itaconates as derivatives of 1,1,1 tris(hydroxymethyl)propane, pentaerithritol and triglycerol molecules can be synthesized according to three different ways.

[0089] (A) Two step synthesis via chlorination reaction: Saponification of dialkylitaconate to 1-alkyl-4-hydrogen itaconate in the presence of an organic acid. Chlorination of 4-hydrogen-1-methyl itaconate to 1-methyl itaconyl chloride with e.g. SOCl2. Reaction between 4-hydrogen-1-methyl itaconate and X—OH (X—OH=1,1,1 tris(hydroxymethyl)propane, pentaerithritol and triglycerol) to the itaconyl derivatives of X—OH.

[0090] (B) Two step reaction via coupling agent: Saponification of dialkylitaconate to 1-alkyl-4-hydrogen itaconate in the presence of an organic acid. Reaction between 4-hydrogen-1-methyl itaconate and X—OH (X—OH=1,1,1 tris(hydroxymethyl)propane, pentaerithritol and triglycerol) in the presene of a coupling agent to the itaconyl derivatives of X—OH

[0091] (C) One step synthesis via transesterification reaction: Reaction between dialkylitaconate and X—OH (X—OH=1,1,1 tris(hydroxymethyl)propane, pentaerithritol and triglycerol) in the presence of e.g. toluene sulfonic acid to the itaconyl derivatives of X—OH.

[0092] In this context, synthesis (B) is preferred.

[0093] c. Additives

[0094] The composition may further comprise at least one thixotropic agent in a range of between 1 to 7 weight % of the total weight of the composition, preferably in a range of between 1.5 to 5 weight % and even more preferably of between 2 to 4 weight %. The thixotropic agent can be of organic (e.g. hydroxypropylcellulose) or inorganic nature such as hydrophilic or hydrophobic silica, smectite and hormite clay. In a preferred embodiment, hydrophilic silica is used as the thixotropic agent.

[0095] The composition further can contain radiopaque agents in order to track the performance of application and to instantaneously detect potential leakage. The detection of leakage is, especially in vertebroplasty, of importance as described hereinbefore. The radiopaque agents can be of organic or inorganic nature. In a preferred embodiment, barium sulfate (BaSO4) is used as radiopaque X-ray contrast agent, preferably in a range of between 4 weight % to 30 weight % of the weight of the total composition, preferably in a range of between 5 to 20 weight %, and even more preferably in a range of between 6 to 10 weight %. Preferably the BaSO4 has a specific surface area of greater than or equal to 25 m2/g and a particle size (diameter) of less than or equal to 100 μm (d50). In another preferred embodiment, zirconium oxide (ZrO2) is used as the X-ray contrast agent. The applicable weight percentages are in the same ranges as for BaSO4.

[0096] Whereas the addition of radiopaque agents of a particle size of less than or equal to 100 μm average diameter in an amount of between 5 to 30 weight % of the weight of the total composition gives a uniform radiopaque background under X-ray radiation, the addition of few radiopaque particles of an average diameter of about 250 to 600 μm in addition to the uniform radiopaque background allow detection of not only the injection front, but also the injection behavior within the bulk material. This is known as dynamic imaging. This can serve as a further tool for guaranteeing the instantaneous detection of leakage. In a preferred embodiment, radiopaque particles with an average diameter of about 250 to 600 μm, preferably 500 μm are added to the biomaterial. A preferred particle material is gold or titan.

[0097] Apart from their function as thixotropic and X-ray contrast agents, silica, zirconium oxide and barium sulfate serve as fillers in the composition. The addition of fillers result in an increase of the mechanical properties (ultimate compressive strength and Young's modulus E) of the biomaterial compared to the mechanical properties of the polymeric network. For example, the Young's modulus E of a polymeric network of 2,4,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane and 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate), in an equivalent weight ratio of 1 (equivalent weight of double bonds to thiol groups), almost doubles by the addition of 25 weight % fillers (SiO2 and BaSO4 and/or ZrO2).

[0098] d. Bases

[0099] The in situ crosslinking of the first and the second precursor component takes place under base catalysis. A variety of bases comply with the requirements of catalyzing the reaction at physiological temperature ranges and of not being detrimental to the patient's body. Tertiary alkyl-amine bases proved to be most suitable in terms of gelation time (preferred is 10 to 15 min) and tolerance for deviation of amount. Preferably the bases are tributylamine, triethylamine, ethyldiisopropylamine, or N,N-dimethylbutylamine. The most preferred base for forming a biomaterial for hard tissue augmentation and vertebroplasty is tributylamine.

[0100] For a given composition, the gelation time is dependant on the amount and type of base. Thus the gelation time of the composition can be controlled and adjusted to the need of application by varying the base concentration and the type of base. For example, when diethanolamine and ethanolamine are used, the gelation time decreases to 1 to 5 min under comparable conditions. Piperidin, morpholine, triethanolamine, or N-Boc-ethanolamine result in slow gelation times, but they may be used if they are mixed with bases which lead to faster gelation.

[0101] e. Solvents

[0102] Although compositions are preferred that do not require the presence of solvents, some of them need the addition of little amounts of solvents, e.g. for better mixing. In that cases solvents and solvent concentrations are chosen that are not detrimental to the patient's body.

[0103] The first and second precursor components and base, and optionally solvents and/or additives, preferably form a single phase system. The weight % of the sum of donor and acceptor molecules, i.e. the mixture of precursor components, is preferably in a range of between 60 to 90% of the total weight of the composition and even more preferably between 70 and 85 weight %.

[0104] II. Biomaterials

[0105] The requirements of biomaterials are dependent on the purpose and site of application in the body. In a preferred embodiment, the biomaterial augments hard tissue and is particularly suitable for the use in vertebroplasty. For this purpose, the biomaterial must not be susceptible to swelling and must impart to the tissue in need of augmentation an acceptable mechanical stability after application. The characteristics of the biomaterial are mainly dependent on the choice of the precursor components which crosslink to a polymeric network which forms the basis of the biomaterial. Whereas the mechanical stability of the biomaterial is essentially dependent on the crosslink density of the polymeric network, the water uptake by the biomaterial is influenced by an interplay of the crosslink density, and the hydrophobicity of the polymeric network. For greater crosslink densities and more hydrophobic polymeric networks, the uptake of water by the biomaterial is decreased. Crosslink density and hydrophobic nature of the biomaterial are to a major extent determined by the structure and ratio of the precursor components. Therefore, water-uptake and mechanical performance of the biomaterial can be controlled and influenced by the appropriate choice of the precursor components.

[0106] In vertebroplasty, the uptake of water by the biomaterial should not exceed 7 weight % of the weight of the biomaterial before it is exposed to a storage period of 1 year at 37° C. in water or in a buffer solution. (Measurement according to ISO 10993-13:1995 (E) in phosphate buffered saline (PBS) 24±2 h after mixing of the precursor components). In the preferred embodiment, the water uptake is less than 5 weight %. In the most preferred embodiment, the water uptake is less than 3 weight %. Preferably each of the precursor components are substantially insoluble in water.

[0107] By measurement of Young's modulus E of polymeric networks, information can be obtained with regard to the stiffness of the polymeric network and as such relative information about the crosslink density of the network. The higher the Young's modulus E of a polymeric network, the higher the crosslink density within the network. Young's modulus E of the polymeric network can be increased by addition of additives. such as fillers. Nevertheless, the base value for Young's modulus E is determined by the chemical structure of precursor components and the ratio of their functional groups. After crosslinking, the structure and the ratio are responsible for a certain crosslink density within the polymeric network. Young's modulus E must achieve a predetermined value to be suitable for augmentation of hard tissue and particularly for the use in vertebroplasty.

[0108] Characteristics of Biomaterials

[0109] The ultimate compressive strength (measure for the load bearing capacity) of the biomaterial-is in a range of between 7 MPa to 50 MPa, preferably at least 10 MPa. Preferably in a range between 10 MPa and 40 MPa and even more preferably of between 15 MPa to 25 MPa. All of the measurerments are taken after storage of the samples at 37° C. for 10 days at a rate of 0.35 mm/s. Preferably the ultimate compressive strength of the biomaterial is 12 MPa after two days storage under dry conditions at 37° C. and reaches at least 5 MPa within the first 4 hours after injection into bone.

[0110] Preferably the Young's modulus E of the biomaterial (plus additives) is roughly in the same range as that of trabecular bone. Therefore, the precursor components are selected such that they cause Young's modulus E of the polymeric network of the biomaterial to be at least 15 MPa at 10% strain 10 days after mixing, preferably at least 20 MPa and even more preferably at least 25 MPa. Young's modulus E of the biomaterial, also measured after storage of 10 days at 37° C. at 0.35 mm/s and 10% strain, is in the range of between 20 MPa and 160 MPa, preferably in the range of between 60 MPa and 150 MPa and even more preferably in the range of between 100 and 140 MPa.

[0111] The injected mixture forms a composite material inside the vertebra. The composites are made of the biomaterial and the spongy tissue. Even a biomaterial with a relatively low Young's modulus E serves its purpose after injection into the spongy tissue. The compressive strength and Young's modulus E are measured according to ISO 5833: 1992 (E).

[0112] Biomaterials which show Young's moduli E at around 200 MPa can be used in vertebroplasty. However, the preferred use for such biomaterials is as cementation material, e.g. in joint replacement.

[0113] The elongation at break of the biomaterial is preferably in a range of between 20% to 60%, more preferably of between 25% and 55% and even more preferably of between 30% to 40% (storage of biomaterial before measurement 10 days 37° C.).

[0114] The biomaterials are stable over a period as set out in the ISO 10993-13:1995 (E), i.e. they do not degrade when stored one year at 37° C. in water or PBS within the margin of error of the respective measurement. At higher temperatures (around 70° C.), the stability of the biomaterial depends to a certain extent on the nature of the conjugated unsaturated group. Biomaterials made from acrylates are more temperature resistant than those made from itaconates, which are more temperature resistant than those made from itaconamides.

[0115] III. Methods of Forming Biomaterials

[0116] A. Storage

[0117] The first and second precursor components are preferably stored under exclusion of oxygen and at low temperatures, e.g. around +4° C., to avoid decomposition of the functional groups prior to use. Preferably the content of functional groups of each precursor component is measured immediately prior to use and the ratio of first and second precursor component (and other precursor component(s), when appropriate) is adjusted according to the predetermined equivalent weight ratio of the functional groups.

[0118] B. Preparation of Composition for Tissue Augmentation

[0119] A composition for use as tissue augmentation agent may be prepared by the following general method:

[0120] a) providing at least one first multifunctional precursor component comprising at least two nucleophilic groups;

[0121] b) providing at least one second multifunctional precursor component comprising at least two electrophilic groups capable of forming covalent linkage with the nucleophilic groups of step a) under physiological conditions;

[0122] c) mixing the first precursor component with at least one filler;

[0123] d) mixing the second precursor component with at least one filler;

[0124] e) filling the mixture obtained in step c) in a delivery device, preferably in a syringe;

[0125] f) filling the mixture-obtained-in step d) in a delivery device, preferably in a syringe.

[0126] The first and second precursor components and the fillers are sterilized prior to mixing. This preferably is done by sterile filtration of the precursor components and gamma irradiation of the fillers. The mixtures obtained in steps e) and f) can be stored over a prolonged time, preferably at low temperatures.

[0127] Immediately prior to application, the contents of the delivery devices obtained in step e) and f) are mixed with one another and secondly with a predetermined amount of sterilized base. A predetermined amount of base is filled in a delivery device, preferably another syringe. Tertiary alkyl-amine bases are most suitable in terms of gelation time (preferred gelation time is 10 to 15 min) and tolerance for deviation of amount. Preferably the bases are tributylamine, triethylamine, ethyldiisopropylamine, or N,N-dimethylbutylamine. The most preferred base for forming a biomaterial for hard tissue augmentation and vertebroplasty is tributylamine.

[0128] There are different modes of mixing the components. In one embodiment, three syringes, one containing the nucleophilic precursor, another containing the electrophilic precursor, and the third containing a base, can be interconnected using a three-way connector device. The contents of the syringes are mixed by being squeezed through a static mixture at the outlet of the three way connector device. The mixed components are injected directly at a site in need of treatment in the body by connecting the static mixer to an injection needle. Alternatively, the mixture is squeezed into another syringe which then is connected to the injection needle.

[0129] In a second embodiment, the mixture containing the electrophilic precursor, obtained in step d), is mixed with the base. This is preferably done by connecting the syringe containing the base to the syringe containing the electrophilic precursor through a connector device, which allows for syringe-to-syringe mixing of the respective contents. A static mixer may be part of the connector device. The mixing is complete when homogenous mixing is achieved, which optionally may be made noticeable by adding biocompatible coloring agents to the base and/or the mixture obtained step d). After mixing, one syringe contains a mixture of the base/second precursor/filler and the other syringe is empty. Then, the empty syringe is removed from the connector device and replaced by the syringe containing the nucleophilic precursor. Again, syringe-to-syringe mixing is one way to achieve homogeneous mixing of both contents. Subsequently the syringe containing the mixture is connected to the injection needle and the mixture is injected at the site of need in the body.

[0130] Alternatively, the syringe containing the base/second precursor/filler mixture and the syringe containing the first precursor/filler mixture, are interconnected through a two-way connector device comprising a static mixer at its outlet. The two-way connector device can be a double compartment syringe. The contents are mixed by squeezing the contents of the syringes through the static mixer. The static mixture is either directly connected to the injection needle or the mixture is squeezed in a further syringe, which then is connected to the injection needle.

[0131] C. Mixture of Precursor Components

[0132] The precursor component mixture has thixotropic properties. Thus it flows when subject to pressure, but recovers, nearly instantaneously, its original viscosity once pressure is removed. When a surgeon detects leakage from the vertebra by X-ray analysis during injection he/she immediately stops pressing the plunger of the syringe, and as a result the mixture stops flowing. Injection will be continued at another location in the vertebra (usually several needles are inserted into one vertebra prior to injection). The material starts being injectable upon a pressure of 4 Pa, preferably however at a higher pressure, such as around 10 Pa.

[0133] The mixture is of low viscosity prior to reaching the gel point so that the mixture flows, penetrates and distributes easily and evenly inside the spongy part of the vertebra.

[0134] D. Crosslinking Reaction Between Nucleophilic and Electrophilic Groups

[0135] After injection, the mixed precursor components crosslink (thus harden) within the next two to four hours to such an extent that the biomaterial can withstand loads to the extent that the patient can stand up and walk. The viscosity profile of the biomaterial takes these requirements into account in that the viscosity only increases slightly the first eight to fifteen minutes after mixing of the precursor components (before reaching the gel point) and then increases exponentially after that. The precursor mixture reaches its gel point at around eight to fifteen minutes, preferably at around twelve minutes. This gives the surgeon sufficient time for the operation. The biomaterial reaches its ultimate strength within 10 days, preferably 5 days after mixing.

[0136] The crosslinking of the first and second precursor component at the site of application is associated with only moderate heat development. The tissue at the site of application is much less harmed by injection of the composition than by injection of PMMA.

[0137] Michael-Type Reaction

[0138] The first and the second precursor components preferably react by a 1,4 addition reaction of a nucleophile on a conjugate unsaturated system. This reaction is referred to as a Michael-type reaction or Michael addition reaction. The reaction mechanism could be purely polar, or proceed through a radical-like intermediate state(s). Lewis acids or bases or appropriately designed hydrogen bonding species can act as catalysts.

[0139] Michael-type addition to conjugated unsaturated groups can take place in substantially quantitative yields at physiological temperatures, in particular at body temperature but also at lower and higher temperatures than that. They take place in mild conditions with a wide variety of nucleophiles. The gel formation kinetics and the mechanical and transport properties of the product are tailored to the needs of the application.

[0140] Compared to the preparation of PMMA in the operating room, it is evident that preparation and handling of this composition-is faster, reproducible, more precise, and avoids health hazards for the people in charge of preparation of the mixture.

[0141] IV. Kits for Forming in Situ Crosslinkable Compositions

[0142] A kit containing at least a first and a second precursor component. The kit may also contain one or more devices, such as syringes, for administering the first and second components. The kit may contain a base for polymerizing the precursor component. Optionally, the first and/or the second precursor component(s) contain one or more additives and/or biologically active agents. The precursor components may be placed in the one or more devices prior to administration to a patient.

[0143] V. Uses for the Compositions

[0144] The multifunctional precursor components are selected and tailored to produce biomaterials with the desired properties. The precursor components are capable of in situ crosslinking at physiological temperature, to specific augmentation requirements. In the preferred embodiment, the biomaterials are used to augment hard tissues, such as bone. However, the precursor components can be tailored to produce biomaterials that are suitable for other types of tissue augmentation.

[0145] A. Hard Tissue Augmentation and Vertebroplasty

[0146] In the preferred embodiment, the in situ crosslinkable composition forms a biomaterial for augmenting hard tissue. In particular, the biomaterial may be used to augment at least one vertebra of the spine. The composition contains at least a first and a second precursor component. In one embodiment, the first precursor component is a thiolated cyclosiloxane derivative, and the second precursor component contains at least three acrylate groups and is a derivative of 1,1,1 tris(hydroxymethyl)propane, pentaerithritol, or triglycerol.

[0147] In the most preferred application, the composition is used in vertebroplasty. A preferred first precursor for this application is 2,4,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21), and a preferred second precursor component is trimethylolpropane triacrylate (28). Although additional components with electrophilic and/or nucleophilic groups can be included in the composition, the best results are obtained if the two components are used alone. Preferably the ratio of the equivalent weight of the functional groups in the two precursor components is from 0.8 to 1.1, and most preferably the ratio is between 0.9 and 1.0.

[0148] Alternatively, the first precursor component is pentaerythritol tetrakis(2-mercaptoproprionat) (26), and the second precursor component is trimethylolpropane triacrylate (28). The ratio of the equivalent weight of the functional groups in the two precursor components is about 1.

[0149] Other suitable compositions for vertebroplasty and hard tissue augmentation contain a thiolated cyclosiloxane derivative, in particular 2,4,6,8-20. Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21), as the first component, and a molecule containing itaconate or itaconamide groups, in particular N,N′,N″,N′″-tetrakis(1-hydrogen-itaconyl)-triethylenetetraamine (32), itaconate derivatives of 1,1,1 tris(hydroxymethyl)propane and triglycerol molecules, and mixtures thereof, as the second component. Preferably, the second component is 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33), Triglycerol-penta(1-n-butyl itaconate) (29), 1,1,1 tris(hydroxymethyl)propane-tris(1-n-butyl itaconate) (30), or Pentaerithritol-tetra(1-n-butyl itaconate) (31).

[0150] B. Medical Indications Other Than Hard Tissue Augmentation and Vertebroplasty

[0151] Tissue augmentation is one of the possible treatments for urinary incontinence in women. There the biomaterial is placed at the base of the bladder to provide sphincter support by enhancing urethal compression. For such applications, the biomaterial must be softer and more elastic than the biomaterials used in hard tissue augmentation. For example, the Young's modulus E should range between 0.5 MPa to 4 MPa at 10% strain and 0.35 mm/s. In contrast to treatments for hard tissue, the prevention of swelling is not important because the surrounding tissue can stretch more than hard tissue, but biomaterials that swell too much will not be acceptable even for soft tissue applications. Thus, for soft tissue applications, such as the treatment of urinary incontinence, the up-take of water by the biomaterial should not exceed 20 weight %.

[0152] a. Modifications to First and Second Precursor Components

[0153] Although the biomaterials as described herein lose some of their stiffness simply due to the fact that an X-ray contrast agent is not needed any longer (the operation is done under camera control) the combination of the precursor components often leads to polymeric networks and biomaterials which are too stiff and hard for soft tissue applications. Therefore for treatments of soft tissue, at least one of the first or second precursor components should to be replaced by a molecule which by its structure and functionality leads to softer biomaterials. In one embodiment, the second precursor molecule is modified to comply with the needs of urological bulking whereas the first precursor component remains unaltered (i.e. the first precursor is the same as the first precursor used in hard tissue augmentation). Alternatively, the first precursor component is modified and the second precursor remains unaltered (i.e. the second precursor is the same as the second precursor used in hard tissue augmentation).

[0154] In a preferred embodiment the second precursor component is a derivative of polypropylene that contains two conjugated unsaturated groups. Particularly preferred are diacrylate polypropylene, such as polypropylene oxide diacrylate with n=12 (35), diitaconamide polypropylene, such as polypropylene α,ω bis (1-propylene itaconamide) with n=6 or 300, acrylamide polypropylene, such as polypropyleneoxide α, ω (bis (1-propylene itaconamide) (37) and derivatives thereof.

4TABLE 4Modified Second Precursor Componentsfor Soft Tissue Applications

[0155] The molecular weight of the molecules are preferably in a range of between 800 and 3000 g/mol, preferably of between 900 and 2600 g/mol and even more preferably of between 1200 and 2400 g/mol.

[0156] In a preferred embodiment, a biomaterial for soft tissue augmentation is formed from at least a first precursor component, which is a multifunctional thiolated cyclohexane derivative, mercaptoalkylether of pentaerithritol, 1,1,1 tris-(hydroxy-methyl)propane and 1,1,1 tris-(hydroxy-methyl)propanol containing at least three alkylether chains with end-standing thiol groups and at least a second precursor component, which is diacrylate-, diacrylamide- or diitaconamide polypropylene or derivatives thereof. In particular, such a biomaterial could be used for urological bulking.

[0157] b. Additives

[0158] The composition may also contain thixotropic agents, such as silica to prevent leakage and uncontrolled flow in a range of between 0.1 to 10% weight percent of the total weight of the composition, preferably in a range of between 1 to 5 weight % and even more preferably between 1.5 and 3 weight %.

[0159] The compositions may also contain bioactive factors, which can diffuse slowly from the biomaterial and thus helping the tissue to regenerate and heal. In such cases, the biomaterial works as both an augmentation material composition-and as a drug delivery matrix. The bioactive factors may be-growth factors, preferably those from the TGF beta superfamily, PTH and PDGF.

[0160] c. Characteristics of Biomaterials for Soft Tissue Augmentation

[0161] The Young's modulus E of the compositions for soft tissue applications is between 0.5 and 4 MPa, and the gel point is between 20 and 40 min. The gel point is important since the injection of the material cannot be done as quickly as in vertebroplasty. The biomaterial has a water uptake of under 20% of the total weight of the composition. The biomaterial is stable for at least 1 year at 37° C. At higher temperatures the itaconamides and itaconates tend to be more stable than the acrylates.

[0162] Other augmentation applications are possible as e.g. in cosmetic surgery. For example, the biomaterial can be made softer by further increasing the length of the alkyl chains of one of the precursor components or by using first and second precursor components which both have increased chain length and thus are made suitable for wrinkle augmentation.

EXAMPLES

[0163]

5

Measurements:

Instrument
Parameter

Viscosity
Bohlin Instruments
Stress ramp: 0.1 Pa to 100 Pa at

CVO 120
25° C.

Gel point
Bohlin Instruments
Frequency: 1H; Temperature:

CVO 120
37° C.; Strain: 0.1; Initial stress

0, 1 Pa; Gap: 100 μm; continuous

oscillation

Compression
ASTM F-451-99a;
if not indicated otherwise:

strength +
MTS Synergie 100
velocity: 0.35 mm/s; maximal

Young's
(1kn-cell)
force: 950 N; sample size: 12 mm

modulus E

height, 6 mm diameter;

Measurement of force

and deformation; Calculation of

stress = force/area, strain = ΔL/L,

B = stress/strain.

Example 1

Synthesis of 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl Itaconate)

[0164] A. Two Step Synthesis Via Coupling Agent

[0165] Three different procedures may be used in the first step of this synthesis.

[0166] Step 1: 4-hydrogen-1-methyl itaconate (first possibility)

[0167] 50.7 g (0.32 mol) of dimethyl itaconate and 25.0 g (0.13 mol) of toluene-4-sulfonic acid monohydrate were dissolved in 25 ml of water and 180 ml of formic acid in a 500 ml round bottom flask, equipped with a reflux condenser and a magnetic stirring bar. The solution was brought to a light reflux by immersing the flask in an oil bath at 120° C. and was stirred for 15 min. Then, the reaction was quenched by pouring the slightly yellow, clear reaction mixture into 200 ml of ice water while stirring. The resulting clear aqueous solution was transferred to a separation funnel, and the product was extracted with six 100 ml portions of dichloromethane. The combined organic layers were dried over Na2SO4, and the solvent was removed by rotary evaporation, yielding 22.2 g (44.8%) of raw product. The raw product was distilled under reduced pressure, yielding 11.7 g of a clear and colorless oil. According to 1H NMR analysis, the product consisted of 4-hydrogen-1-methyl itaconate (92%), 1-hydrogen-4-methyl itaconate (ca. 3%), and dimethyl itaconate (ca. 5%). See H.-Z. Pan, Y. Yan, L. Tang, Z.-Q. Wu, F.-M. Li, Macromol. Rapid Commun. 21, 567-573 (2000)

[0168] Step 1: 4-hydrogen-1-methyl Itaconate (Second Possibility)

[0169] 102.1 g (0.65 mol) of dimethyl itaconate and 35.0 g (0.18 mol) of toluene-4-sulfonic acid monohydrate were dissolved in 50 ml of water and 250 ml of formic acid in a 1000 ml round bottom flask, equipped with a reflux condenser, a thermometer, and a magnetic stirring bar. The solution was brought to a light-reflux by immersing the flask in an oil bath at 120° C. and was stirred for 45 min. Then, the reaction was quenched by pouring the slightly yellow, clear reaction mixture into 300 g of ice while stirring. The resulting clear aqueous solution was transferred to a separation funnel and the product was extracted with three 200 ml portions of dichloromethane. The combined organic layers were dried over MgSO4, and the solvent was removed by rotary evaporation, yielding 64.5 g of raw product. Extracting the aqueous layer once more with 200 ml of dichloromethane yielded another 6.4 g of raw product. A typical acidic smell indicated the presence of some formic acid in the fractions, which was removed by dissolving the combined fractions in 150 ml of dichloromethane and washing twice with 50 ml of saturated aqueous NaCl solution. Drying the organic layer with MgSO4 and evaporating the solvent yielded 60.1 g of a clear and colorless oil, which was distilled under reduced pressure, yielding 55.3 g of a clear and colorless oil. According to 1H NMR analysis the product consisted of 4-hydrogen-1-methyl itaconate (91%), 1-hydrogen-4-methyl itaconate (ca. 5%), and dimethyl itaconate (ca. 4%).

[0170] Step 1: 4-hydrogen-1-methyl Itaconate (Third Possibility)

[0171] 176 g (1.15 mol) of dimethyl itaconate were dissolved in 90 ml of water and 318 ml of formic acid and the mixture was heated to 60-65° C. and stirred at reduced pressure (300-250 mbar) for 4 days. After four days, GC analysis showed a conversion of 71.5%. Then, the pressure was reduced to 200-100 mbar and 170 ml of solvent was distilled off. The reaction mixture was cooled to 20° C., diluted with 350 ml water and 710 ml saturated aqueous NaCl solution, and extracted with three 350 ml portions of dichloromethane. The combined organic layers were concentrated to 15% of their original volume and 1.06 l of saturated aqueous NaHCO3 solution was added while stirring. The organic layer containing 28.7 g of unreacted dimethyl itaconate was discarded, and the aqueous layer was extracted with three 350 ml portions of dichloro-methane, removing another 3.5 g of unreacted dimethyl itaconate. The aqueous layer was reacted with 140 ml of 32% aqueous HCl and extracted with three 350 ml portions of dichloromethane, which, upon evaporation of the solvent, yielded 89.8 g (55%) of 4-hydrogen-1-methyl itaconate in 98.3% purity (GC).

[0172] Step 2: 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl Itaconate) (33)

[0173] 75.0 g (0.39 mol) of N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide hydrochloride was suspended in 300 ml of dichloromethane and 10.47 g (0.078 mol) of 1,1,1-tris-(hydroxymethyl)-propane and 0.95 g (7.8 mmol) of 4-(dimethylamino)-pyridine were added. After evacuating the reactor and flushing with nitrogen, the suspension was cooled to 2° C. and 56.0 g (0.39 mol) of 4-hydrogen-1-methyl itaconate dissolved in 100 ml of dichloromethane was added at such a rate that the temperature of the reaction mixture remains <5° C. Then, the solution, which had become clear, was stirred overnight and extracted with two 300 ml portions of saturated aqueous NaHCO3 solution, two 300 ml portions of 1 M hydrochloric acid, and with 300 ml of water. Colored byproducts were removed by a plug filtration over 40 g of silica gel and the solvent was evaporated, yielding 37.2 g of the desired product as an orange oil. Column chromatography over silica gel afforded the pure product was as a pale yellow oil. Molecular weight 512.54; 5.85 meq/g C═C

[0174] B. Two Step Synthesis Via Chlorination

[0175] Step 1: 4-hydrogen-1-methyl Itaconate

[0176] See synthesis of Step 1 described above.

[0177] Step 2: 1-methyl Itaconyl Chloride

[0178] 7.14 g (46 mmol) of 4-hydrogen-1-methyl itaconate were weighed into a 50 ml two-neck round bottom flask, equipped with a reflux condenser, a septum and a magnetic stirring bar. 5 ml of dry diethyl ether, 1 drop of pyridine and 5 ml (69 mmol) of thionyl chloride were added. T he resulting solution was brought to reflux and stirred for 15 min. Then the oil bath was removed and a light argon stream was led through the reaction mixture in order to remove HCl and SO2. The last traces of these gases and the solvent were removed by distillation under membrane pump vacuum. The resulting yellow oil was distilled under reduced pressure. A clear and colorless oil distilled at 66-68° C./8-9 mbar. The IR spectrum showed carbonyl bands for a saturated acid chloride (1804 cm−1) and a conjugated ester (1724 cm−1). 1H NMR analysis showed the product to consist of 1-methyl itaconyl chloride (89%), 4-methyl itaconyl chloride(ca. 4%), and dimethyl itaconate (ca. 7%). See H.-Z. Pan, Y. Yan, L. Tang, Z.-Q. Wu, F.-M. Li, Macromol. Rapid Commun. 21, 567-573 (2000).

[0179] Step 3: 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl Itaconate) (33)

[0180] 2.64 g (19.7 mmol) of 1,1,1-tris(hydroxymethyl)propane was dissolved in 20 ml of dry 1,4-dioxane and 55 ml of dry dichloromethane were added. The solution was cooled with an ice bath and 10.4 g (64.1 mmol) of 1-methyl itaconyl chloride in 5 ml of dry dichloromethane were added dropwise in 2 min. and the mixture was stirred for 10 min. Then, 7.10 g (70.2 mmol) triethylamine dissolved in 20 ml of dry dichloromethane were added at such a rate that the temperature of the reaction mixture remained below 5° C. (ca. 45 min.). After addition was complete, stirring was continued for 1 hr., after which the ice bath was removed and the reaction mixture brought to a mild reflux and was stirred for another hour. Then the ammonium salts were removed by filtration over ca. 1 cm of neutral Al2O3 and the solvents were rotavaped off the filtrate. The oil was dissolved in diethyl ether and washed with 50 ml of 3% aqueous HCl, twice with 50 ml of saturated aqueous NaHCO3, and once with 50 ml of water. The organic layer was dried with MgSO4 and the solvent was removed by rotary evaporation and 18 mg of MEHQ were added. The resulting greenish brown, clear oil was purified by column chromatography over silica gel (column height ca. 45 cm, ø 5 cm, eluent hexane/ethyl acetate 1/1 @ 16-18 ml/min.) The product was recovered as a pale yellow oil, yield 5.49 g (55%).

[0181] C. One Step Synthesis Via Transesterification; Synthesis (C)

[0182] 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33)

[0183] 7.14 g (0.053 mol) of 1,1,1-tris(hydroxymethyl)propane, 30.03 g (0.190 mol) of dimethyl itaconate, 9.19 g (0.048 mol) of toluene-4-sulfonic acid monohydrate, and 56 mg of 2,6-di-tert-butyl-p-cresol were weighed into a 100 ml round bottom flask, equipped with a Dean Stark trap. The flask was heated to 100° C. and methanol was distilled off under reduced pressure. After 6 hrs. the reaction mixture was dissolved in 25 ml of toluene and the volatiles were removed by rotary evaporation. The resulting clear, amber colored mixture was poured into 60 ml of 1 M aqueous NaHCO3 and 100 ml of diethyl ether were added to dissolve the product. The organic layer was washed with 60 ml of 1 M aqueous NaHCO3 and 60 ml of water, dried with Na2SO4 and the solvent was removed by rotary evaporation, yielding 27.5 g (86%) of raw product. 14.3 g of the raw product were purified by column chromatography over Silicagel 60 with 2/1 hexane/ethyl acetate as eluent. After the excess of dimethyl itaconate had eluted, the eluent was changed for a 1/1 hexane/ethyl acetate mixture and 4.48 (31%) of 1,1,1-tris(1-methyl-itaconoxymethyl)propane were recovered.

Example 2

Synthesis of Triglycerol-penta(1-methyl Itaconate) (29)

[0184]

[0185] 1.25 g (5.2 mmol) of triglycerol, 5.41 g (36.0 mmol) of 4-hydrogen-1-methyl itaconate, and 0.45 g (3.6 mmol) of 4-(dimethylamino)-pyridine were dissolved under an Ar atmosphere in 20 ml of dry chloroform and cooled to 1° C. 7.09 g (36.9 mmol) of N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide hydrochloride was dissolved in 40 ml of dry chloroform and added dropwise at such a rate that the temperature of the reaction mixture remains <5° C. Then the reaction mixture was allowed to slowly warm up to room temperature and stirred overnight. The resulting clear, yellow solution was washed with 50 ml of saturated aqueous NaHCO3 solution, 50 ml of 1 M aqueous KHSO4 solution, 50 ml of saturated aqueous NaHCO3 solution, and 50 ml of saturated aqueous NaCl solution, dried over MgSO4, and filtered over ca. 3 cm of silica gel and Celite 545. Evaporation of the solvents yielded 2.56 g (57%) of the desired product. IR analysis confirmed the complete conversion of the OH groups. M=870.78; 5.74 meq/g C═C.

Example 3

Synthesis of 1,1,1-tris(hydroxymethyl)propane-tris(1-n-butyl Itaconate)

[0186] Step 1: 4-hydrogen-1-n-butyl Itaconate

[0187] 104.7 g (0.43 mol) of di-n-butyl itaconate and 3.93 g (0.021 mol) of toluene-4-sulfonic acid monohydrate were dissolved in 140 ml of formic acid in a 500 ml round bottom flask, equipped with a reflux condenser, a thermometer, and a magnetic stirring bar. 30 ml of water were added and the resulting solution was heated to 66° C. by immersing the flask in an oil bath at 72° C. and was stirred at that temperature for 48 hrs. Then, the reaction was quenched by pouring the slightly yellow, clear reaction mixture into 600 ml of ice water while stirring. The resulting light yellow emulsion was transferred to a separation funnel and the product was extracted by washing three times with 200 ml of dichloromethane. The combined organic layers were washed with 100 ml of saturated aqueous NaCl solution and dried over Na2SO4.Removal of the solvent by rotary evaporation yielded 75.3 g of raw product. According to 1H NMR analysis the raw product consisted for 81% of 4-hydrogen-1-n-butyl itaconate, for ca. 4% of 1-hydrogen-4-n-butyl itaconate, and for ca. 15% of di-n-butyl itaconate. To the raw product 250 ml of saturated aqueous NaHCO3 solution and 17.6 g of NaHCO3 were added, yielding a hazy, red solution, which was washed 3 times with 100 ml of diethyl ether. To the clear, red aqueous layer KHSO4 was added until the pH has dropped from 8.5 to 3.0 and it was washed twice with 100 ml of dichloromethane. Then more KHSO4 was added until the pH value is 2.2 and the solution was washed again twice with 100 ml of dichloromethane. The yellow organic layer was washed with 50 ml of saturated aqueous NaCl solution and dried over MgSO4. Evaporating the solvent yielded 53.6 g (67%) of a clear, yellow oil, which, according to 1H NMR analysis, consisted for 95% of 4-hydrogen-1-n-butyl itaconate and for ca. 5% of 1-hydrogen-4-n-butyl itaconate.

[0188] Step 2: 1,1,1-tris(hydroxymethyl)propane-tris(1-n-butyl Itaconate) (30)

[0189] 2.00 g (14.9 mmol) of 1,1,1-tris-(hydroxymethyl)-propane, 11.3 g (59.0 mmol) of N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide hydrochloride, and 0.43 g (3.5 mmol) of 4-(dimethylamino)-pyridine were suspended in 150 ml of dry dichloromethane under an Ar atmosphere. The suspension was cooled to 1° C. and 9.65 g (51.8 mmol) of 4-hydrogen-1-n-butyl itaconate dissolved in 80 ml of dry dichloromethane were added dropwise at such a rate that the temperature remains below 2° C. After complete addition the clear, yellow reaction mixture was allowed to warm up to room temperature and stirred for another hour. After filtration and removal of the solvent, 100 ml of diethyl ether were added and the solution was washed with 50 ml of saturated aqueous NaHCO3 solution, 50 ml of 3% hydrochloric acid, and 25 ml of saturated aqueous NaHCO3 solution with 25 ml of water. Drying the organic layer with MgSO4 and evaporation of the solvent yielded 7.93 g (80%) of the product as a reddish brown oil. Molecular weight 638.75 g/mol; 4.70 meq/g.

Example 4

Synthesis of Pentaerythritol-tetra(1-n-butyl itaconate) (31)

[0190]

[0191] 1.53 g (11.2 mmol) of pentaerythritol, 12.0 g (62.8 mmol) of N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide hydrochloride, and 0.45 g (3.7 mmol) of 4-(dimethylamino)-pyridine were suspended in 100 ml of dry dichloromethane under an Ar atmosphere. The suspension was cooled to 1° C. and 10.0 g (53.9 mmol) of 4-hydrogen-1-n-butyl itaconate dissolved in 40 ml of dry dichloromethane were added dropwise at such a rate that the temperature remained below 2° C. After complete addition the clear, yellow reaction mixture was allowed to warm up to room temperature in about one hour. Then the solvent was evaporated, 100 ml of diethyl ether were added and the solution was washed with 50 ml of saturated aqueous NaHCO3 solution, 50 ml of 1.0 M aqueous KHSO4 solution, 40 ml of saturated aqueous NaHCO3 solution with 10 ml of water, and 50 ml of water. Drying the organic layer with Na2SO4 and evaporation of the solvent yielded 9.81 g (103%) of the desired product as a clear, brown oil. Molecular weight=880.92 g/mol; 4.54 meq/g C═C

Example 5

Synthesis of N,N′,N″,N′″-tetrakis(1-methyl-itaconyl)-triethylenetetraamine (32)

[0192] Step 1: N,N′,N″,N′″-tetrakis(1-hydrogen-itaconyl)-triethylenetetraamine

[0193] 3.30 g (22.6 mmol) of triethylenetetraamine were dissolved in 200 ml of water and the solution was cooled in an ice bath. Under vigorous stirring 18.73 g (167 mmol) of itaconic anhydride dissolved in 50 ml of dichloromethane were added dropwise in 90 min., at such a rate that the temperature remained between 4 and 6° C. During addition the pH of the reaction mixture was kept at 9.5 by addition of 4 M aqueous NaOH. After addition was complete, the reaction mixture was transferred to a separation funnel and the layers were separated. The aqueous layer was acidified with concentrated hydrochloric acid (pH 2), washed with 100 ml of dichloromethane and left standing at 4° C. to crystallize. The crystalline material was filtered off and dried under vacuum. Yield: 5.46 g (41%).

[0194] Step 2: N,N′,N″,N′″-tetrakis(1-methyl-itaconyl)-triethylenetetraamine (32)

[0195] 5.4 ml (74 mmol) of thionylchloride were added slowly to 100 ml of ice cold methanol. This mixture was added to a slurry of 5.39 g (9.1 mmol) of N,N′,N″,N′″-tetrakis(1-hydrogen-itaconyl)-triethylenetetraamine. The resulting yellow suspension was brought to reflux and stirred for four hours, during which the reaction mixture became clear. Evaporation of the volatiles yielded 4.30 g (73%) of N,N′,N″,N′″-tetrakis(1-hydrogen-itaconyl)-triethylenetetraamine, as identified by IR and 1H NMR. molecular weight =659.68 g/mol; 6.15 meq/g C═C.

Example 6

Synthesis of Trimethylolpropane Tris[poly(propyleneglycol) Itaconamide Terminated]Ether (34)

[0196]

[0197] 10.2 g (53.1 mmol) of N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide hydrochloride and 0.40 g (3.3 mmol) of 4-(dimethylamino)-pyridine were suspended in 50 ml of dry dichloromethane under an Ar atmosphere. The suspension was cooled in an ice bath to 2° C. and 6.09 g of trimethylolpropane tns[poly(propyleneglycol), amine terminated] ether dissolved in 50 ml of dry dichloromethane were added, yielding a clear and colorless solution. 7.15 g (49.6 mmol) of 4-hydrogen-1-methyl itaconate dissolved in 40 ml of dry dichloromethane were added dropwise at such a rate that the temperature remains below 4° C. After complete addition the clear, light yellow reaction mixture was stirred for another hour at 2-3° C. and was then allowed to warm up to room temperature and stirred for one more hour. The solution was transferred to a separation funnel and washed with 50 ml of saturated aqueous NaHCO3 solution, 50 ml of 1 M aqueous KHSO4 solution, and 50 ml of saturated aqueous NaHCO3 solution with 50 ml of saturated aqueous NaCl solution. Drying the organic layer with Na2SO4 and evaporation of the solvent yielded 12.8 g of the product as a clear, reddish brown oil, the structure of which is confirmed by IR, 1H NMR, and 13C NMR spectroscopy.

Example 7

Synthesis of Pentaerythritol Tetrakis(3-mercaptopropyl)ether (27)

[0198] Step 1: Pentaerythritol tetraallylether

[0199] 30.7 g (0.12 mol) of pentaerythritol triallylether was dissolved in 100 ml of dry THF and 4.4 g (0.18 mol) of NaH was added in small portions while stirring. After gas evolution had ceased, 16 ml (0.18 mol) of allyl bromide was added and the reaction mixture was stirred overnight at room temperature. In order to drive the reaction to completion, it was subsequently brought to reflux and stirred for 1 hr. The precipitated salts were removed by filtration over ca. 1 cm of Celite 545 and the solvent and excess allyl bromide were evaporated, yielding 35.3 g (99.5%) of a pale yellow oil. The raw product was dissolved in 100 ml of diethyl ether and washed subsequently with 50 ml of 0.1 M aqueous KHSO4 and 50 ml of saturated aqueous NaHCO3 solution. Drying the organic layer with MgSO4 and evaporation of the solvent yielded 34.4 g (97%) of the pure product.

[0200] Step: 2 Pentaerythritol Tetrakis(3-thioacetopropyl)ether

[0201] 24.8 g (83.8 mmol)of pentaerythritol tetraallylether, 28.8 g (0.378 mol) of thioacetic acid, and 1.08 g (6.6 mmol) of AIBN were dissolved in 100 ml of THF, cooled to 2° C. and degassed by 3 cycles of evacuation and purging with Ar. The solution was brought to reflux and stirred for 17 hrs. Then, another 6.12 g (80.4 mmol) of thioacetic acid, and 0.51 g (3.1 mmol) of AIBN were added and the reaction mixture was stirred under reflux for another 22 hrs., after which the solvent was evaporated. Yield: 55.5 g (110%) of a yellow oil. According to 1H NMR analysis, 98.4% of the allyl groups had been converted.

[0202] Step: 3 Pentaerythritol tetrakis(3-mercaptopropyl)ether (27)

[0203] 7.02 g (0.011 mol) of pentaerythritol tetrakis(3-thioacetopropyl)ether was dissolved in 30 ml of ethanol. The solution was degassed by 3 cycles of evacuation and purging with Ar and heated in a 60° C. oil bath. 30.3 g (0.27 mol) of a 50% aqueous KOH solution was added dropwise in ca. 30 min. After another 30 min. stirring the reaction mixture was allowed to cool down, poured into 100 ml of degassed 1 M aqueous KHSO4 solution and-brought to pH 2 by adding saturated aqueous KHSO4 solution. The product was recovered by extraction with three 80 ml portions of diethyl ether. The combined organic layers were washed subsequently with 100 ml of saturated aqueous NaHCO3 solution and 100 ml of saturated aqueous NaCl solution and dried over Na2SO4. Evaporating the solvent yielded 4.1 g (89%) of an amber colored oil. IR analysis showed the complete disappearance of the carbonyl signal at 1687 cm−1.

Example 8

Synthesis of 1,1,1-Trimethylolpropane tris(3-mercaptopropyl)ether

[0204]

[0205] The first synthesis reaction was similar to the three steps in Example 7, however starting from 1,1,1-trimethylolpropane diallyl ether in step 1, which yielded in 1,1,1-trimethylolpropane tris(3-mercaptopropyl)ether.

[0206] A second synthesis procedure, was started from 1,1,1-tri-methylolpropanol in step 1 of Example 7. The other steps were performed similarly:

Example 9

Synthesis of 1,2,4-Tris(2-mercaptoethyl)cyclohexane

[0207]

[0208] 22.2 g (0.137 mol) of 1,2,4-trivinylcyclohexane, 37.2 g (0.49 mol) of thioacetic acid, and 1.4 g (8.5 mmol) of AIBN were dissolved in 140 ml of THF under an Ar atmosphere. The solution was brought to reflux and stirred for 18 hrs. After cooling down, the solution was stirred for 30 min. with Dowex WGR2 resin, in order to bind the excess of thioacetic acid and filtered. The solvent was removed by rotary evaporation and the product was dispersed in a solution of 79.3 g (1.98 mol) of NaOH in 170 ml of water under an Ar atmosphere. The dispersion was heated to 80° C. and stirred at that temperature for 4 hrs. After cooling to room temperature, concentrated hydrochloric acid was added slowly until the pH is 1 and the product was extracted with three 150 ml portions of dichloromethane. The combined organic layers were washed with 150 ml of 5% aqueous NaHCO3 solution and with 100 ml of water and dried with MgSO4. Removing the solvent yielded 27.3 g (76%) of the desired product.

Example 10

Synthesis of 2,4,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21)

[0209]

[0210] 23.7 g (0.069 mmol) of 2,4,6,8-Tetravinyl-2,4,6,8-tetramethylcyclotetrasiloxane, 25.2 g (0.331 mmol) of thioacetic acid, and 0.91 g (5.5 mmol) of AIBN were dissolved in 1110 ml of THF and flushed with nitrogen. The reaction mixture was heated to reflux for 15 hrs., after which it was cooled down to 40° C. and the THF was distilled off at reduced pressure. The resulting oil was dissolved in 100 ml of ethanol and at room temperature 29 ml of 50% aqueous NaOH were added, causing the temperature to rise to 48° C. After the addition was complete, the mixture was heated to reflux for 4 hrs. and the mixture was concentrated to 25% of its original volume at reduced pressure. After cooling to room temperature, 187 g of 30% H2SO4 in water were added slowly. The product was extracted from the mixture with three 100 ml portions of dichloromethane. The combined organic layers were washed twice with 180 ml of saturated aqueous NaHCO3 solution. Evaporating the solvent and drying on the rotavap at 10 mbar for 5 hrs. yielded 32.9 g (99%) of a viscous, yellow oil. Molecular weight =480.99 g/mol; 8.82 meq/g SH.

Example 11

Synthesis of Tetra(3-mercaptopropyl)silane

[0211]

[0212] The above procedure (Example 10) was used, but starting from tetraallyl silane. Tetra(3-mercaptopropyl)silane was synthesized, with a 94% yield.

Example 12

Synthesis of Tri(3-mercaptopropyl) Trimetylolpropane (25)

[0213] Step 1: Trimethylolpropane Triallylether

[0214] 48 ml (0.224 mol) of trimethylolpropane diallyl ether was slowly added to 120 ml THF and 6.5 g (0.271 mol) of NaH in a 500 ml round bottom flask. Slow development of bubbles indicated the start of the redox reaction between R—OH and Na. The solution was stirred overnight. 23 ml (0.032 mol) of allyl bromide was dropped to the solution. Mixture got warm and milky and the suspension was left overnight. The solution was transferred into a separation funnel and the product was washed with H2O, KHSO4, again H2O and NaCl. The organic layer was dried with MgSO4 and evaporated.

[0215] Step 2: Radical Addition of Thiacetic Acid to Allylic Groups

[0216] 41 g (0.164 mol) of trimethylolpropane triallylether, 36.7 ml (0.59 ml) of thioacetic acid and 1.67 g of AIBN were dissolved in 150 ml of THF in a 500 ml round bottom flask, equipped with reflux condenser, thermometer and magnetic stirrer bar. The solution was stirred at 65° C. for 18 h. To bind thiacetic acid, 37 g of Dowex WGR-2 was added. After 30-40 min of stirring, the solution was filtrated and dried with MgSO4.

[0217] Step 3: Tri(3-mercaptopropyl)trimethylolpropane

[0218] 96 g (2.4 mol) of NaOH and thiolacetyl ester were added in 200 ml of water, stirring at 80° C. for 4 h. By addition of 200 ml of HCl, the suspension was acidiphicated. 200 ml of chloroform was added and after 30 min transferred to a separation funnel. The solution was washed four times with water and 2 times with brine. The organic layer was dried with MgSO4 and the solvent was removed by rotary evaporation, yielding 38.1 g

Example 13

Synthesis of Polypropylenoxid-α,ω-bis(1-propylitaconylamide) (36)

[0219] Step 1: Polypropylenoxid-α,ω-bis(1-propylitaconylamide) Free Acid

[0220] 15.5 g (0.138 mol) itaconic anhydride was dissolved in 100 ml CH2Cl2. The solution was filtered to remove traces of insoluble itaconic acid and was slowly added to 75 ml (0.0375 mol) of Jeffamine D-2000 in 400 ml borate buffer (0.1 M, 9.5pH with NaOH) in a II round bottom flask, equipped with reflux condenser, thermometer, magnetic stirrer bar and dropping funnel. The pH was kept at 9.5 by addition of NaOH. After stirring the reaction mixture overnight, 200 ml of water was added and the resulting suspension was transferred to a separation funnel and the product was extracted by washing five times with 250 ml of diethyl ether and by washing two times with 200 ml of brine. The organic layer was dried over MgSO4 and the solvent was removed by rotary evaporation, yielding 63.1 g (76%) of product.

[0221] Step 2: Polypropylenoxid-α,ω-bis(1-propylitaconylamide) (36)

[0222] 8.2 ml (0.112 mol) of thionyl chloride was slowly added to 100 ml of icecooled 1-propanol from a dropping funnel. 62 g (0.028 mol) of PPOdiItAm free acid, dissolved in 200 ml of primary alcohol, was added. Then the solution was brought to a light reflux and was stirred for 4 h. The solution was concentrated by rotary evaporation and 100 ml of chloroform was added. The solution was transferred to a separation funnel and the product was washed twice with 150 ml of saturated aqueous NaHCO3 solution and twice with 150 ml of brine. The organic layer was dried with MgSO4 and the solvent was removed by rotary evaporation, yielding 49.8 g (81%) of the derived product.

Example 14

Polypropylenoxid-α,ω-bis(1-propyl-acrylamideamide) (37)

[0223] 100 ml (0.049 mol) of Jeffamine D-2000 and 11.4 g (0.107 mol) of Na2CO3 were added to 200 ml chloroform in a 500 ml round bottom flask, equipped with reflux condenser, magnetic stirrer, thermometer and dropping funnel. 8.7 ml (0.107 mol) of acryloyl chloride, dissolved in 20 ml chloroform was added slowly to the solution and stirred for 2 days. The solution was filtrated and transferred to a separation funnel and the product was washed twice with concentrated aqueous NaHCO3 solution and twice with brine. The organic layer was dried with MgSO4, and the solvent was removed by rotary evaporation, yielding 72.3 g (68%) of slightly yellow oil.

Examples 15-26

Formation of Compositions for Use in Vertebroplasty

[0224] The silica used in Examples 15-26 is commercially available from Cabot GmbH under the tradename CAB-O-SIL M-5; it is hydrophil with an average particle size of 12 nm. 100 μm BaSO4 is commercially available from Riedl-de Haehne (No. 11432 in Sigma Aldrich catalogue) or from Sachtleben Chemie GmbH under the trade name Sachtoperse HP, HU-N. Trimethylolpropane triacrylate is commercially available in purities above 95% from Sartomer

[0225] Mixing of the dispersions/mixtures (both terms are used synonymously herein) was performed by a Ultra-Turrax T25 basic equipped with S25N-10G dispersion stick. Mixing took place at level 6 until homogeneity was achieved.

[0226] As used herein, the term “component” includes the reactive species and any additive added beforehand. For example, “thiol component” or “itaconate component” indicates the respective species of thiol or itaconate itself plus fillers, X-ray agents, bases such as SiO2 or BaSO4 or triethylamine.

[0227] As used herein, weight % indicates weight percentages of the total weight of the composition.

Example 15

Formation of Composition from Trimethylolpropane Triacrylate and 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane

[0228] Formation of Bulk Material

[0229] 2 g of BaSO4 and 0.74 g of SiO2 were dispersed in 20 g of trimethylolpropane triacrylate (28) until homogeneity (“acrylate component”). 2 g of BaSO4 and 0.74 g of SiO2 were dispersed in 20 g of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21) and mixed until homogeneity (“thiol component”).

[0230] 150 mg tributylamine was added to 1.16 g of the “acrylate component” and mixed until homogeneity to form the “acrylate/tributylamine component”. Subsequently, 1.5 g of the “thiol component” was mixed with the “acrylate/tributylamine component” until homogeneity was achieved.

[0231] Characteristics of Resulting Biomaterial

[0232] Weight % SiO2: 3.1; Weight % BaSO4: 8.38

[0233] Gelation time: about 10 minutes at 37° C.; Stability: ≧1 year at 37° C.;

[0234] Ultimate compressive strength 27 MPa;

[0235] Young's modulus E: 110 MPa at 10% strain and 0.35 mm/s;

[0236] Water uptake 0.2%.

Example 16

Formation of Composition from 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane and Trimethylolpropane Tris [poly(propylenglycol), Amine Terminated]Ether (“TPGA”)

[0237] Formation of Bulk Material

[0238] 300 mg of SiO2 and 2000 mg of BaSO4 were dispersed in 6000 mg (49.86 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21) (“thiol component”). Then 637.3 mg (3.99 mol —NH2) of trimethylolpropane tris [poly(propylenglycol), amine terminated]ether (“TPGA”) was added to the thiol component and mixed thoroughly (“thiol component”/TPGA mixture).

[0239] 110 mg of SiO2 and 1406 mg of BaSO4 were dispersed in 8531 mg (49.86 mmol C═C) of 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (“itaconate component”) (33).

[0240] Subsequently the “thiol component”/TPGA mixture and the “itaconate component” were combined and mixed until homogeneity was achieved.

[0241] Characteristics of Resulting Biomaterial

[0242] Weight % SiO2: 2.16; Weight % BaSO4: 17.94;

[0243] Weight % of sum of donor and acceptor: 76.55; weight % base: 3.36.

[0244] Gelation time: about 13 minutes at 37° C.; Stability: ≧1 year at 37° C.;

[0245] Young's modulus E 35 MPa at 10% strain and 0.35 mm/s; Water uptake 1.8%;

[0246] Viscosity up to 400 s 3Pa/s.

Example 17

Formation of Composition from Trimethylolpropane Triacrylate and 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane

[0247] Formation of Bulk Material

[0248] 2800 mg (26.11 mmol —C═C—) of commercially available trimethylolpropane triacrylate (28) was mixed homogenously with 100 mg of (1.06 mmol —NH2) triethylamine (“acrylate component”). Then, 3200 mg (26.11 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21) (“thiol component”) was added to the “acrylate component” and the dispersion was mixed until homogeneity was reached.

[0249] Characteristics of Resulting Biomaterial

[0250] Gelation time: about 10 min at 37° C.;

[0251] Stability: ≧1 year at 37° C.; Young's modulus E: 60 MPa at 10% strain and

[0252] 0.35 mm/s; Water uptake 2%.

Example 18

Formation of Composition from 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) and 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane

[0253] Formation of Bulk Material

[0254] 800 mg of (6.653 mmol —C═C—) 1,1,1-tris(hydroxymethyl)propanetris(1-methyl itaconate) (33) was mixed homogenously with 33 mg (0.33 mmol —NH2) of triethylamine (“itaconate component”).

[0255] Subsequently, 1000 mg (8.316 mmol —SH) of 2;3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21) was added to the “itaconate component” and mixing was continued until homogeneity was achieved.

[0256] Characteristics of Resulting Biomaterial

[0257] Gelation time: about 15 min at 37 ?C;

[0258] Stability: ≧1 year at 37° C.; Young's modulus E: 15 MPa at 10% strain and 0.35 mm/s; Water uptake 2.3%.

Example 19

Formation of Composition from 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) and 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclo-tetrasiloxane

[0259] Formation of Bulk Material

[0260] 3570 mg (23.56 mmol —C═C—) of 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33) was mixed homogenously with 92 mg (0.94 mmol —NH2) of triethylamine (“itaconate component”). 2829 mg (23.56 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclo-tetrasiloxane (21) was added to the “itaconate component” and mixing was continued until homogeneity was reached.

[0261] Characteristics of Resulting Biomaterial

[0262] Gelation time: about 14 min at 37° C.; Stability: ≧1 year at 37° C.; Young's modulus E: 25 MPa at 10% strain and 0.35 mm/s; Water uptake 2.4%.

Example 20

Formation of Composition from Tetrakis(1-methyl-itaconyl)-triethylenetetraamine and 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclo-tetrasiloxane

[0263] Formation of Bulk Material

[0264] 21 mg (0.21 mmol —NH2) of triethylamine were added to and mixed with 567 mg (3.94 mmol —C═C—) of tetrakis(1-methyl-itaconyl)-triethylenetetraamine (32) (“itaconamide component”). 420 mg (3.94 mmol —SH) 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclo-tetrasiloxane-(21) was added to the “itaconamide component” and mixing was continued until homogeneity was reached.

[0265] Characteristics of Resulting Biomaterial

[0266] Stability: ≧1 year at 37° C.; Young's modulus E: around 200 MPa at 10% strain and 0.35 mm/s.

Example 21

Formation of Composition from Triglycerol-penta(1-methyl itaconate) and 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane

[0267] Formation of Bulk Material

[0268] 434.5 mg (2.945 mmol —C═C—) of Triglycerol-penta(1-methyl itaconate) (29) was mixed with 12.6 mg (0.124 mmol) of triethylamine (“itaconate component”). 300 mg (2.945 mmol —SH) 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21) was added to the “itaconate component” and mixed until homogeneity was achieved.

[0269] Characteristics of Resulting Biomaterial

[0270] Gelation time: about 30 min at 37° C. Young's modulus E: 30 MPa at 10% strain and 0.35 mm/s. Stability: ≧1 year at 37° C.

Example 22

Formation of Composition from 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane/TGPA and 1,1,1-tris(hydroxymethyl)propane-tris(1-n-butyl Itaconate)

[0271] Formation of Bulk Material

[0272] 34 mg of SiO2 and 289 mg of BaSO4 were dispersed homogenously in 1200 mg (11.09 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21). Then 84 mg (0.83 mmol —NH2) of trimethylolpropane tris [poly(propylenglycol), amine terminated]ether (TPGA) was added to the latter and the dispersion was mixed thoroughly (“thiol component”).

[0273] 63 mg of SiO2 and 531 mg of BaSO4 were dispersed homogenously in 2360 mg (1.09 mmol —C═C—) of 1,1,1-tris(hydroxymethyl)propane-tris(1-n-butyl itaconate) (30) (“itaconate component”). The “thiol component” and the “itaconate component” were combined and mixing of the combined mixture was continued until homogeneity was reached.

[0274] Characteristics of Resulting Biomaterial

[0275] Weight % SiO2: 2.13; Weight % BaSO4: 17.98; Weight % of sum of donor and acceptor: 78.05; weight % base: 1.84.

[0276] Gelation time: 13 min at 37° C.; Stability ≧1 year at 37° C.; Young's modulus E: 30 MPa at 10% strain and 0.35 mm/s; Water-uptake 2.0%.

Example 23

Formation of Composition from 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane/TPGA and Trimethylolpropane Tris [poly(propyleneglycol), Itaconamide Terminated]

[0277] Formation of Bulk Material

[0278] 20 mg of SiO2 and 169 mg of BaSO4 were dispersed homogenously in 700 mg (6.47 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21). In a next step 49 mg (0.49 mmol —NH2) of trimethylolpropane tris [poly(propylenglycol), amine terminated]ether (TPGA) was added to the dispersion which was then mixed thoroughly. (“thiol component”).

[0279] 48 mg of SiO2 and 398 mg of BaSO4 were homogenously dispersed in 1767 mg (6.47 mmol —C═C—) of Trimethylolpropane tris [poly(propyleneglycol), itaconamide terminated] (34) (“itaconamide-component”). In the next step, the “thiol component” and the “itaconamide-component” were combined and mixing of the combined mixture was continued until homogeneity was reached.

[0280] Characteristics of Resulting Biomaterial

[0281] Weight % SiO2: 2.16; Weight % BaSO4: 17.99; Weight % of sum of donor and acceptor: 78.3; weight % base: 1.56.

[0282] Gelation time: 13 min at 37° C.; Stability: ≧1 year at 37° C.;

[0283] Young's modulus E: 25 MPa at 10% strain and 0.35 mm/s; Water uptake 5%.

Example 24

Formation of Composition from Pentaerithritol tetrakis(2-mercaptoproprionate) and Trimethylolpropane Triacrylate

[0284] Formation of Bulk Material

[0285] 0.406 g of SiO2 and 3.456 mg of BaSO4 were homogenously dispersed in 15 g (119.62 mmol —SH) of pentaerithritol tetrakis(2-mercaptoproprionate) (26) (“thiol component”).

[0286] 0.387 g of silica and 2.9 g of BaSO4 were dispersed in 12.91 g (119.62 mmol C═C) of trimethylolpropane triacrylate (28). Then 0.362 g (3.58 mmol —NH2) of triethylamine was added and mixed thoroughly (“acrylate component”) The acrylate component and the thiol component were combined and the combined mixture was mixed until homogeneity was reached.

[0287] Characteristics of Resulting Biomaterial

[0288] Weight % SiO2: 2.24; Weight % BaSO4: 17.94; Weight % of sum of donor and acceptor: 78.8; weight % base: 1.02.

[0289] Young's modulus E 43 MPa at 10% strain and 0.35 mm/s;

[0290] Young's modulus E, uniaxial compressive strength and Poisson's ratio at 0.3% strain and 0.005 mm/s: Young's modulus E 33.3 MPa, Poisson's ratio: 0.47; uniaxial compressive strength of 11.3 MPa.

Example 25

Formation of Composition from 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane/TPGA and 1,1,1-tris(hydroxymethyl) Propane-tris(1-methyl Itaconate)

[0291] Formation of Bulk Material

[0292] 117 mg of SiO2 and 978 mg of BaSO4 were dispersed homogenously in 4000 mg (28.27 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21). Subsequently 349 mg (2.2 mmol —NH2) trimethylolpropane tris [poly(propylenglycol), amine terminated]ether (TPGA) was added to the dispersion which was mixed thoroughly (“thiol component”). 115 mg of SiO2 and 965 mg of BaSO4 were dispersed homogenously in 4289 mg of (22.62 mmol —C═C—) of 1,1,1-tris(hydroxymethyl) propane-tris(1-methyl itaconate) (33) (“itaconate component).

[0293] The “thiol component” were added to the “itaconate component” and mixing of the combined mixture was continued until homogeneity was achieved. Ratio 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33) to 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21)=0.8.

[0294] Characteristics of Resulting Biomaterial

[0295] Weight % SiO2: 2.15; Weight % BaSO4: 17.97; Weight % of sum of donor and acceptor: 76.66; weight % base: 3.23.

[0296] Gelation time: 15 min at 37° C.; Young's modulus E: 30 MPa at 10% strain and 0.35 mm/s; Stability ≧1 year at 37° C.

Example 26

Formation of Composition from 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane/TPGA and 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl Itaconate)

[0297] Formation of Bulk Material

[0298] 187 mg of SiO2 and 978 mg of BaSO4 were dispersed homogenously in 4000 mg (28.27 mmol —SH) of 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21). Subsequently, 349 mg (2.2 mmol —NH2) trimethylolpropane tris [poly(propylenglycol), amine terminated]ether (TPGA) was added to the latter and the dispersion was mixed thoroughly (“thiol component”).

[0299] 184 mg of SiO2 and 965 mg of BaSO4 were dispersed homogenously in 4289 mg (22.62 mmol —C═C—) of 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33) (“itaconate component). The “itaconate component” and “thiol component” were combined and mixing of the combined mixture was continued until homogeneity was achieved.

[0300] Ratio 1,1,1-tris(hydroxymethyl)propane-tris(1-methyl itaconate) (33) to 2,3,6,8-Tetra(2-mercaptoethyl)-2,4,6,8-tetramethylcyclotetrasiloxane (21)=0.8.

[0301] Characteristics of Resulting Biomaterial

[0302] Weight % SiO2: 3.39; Weight % BaSO4: 17.74; Weight % of sum of donor and acceptor: 75.68; weight % base: 3.19.

[0303] Gelation time: 15 min at 37° C.; Young's modulus E: 37 MPa at 10% strain and 0.35 mm/s; Stability ≧1 year at 37° C.

Example 27

Testing of Augmentation Effect on Vertebrae Using Composition of Example 24

[0304] The technique consists of injecting a biomaterial percutaneously into the diseased vertebra to augment its mechanical properties. Vertebroplasty was reported to provide the patient a rapid relief from pain that is most probably due to the immediate mechanical stabilization of existing microfractures. The most commonly used biomaterial for this application is PMMA. PMMA stiffness is significantly higher than the stiffness of healthy vertebral trabecular bone. Injection of PMMA alters therefore the load distribution across the endplate and has been shown to increase the incidence of fractures in adjacent vertebrae. In addition, the consequences of bone remodeling associated with this new load distribution remain unknown.

[0305] The objective of this study was to quantify the augmentation of the mechanical properties of vertebral cancellous bone using a compliant biomaterial. An osteoporotic vertebra of a dead human body was injected and the vertebra was filled completely with composition of Example 24.

[0306] Materials and Methods

[0307] Fresh vertebral bodies were obtained post-mortem from 5 donors and stored at −26° C. After isolation from soft tissues, the vertebral bodies were fixed with cement and a pair of cylindrical cores of 8 mm diameter were extracted from each vertebra with a diamond-coated coring tool. The ends of the cylinders were cut planoparallel with a diamond-coated band saw to provide a length of 10 mm. The marrow of the samples was then removed using 3 successive baths in a smooth soap solution followed by rinsing under water and ultrasound shaking. A preliminary study verified that the morphological and mechanical properties of the cancellous bone specimens were not altered by this procedure (n=15, p>0.63). All specimens were imaged in a μCT system (μCT 40, Scanco Medical, Switzerland) at 20 μm resolution and the datasets subjected to 3D morphological analysis. A mold was designed and built in order to inject a biomaterial into the trabecular structure of the cored and marrow extracted specimens which minimized the presence of air bubbles. For gripping, both extremities of the specimen were embedded into PMMA cylinders of 12 mm length. One specimen of each pair was randomly assigned to be augmented.

[0308] Elastic modulus, ultimate stress (strength), ultimate strain and total energy at ultimate stress were calculated from the resulting stress-strain curves. Volume fraction and tissue density of the control specimens were obtained by Archimedes' method. Student's t-tests were applied to compare the morphological and mechanical properties between the control and augmented specimen groups.

[0309] Results

[0310] The range of bone volume fraction extended from 3.5 to 19.5%. Mean volume fraction of the control and the augmented group was not statistically different (n=24, p>0.43). The structural model index (SMI), the degree of anisotropy and the connectivity density were also comparable in the control and the augmented group (p>0.1). Since the distribution of morphological properties was bimodal, the results are presented for two separate ranges of volume fraction (VF): a low VF (n=5) and a high VF range (n=19) with a cutoff value of 10.0%. As shown in FIG. 1a, the mean elastic modulus of the augmented specimens was not significantly higher than the one of the controls for both low and high VF(p>0.13). For low VF, the ultimate stress increased from 0.69±0.50 to 1.93±0.99 MPa due to augmentation (+180%), and for high VF it increased from 4.63±0.7 to 5.71±1.4 MPa (+23%). The increase in strength was found to be significant in both ranges (p<0.037). The other post yield properties, ultimate strain and total energy were also found to be higher in the augmented group (see FIG. 1b).

[0311] Discussion

[0312] Augmentation of the mechanical properties of vertebral trabecular bone by injection of a compliant biopolymer was evaluated in vitro. The use of an almost incompressible biomaterial with an Young's modulus E as low as 33 MPa was shown to enhance significantly the postyield properties and preserve elasticity of the trabecular structure. The biopolymer provides a gain in strength of approximately 1 MPa, which implies an improved relative augmentation for bone with low VF. The injection of marrow-free cylindrical specimens under laboratory conditions represents a reproducible, but best case scenario for bone augmentation. Nevertheless, the selected biopolymer may stabilize the microfractures existing in diseased vertebra and prevent the accumulation of further damage without altering significantly the stress distribution under physiological loading.

Example 28

Testing of Augmentation Effect on Vertebrae Using Composition of Example 15

[0313] An osteoporotic vertebra of a dead human body was injected and the vertebra was filled completely with composition of Example 15.

[0314] A total of 84 cylindrical specimens (ø 8 mm, L=10 mm) were cored out under constant water irrigation from cadaveric human (three male and one female) thoracic and lumbar vertebrae with age ranging from 29 to 86 years. Half of the specimens were augmented with the composition of Example 15. Since there was no previous study investigating the fatigue behavior of human trabecular bone, a protocol was adapted from one described in the literature for bovine trabecular bone (Michel M. C. et al, 1993, Journal of Biomechanics, 26, 453-463). During mechanical testing, the specimens were immersed in Hank's balanced salt solution at 37° C.

[0315] Results

[0316] The results are presented in FIG. 2, showing the maximal applied stress S max divided by volume fraction FV as a function of the number of cycles to failure Nf. Smax was divided by FV to normalize the data since Smax is strongly dependant upon FV.

[0317] A comparison between the fatigue result of the augmented trabecular bone (augmented group) to non-augmented trabecular bone (control group) shows a substantial increase in the fatigue life of trabecular bone for the augmented group (see FIG. 2).

Example 29

Testing of Compressive Strength of Composition of Example 16 when Applied to Vertebra

[0318] An osteoporotic vertebra of a dead human body was injected and the vertebra was filled completely with composition of Example 16. The compressive strength of osteoporotic vertebra prior to augmentation (spongy part) was 0.7 at 0.03% strain and 0.027 mm/s. The compressive strength of vertebra (spongy part) with augmentation was 2.1 MPa at 0.03% strain and 0.027 mm/s.

Example 30

Composition for Use in Urological Bulking

[0319] 0.092 g of SiO2 was dispersed homogenously in 2.4 g (20.19 mmol —SH) of Tris(3-mercaptopropyl)trimethylolpropane (24). Then, 0.636 g (6.05 mol —NH2) of diethanolamine is added to the thiol/SiO2 dispersion and mixed thoroughly (“thiol component”).

[0320] 0.180 g of SiO2 was dispersed homogenously in 7.067 g (20.19 mmol —C═C—) of polypropyleneoxide α-ω-bis(1-propyl itaconamide) (36) (“itaconamide component”). The “thiol component” and the “itaconamide component” were combined and mixed until homogeneity was achieved.

[0321] Characteristics of Resulting Bioaterial

[0322] Weight % SiO2: 2.63; Gelation time: about 30 minutes at 37° C. At 70° C. the composition is stable for 60 days. The Young's modulus E at 0.1 strain is around 2 MPa; Water-uptake: 15%.

Example 31

Composition for Use in Urological Bulking

[0323] 0.070 g of SiO2 was dispersed homogenously in 2.400 g (19.14 mmol —SH) of pentaerythritol tetrakis(2-mercaptopropionate) (26) (“thiol component”). 0.400 g of SiO2 was dispersed homogenously in 15.074 g (33.49 mmol —C═C—) commercially available poly(propylene oxide) diacrylate (35) (Sigma). Subsequently 0.191 g (0.957 mmol —NH2) of Jeffamine D-400 was added to the acrylate/SiO2 dispersion and mixed thoroughly (“acrylate component”). The “thiol component” and the “acrylate component” were combined and mixing was continued until homogeneity was achieved.

[0324] Characteristics of Resulting Biomaterial

[0325] Weight % SiO2: 2.59; Gelation time: about 30 minutes at 37° C. At 37° C. the composition was stable for more than 250 days; Young's modulus E at 0.1 strain: 0.2 MPa. Water-uptake: 10%.

Example 32

Composition for Use in Urological Bulking

[0326] 0.030 g of SiO2 was dispersed homogenously in 1.100 g (11.64 mmol —SH) of 1,2,4-Tris(2-mercaptoethyl)cyclohexane (22) (“thiol component”).

[0327] 0.130 g of SiO2 was dispersed homogenously in 4.891, g (13.97 mmol —C═C—) of polypropyleneoxide α-ω-bis(1-propyl itaconamide) (36). In a next step 0.116 g (0.957 mmol —NH2) of Jeffamine D-400 was added to the itaconamide/SiO2 mixture and mixed thoroughly (“itaconamide component”). The “itaconamide component” and the “thiol component” were combined and mixing was continued until homogeneity was achieved.

[0328] Characteristics of Resulting Biomaterial

[0329] Weight % SiO2: 2.55; Gelation time: in about 30 minutes at 37° C. Stability ≧1 year at 37° C.; Young's modulus E at 0.1 strain is around 1 MPa. Water-uptake: 12%.

Example 33

Composition for Use in Urological Bulking

[0330] 0.070 g of SiO2 was homogenously dispersed in 2.2 g (17.27 mmol —SH) of Tris(3-mercaptopropyl)trimethylolpropane (24). Subsequently 0.544 g (5.18 mol —NH2) of diethanolamine was added to the thiol/SiO2 mixture and mixed thoroughly (“thiol component”). 0.140 g of SiO2 was homogenously dispersed in 5.182 g (17.27 mmol —C═C—) of polypropyleneoxide α-ω-bis(acrylamide) (37) (“acrylamide component”). The “thiol component” and the “acrylamide component” are combined and mixing continued until homogeneity.

[0331] Characteristics of Resulting Biomaterial

[0332] Weight % SiO2: 2.58; Gelation time: in about 30 minutes at 37° C. At 70° C. the composition is stable for 60 days; Young's modulus E at 0.1 strain is around 2 MPa. Water-uptake: 17%.

[0333] It is understood that the disclosed invention is not limited to the particular methodology, protocols, and reagents described as these may vary. It is also to be understood that the terminology used herein is for the purpose of describing particular embodiments only, and is not intended to limit the scope of the present invention which will be limited only by the appended claims.

[0334] Those skilled in the art will recognize, or be able to ascertain using no more than routine experimentation, many equivalents to the specific embodiments of the invention described herein. Such equivalents are intended to be encompassed by the following claims.

	Number	Date	Country
	60366712	Mar 2002	US
	60408077	Sep 2002	US

Compositions for tissue augmentation

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